Ruth M. Rothstein CORE Center, Chicago, IL, USA.
Section on Infectious Diseases, Wake Forest School of Medicine, Winston-Salem, NC, USA.
HIV Res Clin Pract. 2020 Dec;21(6):151-167. doi: 10.1080/25787489.2020.1844520. Epub 2021 Feb 2.
Darunavir/cobicistat/emtricitabine/tenofovir alafenamide (D/C/F/TAF) 800/150/200/10 mg was investigated in AMBER (treatment-naïve adults; NCT02431247) and EMERALD (treatment-experienced, virologically-suppressed adults; NCT02269917).
To describe a Week 96 pre-planned subgroup analysis of D/C/F/TAF arms by demographic characteristics (age ≤/>50 years, gender, black/non-black race), and baseline clinical characteristics (AMBER: viral load [VL], CD4 count, WHO clinical stage, HIV-1 subtype and antiretroviral resistance; EMERALD: prior virologic failure [VF], antiretroviral experience, screening boosted protease inhibitor [PI], and boosting agent).
Patients in D/C/F/TAF and control arms could continue on/switch to D/C/F/TAF in a single-arm, open-label extension phase after Week 48 until Week 96. Efficacy endpoints were percentage cumulative confirmed VL ≥50 copies/mL (virologic rebound; EMERALD), and VL <50 (virologic response), or ≥50 copies/mL (VF) (FDA snapshot; both trials).
D/C/F/TAF demonstrated high Week 96 virologic responses (AMBER: 85% [308/362]; EMERALD: 91% [692/763]) and low VF rates (AMBER: 6% [20/362]; EMERALD: 1% [9/763]). In EMERALD, D/C/F/TAF showed low virologic rebound cumulative through Week 96 (3% [24/763]). Results were consistent across subgroups, including prior antiretroviral experience in EMERALD. No darunavir, primary PI, or tenofovir resistance-associated mutations were observed post-baseline. Study-drug-related serious adverse events (AEs) and AE-related discontinuations were <1% and 2%, respectively (both D/C/F/TAF arms), and similar across subgroups. eGFR and bone mineral density improved or were stable and lipids increased through Week 96 across demographic subgroups, with small changes in total-cholesterol/HDL-cholesterol ratio.
D/C/F/TAF was effective with a high barrier to resistance and bone/renal safety benefits, regardless of demographic or clinical characteristics for treatment-naïve and treatment-experienced, virologically-suppressed adults.
达芦那韦/考比司他/恩曲他滨/替诺福韦艾拉酚胺(D/C/F/TAF)800/150/200/10mg 在 AMBER(初治成人;NCT02431247)和 EMERALD(经治、病毒学抑制成人;NCT02269917)研究中进行了研究。
按人口统计学特征(年龄≤/>50 岁、性别、黑/非黑人种)和基线临床特征(AMBER:病毒载量[VL]、CD4 计数、世界卫生组织临床分期、HIV-1 亚型和抗逆转录病毒耐药性;EMERALD:先前病毒学失败[VF]、抗逆转录病毒治疗经验、筛查增强型蛋白酶抑制剂[PI]和增强剂),描述 D/C/F/TAF 臂在第 96 周的预先计划的亚组分析。
在第 48 周后,D/C/F/TAF 和对照组患者可以在一项开放性、单臂扩展研究中继续接受/转换为 D/C/F/TAF,直至第 96 周。疗效终点是累计确认 VL≥50 拷贝/mL(病毒学反弹;EMERALD)和 VL<50(病毒学应答)或≥50 拷贝/mL(VF)(FDA 快照;两项试验)的百分比。
D/C/F/TAF 在第 96 周时表现出高的病毒学应答率(AMBER:85%[308/362];EMERALD:91%[692/763])和低的 VF 率(AMBER:6%[20/362];EMERALD:1%[9/763])。在 EMERALD 中,D/C/F/TAF 显示出通过第 96 周的低病毒学反弹累积(3%[24/763])。结果在亚组中一致,包括 EMERALD 中的既往抗逆转录病毒治疗经验。未观察到达芦那韦、主要 PI 或替诺福韦耐药相关突变。研究药物相关的严重不良事件(AE)和因 AE 而停药分别<1%(D/C/F/TAF 两组)和 2%,且在亚组中相似。eGFR 和骨密度在第 96 周时改善或稳定,脂质增加,总胆固醇/高密度脂蛋白胆固醇比值略有变化。
D/C/F/TAF 对初治和经治、病毒学抑制的成年患者具有高耐药屏障和骨骼/肾脏安全性益处,无论其人口统计学或临床特征如何,均具有疗效。
