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HIV-1 颠覆精液中的补体系统以增强病毒传播。

HIV-1 subverts the complement system in semen to enhance viral transmission.

机构信息

Department of Experimental Immunology, Amsterdam Infection and Immunity Institute, Amsterdam University Medical Centers, University of Amsterdam, Amsterdam, the Netherlands.

Institute of Hygiene and Medical Microbiology, Medical University of Innsbruck, Innsbruck, Austria.

出版信息

Mucosal Immunol. 2021 May;14(3):743-750. doi: 10.1038/s41385-021-00376-9. Epub 2021 Feb 10.

Abstract

Semen is important in determining HIV-1 susceptibility but it is unclear how it affects virus transmission during sexual contact. Mucosal Langerhans cells (LCs) are the first immune cells to encounter HIV-1 during sexual contact and have a barrier function as LCs are restrictive to HIV-1. As semen from people living with HIV-1 contains complement-opsonized HIV-1, we investigated the effect of complement on HIV-1 dissemination by human LCs in vitro and ex vivo. Notably, pre-treatment of HIV-1 with semen enhanced LC infection compared to untreated HIV-1 in the ex vivo explant model. Infection of LCs and transmission to target cells by opsonized HIV-1 was efficiently inhibited by blocking complement receptors CR3 and CR4. Complement opsonization of HIV-1 enhanced uptake, fusion, and integration by LCs leading to an increased transmission of HIV-1 to target cells. However, in the absence of both CR3 and CR4, C-type lectin receptor langerin was able to restrict infection of complement-opsonized HIV-1. These data suggest that complement enhances HIV-1 infection of LCs by binding CR3 and CR4, thereby bypassing langerin and changing the restrictive nature of LCs into virus-disseminating cells. Targeting complement factors might be effective in preventing HIV-1 transmission.

摘要

精液在决定 HIV-1 易感性方面很重要,但尚不清楚它如何影响性接触期间的病毒传播。黏膜朗格汉斯细胞 (LCs) 是性接触中首先遇到 HIV-1 的免疫细胞,并且具有屏障功能,因为 LCs 对 HIV-1 具有限制作用。由于 HIV-1 感染者的精液中含有补体调理的 HIV-1,我们研究了补体对体外和离体人类 LCs 中 HIV-1 传播的影响。值得注意的是,与未处理的 HIV-1 相比,精液预处理 HIV-1 增强了离体实验模型中 LCs 的感染。通过补体受体 CR3 和 CR4 阻断,可有效抑制调理 HIV-1 对 LCs 的感染和向靶细胞的传播。然而,在缺乏 CR3 和 CR4 的情况下,C 型凝集素受体 langerin 能够限制补体调理的 HIV-1 的感染。这些数据表明,补体通过结合 CR3 和 CR4 增强了 HIV-1 对 LCs 的感染,从而绕过 langerin 并将 LCs 的限制性质改变为传播病毒的细胞。针对补体因子可能是预防 HIV-1 传播的有效方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0e95/8075950/253c5a7c7583/41385_2021_376_Fig1_HTML.jpg

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