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替代性效应功能分析揭示了在长期高暴露于HIV但未感染个体中广泛的HIV特异性T细胞反应。

Alternative effector-function profiling identifies broad HIV-specific T-cell responses in highly HIV-exposed individuals who remain uninfected.

作者信息

Ruiz-Riol Marta, Llano Anuska, Ibarrondo Javier, Zamarreño Jennifer, Yusim Karina, Bach Vanessa, Mothe Beatriz, Perez-Alvarez Susana, Fernandez Marco A, Requena Gerard, Meulbroek Michael, Pujol Ferran, Leon Agathe, Cobarsi Patricia, Korber Bette T, Clotet Bonaventura, Ganoza Carmela, Sanchez Jorge, Coll Josep, Brander Christian

机构信息

HIVACAT, Irsicaixa AIDS Research Institute, Autonomous University of Barcelona.

Center for HIV Prevention Research, University of California-Los Angeles.

出版信息

J Infect Dis. 2015 Mar 15;211(6):936-46. doi: 10.1093/infdis/jiu534. Epub 2014 Sep 23.

DOI:10.1093/infdis/jiu534
PMID:25249264
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4416125/
Abstract

The characterization of host immune responses to human immunodeficiency virus (HIV) in HIV controllers and individuals with high exposure but seronegativity to HIV (HESN) is needed to guide the development of effective preventive and therapeutic vaccine candidates. However, several technical hurdles severely limit the definition of an effective virus-specific T-cell response. By using a toggle-peptide approach, which takes HIV sequence diversity into account, and a novel, boosted cytokine staining/flow cytometry strategy, we here describe new patterns of T-cell responses to HIV that would be missed by standard assays. Importantly, this approach also allows detection of broad and strong virus-specific T-cell responses in HESN individuals that are characterized by a T-helper type 1 cytokine-like effector profile and produce cytokines that have been associated with potential control of HIV infection, including interleukin 10, interleukin 13, and interleukin 22. These results establish a novel approach to improve the current understanding of HIV-specific T-cell immunity and identify cellular immune responses and individual cytokines as potential markers of relative HIV resistance. As such, the findings also help develop similar strategies for more-comprehensive assessments of host immune responses to other human infections and immune-mediated disorders.

摘要

为指导开发有效的预防性和治疗性候选疫苗,需要对HIV控制者以及高暴露但HIV血清阴性个体(HESN)的宿主免疫反应进行特征分析。然而,一些技术障碍严重限制了对有效病毒特异性T细胞反应的定义。通过采用考虑HIV序列多样性的toggle肽方法以及一种新型的增强细胞因子染色/流式细胞术策略,我们在此描述了标准检测方法会遗漏的T细胞对HIV反应的新模式。重要的是,这种方法还能够检测HESN个体中广泛且强烈的病毒特异性T细胞反应,其特征为1型辅助性细胞因子样效应子谱,并产生与潜在控制HIV感染相关的细胞因子,包括白细胞介素10、白细胞介素13和白细胞介素22。这些结果建立了一种新方法,以改善目前对HIV特异性T细胞免疫的理解,并将细胞免疫反应和个别细胞因子确定为相对HIV抗性的潜在标志物。因此,这些发现也有助于开发类似策略,以更全面地评估宿主对其他人类感染和免疫介导疾病的免疫反应。

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