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CD169-Dependent Cell-Associated HIV-1 Transmission: A Driver of Virus Dissemination

机译:CD169依赖细胞相关的HIV-1传播:病毒传播的驱动程序。

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摘要

Sexual transmission of human immunodeficiency virus type 1 (HIV-1) occurs across mucosal surfaces of the genital and gastrointestinal tracts and accounts for the vast majority of newly acquired infections worldwide. In the absence of an effective vaccine, interventional strategies such as microbicides that target viral attachment and entry into mucosa-resident target cells are particularly attractive and might have the greatest impact on reducing the HIV-1 pandemic. Rational development of microbicides would be greatly aided with a better understanding of several key questions of mucosal HIV-1 transmission, including the molecular mechanism(s) of how HIV-1 traverses mucosal barriers, the type of cells that it initially infects to gain a foothold in the naive host, and how it is disseminated from local sites of infection to draining lymph nodes. In this review, we discuss the role of myeloid dendritic cells (DCs) in cell-associated HIV-1 transmission and in facilitating systemic HIV-1 dissemination. We will evaluate the role of CD169 as a DC-associated HIV-1 attachment factor, investigate the molecular mechanisms by which HIV-1 particles are transferred from DCs to CD4+ T cells across virological synapses, and provide arguments for inclusion of molecules in microbicides that can effectively target HIV-1 attachment to DCs and DC-mediated virus transfer.
机译:人类免疫缺陷病毒1型(HIV-1)的性传播发生在生殖道和胃肠道的粘膜表面,占全世界新感染的绝大部分。在缺乏有效疫苗的情况下,诸如杀微生物剂等靶向病毒附着并进入粘膜驻留靶细胞的干预策略尤其具有吸引力,并且可能对减少HIV-1大流行具有最大的影响。更好地理解粘膜HIV-1传播的几个关键问题,包括对HIV-1如何穿越粘膜屏障的分子机制,最初感染以获取病毒的细胞类型的分子机制,将有助于极大地帮助杀菌剂的合理开发。幼稚宿主的立足点,以及它如何从感染的局部部位传播到引流淋巴结。在这篇综述中,我们讨论了髓样树突状细胞(DCs)在与细胞相关的HIV-1传播和促进系统性HIV-1传播中的作用。我们将评估CD169作为DC相关HIV-1附着因子的作用,研究HIV-1颗粒跨病毒突触从DC转移至CD4 + T细胞的分子机制,并提供关于在杀微生物剂中包含可有效靶向HIV-1附着于DC和DC介导的病毒转移的分子的争论。

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