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首页> 外文期刊>Journal of Leukocyte Biology: An Official Publication of the Reticuloendothelial Society >HIV-1 envelope-receptor interactions required for macrophage infection and implications for current HIV-1 cure strategies
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HIV-1 envelope-receptor interactions required for macrophage infection and implications for current HIV-1 cure strategies

机译:巨噬细胞感染所需的HIV-1包膜受体相互作用及其对当前HIV-1治愈策略的影响

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摘要

Myeloid cells residing in the CNS and lymphoid tissues are targets for productive HIV-1 replication, and their infection contributes to the pathological manifestations of HIV-1 infection. The Envs can adopt altered configurations to overcome entry restrictions in macrophages via a more efficient and/or altered mechanism of engagement with cellular receptors. This review highlights evidence supporting an important role for macrophages in HIV-1 pathogenesis and persistence, which need to be considered for strategies aimed at achieving a functional or sterilizing cure. We also highlight that the molecular mechanisms underlying HIV-1 tropism for macrophages are complex, involving enhanced and/or altered interactions with CD4, CCR5, and/or CXCR4, and that the nature of these interactions may depend on the anatomical location of the virus.
机译:存在于中枢神经系统和淋巴组织中的髓样细胞是生产性HIV-1复制的靶标,它们的感染有助于HIV-1感染的病理表现。 Envs可以采用改变的构型,以通过与细胞受体结合的更有效和/或改变的机制克服巨噬细胞的进入限制。这篇综述强调了支持巨噬细胞在HIV-1发病机制和持久性中发挥重要作用的证据,而对于实现功能性或消毒性治愈的策略则需要考虑这些证据。我们还强调指出,HIV-1嗜性巨噬细胞的分子机制很复杂,涉及与CD4,CCR5和/或CXCR4相互作用的增强和/或改变,这些相互作用的性质可能取决于病毒的解剖位置。

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