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Immunobiology: Capture and transfer of HIV-1 particles by mature dendritic cells converges with the exosome-dissemination pathway

机译:免疫生物学:成熟树突状细胞捕获和转移HIV-1颗粒与外泌体传播途径融合

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摘要

Exosomes are secreted cellular vesicles that can be internalized by dendritic cells (DCs), contributing to antigen-specific naive CD4+ T-cell activation. Here, we demonstrate that human immunodeficiency virus type 1 (HIV-1) can exploit this exosome antigen-dissemination pathway intrinsic to mature DCs (mDCs) for mediating trans-infection of T lymphocytes. Capture of HIV-1, HIV-1 Gag-enhanced green fluorescent protein (eGFP) viral-like particles (VLPs), and exosomes by DCs was up-regulated upon maturation, resulting in localization within a CD81+ compartment. Uptake of VLPs or exosomes could be inhibited by a challenge with either particle, suggesting that the expression of common determinant(s) on VLP or exosome surface is necessary for internalization by mDCs. Capture by mDCs was insensitive to proteolysis but blocked when virus, VLPs, or exosomes were produced from cells treated with sphingolipid biosynthesis inhibitors that modulate the lipid composition of the budding particles. Finally, VLPs and exosomes captured by mDCs were transmitted to T lymphocytes in an envelope glycoprotein-independent manner, underscoring a new potential viral dissemination pathway.
机译:外泌体是分泌的囊泡,可被树突状细胞(DC)内在化,有助于抗原特异性幼稚CD4 + T细胞活化。在这里,我们证明了人类1型免疫缺陷病毒(HIV-1)可以利用成熟DC(mDC)固有的这种外来体抗原传播途径来介导T淋巴细胞的转染。 DCs对DCs的HIV-1,HIV-1 Gag增强型绿色荧光蛋白(eGFP)病毒样颗粒(VLP)和外泌体的捕获在成熟后上调,从而导致CD81 + 隔层。通过任一颗粒的攻击均可抑制VLP或外泌体的摄取,这表明mDCs内在化在VLP或外泌体表面表达共同决定簇是必需的。 mDC的捕获对蛋白水解不敏感,但在用鞘脂生物合成抑制剂处理的细胞中产生病毒,VLP或外来体时,这种捕获被阻断,该细胞调节出芽颗粒的脂质组成。最后,由mDCs捕获的VLP和外泌体以不依赖包膜糖蛋白的方式被传递至T淋巴细胞,这突显了一种新的潜在的病毒传播途径。

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