Laboratoire de Virologie, Hôpital Européen Georges Pompidou, Paris, France.
Ecole Doctorale (ED562) Bio Sorbonne Paris Cité (BioSPC), Université Paris Descartes, Paris, France.
J Antimicrob Chemother. 2019 Jul 1;74(7):2030-2038. doi: 10.1093/jac/dkz099.
The predictive efficacy of integrase (IN) strand transfer inhibitors (INSTIs) was investigated in HIV-infected children born to HIV-infected mothers in Africa.
Plasma was collected at the Complexe Pédiatrique of Bangui, Central African Republic, from INSTI-naive children (n = 8) and adolescents (n = 10) in virological failure (viral load >1000 copies/mL) after 5 years of first- and/or second-line combination ART (cART). IN, reverse transcriptase (RT) and protease (P) genes were genotyped and drug resistance mutations (DRMs) to INSTIs, NRTIs, NNRTIs and PIs were interpreted using the Stanford algorithm.
Successful IN, RT and P genotypes were obtained for 18, 13 and 15 children (median age 11 years, range 5-18; 8 were female), respectively. Two (2/18; 11.1%) viruses from children treated with a first-line regimen had INSTI DRMs at codon 138 (E138K and E138T), which is known to harbour major resistance mutations, and also had the accessory mutations L74I, G140K, G140R and G163R. The majority (16/18; 88.9%) of HIV-1 IN sequences demonstrated full susceptibility to all major INSTIs with a high frequency of natural polymorphic mutations. Most (12/15; 80%) genotyped viruses harboured at least one major DRM conferring resistance to at least one of the WHO-recommended antiretroviral drugs (NNRTIs, NRTIs and PIs) prescribed in first- and second-line regimens.
INSTIs could be proposed in first-line regimens in the majority of African children or adolescents and may constitute relevant therapeutic alternatives as second- and third-line cART regimens in HIV-infected children and adolescents living in sub-Saharan Africa.
研究整合酶(IN) strand transfer 抑制剂(INSTIs)在非洲感染 HIV 的母亲所生的 HIV 感染儿童中的预测疗效。
在中非共和国班吉综合儿科中心,对 8 名接受 INSTI 治疗的儿童(年龄 5-18 岁,中位年龄 11 岁)和 10 名青少年(年龄 5-18 岁,中位年龄 11 岁)进行了研究,这些儿童在接受一线和/或二线联合抗逆转录病毒治疗(cART)5 年后出现病毒学失败(病毒载量>1000 拷贝/mL)。采用斯坦福算法对 IN、逆转录酶(RT)和蛋白酶(P)基因进行了基因分型,并对 INSTIs、NRTIs、NNRTIs 和 PIs 的耐药突变(DRMs)进行了药物解读。
成功获得了 18 名儿童的 IN、RT 和 P 基因型(中位年龄 11 岁,范围 5-18 岁;8 名女性)。一线治疗方案中,2 种(2/18;11.1%)病毒在密码子 138 处(E138K 和 E138T)存在 INSTI DRMs,该位置存在主要耐药突变,此外还存在辅助突变 L74I、G140K、G140R 和 G163R。大多数(16/18;88.9%)HIV-1 IN 序列对所有主要 INSTIs 均表现出完全敏感性,且存在高频的天然多态性突变。大多数(12/15;80%)基因分型的病毒至少携带一种主要的 DRMs,对一线和二线方案中推荐的抗逆转录病毒药物(NNRTIs、NRTIs 和 PIs)中的至少一种具有耐药性。
INSTIs 可作为一线方案中的推荐药物,在非洲大多数儿童或青少年中使用,也可作为生活在撒哈拉以南非洲地区的 HIV 感染儿童和青少年的二线和三线 cART 方案的替代药物。
