Evaluation of the effect of 48 weeks of BIC/F/TAF and DRV/c/F/TAF on platelet function in the context of rapid ART start.

IF 1.7 4区医学 Q3 INFECTIOUS DISEASES HIV Research & Clinical Practice Pub Date : 2025-12-01 Epub Date: 2025-01-07 DOI:10.1080/25787489.2024.2447015

Akif A Khawaja, Gary Whitlock, Sarah Fidler, Alfredo Soler-Carracedo, Merle Henderson, Graham P Taylor, Marta Boffito, Michael Emerson

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Abstract

Introduction: The BIC-T&T study aimed to determine the efficacy of bictegravir/emtricitabine/tenofovir alafenamide (BIC/F/TAF) and darunavir/cobicistat/emtricitabine/tenofovir alafenamide (DRV/c/F/TAF) at suppressing viral load in a two-arm, open-label, multi-centre, randomised trial under a UK test-and-treat setting. This sub-study aimed to evaluate potential off-target cardiovascular impact by examining ex vivo platelet function.

Methods: Platelets were isolated by centrifugation of citrated blood from participants attending Chelsea and Westminster Hospital or St Mary's Hospital at Week 48 following enrolment. Platelet activation was assessed by real-time flow cytometry to examine integrin activation and granule release and platelet aggregation was evaluated by light transmission aggregometry. Statistical significance was determined by 2-way ANOVA with a Šidák's multiple comparisons post-test.

Results: An analysis of 21 participants was performed at Week 48 (96% male and 48% white; mean (range) age was 37 (23-78) years). No difference between arms was observed in ADP-, collagen- or thrombin receptor activator for peptide (TRAP)-6-evoked platelet α_IIbβ₃ integrin activation, granule release or platelet aggregation in response to any of the agonists tested. Despite differences in the demographics between treatment arms, the presence of an unboosted integrase inhibitor or boosted protease inhibitor in a test-and-treat setting did not impact platelet function.

Conclusions: Our study provides no evidence of differences in downstream platelet responses between participants taking BIC/F/TAF compared to DRV/c/F/TAF following 48 wk of treatment. Further data are required to explore whether there are biologically significant off-target effects, including effects on platelets and other components of the cardiovascular system between these two test-and-treat regimens.

Clinical trial number: NCT04653194.

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评价快速启动抗逆转录病毒治疗48周BIC/F/TAF和DRV/c/F/TAF对血小板功能的影响

在英国的一项双组、开放标签、多中心、随机试验中，BIC- t&t研究旨在确定比替格拉韦/恩曲他滨/替诺福韦阿拉那胺（BIC/F/TAF）和达那韦/可比司他/恩曲他滨/替诺福韦阿拉那胺（DRV/c/F/TAF）在抑制病毒载量方面的疗效。本亚研究旨在通过检测体外血小板功能来评估潜在的脱靶心血管影响。方法：在入组后第48周，从切尔西和威斯敏斯特医院或圣玛丽医院就诊的受试者中，用柠檬酸血离心分离血小板。实时流式细胞术检测整合素激活和颗粒释放情况，光透射聚集法检测血小板聚集情况。统计学显著性采用2-way方差分析和Šidák多重比较后验。结果：在第48周对21名参与者进行了分析(96%为男性，48%为白人；平均（范围）年龄为37岁（23-78岁）。在ADP、胶原或凝血酶受体激活肽(TRAP)-6诱发的血小板α ib β3整合素激活、颗粒释放或血小板聚集方面，两组对任何激动剂的反应均无差异。尽管治疗组之间的人口统计学差异，但在试验和治疗环境中，未增强整合酶抑制剂或增强蛋白酶抑制剂的存在并不影响血小板功能。结论：我们的研究没有提供证据表明在治疗48周后，服用BIC/F/TAF的受试者与服用DRV/c/F/TAF的受试者之间下游血小板反应有差异。需要进一步的数据来探索是否存在生物学上显著的脱靶效应，包括这两种试验治疗方案对血小板和心血管系统其他成分的影响。临床试验号：NCT04653194。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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HIV Research & Clinical Practice Multiple-

CiteScore

2.90

自引率

6.20%

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