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HIV Drug Resistance in Newly Diagnosed Young Children in the Western Cape, South Africa

母乳喂养 杜鲁特格拉维尔 医学 抗药性 养生 逆转录酶抑制剂 病毒学 艾滋病毒耐药性 阿巴卡韦 逆转录酶 传输(电信) 儿科 病毒载量 内科学 生物 聚合酶链反应 病毒 抗逆转录病毒疗法 遗传学 基因 电气工程 工程类
作者
Kim Anderson,Gert U. van Zyl,Marvin Hsiao,Mathilda Claassen,Vanessa Mudaly,Jacqueline Voget,Alexa Heekes,Emma Kalk,Florence Phelanyane,Andrew Boulle,Gayathri Sridhar,Leigh Ragone,Vani Vannappagari,Mary‐Ann Davies
出处
期刊:Pediatric Infectious Disease Journal [Ovid Technologies (Wolters Kluwer)]
标识
DOI:10.1097/inf.0000000000004482
摘要

Background: Pretreatment of HIV drug resistance among children living with HIV (CLHIV) can compromise antiretroviral therapy (ART) effectiveness. Resistance may be transmitted directly from mothers or acquired following exposure to antiretrovirals consumed through breastfeeding or administered as prophylaxis. Methods: We performed resistance testing in children aged <3 years, newly diagnosed with HIV in Western Cape, South Africa (2021–2022), who either (1) acquired HIV via possible breastfeeding transmission from mothers who received ART (any regimen) during pregnancy/postpartum and/or (2) were exposed to protease inhibitors or integrase strand transfer inhibitors (INSTIs) in utero. Possible breastfeeding transmission was defined as testing HIV-polymerase chain reaction positive at age >28 days, after previously testing negative. We used surveillance drug–resistance mutation lists to define mutations. Results: We included 135 CLHIV. Most mothers started ART prepregnancy (73%). Overall, 57% (77/135) of children had resistance mutations detected. Nonnucleoside reverse transcriptase inhibitor–associated, nucleoside reverse transcriptase inhibitor–associated, protease inhibitor–associated and INSTI-associated mutations were found in 55% (74/135), 10% (13/135), <1% (1/135) and <1% (1/122) of children tested, respectively. One child with breastfeeding transmission had high-level INSTI resistance detected at HIV diagnosis, aged 18 months (E138K and G118R mutations). Conclusions: Although not clinically relevant, nonnucleoside reverse transcriptase inhibitor–associated mutations were common. Dolutegravir is currently the preferred first-line treatment for adults and CLHIV age ≥4 weeks, and although very low INSTI resistance levels have been observed in adults, limited data exist on genotyping the integrase region in children. Pretreatment INSTI resistance in children is likely to be unusual, but future surveillance, including longitudinal studies with paired mother-child resistance testing, is needed.

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