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HIV免疫治疗试验中的干预后对照

Post-intervention control in HIV immunotherapy trials.

作者信息

Sandel Demi A, Rutishauser Rachel L, Peluso Michael J

机构信息

Division of Experimental Medicine.

Division of HIV, Infectious Diseases, and Global Medicine, University of California, San Francisco, San Francisco, California, USA.

出版信息

Curr Opin HIV AIDS. 2025 Jan 1;20(1):70-79. doi: 10.1097/COH.0000000000000890. Epub 2024 Nov 4.

Abstract

PURPOSE OF REVIEW

While post-treatment control following interruption of standard-of-care antiretroviral therapy (ART) is well described, post-intervention control following immunotherapy in HIV cure-related clinical trials is less well understood. We provide an overview of recent studies that have identified post-intervention controllers and review the mechanisms that may drive this biologically important phenotype.

RECENT FINDINGS

Post-intervention controllers have been identified in recent immunotherapy trials testing broadly neutralizing antibodies, immune modulators, modified T cells, checkpoint inhibitors, and gene therapy administered individually or in combination. Currently, there is substantial variability in how each trial defines post-intervention control, as well as in how the mechanisms underlying such control are evaluated. Such mechanisms include ongoing activity of both exogenous and autologous antibodies, as well as changes in HIV-specific T cell function.

SUMMARY

While no therapeutic strategy to date has succeeded in definitively inducing HIV control, many studies have identified at least a small number of post-intervention controllers. The field would benefit from a standardized approach to defining and reporting this phenotype, as well as standardization in the approach to assessment of how it is achieved. Such efforts would allow for comparisons across clinical trials and could help accelerate efforts toward an HIV cure.

摘要

综述目的

虽然在中断标准抗逆转录病毒疗法(ART)后的治疗后控制情况已有充分描述,但在与HIV治愈相关的临床试验中,免疫治疗后的干预后控制情况却鲜为人知。我们概述了最近确定干预后病毒控制者的研究,并回顾了可能导致这种具有生物学重要性表型的机制。

最新发现

在最近的免疫治疗试验中已确定了干预后病毒控制者,这些试验测试了单独或联合使用的广泛中和抗体、免疫调节剂、经修饰的T细胞、检查点抑制剂和基因疗法。目前,每个试验在定义干预后控制的方式以及评估这种控制背后机制的方式上存在很大差异。这些机制包括外源性和自体抗体的持续活性,以及HIV特异性T细胞功能的变化。

总结

虽然迄今为止没有一种治疗策略能够成功地最终诱导HIV控制,但许多研究已经确定了至少少数干预后病毒控制者。该领域将受益于一种标准化的方法来定义和报告这种表型,以及评估实现该表型方法的标准化。这些努力将有助于跨临床试验进行比较,并可能有助于加速实现HIV治愈的努力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6fc1/11620322/537054d10bf6/cohiv-20-70-g001.jpg

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