随机分组在较低与较高RNA阈值时切换治疗的儿童中HIV-1耐药性及二线治疗情况
HIV-1 Drug Resistance and Second-Line Treatment in Children Randomized to Switch at Low Versus Higher RNA Thresholds.
作者信息
Harrison Linda, Melvin Ann, Fiscus Susan, Saidi Yacine, Nastouli Eleni, Harper Lynda, Compagnucci Alexandra, Babiker Abdel, McKinney Ross, Gibb Diana, Tudor-Williams Gareth
机构信息
*Center for Biostatistics in AIDS Research, Harvard T.H. Chan School of Public Health, Boston, MA; †Seattle Children's Hospital, Seattle, WA; ‡School of Medicine, University of North Carolina at Chapel Hill, Chapel Hill, NC; §INSERM, SC10-US019, Paris, France; ‖University College London Hospitals, University College London, London, United Kingdom; ¶Medical Research Council Clinical Trials Unit, University College London, London, United Kingdom; #Duke University Medical Center, Durham, NC; and **Imperial College London, London, United Kingdom.
出版信息
J Acquir Immune Defic Syndr. 2015 Sep 1;70(1):42-53. doi: 10.1097/QAI.0000000000000671.
BACKGROUND
The PENPACT-1 trial compared virologic thresholds to determine when to switch to second-line antiretroviral therapy (ART). Using PENPACT-1 data, we aimed to describe HIV-1 drug resistance accumulation on first-line ART by virologic threshold.
METHODS
PENPACT-1 had a 2 × 2 factorial design, randomizing HIV-infected children to start protease inhibitor (PI) versus nonnucleoside reverse transcriptase inhibitor (NNRTI)-based ART, and switch at a 1000 copies/mL versus 30,000 copies/mL threshold. Switch criteria were not achieving the threshold by week 24, confirmed rebound above the threshold thereafter, or Center for Disease Control and Prevention stage C event. Resistance tests were performed on samples ≥1000 copies/mL before switch, resuppression, and at 4-years/trial end.
RESULTS
Sixty-seven children started PI-based ART and were randomized to switch at 1000 copies/mL (PI-1000), 64 PIs and 30,000 copies/mL (PI-30,000), 67 NNRTIs and 1000 copies/mL (NNRTI-1000), and 65 NNRTI and 30,000 copies/mL (NNRTI-30,000). Ninety-four (36%) children reached the 1000 copies/mL switch criteria during 5-year follow-up. In 30,000 copies/mL threshold arms, median time from 1000 to 30,000 copies/mL switch criteria was 58 (PI) versus 80 (NNRTI) weeks (P = 0.81). In NNRTI-30,000, more nucleoside reverse transcriptase inhibitor (NRTI) resistance mutations accumulated than other groups. NNRTI mutations were selected before switching at 1000 copies/mL (23% NNRTI-1000, 27% NNRTI-30,000). Sixty-two children started abacavir + lamivudine, 166 lamivudine + zidovudine or stavudine, and 35 other NRTIs. The abacavir + lamivudine group acquired fewest NRTI mutations. Of 60 switched to second-line, 79% PI-1000, 63% PI-30,000, 64% NNRTI-1000, and 100% NNRTI-30,000 were <400 copies/mL 24 weeks later.
CONCLUSIONS
Children on first-line NNRTI-based ART who were randomized to switch at a higher virologic threshold developed the most resistance, yet resuppressed on second-line. An abacavir + lamivudine NRTI combination seemed protective against development of NRTI resistance.
背景
PENPACT - 1试验比较了病毒学阈值,以确定何时切换至二线抗逆转录病毒疗法(ART)。利用PENPACT - 1的数据,我们旨在按病毒学阈值描述一线ART治疗中HIV - 1耐药性的积累情况。
方法
PENPACT - 1采用2×2析因设计,将感染HIV的儿童随机分组,分别起始基于蛋白酶抑制剂(PI)或非核苷类逆转录酶抑制剂(NNRTI)的ART,并在病毒载量为1000拷贝/毫升与30000拷贝/毫升的阈值时进行切换。切换标准为在第24周未达到阈值、此后确认病毒载量反弹超过阈值或出现美国疾病控制与预防中心C期事件。在切换前、重新抑制时以及4年/试验结束时,对病毒载量≥1000拷贝/毫升的样本进行耐药性检测。
结果
67名儿童起始基于PI的ART,并随机分组在病毒载量为1000拷贝/毫升时切换(PI - 1000组)、64名在病毒载量为30000拷贝/毫升时切换(PI - 30000组)、67名起始基于NNRTI的ART并在病毒载量为1000拷贝/毫升时切换(NNRTI - 1000组)、65名在病毒载量为30000拷贝/毫升时切换(NNRTI - 30000组)。在5年随访期间,94名(36%)儿童达到了1000拷贝/毫升的切换标准。在病毒载量为30000拷贝/毫升阈值组中,从1000拷贝/毫升切换至30000拷贝/毫升标准的中位时间,PI组为58周,NNRTI组为80周(P = 0.81)。在NNRTI - 30000组中,比其他组积累了更多的核苷类逆转录酶抑制剂(NRTI)耐药突变。在病毒载量为1000拷贝/毫升切换前,NNRTI突变就已出现(NNRTI - 1000组为23%,NNRTI - 30000组为27%)。62名儿童起始阿巴卡韦+拉米夫定治疗,166名起始拉米夫定+齐多夫定或司他夫定治疗,35名起始其他NRTI治疗。阿巴卡韦+拉米夫定组获得的NRTI突变最少。在60名切换至二线治疗的儿童中,24周后病毒载量<400拷贝/毫升的比例分别为:PI - 1000组79%、PI - 30000组63%、NNRTI - 1000组64%、NNRTI - 30000组100%。
结论
随机分组在较高病毒学阈值时切换的、接受一线基于NNRTI的ART治疗的儿童产生的耐药性最强,但在二线治疗时病毒载量得到了重新抑制。阿巴卡韦+拉米夫定的NRTI组合似乎对NRTI耐药性的产生具有保护作用。
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