Siproteron asetatning yon ta'siri - Side effects of cyproterone acetate

The yon effektlar ning siproteron asetat (CPA), a steroidal antiandrogen va progestin, shu jumladan uning tez-tez va kam uchraydigan yon ta'sirlari o'rganilgan va tavsiflangan. Umuman olganda yaxshitoqat qilingan va dozasi qanday bo'lishidan qat'i nazar, progestin yoki antiandrogen sifatida ishlatilganda yon ta'sirining engil profiliga ega estrogen kabi etinilestradiol yoki estradiol valerat ayollarda.^[1]^[2] CPA ning yon ta'siriga quyidagilar kiradi gipogonadizm va bog'liq alomatlar kabi demaskinizatsiya, jinsiy funktsiya buzilishi, bepushtlik va osteoporoz; ko'krak kabi o'zgarishlar ko'krak bezi, kattalashtirish va jinekomastiya; hissiy kabi o'zgarishlar charchoq va depressiya; va boshqa yon ta'sirlar vitamin B12 etishmasligi, zaif glyukokortikoid effektlar va jigar fermentlarining ko'tarilishi.^[3] Vazn yig'moq yuqori dozalarda ishlatilganda CPA bilan yuzaga kelishi mumkin.^[4]^[5] CPA ning ba'zi bir yon ta'sirlarini yaxshilash yoki uni oldini olish uchun estrogen bilan birlashtirilsa to'liq oldini olish mumkin estrogen etishmovchiligi.^[6]^[7] Kam miqdoriy ma'lumotlar CPA ning ko'plab potentsial yon ta'sirida mavjud.^[8] CPA uchun birlashtirilgan tolerabilitatsiya ma'lumotlari adabiyotda mavjud emas.^[9]

Prostata saratoni bilan og'rigan keksa erkaklarda juda yuqori dozalarda CPA sabab bo'lishi mumkin yurak-qon tomir yon effektlar. Kamdan kam hollarda CPA ishlab chiqarishi mumkin qon pıhtıları, jigar shikastlanishi, haddan tashqari yuqori prolaktin darajasi, prolaktinomalar va meningioma. Ustiga to'xtatish yuqori dozalardan CPA ishlab chiqarishi mumkin buyrak usti etishmovchiligi kabi chekinish effekt.

Umumiy nuqtai

Yuqori dozali siproteron asetatning yon ta'siri
Chastotani	Tizim organlari sinfi	Yon ta'siri
Juda keng tarqalgan (≥10%)	Umumiy kasalliklar va ma'muriyat sayt shartlari	Bosh og'rig'i Charchoq
	Ruhiy kasalliklar	Libidoning pasayishi (erkaklar) Erektil disfunktsiya (erkaklar) Ejakulyatsiya hajmi kamayadi (erkaklar)
	Reproduktiv tizim va ko'krak bezi kasalliklari	Qayta tiklanadigan inhibisyon spermatogenez (erkaklar) Taqiqlash ovulyatsiya va qaytariladigan bepushtlik (ayollar)
	Gepatobiliyer kasalliklari	Jigar fermentlarining ko'payishi
Umumiy (-1% va <10%)	Metabolizm va ovqatlanishning buzilishi	Vazn yig'moq yoki yo'qotish (bilan bog'lash mumkin suyuqlikni ushlab turish )
	Ruhiy kasalliklar	Tushkun kayfiyat Bezovta
	Reproduktiv tizim va ko'krak bezi kasalliklari	Jinekomastiya (erkaklar) Ko'krak og'rig'i / sezgirligi Noqonuniy hayz ko'rish
	Umumiy kasalliklar va ma'muriyat sayt shartlari	Charchoq Issiq chaqmoqlar Terlash
	Nafas olish, ko'krak qafasi va mediastinal buzilishlar	Nafas qisilishi
	Oshqozon-ichak traktining buzilishi	Bulantı Gastrointestinal shikoyatlar
Noyob (≥0,1% va <1%)	Ruhiy kasalliklar	Libidoning pasayishi (ayollar)
Noyob (≥0,1% va <1%)	Teri va teri osti to'qimalarining buzilishi	Rash
Kamdan kam (-0,01% va <0,1%)	Immunitet tizimining buzilishi	Yuqori sezuvchanlik reaktsiyalari (toshma, qichishish, nafas qisilishi )
Kamdan kam (-0,01% va <0,1%)	Ruhiy kasalliklar	Libidoning ko'payishi (ayollar)
Juda kam (<0,01%)	Neoplazmalar benign va zararli	Xavfsiz va jigarning xavfli o'smalari
	Mushak-skelet va biriktiruvchi to'qima kasalliklari	Osteoporoz
	Yurak-qon tomir kasalliklari	Tromboembolik hodisalar Taxikardiya
	Reproduktiv tizim va ko'krak bezi kasalliklari	Galaktore
	Umumiy kasalliklar va ma'muriyat sayt shartlari	Uyquning buzilishi
Belgilanmagan	Saralanmagan	Anemiya Meningioma Giperprolaktinemiya Prolaktinoma Qorin bo'shlig'iga qon quyilishi Ko'krak zo'riqishi Hayz ko'rish Kam Dismenoreya Vaginal oqindi Terining rangsizlanishi Stretch belgilari Noyob Jigarning toksikligi (shu jumladan sariqlik, gepatit, jigar etishmovchiligi )
Izohlar: Yon ta'siri siproteron asetat (Androkur) dozasi kuniga 10 dan 300 mg gacha. Manbalar: Shablonga qarang.

Seksual-HOrmonal Surveillance Study (SEHOST) da siproteron asetatning yon ta'siri.
Yon ta'siri	Erkaklar (kuniga 136 mg)^[a] (n = 1248) (%)	Ayollar (kuniga 18 mg)^[a] (n = 1258) (%)	Jami (kuniga 77 mg)^[a] (n = 2506) (%)
Jigar fermentlarining ko'payishi^[b]	12.5	3.6	9.6
Jinekomastiya, ko'krak og'rig'i	4.9	1.0	2.9
Ortiqcha vazn, vazn yig'moq	0.9	4.1	2.5
Bosh og'rig'i, O'chokli	–	3.4	1.7
Depressiya, tashvish, kabuslar, kayfiyat o'zgarishi	1.0	1.8	1.4
Gastrointestinal disfunktsiya	0.2	2.3	1.2
Qalqonsimon bezning buzilishi	0.2	1.8	1.0
Teri o'zgaradi (pigmentatsiya, xloasma, boshqalar)	0.3	1.4	0.8
Shish	–	1.1	0.6
Adrenal etishmovchilik yoki giperplaziya	0.2	0.8	0.5
Charchoq, sustlik, beparvolik	0.6	0.6	0.6
Alopesiya, soch o'sishi	0.2	0.2	0.2
Kattalashtirilgan astma xuruji stavkalar	–	0.3	0.2
Osteoporoz	0.2	0.08	0.2
Ko'pincha hujumlarga moyil	0.2	0.2	0.2
Qandli diabet	0.08	0.08	0.08
Jami (ko'tarilgan jigar fermentlarini hisobga olmaganda)	9.0	19.1	14.0
Izohlar: SEXual-HOrmonal Surveillance STudy (SEHOST) ma'lumotlari, uzoq muddatli farmakoepidemiologik faol kuzatuvni o'rganish. Namuna 3 yoshdan 75 yoshgacha bo'lgan erkak va ayollarni o'z ichiga olgan erta balog'at yoshi, giperandrogenizm, jinsiy og'ish va / yoki transgenderizm; prostata saratoni kiritilmagan. Manbalar: Shablonga qarang.

Erkaklarda estradiol undesilatning siproteron asetat bilan yon ta'siri
Yon ta'siri	Estradiol undesilat 100 mg / oy i.m. (n = 96)		Siproteron asetat 100 mg / kun og'iz orqali (n = 95)
Yon ta'siri	n	%	n	%
Jinekomastiya *	74	77.1%	12	12.6%
Ko'krak bezi *	84	87.5%	6	6.3%
Jinsiy quvvatsizlik	"Ikkala guruhning deyarli barcha bemorlarida uchraydi"
Oyoq shishishi *	17	17.7%	4	4.2%
Tromboz	4	4.2%	5	5.3%
Yurak-qon tomir o'limi	2	2.1%	2	2.1%
Boshqalar o'lim	1^a	1.0%	0	0%
Izohlar: 191 yilda 6 oy davomida 51 yoshdan 88 yoshgacha bo'lgan erkaklar prostata saratoni. Izohlar: * = Guruhlar o'rtasidagi hodisalardagi farqlar statistik jihatdan ahamiyatli edi. ^a = Noma'lum sabablarga ko'ra. Manbalar: Shablonga qarang.

Gormonlarning past darajasi

CPA ning antandrogenik va antigonadotropik xususiyatlaridan kelib chiqadigan erkaklardagi nojo'ya ta'sirlarga jismoniy ta'sir kiradi demaskinizatsiya, jinsiy funktsiya buzilishi (shu jumladan libidoning yo'qolishi va erektil disfunktsiya ), bo'shashmaslik, nogiron spermatogenez, moyak atrofiyasi va qaytariladigan bepushtlik.^[10]^[11] CPA "shiddatli" bostirishga olib keladi deb ta'riflangan jinsiy aloqada bo'lish prostata saratoni bilan og'rigan erkaklarda erektil kuch, jarrohlik bilan solishtirganda kastratsiya.^[12] Ishlab chiqarishning bostirilishi tufayli estrogenlar, Birgalikda estrogen terapiyasiz yuqori dozali CPA-dan uzoq muddatli foydalanish rivojlanishiga olib kelishi mumkin osteoporoz ikkala jinsda ham.^[13] EBM ba'zida sabab bo'lishi mumkin ko'krak erkaklardagi o'zgarishlar, shu jumladan jinekomastiya (ko'krak rivojlanishi) va ko'krak bezi.^[10] Jinekomastiya darajasi 6 dan 30% gacha bo'lganligi haqida xabar berilgan.^[14]^[15]^[16]^[9] Galaktore (sut chiqishi) CPA ning kuchli progestogen ta'siridan kelib chiqqan holda erkaklarda ham bo'lishi mumkin.^[10] Erkaklarda CPA-dan foydalanish bilan bog'liq selülit, bu androgen etishmovchiligiga ham bog'liq.^[17]

Depressiya

CPA vaqti-vaqti bilan bog'liq bo'lgan depressiv kayfiyat o'zgaradi erkaklarda ham, ayollarda ham.^[18] Xuddi shunday depressiv o'zgarishlar kastratsiya paytida ham kuzatilgan va buning natijasi bo'lishi mumkin androgen etishmovchiligi erkaklarda.^[18] Katta tadkikotlarda, ikkala ayolda ham yuqori dozali CPAni androgenga bog'liq teri va soch sharoitlari uchun estrogen bilan birgalikda qabul qiladigan erkaklarda va yuqori dozada CPA qabul qiladigan erkaklarda yoki prostata kastratsiyasi bilan birgalikda 1 dan 10% gacha bo'lgan. saraton.^[3]^[19]^[20] Ammo ba'zi kichik tadkikotlarda nisbatan past va yuqori dozali CPA bilan ayollarda estrogen bilan birgalikda 20-30% gacha bo'lgan nisbatan yuqori depressiya qayd etilgan.^[21]^[22]^[23] Katta birida randomizatsiyalangan nazorat ostida sinov estrogen bilan birgalikda yuqori dozani (100 mg / kun) past dozali CPA (2 mg / kun) bilan to'g'ridan-to'g'ri taqqoslashni amalga oshirgan, depressiyaning umumiy darajasi 12,7% va stavkalar ikki guruh o'rtasida farq qilmadi.^[5] Depressiya bilan bir qatorda bo'lishiga qaramay, CPAni estrogen bilan birgalikda qabul qilgan ayollarda depressiya holatlari ba'zi tadqiqotchilar tomonidan "juda past" deb ta'riflangan bo'lib, ular androgenik simptomlarning yaxshilanishining ijobiy psixologik ta'siri bilan bog'liq bo'lishi mumkin.^[3]

Kognitiv va hissiy ta'sirlarni taqqoslaydigan tasodifiy boshqariladigan sinov GnRH agonistlari va prostata saratoni bilan kasallangan 82 erkakning CPA-si 6 oylik davolanishdan so'ng Depressiya Anksiyetesi Stress-21 (DASS-21) skorlari bo'yicha sezilarli farqni topmadi.^[24] Shu bilan birga, 62 kishining 12 oylik kuzatuvi CPA-da DASS-21 tomonidan o'lchangan emotsional tanglikning sezilarli darajada oshganligini aniqladi. hushyor kutish GnRH-agonist guruhlariga nisbatan guruhlar.^[25]^[26] Shunga qaramay, emotsional bezovtalikning o'rtacha darajasi odatdagi oraliqda qoldi.^[26]

Retrospektiv tadqiqotlar shuni ko'rsatdiki, depressiya darajasi CPA (8.3%) bilan solishtirganda ko'proq bo'lgan GnRH analoglari (2,2%) ikkalasi ham transgender ayollarda estrogen bilan birgalikda ishlatilganda, ammo ushbu tadqiqot kayfiyat bilan bog'liqligini nazorat qilmadi aralashtirib yuboradi.^[27] Transgender ayollarda o'tkazilgan yana bir retrospektiv tadqiqot Bek depressiyasini inventarizatsiya qilish II va boshqa tarozilarda psixologik farovonlik yoki estrogen va CPA yoki GnRH agonisti birikmasidan qoniqish borasida sezilarli farqlar mavjud emas.^[28] Transgender ayollarda gormonal terapiya, shu jumladan CPA ishlatilgan tadqiqotlar depressiv simptomlarning sezilarli darajada pasayishiga olib keldi.^[29]^[30]

Tug'ilishni nazorat qilish tabletkasi sifatida past dozali CPA va etinilestradiol kombinatsiyasini nisbatan kichik miqdordagi bir qator tadqiqotlarida depressiya tsikllarning 1,3 dan 4% gacha bo'lganligi haqida xabar berilgan.^[31] Bu boshqa progestinlarni o'z ichiga olgan tug'ilishni nazorat qilish tabletkalarida kuzatilgan kayfiyat o'zgarishi tezligiga (<3,5%) o'xshaydi.^[31] A farmakoepidemiologik ma'lumotlaridan foydalanib o'rganish Birlashgan Qirollik Umumiy amaliyot tadqiqotlari ma'lumotlar bazasi CPA o'z ichiga olgan tug'ilishni nazorat qilish tabletkalari bilan tushkunlik holatlari boshqa progestinlarni o'z ichiga olgan tug'ruq nazorat qilish tabletkalari bilan bir xil ekanligini aniqladi (IRR = 0.99).^[32] Menopoz simptomlarini davolash uchun past dozali CPA va estradiol valerat kombinatsiyasining klinik tadkikotlarida oldindan mavjud bo'lgan salbiy kayfiyat alomatlari sezilarli darajada yaxshilanganligi aniqlandi.^[33]

Yomonlashgan depressiv simptomlarning yon ta'siri bo'lishi mumkinligi sababli, depressiya tarixi bo'lgan odamlarda, ayniqsa og'ir bo'lsa, CPA-dan ehtiyotkorlik bilan foydalanish tavsiya etilishi mumkin.^[34]

Suyak yo'qotilishi

Androgen etishmovchiligini davolash, CPA yoki kabi dorilar bilan GnRH modulyatorlari yoki bilan orkiektomiya, erkaklarda ikkala androgen va estrogenlarning chuqur etishmasligiga olib keladi.^[35]^[36] Ushbu gormonlar, xususan estrogenlar, parvarish qilishda muhim ahamiyatga ega ekanligi ma'lum suyak mineral zichligi, erkaklarda ham, ayollarda ham.^[35]^[37] Natijada, androgenni yo'q qilish terapiyasi erkaklarda suyak mineral zichligining tez pasayishiga olib keladi va natijada olib kelishi mumkin osteopeniya yoki osteoporoz uzoq muddatli terapiya bilan.^[35]^[36]

Androgen etishmovchiligini davolash bilan bog'liq bo'lgan suyaklarning yo'qolishi odatda umurtqa pog'onasi, kestirib va bilak, ammo boshqa sohalarda ham bo'lishi mumkin appendikulyar skelet kabi femur bo'yni.^[35] Buni davolanishdan keyin bir yil ichida ko'rish mumkin va keyin ham davom etadi.^[35] Lomber orqa miya erkaklarda androgen etishmovchiligi terapiyasi bilan suyak zichligi yiliga 3 dan 7% gacha kamayishi aniqlandi.^[35] Androgen etishmovchiligini davolash ham kamayadi mushak massasi va bu tushishi mumkin bo'lgan tushish xavfini oshirishi mumkin suyak sinishi shuningdek to'g'ridan-to'g'ri suyak massasini kamaytiradi.^[35] Prostata saratoni bilan og'rigan erkaklarda suyak sinish xavfi, androgen etishmovchiligi terapiyasi 45% ga oshirilganligi taxmin qilinmoqda.^[35] Prostata saratoni bilan kasallangan erkaklarda osteoporoz bilan kasallanish 10 yil davom etgan androgenni yo'q qilish terapiyasidan so'ng 36% dan 80% gacha ko'payadi va shundan so'ng davolangan barcha erkaklarda osteopeniya yoki osteoporoz paydo bo'lishi kutilmoqda.^[38] Erkaklarda androgen etishmovchiligi terapiyasi bilan yuzaga keladigan suyaklarning yo'qolishi, paydo bo'lganlarga o'xshaydi postmenopozal ayollar.^[35]

Androgenlarni yo'q qilish terapiyasi osteoporozni keltirib chiqarishi ma'lum bo'lsa-da, CPA ning osteoporoz xavfi GnRH modulyatorlari yoki orkiektomiyaga qaraganda pastroq bo'lishi mumkin deb o'ylashadi.^[39] Bu CPA ning progestogen faolligi bilan bog'liq deb ishoniladi, bu esa inhibatsiyaga yordam beradi suyak rezorbsiyasi sabab bo'lgan jinsiy gormonlar etishmovchiligi.^[39] Ammo progestogen faollikning suyak sog'lig'iga foydali ta'sir ko'rsatishi haqidagi tushuncha ziddiyatli.^[40] Tushunchaning to'g'ri yoki yo'qligidan qat'i nazar, ish bo'yicha hisobotlar va ish qatori erkaklarda CPA terapiyasi bilan osteoporozning nashr etilgan.^[39]^[36] Bundan tashqari, dan foydalanish faqat progestogen bilan tug'ilishni nazorat qilish ayollarda, EBMga o'xshash progestinlar bilan medroksiprogesteron asetat, suyak mineral zichligini pasayishiga olib kelishi aniqlandi premenopozal ayollar.^[41]^[42]

Kaltsiy va D vitamini qo'shimchalar osteoporoz xavfini erkaklarda androgen etishmovchiligi terapiyasi bilan kamaytirishga yordam beradi.^[35]^[38] Bifosfonatlar androgen etishmovchiligi terapiyasi tufayli suyaklarning yo'qolishini va sinishlarini kamaytirish uchun ishlatilishi mumkin.^[35]^[38] Estrogenni almashtirish va selektiv estrogen retseptorlari modulyatorlari estrogenlar erkaklarda jinekomastiya keltirib chiqarishi va xavfini oshirishi mumkin bo'lsa-da, ishlatilishi mumkin erkak ko'krak bezi saratoni.^[35]^[38]^[37] Selektiv estrogen retseptorlari modulyatorlari 2 yillik terapiyadan so'ng erkaklarda androgen etishmovchiligi terapiyasi tufayli suyak yo'qotish tezligini 50% ga kamaytirishi aniqlandi.^[38] Shu bilan birga, selektiv estrogen retseptorlari modulyatorlari ushbu ko'rsatkich uchun ma'lum bo'lgan ushbu dori uchun eng samarali dorilar bo'lgan estrogenlarga qaraganda sezilarli darajada kam samarali deb ta'riflanadi.^[43]

Yuqori progestogen ta'sir

Prolaktin darajasi yuqori

CPA ortadi prolaktin darajalari va ishlab chiqarishi mumkin giperprolaktinemiya progestogen faolligi va natijada uning stimulyatsiyasi tufayli (prolaktin darajasi yuqori) gipofiz laktotroflar.^[44]^[45]^[46]^[47]^[48]^[49]^[50]^[51]^[52]^[53] Prolaktin darajasining oshishi CPA ning past, o'rta va yuqori dozalarida, estrogen bilan yoki bo'lmasdan sodir bo'lishi mumkin.^[3] Prolaktin darajasining ko'tarilishi ko'proq bo'lishi mumkin va giperprolaktinemiya KPA estrogen bilan birlashganda yuzaga kelishi mumkin, chunki estrogenlar va progestogenlar kombinatsiyasi odam bo'lmagan odamlarda prolaktin darajasining sinergik o'sishini ko'rsatadi primatlar.^[54]^[55]^[56] Giperprolaktinemiya CPA bilan rivojlanishi mumkin bo'lsa-da, prolaktin darajasi kamdan-kam hollarda normal fiziologik ko'rsatkichdan oshadi va CPA bilan prolaktin darajasining oshishi kamdan-kam hollarda klinik ahamiyatga ega.^[3]

Erkaklarda kuniga 10 mg dozada CPA prolaktin miqdorini 75% ga oshirishi aniqlandi.^[57]^[58]^[59] Boshqa bir ishda, kuniga 2 yoki 20 mg CPA ning kombinatsiyasi testosteron undecanoate erkaklarda prolaktin darajasining (+ 96%) o'rtacha o'sishiga olib keldi.^[60] 100 mg / kun oral CPA (+ 118%) bo'lgan erkaklarda prolaktin darajasining oshishi mushak ichiga 100 mg / oy bo'lganidan kamroq ekanligi aniqlandi estradiol undesilat (+192%).^[45] Yuqori dozaning kombinatsiyasi (kuniga 100 mg) etinilestradiol Transgender ayollarda yuqori dozada (100 mg / kun) oral CPA ning cisgender erkaklarga nisbatan giperprolaktinemiya xavfini 425 baravar (20%) ortishi haqida xabar berilgan.^[61] Shu bilan birga, xuddi shu rejimdan foydalangan holda o'tkazilgan boshqa tadqiqotlar giperprolaktinemiyaning past ko'rsatkichlarini aniqladi (masalan, yiliga 4-7%).^[62]^[63] Bir tadqiqotda prolaktin darajasi davolash boshlanganda 18 ng / ml, 3 oy davomida 100 mg / kun CPA dan keyin 23 ng / ml va 6 oydan 15 oygacha 100 mg / kun etinilestradiol va 19 dan 28 ng / ml gacha bo'lgan. Transgender ayollarda 100 mg / kun oral CPA.^[63]

Vaziyat sifatida giperprolaktinemiyaning asosiy belgisi gipogonadizm, bu prolaktinning antigonadotrop ta'siridan kelib chiqadi.^[53] Gipogonadizmga olib keladigan alomatlar kiradi amenore, menopoz belgilari kabi issiq chaqnashlar va qin quruqligi, jinsiy funktsiya buzilishi, bepushtlik, mushaklarning massasi kamayadi va suyak mineral zichligini pasayishi.^[53]^[64]^[65] Shu bilan birga, progestogen ta'siriga va ushbu faoliyat natijasida hosil bo'lgan kuchli antigonadotrop ta'siriga ko'ra CPA giperprolaktinemiya mavjud yoki yo'qligidan qat'iy nazar yon ta'sirga o'xshash alomatlarni keltirib chiqarishi mumkin.^[11]^[35]^[13]

Prolaktin qo'shimcha ravishda to'g'ridan-to'g'ri inhibitiv ta'sirga ega jinsiy istak erkaklarda gipogonadizmdan mustaqil.^[66]^[67]^[68] Giperprolaktinemiya va gipogonadizm bilan kasallangan erkaklarda jinsiy istak tiklanmaydi testosteronni almashtirish terapiyasi, ammo prolaktinni bostiruvchi dorilar yordamida tiklanadi.^[66]^[67] Aksincha, erektil disfunktsiya giperprolaktinemiya bilan kasallangan erkaklarda prolaktinning to'g'ridan-to'g'ri harakatlari tufayli emas, balki gipogonadizm tufayli hisoblanadi.^[66] Boshqa tomondan, prolaktin normal jinsiy aloqa uchun javobgar bo'lishi mumkin deb o'ylashadi refrakter davr erkaklarda va to'g'ridan-to'g'ri qobiliyatini inhibe qilishi mumkin orgazm.^[68]

Gipogonadizm va jinsiy funktsiya buzilishining alomatlaridan tashqari, giperprolaktinemiya sabab bo'lishi mumkin ko'krak kabi o'zgarishlar ko'krak og'rig'i, ko'krak kengayishi, jinekomastiya va galaktore.^[53]^[69]^[70] Giperprolaktinemiya bilan bog'liq bo'lgan ikkinchi galaktorea premenopozal ayollarda juda keng tarqalgan (80%), ammo postmenopozal ayollar va erkaklar kabi ostrogen darajasi past bo'lganlarda kam uchraydi.^[69] Jinekomastiya ham giperprolaktinemiyaga chalingan erkaklarda (23%) nisbatan past darajada uchraydi.^[69] Transgender ayollarda olib borilgan tadqiqotlar galaktore kasalligining past, ammo estrogen va CPA kombinatsiyasi bilan kasallanishini aniqladi.^[63]^[71]^[72]

Prolaktin darajasi oshadi buyrak usti androgenlari kabi dehidroepiandrosteron va dehidroepiandrosteron sulfat dan ishlab chiqarish va sekretsiyasini ko'paytirish orqali buyrak usti bezlari.^[73]^[74]^[75]^[76] Shu sababli giperprolaktinemiya simptomlarni keltirib chiqarishi mumkin giperandrogenizm kabi husnbuzar va hirsutizm ayollarda.^[53]^[77] Shu bilan birga, bunday alomatlar CPA bilan tavsiflanmaydi, buning o'rniga ushbu sharoitlar davolanadi; buni antandrogenik va glyukokortikoid CPA faoliyati.^[3] Bunday harakatlar orqali CPA to'g'ridan-to'g'ri androgenlarning ta'sirini bloklaydi va buyrak usti bezlaridan dehidroepiandrosteron sulfat sekretsiyasini bostirishi mumkin.^[3]^[78]^[79]^[7]

Miya shishi

Estrogen va CPA kombinatsiyasi kamdan-kam bo'lsa ham, odatda bir necha xil turdagi insidensiya va / yoki og'irlashishi bilan bog'liq. benign (saraton bo'lmagan) miya shishi, eng muhimi prolaktinomalar va meningioma.^[80]^[81] Prolaktinomalar - bu yaxshi xulqli o'smalar gipofiz bu sir prolaktin, va ularning bir nechta turlaridan biri yashirin gipofiz adenomalari.^[63]^[61] Ular ishlab chiqarishi mumkin giperprolaktinemiya (prolaktin darajasi g'ayritabiiy darajada yuqori) simptom bo'lib, bu ko'pincha ularga olib keladi tashxis.^[63]^[61] Menenjiyoma odatda yaxshi xulqli o'smalardir miya pardalari, membranalar bu o'rab oladi miya va orqa miya.^[82]^[83] Menenjiom bilan bog'liqligi sababli, CPA deb hisoblanadi kontrendikedir meningioma yoki meningioma tarixi bo'lgan odamlarda.^[84]^[34] Estrogen va / yoki CPA bilan bog'liq bo'lgan benign miya shishi sabab bo'lishi mumkin vizual buzilishlar yoki og'ir holatlarda to'liq ko'rlik siqilish tufayli optik asab va / yoki xiyazma.^[80]

Meningioma ayollarda erkaklarnikiga qaraganda 2-3 baravar ko'p bo'lib, meningioma o'sishining tezlashishi kuzatilgan homiladorlik va mumkin bo'lgan gormonal bog'lanishni ko'rsatadigan hayz davrining luteal bosqichida.^[85] U yerda ifoda PR-ning oldingi gipofiz va menejalarda PRning yuqori darajada ifodalanishi, PRni CPA bilan faollashishi u bilan bog'liq bo'lgan benign miya shishi patogenezida ishtirok etishini anglatadi.^[86] Estrogen retseptorlari gipofizning oldingi qismida,^[87] va PRning ushbu sohadagi ifodasini oshirishi ma'lum.^[88] Shunga muvofiq, estrogenlar va progestogenlar, shu jumladan CPA, prolaktin darajasini, ayniqsa yuqori konsentratsiyalarda oshirishi ma'lum (masalan, homiladorlik ).^[51]^[89] CPA bilan bog'liq bo'lgan benign miya shishi holatlari ko'p hollarda estrogen bilan birgalikda bo'lgan va transgender ayollarda paydo bo'lgan bo'lsa, faqat ikkala cisgender ayollar va erkaklarda ham yuqori dozada CPA bilan bog'liq holatlar mavjud.^[54]^[90] Menenjiyoma kabi benign miya shishi, shuningdek, boshqa progestogenlarning yuqori dozalari bilan bog'liq edi, masalan xlormadinon asetat, megestrol asetat, medroksiprogesteron asetat va nomegestrol asetat, shuningdek homiladorlik bilan.^[85]^[91]^[92]^[93]^[94]

Bir qator ish bo'yicha hisobotlar prolaktinomalar (shuningdek, sir bo'lmagan gipofiz adenomasi),^[95]^[96]^[97]^[98]^[99] meningioma,^[100]^[101]^[102]^[103]^[91]^[90]^[80] va vestibulyar schvanomalar^[81] transgender ayollarda estrogen va CPA terapiyasi bilan bog'liq nashr etilgan.^[104]^[105]^[106]^[81]^[85]^[107] Katta retrospektiv grafikani o'rganish eng ko'p estrogen va CPA bilan davolangan va 23935 kishi yil davomida kuzatilgan 2555 transgender ayollarning 8 ta meningioma (0.31% yoki 320 holatdan 1 tasi) qayd etilganligi; SIR = 4.1 sisgender ayollarga nisbatan, SIR = Sisgender erkaklarga nisbatan 11,9), 9 prolaktinoma (0,35% yoki 284 holatida 1; SIR = 4.3 sisgender ayollarga nisbatan, SIR = Cisgender erkaklarga nisbatan 26,5), bitta sir bo'lmagan gipofiz adenomasi va ikkita vestibulyar shvanomalar.^[81] Yuqori dozali estrogen va CPA bilan davolangan va o'rtacha 4,4 yil davomida (6 oydan 6 oygacha 14 yoshgacha) davolangan 303 transgender ayolni retrospektiv ravishda o'rganish 46 giperprolaktinemiya holatini (sarum prolaktin> 1000 mU / L) qayd etdi ( 15% insidans; cisgender erkaklarga nisbatan 400 barobar ko'paygan xavf).^[61]^[62]^[106]^[63]^[108] Davomiy bo'lgan 23 holatdan 15 tasi kuzatishga qaytgan, 5 holatda gipofiz bezining kengayganligi KTni skanerlash bilan kontrastni kuchaytirish.^[61] Miyaning benign shishlari bilan bog'liq bo'lgan estrogen bilan birgalikda CPA dozalari kuniga 10 mg va undan yuqori bo'lgan.^[81]^[62]^[107]^[90] Estrogen va CPA birikmasidan farqli o'laroq, faqat estrogen transgender ayollarda prolaktinomalarning yagona holatlari bilan bog'liq.^[108]^[109]^[81]

Butun mamlakat bo'ylab aholini o'rganish yilda Daniya erkaklarda menenjiom bilan CPA yoki boshqa antiandrogenlarning sezilarli darajada bog'liqligi topilmadi.^[110] Biroq, o'qish Ispaniya va Birlashgan Qirollik meningioma bilan CPA terapiyasining ijobiy assotsiatsiyasini topdilar.^[110]

A gemangioblastoma CPA bilan davolangan odamda meningiomani taqlid qilish haqida xabar berilgan.^[111]

Siproteron asetat bilan bog'liq prolaktinoma haqida nashr qilingan xabar
#	Yoshi	Jinsiy aloqa	Dori vositalari	Davolashning davomiyligi	Ref	Havola
1	26 yil	MtF	CPA kuniga 100 mg, EE 100 mg / kun, Evropa Ittifoqi 100 mg / 2x hafta	~ 10 oy	Gooren va boshq. (1988)	^[95]
2	32 yil	MtF	CPA kuniga 150 mg, EE 1,5 mg / kun	4 yil	Serri va boshq. (1996)	^[112]
3	52 yil	MtF	CPA kuniga 100 mg, EE 100 mg / kun	15 yil	Bunk va boshq. (2009)	^[98]
4	33 yil	MtF	CPA kuniga 200 mg, CEEs 2,5 mg / kun	6 oy	Garsiya-Malpartida va boshqalar. (2010)	^[97]
5	41 yil	MtF	CPA kuniga 2 mg, EE 35 mg / kun, E2-EN 10 mg / 2 hafta i.m.	18 yosh	Kunha va boshq. (2015)	^[99]
6	32 yil	MtF	CPA kuniga 100 mg, E2 in'ektsiyalari 100 mg / 2 hafta i.m.	53 oy	Nota va boshq. (2018)	^[113]
7	39 yil	MtF	CPA kuniga 100 mg, CEEs 2,5 mg / kun	172 oy	Nota va boshq. (2018)	^[113]
8	27 yil	MtF	CPA, E2 in'ektsiyalari i.m. (dozalari haqida ma'lumot yo'q)	156 oy	Nota va boshq. (2018)	^[113]
9	46 yil	MtF	CPA kuniga 100 mg, EE 100 mg / kun	66 oy	Nota va boshq. (2018)	^[113]
10	24 yil	MtF	CPA kuniga 100 mg (estrogen ko'rsatilmagan)	9 oy	Nota va boshq. (2018)	^[113]
11	47 yil	MtF	CPA kuniga 100 mg, EE 100 mg / kun	91 oy	Nota va boshq. (2018)	^[113]
12	28 yil	MtF	CPA kuniga 50 mg, EV 2 mg / kun og'iz orqali	134 oy	Nota va boshq. (2018)	^[113]
13^a	34 yil	MtF	CPA kuniga 50 mg, EV kuniga 1 mg og'iz orqali	35 oy	Nota va boshq. (2018)	^[113]
Qisqartmalar: CPA = Siproteron asetat. E2 = Estradiol. EV = Estradiol valerat. E2-EN = Estradiol enantat. Evropa Ittifoqi = Estradiol undesilat. Idoralar = Konjuge estrogenlar. EE = Etinilestradiol. MtF = Erkak-ayol (transgender ayol). i.m. = Mushak ichiga yuborish. Izohlar: ^a = Gipofizning maxfiy bo'lmagan adenomasi. Izohlar: Asscheman va boshq. (1988) shuningdek, gipofiz kengayishi va mumkin bo'lgan prolaktinomaning 5 MtF holatini tasvirlab berdi.^[62] van Kesteren va boshq. (1997) gipofiz kengayishining mumkin bo'lgan MtF holatlarini ham tasvirlab berdi.^[114] Faqat beshta estrogenli MtF holatlari (CPA holda) qayd etilgan.^[109]^[98]^[99]^[113] Futterweit (1998) dorilar haqida ma'lumotsiz MtF holatini tasvirlab berdi.^[115] Manbalar: ^[116]

Siproteron asetat bilan bog'liq meningioma haqida e'lon qilingan xabar
#	Yoshi	Jinsiy aloqa	Dori vositalari	Davolashning davomiyligi	Ref	Havola
1	28 yil	MtF	CPA kuniga 100 mg, EE 100 mg / kun	5 yil	Gazzeri va boshq. (2007)	^[100]
2	48 yil	MtF	CPA 100 mg / kun, EE ("ayollashtirish rejimi")	10 yil	Cebula va boshq. (2010)	^[102]
3	46 yil	Ayol	CPA kuniga 50 mg, E2 ("o'rnini bosuvchi")	10 yil	Gonchalves va boshq. (2010)	^[117]
4	83 yil	Erkak	CPA ≥50 mg / kun	2 yil	Gil va boshq. (2011)	^[54]
5	71 yosh	Erkak	CPA ≥50 mg / kun	3 yil	Gil va boshq. (2011)	^[54]
6	66 yil	Ayol	CPA ≥50 mg / kun	3 yil	Gil va boshq. (2011)	^[54]
7	43 yil	Ayol	CPA ≥50 mg / kun	2 yil	Gil va boshq. (2011)	^[54]
8	35 yil	MtF	CPA kuniga 100 mg, E2 100 mg / kunlik yamoq	4 yil	Bergoglio va boshq. (2012)	^[103]
9	60 yil	MtF	CPA kuniga 50 mg, E2 8 mg / kun	10 yil	Knight va boshq. (2013)	^[118]
10	56 yil	MtF	CPA, EV 2 mg / kun og'iz orqali	8 yil	Razavi (2014)	^[119]
11	51 yil	Ayol	CPA kuniga 15 mg	30 yil	Bernat va boshq. (2015)	^[120]
12	47 yil	Ayol	CPA kuniga 25 mg	15 yil	Bernat va boshq. (2015)	^[120]
13	43 yil	Ayol	CPA kuniga 50 mg	12 yil	Bernat va boshq. (2015)	^[120]
14	39 yil	Ayol	CPA kuniga 50 mg	10 yil	Bernat va boshq. (2015)	^[120]
15	61 yosh	Ayol	CPA kuniga 25 mg	24 yil	Bernat va boshq. (2015)	^[120]
16	38 yil	Ayol	CPA kuniga 25 mg	10 yil	Bernat va boshq. (2015)	^[120]
17	45 yil	Ayol	CPA kuniga 50 mg	20 yil	Bernat va boshq. (2015)	^[120]
18	53 yil	Ayol	CPA kuniga 50 mg	20 yil	Bernat va boshq. (2015)	^[120]
19	56 yil	Ayol	CPA kuniga 50 mg	8 yil	Bernat va boshq. (2015)	^[120]
20	55 yosh	Ayol	CPA kuniga 50 mg	30 yil	Bernat va boshq. (2015)	^[120]
21	49 yil	Ayol	CPA kuniga 50 mg	20 yil	Bernat va boshq. (2015)	^[120]
22	49 yil	Ayol	CPA kuniga 50 mg	25 yil	Bernat va boshq. (2015)	^[120]
23	58 yil	Ayol	CPA kuniga 50 mg	18 yosh	Botella va boshq. (2015)	^[121]
24	37 yil	Ayol	CPA kuniga 50 mg	11 yil	Botella va boshq. (2015)	^[121]
25	42 yil	Erkak	CPA kuniga 100 mg	23 yil	Sys & Kestelyn (2015)	^[122]
26	45 yoki 46 yil	MtF	CPA 10 yoki 100 mg / kun, E2 20 mg / 4 oylik implantatsiya	5 yil	ter Vengel va boshq. (2015)	^[91]^[113]
27	51 yil	MtF	CPA kuniga 100 mg, EE 100 mg / kun	25 yil	ter Vengel va boshq. (2015)	^[91]^[113]
28	65 yosh	MtF	CPA kuniga 10 mg, CEEs 1,25 mg / kun	19 yil	ter Vengel va boshq. (2015)	^[91]^[113]
29	26 yil	Ayol	CPA kuniga 50 mg	10 yil	Kalamarides va Peyre (2017)	^[123]
30	43 yil	Ayol	CPA kuniga 25 mg	25 yil	Kalamarides va Peyre (2017)	^[123]
31	83 yil	Erkak	CPA kuniga 200 mg	7 oy	Keilani & Abada (2017)	^[124]
32	65 yosh	Ayol	CPA kuniga 50 mg	15 yil	Bernat va boshq. (2018)	^[125]
33	77 yil	MtF	CPA kuniga 50 mg, E2 50 mg / kun yamoq	24 yil	Boer va boshq. (2018)	^[126]
34	41 yil	MtF	CPA kuniga 50 mg, E2 gel 1-3 mg / kun	9 yil	Manchini va boshq. (2018)	^[90]
35	60 yil	MtF	CPA, CEEs	36 yil	Nizar & Seal (2018)	^[127]
36	51 yil	MtF	CPA 20 mg / week, E2 100 mg / day patch	11 yil	Nota va boshq. (2018)	^[113]
37	66 yil	MtF	CPA kuniga 10 mg	40 yil	Nota va boshq. (2018)	^[113]
38	58 yil	MtF	CPA kuniga 50 mg, E2 100 mg / kun patch	6 yil	Nota va boshq. (2018)	^[113]
39	49 yil	MtF	CPA, EV kuniga 2 mg	16 yil	Nota va boshq. (2018)	^[113]
40	51 yil	MtF	CPA kuniga 100 mg, EE 100 mg / kunlik yamoq	26 yil	Nota va boshq. (2018)	^[113]
41	50 yil	MtF	CPA kuniga 50 mg, E2 0,6 mg / g krem 2x / kun	~ 10 yil	Raj va boshq. (2018)	^[80]
42	48 yil	MtF	CPA kuniga 50 mg, E2 1 mg / g krem 3x / kun	21 yil	Raj va boshq. (2018)	^[80]
43	43 yil	Ayol	CPA kuniga 25-50 mg, EV 2 mg / kun, finasterid 5 mg / kun va boshqalar	23 yil	Chasyor va boshq. (2019)	^[128]
44	67 yosh	MtF	CPA, estrogen	> 14 yil	Alalade va boshq. (2019)	^[129]
45	46 yil	Ayol	CPA 5 mg / day, keyinchalik NOMAC 5 mg / kun	15 yil	Shampan va boshq. (2019)	^[130]
46	58 yil	Ayol	10 kun / tsikl uchun CPA kuniga 25-100 mg	34 yil	Ouens va boshq. (2019)	^[131]
47	?	Erkak	CPA 300 mg / 2 hafta i.m., leuprorelin 11.25 mg / 3 oy i.m.	?	Colstrup va boshq. (2020)	^[132]
Qisqartmalar: CPA = Siproteron asetat. E2 = Estradiol. EV = Estradiol valerat. Idoralar = Konjuge estrogenlar. EE = Etinilestradiol. MtF = Erkak-ayol (transgender ayol). Izohlar: Bernat va boshqalar uchun. (2015) holatlarida, faqat bittasi estrogen (xususan estradiol) olganligi haqida xabar berilgan.^[120] Froelich va boshq. (2008) ko'p sonli meningioma bilan kasallangan qo'shimcha 8 ta ayolning holati (33-62 yosh, o'rtacha 46 yosh; 50 mg / kun CPA; 10-20 yil ta'sir qilish) haqida xabar berdi.^[133] Cea-Soriano va boshq. (2012), shuningdek, 8 ta holat (4 erkak (kuniga 50 mg, Yoki = 3.28), 4 ayol (kuniga 2 mg, Yoki = 1.03)) individual xususiyatlarga ega emas.^[105]^[121] Peyre va boshq. operatsiya qilingan 38 holat haqida xabar berdi.^[134] Portet va boshq. (2019) 30 ta operatsiya haqida xabar berdi.^[135] Boshqa progestinlar bilan bog'liq holatlar ham qayd etilgan.^[120] Deipolyi, Xan va Parsa (2010) MtFda faqatgina E2 100 mg / kun bilan bog'liq bo'lgan holat haqida xabar berishdi.^[101] Manbalar: ^[90]^[91]^[116]

Qon pıhtıları

Bilan birga past dozali (2 mg) CPA ning kombinatsiyasi etinilestradiol (35 mkg), xuddi tug'ruqni nazorat qilish tabletkalarida bo'lgani kabi, yuqori xavf tug'diradi venoz tromboembolizm (VTE).^[136]^[137] CPA o'z ichiga olgan kontratseptiv tabletkalarni iste'mol qiladigan ayollarda VTE rivojlanish xavfi kontratseptiv tabletkalarni iste'mol qilmaydigan ayollarga nisbatan 6-7 baravar ko'payadi va androgenik progestinni o'z ichiga olgan kontratseptiv tabletkalarni iste'mol qiladigan ayollar levonorgestrel.^[138] Etinilestradiol va kam dozada CPA o'z ichiga olgan tug'ilishni nazorat qilish tabletkalari bilan VTE ning mutlaq xavfi 10000 ayol yiliga 1 dan 10 gacha.^[137] O'limga olib keladigan VTE ning kamida to'rtta ommaviy holati etinilestradiol va past dozali CPA o'z ichiga olgan tug'ilishni nazorat qilish tabletkalari bilan bog'liq.^[139] CPA ning progestogen, antiandrogenik va glyukokortikoid faoliyati estrogenlar bilan birgalikda CPA bilan VTE xavfini oshirishi bilan bog'liq deb o'ylashadi.^[140]^[141]

Og'zaki 100 mg / kun etinilestradiol va 100 mg / kun CPA ning kombinatsiyasi 303 transgender ayolda VTE xavfini 45 baravar oshirganligi, 6,3% (19 holat) mutloq kasalligi qayd etilgan.^[142] Xavf yoshga juda bog'liq bo'lib, VTE darajasi 40 yoshdan kichiklarda 2,1% va 40 yoshdan katta bo'lganlarda 12% ni tashkil etdi.^[142] Xuddi shu rejim qo'llanilgan, ammo transdermal estradiol 40 yoshdan oshganlar uchun standart terapiya bo'lib qolgan 816 transgender ayolni keyingi tadqiqotida VTE xavfi umuman 20 baravarga oshdi (45 holat, 5,5% kasallanish) ).^[142] Shu bilan birga, transdermal estradiol bilan davolangan 138 transgender ayol guruhida (0,7% insidans) faqat bitta VTE kasalligi bo'lgan.^[142] Shunga muvofiq transdermal estradiol va kuniga 50 mg siproteron asetat birikmasi VTE xavfi jihatidan nisbatan xavfsizroq ko'rinadi.^[142] VTE xavfi dastlab faqat etinilestradiolga tegishli edi va transgender ayollarda etinilestradioldan foydalanish asosan estradiol kabi boshqa estrogenlar foydasiga qoldirildi.^[142] Biroq, CPA endi VTE xavfini sezilarli darajada oshirishi ma'lum va bu ham o'z hissasini qo'shgan bo'lishi mumkin.^[142] Transgender ayollarda CPA to'xtatilishi kerak jinsiy aloqani almashtirish operatsiyasi yoki orkiektomiya VTE xavfini kamaytirish uchun.^[142] VTE xavfini kamaytirish uchun operatsiyadan kamida 2 hafta oldin uni to'xtatish kerak.^[142]

Katta farmakoepidemiologik o'rganish ichida Birlashgan Qirollik yordamida Umumiy amaliyot tadqiqotlari ma'lumotlar bazasi ning turli shakllari bilan VTE xavfini baholadi androgen etishmovchiligini davolash prostata saratoni uchun.^[143]^[144]^[145] Tadqiqotda a namuna 11,199 erkak, ulardan 229 nafari (2,0%) VTE bilan kasallangan va 14% bu o'limga olib kelgan.^[143]^[145] VTE bilan kasallanish darajasi CPA monoterapiyasi uchun 3.46 ni tashkil etdi steroid bo'lmagan antiandrogen bilan monoterapiya flutamid yoki bikalutamid; 3.35 ga nisbatan CPA monoterapiyasi uchun GnRH agonisti /orkiektomiya monoterapiya; Nisbatan CPA monoterapiyasi uchun 1.25 estrogen bilan monoterapiya dietilstilbestrol yoki estramustin fosfat; va CPA monoterapiyasi uchun 0,60 ga nisbatan estrodiol blokadasi GnRH agonisti / orkiektomiya va CPA bilan.^[144]^[8] The sozlangan koeffitsientlar VTE uchun davolanish uchun 1,00 edi; Nonsteroid antiandrogen terapiyasi uchun 1,29; CPA va GnRH agonisti / orkiektomiya bilan estrodiol androgen blokadasi uchun 3.35; CPA monoterapiyasi uchun 5.23; estrogen monoterapiyasi uchun esa 5.67.^[143]^[145]^[146] GnRH agonistli monoterapiyaga nisbatan GnRH agonisti bo'lgan yoki bo'lmagan holda CPA ning turli xil dozalarini VTE uchun sozlangan stavkalar nisbati 25 yoki 50 mg / kun uchun 3,49, 100 yoki 150 mg / kun uchun 4,93 va 200 dan katta yoki unga teng 4,54 edi. mg / kun.^[145] Prostata saratonini davolashda ishlatiladigan CPA va boshqa dorilarga qo'shimcha ravishda, metastatik prostata saratoni o'zi VTE uchun xavf omilidir.^[142]

Katta randomizatsiyalangan boshqariladigan sinovlar prostata saratoni davolash uchun boshqa dorilarga nisbatan CPA, VTE ning quyidagi holatlari kuzatildi: 100 mg / kun ichidagi CPA uchun 5,3% va mushak ichiga 100 mg / oy uchun 4,2%. estradiol undesilat (n = 191);^[147]^[148] 250 mg / kunlik oral CPA uchun 2,4% va kuniga 200 mg oral medroksiprogesteron asetat uchun 6,1% va 3 mg / kunlik oral dietilstilbestrol uchun 8,2% (n = 269);^[149] va 300 mg / kunlik oral CPA uchun 4,5% va 750 mg / kunlik flutamid uchun 0% (n = 264).^[149]^[150] Shu bilan birga, so'nggi tadqiqotning yakuniy tahlili (EORTC Protokoli 30892) VTE nihoyat flutamid guruhidagi 3 bemorda (2,0%) va CPA guruhidagi 7 bemorda (4,6%) sodir bo'lganligini ko'rsatdi.^[16]

Premenopozal ayollar ombor AOK mumkin medroksiprogesteron asetat, shakli sifatida CPA bilan bog'liq progestin faqat progestogen bilan tug'ilishni nazorat qilish, VTE xavfining 2,2 dan 3,6 martagacha ko'payishi kuzatilgan.^[151]^[152] Ammo, bu VTE xavfi yuqori bo'lgan ayollarga DMPA ning imtiyozli retseptini aks ettirishi mumkin edi.^[152] DMPA ozgina ta'sir qiladi yoki umuman ta'sir qilmaydi qon ivishi va fibrinolitik omillar.^[153]^[154] Bundan tashqari, fiziologik dozalarda o'z-o'zidan progestogenlar tromboz xavfini oshirmaydi.^[152]^[155]

Gormonlarni davolash va tug'ilishni nazorat qilish bilan venoz tromboembolizm (VTE) xavfi (QResearch / CPRD)
Turi	Marshrut	Dori vositalari	Koeffitsientlar nisbati (95% CI )
Menopozli gormonlarni davolash	Og'zaki	Estradiol yolg'iz ≤1 mg / kun > Kuniga 1 mg	1.27 (1.16–1.39)* 1.22 (1.09–1.37)* 1.35 (1.18–1.55)*
		Konjuge estrogenlar yolg'iz ≤0,625 mg / kun > Kuniga 0,625 mg	1.49 (1.39–1.60)* 1.40 (1.28–1.53)* 1.71 (1.51–1.93)*
		Estradiol / medroksiprogesteron asetat	1.44 (1.09–1.89)*
		Estradiol / dydrogesteron ≤1 mg / kun E2 > Kuniga 1 mg E2	1.18 (0.98–1.42) 1.12 (0.90–1.40) 1.34 (0.94–1.90)
		Estradiol / noretisteron ≤1 mg / kun E2 > Kuniga 1 mg E2	1.68 (1.57–1.80)* 1.38 (1.23–1.56)* 1.84 (1.69–2.00)*
		Estradiol / norgestrel yoki estradiol / drospirenone	1.42 (1.00–2.03)
		Konjuge estrogenlar / medroksiprogesteron asetat	2.10 (1.92–2.31)*
		Konjuge estrogenlar / norgestrel ≤0,625 mg / kun Idoralar > Kuniga 0,625 mg Idoralar	1.73 (1.57–1.91)* 1.53 (1.36–1.72)* 2.38 (1.99–2.85)*
		Tibolone yolg'iz	1.02 (0.90–1.15)
		Raloksifen yolg'iz	1.49 (1.24–1.79)*
	Transdermal	Estradiol yolg'iz ≤50 mg / kun > Kuniga 50 mkg	0.96 (0.88–1.04) 0.94 (0.85–1.03) 1.05 (0.88–1.24)
	Transdermal	Estradiol /progestogen	0.88 (0.73–1.01)
	Vaginal	Estradiol yolg'iz	0.84 (0.73–0.97)
	Vaginal	Konjuge estrogenlar yolg'iz	1.04 (0.76–1.43)
Kombinatsiyalangan tug'ilishni nazorat qilish	Og'zaki	Etinilestradiol / noretisteron	2.56 (2.15–3.06)*
		Etinilestradiol / levonorgestrel	2.38 (2.18–2.59)*
		Etinilestradiol / norgestimate	2.53 (2.17–2.96)*
		Etinilestradiol / desogestrel	4.28 (3.66–5.01)*
		Etinilestradiol / gestoden	3.64 (3.00–4.43)*
		Etinilestradiol / drospirenon	4.12 (3.43–4.96)*
		Etinilestradiol / siproteron asetat	4.27 (3.57–5.11)*
Izohlar: (1) Ichki holatlarni nazorat qilish bo'yicha tadqiqotlar (2015, 2019) ma'lumotlar asosida QResearch va Klinik amaliyotni o'rganish Datalink (CPRD) ma'lumotlar bazalari. (2) Bioidentikal progesteron kiritilmagan, ammo faqat estrogenga nisbatan qo'shimcha xavf tug'dirmasligi ma'lum. Izohlar: * = Statistik jihatdan ahamiyatli (p < 0.01). Manbalar: Shablonga qarang.

Yurak-qon tomir salomatligi

The Ayollar salomatligi tashabbusi randomizatsiyalangan boshqariladigan sinovlar xavfining sezilarli darajada oshganligini namoyish etdi yurak tomirlari kasalligi kuniga 0,625 mg konjuge estrogenlar va kuniga 2,5 mg medroksiprogesteron asetat (CPA bilan chambarchas bog'liq bo'lgan progestin) menopausal gormonlarni davolash kuniga 0,625 mg konjuge estrogenlarga nisbatan va platsebo yilda peri- va postmenopozal ayollar.^[156]^[157] Faqatgina estrogen va past dozali CPA ning o'xshash xavf-xatarlari bor-yo'qligi o'rganilmagan va shuning uchun ham noma'lum.^[158]^[159] Biomarker tadqiqotlar shuni ko'rsatadiki, CPA ning androgen faolligining etishmasligi va unga salbiy ta'sir ko'rsatmasligi qon lipidlari kamroq yoki hech qanday xavf tug'dirmasligi mumkin, ammo bu hali kuzatuv ishlari yoki klinik sinovlarda baholanmagan yoki qo'llab-quvvatlanmagan.^[158]^[159]

Erkaklarda prostata saratoni uchun yuqori dozali CPA nisbatan engil holatlarga bog'liq yurak-qon tomir yon effektlar.^[160]^[161]^[162]^[163]^[164] Bunga quyidagilar kiradi qon ivishi o'zgarishlar^[165] va qon pıhtıları (5%),^[160]^[166] suyuqlikni ushlab turish (4%),^[166] ishemik kardiomiopatiya (4–40%),^[9]^[167] va kiruvchi ta'sirlar sarum lipid profillari.^[160]^[161]^[162]^[163]^[164] Bunday dozalarda og'ir yurak-qon tomir asoratlari 10% gacha uchraydi va ba'zida o'limga olib keladi.^[164]^[168] CPA va taqqoslangan katta randomizatsiyalangan nazorat ostida sinov flutamid prostata saratoni bilan kasallangan erkaklarda yurak-qon tomir muammolari darajasi ikki terapiya o'rtasida sezilarli farq qilmasligini aniqladi.^[16] 250 mg / kun CPA ning yurak-qon tomir toksikligi 3 mg / kundan sezilarli darajada past dietilstilbestrol.^[149]^[169]

Ko'krak bezi saratoni

The Ayollar salomatligi tashabbusi randomizatsiyalangan boshqariladigan sinovlar xavfining sezilarli darajada oshganligini namoyish etdi ko'krak bezi saratoni kuniga 0,625 mg konjuge estrogenlar va kuniga 2,5 mg medroksiprogesteron asetat (CPA bilan chambarchas bog'liq bo'lgan progestin) uchun menopausal gormonlarni davolash kuniga 0,625 mg konjuge estrogenlarga nisbatan va platsebo yilda peri- va postmenopozal ayollar.^[156]^[157] Xuddi shunday, menopozal gormonlarni davolash uchun estrogen va past dozali CPA, faqat estrogenga nisbatan ko'krak bezi saratoni xavfi sezilarli darajada yuqori va foydasizdir.^[170] Bundan tashqari, butun mamlakat bo'ylab kuzatish o'rganish estrogen va yuqori dozali CPA ning ko'krak bezi saratoni xavfini 46 barobar oshirish bilan bog'liqligini aniqladi transgender ayollar uchun kutilgan insidansga nisbatan cisgender erkaklar.^[171]^[172]^[173]^[174]

Katta kuzatuv tadqiqotlarida menopauzali gormon terapiyasi bilan ko'krak bezi saratoni xavfi (Mirkin, 2018)
O'qish	Terapiya	Xavf darajasi (95% CI )
E3N-EPIC: Fournier va boshq. (2005)	Faqat estrogen	1.1 (0.8–1.6)
	Estrogen plyusi progesteron Transdermal estrogen Og'iz orqali estrogen	0.9 (0.7–1.2) 0.9 (0.7–1.2) Hech qanday tadbir yo'q
	Estrogen va progestin Transdermal estrogen Og'iz orqali estrogen	1.4 (1.2–1.7) 1.4 (1.2–1.7) 1.5 (1.1–1.9)
E3N-EPIC: Fournier va boshq. (2008)	Faqat og'iz ostrogen	1.32 (0.76–2.29)
	Og'iz orqali estrogen va progestogen Progesteron Didrogesteron Medrogestone Xlormadinon asetat Siproteron asetat Promegestone Nomegestrol asetat Noretisteron asetat Medroksiprogesteron asetat	Tahlil qilinmadi^a 0.77 (0.36–1.62) 2.74 (1.42–5.29) 2.02 (1.00–4.06) 2.57 (1.81–3.65) 1.62 (0.94–2.82) 1.10 (0.55–2.21) 2.11 (1.56–2.86) 1.48 (1.02–2.16)
	Faqat transdermal estrogen	1.28 (0.98–1.69)
	Transdermal estrogen va progestogen Progesteron Didrogesteron Medrogestone Xlormadinon asetat Siproteron asetat Promegestone Nomegestrol asetat Noretisteron asetat Medroksiprogesteron asetat	1.08 (0.89–1.31) 1.18 (0.95–1.48) 2.03 (1.39–2.97) 1.48 (1.05–2.09) Tahlil qilinmadi^a 1.52 (1.19–1.96) 1.60 (1.28–2.01) Tahlil qilinmadi^a Tahlil qilinmadi^a
E3N-EPIC: Fournier va boshq. (2014)	Faqat estrogen	1.17 (0.99–1.38)
	Estrogen plyusi progesteron yoki dydrogesteron	1.22 (1.11–1.35)
	Estrogen va progestin	1.87 (1.71–2.04)
CECILE: Cordina-Duverger va boshq. (2013)	Faqat estrogen	1.19 (0.69–2.04)
CECILE: Cordina-Duverger va boshq. (2013)	Estrogen va progestogen Progesteron Progestinlar Progesteronning hosilalari Testosteron hosilalari	1.33 (0.92–1.92) 0.80 (0.44–1.43) 1.72 (1.11–2.65) 1.57 (0.99–2.49) 3.35 (1.07–10.4)
Izohlar: ^a = Tahlil qilinmagan, 5 holatdan kam. Manbalar: Shablonga qarang.

Boshqa uzoq muddatli ta'sirlar

Xususida ovulyatsiya inhibisyon, CPA ning samarali dozasi kuniga 1,0 mg, medroksiprogesteron asetat esa 10 mg / kun.^[140]^[175] Ovulyatsiyani inhibatsiyasi asosida kuniga 50 mg siproteron asetat dozasi progestogen ta'siridan 200 baravar ko'p bo'ladi. kuch 2,5 mg / kun medroksiprogesteron asetat.^[140]^[175] Progestogen ta'siridan tashqari, CPA ishlab chiqaradi androgen va estrogen etishmovchiligi monoterapiya sifatida foydalanilganda,^[176] va bu sog'liqqa ham ta'sir qiladi.^[177]^[178]^[37]

Uzoq muddatli terapiya bilan yuqori dozali CPA ning sog'liqqa ta'siri yaxshi o'rganilmagan. A meta-tahlil erkaklarda prostata saratoni davolash uchun yuqori dozali CPA ning CPA prostata bezi saratoni o'limining ozgina oshishi bilan bog'liqligini aniqladi.^[179] Bundan tashqari, CPA ning kombinatsiyasi jarrohlik yoki tibbiy kastratsiya prostata saratoni uchun sezilarli darajada kamayganligi aniqlandi umumiy omon qolish faqat kastratsiyaga nisbatan.^[180]

Xotin-qizlar salomatligi tashabbusi (WHI) natijalari menopozal gormon terapiyasi randomizatsiyalangan boshqariladigan tekshiruvlar
Klinik natijalar	Faraz qilingan xavfga ta'siri	Estrogen va progestogen (Idoralar 0,625 mg / kun p.o. + MPA 2,5 mg / kun p.o.) (n = 16,608, bachadon bilan, 5,2-5,6 yil)			Estrogen yolg'iz (Idoralar 0,625 mg / kun p.o.) (n = 10.739, bachadon yo'q, 6.8-7.1 yil)
Klinik natijalar	Faraz qilingan xavfga ta'siri	Kadrlar	95% CI	AR	Kadrlar	95% CI	AR
Koroner yurak kasalligi	Kamaytirilgan	1.24	1.00–1.54	+6 / 10,000 PYs	0.95	0.79–1.15	−3 / 10,000 PYs
Qon tomir	Kamaytirilgan	1.31	1.02–1.68	+8 / 10,000 PYs	1.37	1.09–1.73	+12 / 10,000 PYs
O'pka emboliya	Kattalashtirilgan	2.13	1.45–3.11	+10 / 10,000 PYs	1.37	0.90–2.07	+4 / 10,000 PYs
Venoz tromboembolizmi	Kattalashtirilgan	2.06	1.57–2.70	+18 / 10,000 PYs	1.32	0.99–1.75	+8 / 10,000 PYs
Ko'krak bezi saratoni	Kattalashtirilgan	1.24	1.02–1.50	+8 / 10,000 PYs	0.80	0.62–1.04	-6 / 10,000 PYs
Kolorektal saraton	Kamaytirilgan	0.56	0.38–0.81	−7 / 10,000 PYs	1.08	0.75–1.55	+1 / 10,000 PYs
Endometriyal saraton	–	0.81	0.48–1.36	−1 / 10,000 PYs	–	–	–
Kestirib sinishi	Kamaytirilgan	0.67	0.47–0.96	−5 / 10,000 PYs	0.65	0.45–0.94	−7 / 10,000 PYs
Jami sinish	Kamaytirilgan	0.76	0.69–0.83	-47 / 10,000 PYs	0.71	0.64–0.80	-53 / 10,000 PYs
Jami o'lim	Kamaytirilgan	0.98	0.82–1.18	−1 / 10,000 PYs	1.04	0.91–1.12	+3 / 10,000 PYs
Global indeks	–	1.15	1.03–1.28	+19 / 10,000 PYs	1.01	1.09–1.12	+2 / 10,000 PYs
Qandli diabet	–	0.79	0.67–0.93		0.88	0.77–1.01
O't pufagi kasalligi	Kattalashtirilgan	1.59	1.28–1.97		1.67	1.35–2.06
Stressni ushlab turish	–	1.87	1.61–2.18		2.15	1.77–2.82
Noqulaylikni talab qiling	–	1.15	0.99–1.34		1.32	1.10–1.58
Periferik arteriya kasalligi	–	0.89	0.63–1.25		1.32	0.99–1.77
Mumkin dementia	Kamaytirilgan	2.05	1.21–3.48		1.49	0.83–2.66
Qisqartmalar: Idoralar = konjuge estrogenlar. MPA = medroksiprogesteron asetat. p.o. = og'zaki. HR = xavf darajasi. AR = tegishli xavf. PYs = kishi - yil. CI = ishonch oralig'i. Izohlar: Namuna o'lchamlari (n) o'z ichiga oladi platsebo bemorlarning taxminan yarmi bo'lgan oluvchilar. "Global indeks" har bir ayol uchun eng erta tashxis qo'yish vaqti sifatida belgilanadi yurak tomirlari kasalligi, qon tomir, o'pka emboliya, ko'krak bezi saratoni, kolorektal saraton, endometriyal saraton (faqat estrogen va progestogen guruhi), son suyaklari va o'lim boshqa sabablardan. Manbalar: Shablonga qarang.

Boshqa yon ta'sirlar

Jigarning toksikligi

Hodisalar jigar fermentlarining ko'tarilishi katta faol kuzatuv tadqiqotida har qanday yoshdagi 1685 sog'lom erkak va ayolga siproteron asetatning turli dozalari bilan.^[19]

Eng jiddiy salohiyat yon ta'sir CPA ning qiymati gepatotoksiklik.^[181] Ning turli xil ko'rinishlari jigar kasalligi CPA davolash bilan birgalikda hujjatlashtirilgan, shu jumladan immunoallergik sitotoksik reaktsiyalar, kolestaz, otoimmun gepatit, o'tkir gepatit, fulminant jigar etishmovchiligi va siroz, shuningdek, xavfning ortishi jigar hujayralari karsinomasi.^[182]^[183] Klinik xususiyatlari o'z ichiga olishi mumkin sariqlik, charchoq, ko'ngil aynish, jigar fermentlarining ko'tarilishi, jigar nekroz va yallig'lanish va jigarning xususiyatlari dekompensatsiya.^[183] CPA terapiyasi tufayli gepatotoksikatsiya ko'pincha uzoq vaqt davomida preparatning yuqori dozalari bilan davolanadigan, ammo yoshroq bemorlarda ham uchraydigan keksa bemorlarda uchraydi.^[182] CPA ning gepatotoksikligi uning C1a, 2a bilan bog'liq metilen guruhi.^[78]

In nazoratsiz ochiq yorliq o'rtacha 6,7 yil davomida CPA bilan davolangan (ammo 602 kishida 10 yoshdan oshgan), har qanday yoshdagi 1,685 sog'lom erkak va ayolni (2506 kishining to'liq namunasi uchun 3 yoshdan 75 yoshgacha) faol kuzatuvni o'rganish fermentlar kuniga 2,6 dan 3,1 foizgacha, kuniga 1 dan 20 mg gacha dozada, 8,1 foizda, kuniga 20 dan 50 mg gacha dozada, 10,2 foizda, 50 dan 100 mg gacha bo'lgan dozada fermentlar kuzatilgan. / kun, va 11,1 dan 25,0% gacha 100 mg / kundan ortiq dozada (200 mg / kundan ortiq).^[19]^[181]^[182]^[183] 4 yil davomida kuniga 50 mg CPA qabul qilgan prostata saratoni bilan kasallangan 89 erkak ustidan o'tkazilgan tekshiruvda jigar fermentlarining ko'tarilishi 28,2% ni tashkil etdi.^[183]^[184] 150 mg / kun CPA bilan davolangan 105 bemorni o'rganish natijasida gepatotoksisite darajasi 9,5% ni tashkil etdi, jigarning jiddiy shikastlanishi 3,8% (4/105).^[183] Davolangan 303 transgender ayolni o'rganish yuqori dozali estrogen va kuniga 100 mg CPA 7,2% (22/303) darajasida ko'tarilgan jigar fermentlari bilan kasallanish haqida xabar berdi.^[61]

2002 yilda CPA bilan bog'liq bo'lgan 18 ta nashr etilgan hisobot mavjudligi xabar qilindi gepatit adabiyotda, ushbu holatlarning 6 tasi o'limga olib keladi.^[181] Bundan tashqari, 1995 yilda nashr etilgan Birlashgan Qirollik Dori-darmonlarni nazorat qilish agentligi /Dori vositalari xavfsizligi qo'mitasi uning jurnalida Farmakologik nazoratning dolzarb muammolari gepatotoksisit haqida 96 ta o'z-o'zidan paydo bo'lgan hisobotlarni (91 erkak, 5 ayol) tasvirlab berdi, ulardan 33 tasi o'limga olib keldi.^[185]^[186]^[181] Ushbu nashrda tasvirlangan gepatotoksisitning namoyon bo'lishiga gepatit, xolestatik sariqlik va jigar etishmovchiligi.^[185]^[186] Kasalliklarning aksariyati prostata saratoni uchun juda yuqori dozada CPA (300 mg / kun) bilan davolangan erkaklar edi.^[185]^[186] 2014 yilgi tadqiqotlar shuni ko'rsatdiki, bugungi kunda CPA tomonidan chaqirilgan fulminant (to'satdan boshlangan va og'ir) jigar etishmovchiligining 9 ta holati qayd etilgan bo'lib, ulardan faqat bittasi o'lik emas.^[183] Shunday qilib, CPA tomonidan kelib chiqqan jigar etishmovchiligining prognozi o'limdir.^[183] Ammo jiddiy gepatotoksiklik asosan prostata saratoni bilan og'rigan bemorlarda juda yuqori dozada CPA qabul qiladi va jigarning jiddiy toksikligi transgender ayollarda qayd etilmagan.^[187] Jiddiy gepatotoksikaning 14 ta holati (o'tkir jigar etishmovchiligi va 2014 yilda ko'rib chiqilgan CPA bilan tavsiflangan o'tkir gepatit) kuniga 100 dan 300 mg gacha bo'lgan dozada va prostata saratoni bilan kasallangan keksa erkaklarda (65 yoshdan 92 yoshgacha).^[182] 2015 yildagi nashr CPA bilan birgalikda gepatotoksisitning qo'shimcha 22 ta yangi holatini, shu jumladan kuniga 50 mg dan bitta holat haqida xabar berdi.^[188]

CPA davolash bilan bog'liq bo'lgan gepatotoksiklik va o'lim xavfi, CPA ning AQShda foydalanish uchun FDA tomonidan tasdiqlanmaganligining sababi hisoblanadi.^[189] Yuqori dozali CPA bilan davolanayotgan bemorlar diqqat bilan kuzatilishi kerak jigar funktsiyasi testlari.^[190] Xavf dozaga bog'liq va tug'ilishni nazorat qilish tabletkalarida (2 mg) ishlatiladigan kam miqdordagi CPA dozalari ahamiyatsiz xavfni anglatadi.^[191] Ammo 14 yildan beri Diane-35 (kuniga 2 mg CPA ni) kontratseptsiya uchun qabul qilgan nemis ayol jigar saratonidan vafot etdi va bu giyohvand moddalar nazorati organlari tomonidan xavfsizlikni qayta ko'rib chiqishga va Evropada CPA ni oxirigacha cheklashiga olib keldi. ayollarda husnbuzarlarni davolash ko'rsatkichi.^[139] Qanday bo'lmasin, CPA bilan jigar toksikligi asosan prostata saratoni bilan og'rigan bemorlarda juda yuqori dozani qabul qiladi (kuniga 200-300 mg) va jigar toksikligi odatda past dozalarni qabul qiladigan cisgender yoki transgender ayollarda qayd etilmagan ( 25-100 mg / kun).^[182]^[187]^[6]^[7]

Gepatotoksikligi steroid bo'lmagan antiandrogen flutamid CPA-dan kattaroqdir.^[16]^[192] A randomizatsiyalangan nazorat ostida sinov va prostata saratoni bilan bevosita boshdan-boshga taqqoslash, umumiy stavkalar jigar funktsiyasining yomonlashishi kuniga 750 mg flutamid guruhida 9,9% va 300 mg / kun oral CPA guruhida 5,3% (p To'xtatishni talab qiladigan jigar toksikligi flutamid guruhida 8,6% va CPA guruhida 2,0% ga to'g'ri keldi.^[16] Topilmalar boshqa randomizatsiyalangan nazorat ostida o'tkazilgan tekshiruvda va kuniga 750 mg flutamid va 150 mg / kun oral CPA ni to'g'ridan-to'g'ri bosh bilan taqqoslashda o'xshash edi; gepatotoksiklik darajasi flutamid uchun 15,3% va CPA uchun 9,5% (p = 0,034) va jiddiy gepatotoksislik darajasi flutamid uchun 4,8% va CPA uchun 3,8% ni tashkil etdi.^[192] 2004 yilgi tekshiruvda flutamid bilan birgalikda gepatotoksikaning 46 ta e'lon qilingan holati, CPA bilan 21 ta holat, 4 ta holat bilan nilutamid va 1 ish bilan bikalutamid, barchasi 1986 yildan 2003 yilgacha.^[193]^[194]

CPA va flutamid o'rtasida gepatotoksikozga shubha qilinganligi haqida xabar mavjud.^[195]^[196]

Siproteron asetat bilan bog'liq jigar toksikligi haqida nashr qilingan xabar
#	Jinsiy aloqa	Yoshi	Dozalash	Turi	Boshlanishi	Natija	Omon qolish^a	Ref	Havola
1	Ayol	73 yil	Kuniga 400 mg	AH	2,5 oy	Tirik qoldi	Yo'q	Meijers va boshq. (1986)	^[197]
2	Ayol	85 yil	Kuniga 200 mg	AH	4,8 oy	Tirik qoldi	Yo'q	Meijers va boshq. (1986)	^[197]
3	Erkak	78 yil	Kuniga 200 mg	ALF	6 oy	O'lim	2 hafta	Lévesque va boshq. (1989)	^[198]
4	Erkak	71 yosh	Kuniga 300 mg	AH	5,3 oy	Tirik qoldi	Yo'q	Bleyk va boshq. (1990)	^[199]
5	Erkak	79 yil	200-300 mg / kun	AH	2,5 oy	Tirik qoldi	Yo'q	Dore va boshq. (1990)	^[200]
6	Erkak	80 yil	Kuniga 200 mg	ALF	7 oy	O'lim	~ 1-2 oy	Antoni va boshq. (1991)	^[201]
7	Erkak	75 yosh	Kuniga 300 mg	HCC	1,5 yil	ND	ND	Ohri va boshq. (1991)	^[202]
8	Erkak	72 yosh	Kuniga 300 mg	ALF	ND	Tirik qoldi	Yo'q	Pars va boshq. (1991)	^[203]
9	Erkak	65 yosh	Kuniga 300 mg	ALF	1 yil	O'lim	1,6 oy	Pars va boshq. (1991)	^[203]
10	Erkak	83 yil	Kuniga 300 mg	ALF	1,25 yil	O'lim	2 hafta	Pars va boshq. (1991)	^[203]
11	Erkak	78 yil	Kuniga 150 mg	AH	~ 3 oy	Tirik qoldi	Yo'q	Drakos va boshq. (1992)	^[204]
12	Ayol	24 yil	100 mg / kun (RS)	CH	3 oy	Tirik qoldi	Yo'q	Xassler va boshq. (1992)	^[205]
13	Erkak	74 yosh	Kuniga 200 mg	AH	11 oy	Tirik qoldi	Yo'q	Roila va boshq. (1993)	^[206]
14	Erkak	79 yil	Kuniga 300 mg	ALF	10 oy	O'lim	2 hafta	Bressollette va boshq. (1994)	^[207]
15	Erkak	92 yil	100 mg / kun	ALF	4 oy	O'lim	5 hafta	Xirsh va boshq. (1994)	^[208]
16	Erkak	65 yosh	Kuniga 600 mg	HCC	4 oy	Tirik qoldi	Yo'q	Kattan va boshq. (1994)	^[209]
17	Ayol	22 yil	100-250 mg / kun	HCC	10 yil	O'lim	9 oy	Vatanabe va boshq. (1994)	^[210]^[211]
18	Ayol	19 yil	200-300 mg / kun	HCC	9 yil	Tirik qoldi	Yo'q	Vatanabe va boshq. (1994)	^[210]^[211]
19	Ayol	19 yil	Kuniga 200 mg	HCC	~ 10 yil	Tirik qoldi	Yo'q	Vatanabe va boshq. (1994)	^[210]^[211]
20	Erkak	87 yil	Kuniga 200 mg	ALF	4 oy	O'lim	~ 3,5 hafta	Pinganaud va boshq. (1995)	^[212]
21	Erkak	78 yil	Kuniga 150 mg	ALF	1 yil	O'lim	3 hafta	Pinganaud va boshq. (1995)	^[212]
22	Ayol	45 yil	Kuniga 2 mg (BCP)	HCC	14 yil	O'lim	9 oy	Rudiger va boshq. (1995)	^[213]
23	Erkak	78 yil	200-300 mg / kun	ALF	3 oy	O'lim	9 oy	Castellani va boshq. (1996)	^[214]
24	Erkak	73 yil	Kuniga 300 mg	ALF	4 oy	Tirik qoldi	Yo'q	Merfi va boshq. (1996)	^[215]
25	Erkak	64 yil	100 mg / kun	AH	6 oy	Tirik qoldi	Yo'q	Ruiz-Rebollo va boshq. (1997)	^[216]
26	Ayol	≥8 yil	200-300 mg / kun	HCC	> 4 yil	Tirik qoldi	Yo'q	Vatanabe va boshq. (1997)	^[211]
27	Erkak	21 yil	100-350 mg / kun	HCC	15 yil	Tirik qoldi	Yo'q	Vatanabe va boshq. (1997)	^[211]
28	Erkak	84 yil	ND	ALF	ND	O'lim	1 hafta	Lombardi va boshq. (1998)	^[217]
29	Erkak	81 yil	Kuniga 300 mg	ALF	6 oy	O'lim	1,6 oy	Fridman va boshq. (1999)	^[218]
30	Erkak	66 yil	Kuniga 300 mg	ALF	2 oy	O'lim	4 hafta	Fridman va boshq. (1999)	^[218]
31	Erkak	14 yil	100 mg / kun	Siroz	~ 7,5 yil	O'lim	~ 1 yil	Garti va boshq. (1999)	^[219]
32	Erkak	84 yil	100-300 mg / kun	HCC	10 yil	O'lim	6 kun	Manfredi va boshq. (2000)	^[220]
33	Erkak	87 yil	Kuniga 300 mg	AH	ND	Tirik qoldi	Yo'q	Jiordano va boshq. (2001)	^[221]
34	Ayol	17 yil	Kuniga 2 mg (BCP)	AIH / siroz	2 oy	Tirik qoldi	Yo'q	Kacar va boshq. (2002)	^[222]
35	Erkak	76 yil	Kuniga 150 mg	AH	7 oy	Tirik qoldi	Yo'q	Manolakopoulos et al. (2004)	^[196]
36	Erkak	78 yil	200 mg/day	ALF	3 oy	O'lim	1.0 months	Famularo et al. (2005)	^[223]
37	Erkak	82 yil	200 mg/day	AH	12 oy	Tirik qoldi	Yo'q	Savidou et al. (2006)	^[224]
38	Erkak	83 yil	300 mg/day	AH	7 oy	O'lim	1.4 months	Savidou et al. (2006)	^[224]
39	Erkak	78 yil	300 mg/day	AH	3 oy	Tirik qoldi	Yo'q	Savidou et al. (2006)	^[224]
40	Erkak	78 yil	150 mg/day	ALF	2 oy	Tirik qoldi	Yo'q	Mikel va boshq. (2007)	^[195]
41^b	Ayol	22 yil	2 mg/day (BCP)	BCS	7 kun	ND	ND	U va boshqalar. (2009)	^[225]^[226]
42	Erkak	89 yil	150–300 mg/day	ALF	3.2 months	O'lim	28 kun	Kim va boshq. (2009)	^[227]
43	Erkak	71 yosh	100–200 mg/day	ALF	2-3 oy	O'lim	20 kun	Hsu et al. (2011)	^[228]
44	Erkak	66 yil	200 mg/day	AH/cirrhosis	4 oy	Tirik qoldi	Yo'q	Abenavoli et al. (2013)	^[229]
45	Erkak	75 yosh	200 mg/day	ALF	9 oy	Tirik qoldi	Yo'q	Vodička et al. (2013)	^[230]
46	Erkak	87 yil	200 mg/day	ALF	6 oy	O'lim	20 kun	Kim va boshq. (2014)	^[182]
47	Erkak	80 yil	150 mg/day	AH	4.0 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
48	Erkak	73 yil	200 mg/day	AH	2.1 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
49	Erkak	54 yosh	200 mg/day	AIH	4.0 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
50	Erkak	60 yil	200 mg/day	AH	1.1 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
51	Erkak	74 years	200 mg/day	AH	5.1 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
52	Erkak	66 yil	150 mg/day	ALF	3.2 months	O'lim	ND	Bessone et al. (2016)	^[188]
53	Erkak	77 yil	100 mg/day	AH	8.1 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
54	Erkak	72 yosh	200 mg/day	AH	5.0 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
55	Erkak	80 yil	200 mg/day	AH	1,9 oy	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
56	Erkak	69 years	100 mg/day	AH	4.1 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
57	Erkak	58 yil	200 mg/day	AH	10.1 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
58	Erkak	83 yil	100 mg/day	AH	2.1 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
59	Erkak	75 yosh	200 mg/day	AH	4.9 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
60	Erkak	72 yosh	100 mg/day	AH	8.0 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
61	Erkak	72 yosh	50 mg/day	AH	5.9 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
62	Erkak	66 yil	100 mg/day	AH/CH	1,2 yil	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
63	Erkak	58 yil	200 mg/day	ALF	5.0 months	O'lim	ND	Bessone et al. (2016)	^[188]
64	Erkak	75 yosh	200 mg/day	ALF	7.9 months	O'lim	ND	Bessone et al. (2016)	^[188]
65	Erkak	74 years	150 mg/day	AH	9.9 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
66	Erkak	64 yil	100 mg/day	AH	3.3 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
67	Erkak	64 yil	150 mg/day	AH/CH	4.9 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
68	Erkak	64 yil	150 mg/day	AH/cirrhosis	4.9 months	Tirik qoldi	Yo'q	Bessone et al. (2016)	^[188]
69	Erkak	61 yosh	300 mg/day	ALF	3 oy	O'lim	2.6 months	Nour et al. (2017)	^[231]
Qisqartmalar: BCP = Tug'ilishni nazorat qilish tabletkasi. RS = Reverse sequential (days 5–25 of cycle). ALF = O'tkir jigar etishmovchiligi (fulminant liver failure). AH = O'tkir gepatit. CH = Cholestatic hepatitis. AIH = Otoimmun gepatit. HCC = Gepatotsellulyar karsinoma. BCS = Budd-Chiari sindromi. ND = No data. N/A = Not applicable. Izohlar: ^a = Time until death after onset of liver toxicity. ^b = Probably related to etinilestradiol rather than to cyproterone acetate.^[225] Izohlar: Many additional cases have been described in spontaneous adverse drug reaction reporting systems of individual countries. These include 19 cases (5 deaths) by late 1988^[199] and 96 cases (91 males, 5 females; 33 deaths) by early 1995 in the Birlashgan Qirollik;^[185]^[186] 32 cases (deaths not given) in Avstraliya by 2004;^[232] and 15 cases (no deaths) in Ispaniya 2006 yilga kelib.^[233] The cases from Bessone et al. (2016) were reported between 1993 and 2013 and were from Spanish and Lotin Amerikasi drug-induced liver injury databases (17 cases in Argentina, 2 cases in Urugvay, 3 cases in Spain).^[188] Worldwide, 153 cases of liver abnormalities were reported to Schering, the manufacturer, between 1982 and 1987.^[199] In a large observational study of 2,506 patients, Heinemann et al. (1997) reported 7 cases of benign liver tumors and no cases of serious liver toxicity or HCC.^[19] Large observational studies have found no increased risk of liver toxicity or HCC with cyproterone acetate at BCP doses.^[19]^[234]^[235] A fatal case of ALF in a oddiy shimpanze haqida ham xabar berilgan.^[236] Manbalar: ^[224]^[193]^[218]

Vitamin B12 etishmasligi

Both low-dose (2 mg/day) and high-dose CPA combined with an estrogen have been associated with vitamin B12 etishmasligi in women in some small studies.^[237]^[238]^[7] Vitamin B12 deficiency in turn has been associated with depression, tashvish, asabiylashish va charchoq due to depletion of central monoamin nörotransmitterlari.^[239]^[240] For this reason, it has been suggested that low vitamin B12 levels might be involved in the side effect of depression that has sometimes been associated with CPA.^[23] Serum vitamin B12 monitoring and supplementation (e.g., 100 to 200 μg/day orally) as necessary may be recommended during CPA therapy.^[7]^[237]^[238]

Turli xil

CPA has been associated rarely with retinal vascular disorder, retinal tomir trombozi va optik nevrit.^[241] A case report of symptomatic epidural lipomatosis in association with CPA therapy has been published.^[242] A published case report of lymphocytic pneumonitis in associated with CPA also exists.^[4] There is a case report of severe strech belgilari in association with CPA therapy.^[243]

Dosage dependence

Belisle and Love (1986) directly compared Diane (2 mg/day CPA and 50 μg/day ethinylestradiol) with the combination of 100 mg/day CPA (Androcur) and Diane in 158 women with hirsutism reported no differences in mean incidences of side effects including menometrorragiya (9.9%), husnbuzar (6.5%), decreased libido (9.5%), shish (9.3%), ko'ngil aynish (17.5%), qusish (4.8%), bosh og'rig'i (20.3%), and depressiya (12.7%).^[5] Conversely, the incidences of charchoq va amenore were significantly greater in the Androcur group relative to the Diane group (6.7% vs. 2.5% and 5.4–32.6% vs. 0–4.2%, respectively), the incidence of ko'krak bezi was significantly lower in the Androcur group than in the Diane group (3.6–26.3% vs. 12.5–46.4%), and the percent gain in body weight relative to baseline was significantly greater in the Androcur group than in the Diane group (6.3% vs. 1.1% at 12 months).^[5]

Side effects of estrogen plus high- versus low-dose cyproterone acetate in women
Yon ta'siri	Yuqori doz^[c] (n = 602) (%)	Kam doz^[d] (n = 226) (%)
Charchoq	22.0	13.0
Vazn yig'moq (>2 kg or >4.4 lbs)	18.5	5.5
Libidoning pasayishi	10.0	6.0
Ko'krak bezovtaligi	9.2	15.0
Bulantı	9.0	3.9
Bosh og'rig'i	7.3	10.4
Depressiya	5.1	2.0
Irregular uterine bleeding	3.5	7.2
Uyqu buzilishi	3.5	–
Tromboflebit	1.0	3.0
Xloasma	0.9	–
Kabızlık	0.5	–
Tromboz	0.15	0.9
Og'ir oyoqlari yoki kramplar	–	4.6
Izohlar: ^ ^a ^b ^v Average dosage; range less than 10 mg/day to >200 mg/day. ^ Jigar fermentlari monitored in 1,685 individuals, including 1,131 males and 554 females. ^ Reverse sequential regimen: Ayollarda hirsutizm, cyproterone acetate 100 mg/day from days 5 to 14 of the menstrual cycle and etinilestradiol 50 μg/day from days 5 to 25 of the cycle. ^ Dayan: In women with hirsutism, cyproterone acetate 2 mg/day and ethinylestradiol 50 μg/day from days 5 to 25 of the cycle. Manbalar: Shablonga qarang.

Cheklash

Adrenal etishmovchilik

Abrupt chekinish of CPA can be harmful, and the package insert from Schering AG recommends the daily dose be reduced by no more than 50 mg at intervals of several weeks. The concern is the manner in which CPA affects the buyrak usti bezlari. Due to its glucocorticoid activity, high levels of CPA may reduce ACTH, resulting in buyrak usti etishmovchiligi if discontinued abruptly. In addition, although CPA reduces androgen production in the gonads, it can increase the production of adrenal androgens, in some cases resulting in an overall rise in testosterone levels.^[244] Thus, the sudden withdrawal of CPA could result in undesirable androgenic effects.^{[iqtibos kerak ]} This is a particular concern because androgens, especially DHT, suppress adrenal function, further reducing kortikosteroid ishlab chiqarish.^[245]

Bostirish adrenal function and reduced response to adrenokortikotropik gormon (ACTH) have been reported with CPA treatment. Natijada, buyrak usti etishmovchiligi and hence low kortizol va aldosteron levels and ACTH responsiveness can occur upon discontinuation of CPA. Low aldosterone levels may lead to giponatremi (natriy loss) and giperkalemiya (excess kaliy ). Patients taking CPA should have their cortisol levels and elektrolitlar monitored, and if hyperkalemia develops, should reduce the consumption of foods with high potassium content or discontinue the medication.

Adabiyotlar

^ Bachelot A, Chabbert-Buffet N, Salenave S, Kerlan V, Galand-Portier MB (2010 yil fevral). "Androgenga qarshi davolash". Ann. Endokrinol. (Parij). 71 (1): 19–24. doi:10.1016 / j.ando.2009.12.001. PMID 20096826.
^ Burton JL (December 1979). "Anti-androgen therapy in dermatology: a review". Klinika. Muddati Dermatol. 4 (4): 501–7. doi:10.1111/j.1365-2230.1979.tb01648.x. PMID 394887.
^ ^a ^b ^v ^d ^e ^f ^g Hammerstayn, J. (1990). "Antiandrogenlar: klinik jihatlar". Soch va soch kasalliklari. 827–886 betlar. doi:10.1007/978-3-642-74612-3_35. ISBN 978-3-642-74614-7.
^ ^a ^b Rittmaster RS (June 1999). "Antiandrogen treatment of polycystic ovary syndrome". Endokrinol. Metab. Klinika. Shimoliy Am. 28 (2): 409–21. doi:10.1016/S0889-8529(05)70077-3. PMID 10352926.
^ ^a ^b ^v ^d Belisle S, Love EJ (December 1986). "Clinical efficacy and safety of cyproterone acetate in severe hirsutism: results of a multicentered Canadian study". Urug'lantirish. Steril. 46 (6): 1015–20. doi:10.1016/S0015-0282(16)49873-0. PMID 2946604.
^ ^a ^b Diamanti-Kandarakis E (1998 yil oktyabr). "Polikistik tuxumdon sindromi bo'lgan bemorlarda faqat antiandrogen bilan davolash qanchalik dolzarb?". J. Endokrinol. Investitsiya. 21 (9): 623–9. doi:10.1007 / BF03350788. PMID 9856417.
^ ^a ^b ^v ^d ^e Diamanti-Kandarakis E (1999 yil sentyabr). "Ayollarda antiandrogen terapiyasining dolzarb jihatlari". Curr. Farm. Des. 5 (9): 707–23. PMID 10495361.
^ ^a ^b Guay DR (January 2009). "Drug treatment of paraphilic and nonparaphilic sexual disorders". Klinik The. 31 (1): 1–31. doi:10.1016/j.clinthera.2009.01.009. PMID 19243704. No quantitative data on these adverse events are available, even in the product prescribing information and data sheets.
^ ^a ^b ^v Migliari R, Muscas G, Murru M, Verdacchi T, De Benedetto G, De Angelis M (1999). "Antiandrogenlar: prostata saratoni terapiyasida farmakodinamik xususiyatlari va bardoshliligini qisqacha ko'rib chiqish". Archivio Italiano di Urologia e Andrologia. 71 (5): 293–302. PMID 10673793. The only advantage of cyproterone acetate on pure antiandrogens seems to be the low incidence of hot flushes; [...] However, hepatotoxicity associated with long term daily doses of 300 mg daily and the unacceptably high incidence of cardiovascular side effects (10%) should restrict its use to patients who are intolerant of pure antiandrogen compound. In contrast to steroidal compound nonsteroidal compounds let sexual potency to be retained, [...]
^ ^a ^b ^v Sara H. Vakelin (2002 yil 1-iyun). Dermatologiyada dori-darmonlarni tizimli davolash: qo'llanma. CRC Press. p. 32. ISBN 978-1-84076-013-2.
^ ^a ^b Graf, K.-J .; Brotherton, J .; Neumann, F. (1974). "Clinical Uses of Antiandrogens". Androgenlar II va antiandrogenlar / Androgene II und antiandrogene. 485-542 betlar. doi:10.1007/978-3-642-80859-3_7. ISBN 978-3-642-80861-6.
^ Iversen P, Melezinek I, Schmidt A (January 2001). "Nonsteroidal antiandrogens: a therapeutic option for patients with advanced prostate cancer who wish to retain sexual interest and function". BJU xalqaro. 87 (1): 47–56. doi:10.1046/j.1464-410x.2001.00988.x. PMID 11121992.
^ ^a ^b Terrence Priestman (26 May 2012). Cancer Chemotherapy in Clinical Practice. Springer Science & Business Media. 97– betlar. ISBN 978-0-85729-727-3.
^ Di Lorenzo G, Autorino R, Perdonà S, De Placido S (2005). "Management of gynaecomastia in patients with prostate cancer: a systematic review". Lanset Onkol. 6 (12): 972–9. doi:10.1016/S1470-2045(05)70464-2. PMID 16321765.
^ Hirawat S, Budman DR, Kreis W (June 2003). "The androgen receptor: structure, mutations, and antiandrogens". Saraton kasalligi. 21 (3): 400–17. doi:10.1081/CNV-120018232. PMID 12901287.
^ ^a ^b ^v ^d ^e Schröder FH, Whelan P, de Reijke TM, Kurth KH, Pavone-Macaluso M, Mattelaer J, van Velthoven RF, Debois M, Collette L (April 2004). "Metastatic prostate cancer treated by flutamide versus cyproterone acetate. Final analysis of the "European Organization for Research and Treatment of Cancer" (EORTC) Protocol 30892". Yevro. Urol. 45 (4): 457–64. doi:10.1016/j.eururo.2003.11.016. PMID 15041109.
^ Shiffman, Melvin A. (2012). "Cellulite: Etiology, Classification, Pathology, and Treatment". Estetik tibbiyot. pp. 265–272. doi:10.1007/978-3-642-20113-4_25. ISBN 978-3-642-20112-7.
^ ^a ^b "Mylan-Cyproterone Label" (PDF).
^ ^a ^b ^v ^d ^e Heinemann LA, Will-Shahab L, van Kesteren P, Gooren LJ (May 1997). "Safety of cyproterone acetate: report of active surveillance". Farmakoepidemiol dori vositasi. 6 (3): 169–78. doi:10.1002/(SICI)1099-1557(199705)6:3<169::AID-PDS263>3.0.CO;2-3. PMID 15073785.
^ "Androcur Label" (PDF).
^ James Barrett (2007). Transsexual and Other Disorders of Gender Identity: A Practical Guide to Management. Radcliffe Publishing. p. 174. ISBN 978-1-85775-719-4.
^ Barth JH, Cherry CA, Wojnarowska F, Dawber RP (July 1991). "Cyproterone acetate for severe hirsutism: results of a double-blind dose-ranging study". Klinik endokrinologiya. 35 (1): 5–10. doi:10.1111/j.1365-2265.1991.tb03489.x. PMID 1832346.
^ ^a ^b Rushton DH (July 2002). "Nutritional factors and hair loss". Klinika. Muddati Dermatol. 27 (5): 396–404. doi:10.1046/j.1365-2230.2002.01076.x. PMID 12190640.
^ Green HJ, Pakenham KI, Headley BC, Yaxley J, Nicol DL, Mactaggart PN, Swanson C, Watson RB, Gardiner RA (September 2002). "Altered cognitive function in men treated for prostate cancer with luteinizing hormone-releasing hormone analogues and cyproterone acetate: a randomized controlled trial" (PDF). BJU Int. 90 (4): 427–32. doi:10.1046/j.1464-410X.2002.02917.x. hdl:10072/16905. PMID 12175403.
^ Kaisary AV (2005). "Evaluating the use of early hormonal therapy in patients with localised or locally advanced prostate cancer". Prostate Cancer Prostatic Dis. 8 (2): 140–51. doi:10.1038/sj.pcan.4500800. PMID 15852051.
^ ^a ^b Green HJ, Pakenham KI, Headley BC, Yaxley J, Nicol DL, Mactaggart PN, Swanson CE, Watson RB, Gardiner RA (May 2004). "Quality of life compared during pharmacological treatments and clinical monitoring for non-localized prostate cancer: a randomized controlled trial". BJU Int. 93 (7): 975–9. doi:10.1111/j.1464-410X.2004.04763.x. hdl:10072/16906. PMID 15142146.
^ Seal LJ, Franklin S, Richards C, Shishkareva A, Sinclaire C, Barrett J (December 2012). "Predictive markers for mammoplasty and a comparison of side effect profiles in transwomen taking various hormonal regimens". Klinik endokrinologiya va metabolizm jurnali. 97 (12): 442–8. doi:10.1210/jc.2012-2030. PMID 23055547.
^ Gava G, Cerpolini S, Martelli V, Battista G, Seracchioli R, Meriggiola MC (August 2016). "Cyproterone acetate vs leuprolide acetate in combination with transdermal oestradiol in transwomen: a comparison of safety and effectiveness". Klinika. Endokrinol. (Oxf). 85 (2): 239–46. doi:10.1111/cen.13050. PMID 26932202.
^ Colizzi M, Costa R, Todarello O (January 2014). "Transseksual bemorlarning psixiatrik komorbidligi va o'zaro faoliyat jinsiy gormonal davolashning ruhiy salomatlikka ijobiy ta'siri: bo'ylama tadqiqot natijalari". Psixonuroendokrinologiya. 39: 65–73. doi:10.1016 / j.psyneuen.2013.09.029. PMID 24275005.
^ Fisher AD, Castellini G, Ristori J, Casale H, Cassioli E, Sensi C, Fanni E, Amato AM, Bettini E, Mosconi M, Déttore D, Ricca V, Maggi M (Noyabr 2016). "Jinsiy aloqada gormonlarni davolash va transseksual odamlarda psixobiologik o'zgarishlar: ikki yillik kuzatuv ma'lumotlari" (PDF). J. klinikasi. Endokrinol. Metab. 101 (11): 4260–4269. doi:10.1210 / jc.2016-1276. PMID 27700538.
^ ^a ^b Raudrant D, Rabe T (2003). "Antiandrogenik xususiyatlarga ega progestogenlar". Giyohvand moddalar. 63 (5): 463–92. doi:10.2165/00003495-200363050-00003. PMID 12600226.
^ Dengizchi HE, Snowball J, de Vries CS (2006). "Kiproteron asetat + etinioloestradiol va depressiya xavfi". Farmakoepidemiologiya va dori vositalari xavfsizligi. 15 (S1): S25. doi:10.1002 / pds.1295. ISSN 1053-8569. PMID 16986216.
^ Husmann, Fridrix (1997). "Gormonlarni almashtirish uchun Estradiol Valerate va Cyproterone Acetate kombinatsiyasi bilan klinik tajribalar". Ayollar salomatligi va menopauza. Tibbiyot fanlari bo'yicha simpoziumlar seriyasi. 11. 257-261 betlar. doi:10.1007/978-94-011-5560-1_38. ISBN 978-94-010-6343-2. ISSN 0928-9550.
^ ^a ^b Waken SH, Maibach HI, Archer CB (2015 yil 21-may). Dermatologiyada dori-darmonlarni tizimli davolash bo'yicha qo'llanma (Ikkinchi nashr). CRC Press. 34– betlar. ISBN 978-1-4822-2286-9.
^ ^a ^b ^v ^d ^e ^f ^g ^h ^men ^j ^k ^l ^m Giltay EJ, Gooren LJ (2009). "Jinsiy jinoyatchilarda androgen etishmovchiligini davolashning potentsial yon ta'siri". J. Am. Akad. Psixiatriya qonuni. 37 (1): 53–8. PMID 19297634.
^ ^a ^b ^v Briken P, Hill A, Berner V (avgust 2003). "Luteinlashtiruvchi gormonni chiqaradigan gormonning uzoq muddatli agonistlari bilan parafiliyalarning farmakoterapiyasi: tizimli ko'rib chiqish". J klinik psixiatriya. 64 (8): 890–7. doi:10.4088 / JCP.v64n0806. PMID 12927003.
^ ^a ^b ^v Wibowo E, Schellhammer P, Wassersug RJ (2011 yil yanvar). "Erkakning normal faoliyatidagi estrogenning roli: prostata saratoni bilan og'rigan bemorlarning androgen etishmovchiligini davolash bo'yicha klinik ta'siri". J. Urol. 185 (1): 17–23. doi:10.1016 / j.juro.2010.08.094. PMID 21074215.
^ ^a ^b ^v ^d ^e Yagelska, Beata; Poniatowska, Grenna; Talasevich, Konrad; Demkov, Tomash; Wiechno, Pawel (2017). "Prostata va ko'krak bezi saratonini gormonal davolashda tizimli asoratlar". Nowotwory. Onkologiya jurnali. 67 (3): 206–214. doi:10.5603 / NJO.2017.0034. ISSN 2300-2115.
^ ^a ^b ^v Grassvik LJ, Bredford JM (2003 yil iyul). "Parafiliyani davolash bilan bog'liq osteoporoz: ettita hisobotni klinik ko'rib chiqish". J. Sud-tibbiyot fanlari doktori. 48 (4): 849–55. doi:10.1520 / JFS2002089. PMID 12877306.
^ Lindsay R (1999). "Suyakka progestogen ta'sirining etishmasligi". J Reprod Med. 44 (2 ta qo'shimcha): 215-20. PMID 11392035.
^ Kertis, Ketrin M.; Martins, Yozgi L. (2006). "Faqatgina progestogen kontratseptsiyasi va suyak minerallarining zichligi: tizimli tahlil". Kontratseptsiya. 73 (5): 470–487. doi:10.1016 / j.contraception.2005.12.010. ISSN 0010-7824. PMID 16627031.
^ Sarfati, Juli; de Vernejoul, Mari-Kristin (2009). "Faqatgina estrodiol va progestogen kontratseptiv vositalarining suyak mineral zichligiga ta'siri". Qo'shma suyak umurtqasi. 76 (2): 134–138. doi:10.1016 / j.jbspin.2008.09.014. ISSN 1297-319X. PMID 19181558.
^ Nelson ER, Wardell SE, McDonnell DP (mart 2013). "Estrogenlar, SERMlar va oksisterollarning farmakologik ta'siriga asoslangan molekulyar mexanizmlar: osteoporozni davolash va oldini olish uchun ta'siri". Suyak. 53 (1): 42–50. doi:10.1016 / j.bone.2012.11.011. PMC 3552054. PMID 23168292.
^ Spona J, Lunglmayr G (1980 yil iyul). Prolaktin-Serumspiegel unter Behandlung des Prostatakarzinoms mit Östradiol-17 beta-undezylat und Cyproteronazetat [Estradiol-17 beta-undesilat va siproteron asetat bilan prostata saratonini davolash paytida sarum prolaktin darajasi.]. Wien. Klin. Voxenschr. Verhandlungsbericht der Deutschen Gesellschaft für Urologie (nemis tilida). 92. 494-7 betlar. doi:10.1007/978-3-642-81706-9_120. ISBN 978-3-540-11017-0. ISSN 0043-5325. PMID 6933738.
^ ^a ^b Shюрmeyer, Th .; Graf J.; Senge, Th .; Nieschlag, E. (1986). "Prostata karsinomasi bilan kasallangan bemorlarda estrogen yoki siproteron asetat bilan davolashning adrenokortikal funktsiyaga ta'siri". Acta Endocrinologica. 111 (3): 360–367. doi:10.1530 / akta.0.1110360. ISSN 0804-4643. PMID 2421511.
^ Xolub, G.; Lunglmayr, G.; Spona, J. (1981). "Prostata saratoni bilan kasallangan bemorlarda siproteron / asetatning (SH-714) plazmadagi prolaktinga ta'siri". Urologik tadqiqotlar. 9 (5): 245–7. doi:10.1007 / BF00256895. ISSN 0300-5623. PMID 6458145.
^ Rost, A .; Shmidt-Gollvitser, M.; Xantelmann, V.; Brosig, V. (1981). "Prostata saratoni bilan og'rigan bemorlarga mushak ichiga siproteron asetat yuborilgandan so'ng plazmadagi siproteron asetat, testosteron, LH, FSH va prolaktin miqdori". Prostata. 2 (3): 315–322. doi:10.1002 / pros.2990020310. ISSN 0270-4137. PMID 6458025.
^ Jeffcoate, W. J.; Metyus, R. V.; Edvards, C. R. V.; Field, L. H .; Besser, G. M. (1980). "Kiproteron asetatning qon zardobidagi testosteron, LH, FSH va prolaktinga jinsiy aloqada bo'lgan erkaklarda ta'siri". Klinik endokrinologiya. 13 (2): 189–195. doi:10.1111 / j.1365-2265.1980.tb01041.x. ISSN 0300-0664. PMID 6777092.
^ Graf, K. J., Shmidtgollvitser, M., Koch, U. J., Lorenz, F. va Hammerstayn, J. (1978, yanvar). Kiproteron asetat tomonidan inson sub'ektlarida paydo bo'lgan giperprolaktinemiya. Acta Endocrinologica-da (87-jild, 96-96-betlar).
^ Bercovich, E., Cigno, M., & Soli, M. (1983, yanvar). Prostata karsinomasi bo'lgan bemorlarda siproteron asetat terapiyasi natijasida kelib chiqadigan sarum prolaktin darajasi. Prostatda (4-jild, 4-son, 425-426-betlar).
^ ^a ^b Defreyne J, Nota N, Pereyra S, Shrayner T, Fisher AD, den Heijer M, T'Sjoen G (oktyabr 2017). "Trans ayollarda sarum prolaktinning vaqtincha ko'tarilishi, kiproteron asetat bilan davolash natijasida yuzaga keladi". LGBT sog'liqni saqlash. 4 (5): 328–336. doi:10.1089 / lgbt.2016.0190. PMID 28880825.
^ Fonzo, Domeniko; Anjeli, Alberto; Sivieri, Roberto; Andriolo, Salvatore; Fraxriya, Roberto; Ceresa, Franko (1977). "Kiproteron asetat bilan uzoq muddatli davolanishda idiopatik erta balog'atga etgan qizlarda giperprolaktinemiya". Klinik endokrinologiya va metabolizm jurnali. 45 (1): 164–168. doi:10.1210 / jcem-45-1-164. ISSN 0021-972X. PMID 874063.
^ ^a ^b ^v ^d ^e Mah, tepalik Mann; Vebster, Jonathan (2002). "Giperprolaktinemiya: etiologiya, diagnostika va boshqarish". Reproduktiv tibbiyot bo'yicha seminarlar. 20 (4): 365–374. doi:10.1055 / s-2002-36709. ISSN 1526-8004. PMID 12536359.
^ ^a ^b ^v ^d ^e ^f Gil M, Oliva B, Timoner J, Macia MA, Bryant V, de Abajo FJ (dekabr 2011). "Kiproteron asetatning yuqori dozalarini iste'mol qiluvchilar orasida umumiy populyatsiya bilan taqqoslaganda meningioma xavfi: populyatsiyaga asoslangan kogort tadqiqotining dalillari". Br J Clin Farmakol. 72 (6): 965–8. doi:10.1111 / j.1365-2125.2011.04031.x. PMC 3244644. PMID 21627676.
^ Uilyams, Robert F.; Janfortoni, Jozef G.; Xodgen, Gari D. (1985). "Estrogen-progesteron sinergiyasi keltirib chiqaradigan giperprolaktinemiya: maymunlarda estrogen primeratsiyasining miqdoriy va vaqtinchalik ta'siri *". Klinik endokrinologiya va metabolizm jurnali. 60 (1): 126–132. doi:10.1210 / jcem-60-1-126. ISSN 0021-972X. PMID 3964786.
^ Uilyams, Robert F.; Sartarosh, Donald L.; Kovan, Brayan D. Linch, Almorris; Marut, Edvard L.; Xodgen, Gari D. (1981). "Maymunlarda giperprolaktinemiya: estrogen-progesteron sinergiyasi orqali induksiya". Ukol. 38 (3): 321–331. doi:10.1016 / 0039-128X (81) 90067-2. ISSN 0039-128X. PMID 7303037.
^ Molts, L .; Romler, A .; Pochta, K .; Shvarts, U .; Hammerstayn, J. (1980). "O'rtacha dozada siproteron asetat (CPA): gormon sekretsiyasiga va erkaklarda spermatogenezga ta'siri". Kontratseptsiya. 21 (4): 393–413. doi:10.1016 / S0010-7824 (80) 80017-5. ISSN 0010-7824. PMID 6771095.
^ Molts, L .; Romler, A .; Shvarts, U .; Pochta, K .; Hammerstayn, J. (1978). "252. Cyproterone asetate (CPA) - potentsial erkak kontratseptivi: endokrin parametrlar bilan o'zaro ta'sirlarni o'rganish". Steroid biokimyosi jurnali. 9 (9): 865. doi:10.1016/0022-4731(78)90952-4. ISSN 0022-4731.
^ Molts, L .; Romler, A .; Shvarts, U .; Hammerstayn, J. (1978). "Cyproterone Acetate (CPA) ning gipofiz gonadotrofini chiqarilishiga va erkaklarda LH-RH qo'shaloq stimulyatsiya testlaridan oldin va keyin Androgen sekretsiyasiga ta'siri". Xalqaro Andrologiya jurnali. 1 (s2b): 713-719. doi:10.1111 / j.1365-2605.1978.tb00518.x. ISSN 0105-6263.
^ Meriggiola, M. C .; Kostantino, A .; Cerpolini, S .; Bremner, V. J.; Xyebler, D.; Morselli-Labate, A. M.; Kirsh, B .; Bertachini, A .; Pelusi, S.; Pelusi, G. (2003). "Testosteron undekanoat oddiy erkaklarda kiproteron asetat plyus testosteron undekanoat tomonidan spermatogen ta'sirni to'xtatadi". Klinik endokrinologiya va metabolizm jurnali. 88 (12): 5818–5826. doi:10.1210 / jc.2003-030574. ISSN 0021-972X. PMID 14671175.
^ ^a ^b ^v ^d ^e ^f Asscheman H, Gooren LJ, Eklund PL (sentyabr 1989). "Jinsiy gormonlar bilan davolash qilingan transseksual bemorlarda o'lim va kasallanish" (PDF). Metab. Klinika. Muddati. 38 (9): 869–73. doi:10.1016/0026-0495(89)90233-3. PMID 2528051.
^ ^a ^b ^v ^d Asscheman H, Gooren LJ, Assies J, Smits JP, de Slegte R (iyun 1988). "Prolaktin darajasi va gipofizning kengayishi gormon bilan davolash qilingan erkak va ayol transseksuallari". Klinika. Endokrinol. (Oxf). 28 (6): 583–8. doi:10.1111 / j.1365-2265.1988.tb03849.x. PMID 2978262.
^ ^a ^b ^v ^d ^e ^f Gooren LJ, Harmsen-Louman V, van Kessel H (1985 yil fevral). "Prolaktinom induktsiyasiga nisbatan uzoq muddatli estrogen bilan davolash qilingan erkak va ayol transseksuallarda prolaktin miqdorini kuzatib borish". Klinika. Endokrinol. (Oxf). 22 (2): 201–7. doi:10.1111 / j.1365-2265.1985.tb01081.x. PMID 3157511.
^ Kapozzi, Anna; Skambiya, Jovanni; Pontekorvi, Alfredo; Lello, Stefano (2015). "Giperprolaktinemiya: patofiziologiya va terapevtik yondashuv". Ginekologik endokrinologiya. 31 (7): 506–510. doi:10.3109/09513590.2015.1017810. ISSN 0951-3590. PMID 26291795.
^ Naidoo, U .; Goff, DC; Klibanski, A. (2003). "Giperprolaktinemiya va suyak mineral zichligi: antipsikotik vositalarning potentsial ta'siri". Psixonuroendokrinologiya. 28: 97–108. doi:10.1016 / S0306-4530 (02) 00129-4. ISSN 0306-4530. PMID 12650684.
^ ^a ^b ^v Rastrelli, Giuliya; Korona, Jovanni; Maggi, Mario (2015). "Prolaktinning andrologiyadagi o'rni: nima yangilik?". Endokrin va metabolik kasalliklarning sharhlari. 16 (3): 233–248. doi:10.1007 / s11154-015-9322-3. ISSN 1389-9155. PMID 26542707.
^ ^a ^b Buvat, J (2003). "Giperprolaktinemiya va erkaklarda jinsiy funktsiya: qisqa sharh". Immunitetni o'rganish bo'yicha xalqaro jurnal. 15 (5): 373–377. doi:10.1038 / sj.ijir.3901043. ISSN 0955-9930. PMID 14562140.
^ ^a ^b Kruger, T (2002). "Orgazmdan kelib chiqadigan prolaktin sekretsiyasi: jinsiy aloqani qayta tiklash nazorati?". Neuroscience & Biobehavioral Sharhlar. 26 (1): 31–44. doi:10.1016 / S0149-7634 (01) 00036-7. ISSN 0149-7634. PMID 11835982.
^ ^a ^b ^v Verxelst, Yoxan; Abs, Rojer (2003). "Giperprolaktinemiya". Endokrinologiyada davolash usullari. 2 (1): 23–32. doi:10.2165/00024677-200302010-00003. ISSN 1175-6349. PMID 15871552.
^ La Torre D, Falorni A (2007). "giperprolaktinemiyaning garmonik sabablari". Terapevtik va klinik xatarlarni boshqarish. 3 (5): 929–951. PMC 2376090. PMID 18473017.
^ Schlatterer K, Yassouridis A, fon Verder K, Polsha D, Kemper J, Stalla GK (oktyabr 1998). "Transseksual bemorlarga xoch-gender gormonlarini almashtirish terapiyasining samaradorligini baholash bo'yicha keyingi tadqiqotlar". Arch Sex Behav. 27 (5): 475–92. doi:10.1023 / a: 1018704630036. PMID 9795728.
^ Bazarra-Kastro, M. Á. (2009). Transseksual bemorlarning etiologik jihatlari, terapiya rejimi, yon ta'siri va davolanishdan qoniqishi (doktorlik dissertatsiyasi, LMU Myunxen). doi: 10.5282 / edoc.9984
^ Frouli, L. Stiven; Porter, Tom E.; Kineman, Rhonda D. (1990). "Prolaktinning maqsadli hujayralarga ta'siri". Neyroendokrin istiqbollari. 8. 39-75 betlar. doi:10.1007/978-1-4612-3446-3_2. ISBN 978-1-4612-8014-9. ISSN 0168-0617.
^ Bole-Feysot, Kristin; Goffin, Vinsent; Ederi, Mark; Binart, Nadin; Kelly, Pol A. (1998). "Prolaktin (PRL) va uning retseptorlari: harakatlar, signal uzatish yo'llari va PRL retseptorlari nokautli sichqonlarida kuzatiladigan fenotiplar". Endokrin sharhlar. 19 (3): 225–268. doi:10.1210 / edrv.19.3.0334. ISSN 0163-769X. PMID 9626554.
^ Xiguchi, Kazumi; Navata, Xajime; Maki, Toshio; Xigashizima, Masayoshi; Kato, Ken-Ichi; Ibayashi, Xiroshi (1984). "Prolaktin buyrak usti bezining androgen sekretsiyasiga bevosita ta'sir qiladi". Klinik endokrinologiya va metabolizm jurnali. 59 (4): 714–718. doi:10.1210 / jcem-59-4-714. ISSN 0021-972X. PMID 6090494.
^ Shibinger, Rik J.; Chrousos, Jorj P.; Kulter, Gordon B.; Loriaux, D. Lin (1986). "Qon zardobidagi prolaktinning plazmadagi buyrak usti androgenlariga ta'siri va normal va giperprolaktinemik mavzulardagi dehidroepiandrosteron sulfatning ishlab chiqarish va metabolizm darajasi". Klinik endokrinologiya va metabolizm jurnali. 62 (1): 202–209. doi:10.1210 / jcem-62-1-202. ISSN 0021-972X. PMID 2999177.
^ Langan, Evan A.; Xinde, Eleanora; Paus, Ralf (2018). "Prolaktin sebotrop (h) ic gormoni nomzodi sifatida?". Eksperimental dermatologiya. 27 (7): 729–736. doi:10.1111 / exd.13545. ISSN 0906-6705. PMID 29582473.
^ ^a ^b Pucci E, Petraglia F (1997 yil dekabr). "Ayollarda androgen ortiqcha davolash: kecha, bugun va ertaga". Jinekol. Endokrinol. 11 (6): 411–33. doi:10.3109/09513599709152569. PMID 9476091.
^ Miller JA, Jacobs HS (may 1986). "Hirsutizm va husnbuzarlarni siproteron asetat bilan davolash". Klinik Endokrinol Metab. 15 (2): 373–89. doi:10.1016 / S0300-595X (86) 80031-7. PMID 2941191.
^ ^a ^b ^v ^d ^e Raj R, Korja M, Koroknay-Pal P, Niemelä M (2018). "Gormonlarni almashtirish terapiyasi bilan olib borilgan ikkita erkak-ayol transseksual bemorlarda bir nechta meningioma: ikkita holat bo'yicha hisobot va qisqacha adabiyotlarni ko'rib chiqish". Surg Neurol Int. 9: 109. doi:10.4103 / sni.sni_22_18. PMC 5991277. PMID 29930875.
^ ^a ^b ^v ^d ^e ^f Nota NM, Wiepjes CM, de Blok C, Gooren LJ, Peerdeman SM, Kreukels B, den Heijer M (iyul 2018). "Jinsiy aloqada gormonlarni davolash paytida transseksual odamlarda yaxshi xulqli miya shishi paydo bo'lishi". Miya. 141 (7): 2047–2054. doi:10.1093 / miya / awy108. PMID 29688280.
^ J. Larri Jeymson; Lesli J. De Groot (2015 yil 25-fevral). Endokrinologiya: kattalar va bolalar uchun elektron kitob. Elsevier sog'liqni saqlash fanlari. 2293, 2464, 2479, 6225-betlar. ISBN 978-0-323-32195-2.
^ Meningeal neoplazmalar - tadqiqot va davolashning yutuqlari: 2012 yil nashr: ScholarlyBrief. ScholarlyEditions. 26 dekabr 2012. 99- bet. ISBN 978-1-4816-0002-6.
^ Dikman A (2012 yil 27 sentyabr). Palliativ yordamda giyohvand moddalar. Oksford. 137-138 betlar. ISBN 978-0-19-966039-1.
^ ^a ^b ^v Schmutz JL (2018 yil may). "Méningiomes et acétate de cyprotérone: mise au point" [Cyproterone acetate and meningioma: So'nggi topilmalar]. Ann Dermatol Venereol (frantsuz tilida). 145 (5): 390–391. doi:10.1016 / j.annder.2018.04.001. PMID 29703641.
^ Blankenshteyn MA, Verheijen FM, Jacobs JM, Donker TH, van Duijnhoven MW, Thijssen JH (2000). "Progesteron retseptorlari paydo bo'lishi, boshqarilishi va inson meningiomasida ahamiyati". Ukol. 65 (10–11): 795–800. doi:10.1016 / S0039-128X (00) 00193-8. PMID 11108890.
^ Shlomo Melmed (2010 yil 9-dekabr). Gipofiz. Akademik matbuot. 227– betlar. ISBN 978-0-12-380927-8.
^ Knobil va Neillning ko'payish fiziologiyasi. Akademik matbuot. 2005 yil 12 dekabr. 1557– betlar. ISBN 978-0-08-053527-2.
^ Mark A. Fritz; Leon Speroff (2011). Klinik ginekologik endokrinologiya va bepushtlik. Lippincott Uilyams va Uilkins. 1091– betlar. ISBN 978-0-7817-7968-5.
^ ^a ^b ^v ^d ^e Manchini I, Rotilio A, Coati I, Seracchioli R, Martelli V, Meriggiola MC (iyun 2018). "To'qqiz yillik siproteron asetat va estradiolni qabul qilganidan keyin transminologda meningioma prezentatsiyasi: holatlar bo'yicha hisobot va adabiyotlarni o'rganish". Jinekol. Endokrinol. 34 (6): 456–459. doi:10.1080/09513590.2017.1395839. PMID 29105524.
^ ^a ^b ^v ^d ^e ^f Ter Vengel PV, Martin E, Gooren L, Den Heijer M, Peerdeman SM (dekabr 2016). "Ostrogenlar / progestogenlar va adabiyotlarni ko'rib chiqish yordamida uchta erkak va ayol transgender sub'ektlarida menenjiyomalar". Andrologiya. 48 (10): 1130–1137. doi:10.1111 / va.12550. PMID 26888610.
^ Gruber CJ, Huber JC (2003 yil dekabr). "Progestinlarning miyaga differentsial ta'siri". Maturitalar. 46 Qo'shimcha 1: S71-5. doi:10.1016 / j.maturitas.2003.09.021. PMID 14670648.
^ Hensiek AE, Kellerman AJ, Hill JT (2000 yil avgust). "Buyrak karsinomasida miya yarim metastazlarining o'z-o'zidan regressiyasi, so'ngra medroksiprogesteron asetat terapiyasi ostida meningioma rivojlanishi". Br J Neurosurg. 14 (4): 354–6. doi:10.1080/026886900417388. PMID 11045205.
^ Passeri T, Shampan PO, Bernat AL, Xanakita S, Salle H, Mandonnet E, Froelich S (aprel, 2019). "Nomegestrol asetat uzilishidan so'ng meningiomalarning o'z-o'zidan regressiyasi: uchta bemorning ketma-ketligi". Acta Neurochir (Wien). 161 (4): 761–765. doi:10.1007 / s00701-019-03848-x. PMID 30783806.
^ ^a ^b Gooren LJ, Assies J, Asscheman H, de Slegte R, van Kessel H (fevral, 1988). "Erkakdagi estrogen ta'siridagi prolaktinoma". J. klinikasi. Endokrinol. Metab. 66 (2): 444–6. doi:10.1210 / jcem-66-2-444. PMID 3339116.
^ Serri O, Noiseux D, Robert F, Hardy J (sentyabr 1996). "Estrogen bilan davolash qilingan erkak va ayol transseksual bemorda laktotrof giperplaziyasi". J. klinikasi. Endokrinol. Metab. 81 (9): 3177–9. doi:10.1210 / jcem.81.9.8784065. PMID 8784065.
^ ^a ^b García-Malpartida K, Martin-Gorgojo A, Rocha M, Gomes-Balaguer M, Hernández-Mijares A (avgust 2010). "Erkak va ayol transseksualida estrogen va siproteron asetat tomonidan qo'zg'atilgan prolaktinoma". Urug'lantirish. Steril. 94 (3): 1097.e13-5. doi:10.1016 / j.fertnstert.2010.01.076. PMID 20227072.
^ ^a ^b ^v Bunck MC, Debono M, Giltay EJ, Verheijen AT, Diamant M, Gooren LJ (2009). "An'anaviy estrogen dozalarini qo'llagan holda, transgender bo'lgan ikki erkakdan ayolga avtonom prolaktin sekretsiyasi". BMJ ishi vakili. 2009: bcr0220091589. doi:10.1136 / bcr.02.2009.1589. PMC 3029513. PMID 21829422.
^ ^a ^b ^v Cunha FS, Domenice S, Kamara VL, Sircili MH, Gooren LJ, Mendonça BB, Kosta EM (Avgust 2015). "Yuqori dozada o'zaro faoliyat jinsiy gormonlar terapiyasidan so'ng ikki erkak va ayol transseksual sub'ektlarda prolaktinoma diagnostikasi". Andrologiya. 47 (6): 680–4. doi:10.1111 / va.12317. PMID 25059808.
^ ^a ^b Gazzeri R, Galarza M, Gazzeri G (2007 yil dekabr). "Transseksual bemorda menenjiyomaning estrogen-progestin terapiyasidan keyin o'sishi". N. Engl. J. Med. 357 (23): 2411–2. doi:10.1056 / NEJMc071938. PMID 18057351.
^ ^a ^b Deipolyi AR, Xan SJ, Parsa AT (oktyabr 2010). "Gormon terapiyasini boshlaganidan keyin erkak va ayol transseksualda simptomatik intrakranial meningioma rivojlanishi". J Clin Neurosci. 17 (10): 1324–6. doi:10.1016 / j.jocn.2010.01.036. PMID 20594855.
^ ^a ^b Cebula H, Pham TQ, Boyer P, Froelich S (2010 yil noyabr). "Transseksual bemorda siproteron asetat to'xtatilgandan so'ng meningiomalarning regressiyasi". Acta Neurochir (Wien). 152 (11): 1955–6. doi:10.1007 / s00701-010-0787-2. PMID 20811919.
^ ^a ^b Bergoglio MT, Gomes-Balaguer M, Almonacid Folch E, Hurtado Murillo F, Hernández-Mijares A (may, 2013). "Erkak va ayol transseksualida o'zaro faoliyat jinsiy gormonlarni davolash natijasida kelib chiqadigan simptomatik meningioma". Endokrinol Nutr. 60 (5): 264–7. doi:10.1016 / j.endonu.2012.07.004. PMID 23022362.
^ Myuller A, Gooren L (sentyabr 2008). "Jinsiy gormonlar bilan davolanadigan transseksuallarda gormon bilan bog'liq o'smalar". Yevro. J. Endokrinol. 159 (3): 197–202. doi:10.1530 / EJE-08-0289. PMID 18567667.
^ ^a ^b Cea-Soriano L, Blenk T, Wallander MA, Rodriges LA (aprel 2012). "Gormonal terapiya va meningioma: aloqasi bormi?". Saraton epidemiyasi. 36 (2): 198–205. doi:10.1016 / j.canep.2011.08.003. PMID 21943794.
^ ^a ^b Hembree WC, Cohen-Kettenis PT, Gooren L, Hannema SE, Meyer WJ, Murad MH, Rosenthal SM, Safer JD, Tangpricha V, T'Sjoen GG (2017 yil noyabr). "Gender-disforik / jinsga mos kelmaydigan shaxslarni endokrin davolash: endokrin jamiyatning klinik amaliyoti bo'yicha ko'rsatma". J. klinikasi. Endokrinol. Metab. 102 (11): 3869–3903. doi:10.1210 / jc.2017-01658. PMID 28945902.
^ ^a ^b McFarlane T, Zajac JD, Cheung AS (dekabr 2018). "Genderni tasdiqlovchi gormon terapiyasi va transgenderlarda jinsiy gormonga bog'liq o'smalar paydo bo'lishi xavfi-Tizimli tekshiruv". Klinika. Endokrinol. (Oxf). 89 (6): 700–711. doi:10.1111 / sen.13835. PMID 30107028.
^ ^a ^b Oettel M, Schillinger E (2012 yil 6-dekabr). Estrogenlar va antiestrogenlar II: Estrogenlar va antiestrogenlarning farmakologiyasi va klinik qo'llanilishi. Springer Science & Business Media. 544– betlar. ISBN 978-3-642-60107-1.
^ ^a ^b Kovacs K, Stefaneanu L, Ezzat S, Smith HS (may 1994). "Uzoq muddatli estrogen yuborilishi bilan erkak va ayol transseksual bemorda prolaktin ishlab chiqaradigan gipofiz adenomasi. Morfologik tadqiqot". Arch. Pathol. Laboratoriya laboratoriyasi. Med. 118 (5): 562–5. PMID 8192565.
^ ^a ^b Giraldi, Laura; Xansen, Yorgen Vinslov; Vohlfahrt, Jan; Xayr, jinnilar; Fugleholm, Kare; Munk, Tina Norgaard (2019). "Erkaklar gormonlariga xalaqit beradigan dorilar va meningioma rivojlanishi". Neyro-onkologiya yutuqlari. 1. doi:10.1093 / noajnl / vdz046. ISSN 2632-2498.
^ Kang BM, Youn SM (oktyabr 2019). "Meningiomani simikatsiya qiladigan suprasellar gemangioblastoma holati". Miya o'simtasini davolash. 7 (2): 147–150. doi:10.14791 / btrt.2019.7.e40. PMC 6829077. PMID 31686447.
^ Serri O, Noiseux D, Robert F, Hardy J (sentyabr 1996). "Estrogen bilan davolangan erkak va ayol transseksual bemorda laktotrof giperplaziyasi". J. klinikasi. Endokrinol. Metab. 81 (9): 3177–9. doi:10.1210 / jcem.81.9.8784065. PMID 8784065.
^ ^a ^b ^v ^d ^e ^f ^g ^h ^men ^j ^k ^l ^m ⁿ ^o ^p ^q Nota NM, Wiepjes CM, de Blok C, Gooren LJ, Peerdeman SM, Kreukels B, den Heijer M (iyul 2018). "Jinsiy aloqada gormonlarni davolash paytida transgenderlarda miyada yaxshi xulqli o'smalar paydo bo'lishi". Miya. 141 (7): 2047–2054. doi:10.1093 / miya / awy108. PMID 29688280.
^ van Kesteren PJ, Asscheman H, Megens JA, Gooren LJ (sentyabr 1997). "Jinsiy gormonlar bilan davolash qilingan transseksual sub'ektlarda o'lim va kasallanish". Klinika. Endokrinol. (Oxf). 47 (3): 337–42. doi:10.1046 / j.1365-2265.1997.2601068.x. PMID 9373456.
^ Futterweit V (1998 yil aprel). "Transseksualizmning endokrin terapiyasi va uzoq muddatli davolanishning mumkin bo'lgan asoratlari". Arch Sex Behav. 27 (2): 209–26. doi:10.1023 / A: 1018638715498. PMID 9562902.
^ ^a ^b McFarlane T, Zajac JD, Cheung AS (dekabr 2018). "Genderni tasdiqlovchi gormon terapiyasi va transgenderlarda jinsiy gormonga bog'liq o'smalar xavfi-Tizimli ko'rib chiqish". Klinika. Endokrinol. (Oxf). 89 (6): 700–711. doi:10.1111 / sen.13835. PMID 30107028.
^ Gonsalves AM, Sahifa P, Domigo V, Meder JF, Oppenxaym S (sentyabr 2010). "Kiproteron bilan davolash to'xtatilgandan so'ng meningioma keskin regressiyasi". AJNR Am J Neuroradiol. 31 (8): 1504–5. doi:10.3174 / ajnr.A1978. PMID 20053802.
^ Ritsar, Ema J.; McDonald, Matthew J. (2013). "Ekzogen gormondan foydalanish paytida erkakdan ayolga transgender bo'lgan odamlarda menenjiyomning takrorlanishi va rivojlanishi". Xalqaro transgenderizm jurnali. 14 (1): 18–23. doi:10.1080/15532739.2012.725563. ISSN 1553-2739.
^ Razavi, Hamid Borxey (2014). "Meningioma: estrogen-progesteron terapiyasidan keyin transeksual bemorda g'ayritabiiy o'sish". SOJ Nevrologiyasi. 1 (2). doi:10.15226/2374-6858/1/2/00109. ISSN 2374-6858.
^ ^a ^b ^v ^d ^e ^f ^g ^h ^men ^j ^k ^l ^m ⁿ Bernat AL, Oyama K, Hamdi S, Mandonnet E, Vexiau D, Pocard M, Jorj B, Froelich S (oktyabr 2015). "Siproteron asetat to'xtatilgandan keyin meningiomalarning o'sishini barqarorlashtirish va regressiyasi: 12 ta bemordan iborat seriya". Acta Neurochir (Wien). 157 (10): 1741–6. doi:10.1007 / s00701-015-2532-3. PMID 26264069.
^ ^a ^b ^v Botella C, Coll G, Lemaire JJ, Irthum B (oktyabr 2015). "Méningiomes intracrâniens et utilization prolongée d'acétate de cyprotérone à doz Conventionnelle chez la femme: à suggestions de deux cas de régression tumorale après arrêt du traitement" [Boshsuyagi ichi menenjiyomalari va kiproteron asetat ayollarda an'anaviy ravishda dozada. Davolanish bekor qilingandan so'ng o'smaning kamayishi holatlari to'g'risida hisobot]. Neyroxirurgiya (frantsuz tilida). 61 (5): 339–42. doi:10.1016 / j.neuchi.2015.05.002. PMID 26249273.
^ Sys C, Kestelyn P (2015). "Siproteron asetat bilan davolangan bemorda meningioma sabab bo'lgan bir tomonlama proptoz va ko'rlik". GMS oftalmol kasalliklari. 5: Doc05. doi:10.3205 / oc000027. PMC 5015623. PMID 27625949.
^ ^a ^b Kalamarides M, Peyre M (may 2017). "Progestin bilan davolashni to'xtatgandan so'ng katta menenjiyomalarning qon tomirlari kamayishi bilan dramatik qisqarish". Jahon neyroxirurgiyasi. 101: 814.e7–814.e10. doi:10.1016 / j.wneu.2017.03.013. PMID 28300711.
^ Keilani C, Abada S (2017 yil may). "Kiproteron asetat bilan davolashda tezkor induktsiya qilingan ikki tomonlama kompressiv optik neyropatiya bilan simptomatik ko'p meningiomalarning kam uchraydigan holati". Curr Drug Saf. doi:10.2174/1574886312666170523154548. PMID 28545357.
^ Bernat AL, Bonnin S, Labidi M, Aldahak N, Bresson D, Bouazza S, Froelich S (2018). "Gigant hidli truba menenjiyomining regressiyasi va siproteron asetat to'xtatilgandan so'ng ko'rish keskinligini to'liq tiklash". J Oftalmik Vis Res. 13 (3): 355–358. doi:10.4103 / jovr.jovr_21_17. PMC 6058554. PMID 30090195.
^ Bur, Mirra; Moernaut, Loes; Van Kalenberg, Frank; Lapau, Bruno; T'Sjoen, Yigit (2018). "Transjin ayolda siproteron asetatga javoban meningioma o'zgarishi". Xalqaro transgenderizm jurnali. 19 (1): 92–94. doi:10.1080/15532739.2017.1413615. ISSN 1553-2739.
^ Nizar, Xisham; Seal, Leyton (2018). "Menenjiyomning g'ayritabiiy sababi". Endokrin tezislar. doi:10.1530 / endoabs.59.EP75. ISSN 1479-6848.
^ Kassir, P; Bruno, M; Corvilain, B (2019). "Siproteron asetat ishlatilgandan keyin meningioma kasalligi". Endokrin tezislar. doi:10.1530 / endoabs.64.024. ISSN 1479-6848.
^ Alalade, Endryu; Milward, Kristofer; Pal, Piyali; Gilkes, Ketrin (2019), Transgender bemorda bir nechta bosh suyagi bazasi menenjiyomasi: Case Report and Literature Review, 80, doi:10.1055 / s-0039-1679816, ISSN 2193-634X
^ Shampan PO, Passeri T, Froelich S (mart 2019). "Kiproteron asetat va nomegestrol asetatning meningioma kasalligiga gormonal ta'siri: voqea haqida hisobot". Acta Neurochir (Wien). 161 (3): 589–592. doi:10.1007 / s00701-018-03782-4. PMID 30666456.
^ Ouens, Liza; Xeldeydi, Jeyn; Kerr, Richard; Franks, Stiven (2019). "Kiproteron asetatni uzoq muddat qo'llash bilan bog'liq meningioma kasalligi". Endokrin tezislar. doi:10.1530 / endoabs.62.P36. ISSN 1479-6848.
^ Kolstrup, Xans; Larsen, Ellen D.; Mollerup, Stin; Tarp, Xanna; Soelberg, Yoqub; Rosthøj, Susanne (2020). "GnRH agonisti va siproteron asetat kombinatsiyasi bilan farmakologik ravishda kastrlangan 60 ta qamoqda o'tirgan erkak jinsiy jinoyatchilarni uzoq muddatli kuzatuvi". Sud-psixiatriya va psixologiya jurnali: 1–14. doi:10.1080/14789949.2020.1711957. ISSN 1478-9949.
^ Froelich S, Dali-Youcef N, Boyer P, Kehrli P, Maitrot D, Auwerx J, Schlienger JL (2008). "Siproteron asetat ko'plab meningiomalarga yordam beradimi?". Endokrin tezislar. 16: P158. ISSN 1470-3947.
^ Peyre M, Gaillard S, de Marcellus C, Giry M, Bielle F, Villa C, Boch AL, Loiseau H, Baussart B, Cazabat L, Raffin-Sanson ML, Sanson M, Kalamarides M (mart 2018). "Meningioma mutatsion landshaftining progestin bilan bog'liq siljishi". Ann. Onkol. 29 (3): 681–686. doi:10.1093 / annonc / mdx763. PMID 29206892.
^ Portet, Sylvain; Noufal, Raniya; Tachon, Gall; Simonneau, Adrien; Chalant, Anays; Naar, Amir; Milin, Serj; Bataille, Benua; Karayan-Tapon, Lyusi (2019). "Yuqori dozali siproteron asetat ta'sirida bemorlarda ishlab chiqarilgan intrakranial menenjiyomning histo-molekulyar xarakteristikasi, antandrogen bilan davolash". Neyro-onkologiya yutuqlari. doi:10.1093 / noajnl / vdz003. ISSN 2632-2498.
^ Vasilakis-Skaramozza S, Jik H (2001 yil oktyabr). "Kiproteron yoki levonorgestrel kontratseptivlari bilan venoz tromboembolizm xavfi". Lanset. 358 (9291): 1427–9. doi:10.1016 / S0140-6736 (01) 06522-9. PMID 11705493.
^ ^a ^b Spitzer WO (2003 yil dekabr). "Venoz tromboembolizmi uchun xavfli omil sifatida etinilestradiol bilan siproteron asetat: epidemiologik baholash". J Obstet Gynekol mumkin. 25 (12): 1011–8. doi:10.1016 / S1701-2163 (16) 30342-5. PMID 14663535.
^ Lidegaard Ø, Nilsen LH, Skovlund CW, Skjeldestad FE, Løkkegaard E (oktyabr 2011). "Turli gestagen va estrogen dozalarini o'z ichiga olgan og'zaki kontratseptivlarni qo'llash bilan venoz tromboembolizm xavfi: Daniya kohort tadqiqotlari, 2001-9". BMJ. 343: d6423. doi:10.1136 / bmj.d6423. PMC 3202015. PMID 22027398.
^ ^a ^b Kromm J, Jeerakatil T (iyun 2014). "Qon tomirlari bo'lgan 23 yoshli ayolda siproteron asetat-etinil estradioldan foydalanish". CMAJ. 186 (9): 690–3. doi:10.1503 / cmaj.130579. PMC 4049993. PMID 24491473.
^ ^a ^b ^v Kuhl H (2005). "Estrogenlar va progestogenlarning farmakologiyasi: turli xil qabul qilish yo'llarining ta'siri" (PDF). Klimakterik. 8 Qo'shimcha 1: 3-63. doi:10.1080/13697130500148875. PMID 16112947.
^ Wiegratz I, Kuhl H (sentyabr 2006). "Progestogenlarning metabolik va klinik ta'siri". Eur J Contracept Reprod sog'liqni saqlash. 11 (3): 153–61. doi:10.1080/13625180600772741. PMID 17056444.
^ ^a ^b ^v ^d ^e ^f ^g ^h ^men ^j Asscheman H, T'Sjoen G, Lemaire A, Mas M, Meriggiola MC, Myuller A, Kuhn A, Dhejne C, Morel-Journel N, Gooren LJ (sentyabr 2014). "Vena tromboemboliyasi transseksual sub'ektlarni erkak va ayol o'rtasidagi jinsiy gormonlar bilan davolashning murakkabligi sifatida". Andrologiya. 46 (7): 791–5. doi:10.1111 / va.12150. PMID 23944849.
^ ^a ^b ^v Beyer-Vestendorf J, Vert S, Halbritter K, Vayss N (aprel 2010). "Erkaklarda saraton va venoz tromboembolizm xavfi". Tromb. Res. 125 Qo'shimcha 2: S155-9. doi:10.1016 / S0049-3848 (10) 70035-9. PMID 20433997.
^ ^a ^b Guay DR (dekabr 2008). "Kognitiv jihatdan zaiflashgan keksa odamlarda noo'rin jinsiy xatti-harakatlar". Am J Geriatr farmatsevti. 6 (5): 269–88. doi:10.1016 / j.amjopharm.2008.12.004. PMID 19161930.
^ ^a ^b ^v ^d Seaman HE, Langley SE, Farmer RD, de Vries CS (iyun 2007). "Prostata bezi saratoniga chalingan erkaklarda venoz tromboembolizm va siproteron asetat: Umumiy amaliyot tadqiqotlari bazasidan foydalangan holda o'rganish". BJU Int. 99 (6): 1398–403. doi:10.1111 / j.1464-410X.2007.06859.x. PMID 17537215.
^ Van Hemelrijck M, Adolfsson J, Garmo H, Bill-Akselson A, Bratt O, Ingelsson E, Lambe M, Stattin P, Xolmberg L (may, 2010). "Prostata bezi saratoniga chalingan erkaklarda tromboembolik kasalliklar xavfi: Shvetsiyaning PCBaSe populyatsiyasiga asoslangan natijalar". Lanset Onkol. 11 (5): 450–8. doi:10.1016 / S1470-2045 (10) 70038-3. PMC 2861771. PMID 20395174.
^ Namer M (oktyabr 1988). "Antiandrogenlarning klinik qo'llanilishi". J. Steroid biokimyosi. 31 (4B): 719-29. doi:10.1016/0022-4731(88)90023-4. PMID 2462132.
^ Jakobi, GR; Tunn, UW; Senge, TH (1982 yil 1-dekabr). "Ishlatilmaydigan prostata saratoni palliatsiyasi uchun siproteron asetat bilan klinik tajriba". Jakobida Gyunter H; Hohenfellner, Rudolf (tahrir). Prostata saratoni. Uilyams va Uilkins. 305-319 betlar. ISBN 978-0-683-04354-9.
^ ^a ^b ^v Shreder, Fritz X.; Radlmayer, Albert (2009). "Steroidal antiandrogenlar". V. Kreyg Iordaniyada; Barrington J. A. Furr (tahr.). Ko'krak va prostata saratonida gormonlarni davolash. Humana Press. 325-346 betlar. doi:10.1007/978-1-59259-152-7_15. ISBN 978-1-60761-471-5.
^ Schröder FH (1998). "Antiandrogenlar prostata saratoni uchun monoterapiya sifatida". Evropa urologiyasi. 34 Qo'shimcha 3: 12-7. doi:10.1159/000052291. PMID 9854190.
^ Beyer-Vestendorf J, Bauersachs R, Xach-Vunderl V, Zotz RB, Rott H (oktyabr 2018). "Jinsiy gormonlar va venoz tromboembolizm - kontratseptsiyadan gormonlarni almashtirish terapiyasiga qadar". VASA. 47 (6): 441–450. doi:10.1024 / 0301-1526 / a000726. PMID 30008249.
^ ^a ^b ^v DeLoughery TG (iyun 2011). "Estrogen va tromboz: tortishuvlar va sog'lom fikr". Rev Endocr Metab buzilishi. 12 (2): 77–84. doi:10.1007 / s11154-011-9178-0. PMID 21559819.
^ Van Xilkama Vlieg, A .; Middeldorp, S. (2011). "Gormonlarni davolash va venoz tromboembolizm: biz hozir qayerdamiz?". Tromboz va gemostaz jurnali. 9 (2): 257–266. doi:10.1111 / j.1538-7836.2010.04148.x. ISSN 1538-7933. PMID 21114755.
^ Benagiano, G.; Primiero, F.M. (1983). "Uzoq muddatli kontratseptivlarning hozirgi holati". Giyohvand moddalar. 25 (6): 570–609. doi:10.2165/00003495-198325060-00003. ISSN 0012-6667. PMID 6223801.
^ Manta, S .; Karp, R .; Raghavan, V .; Terrin, N .; Bauer, K. A .; Tsviker, J. I. (2012). "Faqatgina progestinli kontratseptsiya qabul qiladigan ayollarda venoz tromboembolik hodisalar xavfini baholash: meta-tahlil". BMJ. 345 (aug07 2): e4944. doi:10.1136 / bmj.e4944. ISSN 1756-1833. PMC 3413580. PMID 22872710.
^ ^a ^b Deyvi DA (mart 2018). "Menopozli gormon terapiyasi: yaxshiroq va xavfsiz kelajak". Klimakterik. 21 (5): 454–461. doi:10.1080/13697137.2018.1439915. PMID 29526116.
^ ^a ^b Stanczyk FZ, Bhavnani BR (2014 yil iyul). "Postmenopozal ayollarda gormonlarni davolash uchun medroksiprogesteron asetatdan foydalanish: bu xavfsizmi?". J. Steroid biokimyosi. Mol. Biol. 142: 30–8. doi:10.1016 / j.jsbmb.2013.11.011. PMID 24291402.
^ ^a ^b Stanczyk FZ, Hapgood JP, Winer S, Mishell DR (2013 yil aprel). "Postmenopozal gormon terapiyasida ishlatiladigan progestogenlar: ularning farmakologik xususiyatlari, hujayra ichidagi harakatlari va klinik ta'siridagi farqlar". Endokr. Vah. 34 (2): 171–208. doi:10.1210 / er.2012-1008. PMC 3610676. PMID 23238854.
^ ^a ^b Jiang Y, Tian V (noyabr 2017). "Progesteronlarning gormonlarni almashtirish terapiyasida qon lipidlariga ta'siri". Lipidlar sog'lig'i uchun disk. 16 (1): 219. doi:10.1186 / s12944-017-0612-5. PMC 5697110. PMID 29157280.
^ ^a ^b ^v Singx, Shankar; Gautier, Silvain; Labrie, Fernand (2000). "Androgen retseptorlari antagonistlari (antiandrogenlar) tuzilishi-faoliyati munosabatlari". Hozirgi dorivor kimyo. 7 (2): 211–247. doi:10.2174/0929867003375371. ISSN 0929-8673. PMID 10637363. Flutamid bilan taqqoslaganda [siproteron asetat] muhim ichki androgen va estrogen ta'siriga ega. [...] Flutamid va steroidal hosilalar, siproteron asetat, xlormadinon asetat, megestrol asetat va medroksiprogesteron asetatning ta'siri in vivo jonli sichqonlarda, androgenga sezgir bo'lgan ayol sichqonlarida solishtirildi. Barcha steroidal birikmalar o'smaning o'sishini rag'batlantirgan, flutamid esa stimulyator ta'siriga ega bo'lmagan [51]. Shunday qilib, CPA o'zining ichki xususiyatlari tufayli androgenga sezgir parametrlarni va saraton o'sishini rag'batlantiradi. Kastratsiyaga qo'shilgan siproteron asetat hech qachon nazorat qilinadigan biron bir tadqiqotda prostata saratoni kasalliksiz hayotini yoki umuman omon qolish muddatini uzaytirishi hech qachon ko'rsatilmagan [152-155].
^ ^a ^b Newling DW (1997 yil mart). "Yaqinda Evropada o'tkazilgan klinik tadqiqotlar natijalariga ishora qilingan prostata saratoni palyatif terapiyasi". Br J Urol. 79 Qo'shimcha 1: 72-81. doi:10.1111 / j.1464-410X.1997.tb00805.x. PMID 9088277.
^ ^a ^b Mahler C, Verhelst J, Denis L (1998 yil may). "Antiandrogenlarning klinik farmakokinetikasi va ularning prostata saratoni samaradorligi". Farmakokinet klinikasi. 34 (5): 405–17. doi:10.2165/00003088-199834050-00005. PMID 9592622.
^ ^a ^b Anderson J (2003 yil mart). "Prostata bezi saratonini davolashda antiandrogen monoterapiyasining ahamiyati". BJU Int. 91 (5): 455–61. doi:10.1046 / j.1464-410X.2003.04026.x. PMID 12603397.
^ ^a ^b ^v Aronson JK (2009 yil 21 fevral). Meylerning endokrin va metabolik dorilarning yon ta'siri. Elsevier. 150-152 betlar. ISBN 978-0-08-093292-7.
^ Myuller E (2003 yil 18 sentyabr). Onkologik va neyroendokrinning peptidlari va peptidlari bo'lmaganligi: asosiydan klinik tadqiqotgacha. Springer Science & Business Media. 171– betlar. ISBN 978-88-470-0295-1. Arxivlandi asl nusxasidan 2017 yil 8 sentyabrda. [CPA] koagulyatsion tizimga tegishli ta'sirlarni keltirib chiqaradi. Umumiy androgenik blokada bilan bog'liq bo'lgan so'nggi meta-tahlil shuni ko'rsatdiki, kiproteron asetat kastratsiya bilan birlashganda androgen-supressiv davolashning uzoq muddatli samaradorligini pasaytiradi. Aslida, bu asosan yurak-qon tomir asoratlari tufayli davolanish bilan bog'liq o'limning ko'payishiga olib keladi (Mualliflar yo'q, 2000).
^ ^a ^b Furr BJ, Taker H (1996 yil yanvar). "Bikalutamidning klinikadan oldingi rivojlanishi: farmakodinamikasi va ta'sir mexanizmi". Urologiya. 47 (1A Suppl): 13-25, muhokama 29-32. doi:10.1016 / S0090-4295 (96) 80003-3. PMID 8560673.
^ Mahler C, Verhelst J, Denis L (1998 yil may). "Antiandrogenlarning klinik farmakokinetikasi va ularning prostata saratoni samaradorligi". Klinik farmakokinetikasi. 34 (5): 405–17. doi:10.2165/00003088-199834050-00005. PMID 9592622.
^ Chang C (2005 yil 22 mart). Prostata saratoni: asosiy mexanizmlar va terapevtik usullar. Jahon ilmiy. 10-11 betlar. ISBN 978-981-4481-61-8. Arxivlandi asl nusxasidan 2017 yil 8 sentyabrda.
^ Gillatt D (2006 yil avgust). "Prostata saratonining mahalliy darajada rivojlangan antiandrogenli davolash usullari: barchasi bir xilmi?". J. Saraton kasalligi Klinika. Onkol. 132 Qo'shimcha 1: S17-26. doi:10.1007 / s00432-006-0133-5. PMID 16845534.
^ Sturdee DW (2013 yil avgust). "Progestinlar birlashgan HRT rejimining bir qismi sifatida haqiqatan ham zarurmi?". Klimakterik. 16 Qo'shimcha 1: 79-84. doi:10.3109/13697137.2013.803311. PMID 23651281.
^ de Blok CJ, Wiepjes CM, Nota NM, van Engelen K, Adank MA, Dreijerink KM, Barbé E, Konings IR, den Heijer M (may, 2019). "Gormonlar bilan davolanayotgan transgenderlarda ko'krak bezi saratoni xavfi: Gollandiyada butun mamlakat bo'ylab kohort tadqiqotlari". BMJ. 365: l1652. doi:10.1136 / bmj.l1652. PMC 6515308. PMID 31088823.
^ de Blok CJ, Dreijerink KM, den Heijer M (iyun 2019). "Transgender odamlarda saraton xavfi". Endokrinol. Metab. Klinika. Shimoliy Am. 48 (2): 441–452. doi:10.1016 / j.ecl.2019.02.005. PMID 31027551.
^ Feingold KR, Anawalt B, Boyce A, Chrousos G, Dungan K, Grossman A, Xershman JM, Kaltsas G, Koch C, Kopp P, Korbonits M, McLachlan R, Morley JE, New M, Perreault L, Purnell J, Rebar R , Singer F, Trence DL, Vinik A, Wilson DP, Nota NM, den Heijer M, Gooren LJ (2000). "Gender-disforik / jinsga mos kelmaydigan kattalarni baholash va davolash". PMID 31343858. Iqtibos jurnali talab qiladi | jurnal = (Yordam bering)
^ Ivamoto SJ, Defreyne J, Rothman MS, Van Schuylenbergh J, Van de Bruaene L, Motmans J, T'Sjoen G (2019). "Transgender ayollar uchun sog'liqqa oid masalalar va noma'lum bo'lganlar: hikoyalarni ko'rib chiqish". Ther Adv Endokrinol Metab. 10: 2042018819871166. doi:10.1177/2042018819871166. PMC 6719479. PMID 31516689.
^ ^a ^b Endrikat J, Gerlinger S, Richard S, Rozenbaum P, Dysterberg B (dekabr 2011). "Progestinlarning ovulyatsiyani inhibe qilish dozalari: mavjud adabiyotlarni va dunyo bo'ylab sotiladigan preparatlarni muntazam ravishda ko'rib chiqish". Kontratseptsiya. 84 (6): 549–57. doi:10.1016 / j.contraception.2011.04.009. PMID 22078182.
^ Neumann F, Kalmus J (1991). "Jinsiy kasalliklarni davolashda siproteron asetat: farmakologik asos va klinik tajriba". Muddati Klinika. Endokrinol. 98 (2): 71–80. doi:10.1055 / s-0029-1211103. PMID 1838080.
^ Ahmadi H, Daneshmand S (2014). "Prostata saratoni uchun androgenlarni yo'q qilish terapiyasi: uzoq muddatli xavfsizlik va bemorning natijalari". Bemorlarning munosabatlari natijalari. 5: 63–70. doi:10.2147 / PROM.S52788. PMC 4094624. PMID 25045284.
^ Rassell N, Cheung A, Grossmann M (avgust 2017). "Androgenlarni yo'q qilish terapiyasining salbiy ta'sirini kamaytirish uchun estradiol". Endokr. Relat. Saraton. 24 (8): R297-R313. doi:10.1530 / ERC-17-0153. PMID 28667081.
^ Dalesio O, van Tinteren H, Klark M, Peto R, Shreder F, Dechering I, Evans V, Godvin J, Blumenstayn B, Krouford E, Denis L, Xol R, X tepalik, Iversen P, Shipli V, Solouey M, Silvestr R (2000). "Rivojlangan prostata saratonida maksimal androgen blokadasi: randomizatsiyalangan sinovlarga umumiy nuqtai". Lanset. 355 (9214): 1491–1498. doi:10.1016 / S0140-6736 (00) 02163-2. ISSN 0140-6736.
^ Chodak G, Gomella L, Phung de H (sentyabr 2007). "Prostatitning rivojlangan saraton kasalligida estrodiol blokadasi: oldinga qarab orqaga qarab". Genitourin saratoni klinikasi. 5 (6): 371–8. doi:10.3816 / CGC.2007.n.019. PMID 17956709.
^ ^a ^b ^v ^d DeLeve, Laurie D. (2013). "Saraton kasalligining kimyoviy terapiyasi". Giyohvand moddalarni iste'mol qiladigan jigar kasalligi. 541-567 betlar. doi:10.1016 / B978-0-12-387817-5.00030-3. ISBN 9780123878175.
^ ^a ^b ^v ^d ^e ^f Kim JH, Yoo BW, Yang VJ (may 2014). "Siproteron asetat tomonidan qo'zg'atilgan jigar etishmovchiligi: holatlar bo'yicha hisobot va adabiyotlarni o'rganish". Urol Assoc J. 8 (5-6): E458-61. doi:10.5489 / cuaj.1753. PMC 4081269. PMID 25024808.
^ ^a ^b ^v ^d ^e ^f ^g Savidou I, Deutsch M, Soultati AS, Koudouras D, Kafiri G, Dourakis SP (dekabr 2006). "Siproteron asetat tomonidan qo'zg'atilgan gepatotoksiklik: uchta holat haqida hisobot". Jahon Gastroenterologiya jurnali. 12 (46): 7551–5. doi:10.3748 / wjg.v12.i46.7551. PMC 4087608. PMID 17167851.
^ Hinkel A, Berges RR, Pannek J, Schulze H, Senge T (1996). "Prostata bezining rivojlangan saraton kasalligini davolashda siproteron asetat: 89 bemorni uzoq muddatli kuzatuvida jigar zaharliligini retrospektiv tahlil qilish". Yevro. Urol. 30 (4): 464–70. doi:10.1159/000474216. PMID 8977068.
^ ^a ^b ^v ^d Rabe T, Feldmann K, Heinemann L, Runnebaum B (yanvar 1996). "Kiproteron asetat: bu gepato- yoki genotoksikmi?". Dori xavfsizligi. 14 (1): 25–38. doi:10.2165/00002018-199614010-00004. PMID 8713486. Yaqinda Dori-darmonlarni nazorat qilish agentligi (MCA) / Dori vositalari xavfsizligi qo'mitasi (CSM) ning nashrida [5] EBMni uzoq muddat qo'llaganidan keyin jigar zaharli va dozalari bilan bog'liq spontan xabarlarga e'tibor qaratildi. [...] 96 gepatotoksik hodisa kuzatilgan (33 kishi o'limga olib kelgan), shulardan 91 tasi erkaklarda, 5 tasi ayollarda. Jigar reaktsiyalari gepatit, xolestatik sariqlik va jigar etishmovchiligini o'z ichiga olgan. Bemorlarning aksariyati prostata saratoni uchun yuqori dozada CPA (300 mg / kun) bilan davolangan.
^ ^a ^b ^v ^d "Siproteron asetat bilan jigar reaktsiyalari (Kiprostat, Androkur)". Farmakologik nazoratning dolzarb muammolari (21): 1. 1995 yil fevral.
^ ^a ^b Gava, Giuliya; Serakchioli, Renato; Meriggiola, Mariya Kristina (2017). "Jinsiy disforik Natal erkaklarda antiandrogenlar bilan davolash". Moyaklar endokrinologiyasi va erkaklarning ko'payishi. Endokrinologiya. 1199–1209 betlar. doi:10.1007/978-3-319-44441-3_42. ISBN 978-3-319-44440-6. ISSN 2510-1927.
^ ^a ^b ^v ^d ^e ^f ^g ^h ^men ^j ^k ^l ^m ⁿ ^o ^p ^q ^r ^s ^t ^siz ^v ^w ^x Bessone F, Lucena MI, Roma MG, Stefens C, Medina-Kaliz I, Frider B, Tsariktsian G, Ernandes N, Brugera M, Gualano G, Fassio E, Montero J, Reggiardo MV, Ferretti S, Kolombato L, Tanno F, Ferrer J, Zeno L, Tanno H, Andrade RJ (fevral 2016). "Kiproteron asetat jigarning keng spektrli shikastlanishini, shu jumladan kortikosteroidlarga ta'sir qiluvchi gepatitni keltirib chiqaradi: 22 ta holat to'g'risida hisobot". Jigar Int. 36 (2): 302–10. doi:10.1111 / liv.12899. PMID 26104271.
^ Marius Dyuker (2016 yil 23-may). Mehnatga layoqatsizlik: tendentsiyalar va yangi istiqbollar. Yo'nalish. 139– betlar. ISBN 978-1-317-11767-4.
^ Berlex Canada, Inc. (2003-02-10). "Cyproterone acetate tabletkalari va in'ektsiyalari uchun mahsulot monografiyalari (qayta ishlangan versiyasi)" (PDF). Arxivlandi asl nusxasi (PDF) 2006-09-24 kunlari.
^ Giyohvand moddalarga salbiy ta'sir ko'rsatishi bo'yicha maslahat qo'mitasi (2004 yil fevral). "Avstraliyadagi nojo'ya reaktsiyalar byulleteni, 23-jild, 1-son".
^ ^a ^b Lin AD, Chen KK, Lin AT, Chang YH, Vu HH, Kuo JY, Huang WJ, Hsu YS, Chung HJ, Chang LS (dekabr 2003). "Prostatitning rivojlangan saratonini davolashda antiandrogen bilan bog'liq gepatotoksiklik". J Chin Med dos. 66 (12): 735–40. PMID 15015823.
^ ^a ^b Thole Z, Manso G, Salgueiro E, Revuelta P, Hidalgo A (2004). "Antiandrogenlar tomonidan qo'zg'atilgan gepatotoksiklik: adabiyotlarni ko'rib chiqish". Urol. Int. 73 (4): 289–95. doi:10.1159/000081585. PMID 15604569.
^ Chitturi, Shivakumar; Farrel, Geoffrey C (2013). "Gormonlar va gormon antagonistlarining jigarga salbiy ta'siri". Giyohvand moddalarni iste'mol qiladigan jigar kasalligi. 605-619 betlar. doi:10.1016 / B978-0-12-387817-5.00033-9. ISBN 9780123878175.
^ ^a ^b Mikel M, Soler A, Vaqué A, Ojanguren I, Kosta J, Planas R (oktyabr 2007). "Flutamid va siproteron asetatning o'zaro gepatotoksikligiga shubha qilingan". Jigar Int. 27 (8): 1144–7. doi:10.1111 / j.1478-3231.2007.01549.x. PMID 17845544.
^ ^a ^b Manolakopulos S, Bethanis S, Armonis A, Ekonomou M, Avgerinos A, Tsurmakliotis D (2004 yil mart). "Flutamid va siproteron asetat ketma-ket kiritilgandan so'ng toksik gepatit". Qazish. Dis. Ilmiy ish. 49 (3): 462–5. doi:10.1023 / B: DDAS.0000020504.41500.9c. PMID 15139499.
^ ^a ^b Meijers WH, Willemse PH, Sleijfer DT, Mulder NH, Grond J (sentyabr 1986). "Siproteron asetat bilan gepatosellular zararlanish". Eur J onkologiya klinikasi. 22 (9): 1121–2. doi:10.1016/0277-5379(86)90017-9. PMID 2946585.
^ Lévesque H, Trivalle C, Manchon ND, Vinel JP, Mur N, Hémet J, Kurtua H, Bercoff E, Bourreille J (yanvar 1989). "Tsiproteron asetat tufayli fulminant gepatit". Lanset. 1 (8631): 215–6. doi:10.1016 / S0140-6736 (89) 91225-7. PMID 2563116.
^ ^a ^b ^v Bleyk JC, Sawyerr AM, Dooley JS, Scheuer PJ, McIntyre N (may 1990). "Kiproteron asetat keltirib chiqaradigan og'ir gepatit". Ichak. 31 (5): 556–7. doi:10.1136 / gut.31.5.556. PMC 1378574. PMID 2140997. Bir nechta holatlar bo'yicha hisobotlar chop etilgan bo'lsa-da, Dori vositalari xavfsizligi qo'mitasi Buyuk Britaniyada 1988 yil noyabrgacha siproteron asetat bilan bog'liq bo'lgan jigarning salbiy reaktsiyalari to'g'risida 19 ta hisobot oldi (shaxsiy aloqa, Dori vositalari xavfsizligi qo'mitasi). Ushbu holatlarning beshtasi o'limga olib keldi.
^ Dore B, Orget J, Eroniy J, Aubert J (1990). "Hépatite après traitement par acétate de cyprotérone. A Pro d'un cas" [Siproteron asetat bilan davolashdan keyin gepatit. Ishning aproposlari]. J Urol (Parij) (frantsuz tilida). 96 (3): 169–71. ISSN 0248-0018. PMID 2145371.
^ Antoni M, Bourliere M, Tullec J, Maillot A, Botta-Fridlund D, Gautier A (1991). "Gepatit sub-fulminante d'evolution mortelle a l'acetate de cyproterone" [Kiproteron asetat keltirib chiqaradigan halokatli subfulminant gepatit]. Gastroenterol. Klinika. Biol. (frantsuz tilida). 15 (10): 772–3. ISSN 0399-8320. PMID 1840042.
^ Ohri SK, Gaer JA, Kin PF (1991 yil fevral). "Gepatotsellulyar karsinoma va siproteron asetat bilan davolash". Br J Urol. 67 (2): 213. doi:10.1111 / j.1464-410X.1991.tb15113.x. PMID 1848454.
^ ^a ^b ^v Parys BT, Hamid S, Tomson RG (1991 yil mart). "Siproteron asetat terapiyasidan so'ng og'ir gepatotsellular disfunktsiya". Br J Urol. 67 (3): 312–3. doi:10.1111 / j.1464-410X.1991.tb15142.x. PMID 1827039.
^ Drakos PE, Gez E, Katane R (1992). "Siproteron asetat tufayli gepatit". Yevro. J. Saraton. 28A (11): 1931–2. doi:10.1016 / 0959-8049 (92) 90041-Y. PMID 1389539.
^ Xassler P, Dyuchen R (1992). "Hépatotoxicité de l'acétate de cyprotérone" [siproteron asetatning gepatotoksikligi]. Rev Med Interne (frantsuz tilida). 13 (3): 245. doi:10.1016 / S0248-8663 (05) 81339-6. PMID 1410910.
^ Roila F, Crinò L, Carloni G, Natalini G (sentyabr 1993). "Kiproteron asetat: gepatotoksiklik va prostata saratoni davolash". Ann. Onkol. 4 (8): 701. doi:10.1093 / oxfordjournals.annonc.a058631. PMID 8241005.
^ Bressollette L, Dubois A, Carlhant D, Morand C, Mottier D, Riche C (1994). "Hépatite mortelle a l'acétate de cyprotérone" [Kiproteron asetat keltirib chiqaradigan o'limga olib keladigan gepatit]. Terapiya (frantsuz tilida). 49 (2): 153. PMID 7817350.
^ Xirsch D, Kovatz S, Bernxaym J, Shenkman L (mart 1994). "Fatal fulminant hepatitis from cyproterone acetate". Isr. J. Med. Ilmiy ish. 30 (3): 238–40. PMID 8181926.
^ Kattan J, Spatz A, Culine S, Terrier-Lacombe MJ, Elias D, Droz JP (October 1994). "Hepatocellular carcinoma during hormonotherapy for prostatic cancer". Am. J. klinikasi. Onkol. 17 (5): 390–2. doi:10.1097/00000421-199410000-00006. PMID 8092108.
^ ^a ^b ^v Watanabe S, Yamasaki S, Tanae A, Hibi I, Honna T (December 1994). "Three cases of hepatocellular carcinoma among cyproterone users. Ad hoc Committee on Androcur Users". Lanset. 344 (8936): 1567–8. doi:10.1016/S0140-6736(94)90373-5. PMID 7983963.
^ ^a ^b ^v ^d ^e Watanabe S, Cui Y, Tanae A, Tanaka T, Fujimoto M, Matsuo Y, Tachibana K, Yamasaki S (September 1997). "Follow-up study of children with precocious puberty treated with cyproterone acetate. Ad hoc Committee for CPA". J Epidemiol. 7 (3): 173–8. doi:10.2188/jea.7.173. PMID 9337516.
^ ^a ^b Pinganaud G, Chaslerie A, Bourdel Marchasson I, Decamps A, Manciet G, Emeriau JP (June 1995). "Cyproterone-induced hepatotoxicity". Ann Farmacother. 29 (6): 634. doi:10.1177/106002809502900619. PMID 7663042.
^ Rüdiger T, Beckmann J, Queisser W (February 1995). "Hepatocellular carcinoma after treatment with cyproterone acetate combined with ethinyloestradiol". Lanset. 345 (8947): 452–3. doi:10.1016/S0140-6736(95)90434-4. PMID 7853970.
^ Castellani P, Bernardini D, Renou C, Zamora C, Portal I, Gauthier A, Botta-Fridlund D (1996). "Hépatite subfulminante mortelle à l'acétate de cyprotérone. Un nouveau cas" [Fatal sub-fulminant hepatitis caused by cyproterone acetate. A new case]. Gastroenterol. Klinika. Biol. (frantsuz tilida). 20 (10): 915–6. ISSN 0399-8320. PMID 8991155.
^ Murphy BJ, Collins BJ (October 1996). "Severe hepatitis and liver failure induced by cyproterone acetate". Aust N Z J Med. 26 (5): 724. doi:10.1111/j.1445-5994.1996.tb02956.x. PMID 8958378.
^ Ruiz-Rebollo ML, Polo F, Palenzuela R, Moretó M (1997). "Hepatitis aguda severa por ciproterona" [Severe acute hepatitis due to cyproterone]. Gastroenterol gepatol (ispan tilida). 20 (7): 385. ISSN 0210-5705. PMID 9377242.
^ Lombardi A, Ferrazza P, Castaldi F, Covotta L, Tesoriere A, Urbano V, Midiri G (April 1998). "[Acute hepatic necrosis in a patient treated with cyproterone acetate]". G Chir (italyan tilida). 19 (4): 161–3. PMID 9628065.
^ ^a ^b ^v Friedman G, Lamoureux E, Sherker AH (July 1999). "Fatal fulminant hepatic failure due to cyproterone acetate". Qazish. Dis. Ilmiy ish. 44 (7): 1362–3. doi:10.1023/A:1026639432428. PMID 10489919.
^ Garty BZ, Dinari G, Gellvan A, Kauli R (May 1999). "Cirrhosis in a child with hypothalamic syndrome and central precocious puberty treated with cyproterone acetate". Yevro. J. Pediatr. 158 (5): 367–70. doi:10.1007/s004310051093. PMID 10333116.
^ Manfredi S, Lenfant L, Gresset AC, Bonnotte B, Lorcerie B, Chauffert B (November 2000). "Carcinome hépatocellulaire sur foie sain potentiellement imputable à la prise au long cours d'acétate de cyprotérone" [Hepatocellular carcinoma in a healthy liver possibly due to long-term use of cyproterone acetate]. Med-ni bosing (frantsuz tilida). 29 (36): 1983. ISSN 0755-4982. PMID 11149080.
^ Giordano N, Nardi P, Santacroce C, Geraci S, Gennari C (September 2001). "Acute hepatitis induced by cyproterone acetate". Ann Farmacother. 35 (9): 1053–5. doi:10.1177/106002800103500902. PMID 11573856.
^ Kacar S, Akdogan M, Koşar Y, Parlak E, Sasmaz N, Oguz P, Aydog G (July 2002). "Estrogen and cyproterone acetate combination-induced autoimmune hepatitis". J. klinikasi. Gastroenterol. 35 (1): 98–100. doi:10.1097/00004836-200207000-00023. PMID 12080237.
^ Famularo G, Minisola G, Grieco A, Miele L (September 2005). "Fulminant liver failure caused by cyproterone". Dig Dis Dis. 37 (9): 718–9. doi:10.1016/j.dld.2005.04.018. PMID 15936995.
^ ^a ^b ^v ^d Savidou I, Deutsch M, Soultati AS, Koudouras D, Kafiri G, Dourakis SP (December 2006). "Hepatotoxicity induced by cyproterone acetate: a report of three cases". Dunyo J. Gastroenterol. 12 (46): 7551–5. doi:10.3748/wjg.v12.i46.7551. PMC 4087608. PMID 17167851.
^ ^a ^b He JC, Xu P, Peng LB (December 2009). "[A case of Budd-Chiari syndrome induced by ethinylestradiol and cyproterone acetate]". Zhonghua Gan Zang Bing Za Zhi (xitoy tilida). 17 (12): 954. doi:10.3760/cma.j.issn.1007-3418.2009.12.020. ISSN 1007-3418. PMID 20038345.
^ "Ethinylestradiol/cyproterone. Budd-Chiari syndrome: case report". Reaksiyalar haftalik (1340): 20. February 2011. doi:10.2165/00128415-201113400-00066. ISSN 0114-9954.
^ Kim BH, Kim DJ, Sohn KM, Yang HN, Choi MJ, Lee CW, Choi KC (2009). "잠복간경변 환자에서 cyproterone acetate에 의해 발생한 전격간부전 1예" [A case of fulminant hepatic failure due to cyproterone acetate in a patient with cryptogenic liver cirrhosis]. Korean J Med. 77 (Suppl 1): S31-5. ISSN 1738-9364.
^ Hsu YC, Tai DI (2011). "Unusually high alanine aminotransferase to aspartate aminotransferase ratio in a patient with cyproterone-induced icteric hepatitis". Chang Gung Med J. 34 (6 Suppl): 34–8. PMID 22490456.
^ Abenavoli L, Milic N, Beaugrand M (2013). "Severe hepatitis induced by cyproterone acetate: role of corticosteroids. A case report". Ann Hepatol. 12 (1): 152–5. PMID 23293208.
^ Vodička M, Sálek T, Röderová E, Cerný D (2013). "Hepatotoxicita po cyproteron acetátu v léčbě karcinomu prostaty – kazuistika" [Hepatotoxicity induced by cyproterone acetate in the prostate carcinoma treatment - a case report]. Klin Onkol (chex tilida). 26 (1): 47–8. PMID 23528173.
^ Nour E, Mehdi K, Hanene J, Hammami A, Ben Slama A, Ali J (December 2017). "Fatal acute liver failure induced by cyproterone acetate: A new case". Med-ni bosing. 46 (12 Pt 1): 1231–1232. doi:10.1016/j.lpm.2017.09.003. PMID 29129412.
^ "High dose cyproterone and hepatotoxicity". Australian Adverse Drug Reactions Bulletin. 23 (1): 3. 2004. ISSN 1325-8540. High dose cyproterone (50mg, 100mg; Androcur, Androcur-100) is used predominantly for advanced prostate carcinoma. For the year ending June 2003, 59,000 prescriptions were dispensed for the 50mg or 100mg tablets and 97% of patients prescribed these tablets were male. [...] Over the years, ADRAC has received 105 reports implicating high-dose cyproterone. The most common adverse reactions are related to the liver with 32 reports. Other more commonly reported reactions include fatigue, dyspnoea, asthenia, confusion, depression and deep vein thrombosis. [...] All except one of the hepatic reactions involved male patients being treated for prostate cancer, whose ages ranged from 56 to 92 (median: 77) years. Time to onset of liver dysfunction ranged from 4 days to 4 years (median: 4-5 months); only 4 cases had a time to onset under a month.
^ Manso G, Thole Z, Salgueiro E, Revuelta P, Hidalgo A (April 2006). "Spontaneous reporting of hepatotoxicity associated with antiandrogens: data from the Spanish pharmacovigilance system". Farmakoepidemiol dori vositasi. 15 (4): 253–9. doi:10.1002/pds.1168. PMID 16294367.
^ "Oral contraceptives and liver cancer. Results of the Multicentre International Liver Tumor Study (MILTS)". Kontratseptsiya. 56 (5): 275–84. 1997 yil noyabr. PMID 9437555.
^ Seaman HE, de Vries CS, Farmer RD (2003). "The risk of liver disorders in women prescribed cyproterone acetate in combination with ethinyloestradiol (Dianette): a nested case-control study using the GPRD". Farmakoepidemiol dori vositasi. 12 (7): 541–50. doi:10.1002/pds.857. PMID 14558177.
^ Roe WD, Geschke K, Pease C (December 2009). "Fatal fulminant hepatitis in a chimpanzee (Pan troglodytes) receiving cyproterone acetate". J. Zoo Wildl. Med. 40 (4): 799–802. doi:10.1638/2009-0031.1. PMID 20063830.
^ ^a ^b Ralph M. Trüeb (26 February 2013). Female Alopecia: Guide to Successful Management. Springer Science & Business Media. 46- bet. ISBN 978-3-642-35503-5.
^ ^a ^b Ramsay ID, Rushton DH (July 1990). "Reduced serum vitamin B12 levels during oral cyproterone-acetate and ethinyl-oestradiol therapy in women with diffuse androgen-dependent alopecia". Klinik va eksperimental dermatologiya. 15 (4): 277–81. doi:10.1111/j.1365-2230.1990.tb02089.x. PMID 2145099.
^ Sadock BJ, Sadock VA (2010). Kaplan va Sadokning "Klinik psixiatriyaning cho'ntak qo'llanmasi". Lippincott Uilyams va Uilkins. 582– betlar. ISBN 978-1-60547-264-5.
^ Musisi S, Jacobson S (14 April 2015). Brain Degeneration and Dementia in Sub-Saharan Africa. Springer. 60- betlar. ISBN 978-1-4939-2456-1.
^ Ní Mhéalóid Á, Cunniffe G (August 2017). "Optic neuritis secondary to antiandrogen therapy". Ir J Med Sci. 186 (3): 565–570. doi:10.1007/s11845-016-1544-1. PMID 28039596.
^ Grayling M, Jardine DL, McClintock AD, Spar J, Wilton GN (March 2000). "Symptomatic epidural lipomatosis following cyproterone acetate therapy". Aust N Z J Surg. 70 (3): 233–5. doi:10.1046/j.1440-1622.2000.01793.x. PMID 10765911.
^ Mohan D, Taylor R, Mackeith JA (1998). "Cyproterone acetate and striae". Klinik amaliyotda xalqaro psixiatriya jurnali. 2 (2): 147–8. doi:10.3109/13651509809115348. PMID 24946296.
^ van der Vange N, Blankenstein MA, Kloosterboer HJ, Haspels AA, Thijssen JH (April 1990). "Effects of seven low-dose combined oral contraceptives on sex hormone binding globulin, corticosteroid binding globulin, total and free testosterone". Kontratseptsiya. 41 (4): 345–52. doi:10.1016/0010-7824(90)90034-S. PMID 2139843.
^ Stalvey JR (July 2002). "Inhibition of 3beta-hydroxysteroid dehydrogenase-isomerase in mouse adrenal cells: a direct effect of testosterone". Ukol. 67 (8): 721–31. doi:10.1016/S0039-128X(02)00023-5. PMID 12117620.

[avg-dose-10] v Average dosage; range less than 10 mg/day to >200 mg/day.

[liver-enzymes-11] Jigar fermentlari monitored in 1,685 individuals, including 1,131 males and 554 females.

[246] Reverse sequential regimen: Ayollarda hirsutizm, cyproterone acetate 100 mg/day from days 5 to 14 of the menstrual cycle and etinilestradiol 50 μg/day from days 5 to 25 of the cycle.

[247] Dayan: In women with hirsutism, cyproterone acetate 2 mg/day and ethinylestradiol 50 μg/day from days 5 to 25 of the cycle.

[pmid20096826-1] Bachelot A, Chabbert-Buffet N, Salenave S, Kerlan V, Galand-Portier MB (2010 yil fevral). "Androgenga qarshi davolash". Ann. Endokrinol. (Parij). 71 (1): 19–24. doi:10.1016 / j.ando.2009.12.001. PMID 20096826.

[pmid394887-2] Burton JL (December 1979). "Anti-androgen therapy in dermatology: a review". Klinika. Muddati Dermatol. 4 (4): 501–7. doi:10.1111/j.1365-2230.1979.tb01648.x. PMID 394887.

[Hammerstein1990-3] v ^d ^e ^f ^g Hammerstayn, J. (1990). "Antiandrogenlar: klinik jihatlar". Soch va soch kasalliklari. 827–886 betlar. doi:10.1007/978-3-642-74612-3_35. ISBN 978-3-642-74614-7.

[pmid10352926-4] Rittmaster RS (June 1999). "Antiandrogen treatment of polycystic ovary syndrome". Endokrinol. Metab. Klinika. Shimoliy Am. 28 (2): 409–21. doi:10.1016/S0889-8529(05)70077-3. PMID 10352926.

[pmid2946604-5] v ^d Belisle S, Love EJ (December 1986). "Clinical efficacy and safety of cyproterone acetate in severe hirsutism: results of a multicentered Canadian study". Urug'lantirish. Steril. 46 (6): 1015–20. doi:10.1016/S0015-0282(16)49873-0. PMID 2946604.

[pmid9856417-6] Diamanti-Kandarakis E (1998 yil oktyabr). "Polikistik tuxumdon sindromi bo'lgan bemorlarda faqat antiandrogen bilan davolash qanchalik dolzarb?". J. Endokrinol. Investitsiya. 21 (9): 623–9. doi:10.1007 / BF03350788. PMID 9856417.

[pmid10495361-7] v ^d ^e Diamanti-Kandarakis E (1999 yil sentyabr). "Ayollarda antiandrogen terapiyasining dolzarb jihatlari". Curr. Farm. Des. 5 (9): 707–23. PMID 10495361.

[pmid19243704-8] Guay DR (January 2009). "Drug treatment of paraphilic and nonparaphilic sexual disorders". Klinik The. 31 (1): 1–31. doi:10.1016/j.clinthera.2009.01.009. PMID 19243704. No quantitative data on these adverse events are available, even in the product prescribing information and data sheets.

[pmid10673793-9] v Migliari R, Muscas G, Murru M, Verdacchi T, De Benedetto G, De Angelis M (1999). "Antiandrogenlar: prostata saratoni terapiyasida farmakodinamik xususiyatlari va bardoshliligini qisqacha ko'rib chiqish". Archivio Italiano di Urologia e Andrologia. 71 (5): 293–302. PMID 10673793. The only advantage of cyproterone acetate on pure antiandrogens seems to be the low incidence of hot flushes; [...] However, hepatotoxicity associated with long term daily doses of 300 mg daily and the unacceptably high incidence of cardiovascular side effects (10%) should restrict its use to patients who are intolerant of pure antiandrogen compound. In contrast to steroidal compound nonsteroidal compounds let sexual potency to be retained, [...]

[Wakelin2002-12] v Sara H. Vakelin (2002 yil 1-iyun). Dermatologiyada dori-darmonlarni tizimli davolash: qo'llanma. CRC Press. p. 32. ISBN 978-1-84076-013-2.

[GräfBrotherton1974-13] Graf, K.-J .; Brotherton, J .; Neumann, F. (1974). "Clinical Uses of Antiandrogens". Androgenlar II va antiandrogenlar / Androgene II und antiandrogene. 485-542 betlar. doi:10.1007/978-3-642-80859-3_7. ISBN 978-3-642-80861-6.

[IversenMelezinek2001-14] Iversen P, Melezinek I, Schmidt A (January 2001). "Nonsteroidal antiandrogens: a therapeutic option for patients with advanced prostate cancer who wish to retain sexual interest and function". BJU xalqaro. 87 (1): 47–56. doi:10.1046/j.1464-410x.2001.00988.x. PMID 11121992.

[Priestman2012-15] Terrence Priestman (26 May 2012). Cancer Chemotherapy in Clinical Practice. Springer Science & Business Media. 97– betlar. ISBN 978-0-85729-727-3.

[pmid16321765-16] Di Lorenzo G, Autorino R, Perdonà S, De Placido S (2005). "Management of gynaecomastia in patients with prostate cancer: a systematic review". Lanset Onkol. 6 (12): 972–9. doi:10.1016/S1470-2045(05)70464-2. PMID 16321765.

[pmid12901287-17] Hirawat S, Budman DR, Kreis W (June 2003). "The androgen receptor: structure, mutations, and antiandrogens". Saraton kasalligi. 21 (3): 400–17. doi:10.1081/CNV-120018232. PMID 12901287.

[pmid15041109-18] v ^d ^e Schröder FH, Whelan P, de Reijke TM, Kurth KH, Pavone-Macaluso M, Mattelaer J, van Velthoven RF, Debois M, Collette L (April 2004). "Metastatic prostate cancer treated by flutamide versus cyproterone acetate. Final analysis of the "European Organization for Research and Treatment of Cancer" (EORTC) Protocol 30892". Yevro. Urol. 45 (4): 457–64. doi:10.1016/j.eururo.2003.11.016. PMID 15041109.

[Shiffman2012-19] Shiffman, Melvin A. (2012). "Cellulite: Etiology, Classification, Pathology, and Treatment". Estetik tibbiyot. pp. 265–272. doi:10.1007/978-3-642-20113-4_25. ISBN 978-3-642-20112-7.

[Mylan-CyproteroneLabel-20] "Mylan-Cyproterone Label" (PDF).

[pmid15073785-21] v ^d ^e Heinemann LA, Will-Shahab L, van Kesteren P, Gooren LJ (May 1997). "Safety of cyproterone acetate: report of active surveillance". Farmakoepidemiol dori vositasi. 6 (3): 169–78. doi:10.1002/(SICI)1099-1557(199705)6:3<169::AID-PDS263>3.0.CO;2-3. PMID 15073785.

[AndrocurLabel-22] "Androcur Label" (PDF).

[Barrett2007-23] James Barrett (2007). Transsexual and Other Disorders of Gender Identity: A Practical Guide to Management. Radcliffe Publishing. p. 174. ISBN 978-1-85775-719-4.

[BarthCherry1991-24] Barth JH, Cherry CA, Wojnarowska F, Dawber RP (July 1991). "Cyproterone acetate for severe hirsutism: results of a double-blind dose-ranging study". Klinik endokrinologiya. 35 (1): 5–10. doi:10.1111/j.1365-2265.1991.tb03489.x. PMID 1832346.

[pmid12190640-25] Rushton DH (July 2002). "Nutritional factors and hair loss". Klinika. Muddati Dermatol. 27 (5): 396–404. doi:10.1046/j.1365-2230.2002.01076.x. PMID 12190640.

[pmid12175403-26] Green HJ, Pakenham KI, Headley BC, Yaxley J, Nicol DL, Mactaggart PN, Swanson C, Watson RB, Gardiner RA (September 2002). "Altered cognitive function in men treated for prostate cancer with luteinizing hormone-releasing hormone analogues and cyproterone acetate: a randomized controlled trial" (PDF). BJU Int. 90 (4): 427–32. doi:10.1046/j.1464-410X.2002.02917.x. hdl:10072/16905. PMID 12175403.

[pmid15852051-27] Kaisary AV (2005). "Evaluating the use of early hormonal therapy in patients with localised or locally advanced prostate cancer". Prostate Cancer Prostatic Dis. 8 (2): 140–51. doi:10.1038/sj.pcan.4500800. PMID 15852051.

[pmid15142146-28] Green HJ, Pakenham KI, Headley BC, Yaxley J, Nicol DL, Mactaggart PN, Swanson CE, Watson RB, Gardiner RA (May 2004). "Quality of life compared during pharmacological treatments and clinical monitoring for non-localized prostate cancer: a randomized controlled trial". BJU Int. 93 (7): 975–9. doi:10.1111/j.1464-410X.2004.04763.x. hdl:10072/16906. PMID 15142146.

[SealFranklin2012-29] Seal LJ, Franklin S, Richards C, Shishkareva A, Sinclaire C, Barrett J (December 2012). "Predictive markers for mammoplasty and a comparison of side effect profiles in transwomen taking various hormonal regimens". Klinik endokrinologiya va metabolizm jurnali. 97 (12): 442–8. doi:10.1210/jc.2012-2030. PMID 23055547.

[pmid26932202-30] Gava G, Cerpolini S, Martelli V, Battista G, Seracchioli R, Meriggiola MC (August 2016). "Cyproterone acetate vs leuprolide acetate in combination with transdermal oestradiol in transwomen: a comparison of safety and effectiveness". Klinika. Endokrinol. (Oxf). 85 (2): 239–46. doi:10.1111/cen.13050. PMID 26932202.

[pmid24275005-31] Colizzi M, Costa R, Todarello O (January 2014). "Transseksual bemorlarning psixiatrik komorbidligi va o'zaro faoliyat jinsiy gormonal davolashning ruhiy salomatlikka ijobiy ta'siri: bo'ylama tadqiqot natijalari". Psixonuroendokrinologiya. 39: 65–73. doi:10.1016 / j.psyneuen.2013.09.029. PMID 24275005.

[pmid27700538-32] Fisher AD, Castellini G, Ristori J, Casale H, Cassioli E, Sensi C, Fanni E, Amato AM, Bettini E, Mosconi M, Déttore D, Ricca V, Maggi M (Noyabr 2016). "Jinsiy aloqada gormonlarni davolash va transseksual odamlarda psixobiologik o'zgarishlar: ikki yillik kuzatuv ma'lumotlari" (PDF). J. klinikasi. Endokrinol. Metab. 101 (11): 4260–4269. doi:10.1210 / jc.2016-1276. PMID 27700538.

[pmid12600226-33] Raudrant D, Rabe T (2003). "Antiandrogenik xususiyatlarga ega progestogenlar". Giyohvand moddalar. 63 (5): 463–92. doi:10.2165/00003495-200363050-00003. PMID 12600226.

[SeamanSnowball2006-34] Dengizchi HE, Snowball J, de Vries CS (2006). "Kiproteron asetat + etinioloestradiol va depressiya xavfi". Farmakoepidemiologiya va dori vositalari xavfsizligi. 15 (S1): S25. doi:10.1002 / pds.1295. ISSN 1053-8569. PMID 16986216.

[Husmann1997-35] Husmann, Fridrix (1997). "Gormonlarni almashtirish uchun Estradiol Valerate va Cyproterone Acetate kombinatsiyasi bilan klinik tajribalar". Ayollar salomatligi va menopauza. Tibbiyot fanlari bo'yicha simpoziumlar seriyasi. 11. 257-261 betlar. doi:10.1007/978-94-011-5560-1_38. ISBN 978-94-010-6343-2. ISSN 0928-9550.

[WakelinMaibach2015-36] Waken SH, Maibach HI, Archer CB (2015 yil 21-may). Dermatologiyada dori-darmonlarni tizimli davolash bo'yicha qo'llanma (Ikkinchi nashr). CRC Press. 34– betlar. ISBN 978-1-4822-2286-9.

[pmid19297634-37] v ^d ^e ^f ^g ^h ^men ^j ^k ^l ^m Giltay EJ, Gooren LJ (2009). "Jinsiy jinoyatchilarda androgen etishmovchiligini davolashning potentsial yon ta'siri". J. Am. Akad. Psixiatriya qonuni. 37 (1): 53–8. PMID 19297634.

[pmid12927003-38] v Briken P, Hill A, Berner V (avgust 2003). "Luteinlashtiruvchi gormonni chiqaradigan gormonning uzoq muddatli agonistlari bilan parafiliyalarning farmakoterapiyasi: tizimli ko'rib chiqish". J klinik psixiatriya. 64 (8): 890–7. doi:10.4088 / JCP.v64n0806. PMID 12927003.

[pmid21074215-39] v Wibowo E, Schellhammer P, Wassersug RJ (2011 yil yanvar). "Erkakning normal faoliyatidagi estrogenning roli: prostata saratoni bilan og'rigan bemorlarning androgen etishmovchiligini davolash bo'yicha klinik ta'siri". J. Urol. 185 (1): 17–23. doi:10.1016 / j.juro.2010.08.094. PMID 21074215.

[JagielskaPoniatowska2017-40] v ^d ^e Yagelska, Beata; Poniatowska, Grenna; Talasevich, Konrad; Demkov, Tomash; Wiechno, Pawel (2017). "Prostata va ko'krak bezi saratonini gormonal davolashda tizimli asoratlar". Nowotwory. Onkologiya jurnali. 67 (3): 206–214. doi:10.5603 / NJO.2017.0034. ISSN 2300-2115.

[pmid12877306-41] v Grassvik LJ, Bredford JM (2003 yil iyul). "Parafiliyani davolash bilan bog'liq osteoporoz: ettita hisobotni klinik ko'rib chiqish". J. Sud-tibbiyot fanlari doktori. 48 (4): 849–55. doi:10.1520 / JFS2002089. PMID 12877306.

[pmid11392035-42] Lindsay R (1999). "Suyakka progestogen ta'sirining etishmasligi". J Reprod Med. 44 (2 ta qo'shimcha): 215-20. PMID 11392035.

[CurtisMartins2006-43] Kertis, Ketrin M.; Martins, Yozgi L. (2006). "Faqatgina progestogen kontratseptsiyasi va suyak minerallarining zichligi: tizimli tahlil". Kontratseptsiya. 73 (5): 470–487. doi:10.1016 / j.contraception.2005.12.010. ISSN 0010-7824. PMID 16627031.

[Sarfatide_Vernejoul2009-44] Sarfati, Juli; de Vernejoul, Mari-Kristin (2009). "Faqatgina estrodiol va progestogen kontratseptiv vositalarining suyak mineral zichligiga ta'siri". Qo'shma suyak umurtqasi. 76 (2): 134–138. doi:10.1016 / j.jbspin.2008.09.014. ISSN 1297-319X. PMID 19181558.

[pmid23168292-45] Nelson ER, Wardell SE, McDonnell DP (mart 2013). "Estrogenlar, SERMlar va oksisterollarning farmakologik ta'siriga asoslangan molekulyar mexanizmlar: osteoporozni davolash va oldini olish uchun ta'siri". Suyak. 53 (1): 42–50. doi:10.1016 / j.bone.2012.11.011. PMC 3552054. PMID 23168292.

[pmid6933738-46] Spona J, Lunglmayr G (1980 yil iyul). Prolaktin-Serumspiegel unter Behandlung des Prostatakarzinoms mit Östradiol-17 beta-undezylat und Cyproteronazetat [Estradiol-17 beta-undesilat va siproteron asetat bilan prostata saratonini davolash paytida sarum prolaktin darajasi.]. Wien. Klin. Voxenschr. Verhandlungsbericht der Deutschen Gesellschaft für Urologie (nemis tilida). 92. 494-7 betlar. doi:10.1007/978-3-642-81706-9_120. ISBN 978-3-540-11017-0. ISSN 0043-5325. PMID 6933738.

[SchürmeyerGraff1986-47] Shюрmeyer, Th .; Graf J.; Senge, Th .; Nieschlag, E. (1986). "Prostata karsinomasi bilan kasallangan bemorlarda estrogen yoki siproteron asetat bilan davolashning adrenokortikal funktsiyaga ta'siri". Acta Endocrinologica. 111 (3): 360–367. doi:10.1530 / akta.0.1110360. ISSN 0804-4643. PMID 2421511.

[HolubLunglmayr1981-48] Xolub, G.; Lunglmayr, G.; Spona, J. (1981). "Prostata saratoni bilan kasallangan bemorlarda siproteron / asetatning (SH-714) plazmadagi prolaktinga ta'siri". Urologik tadqiqotlar. 9 (5): 245–7. doi:10.1007 / BF00256895. ISSN 0300-5623. PMID 6458145.

[RostSchmidt-Gollwitzer1981-49] Rost, A .; Shmidt-Gollvitser, M.; Xantelmann, V.; Brosig, V. (1981). "Prostata saratoni bilan og'rigan bemorlarga mushak ichiga siproteron asetat yuborilgandan so'ng plazmadagi siproteron asetat, testosteron, LH, FSH va prolaktin miqdori". Prostata. 2 (3): 315–322. doi:10.1002 / pros.2990020310. ISSN 0270-4137. PMID 6458025.

[JeffcoateMatthews1980-50] Jeffcoate, W. J.; Metyus, R. V.; Edvards, C. R. V.; Field, L. H .; Besser, G. M. (1980). "Kiproteron asetatning qon zardobidagi testosteron, LH, FSH va prolaktinga jinsiy aloqada bo'lgan erkaklarda ta'siri". Klinik endokrinologiya. 13 (2): 189–195. doi:10.1111 / j.1365-2265.1980.tb01041.x. ISSN 0300-0664. PMID 6777092.

[GrafSchmidtgollwitzer1978-51] Graf, K. J., Shmidtgollvitser, M., Koch, U. J., Lorenz, F. va Hammerstayn, J. (1978, yanvar). Kiproteron asetat tomonidan inson sub'ektlarida paydo bo'lgan giperprolaktinemiya. Acta Endocrinologica-da (87-jild, 96-96-betlar).

[BercovichCigno1983-52] Bercovich, E., Cigno, M., & Soli, M. (1983, yanvar). Prostata karsinomasi bo'lgan bemorlarda siproteron asetat terapiyasi natijasida kelib chiqadigan sarum prolaktin darajasi. Prostatda (4-jild, 4-son, 425-426-betlar).

[pmid28880825-53] Defreyne J, Nota N, Pereyra S, Shrayner T, Fisher AD, den Heijer M, T'Sjoen G (oktyabr 2017). "Trans ayollarda sarum prolaktinning vaqtincha ko'tarilishi, kiproteron asetat bilan davolash natijasida yuzaga keladi". LGBT sog'liqni saqlash. 4 (5): 328–336. doi:10.1089 / lgbt.2016.0190. PMID 28880825.

[FonzoAngeli1977-54] Fonzo, Domeniko; Anjeli, Alberto; Sivieri, Roberto; Andriolo, Salvatore; Fraxriya, Roberto; Ceresa, Franko (1977). "Kiproteron asetat bilan uzoq muddatli davolanishda idiopatik erta balog'atga etgan qizlarda giperprolaktinemiya". Klinik endokrinologiya va metabolizm jurnali. 45 (1): 164–168. doi:10.1210 / jcem-45-1-164. ISSN 0021-972X. PMID 874063.

[MahWebster2002-55] v ^d ^e Mah, tepalik Mann; Vebster, Jonathan (2002). "Giperprolaktinemiya: etiologiya, diagnostika va boshqarish". Reproduktiv tibbiyot bo'yicha seminarlar. 20 (4): 365–374. doi:10.1055 / s-2002-36709. ISSN 1526-8004. PMID 12536359.

[pmid21627676-56] v ^d ^e ^f Gil M, Oliva B, Timoner J, Macia MA, Bryant V, de Abajo FJ (dekabr 2011). "Kiproteron asetatning yuqori dozalarini iste'mol qiluvchilar orasida umumiy populyatsiya bilan taqqoslaganda meningioma xavfi: populyatsiyaga asoslangan kogort tadqiqotining dalillari". Br J Clin Farmakol. 72 (6): 965–8. doi:10.1111 / j.1365-2125.2011.04031.x. PMC 3244644. PMID 21627676.

[WilliamsGianfortoni1985-57] Uilyams, Robert F.; Janfortoni, Jozef G.; Xodgen, Gari D. (1985). "Estrogen-progesteron sinergiyasi keltirib chiqaradigan giperprolaktinemiya: maymunlarda estrogen primeratsiyasining miqdoriy va vaqtinchalik ta'siri *". Klinik endokrinologiya va metabolizm jurnali. 60 (1): 126–132. doi:10.1210 / jcem-60-1-126. ISSN 0021-972X. PMID 3964786.

[WilliamsBarber1981-58] Uilyams, Robert F.; Sartarosh, Donald L.; Kovan, Brayan D. Linch, Almorris; Marut, Edvard L.; Xodgen, Gari D. (1981). "Maymunlarda giperprolaktinemiya: estrogen-progesteron sinergiyasi orqali induksiya". Ukol. 38 (3): 321–331. doi:10.1016 / 0039-128X (81) 90067-2. ISSN 0039-128X. PMID 7303037.

[MoltzRömmler1980-59] Molts, L .; Romler, A .; Pochta, K .; Shvarts, U .; Hammerstayn, J. (1980). "O'rtacha dozada siproteron asetat (CPA): gormon sekretsiyasiga va erkaklarda spermatogenezga ta'siri". Kontratseptsiya. 21 (4): 393–413. doi:10.1016 / S0010-7824 (80) 80017-5. ISSN 0010-7824. PMID 6771095.

[MoltzRömmler1978a-60] Molts, L .; Romler, A .; Shvarts, U .; Pochta, K .; Hammerstayn, J. (1978). "252. Cyproterone asetate (CPA) - potentsial erkak kontratseptivi: endokrin parametrlar bilan o'zaro ta'sirlarni o'rganish". Steroid biokimyosi jurnali. 9 (9): 865. doi:10.1016/0022-4731(78)90952-4. ISSN 0022-4731.

[MoltzRömmler1978b-61] Molts, L .; Romler, A .; Shvarts, U .; Hammerstayn, J. (1978). "Cyproterone Acetate (CPA) ning gipofiz gonadotrofini chiqarilishiga va erkaklarda LH-RH qo'shaloq stimulyatsiya testlaridan oldin va keyin Androgen sekretsiyasiga ta'siri". Xalqaro Andrologiya jurnali. 1 (s2b): 713-719. doi:10.1111 / j.1365-2605.1978.tb00518.x. ISSN 0105-6263.

[MeriggiolaCostantino2003-62] Meriggiola, M. C .; Kostantino, A .; Cerpolini, S .; Bremner, V. J.; Xyebler, D.; Morselli-Labate, A. M.; Kirsh, B .; Bertachini, A .; Pelusi, S.; Pelusi, G. (2003). "Testosteron undekanoat oddiy erkaklarda kiproteron asetat plyus testosteron undekanoat tomonidan spermatogen ta'sirni to'xtatadi". Klinik endokrinologiya va metabolizm jurnali. 88 (12): 5818–5826. doi:10.1210 / jc.2003-030574. ISSN 0021-972X. PMID 14671175.

[pmid2528051-63] v ^d ^e ^f Asscheman H, Gooren LJ, Eklund PL (sentyabr 1989). "Jinsiy gormonlar bilan davolash qilingan transseksual bemorlarda o'lim va kasallanish" (PDF). Metab. Klinika. Muddati. 38 (9): 869–73. doi:10.1016/0026-0495(89)90233-3. PMID 2528051.

[pmid2978262-64] v ^d Asscheman H, Gooren LJ, Assies J, Smits JP, de Slegte R (iyun 1988). "Prolaktin darajasi va gipofizning kengayishi gormon bilan davolash qilingan erkak va ayol transseksuallari". Klinika. Endokrinol. (Oxf). 28 (6): 583–8. doi:10.1111 / j.1365-2265.1988.tb03849.x. PMID 2978262.

[pmid3157511-65] v ^d ^e ^f Gooren LJ, Harmsen-Louman V, van Kessel H (1985 yil fevral). "Prolaktinom induktsiyasiga nisbatan uzoq muddatli estrogen bilan davolash qilingan erkak va ayol transseksuallarda prolaktin miqdorini kuzatib borish". Klinika. Endokrinol. (Oxf). 22 (2): 201–7. doi:10.1111 / j.1365-2265.1985.tb01081.x. PMID 3157511.

[CapozziScambia2015-66] Kapozzi, Anna; Skambiya, Jovanni; Pontekorvi, Alfredo; Lello, Stefano (2015). "Giperprolaktinemiya: patofiziologiya va terapevtik yondashuv". Ginekologik endokrinologiya. 31 (7): 506–510. doi:10.3109/09513590.2015.1017810. ISSN 0951-3590. PMID 26291795.

[NaidooGoff2003-67] Naidoo, U .; Goff, DC; Klibanski, A. (2003). "Giperprolaktinemiya va suyak mineral zichligi: antipsikotik vositalarning potentsial ta'siri". Psixonuroendokrinologiya. 28: 97–108. doi:10.1016 / S0306-4530 (02) 00129-4. ISSN 0306-4530. PMID 12650684.

[RastrelliCorona2015-68] v Rastrelli, Giuliya; Korona, Jovanni; Maggi, Mario (2015). "Prolaktinning andrologiyadagi o'rni: nima yangilik?". Endokrin va metabolik kasalliklarning sharhlari. 16 (3): 233–248. doi:10.1007 / s11154-015-9322-3. ISSN 1389-9155. PMID 26542707.

[Buvat2003-69] Buvat, J (2003). "Giperprolaktinemiya va erkaklarda jinsiy funktsiya: qisqa sharh". Immunitetni o'rganish bo'yicha xalqaro jurnal. 15 (5): 373–377. doi:10.1038 / sj.ijir.3901043. ISSN 0955-9930. PMID 14562140.

[Krüger2002-70] Kruger, T (2002). "Orgazmdan kelib chiqadigan prolaktin sekretsiyasi: jinsiy aloqani qayta tiklash nazorati?". Neuroscience & Biobehavioral Sharhlar. 26 (1): 31–44. doi:10.1016 / S0149-7634 (01) 00036-7. ISSN 0149-7634. PMID 11835982.

[VerhelstAbs2003-71] v Verxelst, Yoxan; Abs, Rojer (2003). "Giperprolaktinemiya". Endokrinologiyada davolash usullari. 2 (1): 23–32. doi:10.2165/00024677-200302010-00003. ISSN 1175-6349. PMID 15871552.

[pmid18473017-72] La Torre D, Falorni A (2007). "giperprolaktinemiyaning garmonik sabablari". Terapevtik va klinik xatarlarni boshqarish. 3 (5): 929–951. PMC 2376090. PMID 18473017.

[pmid9795728-73] Schlatterer K, Yassouridis A, fon Verder K, Polsha D, Kemper J, Stalla GK (oktyabr 1998). "Transseksual bemorlarga xoch-gender gormonlarini almashtirish terapiyasining samaradorligini baholash bo'yicha keyingi tadqiqotlar". Arch Sex Behav. 27 (5): 475–92. doi:10.1023 / a: 1018704630036. PMID 9795728.

[Bazarra-Castro2009-74] Bazarra-Kastro, M. Á. (2009). Transseksual bemorlarning etiologik jihatlari, terapiya rejimi, yon ta'siri va davolanishdan qoniqishi (doktorlik dissertatsiyasi, LMU Myunxen). doi: 10.5282 / edoc.9984

[FrawleyPorter1990-75] Frouli, L. Stiven; Porter, Tom E.; Kineman, Rhonda D. (1990). "Prolaktinning maqsadli hujayralarga ta'siri". Neyroendokrin istiqbollari. 8. 39-75 betlar. doi:10.1007/978-1-4612-3446-3_2. ISBN 978-1-4612-8014-9. ISSN 0168-0617.

[Bole-FeysotGoffin1998-76] Bole-Feysot, Kristin; Goffin, Vinsent; Ederi, Mark; Binart, Nadin; Kelly, Pol A. (1998). "Prolaktin (PRL) va uning retseptorlari: harakatlar, signal uzatish yo'llari va PRL retseptorlari nokautli sichqonlarida kuzatiladigan fenotiplar". Endokrin sharhlar. 19 (3): 225–268. doi:10.1210 / edrv.19.3.0334. ISSN 0163-769X. PMID 9626554.

[HiguchiNawata1984-77] Xiguchi, Kazumi; Navata, Xajime; Maki, Toshio; Xigashizima, Masayoshi; Kato, Ken-Ichi; Ibayashi, Xiroshi (1984). "Prolaktin buyrak usti bezining androgen sekretsiyasiga bevosita ta'sir qiladi". Klinik endokrinologiya va metabolizm jurnali. 59 (4): 714–718. doi:10.1210 / jcem-59-4-714. ISSN 0021-972X. PMID 6090494.

[SchiebingerChrousos1986-78] Shibinger, Rik J.; Chrousos, Jorj P.; Kulter, Gordon B.; Loriaux, D. Lin (1986). "Qon zardobidagi prolaktinning plazmadagi buyrak usti androgenlariga ta'siri va normal va giperprolaktinemik mavzulardagi dehidroepiandrosteron sulfatning ishlab chiqarish va metabolizm darajasi". Klinik endokrinologiya va metabolizm jurnali. 62 (1): 202–209. doi:10.1210 / jcem-62-1-202. ISSN 0021-972X. PMID 2999177.

[LanganHinde2018-79] Langan, Evan A.; Xinde, Eleanora; Paus, Ralf (2018). "Prolaktin sebotrop (h) ic gormoni nomzodi sifatida?". Eksperimental dermatologiya. 27 (7): 729–736. doi:10.1111 / exd.13545. ISSN 0906-6705. PMID 29582473.

[pmid9476091-80] Pucci E, Petraglia F (1997 yil dekabr). "Ayollarda androgen ortiqcha davolash: kecha, bugun va ertaga". Jinekol. Endokrinol. 11 (6): 411–33. doi:10.3109/09513599709152569. PMID 9476091.

[pmid2941191-81] Miller JA, Jacobs HS (may 1986). "Hirsutizm va husnbuzarlarni siproteron asetat bilan davolash". Klinik Endokrinol Metab. 15 (2): 373–89. doi:10.1016 / S0300-595X (86) 80031-7. PMID 2941191.

[pmid29930875-82] v ^d ^e Raj R, Korja M, Koroknay-Pal P, Niemelä M (2018). "Gormonlarni almashtirish terapiyasi bilan olib borilgan ikkita erkak-ayol transseksual bemorlarda bir nechta meningioma: ikkita holat bo'yicha hisobot va qisqacha adabiyotlarni ko'rib chiqish". Surg Neurol Int. 9: 109. doi:10.4103 / sni.sni_22_18. PMC 5991277. PMID 29930875.

[pmid29688280a-83] v ^d ^e ^f Nota NM, Wiepjes CM, de Blok C, Gooren LJ, Peerdeman SM, Kreukels B, den Heijer M (iyul 2018). "Jinsiy aloqada gormonlarni davolash paytida transseksual odamlarda yaxshi xulqli miya shishi paydo bo'lishi". Miya. 141 (7): 2047–2054. doi:10.1093 / miya / awy108. PMID 29688280.

[JamesonGroot2015-84] J. Larri Jeymson; Lesli J. De Groot (2015 yil 25-fevral). Endokrinologiya: kattalar va bolalar uchun elektron kitob. Elsevier sog'liqni saqlash fanlari. 2293, 2464, 2479, 6225-betlar. ISBN 978-0-323-32195-2.

[ScholarlyEditions2012-85] Meningeal neoplazmalar - tadqiqot va davolashning yutuqlari: 2012 yil nashr: ScholarlyBrief. ScholarlyEditions. 26 dekabr 2012. 99- bet. ISBN 978-1-4816-0002-6.

[Dickman2012-86] Dikman A (2012 yil 27 sentyabr). Palliativ yordamda giyohvand moddalar. Oksford. 137-138 betlar. ISBN 978-0-19-966039-1.

[pmid29703641-87] v Schmutz JL (2018 yil may). "Méningiomes et acétate de cyprotérone: mise au point" [Cyproterone acetate and meningioma: So'nggi topilmalar]. Ann Dermatol Venereol (frantsuz tilida). 145 (5): 390–391. doi:10.1016 / j.annder.2018.04.001. PMID 29703641.

[pmid11108890-88] Blankenshteyn MA, Verheijen FM, Jacobs JM, Donker TH, van Duijnhoven MW, Thijssen JH (2000). "Progesteron retseptorlari paydo bo'lishi, boshqarilishi va inson meningiomasida ahamiyati". Ukol. 65 (10–11): 795–800. doi:10.1016 / S0039-128X (00) 00193-8. PMID 11108890.

[Melmed2010-89] Shlomo Melmed (2010 yil 9-dekabr). Gipofiz. Akademik matbuot. 227– betlar. ISBN 978-0-12-380927-8.

[AcademicPress2005-90] Knobil va Neillning ko'payish fiziologiyasi. Akademik matbuot. 2005 yil 12 dekabr. 1557– betlar. ISBN 978-0-08-053527-2.

[FritzSperoff2011p1091-91] Mark A. Fritz; Leon Speroff (2011). Klinik ginekologik endokrinologiya va bepushtlik. Lippincott Uilyams va Uilkins. 1091– betlar. ISBN 978-0-7817-7968-5.

[pmid29105524-92] v ^d ^e Manchini I, Rotilio A, Coati I, Seracchioli R, Martelli V, Meriggiola MC (iyun 2018). "To'qqiz yillik siproteron asetat va estradiolni qabul qilganidan keyin transminologda meningioma prezentatsiyasi: holatlar bo'yicha hisobot va adabiyotlarni o'rganish". Jinekol. Endokrinol. 34 (6): 456–459. doi:10.1080/09513590.2017.1395839. PMID 29105524.

[pmid26888610-93] v ^d ^e ^f Ter Vengel PV, Martin E, Gooren L, Den Heijer M, Peerdeman SM (dekabr 2016). "Ostrogenlar / progestogenlar va adabiyotlarni ko'rib chiqish yordamida uchta erkak va ayol transgender sub'ektlarida menenjiyomalar". Andrologiya. 48 (10): 1130–1137. doi:10.1111 / va.12550. PMID 26888610.

[pmid14670648-94] Gruber CJ, Huber JC (2003 yil dekabr). "Progestinlarning miyaga differentsial ta'siri". Maturitalar. 46 Qo'shimcha 1: S71-5. doi:10.1016 / j.maturitas.2003.09.021. PMID 14670648.

[pmid11045205-95] Hensiek AE, Kellerman AJ, Hill JT (2000 yil avgust). "Buyrak karsinomasida miya yarim metastazlarining o'z-o'zidan regressiyasi, so'ngra medroksiprogesteron asetat terapiyasi ostida meningioma rivojlanishi". Br J Neurosurg. 14 (4): 354–6. doi:10.1080/026886900417388. PMID 11045205.

[pmid30783806-96] Passeri T, Shampan PO, Bernat AL, Xanakita S, Salle H, Mandonnet E, Froelich S (aprel, 2019). "Nomegestrol asetat uzilishidan so'ng meningiomalarning o'z-o'zidan regressiyasi: uchta bemorning ketma-ketligi". Acta Neurochir (Wien). 161 (4): 761–765. doi:10.1007 / s00701-019-03848-x. PMID 30783806.

[pmid3339116-97] Gooren LJ, Assies J, Asscheman H, de Slegte R, van Kessel H (fevral, 1988). "Erkakdagi estrogen ta'siridagi prolaktinoma". J. klinikasi. Endokrinol. Metab. 66 (2): 444–6. doi:10.1210 / jcem-66-2-444. PMID 3339116.

[pmid8784065a-98] Serri O, Noiseux D, Robert F, Hardy J (sentyabr 1996). "Estrogen bilan davolash qilingan erkak va ayol transseksual bemorda laktotrof giperplaziyasi". J. klinikasi. Endokrinol. Metab. 81 (9): 3177–9. doi:10.1210 / jcem.81.9.8784065. PMID 8784065.

[pmid20227072-99] García-Malpartida K, Martin-Gorgojo A, Rocha M, Gomes-Balaguer M, Hernández-Mijares A (avgust 2010). "Erkak va ayol transseksualida estrogen va siproteron asetat tomonidan qo'zg'atilgan prolaktinoma". Urug'lantirish. Steril. 94 (3): 1097.e13-5. doi:10.1016 / j.fertnstert.2010.01.076. PMID 20227072.

[pmid21829422-100] v Bunck MC, Debono M, Giltay EJ, Verheijen AT, Diamant M, Gooren LJ (2009). "An'anaviy estrogen dozalarini qo'llagan holda, transgender bo'lgan ikki erkakdan ayolga avtonom prolaktin sekretsiyasi". BMJ ishi vakili. 2009: bcr0220091589. doi:10.1136 / bcr.02.2009.1589. PMC 3029513. PMID 21829422.

[pmid25059808-101] v Cunha FS, Domenice S, Kamara VL, Sircili MH, Gooren LJ, Mendonça BB, Kosta EM (Avgust 2015). "Yuqori dozada o'zaro faoliyat jinsiy gormonlar terapiyasidan so'ng ikki erkak va ayol transseksual sub'ektlarda prolaktinoma diagnostikasi". Andrologiya. 47 (6): 680–4. doi:10.1111 / va.12317. PMID 25059808.

[pmid18057351-102] Gazzeri R, Galarza M, Gazzeri G (2007 yil dekabr). "Transseksual bemorda menenjiyomaning estrogen-progestin terapiyasidan keyin o'sishi". N. Engl. J. Med. 357 (23): 2411–2. doi:10.1056 / NEJMc071938. PMID 18057351.

[pmid20594855-103] Deipolyi AR, Xan SJ, Parsa AT (oktyabr 2010). "Gormon terapiyasini boshlaganidan keyin erkak va ayol transseksualda simptomatik intrakranial meningioma rivojlanishi". J Clin Neurosci. 17 (10): 1324–6. doi:10.1016 / j.jocn.2010.01.036. PMID 20594855.

[pmid20811919-104] Cebula H, Pham TQ, Boyer P, Froelich S (2010 yil noyabr). "Transseksual bemorda siproteron asetat to'xtatilgandan so'ng meningiomalarning regressiyasi". Acta Neurochir (Wien). 152 (11): 1955–6. doi:10.1007 / s00701-010-0787-2. PMID 20811919.

[pmid23022362-105] Bergoglio MT, Gomes-Balaguer M, Almonacid Folch E, Hurtado Murillo F, Hernández-Mijares A (may, 2013). "Erkak va ayol transseksualida o'zaro faoliyat jinsiy gormonlarni davolash natijasida kelib chiqadigan simptomatik meningioma". Endokrinol Nutr. 60 (5): 264–7. doi:10.1016 / j.endonu.2012.07.004. PMID 23022362.

[pmid18567667-106] Myuller A, Gooren L (sentyabr 2008). "Jinsiy gormonlar bilan davolanadigan transseksuallarda gormon bilan bog'liq o'smalar". Yevro. J. Endokrinol. 159 (3): 197–202. doi:10.1530 / EJE-08-0289. PMID 18567667.

[pmid21943794-107] Cea-Soriano L, Blenk T, Wallander MA, Rodriges LA (aprel 2012). "Gormonal terapiya va meningioma: aloqasi bormi?". Saraton epidemiyasi. 36 (2): 198–205. doi:10.1016 / j.canep.2011.08.003. PMID 21943794.

[pmid28945902-108] Hembree WC, Cohen-Kettenis PT, Gooren L, Hannema SE, Meyer WJ, Murad MH, Rosenthal SM, Safer JD, Tangpricha V, T'Sjoen GG (2017 yil noyabr). "Gender-disforik / jinsga mos kelmaydigan shaxslarni endokrin davolash: endokrin jamiyatning klinik amaliyoti bo'yicha ko'rsatma". J. klinikasi. Endokrinol. Metab. 102 (11): 3869–3903. doi:10.1210 / jc.2017-01658. PMID 28945902.

[pmid30107028a-109] McFarlane T, Zajac JD, Cheung AS (dekabr 2018). "Genderni tasdiqlovchi gormon terapiyasi va transgenderlarda jinsiy gormonga bog'liq o'smalar paydo bo'lishi xavfi-Tizimli tekshiruv". Klinika. Endokrinol. (Oxf). 89 (6): 700–711. doi:10.1111 / sen.13835. PMID 30107028.

[OettelSchillinger2012-110] Oettel M, Schillinger E (2012 yil 6-dekabr). Estrogenlar va antiestrogenlar II: Estrogenlar va antiestrogenlarning farmakologiyasi va klinik qo'llanilishi. Springer Science & Business Media. 544– betlar. ISBN 978-3-642-60107-1.

[pmid8192565-111] Kovacs K, Stefaneanu L, Ezzat S, Smith HS (may 1994). "Uzoq muddatli estrogen yuborilishi bilan erkak va ayol transseksual bemorda prolaktin ishlab chiqaradigan gipofiz adenomasi. Morfologik tadqiqot". Arch. Pathol. Laboratoriya laboratoriyasi. Med. 118 (5): 562–5. PMID 8192565.

[GiraldiHansen2019-112] Giraldi, Laura; Xansen, Yorgen Vinslov; Vohlfahrt, Jan; Xayr, jinnilar; Fugleholm, Kare; Munk, Tina Norgaard (2019). "Erkaklar gormonlariga xalaqit beradigan dorilar va meningioma rivojlanishi". Neyro-onkologiya yutuqlari. 1. doi:10.1093 / noajnl / vdz046. ISSN 2632-2498.

[pmid31686447-113] Kang BM, Youn SM (oktyabr 2019). "Meningiomani simikatsiya qiladigan suprasellar gemangioblastoma holati". Miya o'simtasini davolash. 7 (2): 147–150. doi:10.14791 / btrt.2019.7.e40. PMC 6829077. PMID 31686447.

[pmid8784065-114] Serri O, Noiseux D, Robert F, Hardy J (sentyabr 1996). "Estrogen bilan davolangan erkak va ayol transseksual bemorda laktotrof giperplaziyasi". J. klinikasi. Endokrinol. Metab. 81 (9): 3177–9. doi:10.1210 / jcem.81.9.8784065. PMID 8784065.

[pmid29688280-115] v ^d ^e ^f ^g ^h ^men ^j ^k ^l ^m ⁿ ^o ^p ^q Nota NM, Wiepjes CM, de Blok C, Gooren LJ, Peerdeman SM, Kreukels B, den Heijer M (iyul 2018). "Jinsiy aloqada gormonlarni davolash paytida transgenderlarda miyada yaxshi xulqli o'smalar paydo bo'lishi". Miya. 141 (7): 2047–2054. doi:10.1093 / miya / awy108. PMID 29688280.

[pmid9373456-116] van Kesteren PJ, Asscheman H, Megens JA, Gooren LJ (sentyabr 1997). "Jinsiy gormonlar bilan davolash qilingan transseksual sub'ektlarda o'lim va kasallanish". Klinika. Endokrinol. (Oxf). 47 (3): 337–42. doi:10.1046 / j.1365-2265.1997.2601068.x. PMID 9373456.

[pmid9562902-117] Futterweit V (1998 yil aprel). "Transseksualizmning endokrin terapiyasi va uzoq muddatli davolanishning mumkin bo'lgan asoratlari". Arch Sex Behav. 27 (2): 209–26. doi:10.1023 / A: 1018638715498. PMID 9562902.

[pmid30107028-118] McFarlane T, Zajac JD, Cheung AS (dekabr 2018). "Genderni tasdiqlovchi gormon terapiyasi va transgenderlarda jinsiy gormonga bog'liq o'smalar xavfi-Tizimli ko'rib chiqish". Klinika. Endokrinol. (Oxf). 89 (6): 700–711. doi:10.1111 / sen.13835. PMID 30107028.

[pmid20053802-119] Gonsalves AM, Sahifa P, Domigo V, Meder JF, Oppenxaym S (sentyabr 2010). "Kiproteron bilan davolash to'xtatilgandan so'ng meningioma keskin regressiyasi". AJNR Am J Neuroradiol. 31 (8): 1504–5. doi:10.3174 / ajnr.A1978. PMID 20053802.

[KnightMcDonald2013-120] Ritsar, Ema J.; McDonald, Matthew J. (2013). "Ekzogen gormondan foydalanish paytida erkakdan ayolga transgender bo'lgan odamlarda menenjiyomning takrorlanishi va rivojlanishi". Xalqaro transgenderizm jurnali. 14 (1): 18–23. doi:10.1080/15532739.2012.725563. ISSN 1553-2739.

[Razavi2014-121] Razavi, Hamid Borxey (2014). "Meningioma: estrogen-progesteron terapiyasidan keyin transeksual bemorda g'ayritabiiy o'sish". SOJ Nevrologiyasi. 1 (2). doi:10.15226/2374-6858/1/2/00109. ISSN 2374-6858.

[pmid26264069-122] v ^d ^e ^f ^g ^h ^men ^j ^k ^l ^m ⁿ Bernat AL, Oyama K, Hamdi S, Mandonnet E, Vexiau D, Pocard M, Jorj B, Froelich S (oktyabr 2015). "Siproteron asetat to'xtatilgandan keyin meningiomalarning o'sishini barqarorlashtirish va regressiyasi: 12 ta bemordan iborat seriya". Acta Neurochir (Wien). 157 (10): 1741–6. doi:10.1007 / s00701-015-2532-3. PMID 26264069.

[pmid26249273-123] v Botella C, Coll G, Lemaire JJ, Irthum B (oktyabr 2015). "Méningiomes intracrâniens et utilization prolongée d'acétate de cyprotérone à doz Conventionnelle chez la femme: à suggestions de deux cas de régression tumorale après arrêt du traitement" [Boshsuyagi ichi menenjiyomalari va kiproteron asetat ayollarda an'anaviy ravishda dozada. Davolanish bekor qilingandan so'ng o'smaning kamayishi holatlari to'g'risida hisobot]. Neyroxirurgiya (frantsuz tilida). 61 (5): 339–42. doi:10.1016 / j.neuchi.2015.05.002. PMID 26249273.

[pmid27625949-124] Sys C, Kestelyn P (2015). "Siproteron asetat bilan davolangan bemorda meningioma sabab bo'lgan bir tomonlama proptoz va ko'rlik". GMS oftalmol kasalliklari. 5: Doc05. doi:10.3205 / oc000027. PMC 5015623. PMID 27625949.

[pmid28300711-125] Kalamarides M, Peyre M (may 2017). "Progestin bilan davolashni to'xtatgandan so'ng katta menenjiyomalarning qon tomirlari kamayishi bilan dramatik qisqarish". Jahon neyroxirurgiyasi. 101: 814.e7–814.e10. doi:10.1016 / j.wneu.2017.03.013. PMID 28300711.

[pmid28545357-126] Keilani C, Abada S (2017 yil may). "Kiproteron asetat bilan davolashda tezkor induktsiya qilingan ikki tomonlama kompressiv optik neyropatiya bilan simptomatik ko'p meningiomalarning kam uchraydigan holati". Curr Drug Saf. doi:10.2174/1574886312666170523154548. PMID 28545357.

[pmid30090195-127] Bernat AL, Bonnin S, Labidi M, Aldahak N, Bresson D, Bouazza S, Froelich S (2018). "Gigant hidli truba menenjiyomining regressiyasi va siproteron asetat to'xtatilgandan so'ng ko'rish keskinligini to'liq tiklash". J Oftalmik Vis Res. 13 (3): 355–358. doi:10.4103 / jovr.jovr_21_17. PMC 6058554. PMID 30090195.

[BoerMoernaut2018-128] Bur, Mirra; Moernaut, Loes; Van Kalenberg, Frank; Lapau, Bruno; T'Sjoen, Yigit (2018). "Transjin ayolda siproteron asetatga javoban meningioma o'zgarishi". Xalqaro transgenderizm jurnali. 19 (1): 92–94. doi:10.1080/15532739.2017.1413615. ISSN 1553-2739.

[NizarSeal2018-129] Nizar, Xisham; Seal, Leyton (2018). "Menenjiyomning g'ayritabiiy sababi". Endokrin tezislar. doi:10.1530 / endoabs.59.EP75. ISSN 1479-6848.

[ChasseurBruneau2019-130] Kassir, P; Bruno, M; Corvilain, B (2019). "Siproteron asetat ishlatilgandan keyin meningioma kasalligi". Endokrin tezislar. doi:10.1530 / endoabs.64.024. ISSN 1479-6848.

[AlaladeMillward2019-131] Alalade, Endryu; Milward, Kristofer; Pal, Piyali; Gilkes, Ketrin (2019), Transgender bemorda bir nechta bosh suyagi bazasi menenjiyomasi: Case Report and Literature Review, 80, doi:10.1055 / s-0039-1679816, ISSN 2193-634X

[pmid30666456-132] Shampan PO, Passeri T, Froelich S (mart 2019). "Kiproteron asetat va nomegestrol asetatning meningioma kasalligiga gormonal ta'siri: voqea haqida hisobot". Acta Neurochir (Wien). 161 (3): 589–592. doi:10.1007 / s00701-018-03782-4. PMID 30666456.

[OwensHalliday2019-133] Ouens, Liza; Xeldeydi, Jeyn; Kerr, Richard; Franks, Stiven (2019). "Kiproteron asetatni uzoq muddat qo'llash bilan bog'liq meningioma kasalligi". Endokrin tezislar. doi:10.1530 / endoabs.62.P36. ISSN 1479-6848.

[ColstrupLarsen2020-134] Kolstrup, Xans; Larsen, Ellen D.; Mollerup, Stin; Tarp, Xanna; Soelberg, Yoqub; Rosthøj, Susanne (2020). "GnRH agonisti va siproteron asetat kombinatsiyasi bilan farmakologik ravishda kastrlangan 60 ta qamoqda o'tirgan erkak jinsiy jinoyatchilarni uzoq muddatli kuzatuvi". Sud-psixiatriya va psixologiya jurnali: 1–14. doi:10.1080/14789949.2020.1711957. ISSN 1478-9949.

[FroelichDali-Youcef2008-135] Froelich S, Dali-Youcef N, Boyer P, Kehrli P, Maitrot D, Auwerx J, Schlienger JL (2008). "Siproteron asetat ko'plab meningiomalarga yordam beradimi?". Endokrin tezislar. 16: P158. ISSN 1470-3947.

[pmid29206892-136] Peyre M, Gaillard S, de Marcellus C, Giry M, Bielle F, Villa C, Boch AL, Loiseau H, Baussart B, Cazabat L, Raffin-Sanson ML, Sanson M, Kalamarides M (mart 2018). "Meningioma mutatsion landshaftining progestin bilan bog'liq siljishi". Ann. Onkol. 29 (3): 681–686. doi:10.1093 / annonc / mdx763. PMID 29206892.

[PortetNaoufal2019-137] Portet, Sylvain; Noufal, Raniya; Tachon, Gall; Simonneau, Adrien; Chalant, Anays; Naar, Amir; Milin, Serj; Bataille, Benua; Karayan-Tapon, Lyusi (2019). "Yuqori dozali siproteron asetat ta'sirida bemorlarda ishlab chiqarilgan intrakranial menenjiyomning histo-molekulyar xarakteristikasi, antandrogen bilan davolash". Neyro-onkologiya yutuqlari. doi:10.1093 / noajnl / vdz003. ISSN 2632-2498.

[pmid11705493-138] Vasilakis-Skaramozza S, Jik H (2001 yil oktyabr). "Kiproteron yoki levonorgestrel kontratseptivlari bilan venoz tromboembolizm xavfi". Lanset. 358 (9291): 1427–9. doi:10.1016 / S0140-6736 (01) 06522-9. PMID 11705493.

[pmid14663535-139] Spitzer WO (2003 yil dekabr). "Venoz tromboembolizmi uchun xavfli omil sifatida etinilestradiol bilan siproteron asetat: epidemiologik baholash". J Obstet Gynekol mumkin. 25 (12): 1011–8. doi:10.1016 / S1701-2163 (16) 30342-5. PMID 14663535.

[pmid22027398-140] Lidegaard Ø, Nilsen LH, Skovlund CW, Skjeldestad FE, Løkkegaard E (oktyabr 2011). "Turli gestagen va estrogen dozalarini o'z ichiga olgan og'zaki kontratseptivlarni qo'llash bilan venoz tromboembolizm xavfi: Daniya kohort tadqiqotlari, 2001-9". BMJ. 343: d6423. doi:10.1136 / bmj.d6423. PMC 3202015. PMID 22027398.

[pmid24491473-141] Kromm J, Jeerakatil T (iyun 2014). "Qon tomirlari bo'lgan 23 yoshli ayolda siproteron asetat-etinil estradioldan foydalanish". CMAJ. 186 (9): 690–3. doi:10.1503 / cmaj.130579. PMC 4049993. PMID 24491473.

[pmid16112947-142] v Kuhl H (2005). "Estrogenlar va progestogenlarning farmakologiyasi: turli xil qabul qilish yo'llarining ta'siri" (PDF). Klimakterik. 8 Qo'shimcha 1: 3-63. doi:10.1080/13697130500148875. PMID 16112947.

[pmid17056444-143] Wiegratz I, Kuhl H (sentyabr 2006). "Progestogenlarning metabolik va klinik ta'siri". Eur J Contracept Reprod sog'liqni saqlash. 11 (3): 153–61. doi:10.1080/13625180600772741. PMID 17056444.

[pmid23944849-144] v ^d ^e ^f ^g ^h ^men ^j Asscheman H, T'Sjoen G, Lemaire A, Mas M, Meriggiola MC, Myuller A, Kuhn A, Dhejne C, Morel-Journel N, Gooren LJ (sentyabr 2014). "Vena tromboemboliyasi transseksual sub'ektlarni erkak va ayol o'rtasidagi jinsiy gormonlar bilan davolashning murakkabligi sifatida". Andrologiya. 46 (7): 791–5. doi:10.1111 / va.12150. PMID 23944849.

[pmid20433997-145] v Beyer-Vestendorf J, Vert S, Halbritter K, Vayss N (aprel 2010). "Erkaklarda saraton va venoz tromboembolizm xavfi". Tromb. Res. 125 Qo'shimcha 2: S155-9. doi:10.1016 / S0049-3848 (10) 70035-9. PMID 20433997.

[pmid19161930-146] Guay DR (dekabr 2008). "Kognitiv jihatdan zaiflashgan keksa odamlarda noo'rin jinsiy xatti-harakatlar". Am J Geriatr farmatsevti. 6 (5): 269–88. doi:10.1016 / j.amjopharm.2008.12.004. PMID 19161930.

[pmid17537215-147] v ^d Seaman HE, Langley SE, Farmer RD, de Vries CS (iyun 2007). "Prostata bezi saratoniga chalingan erkaklarda venoz tromboembolizm va siproteron asetat: Umumiy amaliyot tadqiqotlari bazasidan foydalangan holda o'rganish". BJU Int. 99 (6): 1398–403. doi:10.1111 / j.1464-410X.2007.06859.x. PMID 17537215.

[pmid20395174-148] Van Hemelrijck M, Adolfsson J, Garmo H, Bill-Akselson A, Bratt O, Ingelsson E, Lambe M, Stattin P, Xolmberg L (may, 2010). "Prostata bezi saratoniga chalingan erkaklarda tromboembolik kasalliklar xavfi: Shvetsiyaning PCBaSe populyatsiyasiga asoslangan natijalar". Lanset Onkol. 11 (5): 450–8. doi:10.1016 / S1470-2045 (10) 70038-3. PMC 2861771. PMID 20395174.

[pmid2462132-149] Namer M (oktyabr 1988). "Antiandrogenlarning klinik qo'llanilishi". J. Steroid biokimyosi. 31 (4B): 719-29. doi:10.1016/0022-4731(88)90023-4. PMID 2462132.

[JacobiHohenfellner1982-150] Jakobi, GR; Tunn, UW; Senge, TH (1982 yil 1-dekabr). "Ishlatilmaydigan prostata saratoni palliatsiyasi uchun siproteron asetat bilan klinik tajriba". Jakobida Gyunter H; Hohenfellner, Rudolf (tahrir). Prostata saratoni. Uilyams va Uilkins. 305-319 betlar. ISBN 978-0-683-04354-9.

[SchröderRadlmaier2009-151] v Shreder, Fritz X.; Radlmayer, Albert (2009). "Steroidal antiandrogenlar". V. Kreyg Iordaniyada; Barrington J. A. Furr (tahr.). Ko'krak va prostata saratonida gormonlarni davolash. Humana Press. 325-346 betlar. doi:10.1007/978-1-59259-152-7_15. ISBN 978-1-60761-471-5.

[pmid9854190-152] Schröder FH (1998). "Antiandrogenlar prostata saratoni uchun monoterapiya sifatida". Evropa urologiyasi. 34 Qo'shimcha 3: 12-7. doi:10.1159/000052291. PMID 9854190.

[pmid30008249-153] Beyer-Vestendorf J, Bauersachs R, Xach-Vunderl V, Zotz RB, Rott H (oktyabr 2018). "Jinsiy gormonlar va venoz tromboembolizm - kontratseptsiyadan gormonlarni almashtirish terapiyasiga qadar". VASA. 47 (6): 441–450. doi:10.1024 / 0301-1526 / a000726. PMID 30008249.

[pmid21559819-154] v DeLoughery TG (iyun 2011). "Estrogen va tromboz: tortishuvlar va sog'lom fikr". Rev Endocr Metab buzilishi. 12 (2): 77–84. doi:10.1007 / s11154-011-9178-0. PMID 21559819.

[Van_Hylckama_VliegMiddeldorp2011-155] Van Xilkama Vlieg, A .; Middeldorp, S. (2011). "Gormonlarni davolash va venoz tromboembolizm: biz hozir qayerdamiz?". Tromboz va gemostaz jurnali. 9 (2): 257–266. doi:10.1111 / j.1538-7836.2010.04148.x. ISSN 1538-7933. PMID 21114755.

[BenagianoPrimiero1983-156] Benagiano, G.; Primiero, F.M. (1983). "Uzoq muddatli kontratseptivlarning hozirgi holati". Giyohvand moddalar. 25 (6): 570–609. doi:10.2165/00003495-198325060-00003. ISSN 0012-6667. PMID 6223801.

[ManthaKarp2012-157] Manta, S .; Karp, R .; Raghavan, V .; Terrin, N .; Bauer, K. A .; Tsviker, J. I. (2012). "Faqatgina progestinli kontratseptsiya qabul qiladigan ayollarda venoz tromboembolik hodisalar xavfini baholash: meta-tahlil". BMJ. 345 (aug07 2): e4944. doi:10.1136 / bmj.e4944. ISSN 1756-1833. PMC 3413580. PMID 22872710.

[pmid29526116-158] Deyvi DA (mart 2018). "Menopozli gormon terapiyasi: yaxshiroq va xavfsiz kelajak". Klimakterik. 21 (5): 454–461. doi:10.1080/13697137.2018.1439915. PMID 29526116.

[pmid24291402-159] Stanczyk FZ, Bhavnani BR (2014 yil iyul). "Postmenopozal ayollarda gormonlarni davolash uchun medroksiprogesteron asetatdan foydalanish: bu xavfsizmi?". J. Steroid biokimyosi. Mol. Biol. 142: 30–8. doi:10.1016 / j.jsbmb.2013.11.011. PMID 24291402.

[pmid23238854-160] Stanczyk FZ, Hapgood JP, Winer S, Mishell DR (2013 yil aprel). "Postmenopozal gormon terapiyasida ishlatiladigan progestogenlar: ularning farmakologik xususiyatlari, hujayra ichidagi harakatlari va klinik ta'siridagi farqlar". Endokr. Vah. 34 (2): 171–208. doi:10.1210 / er.2012-1008. PMC 3610676. PMID 23238854.

[pmid29157280-161] Jiang Y, Tian V (noyabr 2017). "Progesteronlarning gormonlarni almashtirish terapiyasida qon lipidlariga ta'siri". Lipidlar sog'lig'i uchun disk. 16 (1): 219. doi:10.1186 / s12944-017-0612-5. PMC 5697110. PMID 29157280.

[SinghGauthier2000-162] v Singx, Shankar; Gautier, Silvain; Labrie, Fernand (2000). "Androgen retseptorlari antagonistlari (antiandrogenlar) tuzilishi-faoliyati munosabatlari". Hozirgi dorivor kimyo. 7 (2): 211–247. doi:10.2174/0929867003375371. ISSN 0929-8673. PMID 10637363. Flutamid bilan taqqoslaganda [siproteron asetat] muhim ichki androgen va estrogen ta'siriga ega. [...] Flutamid va steroidal hosilalar, siproteron asetat, xlormadinon asetat, megestrol asetat va medroksiprogesteron asetatning ta'siri in vivo jonli sichqonlarda, androgenga sezgir bo'lgan ayol sichqonlarida solishtirildi. Barcha steroidal birikmalar o'smaning o'sishini rag'batlantirgan, flutamid esa stimulyator ta'siriga ega bo'lmagan [51]. Shunday qilib, CPA o'zining ichki xususiyatlari tufayli androgenga sezgir parametrlarni va saraton o'sishini rag'batlantiradi. Kastratsiyaga qo'shilgan siproteron asetat hech qachon nazorat qilinadigan biron bir tadqiqotda prostata saratoni kasalliksiz hayotini yoki umuman omon qolish muddatini uzaytirishi hech qachon ko'rsatilmagan [152-155].

[pmid9088277-163] Newling DW (1997 yil mart). "Yaqinda Evropada o'tkazilgan klinik tadqiqotlar natijalariga ishora qilingan prostata saratoni palyatif terapiyasi". Br J Urol. 79 Qo'shimcha 1: 72-81. doi:10.1111 / j.1464-410X.1997.tb00805.x. PMID 9088277.

[pmid9592622-164] Mahler C, Verhelst J, Denis L (1998 yil may). "Antiandrogenlarning klinik farmakokinetikasi va ularning prostata saratoni samaradorligi". Farmakokinet klinikasi. 34 (5): 405–17. doi:10.2165/00003088-199834050-00005. PMID 9592622.

[pmid12603397-165] Anderson J (2003 yil mart). "Prostata bezi saratonini davolashda antiandrogen monoterapiyasining ahamiyati". BJU Int. 91 (5): 455–61. doi:10.1046 / j.1464-410X.2003.04026.x. PMID 12603397.

[Aronson2009-166] v Aronson JK (2009 yil 21 fevral). Meylerning endokrin va metabolik dorilarning yon ta'siri. Elsevier. 150-152 betlar. ISBN 978-0-08-093292-7.

[Müller2003-167] Myuller E (2003 yil 18 sentyabr). Onkologik va neyroendokrinning peptidlari va peptidlari bo'lmaganligi: asosiydan klinik tadqiqotgacha. Springer Science & Business Media. 171– betlar. ISBN 978-88-470-0295-1. Arxivlandi asl nusxasidan 2017 yil 8 sentyabrda. [CPA] koagulyatsion tizimga tegishli ta'sirlarni keltirib chiqaradi. Umumiy androgenik blokada bilan bog'liq bo'lgan so'nggi meta-tahlil shuni ko'rsatdiki, kiproteron asetat kastratsiya bilan birlashganda androgen-supressiv davolashning uzoq muddatli samaradorligini pasaytiradi. Aslida, bu asosan yurak-qon tomir asoratlari tufayli davolanish bilan bog'liq o'limning ko'payishiga olib keladi (Mualliflar yo'q, 2000).

[FurrTucker1996-168] Furr BJ, Taker H (1996 yil yanvar). "Bikalutamidning klinikadan oldingi rivojlanishi: farmakodinamikasi va ta'sir mexanizmi". Urologiya. 47 (1A Suppl): 13-25, muhokama 29-32. doi:10.1016 / S0090-4295 (96) 80003-3. PMID 8560673.

[MahlerVerhelst1998-169] Mahler C, Verhelst J, Denis L (1998 yil may). "Antiandrogenlarning klinik farmakokinetikasi va ularning prostata saratoni samaradorligi". Klinik farmakokinetikasi. 34 (5): 405–17. doi:10.2165/00003088-199834050-00005. PMID 9592622.

[Chang2005-170] Chang C (2005 yil 22 mart). Prostata saratoni: asosiy mexanizmlar va terapevtik usullar. Jahon ilmiy. 10-11 betlar. ISBN 978-981-4481-61-8. Arxivlandi asl nusxasidan 2017 yil 8 sentyabrda.

[pmid16845534-171] Gillatt D (2006 yil avgust). "Prostata saratonining mahalliy darajada rivojlangan antiandrogenli davolash usullari: barchasi bir xilmi?". J. Saraton kasalligi Klinika. Onkol. 132 Qo'shimcha 1: S17-26. doi:10.1007 / s00432-006-0133-5. PMID 16845534.

[pmid23651281-172] Sturdee DW (2013 yil avgust). "Progestinlar birlashgan HRT rejimining bir qismi sifatida haqiqatan ham zarurmi?". Klimakterik. 16 Qo'shimcha 1: 79-84. doi:10.3109/13697137.2013.803311. PMID 23651281.

[pmid31088823-173] Blok CJ, Wiepjes CM, Nota NM, van Engelen K, Adank MA, Dreijerink KM, Barbé E, Konings IR, den Heijer M (may, 2019). "Gormonlar bilan davolanayotgan transgenderlarda ko'krak bezi saratoni xavfi: Gollandiyada butun mamlakat bo'ylab kohort tadqiqotlari". BMJ. 365: l1652. doi:10.1136 / bmj.l1652. PMC 6515308. PMID 31088823.

[pmid31027551-174] Blok CJ, Dreijerink KM, den Heijer M (iyun 2019). "Transgender odamlarda saraton xavfi". Endokrinol. Metab. Klinika. Shimoliy Am. 48 (2): 441–452. doi:10.1016 / j.ecl.2019.02.005. PMID 31027551.

[pmid31343858-175] Feingold KR, Anawalt B, Boyce A, Chrousos G, Dungan K, Grossman A, Xershman JM, Kaltsas G, Koch C, Kopp P, Korbonits M, McLachlan R, Morley JE, New M, Perreault L, Purnell J, Rebar R , Singer F, Trence DL, Vinik A, Wilson DP, Nota NM, den Heijer M, Gooren LJ (2000). "Gender-disforik / jinsga mos kelmaydigan kattalarni baholash va davolash". PMID 31343858. Iqtibos jurnali talab qiladi | jurnal = (Yordam bering)

[pmid31516689-176] Ivamoto SJ, Defreyne J, Rothman MS, Van Schuylenbergh J, Van de Bruaene L, Motmans J, T'Sjoen G (2019). "Transgender ayollar uchun sog'liqqa oid masalalar va noma'lum bo'lganlar: hikoyalarni ko'rib chiqish". Ther Adv Endokrinol Metab. 10: 2042018819871166. doi:10.1177/2042018819871166. PMC 6719479. PMID 31516689.

[pmid22078182-177] Endrikat J, Gerlinger S, Richard S, Rozenbaum P, Dysterberg B (dekabr 2011). "Progestinlarning ovulyatsiyani inhibe qilish dozalari: mavjud adabiyotlarni va dunyo bo'ylab sotiladigan preparatlarni muntazam ravishda ko'rib chiqish". Kontratseptsiya. 84 (6): 549–57. doi:10.1016 / j.contraception.2011.04.009. PMID 22078182.

[pmid1838080-178] Neumann F, Kalmus J (1991). "Jinsiy kasalliklarni davolashda siproteron asetat: farmakologik asos va klinik tajriba". Muddati Klinika. Endokrinol. 98 (2): 71–80. doi:10.1055 / s-0029-1211103. PMID 1838080.

[pmid25045284-179] Ahmadi H, Daneshmand S (2014). "Prostata saratoni uchun androgenlarni yo'q qilish terapiyasi: uzoq muddatli xavfsizlik va bemorning natijalari". Bemorlarning munosabatlari natijalari. 5: 63–70. doi:10.2147 / PROM.S52788. PMC 4094624. PMID 25045284.

[pmid28667081-180] Rassell N, Cheung A, Grossmann M (avgust 2017). "Androgenlarni yo'q qilish terapiyasining salbiy ta'sirini kamaytirish uchun estradiol". Endokr. Relat. Saraton. 24 (8): R297-R313. doi:10.1530 / ERC-17-0153. PMID 28667081.

[DalesiovanTinteren2000-181] Dalesio O, van Tinteren H, Klark M, Peto R, Shreder F, Dechering I, Evans V, Godvin J, Blumenstayn B, Krouford E, Denis L, Xol R, X tepalik, Iversen P, Shipli V, Solouey M, Silvestr R (2000). "Rivojlangan prostata saratonida maksimal androgen blokadasi: randomizatsiyalangan sinovlarga umumiy nuqtai". Lanset. 355 (9214): 1491–1498. doi:10.1016 / S0140-6736 (00) 02163-2. ISSN 0140-6736.

[pmid17956709-182] Chodak G, Gomella L, Phung de H (sentyabr 2007). "Prostatitning rivojlangan saraton kasalligida estrodiol blokadasi: oldinga qarab orqaga qarab". Genitourin saratoni klinikasi. 5 (6): 371–8. doi:10.3816 / CGC.2007.n.019. PMID 17956709.

[DeLeve2013-183] v ^d DeLeve, Laurie D. (2013). "Saraton kasalligining kimyoviy terapiyasi". Giyohvand moddalarni iste'mol qiladigan jigar kasalligi. 541-567 betlar. doi:10.1016 / B978-0-12-387817-5.00030-3. ISBN 9780123878175.

[pmid25024808-184] v ^d ^e ^f Kim JH, Yoo BW, Yang VJ (may 2014). "Siproteron asetat tomonidan qo'zg'atilgan jigar etishmovchiligi: holatlar bo'yicha hisobot va adabiyotlarni o'rganish". Urol Assoc J. 8 (5-6): E458-61. doi:10.5489 / cuaj.1753. PMC 4081269. PMID 25024808.

[Savidou2006-185] v ^d ^e ^f ^g Savidou I, Deutsch M, Soultati AS, Koudouras D, Kafiri G, Dourakis SP (dekabr 2006). "Siproteron asetat tomonidan qo'zg'atilgan gepatotoksiklik: uchta holat haqida hisobot". Jahon Gastroenterologiya jurnali. 12 (46): 7551–5. doi:10.3748 / wjg.v12.i46.7551. PMC 4087608. PMID 17167851.

[pmid8977068-186] Hinkel A, Berges RR, Pannek J, Schulze H, Senge T (1996). "Prostata bezining rivojlangan saraton kasalligini davolashda siproteron asetat: 89 bemorni uzoq muddatli kuzatuvida jigar zaharliligini retrospektiv tahlil qilish". Yevro. Urol. 30 (4): 464–70. doi:10.1159/000474216. PMID 8977068.

[pmid8713486-187] v ^d Rabe T, Feldmann K, Heinemann L, Runnebaum B (yanvar 1996). "Kiproteron asetat: bu gepato- yoki genotoksikmi?". Dori xavfsizligi. 14 (1): 25–38. doi:10.2165/00002018-199614010-00004. PMID 8713486. Yaqinda Dori-darmonlarni nazorat qilish agentligi (MCA) / Dori vositalari xavfsizligi qo'mitasi (CSM) ning nashrida [5] EBMni uzoq muddat qo'llaganidan keyin jigar zaharli va dozalari bilan bog'liq spontan xabarlarga e'tibor qaratildi. [...] 96 gepatotoksik hodisa kuzatilgan (33 kishi o'limga olib kelgan), shulardan 91 tasi erkaklarda, 5 tasi ayollarda. Jigar reaktsiyalari gepatit, xolestatik sariqlik va jigar etishmovchiligini o'z ichiga olgan. Bemorlarning aksariyati prostata saratoni uchun yuqori dozada CPA (300 mg / kun) bilan davolangan.

[MCA/CSM1995-188] v ^d "Siproteron asetat bilan jigar reaktsiyalari (Kiprostat, Androkur)". Farmakologik nazoratning dolzarb muammolari (21): 1. 1995 yil fevral.

[GavaSeracchioli2017-189] Gava, Giuliya; Serakchioli, Renato; Meriggiola, Mariya Kristina (2017). "Jinsiy disforik Natal erkaklarda antiandrogenlar bilan davolash". Moyaklar endokrinologiyasi va erkaklarning ko'payishi. Endokrinologiya. 1199–1209 betlar. doi:10.1007/978-3-319-44441-3_42. ISBN 978-3-319-44440-6. ISSN 2510-1927.

[pmid26104271-190] v ^d ^e ^f ^g ^h ^men ^j ^k ^l ^m ⁿ ^o ^p ^q ^r ^s ^t ^siz ^v ^w ^x Bessone F, Lucena MI, Roma MG, Stefens C, Medina-Kaliz I, Frider B, Tsariktsian G, Ernandes N, Brugera M, Gualano G, Fassio E, Montero J, Reggiardo MV, Ferretti S, Kolombato L, Tanno F, Ferrer J, Zeno L, Tanno H, Andrade RJ (fevral 2016). "Kiproteron asetat jigarning keng spektrli shikastlanishini, shu jumladan kortikosteroidlarga ta'sir qiluvchi gepatitni keltirib chiqaradi: 22 ta holat to'g'risida hisobot". Jigar Int. 36 (2): 302–10. doi:10.1111 / liv.12899. PMID 26104271.

[Duker2016-191] Marius Dyuker (2016 yil 23-may). Mehnatga layoqatsizlik: tendentsiyalar va yangi istiqbollar. Yo'nalish. 139– betlar. ISBN 978-1-317-11767-4.

[Berlex-192] Berlex Canada, Inc. (2003-02-10). "Cyproterone acetate tabletkalari va in'ektsiyalari uchun mahsulot monografiyalari (qayta ishlangan versiyasi)" (PDF). Arxivlandi asl nusxasi (PDF) 2006-09-24 kunlari.

[193] Giyohvand moddalarga salbiy ta'sir ko'rsatishi bo'yicha maslahat qo'mitasi (2004 yil fevral). "Avstraliyadagi nojo'ya reaktsiyalar byulleteni, 23-jild, 1-son".

[pmid15015823-194] Lin AD, Chen KK, Lin AT, Chang YH, Vu HH, Kuo JY, Huang WJ, Hsu YS, Chung HJ, Chang LS (dekabr 2003). "Prostatitning rivojlangan saratonini davolashda antiandrogen bilan bog'liq gepatotoksiklik". J Chin Med dos. 66 (12): 735–40. PMID 15015823.

[pmid15604569-195] Thole Z, Manso G, Salgueiro E, Revuelta P, Hidalgo A (2004). "Antiandrogenlar tomonidan qo'zg'atilgan gepatotoksiklik: adabiyotlarni ko'rib chiqish". Urol. Int. 73 (4): 289–95. doi:10.1159/000081585. PMID 15604569.

[ChitturiFarrell2013-196] Chitturi, Shivakumar; Farrel, Geoffrey C (2013). "Gormonlar va gormon antagonistlarining jigarga salbiy ta'siri". Giyohvand moddalarni iste'mol qiladigan jigar kasalligi. 605-619 betlar. doi:10.1016 / B978-0-12-387817-5.00033-9. ISBN 9780123878175.

[pmid17845544-197] Mikel M, Soler A, Vaqué A, Ojanguren I, Kosta J, Planas R (oktyabr 2007). "Flutamid va siproteron asetatning o'zaro gepatotoksikligiga shubha qilingan". Jigar Int. 27 (8): 1144–7. doi:10.1111 / j.1478-3231.2007.01549.x. PMID 17845544.

[pmid15139499-198] Manolakopulos S, Bethanis S, Armonis A, Ekonomou M, Avgerinos A, Tsurmakliotis D (2004 yil mart). "Flutamid va siproteron asetat ketma-ket kiritilgandan so'ng toksik gepatit". Qazish. Dis. Ilmiy ish. 49 (3): 462–5. doi:10.1023 / B: DDAS.0000020504.41500.9c. PMID 15139499.

[pmid2946585-199] Meijers WH, Willemse PH, Sleijfer DT, Mulder NH, Grond J (sentyabr 1986). "Siproteron asetat bilan gepatosellular zararlanish". Eur J onkologiya klinikasi. 22 (9): 1121–2. doi:10.1016/0277-5379(86)90017-9. PMID 2946585.

[pmid2563116-200] Lévesque H, Trivalle C, Manchon ND, Vinel JP, Mur N, Hémet J, Kurtua H, Bercoff E, Bourreille J (yanvar 1989). "Tsiproteron asetat tufayli fulminant gepatit". Lanset. 1 (8631): 215–6. doi:10.1016 / S0140-6736 (89) 91225-7. PMID 2563116.

[pmid2140997-201] v Bleyk JC, Sawyerr AM, Dooley JS, Scheuer PJ, McIntyre N (may 1990). "Kiproteron asetat keltirib chiqaradigan og'ir gepatit". Ichak. 31 (5): 556–7. doi:10.1136 / gut.31.5.556. PMC 1378574. PMID 2140997. Bir nechta holatlar bo'yicha hisobotlar chop etilgan bo'lsa-da, Dori vositalari xavfsizligi qo'mitasi Buyuk Britaniyada 1988 yil noyabrgacha siproteron asetat bilan bog'liq bo'lgan jigarning salbiy reaktsiyalari to'g'risida 19 ta hisobot oldi (shaxsiy aloqa, Dori vositalari xavfsizligi qo'mitasi). Ushbu holatlarning beshtasi o'limga olib keldi.

[pmid2145371-202] Dore B, Orget J, Eroniy J, Aubert J (1990). "Hépatite après traitement par acétate de cyprotérone. A Pro d'un cas" [Siproteron asetat bilan davolashdan keyin gepatit. Ishning aproposlari]. J Urol (Parij) (frantsuz tilida). 96 (3): 169–71. ISSN 0248-0018. PMID 2145371.

[pmid1840042-203] Antoni M, Bourliere M, Tullec J, Maillot A, Botta-Fridlund D, Gautier A (1991). "Gepatit sub-fulminante d'evolution mortelle a l'acetate de cyproterone" [Kiproteron asetat keltirib chiqaradigan halokatli subfulminant gepatit]. Gastroenterol. Klinika. Biol. (frantsuz tilida). 15 (10): 772–3. ISSN 0399-8320. PMID 1840042.

[pmid1848454-204] Ohri SK, Gaer JA, Kin PF (1991 yil fevral). "Gepatotsellulyar karsinoma va siproteron asetat bilan davolash". Br J Urol. 67 (2): 213. doi:10.1111 / j.1464-410X.1991.tb15113.x. PMID 1848454.

[pmid1827039-205] v Parys BT, Hamid S, Tomson RG (1991 yil mart). "Siproteron asetat terapiyasidan so'ng og'ir gepatotsellular disfunktsiya". Br J Urol. 67 (3): 312–3. doi:10.1111 / j.1464-410X.1991.tb15142.x. PMID 1827039.

[pmid1389539-206] Drakos PE, Gez E, Katane R (1992). "Siproteron asetat tufayli gepatit". Yevro. J. Saraton. 28A (11): 1931–2. doi:10.1016 / 0959-8049 (92) 90041-Y. PMID 1389539.

[pmid1410910-207] Xassler P, Dyuchen R (1992). "Hépatotoxicité de l'acétate de cyprotérone" [siproteron asetatning gepatotoksikligi]. Rev Med Interne (frantsuz tilida). 13 (3): 245. doi:10.1016 / S0248-8663 (05) 81339-6. PMID 1410910.

[pmid8241005-208] Roila F, Crinò L, Carloni G, Natalini G (sentyabr 1993). "Kiproteron asetat: gepatotoksiklik va prostata saratoni davolash". Ann. Onkol. 4 (8): 701. doi:10.1093 / oxfordjournals.annonc.a058631. PMID 8241005.

[pmid7817350-209] Bressollette L, Dubois A, Carlhant D, Morand C, Mottier D, Riche C (1994). "Hépatite mortelle a l'acétate de cyprotérone" [Kiproteron asetat keltirib chiqaradigan o'limga olib keladigan gepatit]. Terapiya (frantsuz tilida). 49 (2): 153. PMID 7817350.

[pmid8181926-210] Xirsch D, Kovatz S, Bernxaym J, Shenkman L (mart 1994). "Fatal fulminant hepatitis from cyproterone acetate". Isr. J. Med. Ilmiy ish. 30 (3): 238–40. PMID 8181926.

[pmid8092108-211] Kattan J, Spatz A, Culine S, Terrier-Lacombe MJ, Elias D, Droz JP (October 1994). "Hepatocellular carcinoma during hormonotherapy for prostatic cancer". Am. J. klinikasi. Onkol. 17 (5): 390–2. doi:10.1097/00000421-199410000-00006. PMID 8092108.

[pmid7983963-212] v Watanabe S, Yamasaki S, Tanae A, Hibi I, Honna T (December 1994). "Three cases of hepatocellular carcinoma among cyproterone users. Ad hoc Committee on Androcur Users". Lanset. 344 (8936): 1567–8. doi:10.1016/S0140-6736(94)90373-5. PMID 7983963.

[pmid9337516-213] v ^d ^e Watanabe S, Cui Y, Tanae A, Tanaka T, Fujimoto M, Matsuo Y, Tachibana K, Yamasaki S (September 1997). "Follow-up study of children with precocious puberty treated with cyproterone acetate. Ad hoc Committee for CPA". J Epidemiol. 7 (3): 173–8. doi:10.2188/jea.7.173. PMID 9337516.

[pmid7663042-214] Pinganaud G, Chaslerie A, Bourdel Marchasson I, Decamps A, Manciet G, Emeriau JP (June 1995). "Cyproterone-induced hepatotoxicity". Ann Farmacother. 29 (6): 634. doi:10.1177/106002809502900619. PMID 7663042.

[pmid7853970-215] Rüdiger T, Beckmann J, Queisser W (February 1995). "Hepatocellular carcinoma after treatment with cyproterone acetate combined with ethinyloestradiol". Lanset. 345 (8947): 452–3. doi:10.1016/S0140-6736(95)90434-4. PMID 7853970.

[pmid8991155-216] Castellani P, Bernardini D, Renou C, Zamora C, Portal I, Gauthier A, Botta-Fridlund D (1996). "Hépatite subfulminante mortelle à l'acétate de cyprotérone. Un nouveau cas" [Fatal sub-fulminant hepatitis caused by cyproterone acetate. A new case]. Gastroenterol. Klinika. Biol. (frantsuz tilida). 20 (10): 915–6. ISSN 0399-8320. PMID 8991155.

[pmid8958378-217] Murphy BJ, Collins BJ (October 1996). "Severe hepatitis and liver failure induced by cyproterone acetate". Aust N Z J Med. 26 (5): 724. doi:10.1111/j.1445-5994.1996.tb02956.x. PMID 8958378.

[pmid9377242-218] Ruiz-Rebollo ML, Polo F, Palenzuela R, Moretó M (1997). "Hepatitis aguda severa por ciproterona" [Severe acute hepatitis due to cyproterone]. Gastroenterol gepatol (ispan tilida). 20 (7): 385. ISSN 0210-5705. PMID 9377242.

[pmid9628065-219] Lombardi A, Ferrazza P, Castaldi F, Covotta L, Tesoriere A, Urbano V, Midiri G (April 1998). "[Acute hepatic necrosis in a patient treated with cyproterone acetate]". G Chir (italyan tilida). 19 (4): 161–3. PMID 9628065.

[pmid10489919-220] v Friedman G, Lamoureux E, Sherker AH (July 1999). "Fatal fulminant hepatic failure due to cyproterone acetate". Qazish. Dis. Ilmiy ish. 44 (7): 1362–3. doi:10.1023/A:1026639432428. PMID 10489919.

[pmid10333116-221] Garty BZ, Dinari G, Gellvan A, Kauli R (May 1999). "Cirrhosis in a child with hypothalamic syndrome and central precocious puberty treated with cyproterone acetate". Yevro. J. Pediatr. 158 (5): 367–70. doi:10.1007/s004310051093. PMID 10333116.

[pmid11149080-222] Manfredi S, Lenfant L, Gresset AC, Bonnotte B, Lorcerie B, Chauffert B (November 2000). "Carcinome hépatocellulaire sur foie sain potentiellement imputable à la prise au long cours d'acétate de cyprotérone" [Hepatocellular carcinoma in a healthy liver possibly due to long-term use of cyproterone acetate]. Med-ni bosing (frantsuz tilida). 29 (36): 1983. ISSN 0755-4982. PMID 11149080.

[pmid11573856-223] Giordano N, Nardi P, Santacroce C, Geraci S, Gennari C (September 2001). "Acute hepatitis induced by cyproterone acetate". Ann Farmacother. 35 (9): 1053–5. doi:10.1177/106002800103500902. PMID 11573856.

[pmid12080237-224] Kacar S, Akdogan M, Koşar Y, Parlak E, Sasmaz N, Oguz P, Aydog G (July 2002). "Estrogen and cyproterone acetate combination-induced autoimmune hepatitis". J. klinikasi. Gastroenterol. 35 (1): 98–100. doi:10.1097/00004836-200207000-00023. PMID 12080237.

[pmid15936995-225] Famularo G, Minisola G, Grieco A, Miele L (September 2005). "Fulminant liver failure caused by cyproterone". Dig Dis Dis. 37 (9): 718–9. doi:10.1016/j.dld.2005.04.018. PMID 15936995.

[pmid17167851-226] v ^d Savidou I, Deutsch M, Soultati AS, Koudouras D, Kafiri G, Dourakis SP (December 2006). "Hepatotoxicity induced by cyproterone acetate: a report of three cases". Dunyo J. Gastroenterol. 12 (46): 7551–5. doi:10.3748/wjg.v12.i46.7551. PMC 4087608. PMID 17167851.

[pmid20038345-227] He JC, Xu P, Peng LB (December 2009). "[A case of Budd-Chiari syndrome induced by ethinylestradiol and cyproterone acetate]". Zhonghua Gan Zang Bing Za Zhi (xitoy tilida). 17 (12): 954. doi:10.3760/cma.j.issn.1007-3418.2009.12.020. ISSN 1007-3418. PMID 20038345.

[RW2011-228] "Ethinylestradiol/cyproterone. Budd-Chiari syndrome: case report". Reaksiyalar haftalik (1340): 20. February 2011. doi:10.2165/00128415-201113400-00066. ISSN 0114-9954.

[KimKim2009-229] Kim BH, Kim DJ, Sohn KM, Yang HN, Choi MJ, Lee CW, Choi KC (2009). "잠복간경변 환자에서 cyproterone acetate에 의해 발생한 전격간부전 1예" [A case of fulminant hepatic failure due to cyproterone acetate in a patient with cryptogenic liver cirrhosis]. Korean J Med. 77 (Suppl 1): S31-5. ISSN 1738-9364.

[pmid22490456-230] Hsu YC, Tai DI (2011). "Unusually high alanine aminotransferase to aspartate aminotransferase ratio in a patient with cyproterone-induced icteric hepatitis". Chang Gung Med J. 34 (6 Suppl): 34–8. PMID 22490456.

[pmid23293208-231] Abenavoli L, Milic N, Beaugrand M (2013). "Severe hepatitis induced by cyproterone acetate: role of corticosteroids. A case report". Ann Hepatol. 12 (1): 152–5. PMID 23293208.

[pmid23528173-232] Vodička M, Sálek T, Röderová E, Cerný D (2013). "Hepatotoxicita po cyproteron acetátu v léčbě karcinomu prostaty – kazuistika" [Hepatotoxicity induced by cyproterone acetate in the prostate carcinoma treatment - a case report]. Klin Onkol (chex tilida). 26 (1): 47–8. PMID 23528173.

[pmid29129412-233] Nour E, Mehdi K, Hanene J, Hammami A, Ben Slama A, Ali J (December 2017). "Fatal acute liver failure induced by cyproterone acetate: A new case". Med-ni bosing. 46 (12 Pt 1): 1231–1232. doi:10.1016/j.lpm.2017.09.003. PMID 29129412.

[MCGOPR2004-234] "High dose cyproterone and hepatotoxicity". Australian Adverse Drug Reactions Bulletin. 23 (1): 3. 2004. ISSN 1325-8540. High dose cyproterone (50mg, 100mg; Androcur, Androcur-100) is used predominantly for advanced prostate carcinoma. For the year ending June 2003, 59,000 prescriptions were dispensed for the 50mg or 100mg tablets and 97% of patients prescribed these tablets were male. [...] Over the years, ADRAC has received 105 reports implicating high-dose cyproterone. The most common adverse reactions are related to the liver with 32 reports. Other more commonly reported reactions include fatigue, dyspnoea, asthenia, confusion, depression and deep vein thrombosis. [...] All except one of the hepatic reactions involved male patients being treated for prostate cancer, whose ages ranged from 56 to 92 (median: 77) years. Time to onset of liver dysfunction ranged from 4 days to 4 years (median: 4-5 months); only 4 cases had a time to onset under a month.

[pmid16294367-235] Manso G, Thole Z, Salgueiro E, Revuelta P, Hidalgo A (April 2006). "Spontaneous reporting of hepatotoxicity associated with antiandrogens: data from the Spanish pharmacovigilance system". Farmakoepidemiol dori vositasi. 15 (4): 253–9. doi:10.1002/pds.1168. PMID 16294367.

[pmid9437555-236] "Oral contraceptives and liver cancer. Results of the Multicentre International Liver Tumor Study (MILTS)". Kontratseptsiya. 56 (5): 275–84. 1997 yil noyabr. PMID 9437555.

[pmid14558177-237] Seaman HE, de Vries CS, Farmer RD (2003). "The risk of liver disorders in women prescribed cyproterone acetate in combination with ethinyloestradiol (Dianette): a nested case-control study using the GPRD". Farmakoepidemiol dori vositasi. 12 (7): 541–50. doi:10.1002/pds.857. PMID 14558177.

[pmid20063830-238] Roe WD, Geschke K, Pease C (December 2009). "Fatal fulminant hepatitis in a chimpanzee (Pan troglodytes) receiving cyproterone acetate". J. Zoo Wildl. Med. 40 (4): 799–802. doi:10.1638/2009-0031.1. PMID 20063830.

[Trüeb2013-239] Ralph M. Trüeb (26 February 2013). Female Alopecia: Guide to Successful Management. Springer Science & Business Media. 46- bet. ISBN 978-3-642-35503-5.

[pmid2145099-240] Ramsay ID, Rushton DH (July 1990). "Reduced serum vitamin B12 levels during oral cyproterone-acetate and ethinyl-oestradiol therapy in women with diffuse androgen-dependent alopecia". Klinik va eksperimental dermatologiya. 15 (4): 277–81. doi:10.1111/j.1365-2230.1990.tb02089.x. PMID 2145099.

[SadockSadock2010-241] Sadock BJ, Sadock VA (2010). Kaplan va Sadokning "Klinik psixiatriyaning cho'ntak qo'llanmasi". Lippincott Uilyams va Uilkins. 582– betlar. ISBN 978-1-60547-264-5.

[MusisiJacobson2015-242] Musisi S, Jacobson S (14 April 2015). Brain Degeneration and Dementia in Sub-Saharan Africa. Springer. 60- betlar. ISBN 978-1-4939-2456-1.

[pmid28039596-243] Ní Mhéalóid Á, Cunniffe G (August 2017). "Optic neuritis secondary to antiandrogen therapy". Ir J Med Sci. 186 (3): 565–570. doi:10.1007/s11845-016-1544-1. PMID 28039596.

[pmid10765911-244] Grayling M, Jardine DL, McClintock AD, Spar J, Wilton GN (March 2000). "Symptomatic epidural lipomatosis following cyproterone acetate therapy". Aust N Z J Surg. 70 (3): 233–5. doi:10.1046/j.1440-1622.2000.01793.x. PMID 10765911.

[pmid24946296-245] Mohan D, Taylor R, Mackeith JA (1998). "Cyproterone acetate and striae". Klinik amaliyotda xalqaro psixiatriya jurnali. 2 (2): 147–8. doi:10.3109/13651509809115348. PMID 24946296.

[248] van der Vange N, Blankenstein MA, Kloosterboer HJ, Haspels AA, Thijssen JH (April 1990). "Effects of seven low-dose combined oral contraceptives on sex hormone binding globulin, corticosteroid binding globulin, total and free testosterone". Kontratseptsiya. 41 (4): 345–52. doi:10.1016/0010-7824(90)90034-S. PMID 2139843.

[249] Stalvey JR (July 2002). "Inhibition of 3beta-hydroxysteroid dehydrogenase-isomerase in mouse adrenal cells: a direct effect of testosterone". Ukol. 67 (8): 721–31. doi:10.1016/S0039-128X(02)00023-5. PMID 12117620.

[1]

[2]

[3]

[4]

[5]

[6]

[7]

[8]

[9]

[a]

[b]

[10]

[11]

[12]

[13]

[14]

[15]

[16]

[17]

[18]

[19]

[20]

[21]

[22]

[23]

[24]

[25]

[26]

[27]

[28]

[29]

[30]

[31]

[32]

[33]

[34]

[35]

[36]

[37]

[38]

[39]

[40]

[41]

[42]

[43]

[44]

[45]

[46]

[47]

[48]

[49]

[50]

[51]

[52]

[53]

[54]

[55]

[56]

[57]

[58]

[59]

[60]

[61]

[62]

[63]

[64]

[65]

[66]

[67]

[68]

[69]

[70]

[71]

[72]

[73]

[74]

[75]

[76]

[77]

[78]

[79]

[80]

[81]

[82]

[83]

[84]

[85]

[86]

[87]

[88]

[89]

[90]

[91]

[92]

[93]

[94]

[95]

[96]

[97]

[98]

Siproteron asetat
Mavzular	Siproteron asetatning yon ta'siri Siproteron asetat farmakologiyasi
Metabolitlar	15β-gidroksitsiproteron asetat (katta) Kiproteron (kichik) Sirka kislotasi (kichik)
Kombinatsiyalar	Estradiol valerat / siproteron asetat Etinilestradiol / siproteron asetat
Bilan bog'liq dorilar	Steroidal antiandrogenlar: Sof antiandrogenlar: Kiproteron; Antigonadotropik: Xlormadinon asetat Medroksiprogesteron asetat Megestrol asetat