Bezgakka qarshi dori - Antimalarial medication

Bezgakka qarshi dorilar yoki oddiygina bezgakka qarshi vositalar ning bir turi parazitga qarshi ko'pincha kimyoviy vosita tabiiy ravishda olingan, davolash yoki oldini olish uchun ishlatilishi mumkin bezgak, ikkinchi holda, ko'pincha ikkita sezgir maqsadli guruhga, yosh bolalarga va homilador ayollarga qaratilgan.^[1] 2018 yildan boshlab zamonaviy davolash usullari, shu jumladan og'ir bezgakni davolash, tarixan kelib chiqadigan davolash usullariga bog'liq bo'lib qoldi xinin va artesunate, ikkalasi ham parenteral (in'ektsiya yo'li bilan) giyohvand moddalar, u erdan mavjud bo'lgan zamonaviy dorilarning ko'plab sinflariga kengayib boradi.^[1] Kasallik va tarqalish darajasi ("bezgak yuki") ko'p yillar davomida global miqyosda yuqori bo'lib qolishi kutilmoqda; bezgak parazitida qarshilik ko'rsatadigan ma'lum antimalarial dorilar bir necha bor kuzatilgan, shu jumladan kombinatsiyalangan davolash usullari artemisinin, a so'nggi chora dori, hozirda Janubi-Sharqiy Osiyoda qarshilik kuzatilgan.^[1] Shunday qilib, bezgakka qarshi yangi vositalarga bo'lgan ehtiyoj va davolashning yangi strategiyalari (masalan, yangi kombinatsiyalangan davolash usullari) tropik tibbiyot.^[1] Shuningdek, ko'plab zamonaviy davolash usullarining ijobiy natijalariga qaramay, jiddiy yon effektlar standart dozalarni qabul qiladigan ba'zi bir shaxslarga ta'sir qilishi mumkin (masalan, retinopatiya bilan xlorokin, o'tkir gemolitik anemiya bilan tafenokin ).^[2]^[3]^[1]

Xususan, bezgakka qarshi dorilar uchta toifadagi odamlarda bezgakni davolash uchun ishlatilishi mumkin, (i) yuqtirilganligi shubha qilingan yoki tasdiqlangan, (ii) immunitetga ega bo'lmagan bezgak-endemik mintaqalarga tashrif buyurganlar, yuqtirishni oldini olish uchun bezgak profilaktikasi va (iii) yoki odamlarning keng guruhlarida, bezgak orqali yuqadigan hududlarda muntazam, ammo vaqti-vaqti bilan profilaktik davolanish. davriy profilaktika terapiyasi.^{[tanasida tasdiqlanmagan ]} Bezgak kasalligini davolash amaliyoti ko'pincha kontseptsiyasiga asoslangan kombinatsiyalangan davolash^{[tekshirish kerak ]} (masalan, kabi agentlardan foydalanish artemeter va lumefantrin xlorokinga chidamli Plazmodium falciparum infektsiya^{[tekshirish kerak ]}^{[iqtibos kerak ]}), chunki bu afzalliklarni o'z ichiga oladi, shu jumladan davolash etishmovchiligi xavfini kamaytiradi, rivojlangan qarshilik xavfini kamaytiradi va yon ta'sirlarni kamaytirish imkoniyatini beradi.^{[tanasida tasdiqlanmagan ]} Davolashni boshlashdan oldin bezgakka shubha qilingan barcha bemorlarda mikroskopiya yoki alternativa sifatida tezkor diagnostika testlari bilan parazitologik tasdiqlash tavsiya etiladi.^[4]^{[sahifa kerak ]} Faqatgina klinik shubha asosida davolash parazitologik tashxis qo'yish mumkin bo'lmagan hollarda ko'rib chiqiladi.^[4]^{[sahifa kerak ]}

Dori vositalari

Bezgakka qarshi vositalarni kimyoviy tuzilishi bo'yicha ko'rib chiqish maqsadga muvofiqdir, chunki bu har bir preparatning ta'sir qilish mexanizmi kabi muhim xususiyatlari bilan bog'liq.^{[iqtibos kerak ]}

Xinin va unga aloqador vositalar

Xinin uzoq tarixga ega Peru va kashfiyot cinchona hozirgi kungacha daraxt va uning qobig'idan potentsial foydalanish^{[qachon? ]} va bezgakni oldini olish va davolashda hali ham tez-tez ishlatiladigan derivativlar to'plami. Xinin an alkaloid qon kabi ishlaydi shizontitsid va kuchsiz gametotsid qarshi Plazmodium vivax va Plazmodium bezgak. Alkaloid sifatida u ovqat tarkibida to'planadi vakuolalar ning Plazmodium turlari, ayniqsa Plazmodium falciparum. Bu inhibe qilish orqali harakat qiladi gemozoin biokristallanish Shunday qilib, ning birlashishini osonlashtiradi sitotoksik heme. Xinin qon shizontitsid agenti sifatida samarasiz va toksikroqdir xlorokin; ammo, u hali ham juda samarali va og'ir og'ir holatlarni davolashda keng qo'llaniladi P. falciparum. Xlorokinga yuqori darajada qarshilik ko'rsatadigan joylarda, ayniqsa foydalidir, meflokin va sulfat preparati bilan birikmalar pirimetamin. Xinin bezgak kasalligi bo'lgan hududdan qaytib kelgan odamlarni ta'siridan keyingi davolashda ham qo'llaniladi endemik.

Xininni davolash rejimi murakkab va asosan parazitning qarshilik darajasi va dori terapiyasining sababi (ya'ni o'tkir davolash yoki profilaktika) bilan belgilanadi. The Jahon Sog'liqni saqlash tashkiloti xinin uchun tavsiya birinchi marta 20 mg / kg ni tashkil qiladi va parazitlar kininga sezgir bo'lgan har besh soatda har sakkiz soatda 10 mg / kg ni tashkil qiladi. doksisiklin, tetratsiklin yoki klindamitsin. Dozalar og'iz orqali berilishi mumkin, vena ichiga yuborish yoki mushak ichiga marshrutlar. Tavsiya etilgan usul davolanishning dolzarbligi va mavjud manbalarga bog'liq (ya'ni IV yoki IM in'ektsiyalari uchun sterilizatsiya qilingan ignalar).

Xininni qo'llash tez-tez uchraydigan sindrom bilan tavsiflanadi cinchonism. Tinnitus (eshitish qobiliyati buzilishi), toshmalar, bosh aylanishi, ko'ngil aynishi, qusish va qorin og'rig'i eng keng tarqalgan alomatlardir. Nörolojik ta'sir ba'zi holatlarda preparat tufayli yuzaga keladi neyrotoksik xususiyatlari. Ushbu harakatlar xinining ta'sirchanligini pasayishiga olib keladigan o'zaro ta'sirlari orqali amalga oshiriladi vosita neyroni so'nggi plitalar. Bu ko'pincha funktsional buzilishiga olib keladi sakkizinchi kranial asab, tartibsizlikka olib keladi, deliryum va koma. Xinin sabab bo'lishi mumkin gipoglikemiya uning rag'batlantiruvchi harakati orqali insulin sekretsiya; bu terapevtik dozalarda uchraydi va shuning uchun glyukoza miqdori har 4-6 soatda barcha bemorlarda kuzatilishi tavsiya etiladi. Homiladorlik paytida bu ta'sirni oshirib yuborish mumkin, shuning uchun dozani buyurish va nazorat qilishda qo'shimcha ehtiyotkorlik zarur. Takroriy yoki haddan tashqari dozani keltirib chiqarishi mumkin buyrak etishmovchiligi va depressiya orqali o'lim nafas olish tizimi.

Kvinimaks va xinidin bezgakni davolash yoki oldini olishda xinin bilan bog'liq bo'lgan eng ko'p ishlatiladigan ikki alkaloiddir. Kvinimaks - bu to'rtta alkaloid (xinin, xinidin, xinhoin va xinxonidin) birikmasidir. Ushbu kombinatsiya bir nechta tadkikotlarda xinindan ko'ra samaraliroq ekanligi, go'yoki to'rtta sinxona hosilalari orasidagi sinergetik ta'sir tufayli ko'rsatildi. Xinidin - xininning bevosita hosilasi. Bu distereoizomer, shuning uchun ota-ona birikmasiga o'xshash bezgakka qarshi xususiyatlarga ega. Kinidin faqat bezgakning og'ir holatlarini davolash uchun tavsiya etiladi.

Warburgning damlamasi tomonidan ishlab chiqarilgan febrifuge edi Karl Warburg 1834 yilda xinin asosiy tarkibiy qism sifatida kiritilgan. 19-asrda bu taniqli bezgakka qarshi dori edi. Dastlab maxfiy dori sifatida sotilgan bo'lsa-da, Warburgning damlamasi uni ko'plab kinoteatrlardan ustun deb bilgan taniqli tibbiyot mutaxassislari tomonidan yuqori baholangan (masalan, general-jarroh V. C. Maklin, Britaniya armiyasi tibbiyot maktabi harbiy tibbiyot professori, Netli). Warburgning damlamasi paydo bo'ldi Martindeyl: Dori haqida to'liq ma'lumot 1883 yildan taxminan 1920 yilgacha. Formulasi nashr etilgan Lanset 1875.^[5]

Xlorokin

Xlorokin yaqin vaqtgacha bezgakka qarshi eng ko'p qo'llanilgan. Bu davolashning ko'p usullari olingan asl prototip edi. Bu, shuningdek, mavjud bo'lgan barcha dorilar orasida eng arzon, eng yaxshi sinovdan o'tgan va xavfsiz hisoblanadi. Dori-darmonlarga chidamli parazitar shtammlarning paydo bo'lishi uning samaradorligini tezda pasaytiradi; ammo, u hali ham ko'pchilik tanlov birinchi qator dori hisoblanadi Saxro Afrikasi mamlakatlar. Endi uning samaradorligini oshirish uchun uni boshqa antimalarial dorilar bilan birgalikda ishlatish taklif qilinmoqda. Xlorokin fosfat (shuningdek, nivaquin deb ham ataladi) asosida mashhur dorilar xlorokin FNK, Resochin va Dawaquindir.

Xlorokin - bu 4-aminokinolon murakkab va hali ham noaniq ta'sir mexanizmi bilan birikma. Parazit vakuolalarida yuqori kontsentratsiyaga erishadi, bu esa ishqoriy tabiati tufayli ichki pH. U toksik moddalarning konversiyasini boshqaradi heme ga gemozoin inhibe qilish orqali biokristallanish ning gemozoin, shuning uchun parazitni ortiqcha toksiklik darajasi bilan zaharlaydi. U ta'sir qilishi mumkin bo'lgan boshqa potentsial mexanizmlarga parazitar biosintezga aralashish kiradi nuklein kislotalar va xlorokin-haem yoki xlorokin- hosil bo'lishiDNK murakkab. Topilgan faoliyatning eng muhim darajasi shizontslarning barcha shakllariga qarshi (xlorokinlarga chidamli bo'lgan aniq istisnolardan tashqari) P. falciparum va P. vivax shtammlari) va gametotsitlar ning P. vivax, P. bezgak, P. ovale ning pishmagan gametotsitlari kabi P. falciparum. Xlorokin ham muhim ahamiyatga ega piretikaga qarshi va yallig'lanishga qarshi davolash uchun foydalanilganda ta'sir P. vivax infektsiyalarni yuqtiradi va shu bilan qarshilik yanada kengroq bo'lgan taqdirda ham foydali bo'lib qolishi mumkin. Ilmiy va taraqqiyot tarmog'i veb-sahifasining Afrikaning Saxaradan janubiy qismida joylashgan hisobotga ko'ra, Madagaskar orolida bezgak bilan kasallangan bolalar orasida giyohvandlikka chidamlilik juda kam, ammo xloroxininga qarshi qanday dori qarshilik mavjud.

Bolalar va kattalar uch kun davomida berilgan har bir kg uchun 25 mg xlorokinni olishlari kerak. A farmakokinetik jihatdan JSST tomonidan tavsiya etilgan yuqori rejim, dastlabki dozani 10 mg / kg dan keyin 6-8 soatdan keyin 5 mg / kg, so'ngra keyingi ikki kun ichida 5 mg / kg berishni o'z ichiga oladi. Uchun kemoprofilaktika: Haftasiga 5 mg / kg (bir martalik dozada) yoki olti sutkalik dozalarga bo'lingan holda 10 mg / kg / haftada tavsiya etiladi. Xlorokin faqat a sifatida tavsiya etiladi profilaktik dori faqat ta'sirlangan hududlarda P. vivax va sezgir P. falciparum shtammlar. Xlorokin bezgakni davolashda ko'p yillar davomida ishlatilgan va yo'q abort qilish yoki teratogen bu vaqt ichida ta'siri haqida xabar berilgan; shuning uchun homiladorlik paytida foydalanish juda xavfsiz hisoblanadi. Biroq, qichishish toqat qilib bo'lmaydigan darajada paydo bo'lishi mumkin va xlorokinin provokatsion omil bo'lishi mumkin toshbaqa kasalligi.

Gidroksixloroxin

Gidroksixloroxin qo'shib 1950-yillarda olingan gidroksi guruhi mavjudga Xlorokin, uni o'zi xlorokindan ko'ra toqatli qiladi.^[6]^[7]^[8]

Amodiakvin

Amodiakvin bu xloroxinga tuzilishi va ta'sir mexanizmi jihatidan 4-aminokinolon bezgakka qarshi dori. Amodiakvin xlorokinga qarshilik ko'rsatadigan joylarda qo'llaniladi, ba'zi bemorlar xlorokinga qaraganda kamroq qichishishni keltirib chiqaradi. Amodiakvin endi artesunat bilan aralash formulada mavjud (ASAQ ) va Jahon sog'liqni saqlash tashkiloti tomonidan tavsiya etilgan artemisinin kombinatsiyalangan davolash usullari qatoriga kiradi. Sulfadoksin = pirimetamin bilan biriktirish tavsiya etilmaydi.^[4]

Preparat 25 mg / kg dan 35 mg / kg gacha bo'lgan dozalarda uch kun davomida xlorokin yuborishda ishlatiladigan usulga o'xshash usulda berilishi kerak. Noqulay reaktsiyalar, odatda, og'irligi va turi bo'yicha xlorokinni davolashda ko'rilganiga o'xshashdir. Bunga qo'chimcha, bradikardiya, qichishish, ko'ngil aynish, qusish va qorin og'rig'i qayd etilgan. Bir oz qon va jigar buzilishlar kam sonli bemorlarda ham kuzatilgan.

Pirimetamin

Pirimetamin asoratsiz bezgakni davolashda ishlatiladi. Ayniqsa, xlorokinga chidamli holatlarda foydalidir P. falciparum shtammlari bilan birlashganda sulfadoksin. Bu inhibisyon bilan harakat qiladi dihidrofolat reduktaza parazitda shunday qilib biosintezining oldini oladi purinlar va pirimidinlar, shu bilan. jarayonlarini to'xtatish DNKning replikatsiyasi, hujayraning bo'linishi va ko'payish. U birinchi navbatda eritrotsitlar fazasida shizonlarga ta'sir qiladi va hozirgi kunda faqat sulfanamid.

Proguanil

Proguanil (xloroguanid) a biguanid; pirimidinning sintetik hosilasi. U 1945 yilda Britaniyaning bezgakka qarshi tadqiqot guruhi tomonidan ishlab chiqilgan. Uning ko'plab harakat mexanizmlari bor, lekin birinchi navbatda faolga o'tish orqali vositachilik qilinadi metabolit sikloguanil. Bu bezgak dihidrofolat reduktaza fermentini inhibe qiladi. Uning eng asosiy ta'siri to'qimalarning birlamchi bosqichlariga ta'sir qiladi P. falciparum, P. vivax va P. ovale. Bu qarshi ma'lum ta'sirga ega emas gipnozitlar shuning uchun relapsning oldini olishda foydalanilmaydi. Qonda shizontitsid faolligi zaif va o'tkir infektsiyani davolash uchun tavsiya etilmaydi. Ammo bu foydali profilaktika bilan birlashtirilganda atovaquone yoki xlorokin (xlorokin qarshiligi bo'lmagan joylarda). Kuniga 3 mg / kg tavsiya etilgan dozadir (shuning uchun taxminan kattalar dozasi 200 mg ni tashkil qiladi). Dori-darmonlarning farmakokinetik profilidan shuni ko'rsatadiki, kuniga ikki marta yarim dozani saqlab turadi plazma yuqori darajadagi izchillik darajalari, shuning uchun yuqori darajadagi himoya beradi. Proguanil-xlorokin kombinatsiyasi chidamli shtammlardan samarali himoya qilmaydi P. falciparum. Proguanilning yon ta'siri juda kam, profilaktik foydalanishdan keyin vaqti-vaqti bilan ozgina soch to'kilishi va og'iz yarasi haqida xabar beriladi. Proguanil gidroxloridi sifatida sotiladi Paludrin tomonidan AstraZeneca.

Sulfonamidlar

Sulfadoksin va sulfametoksipiridazin fermentning o'ziga xos inhibitorlari dihidropteroat sintetaza bezgak parazitlarining tetrahidrofolat sintez yo'lida. Ular strukturaviy analoglari p-aminobenzoy kislota (PABA) va uning dihidrofolik kislotaga aylanishini blokirovka qilish uchun PABA bilan raqobatlashing. Sulfonamidlar eritrotsitlar (jinssiz) tsiklining shizont bosqichlarida harakat qiladi. Sulfanilamidlar yolg'iz yuborilganda bezgakni davolashda samarali emas, ammo antifolat bilan birgalikda qabul qilish pirimetamin, odatda, belgilangan dozada sulfadoksin-pirimetamin (Fansidar ) ishlab chiqaradi sinergik bezgakning sezgir shtammlarini davolash uchun etarli ta'sir.

Sulfanilamidlar kamdan-kam, ammo og'ir teri reaktsiyalari tufayli kemoprofilaktikada tavsiya etilmaydi. Ammo u kasallikning klinik epizodlari uchun tez-tez ishlatiladi.

Meflokin

Meflokin davomida ishlab chiqilgan Vetnam urushi va xinin bilan kimyoviy jihatdan bog'liqdir. U Amerika qo'shinlarini qarshi himoya qilish uchun ishlab chiqilgan ko'p dori-darmonlarga chidamli P. falciparum. Bu uzoq vaqt davomida juda kuchli qonli shizontitsid yarim hayot. Parazit oziq-ovqat vakuolalariga zarar etkazadigan toksik gem komplekslarini hosil qilish orqali harakat qiladi deb o'ylashadi. Meflokin samarali hisoblanadi profilaktika va o'tkir terapiya uchun. Endi u faqat chidamli shtammlarning oldini olish uchun ishlatiladi P. falciparum (odatda bilan birlashtiriladi Artesunate ) qarshi samarali bo'lishiga qaramay P. vivax, P. ovale va P. marlariae. Xlorokin / proguanil yoki sulfadagi dori-pirimetamin kombinatsiyalaridan boshqa barcha plazmodiya infektsiyalarida foydalanish kerak.

Meflokinga asoslangan bezgakni davolashning yirik tijorat ishlab chiqaruvchisi - bu dorini savdo nomi ostida sotadigan Roche Pharmaceuticals "Lariam ". Lariam har bir planshet uchun taxminan uch evroga qimmat (2000 yildagi narxlar).

Meflokin qarshiligining tarqalishiga qarab, 15-25 mg / kg dozani tavsiya etiladi. Dozaning ko'payishi, ayniqsa kichik yoshdagi bolalarda toqat qilmaslik darajasining yuqori darajasi bilan bog'liq; gijjalar va ezofagit. Birinchi trimestrda foydalanish tavsiya etilmagan, garchi ikkinchi va uchinchi trimestrlarda xavfsiz deb hisoblansa; Shunga qaramay, 2011 yil oktyabr oyida Kasalliklarni nazorat qilish va profilaktika markazlari (CDC) barcha trimestrlarda bezgakni profilaktika qilish va davolash uchun meflokinni o'z tavsiyasini o'zgartirdi va ma'qulladi, oziq-ovqat va farmatsevtika idorasi (FDA) o'z toifasini C dan o'zgartirdi. B. Mefloxin ko'pincha ko'ngil aynish, qusish, diareya, qorin og'rig'i va bosh aylanishini o'z ichiga olgan nojo'ya ta'sirlarni keltirib chiqaradi. Nevrologik hodisalar bilan bir nechta uyushmalar, ya'ni ta'sirchan va tashvishlanish buzilishi, gallyutsinatsiyalar, uyquning buzilishi, psixoz, toksik ensefalopatiya, konvulsiyalar va deliryum. Yurak-qon tomir effektlari bradikardiya bilan qayd etilgan va sinus aritmiyasi meflokin bilan davolangan bemorlarning 68 foizida doimiy ravishda qayd etilmoqda (bitta kasalxonada o'tkazilgan tadqiqotda).

Mefloxinni faqat olti oygacha bo'lgan muddat davomida nojo'ya ta'sirlari tufayli ichish mumkin. Shundan so'ng, boshqa dorilarni (masalan, paludrin / nivaquinga asoslangan preparatlarni) yana ichish kerak.^[9]^{[tibbiy ma'lumotnoma kerak ]}

Atovakuone

Atovakuone nomi ostida proguanil bilan birgalikda mavjud Bezgak, dan yuqori narxda bo'lsa ham Lariam. Bu odatda ishlatiladi profilaktika sayohatchilar tomonidan va rivojlangan mamlakatlarda falciparum bezgak kasalligini davolash uchun ishlatilgan. Atovakuonning suyuq og'iz suspenziyasi Mepron nomi ostida mavjud.

Primakvin

Primakvin qarshi faol bo'lgan juda faol 8-aminokinolon P. falcipaum gametotsitlar, shuningdek, qon oqimidagi merozoitlarga va gipnozitlarga, uxlab yotgan jigar shakllariga ham ta'sir qiladi. P. vivax va P. ovale.^[10] Bu bezgakning qaytalanuvchi infektsiyalarini va o'tkir holatlarni davolash uchun yagona ma'lum dori. Ta'sir mexanizmi to'liq tushunilmagan, ammo plazmodiyadagi oksidlanish metabolizmini blokirovka qiladi deb o'ylashadi. Bundan tashqari, u metilen ko'k bilan birlashtirilishi mumkin.^[11]

In relapsning oldini olish uchun P. vivax va P. ovale 0,15 mg / kg 14 kun davomida berilishi kerak. Gametotsitotsid dori sifatida P. falciparum infektsiyalar, etti kundan keyin takrorlangan 0,75 mg / kg bitta dozasi etarli. Ushbu davolash usuli faqat boshqa samarali qonli shizontitsid preparati bilan birgalikda qo'llaniladi. Kam miqdordagi nojo'ya ta'sirlar mavjud, ammo primakinning sabab bo'lishi mumkinligi ko'rsatilgan anoreksiya, ko'ngil aynishi, qusish, kramplar, ko'krak qafasidagi zaiflik, anemiya, ba'zi bir bostirish miyeloid faoliyat va qorin og'rig'i. Dozani oshirib yuborish holatlarida granulotsitopeniya sodir bo'lishi mumkin.^{[iqtibos kerak ]}

Artemisinin va hosilalari

Artemisinin bu xitoylik o'simlik (qinghaosu 1000 yildan ortiq vaqt davomida isitmani davolashda ishlatilgan,^[12] Shunday qilib, g'arbiy dunyoda Xininni ishlatishdan oldin. Bu o'simlikdan olingan Artemisia annua, bezgakni davolashda muvaffaqiyatli terapevtik vosita sifatida birinchi hujjatlar bilan milodiy 340 yilda Ge Xong uning kitobida Chjou Xou Bey Dji Fang (Favqulodda vaziyatlar uchun retseptlar bo'yicha qo'llanma).^[13] Ge Hong artemesini oddiy yordamida qazib oldi mo''tadil, va ushbu usul bugungi kunda ham qo'llanilmoqda.^[14] Faol birikma birinchi bo'lib 1971 yilda ajratilgan va artemisinin deb nomlangan. Bu sesquiterpen laktoni kimyoviy jihatdan kam uchraydigan peroksidli ko'prik aloqasi bilan.^{[iqtibos kerak ]} Bu^{[tushuntirish kerak ]} parazit ichidagi nishon munozarali bo'lib qolishiga qaramay, bezgakka qarshi ta'sirining aksariyat qismi uchun javobgar deb hisoblanadi.^{[kimga ko'ra? ]} Ayni vaqtda^{[qachon? ]} u JSST ko'rsatmalariga muvofiq qat'iy nazorat qilinadi, chunki u ko'p dori-darmonlarga chidamli bo'lgan barcha turlarga qarshi samarali ekanligi isbotlangan P. falciparumShunday qilib, qarshilikni rivojlantirish bilan bog'liq boshqa xatti-harakatlar bilan birgalikda muvofiqlik va rioya qilishni ta'minlash uchun har qanday g'amxo'rlik ko'rsatiladi.^{[iqtibos kerak ]} Shuningdek, u boshqa bezgakka qarshi vositalar bilan birgalikda beriladi.^{[iqtibos kerak ]}

Artemisinin juda tez ta'sirga ega va davolangan o'tkir bemorlarning aksariyati davolanishdan keyin 1-3 kun ichida sezilarli yaxshilanishni ko'rsatmoqda.^{[iqtibos kerak ]} Ayni paytda u bezgakka qarshi barcha vositalardan eng tezkor tozalanishini namoyish etdi^{[qachon? ]} ishlatilgan va birinchi navbatda trofozit fazasiga ta'sir qiladi, shu bilan kasallikning rivojlanishini oldini oladi.^{[iqtibos kerak ]} Yarim sintetik artemisinin hosilalarini (masalan, artesunat, artemeter) ota-ona birikmasiga qaraganda ishlatish osonroq va tanada bir marta faol dihidroartemasining birikmasiga aylanadi.^{[iqtibos kerak ]} Davolashning birinchi kunida ko'pincha 20 mg / kg beriladi, so'ngra keyingi olti kun davomida dozasi kuniga 10 mg / kg gacha kamayadi.^{[iqtibos kerak ]} Kam sonli yon ta'sirlar artemesinin foydalanish bilan bog'liq.^{[iqtibos kerak ]} Shu bilan birga, bosh og'rig'i, ko'ngil aynishi, qusish, g'ayritabiiy qon ketish, siydikning quyuqlashishi, qichishish va boshqalar dori isitmasi oz sonli bemorlar tomonidan xabar qilingan.^{[iqtibos kerak ]} Klinik tekshiruv paytida ba'zi bir yurak o'zgarishlari, xususan, o'ziga xos bo'lmagan ST o'zgarishlari va birinchi daraja haqida xabar berilgan atrioventrikulyar blok (bemorlar bezgak bezgagidan xalos bo'lganda bular g'oyib bo'ldi).^{[iqtibos kerak ]}
Artemether a metil efir dihidroartemesinin hosilasi. Ta'sir uslubi jihatidan artemesiga o'xshaydi, ammo gipnozoititsidli birikma sifatida qobiliyatini pasaytiradi, aksincha gametotsitlar tashilishini kamaytirish uchun sezilarli ta'sir ko'rsatadi. Qarshilik rivojlanishiga yo'l qo'ymaslik uchun artemesidagi kabi o'xshash cheklovlar mavjud, shuning uchun u faqat dori-darmonlarga chidamli og'ir o'tkir holatlarda kombinatsiyalangan davolashda qo'llaniladi P. falciparum. Uni 7 kunlik kursda uch kun davomida kuniga 4 mg / kg, so'ngra uch kun davomida 1,6 mg / kg bilan berish kerak. Preparatning nojo'ya ta'siri kam, ammo yuqori dozalar berilsa, potentsial neyrotoksikani rivojlantiradi.^{[iqtibos kerak ]}
Artesunate a gemisuksinat faol metabolit dihidroartemizinning hosilasi. Hozirda^{[qachon? ]} bu artemesinin tipidagi barcha dorilar orasida eng ko'p ishlatiladigan dori. Uning yagona ta'siri gametotsitlar uzatilishini kamaytirish orqali amalga oshiriladi. U kombinatsiyalangan terapiyada qo'llaniladi va asoratlanmagan hollarda samarali bo'ladi P. falciparum. JSST tomonidan tavsiya etilgan doz besh-etti kunlik (taxmin qilingan rioya darajasiga qarab) 4 mg / kg uch kun davomida (odatda meflokin bilan birgalikda beriladi), so'ngra qolgan ikki yoki to'rt kun davomida 2 mg / kg ni tashkil qiladi. . Tailandda 10000 dan ortiq bemorlarda o'tkazilgan katta tadqiqotlarda nojo'ya ta'sir ko'rsatilmagan.^{[iqtibos kerak ]}
Dihidroartemisinin artemesinin kamaytiriladigan faol metabolitidir. Bu eng samarali artemesinin birikmasi va eng kami barqaror. U kuchli qonli shizontitsid ta'siriga ega va gametotsitlarning tarqalishini kamaytiradi. Bu chidamli va asoratlanmagan holatlarni terapevtik davolash uchun ishlatiladi P. falciparum. Terapiyaning birinchi kunida 4 mg / kg dozadan keyin olti kun davomida 2 mg / kg dan tavsiya etiladi. Artesunate singari, davolanish uchun hech qanday nojo'ya ta'sirlar hozirgacha qayd etilmagan.^{[iqtibos kerak ]}
Arteether bu etil efir dihidroartemisinin hosilasi. Bu murakkab bo'lmagan chidamli holatlar uchun kombinatsiyalangan terapiyada qo'llaniladi P. falciparum. Tavsiya etilgan doz - IM in'ektsiyalari bilan uch kun davomida kuniga 150 mg / kg. Quyidagi neyrotoksikatsiyani ko'rsatadigan oz sonli holatlar bundan mustasno parenteral administratsiyasi nojo'ya ta'sirlari qayd etilmagan.^{[iqtibos kerak ]}

Halofantrin

Halofantrin tomonidan ishlab chiqarilgan nisbatan yangi dori Valter Rid armiyasi tadqiqot instituti 1960-yillarda. Bu fenantren metanol, kimyoviy xinin bilan bog'liq va qon shizontitsid vazifasini bajaruvchiga ta'sir qiladi Plazmodium parazitlar. Uning ta'sir mexanizmi boshqa bezgakka qarshi vositalarga o'xshaydi. Sitotoksik komplekslar hosil bo'ladi ferritoporfirin XI plazmodial membranani shikastlanishiga olib keladi. Dori-darmonlarga chidamli parazitlarga qarshi samarali bo'lishiga qaramay, halofantrin bezgakni davolashda (profilaktik yoki terapevtik) yuqori narxga ega bo'lganligi sababli keng qo'llanilmaydi. Bu juda o'zgaruvchan bioavailabilityga ega va potentsial yuqori darajalarga ega ekanligi ko'rsatilgan kardiotoksiklik. U hali ham foydali dori bo'lib, uni yurak xastaligi yo'qligi ma'lum bo'lgan va o'tkir bezgakning og'ir va chidamli shakllari bilan og'rigan bemorlarda qo'llash mumkin. Halofantrin asosidagi mashhur dori - Halfan. Hukumat nazorati darajasi va uni ishlatish mumkin bo'lgan retsept bo'yicha asos xarajatlarga yordam beradi, shuning uchun halofantrin tez-tez ishlatilmaydi.

8 mg / kg halofantrin dozasini klinik epizod davomiyligi davomida olti soatlik interval bilan uch dozada berish tavsiya etiladi. 10 kilogrammgacha bo'lgan bolalar uchun foydalanishni qo'llab-quvvatlovchi va yaxshi muhosaba qilinganligini ko'rsatadigan ma'lumotlarga qaramay tavsiya etilmaydi. Eng tez-tez uchraydigan nojo'ya ta'sirlarga ko'ngil aynish, qorin og'rig'i, diareya va qichishish kiradi. Og'ir qorincha buzilishi, vaqti-vaqti bilan o'limga olib keladigan yuqori dozalar kiritilganda kuzatiladi. Buning sababi QTc oralig'ini uzaytirish. Halofantrinni homiladorlik va laktatsiya davrida, kichik bolalarda yoki ilgari meflokin qabul qilgan bemorlarda qo'llash tavsiya etilmaydi.

Lumefantrin

Lumefantrin ba'zi bir kombinatsiyalangan antimalarial rejimlarda ishlatiladigan halofantrinning qarindoshi.^[15]

Doksisiklin

Ehtimol, nisbiy samaradorligi va arzonligi sababli, buyurilgan antimalarial dorilarning biri, doksisiklin a tetratsiklin dan olingan birikma oksitratsiklin. Tetratsiklinlar ishlab chiqarilgan antibiotiklarning dastlabki guruhlaridan biri bo'lgan va hozirgacha ko'plab infektsiyalarda keng qo'llanilmoqda. Bu bakteriostatik jarayonini inhibe qiluvchi vosita oqsil sintezi ga bog'lash orqali 30S ribosomal subunit shunday qilib 50 va 30-yillarning birlashishini oldini oladi. Doksisiklin asosan ishlatiladi kemoprofilaktika xlorokin qarshilik mavjud bo'lgan joylarda. Shuningdek, uni xinin bilan birgalikda, chidamli holatlarni davolash uchun ishlatish mumkin P. falciparum ammo o'tkir bezgakda juda sekin harakatga ega va monoterapiya sifatida ishlatilmasligi kerak.

O'tkir holatlarni davolashda va xinin bilan birgalikda berilganda; Etti kun davomida kuniga 100 mg doksisiklin berilishi kerak. Profilaktik terapiyada har kuni bezgak ta'sirida 100 mg (kattalar dozasi) doksisiklin berilishi kerak.

Eng tez-tez uchraydigan nojo'ya ta'sirlar doimiydir emal gipoplaziyasi, suyak o'sishining vaqtinchalik depressiyasi, oshqozon-ichak traktining buzilishi va ba'zi bir ko'tarilgan darajalar fotosensitivlik. Suyak va tish o'sishining ta'siri tufayli u 8 yoshgacha bo'lgan bolalar, homilador yoki emizikli ayollar va jigar funktsiyasi buzilishi ma'lum bo'lganlarda qo'llanilmaydi.

Tetratsiklin faqat o'tkir holatlarni davolash uchun birgalikda qo'llaniladi P. falciparum infektsiyalar. Bu uning sekin boshlanishi bilan bog'liq. Doksisiklindan farqli o'laroq, u ximoprofilaktikada ishlatilmaydi. Tetratsiklin uchun 250 mg kattalar uchun tavsiya etilgan dozadir (uni bolalarda qo'llash mumkin emas), kutilgan rioya va muvofiqlik darajasiga qarab besh yoki etti kun davomida. Qizilo'ngach oshqozon yarasi, oshqozon-ichak trakti va jarayonga aralashish suyaklanish va suyak o'sishining tushkunligi paydo bo'lishi ma'lum. Doksisiklin bilan bog'liq yon ta'sirlarning aksariyati tajribaga ega.

Klindamitsin

Klindamitsin ning lotinidir Linkomitsin, qon shizontitsidlariga qarshi sekin harakat bilan. Bu faqat chidamli o'tkir holatlarni davolashda xinin bilan birgalikda qo'llaniladi P. falciparum infektsiyalar va profilaktika sifatida emas. Boshqa antibiotik alternativalariga qaraganda toksikroq bo'lib, u faqat Tetratsiklinlar kontrendikatsiyalangan hollarda qo'llaniladi (masalan, bolalarda).

Klindamitsin xinin bilan birgalikda kuniga to'rt marta 300 mg dozada (kattalarda) besh kun davomida berilishi kerak. Klindamitsinni qabul qilgan bemorlarda qayd etilgan yagona nojo'ya ta'sirlar bu ko'ngil aynish, qusish va qorin og'rig'i va kramplardir. Ammo bu preparatni qabul qilishda ko'p miqdorda suv va oziq-ovqat iste'mol qilish orqali ularni engillashtirishi mumkin. Psevdomembranoz kolit (sabab bo'lgan Clostridium difficile ) ba'zi bemorlarda ham rivojlangan; bu holat ozgina hollarda o'limga olib kelishi mumkin.

Qarshilik

Bezgakka qarshi dorilarga qarshilik quyidagicha ta'riflangan: "parazitning odatda tavsiya etilgan dozalarga teng yoki undan yuqori bo'lgan dozalarda berilganiga qaramay, qabul qilinganligi va so'rilganiga qaramay parazitning omon qolish va / yoki ko'payish qobiliyati, ammo sub'ektning bag'rikengligi doirasida. Ko'rib chiqilayotgan preparat kirish huquqiga ega bo'lishi kerak. parazitga yoki yuqtirilgan qizil qon hujayralariga uning normal harakatlari uchun zarur bo'lgan vaqt davomida. "^{[Ushbu taklifga iqtibos keltirish kerak ]} Bezgakka qarshi dorilarga qarshilik keng tarqalgan.^[16]Ko'pgina hollarda, bu kuzatilgan davolanishdan kelib chiqadigan parazitlarga tegishli; shuning uchun u bezgakka qarshi profilaktika muvaffaqiyatsiz tugagan barcha holatlarni istisno qiladi.^{[iqtibos kerak ]} Ishni chidamli deb aniqlash uchun, ko'rib chiqilayotgan bemor ma'lum va kuzatilgan bezgakka qarshi terapiyani olgan bo'lishi kerak, shu bilan birga qon preparati va metabolit konsentratsiyasini kuzatib borish kerak; buni namoyish qilish uchun ishlatiladigan texnikani o'z ichiga oladi jonli ravishda, in vitrova hayvon modeli sinov va yaqinda ishlab chiqilgan molekulyar texnikalar.^{[iqtibos kerak ]}

Dori-darmonlarga chidamli parazitlar ko'pincha bezgakni davolashda muvaffaqiyatsizlikni tushuntirish uchun ishlatiladi. Biroq, ular ikkita potentsial jihatdan juda boshqacha klinik stsenariydir. Tozalash amalga oshmadi parazitemiya va tegishli davo tayinlanganda o'tkir klinik epizoddan qutulish bezgakka qarshi chidamlilikning asl shaklida. Giyohvand moddalarga chidamliligi davolashning muvaffaqiyatsiz bo'lishiga olib kelishi mumkin, ammo davolanish muvaffaqiyatsiz bo'lishiga, dori vositalarining rivojlanishiga yordam berishiga qaramay, qarshilik ko'rsatish sabab bo'lmaydi. Jarayonlarda ko'plab omillar ishtirok etishi mumkin, ular mos kelmaslik va rioya qilish bilan bog'liq muammolar, dori sifatining pastligi, boshqa farmatsevtika bilan o'zaro aloqalar, yomon emilim, noto'g'ri tashxis va noto'g'ri dozalar. Ushbu omillarning aksariyati, shuningdek, giyohvandlikka chidamliligini rivojlanishiga yordam beradi.

Qarshilik avlodi murakkab bo'lishi mumkin va ular orasida o'zgarib turadi Plazmodium turlari. Asosan a orqali boshlash odatda qabul qilinadi spontan mutatsiya bu ba'zi beradi evolyutsion foyda, shuning uchun bezgakka qarshi ishlatiladigan sezgirlikning pasaytirilgan darajasini beradi. Bunga bitta sabab bo'lishi mumkin nuqta mutatsiyasi yoki bir nechta mutatsiyalar. Ko'pgina hollarda mutatsiya parazit uchun o'limga olib keladi yoki dori bosimi sezgir bo'lib qolgan parazitlarni olib tashlaydi, ammo ba'zi chidamli parazitlar omon qoladi. Qarshilik uzoq vaqt davomida mavjud bo'lgan parazit populyatsiyasi ichida mustahkam o'rnashishi mumkin.

E'tirof etilgan birinchi turdagi qarshilik 1957 yilda Tailandda xloroxin bo'lgan. Ushbu qarshilik ortidagi biologik mexanizm keyinchalik xlorokinni parazitdan chiqarib yuboradigan oqim jarayonining rivojlanishi bilan bog'liq bo'lib, jarayonni samarali ravishda inhibe qilish uchun zarur bo'lgan darajadan oldin tan olingan. gem polimerizatsiyasi (bu gemoglobinni hazm qilish natijasida hosil bo'lgan toksik yon mahsulotlarning ko'payishini oldini olish uchun zarur). Ushbu nazariya oqimni to'xtatadigan moddalar qo'shilishi bilan qarshilikni samarali ravishda qaytarish mumkinligini ko'rsatadigan dalillar bilan tasdiqlangan. Aminodiakin, mefloxin, halofantrin va xinin kabi boshqa kinolon bezgakka qarshi vositalarning qarshiligi ham shu kabi mexanizmlar bilan sodir bo'lgan deb o'ylashadi.

Plazmodium qarshi qarshilikni rivojlantirdilar antifolat kombinatsiyalangan dorilar, eng ko'p ishlatiladigan sulfadoksin va pirimetamin. Ikki gen mutatsiyasi mas'ul deb hisoblanib, unda ishtirok etgan ikkita fermentning sinergetik bloklanishiga imkon beradi folat sintez. Muayyan mutatsiyalarning mintaqaviy o'zgarishlari har xil qarshilik darajalarini beradi.

Atovakuone faqat boshqa bezgakka qarshi birikma bilan birgalikda foydalanish tavsiya etiladi, chunki chidamli parazitlarning tanlanishi mono-terapiyada qo'llanganda juda tez sodir bo'ladi. Qarshilik sitoxrom-b uchun genlarni kodlashda bir nuqtali mutatsiyadan kelib chiqadi deb o'ylashadi.

Qarshilik tarqalishi

Giyohvand moddalarga chidamliligining tarqalishiga eng katta ta'sir ko'rsatadigan yagona omil yo'q, ammo o'sish bilan bog'liq bir qator ishonchli sabablar tan olingan. Bularga iqtisodiyot, odamlarning xulq-atvori, farmakokinetikasi va biologiyasi kabi jihatlar kiradi vektorlar va parazitlar.

Eng ta'sirli sabablar quyida ko'rib chiqiladi:

Biologik ta'sirlar parazitlarning bezgakka qarshi mavjudligidan omon qolish qobiliyatiga asoslangan bo'lib, qarshilikning davomiyligini va davolanishga qaramasdan keyingi yuqish imkoniyatini beradi. Oddiy sharoitlarda davolanishdan keyin davom etadigan har qanday parazitlar mezbonning immun tizimi tomonidan yo'q qilinadi, shuning uchun parazitlarni yo'q qilishni kamaytiradigan har qanday omillar qarshilikning rivojlanishiga yordam berishi mumkin. Bu bilan bog'liq bo'lgan kambag'al javobni tushuntirishga urinishlar immunitet tanqisligi jismoniy shaxslar, homilador ayollar va yosh bolalar.
Ba'zi parazit-vektor birikmalarining muqobil ravishda chidamli parazitlarning tarqalishini kuchaytirishi yoki inhibe qilishi mumkinligi va qarshilikning "cho'ntakka o'xshash" maydonlarini keltirib chiqarishi mumkinligi haqida dalillar mavjud.
Shunga o'xshash asosiy kimyoviy birikmalardan ishlab chiqarilgan bezgakka qarshi vositalardan foydalanish qarshilik rivojlanish tezligini oshirishi mumkin, masalan xlorokin va amiodiakuinga, ikkita 4-aminokinolonlar va xofin va halofantringa qarshilik ko'rsatadigan meflokinlarga o'zaro qarshilik. Ushbu hodisa keng miqyosda foydalanishdan oldin yangi ishlab chiqilgan davolash usullarining foydasini kamaytirishi mumkin.
Bezgakka qarshi chidamliligi ba'zi turlarida uchraydigan jarayon bilan kuchayishi mumkin Plazmodium, bu erda daraja fenotipik plastika namoyish etildi, bu preparat ilgari tajribaga ega bo'lmagan bo'lsa ham, yangi dori-darmonga qarshilikning tez rivojlanishiga imkon berdi.
Tanlangan bezgakka qarshi vositaning farmakokinetikasi asosiy hisoblanadi; tez metabolizmga uchragan preparat bo'yicha uzoq umrni tanlash qarori murakkab va hanuzgacha noaniq bo'lib qolmoqda. Yarim umr ko'rish muddati pastroq bo'lgan dorilar to'g'ri plazmadagi konsentratsiyani saqlab qolish uchun tez-tez yuborishni talab qiladi, shuning uchun agar rioya qilish va muvofiqlik darajasi ishonchsiz bo'lsa, ko'proq muammolarni keltirib chiqarishi mumkin, ammo uzoqroq davom etadigan preparatlar uzoq muddatli past konsentratsiyasi tufayli qarshilik rivojlanishini oshirishi mumkin. .
Bezgakka qarshi vositalarning farmakokinetikasi kombinatsiyalangan terapiyani qo'llashda muhim ahamiyatga ega. Uyg'un bo'lmagan dori kombinatsiyalari, masalan, bitta dori ustun bo'lgan "himoya qilinmagan" davrga chidamli parazitlarni tanlash ehtimolini jiddiy ravishda oshirishi mumkin.
Ekologik jihatdan translyatsiya darajasi va qarshilikning rivojlanishi o'rtasida bog'liqlik mavjud, ammo hozirgi paytda bu hali ham noaniqligicha qolmoqda.
Belgilangan davolash rejimi qarshilik rivojlanishiga katta ta'sir ko'rsatishi mumkin. Bu preparatni qabul qilish, kombinatsiyasi va o'zaro ta'sirini, shuningdek preparatning farmakokinetik va dinamik xususiyatlarini o'z ichiga olishi mumkin.

Oldini olish

Bezgakka qarshi dori qarshiligining oldini olish juda katta xalq salomatligi ahamiyati. Hozirgi vaqtda terapiya yo'q deb taxmin qilish mumkin^{[qachon? ]} yaqin kelajakda ishlab chiqilayotgan yoki ishlab chiqariladigan bezgak kasalligidan butunlay himoya qiladi. Shunga muvofiq, ishlab chiqilgan har qanday terapiyaga qarshilik ko'rsatish ehtimoli mavjud. Bu jiddiy tashvish tug'diradi, chunki yangi dori-darmonlarni ishlab chiqarish darajasi qarshilikning rivojlanish darajasiga to'g'ri kelmaydi. Bundan tashqari, eng yangi ishlab chiqilgan terapevtik vositalar dunyodagi eng qashshoq hududlar tomonidan eng qimmatga talab qilinadi va eng ko'p miqdorda talab qilinadi. Shu sababli, bezgakka qarshi kurashish darajasi qarshilikning har qanday rivojlanishini iloji boricha cheklash uchun mavjud dori vositalaridan ehtiyotkorlik bilan foydalanishga bog'liq ekanligi aniq.

Ushbu jarayon uchun muhim qoidalar tez tibbiy yordamni ko'rsatishni o'z ichiga oladi, bu erda xodimlar yaxshi o'qitiladi va samarali davolanish uchun zarur materiallar bilan ta'minlanadi. Bu o'z-o'zidan bezgak kasalligi keng tarqalgan hududlarda etarli emas, shuning uchun dastlabki muammoni keltirib chiqaradi. Tavsiya etilgan usullardan biri, ayrim mamlakatlarning sog'liqni saqlash tizimidagi etishmovchilikni oldini olishga qaratilgan infratuzilma bu ba'zi sohalarni xususiylashtirishdir, shu bilan dori vositalarini sog'liqni saqlash sohasi bilan rasman bog'liq bo'lmagan manbalardan ochiq bozorda sotib olishga imkon beradi. Garchi bu hozirda biron bir qo'llab-quvvatlanayotgan bo'lsa-da, cheklangan kirish va giyohvand moddalarni noto'g'ri ishlatish bilan bog'liq ko'plab muammolar mavjud, bu esa qarshilik rivojlanish tezligini yanada oshirishi mumkin.

Qarshilik tarqalishining oldini olish uchun ikkita umumiy yondashuv mavjud: bezgak infektsiyalarining oldini olish, and preventing the transmission of resistant parasites.

Preventing malaria infections developing has a substantial effect on the potential rate of development of resistance, by directly reducing the number of cases of malaria thus decreasing the need for anti-malarial therapy.Preventing the transmission of resistant parasites limits the risk of resistant malarial infections becoming endemic and can be controlled by a variety of non-medical methods including hasharotlar - davolangan to'shak to'rlari, yopiq qoldiq purkash, environmental controls (such as swamp draining) and personal protective methods such as using chivinlarga qarshi vosita. Chemoprophylaxis is also important in the transmission of malaria infection and resistance in defined populations (for example travelers).

A hope for future of anti-malarial therapy is the development of an effective bezgakka qarshi emlash. This could have enormous public health benefits, providing a cost-effective and easily applicable approach to preventing not only the onset of malaria but the transmission of gametocytes, thus reducing the risk of resistance developing. Anti-malarial therapy also could be diversified by combining a potentially effective vaccine with current^{[qachon? ]} chemotherapy, thereby reducing the chance of vaccine resistance developing.

Kombinatsiyalangan terapiya

The problem of the development of malaria resistance must be weighed against the essential goal of anti-malarial care; that is to reduce kasallanish va o'lim. Thus a balance must be reached that attempts to achieve both goals while not compromising either too much by doing so. The most successful attempts so far have been in the administration of combination therapy. This can be defined as, 'the simultaneous use of two or more blood schizonticidal drugs with independent modes of action and different biochemical targets in the parasite'.^[17] There is much evidence to support the use of combination therapies, some of which has been discussed previously, however several problems prevent the wide use in the areas where its use is most advisable. These include: problems identifying the most suitable drug for different epidemiological situations, the expense of combined therapy (it is over 10 times more expensive than traditional mono-therapy), how soon the programmes should be introduced and problems linked with policy implementation and issues of compliance.

The combinations of drugs currently^{[qachon? ]} prescribed can be divided into two categories: non-artemesinin-based combinations and artemesinin based combinations. It is also important to distinguish fixed-dose combination therapies (in which two or more drugs are co-formulated into a single tablet) from combinations achieved by taking two separate antimalarials.

Non-artemisinin based combinations

Komponentlar	Tavsif	Doz
Sulfadoxine-pyrimethamine (SP) (Fansidar)	This fixed-dose combination has been used for many years, causes few adverse effects, is cheap and effective in a single dose, thus decreasing problems associated with adherence and compliance. In technical terms Fansidar is not generally considered a true combination therapy since the components do not possess independent curative activity.^[4]^{[sahifa kerak ]} Fansidar should no longer be used alone for treatment of falciparum malaria.	25 mg/kg of sulfadoxine and 1.25 mg/kg of pyrimethamine.
SP plus chloroquine	High levels of resistance to one or both components means this combination is effective in few locations and it is not recommended by the Jahon Sog'liqni saqlash tashkiloti (JSSV).^[4]^{[sahifa kerak ]}	Chloroquine 25 mg/kg over three days with a single dose of SP as described above.
SP plus amodiaquine	This combination has been shown to produce a faster rate of clinical recovery than SP and chloroquine, but is clearly inferior to artemisinin-based combinations (ACTs) for the treatment of malaria.^[4]^{[sahifa kerak ]}	10 mg/kg of Amodiaquine per day for three days with a single standard dose of SP.
SP plus mefloquine (Fansimef)	This single dose pill offered obvious advantages of convenience over more complex regimes but it has not been recommended for use for many years owing to widespread resistance to the components.
Quinine plus tetracycline/doxycycline	This combination retains a high cure rate in many areas. Problems with this regime include the relatively complicated drug regimen, where quinine must be taken every eight hours for seven days. Additionally, there are significant side effects with quinine ('cinchonism ') and tetracyclines are contraindicated in children and pregnant women (these groups should use clindamycin instead). With the advent of artemisinin-combination therapies, quinine-based treatment is less popular than previously.	Quinine 10 mg/kg doses every eight hours and tetracycline in 4 mg/kg doses every six hours for seven days.

Artemisinin-based combination therapies should be used in preference to amodiaquine plus sulfadoxine-pyrimethamine for the treatment of uncomplicated P. falciparum bezgak.^[4]^{[sahifa kerak ]}

Artemisinin-based combination therapies (ACTs)

Artemesinin has a very different mode of action than conventional anti-malarials (see information above), which makes it particularly useful in the treatment of resistant infections. However, to prevent the development of resistance to this drug it is only recommended in combination with another non-artemesinin based therapy. It produces a very rapid reduction in the parasite biomass with an associated reduction in clinical symptoms and is known to cause a reduction in the transmission of gametocytes thus decreasing the potential for the spread of resistant alleles. At present there is no known resistance to Artemesinin (though some resistant strains may be emerging)^[18] and very few reported side-effects to drug usage, however this data is limited.

Komponentlar	Tavsif	Doz
Artesunate and amodiakvin (Coarsucam yoki ASAQ )	This combination has been tested and proved to be efficacious in many areas where amodiaquine retains some efficacy. A potential disadvantage is a suggested link with neytropeniya. It's recommended by the WHO for uncomplicated falciparum bezgak.^[4]^{[sahifa kerak ]}	Dosage is as a fixed-dose combination (ASAQ ) recommended as 4 mg/kg of Artesunate and 10 mg/kg of Amodiaquine per day for three days.
Artesunate and meflokin (Artequin yoki ASMQ)	This has been used as an efficacious first-line treatment regimen in areas of Thailand for many years. Mefloquine is known to cause vomiting in children and induces some neuropsychiatric and cardiotoxic effects. These adverse reactions seem to be reduced when the drug is combined with artesunate, it is suggested that this is due to a delayed onset of action of mefloquine. This is not considered a viable option to be introduced in Africa due to the long half-life of mefloquine, which potentially could exert a high selection pressure on parasites. It's recommended by the WHO for uncomplicated falciparum bezgak.^[4]^{[sahifa kerak ]}	The standard dose required is 4 mg/kg per day of Artesunate plus 25 mg/kg of Mefloquine as a split dose of 15 mg/kg on day two and 10 mg/kg on day three.
Artemether and lumefantrin (Koartem Riamet, Faverid, Amatem, Lonart yoki AL)	This combination has been extensively tested in 16 clinical trials, proving effective in children under five and has been shown to be better tolerated than artesunate plus mefloquine combinations. There are no serious side effects documented but the drug is not recommended in pregnant or lactating women due to limited safety testing in these groups. This is the most viable option for widespread use and is available in fixed-dose formulas thus increasing compliance and adherence. It's recommended by the WHO for uncomplicated falciparum bezgak.^[4]^{[sahifa kerak ]}
Artesunate and sulfadoksin /pirimetamin (Ariplus yoki Amalar plus)	This is a well tolerated combination but the overall level of efficacy still depends on the level of resistance to sulfadoxine and pyrimethamine thus limiting is usage. It is recommended by the WHO for uncomplicated falciparum bezgak.^[4]^{[sahifa kerak ]}	It is recommended in doses of 4 mg/kg of Artesunate per day for three days and a single dose of 25 mg/kg of SP.
Dihidroartemisinin -piperakvin (Duo-Cotecxin, yoki Artekin)	Has been studied mainly in China, Vietnam and other countries in SEAsia. The drug has been shown to be highly efficacious (greater than 90%). It's recommended by the WHO for uncomplicated falciparum bezgak.^[4]^{[sahifa kerak ]}
Artesinin/piperaguine/primaquine (Fast Elimination of Malaria through Source Eradication (FEMSE))	This protocol involves three doses of Artequick, spaced a month apart. The first dose is accompanied by one of primakvin. An experimental program in the Comoros islands employed the protocol. At the outset, more than 90% of the inhabitants of some villages had malaria. On one island the number of cases fell by 95%. In 2012, on the second island, the number of cases fell by 97%.^[19]
Pyronaridine and artesunate (Pyramax)	Pyramax developed by Shin Poong Pharmaceutical and Medicines for Malaria Venture (MMV). This is a first fixed-dose artemisinin-based combination therapy to be granted a positive scientific opinion for efficacy, safety and quality from European Medicines Agency (EMA) under Article 58 for the treatment of P. falciparum va P. vivax in adults and children over 20 kg based on five multi-centre phase III trials conducted in Africa and South-East Asia. Pyramax has been shown to be highly efficacious (greater than 97%) in both species and only ACT approved by stringent regulatory authority for treatment of both P. falciparum va P vivax hozirgacha.

Boshqa kombinatsiyalar

Several other anti-malarial combinations have been used or are in development. Masalan, Xlorproguanil -dapsone and artesunate (CDA) appears efficacious but the problem of haemolysis in patients with glyukoza-6-fosfat dehidrogenaza (G6PD) deficiency is likely to prevent widespread use.^[20]

By type of malaria

Antimalarial drugs and combinations may also be sorted according to the type of malaria in which they are used.

Falciparum bezgak

Artemisinin-based combination therapies (ACTs) are the recommended antimalarial treatments for uncomplicated malaria caused by P. falciparum.^[4]^{[sahifa kerak ]} The choice of ACT in a country or region will be based on the level of resistance to the constituents in the combination.^[4]^{[sahifa kerak ]} For pregnant women, the recommended first-line treatment during the birinchi trimestr is quinine plus clindamycin to be given for seven days.^[4]^{[sahifa kerak ]} In second and third trimesters, it is recommended to give ACTs known to be effective in the country/region or artesunate plus clindamycin for seven days, or quinine plus clindamycin to be given for seven days.^[4]^{[sahifa kerak ]} Lactating women should receive standard antimalarial treatment (including ACTs) except for dapsone, primakvin va tetratsiklinlar. In infants and young children, it is recommended to give ACTs for first-line treatment, with attention to accurate dosing and ensuring the administered dose is retained.^[4]^{[sahifa kerak ]}

Og'ir holatda falciparum malaria, it is recommended that rapid clinical assessment and confirmation of the diagnosis is made, followed by administration of full doses of parenteral antimalarial treatment without delay with whichever effective antimalarial is first available.^[4]^{[sahifa kerak ]} For adults, vena ichiga yuborish (IV) or mushak ichiga (IM) artesunate is recommended.^[4] Quinine is an acceptable alternative if parenteral artesunate is not available.^[4]^{[sahifa kerak ]} Parenteral antimalarials should be administered for a minimum of 24 h in the treatment of severe malaria, irrespective of the patient's ability to tolerate oral medication earlier.^[4]^{[sahifa kerak ]} Thereafter, it is recommended to complete treatment by giving a complete course of any of the following:^[4]^{[sahifa kerak ]}

an ACT
artesunate plus clindamycin or doxycycline;
quinine plus clindamycin or doxycycline.

Vivaks bezgak

Xlorokin remains the treatment of choice for vivaks bezgak,^[4]^{[sahifa kerak ]} except in Indonesia's Irian Jaya (G'arbiy Yangi Gvineya ) region and the geographically contiguous Papua-Yangi Gvineya, where chloroquine resistance is common (up to 20% resistance).

Shuningdek qarang

Diospyros melanoxylon, tree with possible antiplazmodial xususiyatlari
Bezgak profilaktikasi
Medicines for Malaria Venture (MMV) – a not-for-profit organization which is managing the largest–ever portfolio of over 50 antimalarial projects in collaboration with over 100 pharmaceutical, academic, and endemic-country partners in 38 countries.
Amazon bezgak tashabbusi – a regional USAID project in 11 countries in the Latin America and the Caribbean region.
RAVREDA – a regional network of national malaria control programs that conduct antimalarial drug efficacy surveillance and other activities to address malaria.
Loyiha 523

Adabiyotlar

^ ^a ^b ^v ^d ^e Eshli, Yelizaveta A .; Phyo, Aung Pyae (25 May 2018). "Drugs in Development for Malaria". Giyohvand moddalar. 78 (9): 861–879. doi:10.1007/s40265-018-0911-9. PMC 6013505. PMID 29802605.
^ Mittra, Robert A.; Mieler, William F. (2013). "Drug Toxicity of the Posterior Segment". Retina. pp. 1532–1554. doi:10.1016/B978-1-4557-0737-9.00089-8. ISBN 978-1-4557-0737-9.
^ "Updating the WHO G6PD classification of variants and the International Classification of Diseases" (PDF). www.who.int. 2019. Olingan 2020-03-24.
^ ^a ^b ^v ^d ^e ^f ^g ^h ^men ^j ^k ^l ^m ⁿ ^o ^p ^q ^r ^s ^t ^siz ^v ^w Jahon sog'liqni saqlash tashkiloti (2015). Guidelines for the treatment of malaria (Uchinchi nashr). Jahon Sog'liqni saqlash tashkiloti (JSSV). hdl:10665/162441. ISBN 978-92-4-154912-7.
^ Sparkes, Roland. Article, www.belmonthistory.org.uk [1], olingan 2010-01-05^{[to'liq iqtibos kerak ]}
^ https://www.reuters.com/article/uk-factcheck-quinine-idUSKBN2370R9#:~:text=Hydroxychloroquine%2C%20developed%20in%20the%201950s%20from%20chloroquine%2C%20an,such%20as%20Plaquenil%2C%20Quensyl%20and%20Plaquinol.%20French%20
^ https://patents.google.com/patent/WO2010027150A2/en
^ https://patents.google.com/patent/CN104230803A/en
^ Frans Timmerhuis (2013-02-04). Handboek wereldreiziger. Elmar B.V., Uitgeverij. ISBN 978-90-389-2055-9.
^ Markus, MB (2018). "Biological Concepts in Recurrent Plazmodium vivax Malaria". Parazitologiya. 145 (13): 1765–1771. doi:10.1017/S003118201800032X. PMID 29564998.
^ Dicko, Alassane; Roh, Michelle E; Diawara, Halimatou; Mahamar, Almahamoudou; Soumare, Harouna M; Lanke, Kjerstin; Bredli, Jon; Sanogo, Koualy; Kone, Daouda T; Diarra, Kalifa; Keita, Sekouba; Issiaka, Djibrilla; Traore, Sekou F; McCulloch, Charles; Stone, Will J R; Hwang, Jimee; Myuller, Olaf; Brown, Joelle M; Srinivasan, Vinay; Drakeley, Chris; Gosling, Roly; Chen, Ingrid; Bousema, Teun (June 2018). "Efficacy and safety of primaquine and methylene blue for prevention of Plasmodium falciparum transmission in Mali: a phase 2, single-blind, randomised controlled trial". Lanset yuqumli kasalliklar. 18 (6): 627–639. doi:10.1016/S1473-3099(18)30044-6. PMC 5968371. PMID 29422384.
^ "Rectal artemisinins rapidly eliminate malarial parasites". EurekAlert!. 2008-03-27. Arxivlandi asl nusxasidan 2008 yil 3 aprelda. Olingan 2008-03-28.
^ "The History of Traditional Chinese Medicine". Arxivlandi asl nusxasi 2007 yil 25 dekabrda. Olingan 2007-12-19.
^ (PDF). 2008 yil 13-noyabr https://web.archive.org/web/20081113064411/http://www.icei.it/pdf/Report_Artemisia_ICEI.pdf. Arxivlandi asl nusxasi (PDF) 2008-11-13 kunlari. Yo'qolgan yoki bo'sh sarlavha = (Yordam bering)
^ van Vugt M, Brockman A, Gemperli B, Luxemburger C, Gathmann I, Royce C, Slight T, Looareesuwan S, White NJ, Nosten F (January 1998). "Randomized comparison of artemether-benflumetol and artesunate-mefloquine in treatment of multidrug-resistant falciparum malaria". Mikroblarga qarshi vositalar va kimyoviy terapiya. 42 (1): 135–9. doi:10.1128/AAC.42.1.135. PMC 105468. PMID 9449273.
^ White NJ (April 2004). "Antimalarial drug resistance". J. klinikasi. Investitsiya. 113 (8): 1084–92. doi:10.1172/JCI21682. PMC 385418. PMID 15085184.
^ Antony HA, Parija SC (2016). "Antimalarial drug resistance: An overview". Tropical Parasitology. 6 (1): 30–41. doi:10.4103/2229-5070.175081. PMC 4778180. PMID 26998432.
^ Lim P; Alker AP; Khim N; va boshq. (2009). "Pfmdr1 copy number and arteminisin derivatives combination therapy failure in falciparum malaria in Cambodia". Bezgak. J. 8: 11. doi:10.1186/1475-2875-8-11. PMC 2627910. PMID 19138391.
^ "Malaria eradication: Cure all?". Iqtisodchi. 2014-01-25. Olingan 2014-02-16.
^ Premji Z, Umeh RE, Owusu-Agyei S, et al. (2009). "Chlorproguanil-dapsone-artesunate versus artemether-lumefantrine: a randomized, double-blind phase III trial in African children and adolescents with uncomplicated Plazmodium falciparum bezgak ". PLOS ONE. 4 (8): e6682. Bibcode:2009PLoSO...4.6682P. doi:10.1371/journal.pone.0006682. PMC 2724683. PMID 19690618.

Qo'shimcha o'qish

Jahon sog'liqni saqlash tashkiloti (2015). Guidelines for the treatment of malaria (Uchinchi nashr). Jahon Sog'liqni saqlash tashkiloti (JSSV). hdl:10665/162441. ISBN 978-92-4-154912-7.
Jahon sog'liqni saqlash tashkiloti (2012). Management of severe malaria: a practical handbook (Uchinchi nashr). Jahon Sog'liqni saqlash tashkiloti (JSSV). hdl:10665/79317. ISBN 978-92-4-154852-6.

Tashqi havolalar

Scholia bor mavzu uchun profil Bezgakka qarshi dori.

Medicines for Malaria Venture (MMV) [MMV] « MMV Science » – for information on the largest–ever portfolio of over 50 antimalarial projects, working in collaboration with over 100 pharmaceutical, academic, and endemic-country partners in 38 countries.
The Worldwide Antimalarial Resistance Network (WWARN) is a global collaboration generating quality-assured, timely information to track the emergence and spread of antimalarial resistance — critical information for ensuring that anyone infected with malaria receives safe and effective treatment.
2007 yildagi ko'rsatmalar mavjud UK Health Protection Agency website as a PDF file and includes detailed country-specific information for UK travelers.
The Jahon Sog'liqni saqlash tashkiloti bezgakning oldini olish bo'yicha mamlakatga xos tavsiyalar beradi. HPA va JSST maslahatlari bir-biriga to'liq mos keladi (garchi ba'zi farqlar mavjud bo'lsa ham).
The Kasalliklarni nazorat qilish va oldini olish markazlari veb-saytida bezgak kasalligi bo'yicha doimiy ravishda mamlakatga tegishli ma'lumotlar yangilanadi. Ushbu veb-saytda berilgan tavsiyalar unchalik batafsil emas, juda ehtiyotkor va ma'lum bir mamlakat ichidagi barcha sohalarga mos kelmasligi mumkin. This is the preferred site for travelers from the US.

[AshleyPhyo2018-1] v ^d ^e Eshli, Yelizaveta A .; Phyo, Aung Pyae (25 May 2018). "Drugs in Development for Malaria". Giyohvand moddalar. 78 (9): 861–879. doi:10.1007/s40265-018-0911-9. PMC 6013505. PMID 29802605.

[2] Mittra, Robert A.; Mieler, William F. (2013). "Drug Toxicity of the Posterior Segment". Retina. pp. 1532–1554. doi:10.1016/B978-1-4557-0737-9.00089-8. ISBN 978-1-4557-0737-9.

[3] "Updating the WHO G6PD classification of variants and the International Classification of Diseases" (PDF). www.who.int. 2019. Olingan 2020-03-24.

[WHO_Guidelines-4] v ^d ^e ^f ^g ^h ^men ^j ^k ^l ^m ⁿ ^o ^p ^q ^r ^s ^t ^siz ^v ^w Jahon sog'liqni saqlash tashkiloti (2015). Guidelines for the treatment of malaria (Uchinchi nashr). Jahon Sog'liqni saqlash tashkiloti (JSSV). hdl:10665/162441. ISBN 978-92-4-154912-7.

[5] Sparkes, Roland. Article, www.belmonthistory.org.uk [1], olingan 2010-01-05^{[to'liq iqtibos kerak ]}

[6] ttps://www.reuters.com/article/uk-factcheck-quinine-idUSKBN2370R9#:~:text=Hydroxychloroquine%2C%20developed%20in%20the%201950s%20from%20chloroquine%2C%20an,such%20as%20Plaquenil%2C%20Quensyl%20and%20Plaquinol.%20French%20

[7] ttps://patents.google.com/patent/WO2010027150A2/en

[8] ttps://patents.google.com/patent/CN104230803A/en

[Timmerhuis-9] Frans Timmerhuis (2013-02-04). Handboek wereldreiziger. Elmar B.V., Uitgeverij. ISBN 978-90-389-2055-9.

[10] Markus, MB (2018). "Biological Concepts in Recurrent Plazmodium vivax Malaria". Parazitologiya. 145 (13): 1765–1771. doi:10.1017/S003118201800032X. PMID 29564998.

[11] Dicko, Alassane; Roh, Michelle E; Diawara, Halimatou; Mahamar, Almahamoudou; Soumare, Harouna M; Lanke, Kjerstin; Bredli, Jon; Sanogo, Koualy; Kone, Daouda T; Diarra, Kalifa; Keita, Sekouba; Issiaka, Djibrilla; Traore, Sekou F; McCulloch, Charles; Stone, Will J R; Hwang, Jimee; Myuller, Olaf; Brown, Joelle M; Srinivasan, Vinay; Drakeley, Chris; Gosling, Roly; Chen, Ingrid; Bousema, Teun (June 2018). "Efficacy and safety of primaquine and methylene blue for prevention of Plasmodium falciparum transmission in Mali: a phase 2, single-blind, randomised controlled trial". Lanset yuqumli kasalliklar. 18 (6): 627–639. doi:10.1016/S1473-3099(18)30044-6. PMC 5968371. PMID 29422384.

[12] "Rectal artemisinins rapidly eliminate malarial parasites". EurekAlert!. 2008-03-27. Arxivlandi asl nusxasidan 2008 yil 3 aprelda. Olingan 2008-03-28.

[13] "The History of Traditional Chinese Medicine". Arxivlandi asl nusxasi 2007 yil 25 dekabrda. Olingan 2007-12-19.

[14] (PDF). 2008 yil 13-noyabr https://web.archive.org/web/20081113064411/http://www.icei.it/pdf/Report_Artemisia_ICEI.pdf. Arxivlandi asl nusxasi (PDF) 2008-11-13 kunlari. Yo'qolgan yoki bo'sh sarlavha = (Yordam bering)

[pmid9449273-15] van Vugt M, Brockman A, Gemperli B, Luxemburger C, Gathmann I, Royce C, Slight T, Looareesuwan S, White NJ, Nosten F (January 1998). "Randomized comparison of artemether-benflumetol and artesunate-mefloquine in treatment of multidrug-resistant falciparum malaria". Mikroblarga qarshi vositalar va kimyoviy terapiya. 42 (1): 135–9. doi:10.1128/AAC.42.1.135. PMC 105468. PMID 9449273.

[pmid15085184-16] White NJ (April 2004). "Antimalarial drug resistance". J. klinikasi. Investitsiya. 113 (8): 1084–92. doi:10.1172/JCI21682. PMC 385418. PMID 15085184.

[tropicalparasitology2016-17] Antony HA, Parija SC (2016). "Antimalarial drug resistance: An overview". Tropical Parasitology. 6 (1): 30–41. doi:10.4103/2229-5070.175081. PMC 4778180. PMID 26998432.

[pmid19138391-18] Lim P; Alker AP; Khim N; va boshq. (2009). "Pfmdr1 copy number and arteminisin derivatives combination therapy failure in falciparum malaria in Cambodia". Bezgak. J. 8: 11. doi:10.1186/1475-2875-8-11. PMC 2627910. PMID 19138391.

[19] "Malaria eradication: Cure all?". Iqtisodchi. 2014-01-25. Olingan 2014-02-16.

[20] Premji Z, Umeh RE, Owusu-Agyei S, et al. (2009). "Chlorproguanil-dapsone-artesunate versus artemether-lumefantrine: a randomized, double-blind phase III trial in African children and adolescents with uncomplicated Plazmodium falciparum bezgak ". PLOS ONE. 4 (8): e6682. Bibcode:2009PLoSO...4.6682P. doi:10.1371/journal.pone.0006682. PMC 2724683. PMID 19690618.

[1]

[2]

[3]

[4]

[5]

[6]

[7]

[8]

[9]

[10]

[11]

[12]

[13]

[14]

[15]

[16]

[17]

[18]

[19]

[20]

Bezgak
Biologiya	Bezgak Miya Quartan isitmasi Qora suv isitmasi Homiladorlik bilan bog'liq Plazmodium biologiya hayot davrasi vivaks falciparum ovale bezgak bilimdonlar Anofel pashshasi Hayot davrasi Shizont Merozoit Gipnozoit Gametotsit
Nazorat va profilaktika	Aholi salomatligi DDT Chivinli to'r Bezgak profilaktikasi Chivinlarga qarshi kurash Steril hasharotlar texnikasi Genetic resistance Duffy antijeni O'roqsimon hujayrali anemiya Talassemiya G6PDH etishmovchiligi Bezgakka qarshi emlash RTS, S
Tashxis va davolash	Bezgak tashxisi Bezgak madaniyati Qon plyonkasi Bezgak antigenini aniqlash testlari Bezgakka qarshi vositalar Artemisinin Meflokin Proguanil
Jamiyat va bezgak	Qashshoqlik kasalliklari Mingyillik rivojlanish maqsadlari Bezgak tarixi Xronologiya Rim isitmasi Bezgakni yo'q qilish milliy dasturi Butunjahon bezgakka qarshi kurash kuni Epidemiologiya Bezgak va Karib havzasi Bezgak atlasi loyihasi
Tashkilotlar	Bezgak konsortsiumi Bezgakka qarshi kurash fondi Bill va Melinda Geyts jamg'armasi Bezgak yo'qligini tasavvur qiling Endi bezgak yo'q Afrikada bezgakka qarshi kurash Afrika bezgak tarmog'iga ishonish Janubiy Afrikada bezgak tashabbusi Afrika rahbarlari bezgak alyansi Amazon bezgak tashabbusi OITS, sil va bezgakka qarshi kurash bo'yicha global fond Bezgak kasalligiga qarshi dorilar
Turkum