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Moving towards a reliable HIV incidence test - current status, resources available, future directions and challenges ahead.迈向可靠的艾滋病毒发病率检测——现状、可用资源、未来方向及面临的挑战
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Novel Monoclonal Antibodies for Studies of Human and Rhesus Macaque Secretory Component and Human J-Chain.用于研究人类和恒河猴分泌成分及人类J链的新型单克隆抗体。
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Human Non-neutralizing HIV-1 Envelope Monoclonal Antibodies Limit the Number of Founder Viruses during SHIV Mucosal Infection in Rhesus Macaques.人源非中和性HIV-1包膜单克隆抗体可限制恒河猴黏膜感染SHIV期间初始病毒的数量。
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计算分析抗体动力学可识别近期 HIV-1 感染。

Computational analysis of antibody dynamics identifies recent HIV-1 infection.

机构信息

Duke Human Vaccine Institute, Department of Medicine, Durham, North Carolina, USA.

South African Centre for Epidemiological Modelling and Analysis, Stellenbosch University, Stellenbosch, South Africa.

出版信息

JCI Insight. 2017 Dec 21;2(24):94355. doi: 10.1172/jci.insight.94355.

DOI:10.1172/jci.insight.94355
PMID:29263306
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5752300/
Abstract

Accurate HIV-1 incidence estimation is critical to the success of HIV-1 prevention strategies. Current assays are limited by high false recent rates (FRRs) in certain populations and a short mean duration of recent infection (MDRI). Dynamic early HIV-1 antibody response kinetics were harnessed to identify biomarkers for improved incidence assays. We conducted retrospective analyses on circulating antibodies from known recent and longstanding infections and evaluated binding and avidity measurements of Env and non-Env antigens and multiple antibody forms (i.e., IgG, IgA, IgG3, IgG4, dIgA, and IgM) in a diverse panel of 164 HIV-1-infected participants (clades A, B, C). Discriminant function analysis identified an optimal set of measurements that were subsequently evaluated in a 324-specimen blinded biomarker validation panel. These biomarkers included clade C gp140 IgG3, transmitted/founder clade C gp140 IgG4 avidity, clade B gp140 IgG4 avidity, and gp41 immunodominant region IgG avidity. MDRI was estimated at 215 day or alternatively, 267 days. FRRs in untreated and treated subjects were 5.0% and 3.6%, respectively. Thus, computational analysis of dynamic HIV-1 antibody isotype and antigen interactions during infection enabled design of a promising HIV-1 recency assay for improved cross-sectional incidence estimation.

摘要

准确估计 HIV-1 的感染率对于 HIV-1 预防策略的成功至关重要。目前的检测方法存在一定局限性,某些人群的假近期率(FRR)较高,近期感染的平均持续时间(MDRI)较短。人们利用早期 HIV-1 抗体反应动力学来寻找改善感染率检测的生物标志物。我们对已知近期和长期感染患者的循环抗体进行了回顾性分析,并评估了 164 名 HIV-1 感染者(A、B、C 型)中多样化面板中 Env 和非 Env 抗原以及多种抗体形式(即 IgG、IgA、IgG3、IgG4、dIgA 和 IgM)的结合和亲和力测量。判别函数分析确定了一组最佳测量值,随后在 324 份盲法生物标志物验证面板中进行了评估。这些生物标志物包括 C 型 gp140 IgG3、传播/创始者 C 型 gp140 IgG4 亲和力、B 型 gp140 IgG4 亲和力和 gp41 免疫显性区 IgG 亲和力。MDRI 估计为 215 天或 267 天。未治疗和治疗患者的 FRR 分别为 5.0%和 3.6%。因此,对感染期间 HIV-1 抗体同种型和抗原相互作用的计算分析,使得设计出一种有前途的 HIV-1 近期检测方法,用于改善横断面感染率估计。