Chuqur tomir trombozi - Deep vein thrombosis

"DVT" bu erga yo'naltiriladi. Boshqa maqsadlar uchun qarang DVT (ajralish).

Chuqur tomir trombozi
Boshqa ismlarChuqur venoz tromboz
O'ng oyoqning chuqur tomir trombozi.jpg
Shish va qizarish bilan o'ng oyoqdagi DVT
MutaxassisligiTurli xil
AlomatlarOg'riq, shish, qizarish, ta'sirlangan a'zoning kengaygan tomirlari[1]
MurakkabliklarPost-trombotik sindrom, takrorlanadigan VTE[2]
Xavf omillariSo'nggi operatsiya, yoshi kattaroq, faol saraton, semirish, shaxsiy tarix yoki oila tarixi VTE, jarohatlar, shikastlanish, harakat etishmasligi, gormonal tug'ilishni nazorat qilish, homiladorlik va etkazib berishdan keyingi davr, antifosfolipid sindromi, ba'zi genetik omillar[3][4]
Diagnostika usuliUltratovush[5]
Differentsial diagnostikaYirtilgan Beyker kistasi, selülit, gematoma, limfedema va surunkali venoz etishmovchilik
Oldini olishTez-tez yurish, buzoq mashqlari, tana vaznini saqlash, antikoagulyantlar (qonni suyultiruvchi), vaqti-vaqti bilan pnevmatik siqish, tugatilgan siqish paypoqlari, aspirin[6][7]
DavolashAntikoagulyatsiya, kateterga yo'naltirilgan tromboliz
Dori-darmonTo'g'ridan-to'g'ri og'iz antikoagulyantlari, past molekulyar og'irlikdagi geparin, fondaparinux, sintez qilinmagan geparin, varfarin
ChastotaniEvropa ajdodlari bilan yiliga 1000 kishidan 1,0-1,8[3]

Chuqur tomir trombozi (DVT) shakllanishidir qon pıhtısı a chuqur tomir, ko'pincha oyoqlarda yoki tosda.[8][a] Semptomlarga og'riq, shishish, qizarish va zararlangan hududdagi kengaygan tomirlar kirishi mumkin, ammo ba'zi DVTlarda simptomlar yo'q.[1] DVT bilan bog'liq hayotga tahdid soladigan eng keng tarqalgan tashvish - bu qon quyilishi (yoki bir nechta quyqalar) paydo bo'lishi tomirlardan ajrating (embolize), yurakning o'ng tomoni bo'ylab harakatlaning va o'pkaga qon etkazib beradigan arteriyalarga yopishib oling. Bu deyiladi o'pka emboliya (Pe). Ikkala DVT va PE ham bir xil umumiy kasallik jarayonining bir qismi sifatida qaraladi, bu deyiladi venoz tromboembolizm (VTE). VTE faqat DVT sifatida, DVT bilan PE yoki DVTsiz PE kabi bo'lishi mumkin.[3] Eng tez-tez uzoq muddatli asorat bu post-trombotik sindrom, og'riq, shishish, og'irlik hissi, qichishish va og'ir holatlarda olib kelishi mumkin, oshqozon yarasi.[5] Shuningdek, takroriy VTE dastlabki VTEdan keyingi o'n yil ichida taxminan 30% da uchraydi.[3]

Pıhtı hosil bo'lish mexanizmi odatda ba'zi bir kombinatsiyani o'z ichiga oladi qon oqimining pasayishi, oshdi pıhtılaşmaya moyilligi va shikastlanish qon tomirlari devori.[9] Xavf omillari orasida yaqinda o'tkazilgan jarrohlik, katta yoshdagi, faol saraton, semirish, shaxsiy tarix va oila tarixi VTE, travma, jarohatlar, harakat etishmasligi, gormonal tug'ilishni nazorat qilish, homiladorlik va tug'ilishdan keyingi davr va antifosfolipid sindromi. VTE kuchli genetik komponentga ega, bu VTE stavkalarining o'zgaruvchanligining taxminan 50-60 foizini tashkil qiladi.[4] Genetik omillarga O bo'lmagan moddalar kiradi qon guruhi, kamchiliklar antitrombin, oqsil C va oqsil S va mutatsiyalari omil V Leyden va protrombin G20210A. Umuman olganda, o'nlab genetik xavf omillari aniqlandi.[4][10]

DVT bilan kasallanganlikda gumon qilingan odamlarni a yordamida baholash mumkin bashorat qilish qoidasi kabi Uells hisobi. A Dim-dimer test shuningdek, tashxisni istisno qilishga yordam berish yoki qo'shimcha tekshiruvlar zarurligini ko'rsatish uchun ishlatilishi mumkin.[5] Tashxisni ko'pincha tasdiqlaydi ultratovush shubhali tomirlar.[5] Taxminan 4-10% DVT qo'llarga ta'sir qiladi.[11] Taxminan 5–11 foiz odam VTEni hayoti davomida rivojlantiradi, VTE esa yoshga qarab ancha keng tarqalgan.[12][13] 40 va undan past yoshdagilar bilan taqqoslaganda, 65 va undan yuqori yoshdagi odamlar taxminan 15 baravar yuqori xavfga ega.[14] Biroq, mavjud ma'lumotlar tarixiy jihatdan Evropa va Shimoliy Amerika aholisi tomonidan boshqarilgan,[15] va Osiyoning va Ispaniyaliklarning VTE xavfi oq yoki qora tanlilarga qaraganda past.[4]

Qonni suyultiruvchi vositalardan foydalanish (antikoagulyatsiya ) standart davolash usuli hisoblanadi va odatdagi dorilar kiradi rivaroksaban, apiksaban va varfarin. Varfarin bilan davolashni boshlash uchun qo'shimcha og'iz bo'lmagan antikoagulyant, ko'pincha in'ektsiya kerak geparin.[16][17][18] Oddiy aholi uchun VTE profilaktikasi semirishdan saqlanish va faol turmush tarzini saqlashni o'z ichiga oladi. Xavfi past bo'lgan operatsiyadan keyingi profilaktika ishlari erta va tez-tez yurishni o'z ichiga oladi. Xavfli operatsiyalar, odatda qonni suyultiruvchi vosita bilan VTE ni oldini oladi aspirin bilan birlashtirilgan vaqti-vaqti bilan pnevmatik siqish.[7]

Fon

Qon tomirlari shikastlanganda qon quyulishga tabiiy moyilligi bor (gemostaz ) qon yo'qotilishini minimallashtirish uchun.[19] Pıhtılaşma koagulyatsion kaskad va endi kerak bo'lmagan pıhtıların tozalanishi tomonidan amalga oshiriladi fibrinolitik tizim yoki fibrinoliz.[19] Fibrinolizning pasayishi yoki koagulyatsiyaning ko'payishi DVT xavfini oshirishi mumkin.[19]

DVT bilan bog'liq o'limning eng keng tarqalgan sababi qon pıhtılaşmasıdır (yoki bir nechta pıhtı) tomirlardan ajrating (embolize), yurakning o'ng tomoni bo'ylab harakatlaning va tiqilib qoling o'pka arteriyalari kislorod bilan ta'minlash uchun o'pkaga oksidlanishsiz qon etkazib beradigan. O'pka qon oqimining bu tiqilib qolishi deyiladi o'pka emboliya (Pe). PE ko'pincha sonda yoki tosda paydo bo'ladigan kattaroq DVTlarda uchraydi. Ham DVT, ham PE bir xil umumiy kasallik jarayonining bir qismi sifatida qaraladi, venoz tromboembolizm (VTE), bu DVT yoki DVT bilan yoki DVTsiz bo'lishi mumkin.[3] VTE o'lim sabablari orasida uchinchi o'rinda turadi yurak-qon tomir kasalliklari, eng yaxshi ikkita sabab yurak tomirlari kasalligi va ishemik qon tomir.[20] PEdan tashqari, DVT bilan bog'liq hayotga xavf soladigan yana bir tashvish, kamdan-kam bo'lsa ham, og'ir holatlar tananing bir mintaqasining venoz chiqishini butunlay to'sib qo'yganda. Bunga olib keladigan bosim kuchayishi mumkin bo'lim sindromi va oksijenatsiyaning pasayishiga olib keladi gangrena.

Belgilari va alomatlari

DVT belgilari va alomatlari juda o'zgaruvchan bo'lsa ham, og'riq yoki yumshoqlik, shishish, issiqlik, sirt tomirlarining kengayishi, qizarish yoki rang o'zgarishi va siyanoz isitma bilan.[5] Biroq, DVT bilan og'riganlarning ba'zilarida hech qanday alomat yo'q.[18] Faqatgina alomatlar va alomatlar etarli emas sezgir yoki o'ziga xos tashxis qo'yish uchun, lekin bilan birgalikda ko'rib chiqilganda sinovdan oldin ehtimollik, DVT ehtimolligini aniqlashga yordam beradi.[18] Ko'pgina shubhali holatlarda DVT baholashdan so'ng chiqarib tashlanadi,[21] va alomatlar ko'pincha boshqa sabablarga bog'liq, masalan, yorilish Beyker kistasi, selülit, gematoma, limfedema va surunkali venoz etishmovchilik.[1] Boshqalar differentsial diagnostika venoz yoki arterial shishlarni o'z ichiga oladi anevrizmalar va biriktiruvchi to'qima kasalliklari.[22]

Sabablari

Chuqur tomir trombozini tasvirlash

Uch omil Virchovning uchligivenoz staz, giperkoagulyatsiya va o'zgarishlar endoteliy qon tomirlari qoplamasi - VTEga hissa qo'shadi va uning shakllanishini tushuntirish uchun ishlatiladi.[23] Vena staziyasi bu uchta omilning eng natijasidir.[9] Bilan bog'liq boshqa sabablarga ko'ra aktivlashtirish kiradi immunitet tizimi komponentlari, holati mikropartikulalar qonda, kislorod kontsentratsiyasi va mumkin trombotsit faollashtirish.[24] VTEga turli xil xavf omillari, shu jumladan genetik va atrof-muhit omillari yordam beradi, ammo ko'pgina xavf omillari bo'lgan ko'pchilik uni hech qachon rivojlantirmaydi.[25][12]

Qabul qilingan xavf omillariga keksa yoshdagi kuchli xavf omili kiradi,[5] pıhtılaşmaya yordam beradigan qon tarkibini o'zgartiradi.[26] Oldingi VTE, ayniqsa, sababsiz VTE, kuchli xavf omilidir.[27] Katta jarrohlik va travma tufayli xavfni oshiradi to'qima omili qonga kiradigan qon tomir tizimining tashqarisidan.[28] Engil jarohatlar,[29] pastki oyoq amputatsiyasi,[30] kestirib, sinish va uzun suyak singan yoriqlar ham xavflidir.[8] Yilda ortopedik jarrohlik, protsedura doirasida qon oqimining to'xtashi bilan venoz stazni vaqtincha qo'zg'atishi mumkin.[24] Harakatsizlik va immobilizatsiya venoz stazaga yordam beradi ortopedik tashuvchilar,[31] falaj, o'tirish, uzoq muddatli sayohat, yotoqda dam olish, kasalxonaga yotqizish,[28] va o'tkir kasallikdan omon qolganlarda qon tomir.[32] Tomirlarda buzilgan qon oqimini o'z ichiga olgan holatlar May-Thurner sindromi, bu erda tos venasi siqilgan va venoz ko'krak qafasi sindromi o'z ichiga oladi Paget-Shroetter sindromi, bu erda bo'yin tagiga yaqin siqilish paydo bo'ladi.[33][34][35]

Saraton tomirlar atrofida va atrofida o'sib, venoz stazni keltirib chiqarishi va shuningdek to'qima omilining ko'payishini rag'batlantirishi mumkin.[36] Suyak, tuxumdon, miya, oshqozon osti bezi va limfomalarning saraton kasalliklari, ayniqsa VTE xavfini oshiradi.[30] Kimyoviy terapiya davolash ham xavfni oshiradi.[37] Semirib ketish qonning ivish qobiliyatini oshiradi, homiladorlik kabi. In tug'ruqdan keyingi, plasental pıhtılaşmaya yordam beradigan moddalarni ajratish. Og'iz kontratseptivlari[b] va gormonal almashtirish terapiyasi qonning koagulyatsion oqsil darajasi o'zgargan va kamaytirilgan, shu jumladan turli xil mexanizmlar orqali xavfni oshiradi fibrinoliz.[24]

The qon ivishi tizimi, ko'pincha a "kaskad", o'zaro ta'sirlanib qon pıhtısını hosil qiladigan oqsillar guruhidan iborat. Kaskaddagi anormallik tufayli DVT xavfi ortadi. Regulyatorlar, antitrombin (DTHR) va faollashtirilgan S (APC) oqsili ular ta'sir qiladigan qon ivish omillari ustida yashil rangda ko'rsatilgan.

VTE stavkalari o'zgaruvchanligining taxminan 50 dan 60 foizigacha irsiy omillar.[4] Oila tarixi VTE ning birinchi VTE uchun xavf omilidir.[39] VTE xavfini oshiradigan genetik omillar orasida odatda qon ivishining oldini oladigan uchta oqsilning etishmasligi mavjud.oqsil C, oqsil S va antitrombin. Antitrombin etishmovchiligi, oqsil C va oqsil S[c] kamdan-kam, ammo kuchli yoki o'rtacha darajada kuchli xavf omillari.[28][24] Ushbu uchta kamchilik VTE xavfini taxminan 10 barobar oshiradi.[40] V omil Leyden qiladi omil V tomonidan inaktivatsiyaga chidamli faollashtirilgan protein C,[39] VTE xavfini taxminan uch baravar oshirib yuboradi.[10][39] Qon bo'lmagan qon guruhiga ega bo'lish VTE xavfini taxminan ikki baravar oshiradi.[24] Qon bo'lmagan qon guruhi dunyo miqyosida keng tarqalgan bo'lib, uni muhim xavf omiliga aylantiradi.[41] Qon guruhi bo'lmagan odamlarda qon darajasi yuqori fon Uilbrand omili va omil VIII pıhtılaşma ehtimolini oshirib, O qon guruhiga ega bo'lganlarga qaraganda.[41] Umumiy uchun homozigot bo'lganlar fibrinogen gamma geni rs2066865 variantida VTE xavfi taxminan 1,6 baravar yuqori.[42] Genetik variant protrombin G20210A, bu protrombin darajasini oshiradi,[28] xavfni taxminan 2,5 baravar oshiradi.[10] Bundan tashqari, odamlarning taxminan 5% V faktor Leyden va protrombin G20210A mutatsiyalari bilan taqqoslanadigan fon genetik xavfi bilan aniqlangan.[10]

Yuqtirish, shu jumladan COVID-19, xavfni oshiradi.[43][44] Yallig'lanish kasalliklari[24][45] kabi Behchet sindromi,[46] va ba'zilari otoimmun kasalliklar,[47] boshlang'ich kabi antifosfolipid sindromi[48] va tizimli eritematoz (SLE),[49] xavfni oshirish. SLE ning o'zi tez-tez ikkilamchi antifosfolipid sindromi bilan bog'liq.[50] Boshqa bog'liq sharoitlar kiradi geparindan kelib chiqqan trombotsitopeniya,[51] trombotik bo'ron,[52] katastrofik antifosfolipid sindromi,[53] paroksismal tungi gemoglobinuriya,[54] nefrotik sindrom,[12] surunkali buyrak kasalligi,[55] OIV,[56] politsitemiya,[31] vena ichiga giyohvand moddalarni iste'mol qilish,[57] va chekish.[d] Qonning o'zgarishi, shu jumladan disfibrinogenemiya,[31] past oqsil S,[12] faollashtirilgan protein S qarshiligi,[12] homosistinuriya,[59] giperhomotsisteinemiya,[28] yuqori fibrinogen darajalar,[28] yuqori omil IX darajalar,[28] va yuqori omil XI darajalar[28] yuqori xavf bilan bog'liq.

DVT ning tanadagi joylashishiga ba'zi xavf omillari ta'sir qiladi. Izolyatsiya qilingan distal DVTda xavf omillari profili proksimal DVTdan farq qiladi. Jarrohlik va immobilizatsiya kabi vaqtinchalik omillar, trombofilialar esa ustunlik qiladi[e] va yoshi xavfni oshirmaydi.[61] Yuqori ekstremal DVTga olib keladigan umumiy xavf omillari orasida mavjud bo'lgan begona jismga ega bo'lish (masalan, markaziy venoz kateter, yurak stimulyatori yoki uch karra lümenli PICC liniyasi), saraton kasalligi va yaqinda o'tkazilgan operatsiya.[11]

Tasnifi

Yon tomirlarga (tos suyagida) tashqi yonbosh venasi, ichki yonbosh venasi va umumiy yonbosh venasi kiradi. Umumiy femoral tomir tashqi yonbosh venasi ostida ko'rinadi. (Bu erda oddiygina "femoral" deb nomlangan.)

G'azablangan DVTlar jarrohlik, og'iz kontratseptivlari, travma, harakatsizlik, semirish yoki saraton kabi xavf omillari bilan birgalikda yuzaga keladi; sotib olingan holatlarsiz holatlar chaqirilmagan yoki idyopatik.[62] O'tkir DVT og'riq va shish bilan tavsiflanadi[63] va odatda okklyuziv,[64] bu qon oqimiga to'sqinlik qiladi, okklyuziv bo'lmagan DVT esa kamroq simptomatikdir.[65] Yorliq "surunkali "10 dan 14 kungacha davom etadigan simptomatik DVTga qo'llanildi.[66] Hech qanday alomatlari bo'lmagan, ammo faqat skrining orqali topilgan DVT asemptomatik yoki tasodifiy deb belgilanadi.[67][68] DVTning dastlabki epizodi voqea deb ataladi va keyingi DVT takrorlanuvchi deb nomlanadi.[69][70] Ikki tomonlama DVT ikkala oyog'idagi pıhtılarni anglatadi, bir tomonlama esa faqat bitta oyoq ta'sirlanishini anglatadi.[71]

Oyoqlarda DVT tizzadan yuqorisida proksimal, tizzadan pastda distal (yoki buzoq).[72][73] Popliteal tomir ostidagi DVT, tizzaning orqasida proksimal tomir distal deb tasniflanadi[64] va cheklangan klinik ahamiyati proksimal DVT bilan taqqoslaganda.[74] Iliofemoral DVT iliak yoki umumiy femoral tomir;[75] boshqa joylarda, bu minimal darajada ishtirok etish deb ta'riflangan umumiy yonbosh venasi, bu tos suyagi tepasiga yaqin.[18] Yuqori ekstremal DVT qo'llarda yoki bo'yin tagida paydo bo'ladi. Kamdan-kam uchraydigan DVT muhim to'siqlarni keltirib chiqaradi flegmasiya cerulea dolens bilan kuzatilgan holatlar tufayli shunday nomlangan ko'k yoki binafsha rang.[76][77][f] Bu o'tkir, proksimal va okklyuziv DVTning ayniqsa og'ir shakli. Bu hayot uchun xavfli, oyoq-qo'l uchun xavfli va venoz qon tomir xavfini tug'diradi gangrena.[78] Bu qo'lda paydo bo'lishi mumkin, lekin ko'pincha oyoqqa ta'sir qiladi.[65][79]

Patofiziologiya

2136ab pastki ekstremal tomirlar oldingi Posterior.jpg

DVT ko'pincha buzoq tomirlarida rivojlanib, venoz oqim yo'nalishi bo'yicha, yurakka qarab "o'sadi".[80] DVT o'smasa, u tabiiy ravishda tozalanishi va qonda eritilishi mumkin (fibrinoliz).[81] Ko'pincha oyoq yoki tos suyagi tomirlari ta'sir qiladi,[8] shu jumladan popliteal tomir (tizzaning orqasida), femoral tomir (sonning) va tosning yonbosh venalari. Keng ekstremal DVT hatto ichiga kirishi mumkin pastki vena kava (qorin bo'shlig'ida).[82] Yuqori ekstremal DVT odatda subklavian, aksiller va bo'yin tomirlari.[11]

Yuqori ekstremal DVTlar subklavian, aksiller, brakiyal, ulnar va radial tomirlarda (rasmda) va bo'yinli va brakiyosefalik tomirlar (rasmda emas). Sefalik va bazilik tomirlar esa yuzaki tomirlardir.[11]

Sabablari arterial tromboz kabi, bilan yurak xurujlari, venoz trombozga qaraganda aniqroq tushuniladi.[83] Arterial tromboz bilan qon tomirlari devorlarini shikastlanishi kerak, chunki u boshlanadi qon ivishi,[83] ammo tomirlarda pıhtılaşma asosan bunday zarar ko'rmasdan sodir bo'ladi.[28] Vena trombozining boshlanishiga protrombinni trombinga, so'ngra fibrinni cho'ktirishga olib keladigan to'qima omili sabab bo'ladi deb o'ylashadi.[37] Qizil qon hujayralari va fibrin venoz trombining asosiy tarkibiy qismlari,[28] va fibrin qon ivishining devorlariga (endoteliyga) yopishgan ko'rinadi, bu odatda pıhtılaşmayı oldini olish uchun harakat qiladi.[83] Trombotsitlar va oq qon hujayralari shuningdek, tarkibiy qismlardir. Trombotsitlar arterial qon tomirlarida bo'lgani kabi venoz pıhtılarda ham mashhur emas, ammo ular rol o'ynashi mumkin.[24] Yallig'lanish VTE bilan bog'liq,[g] va oq qon hujayralari venoz pıhtıların shakllanishi va echilishida rol o'ynaydi.[81]

D-dimer ishlab chiqarish

Ko'pincha DVT tomirlarning qopqog'idan boshlanadi.[81] Vanalardagi qon oqimi qonda past kislorod kontsentratsiyasini keltirib chiqarishi mumkin (gipoksemiya ) qopqoq sinusining. Gipoksemiya, venoz staziya bilan yomonlashadi, yo'llarni faollashtiradi - ular kiradi gipoksiyani keltirib chiqaradigan omil-1 va erta o'sishga javob beradigan protein 1. Gipoksemiya ham ishlab chiqarishga olib keladi reaktiv kislorod turlari, bu yo'llarni faollashtirishi mumkin, shuningdek yadro omili-DB, gipoksiyani keltirib chiqaradigan omil-1ni boshqaradi transkripsiya.[37] Gipoksiya keltirib chiqaradigan omil-1 va o'sishga erta javob beradigan oqsil 1, masalan, endotelial oqsillari bilan monotsitlar birikmasiga hissa qo'shadi. P-tanlovi, monotsitlarni to'qima omillari bilan to'ldirilishini talab qiladi mikrovezikulalar, bu endotelial yuzasiga bog'langanidan keyin pıhtılaşmayı boshlaydi.[37]

D-dimerlar a fibrin parchalanish mahsuloti, ning tabiiy yon mahsuloti fibrinoliz odatda qonda uchraydi. Yuqori daraja[h] dan kelib chiqishi mumkin plazmin pıhtının tarqalishi yoki boshqa holatlar.[84] Kasalxonaga yotqizilgan bemorlar ko'pincha bir necha sabablarga ko'ra yuqori darajaga ega.[21] Antikoagulyatsiya, DVT uchun standart davolash, pıhtıların o'sishini va PE ning oldini oladi, lekin to'g'ridan-to'g'ri mavjud bo'lgan pıhtılara ta'sir qilmaydi.[85]

Tashxis

Suyuqlikdan shish (shish) dan oyoq shishishi bosim o'tkazilgandan keyin "chuqurchaga" olib kelishi mumkin

A klinik ehtimollarni baholash yordamida Uells hisobi (quyidagi jadvaldagi ajratilgan ustunga qarang) potentsial DVT "ehtimol" yoki "ehtimol" emasligini aniqlash uchun diagnostika jarayonining birinchi bosqichi hisoblanadi. Bal birinchi tibbiy yordam va ambulatoriya sharoitida, shu jumladan birinchi pastki ekstremal DVT (hech qanday PE belgilarisiz) shubha qilinganida qo'llaniladi. favqulodda yordam bo'limi.[1][5] Raqamli natija (mumkin bo'lgan ball -2 dan 9 gacha) ko'pincha "mumkin emas" yoki "ehtimol" toifalarga bo'linadi.[1][5] Uellsning ikki yoki undan ko'p ball to'plashi DVTni "ehtimol" (taxminan 28% imkoniyat), undan past ball to'plaganlar esa DVTga ega bo'lishi "ehtimoldan yiroq" (taxminan 6% imkoniyat) deb hisoblanadi.[21] DVT bilan og'rigan bemorlarda tashxis salbiy D-dimer qon tekshiruvi bilan chiqarib tashlanadi.[1] DVT bilan kasallangan odamlarda, ultratovush standart hisoblanadi tasvirlash tashxisni tasdiqlash yoki chiqarib tashlash uchun ishlatiladi.[5] Bundan tashqari, DVT kasalligiga chalingan va dastlab DVTga ega bo'lishi mumkin emas deb tasniflangan, ammo D-dimer testi ijobiy bo'lgan kasalxonaga yotqizilgan bemorlar uchun tasvirlash zarur.[1]

Uells ballari DVT uchun ustun va eng ko'p o'rganilgan klinik bashorat qilish qoidasi bo'lsa-da,[21][86] uning kamchiliklari bor. Uells ballari muqobil tashxis qo'yish ehtimoli bo'yicha sub'ektiv baholashni talab qiladi va keksa yoshdagi va ilgari DVT bilan kasallanganlarda bu ko'rsatkich ancha past. The Gollandiyalik birlamchi tibbiy yordam qoidasi foydalanish uchun ham tasdiqlangan. U faqat ob'ektiv mezonlarni o'z ichiga oladi, ammo D-dimer qiymatini olishni talab qiladi.[87] Ushbu taxmin qoidasi bilan uch yoki undan kam ball odam DVT uchun past xavfni anglatadi. To'rt yoki undan ko'p ball natijasi ultratovushga ehtiyoj borligini ko'rsatadi.[87] Tajribali shifokorlar bashorat qilish qoidasini ishlatish o'rniga, klinik baholash va gestalt yordamida DVT ehtimolligini oldindan baholashlari mumkin, ammo bashorat qilish qoidalari ishonchliroqdir.[1]

MezonDVT uchun quduq ballari[men]Gollandiyalik birlamchi tibbiy yordam qoidasi
Aktiv saraton (oxirgi 6 oy ichida davolash yoki palyatif)+1 ball+1 ball
Buzoqning shishishi asemptomatik buzoq bilan taqqoslaganda ≥ 3 sm (pastda 10 sm) tibial tuberozlik )+1 ball+2 ball
Shishgan bir tomonlama yuzaki tomirlar (varikozsiz, simptomatik oyoqda)+1 ball+1 ball
Bir tomonlama chuqurlik shishishi (simptomatik oyoqda)+1 ball
Oldingi hujjatlashtirilgan DVT+1 ball
Butun oyoqning shishishi+1 ball
Chuqur venoz tizim bo'ylab mahalliylashtirilgan noziklik+1 ball
Falaj, parez, yoki pastki ekstremitalarning so'nggi gips immobilizatsiyasi+1 ball
Yaqinda rid 3 kun yotoqda yoki oxirgi 12 hafta ichida mintaqaviy yoki umumiy og'riqsizlantirishni talab qiladigan og'ir operatsiya+1 ball+1 ball
Hech bo'lmaganda ehtimoliy alternativ diagnostika−2 ball
Ijobiy D-dimer (≥ 0,5 mkg / ml yoki 1,7 nmol / L)+6 ball
Oyoq travmasının yo'qligi+1 ball
Erkak jinsi+1 ball
Og'iz kontratseptivlaridan foydalanish+1 ball[5][87]

Siqish chuqur tomir tromboziga shubha qilingan ultratovush tekshiruvi standart diagnostika usuli bo'lib, u dastlabki DVTni aniqlashda juda sezgir.[13] A siqishni ultratovush Oddiy siqilgan tomirlarning tomir devorlari yumshoq bosim ostida qulab tushmasa ijobiy hisoblanadi.[21] Ba'zida pıhtı vizualizatsiyasi mumkin, ammo talab qilinmaydi.[88] Uchta siqishni ultratovush tekshiruvi usulidan foydalanish mumkin, uchta usuldan ikkitasi bir necha kundan keyin tashxisni istisno qilish uchun ikkinchi ultratovush tekshiruvini talab qiladi.[13] Butun oyoq ultratovush - bu takroriy ultratovushni talab qilmaydigan variant,[13] ammo proksimal kompressiya ultratovush tekshiruvi tez-tez ishlatiladi, chunki distal DVT kamdan kam hollarda klinik ahamiyatga ega.[9] Ultratovush usullari, shu jumladan dupleks va rang oqimi Doppler quyqani yanada tavsiflash uchun ishlatilishi mumkin[9] va doppler ultratovush, ayniqsa siqilmaydigan yonbosh tomirlarida yordam beradi.[88]

Tomografiya tomografiyasi, MRI venografiyasi yoki kontrastli bo'lmagan MRI ham diagnostik imkoniyatlardir.[89] The oltin standart ko'rish usullarini baholash uchun qarama-qarshilik mavjud venografiya, ta'sirlangan a'zoning periferik venasini kontrastli vosita bilan yuborish va rentgen nurlarini olish, venoz ta'minotga to'siq qo'yilganligini aniqlashni o'z ichiga oladi. Uning narxi, invazivligi, mavjudligi va boshqa cheklovlari tufayli ushbu test kamdan-kam hollarda amalga oshiriladi.[21]

  • Chapdagi umumiy femoral venada qon pıhtısı ko'rinadigan ultratovush tekshiruvi. (Umumiy femoral tomir tashqi yonbosh venasi bilan distaldir.)

  • Doppler ultratovush tekshiruvi pıhtıdaki oqim va hiperekojenik tarkib yo'qligini ko'rsatib beradi femoral tomir (pastki qism deb nomlangan[j]) ning dallanma nuqtasiga distal chuqur femoral tomir. Ushbu pıhtı bilan taqqoslaganda, umumiy femoral tomirni to'sib qo'yadigan pıhtılar, oyoqning sezilarli darajada katta qismiga ta'sir qilishi tufayli yanada jiddiy ta'sir ko'rsatadi.[91]

  • Qorin bo'shlig'i tomografiyasi, tos suyagining o'ng umumiy yonbosh venasida qon quyilishi bilan, iliofemoral DVTni namoyish etadi.

Menejment

Agar tromblar proksimal, distal va simptomatik yoki yuqori ekstremal va simptomatik bo'lsa, DVTni davolash kafolatlanadi.[2] Antikoagulyatsiyani yoki qonni suyultiradigan dori-darmonlarni taqdim etish, bemorlarni tekshiruvdan o'tkazilgandan so'ng, ular duchor bo'lmasligini tekshirish uchun odatiy davolash usuli hisoblanadi. qon ketish.[2][k] Ammo davolanish DVT joylashuviga qarab farq qiladi. Masalan, izolyatsiya qilingan distal DVT holatlarida ultratovush nazorati (proksimal pıhtılaşma borligini tekshirish uchun 2 haftadan so'ng ikkinchi ultratovush tekshiruvi) ishlatilishi mumkin.[5][93] VTE qaytalanish xavfi yuqori bo'lgan izolyatsiya qilingan distal DVTga ega bo'lganlar odatda proksimal DVTga o'xshab antikoagulyatsiya qilinadi. Qayta tiklanish xavfi past bo'lganlar to'rt-olti haftalik antikoagulyatsiya kursini, past dozalarni yoki umuman antikoagulyatsiyani qabul qilishlari mumkin.[5] Aksincha, DVT proksimal bo'lganlar kamida 3 oylik antikoagulyatsiyani qabul qilishlari kerak.[5]

Ba'zi antikoagulyantlarni og'iz orqali qabul qilish mumkin va bu dorilarga kiradi varfarin (a vitamin K antagonisti ), rivaroksaban (a omil Xa inhibitori ), apiksaban (omil Xa inhibitori), dabigatran (a to'g'ridan-to'g'ri trombin inhibitori ) va edoxaban (omil Xa inhibitori).[2] Boshqa antikoagulyantlarni og'iz orqali qabul qilish mumkin emas. Bular parenteral (og'iz orqali qabul qilinmaydigan) dorilar kiradi past molekulyar og'irlikdagi geparin, fondaparinux va sintez qilinmagan geparin. Ba'zi bir og'iz dori-darmonlarni yolg'iz qabul qilish etarli, boshqalari esa qo'shimcha ravishda parenteral qonni suyultiruvchi vositadan foydalanishni talab qiladi. Rivaroksaban va apiksaban odatda birinchi darajali dorilar bo'lib, ular og'iz orqali qabul qilishda etarli.[18] Rivaroksaban kuniga bir marta, apiksaban esa kuniga ikki marta olinadi.[5] Varfarin, dabigatran va edoksaban parenteral antikoagulyantdan og'iz orqali antikoagulyant terapiyani boshlashni talab qiladi.[18][94] VTE davolash uchun varfarin boshlanganda, 5 kunlik parenteral antikoagulyant[l] warfarin bilan birga beriladi, undan keyin faqat terapiya qo'llaniladi.[16][17] Varfarin anni saqlash uchun olinadi xalqaro normallashtirilgan nisbat (INR) 2.0-3.0, maqsad sifatida 2.5 bo'lgan.[96] Varfarinni qabul qilishning foydasi davolanish davomiyligi pasayganda kamayadi,[97] va qon ketish xavfi yoshga qarab ortadi.[98] Birinchi darajali to'g'ridan-to'g'ri og'iz antikoagulyantlaridan foydalanilganda vaqti-vaqti bilan INR nazorati zarur emas. Umuman olganda, antikoagulyatsion terapiya murakkab va ko'plab holatlar ushbu terapiyani qanday boshqarilishiga ta'sir qilishi mumkin.[99]

Geparin
Fondaparinux
Geparinlar umurtqa pog'onasining strukturaviy namoyishlari (chap), ularning zanjiri kattaligi bilan farq qiladigan va sintetik pentasakarid (beshta shakar) fondaparinux (to'g'ri)

Antikoagulyatsion terapiyaning davomiyligi (u 4 haftadan 6 haftagacha davom etadimi, yo'qmi,[5] 6 dan 12 haftagacha, 3 oydan 6 oygacha,[18] yoki cheksiz) klinikaning asosiy omilidir Qaror qabul qilish.[100] Proksimal DVT jarrohlik yoki travma bilan qo'zg'atilganda, 3 oylik antikoagulyatsiya kursi standart hisoblanadi.[18] Agar birinchi VTE proksimal DVT bo'lsa, u asossiz yoki vaqtincha jarrohlik bo'lmagan xavf omili bilan bog'liq bo'lsa, 3 oydan 6 oygacha bo'lgan past dozali antikoagulyatsiya qo'llanilishi mumkin.[18] VTE ning yillik xavfi 9% dan yuqori bo'lganlarda, masalan, asossiz epizoddan keyin, antikoagulyatsiya kengayishi mumkin.[101] D-dimer darajasining ko'tarilishi bilan idyopatik VTE dan keyin varfarin bilan davolashni tugatganlar takroriy VTE xavfini oshiradi (normal natijalar uchun taxminan 9% va taxminan 4%) va bu natijadan klinik qarorlarni qabul qilishda foydalanish mumkin.[102] Trombofiliya test natijalari kamdan-kam davolanish muddatida rol o'ynaydi.[48]

Oyoqning o'tkir DVT kasalligini davolash kasalxonaga yotqizilish o'rniga uyda davom etishi mumkin. Bu shaxslar bunga tayyorligini his qilganda va oyoqning og'ir alomatlari bo'lganlarda qo'llaniladi qo'shma kasalliklar saralashga qodir emas. Uy sharoitida tegishli sharoitlar kutilmoqda: agar kerak bo'lsa kasalxonaga tezda qaytish, oila a'zolari yoki do'stlari tomonidan qo'llab-quvvatlash va telefonga kirish.[103] Kuchli og'riq yoki shish paydo bo'lmaganlarga yurish tavsiya etiladi.[104] Bitirgan siqish paypoqlari, ular oyoq Bilagi zo'rlikda va tizzadan pastroq bosim o'tkazadi[95] o'tkir DVT belgilarini simptomatik boshqarish uchun tekshirilishi mumkin, ammo ular xavfini kamaytirish uchun tavsiya etilmaydi post-trombotik sindrom,[94] chunki ularni ushbu maqsad uchun ishlatishning potentsial foydasi "noaniq bo'lishi mumkin".[5] Shuningdek, siqilgan paypoqlar VTE takrorlanishini kamaytirmaydi.[105] Biroq, ular distal DVT bilan ta'minlanganlarda tavsiya etiladi.[5]

Saraton kasalligini tekshirish

Shubhasiz VTE noma'lum saraton kasalligini ko'rsatishi mumkin, chunki bu 10 foizgacha sabab bo'lmagan holatlar.[1] To'liq klinik baholash zarur va u quyidagilarni o'z ichiga olishi kerak fizik tekshiruv, sharh kasallik tarixi va universal saraton tekshiruvi o'sha yoshdagi odamlarda amalga oshiriladi.[18][106] Oldingi tasvirlarni ko'rib chiqish, shu jumladan, "qon testining dastlabki natijalarini ko'rib chiqish kabi foydali hisoblanadi to'liq qon ro'yxati, buyrak va jigar funktsiyasi, PT va APTT."[106] Amalga oshirish tavsiya etilmaydi o'simta belgilari yoki a Qorin va tos suyagi tomografiyasi asemptomatik odamlarda.[1] Yaxshi tegishli tekshiruv belgilari yoki alomatlari bo'lmaganlarda qo'shimcha tekshiruvlar asossiz o'tkazilishini tavsiya qiladi.[106]

Aralashuvlar

Tromboliz qon quyqalarini eritib yuborish uchun tomirlarga ferment yuborish va bu davolash hayot uchun xavfli bo'lgan favqulodda qon tomirlari va yurak xurujlari, tasodifiy boshqariladigan sinovlarga qarshi samarali ekanligi isbotlangan.[107][108][109] O'tkir proksimal DVT bilan kasallanganlarda aniq foyda o'rnatmagan.[5][110] Kamchiliklari kateterga yo'naltirilgan tromboliz (pıhtılaşan fermentni boshqarishning afzal usuli[5]) qon ketish xavfi, murakkablik,[m] va protsedura narxi.[94] Shunday qilib, antikoagulyatsiya DVT uchun eng maqbul davolash usuli hisoblanadi.[94] Ammo, bu imtiyoz DVT bilan kasallanganlarga nisbatan tatbiq etilmaydi, shunda "yaqinlashib kelayotgan venoz gangrena" mavjud.[94] 2016 yildan boshlab kateterga yo'naltirilgan tromboz uchun eng yaxshi nomzodlar deb hisoblanuvchilar iliofemoral DVT, simptomlari 14 kundan kam, yaxshi funktsional holatga ega (o'z qobiliyatini bajarish qobiliyati) kundalik hayot faoliyati ), kamida 1 yil umr ko'rish va qon ketish xavfi past.[111][yangilanishga muhtoj ][94] Shunisi e'tiborga loyiqki, turli xil trombolizga qarshi ko'rsatmalar mavjud.[94] Iliofemoral DVTga qarshi kateterga yo'naltirilgan tromboliz, taxminan 138000 AQSh dollari miqdoridagi iqtisodiy samaradorlik darajasida post-trombotik sindromning og'irligini pasayishi bilan bog'liq.[n] har bir daromad uchun QALY.[112][113] Flegmasiya cerulea dolens (pastki chap rasm) kateterga yo'naltirilgan tromboliz bilan davolash mumkin.[18] Agar o'tkir holatida bo'lsa bo'lim sindromi, shoshilinch fassiotomiya kafolatlangan.[114]

IVC filtri

An joylashishi pastki vena kava filtri (IVC filtri) - bu davolanishning mumkin bo'lgan variantidir, agar o'tkir DVT, antikoagulyatsiya uchun standart davolash bo'lsa mutlaqo kontrendikedir (mumkin emas), yoki agar kimdir antikoagulyatsiyaga qaramay PE rivojlansa.[106] Biroq, 2020 yilgi NICE sharhida ulardan foydalanish uchun "ozgina yaxshi dalillar" topildi.[106] 2018 yilda o'tkazilgan IVC filtri joylashuvi PEning 50% kamayishi, DVT ning 70% o'sishi va 30 kunlik o'limning 18% ga ko'payishi bilan bog'liq.[1][116] Shunday qilib, agar kimdir antikoagulyatsiyaga qaramasdan PEni rivojlantirsa, IVC filtrini joylashtirishdan oldin antikoagulyatsion davolanishni optimallashtirish va shu bilan bog'liq boshqa muammolarni hal qilish uchun ehtiyot bo'lish kerak.[106]

Mexanik trombektomiya vositasi venoz pıhtılarni olib tashlashi mumkin, ammo ACCP buni quyidagi shartlar mavjud bo'lganda tanlaydi: "iliofemoral DVT, semptomlar <7 kun (bitta randomizatsiyalangan tekshiruvda ishlatiladigan mezon), yaxshi funktsional holat, umr ko'rish davomiyligi ≥ 1 yil, va ikkala resurs va tajriba mavjud. "[95] Trombektomiya orqali faqat antikoagulyatsiya taklif etiladi.[117]

Oldini olish

Uchun qon pıhtılarının oldini olish umumiy populyatsiyada oyoq mashqlarini kiritish va soatlab o'tirganda yurish, faol hayot tarziga ega bo'lish va tana vaznini sog'lom saqlash tavsiya etiladi.[6] Yurish oyoq tomirlari orqali qon oqimini oshiradi.[118] Tana vaznining ko'pligi, aksariyat xavf omillaridan farqli o'laroq o'zgarishi mumkin va ortiqcha vazn yoki semirib ketgan odamga yordam beradigan aralashuvlar yoki turmush tarzini o'zgartirish. vazn yo `qotish DVT xavfini kamaytirish.[39] Statinlar tekshirildi birlamchi profilaktika, va YUPITER sinovi, ishlatilgan rosuvastatin, samaradorlikning taxminiy dalillarini keltirdi.[10][119] O'rganilgan barcha statinlar orasida rosuvastatin VTE xavfini kamaytiradigan yagona narsa bo'lib ko'rinadi.[120] Biroq, davolash uchun zarur bo'lgan raqam bitta boshlang'ich VTE ning oldini olish uchun uning qo'llanilishi cheklanib, taxminan 2000 ga teng.[121]

VTE-dan keyin

Qon ketish xavfini oshiradigan antikoagulyatsiya, ba'zida takrorlanish xavfi yuqori bo'lganlarda abadiy qo'llaniladi (umrbod davolash). Uzoq muddatli antikoagulyatsiya bilan katta qon ketish xavfi yiliga taxminan 3% ni tashkil qiladi,[40] va yillik VTE xavfi uzoq muddatli antikoagulyatsiyani kafolatlaydi deb hisoblanadigan nuqta 3 dan 9% gacha baholanadi.[101] Odatda, jismoniy shaxslar yillik VTE xavfidan 9% dan oshganda, uzoq muddatli antikoagulyatsiya odatiy hisoblanadi.[101] Masalan, antitrombin etishmovchiligi, kuchli yoki o'rtacha darajada kuchli xavf omili, VTE yillik xavfini atigi 0,8-1,5% tashkil qiladi;[40] trombofili bo'lgan asemptomatik odamlar uzoq muddatli antikoagulyatsiyani kafolatlamaydilar.[122] Agar kimdir umrbod antikoagulyatsiya o'rniga, sababsiz VTE dan keyin antikoagulyatsiyani to'xtatishga qaror qilsa, takroriy takrorlanish xavfini kamaytirish uchun aspirin ishlatilishi mumkin,[123] ammo VTE ning oldini olishda antikoagulyatsiyaga qaraganda samarasi kam.[iqtibos kerak ][miqdorini aniqlash ] Statinlar, shuningdek, takroriy VTE stavkalarini pasaytirish potentsiali uchun tekshirildi, ba'zi tadqiqotlar samaradorligini ko'rsatmoqda.[124]

Kasalxona (jarrohlik bo'lmagan) bemorlar

Kam molekulyar og'irlikdagi geparin odatda ushbu rangli joylarning teri ostiga igna bilan teri ostiga in'ektsiya yo'li bilan yuboriladi.

O'tkir kasal kasalxonaga yotqizilgan bemorlarga parenteral antikoagulyantni qabul qilish tavsiya etiladi, ammo ularning aniq foydasi noaniq.[29] Kasalxonada og'ir ahvolda bo'lgan bemorlarga yuqorida aytib o'tilgan dori-darmonlarning o'rniga sintez qilinmagan geparin yoki past molekulyar og'irlikdagi geparinni berish tavsiya etiladi.[29]

Jarrohlikdan keyin

Tugatish uchun kesma tizzalarini almashtirish operatsiyasi, DVT shakllanishini tezlashtirishi mumkin bo'lgan protsedura

Katta ortopedik jarrohlik -umumiy kestirib almashtirish, umumiy tizzani almashtirish, yoki kestirib, sinishi bo'yicha operatsiya - VTE ni keltirib chiqarish xavfi yuqori.[125] Agar ushbu operatsiyalardan keyin profilaktika qo'llanilmasa, simptomatik VTE 35 kun ichida rivojlanish ehtimoli taxminan 4% ni tashkil qiladi.[126] Kuchli ortopedik jarrohlik amaliyotidan so'ng, qonni suyultiruvchi yoki aspirin bilan odatda qo'shiladi vaqti-vaqti bilan pnevmatik siqish, bu tugallangan siqish paypog'idan afzal qilingan mexanik profilaktika.[7]

Ortopedik bo'lmagan jarrohlik amaliyotidan so'ng odamlarda VTE profilaktikasi variantlari orasida VTE xavfi, katta qon ketish xavfi va odamga qarab erta yurish, mexanik profilaktika va qonni suyultiruvchi vositalar (past molekulyar og'irlikdagi geparin va past dozada fraktsion bo'lmagan geparin) mavjud. afzalliklar.[127] Kam xavfli operatsiyalardan so'ng, erta va tez-tez yurish eng yaxshi profilaktika chorasi hisoblanadi.[7]

Homiladorlik

VTE xavfi homiladorlikda homiladorlikda taxminan besh baravar ko'payadi[40][128] giperkoagulyatsiyalanadigan holat tufayli, o'limga qarshi moslashish tug'ruqdan keyingi qon ketish.[129] Bundan tashqari, genetik xavf omillari bo'lgan homilador ayollar VTE uchun tahminan uchdan 30 martagacha ko'payadi.[130] Giperkoagulyatsiyali ayollarda homiladorlik bilan bog'liq VTE uchun profilaktika muolajalari 2012 yilda ACCP tomonidan taklif qilingan. Gomozigot oilaviy tarixi VTE bo'lgan V Leyden yoki protrombin G20210A omillarini tashuvchilar taklif qilingan tug'ruqdan oldin LMWH va LMWH yoki a vitamin K antagonisti (VKA) tug'ruqdan keyingi olti hafta davomida. Boshqa trombofili va oilaviy tarixga ega bo'lganlar, ammo ilgari VTEga ega bo'lmaganlar hushyor kutish homiladorlik va LMWH paytida yoki - S yoki S oqsil etishmovchiligi bo'lganlar uchun - VKA. Shaxsiy va oilaviy tarixga ega bo'lmagan V Leyden faktori yoki protrombin G20210A gomozigot tashuvchilari homiladorlik paytida ehtiyotkorlik bilan kutish va LMWH yoki VKA tug'ilgandan keyin olti hafta davomida tavsiya etilgan. Boshqa trombofili bilan og'rigan, ammo oilasi yoki VTE ning shaxsiy tarixi bo'lmaganlar faqat ehtiyotkorlik bilan kutish uchun taklif qilingan.[131] Warfarin, oddiy VKA, homilaga zarar etkazishi mumkin va homiladorlik paytida VTE oldini olish uchun ishlatilmaydi.[130][132]

Sayohatchilar

Siqilgan paypoqqa misol

Xavf ostida bo'lgan uzoq muddatli sayohatchilar uchun takliflar[o] yurishni osonlashtirish uchun buzoq mashqlari, tez-tez yurish va samolyotlarda yo'lakka o'tirish kiradi.[133][134] Bitirilgan kompressor paypoqlari aviakompaniyada yo'lovchilarda asemptomatik DVT darajasini keskin pasaytirdi, ammo simptomatik DVT, PE yoki o'limga ta'siri noma'lum, chunki o'rganilgan shaxslarning hech biri ushbu natijalarni ishlab chiqmagan.[135] Biroq, VTE uchun xavf omillari bo'lmagan uzoq masofali sayohatchilar uchun (> 4 soat) tugatilgan siqish paypoqlari tavsiya etilmaydi. Xuddi shu tarzda, uzoq muddatli sayohatni amalga oshiradigan umumiy aholi orasida aspirin va antikoagulyantlar taklif qilinmaydi.[29] Muhim VTE xavf omillariga ega bo'lganlar[p] uzoq masofalarga sayohat qilish, VTE ning oldini olish uchun tugatilgan siqish paypoqlaridan yoki LMWH dan foydalanish tavsiya etiladi. Agar ushbu ikki usulning ikkalasi ham mumkin bo'lmasa, u holda aspirin tavsiya etiladi.[29]

Prognoz

DVT ko'pincha qariyalar uylari, kasalxonalar va faol saraton sharoitida yuzaga keladigan keksa yoshdagi kasallikdir.[3] Bu 30 kunlik bilan bog'liq o'lim darajasi taxminan 6% ni tashkil etadi, chunki PE bu o'limlarning ko'pchiligiga sabab bo'ladi.[1] Proximal DVT is frequently associated with PE, unlike distal DVT, which is rarely if ever associated with PE.[21] Around 56% of those with proximal DVT also have PE, although a chest CT is not needed simply because of the presence of DVT.[1] If proximal DVT is left untreated, in the following 3 months approximately half of people will experience symptomatic PE.[8]

Another frequent complication of proximal DVT, and the most frequent chronic complication, is post-trombotik sindrom, where individuals have chronic venous symptoms.[5] Symptoms can include pain, itching, swelling, paresthesia, a sensation of heaviness, and in severe cases, leg ulcers.[5] After proximal DVT, an estimated 20–50% of people develop the syndrome, with 5–10% experiencing severe symptoms.[136] Post-thrombotic syndrome can also be a complication of distal DVT, though to a lesser extent than with proximal DVT.[137]

Recurrence of DVT is another potential consequence. In the 10 years following an initial VTE, about 30% of people will have a recurrence.[138][3] VTE recurrence in those with prior DVT is more likely to recur as DVT than PE.[139] Saraton[5] and unprovoked DVT are strong risk factors for recurrence.[27] After initial proximal unprovoked DVT with and without PE, 16–17% of people will have recurrent VTE in the 2 years after they complete their course of anticoagulants. VTE recurrence is less common in distal DVT than proximal DVT.[140] In upper extremity DVT, annual VTE recurrence is about 2–4%.[98] After surgery, a provoked proximal DVT or PE has an annual recurrence rate of only 0.7%.[27]

Epidemiologiya

About 1.5 out of 1000 adults a year have a first VTE in high-income countries,[141][142] and about 5–11% of people will develop VTE in their lifetime.[12][13] VTE becomes much more common with age.[12] VTE rarely occurs in children, but when it does, it predominantly affects hospitalized children.[143] Children in North America and the Netherlands have VTE rates that range from 0.07 to 0.49 out of 10,000 children annually.[143] Meanwhile, almost 1% of those aged 85 and above experience VTE each year.[3] About 60% of all VTEs occur in those 70 years of age or older,[8] and those aged 65 and above are subject to about a 15 times higher risk than those aged 40 and below.[14] Incidence is about 18% higher in males than in females.[4] VTE occurs in association with hospitalization or nursing home residence about 60% of the time, active cancer about 20% of the time, and a central venous catheter or transvenous pacemaker about 9% of the time.[3]

During pregnancy and after childbirth, acute VTE occurs about 1.2 of 1000 deliveries. Despite it being relatively rare, it is a leading cause of maternal morbidity and mortality.[144] After surgery with preventive treatment, VTE develops in about 10 of 1000 people after total or partial knee replacement, and in about 5 of 1000 after total or partial hip replacement.[145] About 400,000 Americans develop an initial VTE each year, with 100,000 deaths or more attributable to PE.[142] In England, an estimated 25,000 a year die from hospital-related VTE.[146] Asian and Hispanic individuals have a lower VTE risk than whites or Blacks.[4]

In North American and European populations, around 4–8% of people have a thrombophilia,[40] most commonly factor V leiden and prothrombin G20210A. For populations in China, Japan, and Thailand, deficiences in protein S, protein C, and antithrombin predominate.[147] Non-O blood type is present in around 50% of the general population and varies with ethnicity, and it is present in about 70% of those with VTE.[41][148] Altogether, global data is incomplete,[149] and as of 2011, available data was dominated by North American and European populations.[15]

DVT occurs in the upper extremities in about 4–10% of cases,[11] with an incidence of 0.4–1.0 people out of 10,000 a year.[5] A minority of upper extremity DVTs are due to Paget–Schroetter syndrome, also called effort thrombosis, which occurs in 1–2 people out of 100,000 a year, usually in athletic males around 30 years of age or in those who do significant amounts of overhead manual labor.[34][115]

Ijtimoiy

Serena Uilyams has spoken at length about a frightening encounter she had with VTE while she was hospitalized in 2017.[150]

Being on blood thinners because of DVT can be life-changing because it may prevent lifestyle activities such as contact or winter sports to prevent bleeding after potential injuries.[151] Head injuries prompting brain bleeds are of particular concern. This has caused NASCAR driver Brayan Vikers to forego participation in races. Professional basketball players including NBA players Kris Bosh and hall of famer Hakeem Olajuwon have dealt with recurrent blood clots,[152] and Bosh's career was significantly hampered by DVT and PE.[153]

Tennis star Serena Uilyams was hospitalized in 2011 for PE thought to have originated from DVT.[154] Years later, in 2017, due to her knowledge of DVT and PE, Serena accurately advocated for herself to have a PE diagnosed and treated. During this encounter with VTE, she was hospitalized after a C bo'limi surgery and was off of blood thinners. After feeling the sudden onset of a PE symptom, shortness of breath, she told her nurse and requested a CT scan and an IV heparin drip, all while gasping for air. She started to receive an ultrasound to look for DVT in the legs, prompting her to express dissatisfaction to the medical staff that they were not looking for clots where she had symptoms (her lungs), and they were not yet treating her presumed PE. After being diagnosed with PE and not DVT, and after receiving heparin by IV, the coughing from the PE caused her C-section surgical site to open and the heparin contributed to bleeding at the site. Serena later received an IVC filter while in the hospital.[150]

Other notable people have been affected by DVT. AQShning sobiq prezidenti Richard Nikson had recurrent DVT,[155] and so has former Secretary of State Hillari Klinton. She was first diagnosed while Birinchi xonim in 1998 and again in 2009.[156] Dik Cheyni was diagnosed with an episode while Vitse prezident,[157] va teledasturlar boshlovchisi Regis Filbin had DVT after hip-replacement surgery.[158] DVT has also contributed to the deaths of famous people. For example, DVT and PE played a role in rapper Og'ir D 's death at age 44.[159] NBC jurnalisti David Bloom died at age 39 while covering the Iraq War from a PE that was thought to have progressed from a missed DVT.[160] And actor Jimmi Styuart had DVT that progressed to a PE and triggered a fatal heart attack when he was 89.[158][161]

Field of medicine

Patients with a history of DVT might be managed by primary care, umumiy ichki kasalliklar, gematologiya, kardiologiya, qon tomir jarrohlik, yoki vascular medicine.[162] Patients suspected of having an acute DVT are often referred to the emergency department for evaluation.[163] Interventsion rentgenologiya is the specialty that typically places and retrieves IVC filters,[164] and vascular surgery might do catheter directed thrombosis for some severe DVTs.[115]

Tarix

Rudolf Virchow
Warfarin, a common vitamin K antagonist, was the mainstay of pharmocological treatment for about 50 years.

Kitob Sushruta Samhita, an Ayurveda text published around 600–900 BC, contains what has been cited as the first description of DVT.[165] In 1271, DVT symptoms in the leg of a 20-year-old male were described in a French manuscript, which has been cited as the first case or the first Western reference to DVT.[165][166]

In 1856, German physician and pathologist Rudolf Virchow published his analysis after the insertion of foreign bodies into the jugular veins of dogs, which migrated to the pulmonary arteries. These foreign bodies caused pulmonary emboli, and Virchow was focused on explaining their consequences.[167] He cited three factors, which are now understood as hypercoaguability, stasis, and endothelial injury.[168] It was not until 1950 that this framework was cited as Virchow's triad,[167] but the teaching of Virchow's triad has continued in light of its utility as a theoretical framework and as a recognition of the significant progress Virchow made in expanding the understanding of VTE.[167][168]

Methods to observe DVT by ultrasound were established in the 1960s.[89] Diagnoses were commonly performed by impedans pletizmografiyasi 1970-80 yillarda,[169] but ultrasound, particularly after utility of probe compression was demonstrated in 1986, became the preferred diagnostic method.[165] Yet, in the mid 1990s, contrast venography and impedance plethysmography were still described as common.[170]

Multiple pharmacological therapies for DVT were introduced in the 20th century: oral anticoagulants in the 1940s, subcutaneous injections of LDUH in 1962 and subcutaneous injections of LMWH in 1982.[171] For around 50 years, a months-long warfarin (Coumadin) regimen was the mainstay of pharmacological treatment.[172][173] To avoid the blood monitoring required with warfarin and the injections required by heparin and heparin-like medicines, a new generation of oral anticoagulant pills that do not require blood monitoring has sought to replace these traditional anticoagulants.[173] 2000-yillarning oxiri - 2010-yillarning boshlarida, to'g'ridan-to'g'ri og'iz antikoagulyantlari - shu jumladan rivaroksaban (Xarelto), apiksaban (Eliquis), and dabigatran (Pradaxa)—came to the market, making this field of medicine fast changing.[27] The New York Times described a "furious battle" among the three makers of these drugs "for the prescription pads of doctors".[172]

Iqtisodiyot

Initial DVT costs for an average hospitalized patient in the U.S. are around $7,700–$10,800.[174] VTE follow-up costs at three months, six months, and a year are about $5,000, $10,000, and $33,000 respectively; in Europe, the three and six-month figures are about 1,800 and €3,200.[175] Post-thrombotic syndrome is a significant contributor to DVT follow-up costs.[174] Annual DVT costs in the U.S. are an estimated $5 billion[176] or in excess of $8 billion,[177][178] and the average annual cost per treated individual is thought to be about $20,000.[177] As an example, if 300,000 symptomatic DVT patients were treated at costs averaging $20,000 annually, that would cost $6 billion a year.

Research directions

2019 yilda nashr etilgan tadqiqot Tabiat genetikasi reported more than doubling the known genetic lokuslar associated with VTE.[10] In their updated 2018 clinical practice guidelines, the American Society of Hematology identified 29 separate research priorities, most of which related to patients who are acutely or critically ill.[29] Inhibition of Factor XI, P-selectin, Elektron tanlov, and a reduction in formation of neutrophil extracellular traps are potential therapies that might treat VTE without increasing bleeding risk.[179]

Shuningdek qarang

Izohlar

  1. ^ Thrombosis associated with the head (cerebral venous sinus thrombosis ) and the abdominal organs (ichki organlar )-kabi portal tomir trombozi, buyrak venalari trombozi va Budd-Chiari sindromi —are separate diseases excluded from the scope of this definition.
  2. ^ Third-generation estrodiol kontratseptiv vositalar (COCs) have an approximate two to three times higher risk than second-generation COCs.[30] Progestogen-only pill use is not associated with increased VTE risk.[38]
  3. ^ I toifa[12]
  4. ^ "It is important to note that smoking is not an independent risk factor, although it increases the risk for cancers and other comorbidities and works synergistically with other independent risk factors."[58]
  5. ^ The term 'thrombophilia' as used here applies to the five inherited abnormalities of antithrombin, protein C, protein S, factor V, and prothrombin, as is done elsewhere.[40][60]
  6. ^ Cerulea is from Latin, and denotes a bluish color, as does the related English word serulean.
  7. ^ VTE might cause the observed inflammation.[24]
  8. ^ An elevated level is greater than 250 ng /mL D-dimer units (DDU) or greater than 0.5 mg /mL fibrinogen equivalent units (FEU). A normal level is below these values.[84]
  9. ^ The Wells score as displayed here is the more recent modified score, which added a criteron for a previous documented DVT and increased the time range after a surgery to 12 weeks from 4 weeks.[9]
  10. ^ (Subsartorial is a proposed name for a section of the femoral vein.)[90]
  11. ^ Evidence for anticoagulation comes from studies other than definitive randomizatsiyalangan boshqariladigan sinovlar that demonstrate samaradorlik and safety for anticoagulation vs. placebo or using NSAID.[92]
  12. ^ The international normalized ratio should be ≥ 2.0 for 24 hours minimum,[17] but if the ratio is > 3.0, then the parenteral anticoagulant is not needed for five days.[95]
  13. ^ "Up to 83% of patients treated by any catheter-based therapy, need adjunctive angioplasty, and stenting".[5]
  14. ^ Estimated in United States dollars, estimate published in 2019
  15. ^ Specified as those with "previous VTE, recent surgery or trauma, active malignancy, pregnancy, estrogen use, advanced age, limited mobility, severe obesity, or known thrombophilic disorder"
  16. ^ For example "recent surgery, history of VTE, postpartum women, active malignancy, or ≥2 risk factors, including combinations of the above with hormone replacement therapy, obesity, or pregnancy"[29]

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