Post Frank A, Yazdanpanah Yazdan, Schembri Gabriel, Lazzarin Adriano, Reynes Jacques, Maggiolo Franco, Yan Mingjin, Abram Michael E, Tran-Muchowski Cecilia, Cheng Andrew, Rhee Martin S
a Kings College Hospital NHS Foundation Trust , Weston Education Centre (2.53) , London , UK.
b Service des Maladies Infectieuses et Tropicales , Hospital Bichat-Claude Bernard , Paris , France.
HIV Clin Trials. 2017 May;18(3):135-140. doi: 10.1080/15284336.2017.1291867. Epub 2017 Mar 17.
FTC/TAF was shown to be noninferior to FTC/TDF with advantages in markers of renal and bone safety.
To evaluate the efficacy and safety of switching to FTC/TAF from FTC/TDF by third agent (boosted protease inhibitor [PI] vs. unboosted third agent).
We conducted a 48-week subgroup analysis based on third agent from a randomized, double blind study in virologically suppressed adults on a FTC/TDF-containing regimen who switched to FTC/TAF vs. continued FTC/TDF while remaining on the same third agent.
We randomized (1:1) 663 participants to either switch to FTC/TAF (N = 333) or continue FTC/TDF (N = 330), each with baseline third agent stratifying by class of third agent in the prior treatment regimen (boosted PI 46%, unboosted third agent 54%). At week 48, significant differences in renal biomarkers and bone mineral density were observed favoring FTC/TAF over FTC/TDF (p < 0.05 for all), with similar improvements in the FTC/TAF arm in those who received boosted PI vs. unboosted third agents. At week 48, virologic success rates were similar between treatment groups for those who received a boosted PI (FTC/TAF 92%, FTC/TDF 93%) and for those who received an unboosted third agent (97% vs. 93%).
In virologically suppressed patients switching to FTC/TAF from FTC/TDF, high rates of virologic suppression were maintained, while renal and bone safety parameters improved, regardless of whether participants were receiving a boosted PI or an unboosted third agent. FTC/TAF offers safety advantages over FTC/TDF and can be an important option as an NRTI backbone given with a variety of third agents.
已证明富马酸替诺福韦酯/丙酚替诺福韦(FTC/TAF)不劣于富马酸替诺福韦酯/替诺福韦二吡呋酯(FTC/TDF),在肾脏和骨骼安全性指标方面具有优势。
评估通过第三种药物(增强型蛋白酶抑制剂[PI]与未增强的第三种药物)从FTC/TDF转换为FTC/TAF的疗效和安全性。
我们基于一项随机、双盲研究中的第三种药物进行了为期48周的亚组分析,该研究针对病毒学抑制的成年人,他们采用含FTC/TDF的治疗方案,转换为FTC/TAF与继续使用FTC/TDF,同时继续使用相同的第三种药物。
我们将663名参与者随机(1:1)分为转换为FTC/TAF组(N = 333)或继续使用FTC/TDF组(N = 330),每组根据先前治疗方案中第三种药物的类别进行基线第三种药物分层(增强型PI占46%,未增强的第三种药物占54%)。在第48周时,观察到肾脏生物标志物和骨密度存在显著差异,FTC/TAF优于FTC/TDF(所有p < 0.05),在接受增强型PI与未增强的第三种药物的FTC/TAF组中改善情况相似。在第48周时,接受增强型PI的治疗组(FTC/TAF为92%,FTC/TDF为93%)和接受未增强的第三种药物的治疗组(97%对93%)的病毒学成功率相似。
在从FTC/TDF转换为FTC/TAF的病毒学抑制患者中,无论参与者接受的是增强型PI还是未增强的第三种药物,均能维持较高的病毒学抑制率,同时肾脏和骨骼安全性参数得到改善。FTC/TAF比FTC/TDF具有安全性优势,作为与多种第三种药物联合使用的核苷类逆转录酶抑制剂主干药物,它可能是一个重要选择。
