埃替拉韦仑/考比司他/恩曲他滨/替诺福韦酯与阿扎那韦+利托那韦+恩曲他滨/替诺福韦酯在HIV-1感染女性中的第48周耐药性分析(WAVES研究GS-US-236-0128)
Week 48 resistance analysis of Elvitegravir/Cobicistat/Emtricitabine/Tenofovir DF versus Atazanavir + Ritonavir + Emtricitabine/Tenofovir DF in HIV-1 infected women (WAVES study GS-US-236-0128).
作者信息
Kulkarni Rima, Hodder Sally L, Cao Huyen, Chang Silvia, Miller Michael D, White Kirsten L
机构信息
a Clinical Virology , Gilead Sciences, Inc. , Foster City , CA , USA.
b Health Sciences Center , West Virginia Clinical and Translational Science Institute Morgantown , WV , USA.
出版信息
HIV Clin Trials. 2017 Jul;18(4):164-173. doi: 10.1080/15284336.2017.1370059.
Background Women and those with non-B subtype HIV-1 are typically underrepresented in clinical trials. WAVES (GS-US-236-0128) was a double-blind phase 3b study among treatment-naïve HIV-1-infected women that demonstrated that elvitegravir/cobicistat/emtricitabine/tenofovir DF (EVG/COBI/FTC/TDF; N = 289) was superior to atazanavir + ritonavir + FTC/TDF (ATV + RTV + FTC/TDF; N = 286) for HIV-1 RNA < 50 copies/mL by FDA snapshot analysis at week 48. Here, we describe resistance development through week 48 in women with virologic failure and determine the impact of pre-existing mutations and HIV-1 subtype on viral suppression. Methods Genotypic analyses (population and deep sequencing) and phenotypic analyses of HIV-1 protease, reverse transcriptase (RT), and integrase (IN) were performed. The resistance analysis population (participants with HIV-1 RNA ≥ 400 copies/mL at confirmed virologic failure, at discontinuation ≥ week 8, or at week 48) had genotypic and phenotypic analyses at failure and baseline. Results The proportion of women qualifying for resistance analyses was similar between treatment groups (6.2% EVG/COBI/FTC/TDF; 7.3% ATV + RTV + FTC/TDF). Emergent resistance was rare (0% EVG/COBI/FTC/TDF; 1% ATV + RTV + FTC/TDF - 3 with M184V/I in RT). Deep sequencing of HIV-1 did not detect additional resistance development. Pre-existing mutations did not lead to virologic failure; most with the polymorphic primary IN substitution T97A (92%), or with substitutions in RT (i.e. A62V, V90I, K103N, or E138A/G/K/Q; 68-82%) demonstrated virologic suppression at week 48, with no resistance development except for one patient with M184V and pre-existing K103N in the ATV + RTV + FTC/TDF group. Most participants (74%) had non-B HIV-1, and subtype did not affect outcome. Conclusions Emergent resistance to study drugs was rare in this study of women, with no resistance observed among EVG/COBI/FTC/TDF-treated participants, despite a high proportion of participants with natural or transmitted viral mutations and non-B HIV-1 subtypes.
背景
在临床试验中,女性以及感染非B亚型HIV-1的人群通常代表性不足。WAVES(GS-US-236-0128)是一项针对初治HIV-1感染女性的双盲3b期研究,该研究表明,根据美国食品药品监督管理局(FDA)在第48周的快照分析,艾维雷韦/考比司他/恩曲他滨/替诺福韦酯(EVG/COBI/FTC/TDF;N = 289)在使HIV-1 RNA水平低于50拷贝/毫升方面优于阿扎那韦+利托那韦+FTC/TDF(ATV + RTV + FTC/TDF;N = 286)。在此,我们描述了病毒学失败女性至第48周的耐药性发展情况,并确定了预先存在的突变和HIV-1亚型对病毒抑制的影响。方法:对HIV-1蛋白酶、逆转录酶(RT)和整合酶(IN)进行了基因分型分析(群体测序和深度测序)以及表型分析。耐药性分析人群(在确认病毒学失败时、停药≥第8周时或第48周时HIV-1 RNA≥400拷贝/毫升的参与者)在失败时和基线时进行了基因分型和表型分析。结果:治疗组之间符合耐药性分析条件的女性比例相似(EVG/COBI/FTC/TDF组为6.2%;ATV + RTV + FTC/TDF组为7.3%)。出现耐药的情况很少见(EVG/COBI/FTC/TDF组为0%;ATV + RTV + FTC/TDF组为1% - 3例RT中出现M184V/I)。HIV-1深度测序未检测到额外的耐药性发展。预先存在的突变未导致病毒学失败;大多数携带多态性主要IN替代T97A(92%)或RT中替代(即A62V、V90I、K103N或E138A/G/K/Q;68 - 82%)的患者在第48周表现出病毒学抑制,除了ATV + RTV + FTC/TDF组中1例同时携带M184V和预先存在的K103N的患者外,未出现耐药性发展。大多数参与者(74%)感染的是非B亚型HIV-1,亚型不影响结果。结论:在这项针对女性的研究中,对研究药物出现耐药的情况很少见,在接受EVG/COBI/FTC/TDF治疗的参与者中未观察到耐药情况,尽管有很大比例的参与者携带自然或传播的病毒突变以及非B亚型HIV-1。
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