临床研究中潜伏逆转药物在重新激活HIV-1病毒库中的疗效和耐受性:一项系统综述

IF 3.5 4区 医学 Q2 IMMUNOLOGY
Quinten Debrabander , Kathryn S. Hensley , Christina K. Psomas , Wichor Bramer , Tokameh Mahmoudi , Berend J. van Welzen , Annelies Verbon , Casper Rokx
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引用次数: 0

摘要

引言了解潜伏逆转剂(LRAs)对HIV-1宿主的临床效力有助于部署未来的策略。这篇系统综述评估了LRA在人类干预研究中的作用。方法利用医学数据库进行文献检索,重点研究接受LRAs的HIV-1感染者。资格标准要求参与者来自前瞻性临床研究、假设为LRA的研究化合物以及再激活或耐受性评估。提取了相关人口统计数据、LRA再活化能力、水库规模和不良事件。采用RoB2和ROBINS-I工具对研究质量进行评估,并对偏倚进行分析。主要终点是通过细胞相关的未剪接HIV-1 RNA量化的LRA治疗后HIV-1库的再激活,以及通过不良事件定义的LRA耐受性。次要结果是储液池大小和LRA对分析性治疗中断(ATI)持续时间的影响。结果排除重复后,共筛选出5182篇出版物。总共有45篇出版物符合资格标准,包括26项干预研究和16项随机试验。偏倚的风险被评估为高。染色质调制器是24项研究中主要研究的LRA类别。参与者大多为男性(90.1%)。据报道,HIV-1亚型B最常见。LRA治疗后的反应发生在78%的研究中,并且在几乎所有染色质调节剂中都观察到。当测量时,再激活大多发生在治疗开始后24小时内。LRA组合策略很少被研究,也没有协同再激活。报告的不良事件大多是低级别的,但经常发生。七项研究中有个体因相关不良事件而停用LRA。在80%的研究中,通过HIV-1 DNA评估储层大小。在三项关于免疫检查点抑制剂和组蛋白脱乙酰酶抑制剂romidepsin和chidamide的研究中观察到储库的小幅减少。未观察到LRA对ATI持续时间的明显影响。结论本系统综述总结了当前临床试验中使用的LRAs的再激活,同时强调了药物警戒的重要性。在解释这些结果时,应考虑高度异质性的研究设计和相关患者群体的代表性不足。观察到的再活化没有导致储层的固化或尺寸的显著减小。需要通过包括精心设计的研究来找到更有效的LRA,以确定减少HIV-1库所需的再激活水平。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

The efficacy and tolerability of latency-reversing agents in reactivating the HIV-1 reservoir in clinical studies: a systematic review

The efficacy and tolerability of latency-reversing agents in reactivating the HIV-1 reservoir in clinical studies: a systematic review

The efficacy and tolerability of latency-reversing agents in reactivating the HIV-1 reservoir in clinical studies: a systematic review

The efficacy and tolerability of latency-reversing agents in reactivating the HIV-1 reservoir in clinical studies: a systematic review

Introduction

Understanding the clinical potency of latency-reversing agents (LRAs) on the HIV-1 reservoir is useful to deploy future strategies. This systematic review evaluated the effects of LRAs in human intervention studies.

Methods

A literature search was performed using medical databases focusing on studies with adults living with HIV-1 receiving LRAs. Eligibility criteria required participants from prospective clinical studies, a studied compound hypothesised as LRA, and reactivation or tolerability assessments. Relevant demographical data, LRA reactivation capacity, reservoir size, and adverse events were extracted. A study quality assessment with analysis of bias was performed by RoB 2 and ROBINS-I tools. The primary endpoints were HIV-1 reservoir reactivation after LRA treatment quantified by cell-associated unspliced HIV-1 RNA, and LRA tolerability defined by adverse events. Secondary outcomes were reservoir size and the effect of LRAs on analytical treatment interruption (ATI) duration.

Results

After excluding duplicates, 5182 publications were screened. In total 45 publications fulfilled eligibility criteria including 26 intervention studies and 16 randomised trials. The risk of bias was evaluated as high. Chromatin modulators were the main investigated LRA class in 24 studies. Participants were mostly males (90.1%). Where reported, HIV-1 subtype B was most frequently observed. Reactivation after LRA treatment occurred in 78% of studies and was observed with nearly all chromatin modulators. When measured, reactivation mostly occurred within 24 h after treatment initiation. Combination LRA strategies have been infrequently studied and were without synergistic reactivation. Adverse events, where reported, were mostly low grade, yet occurred frequently. Seven studies had individuals who discontinued LRAs for related adverse events. The reservoir size was assessed by HIV-1 DNA in 80% of studies. A small decrease in reservoir was observed in three studies on immune checkpoint inhibitors and the histone deacetylase inhibitors romidepsin and chidamide. No clear effect of LRAs on ATI duration was observed.

Conclusion

This systematic review provides a summary of the reactivation of LRAs used in current clinical trials whilst highlighting the importance of pharmacovigilance. Highly heterogeneous study designs and underrepresentation of relevant patient groups are to be considered when interpreting these results. The observed reactivation did not lead to cure or a significant reduction in the size of the reservoir. Finding more effective LRAs by including well-designed studies are needed to define the required reactivation level to reduce the HIV-1 reservoir.

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来源期刊
Journal of Virus Eradication
Journal of Virus Eradication Medicine-Public Health, Environmental and Occupational Health
CiteScore
6.10
自引率
1.80%
发文量
28
审稿时长
39 weeks
期刊介绍: The Journal of Virus Eradication aims to provide a specialist, open-access forum to publish work in the rapidly developing field of virus eradication. The Journal covers all human viruses, in the context of new therapeutic strategies, as well as societal eradication of viral infections with preventive interventions. The Journal is aimed at the international community involved in the prevention and management of viral infections. It provides an academic forum for the publication of original research into viral reservoirs, viral persistence and virus eradication and ultimately development of cures. The Journal not only publishes original research, but provides an opportunity for opinions, reviews, case studies and comments on the published literature. It focusses on evidence-based medicine as the major thrust in the successful management of viral infections.The Journal encompasses virological, immunological, epidemiological, modelling, pharmacological, pre-clinical and in vitro, as well as clinical, data including but not limited to drugs, immunotherapy and gene therapy. It is an important source of information on the development of vaccine programs and preventative measures aimed at virus eradication.
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