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感染HIV-1的血液单核细胞形成一种整合素和聚集蛋白聚糖依赖性病毒突触,以诱导HIV-1高效跨上皮细胞单层转胞吞作用。

HIV-1-infected blood mononuclear cells form an integrin- and agrin-dependent viral synapse to induce efficient HIV-1 transcytosis across epithelial cell monolayer.

作者信息

Alfsen Annette, Yu Huifeng, Magérus-Chatinet Aude, Schmitt Alain, Bomsel Morgane

机构信息

Entrée Muqueuse du VIH et Immunité muqueuse, Departement de Biologie Cellulaire, Institut Cochin, CNRS, INSERM, Université René Descartes, 75014 Paris, France.

出版信息

Mol Biol Cell. 2005 Sep;16(9):4267-79. doi: 10.1091/mbc.e05-03-0192. Epub 2005 Jun 22.

Abstract

The heparan sulfate proteoglycan agrin and adhesion molecules are key players in the formation of neuronal and immune synapses that evolved for efficient communication at the sites of cell-cell contact. Transcytosis of infectious virus across epithelial cells upon contact between HIV-1-infected cells and the mucosal pole of the epithelial cells is one mechanism for HIV-1 entry at mucosal sites. In contrast, transcytosis of cell-free HIV-1 is not efficient. A synapse between HIV-1-infected cells and the mucosal epithelial surface that resembles neuronal and immune synapses is visualized by electron microscopy. We have termed this the "viral synapse." Similarities of the viral synapse also extend to the functional level. HIV-1-infected cell-induced transcytosis depends on RGD-dependent integrins and efficient cell-free virus transcytosis is inducible upon RGD-dependent integrin cross-linking. Agrin appears differentially expressed at the apical epithelial surface and acts as an HIV-1 attachment receptor. Envelope glycoprotein subunit gp41 binds specifically to agrin, reinforcing the interaction of gp41 to its epithelial receptor galactosyl ceramide.

摘要

硫酸乙酰肝素蛋白聚糖聚集蛋白和黏附分子是神经元和免疫突触形成中的关键参与者,这些突触是为了在细胞间接触部位进行高效通讯而进化而来的。HIV-1感染细胞与上皮细胞的黏膜极接触后,感染性病毒跨上皮细胞的转胞吞作用是HIV-1在黏膜部位进入的一种机制。相比之下,游离HIV-1的转胞吞作用效率不高。通过电子显微镜可以观察到HIV-1感染细胞与黏膜上皮表面之间类似神经元和免疫突触的突触。我们将其称为“病毒突触”。病毒突触的相似性也延伸到了功能层面。HIV-1感染细胞诱导的转胞吞作用依赖于RGD依赖的整合素,并且在RGD依赖的整合素交联后可诱导高效的游离病毒转胞吞作用。聚集蛋白在上皮细胞顶端表面呈差异表达,并作为HIV-1附着受体发挥作用。包膜糖蛋白亚基gp41特异性结合聚集蛋白,增强gp41与其上皮受体半乳糖神经酰胺的相互作用。

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