首页> 美国卫生研究院文献>Journal of Virology >Pseudorabies Virus Glycoprotein gD Contains a Functional Endocytosis Motif That Acts in Concert with an Endocytosis Motif in gB To Drive Internalization of Antibody-Antigen Complexes from the Surface of Infected Monocytes
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Pseudorabies Virus Glycoprotein gD Contains a Functional Endocytosis Motif That Acts in Concert with an Endocytosis Motif in gB To Drive Internalization of Antibody-Antigen Complexes from the Surface of Infected Monocytes

机译:伪狂犬病病毒糖蛋白gD包含功能性内吞作用基序该功能与gB中的内吞作用基序协同作用以从感染的单核细胞表面驱动抗体-抗原复合物的内在化

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摘要

Viral glycoproteins gB and gD of the swine alphaherpesvirus pseudorabies virus (PRV), which is closely related to human herpes simplex virus and varicella-zoster virus, are able to drive internalization of antibody-antigen complexes that may form at the cell surface of infected monocytes, thereby protecting these cells from efficient antibody-mediated lysis. We found earlier that gB relies on an endocytosis motif in its cytoplasmic domain for its function during this internalization process. Here, we report that the PRV gD protein also contains a functional endocytosis motif (YRLL) in its cytoplasmic domain that drives spontaneous endocytosis of gD from the cell surface early in infection and that acts in concert with the endocytosis motif in gB to contribute to efficient internalization of antibody-antigen complexes in PRV-infected monocytes.
机译:与人单纯疱疹病毒和水痘带状疱疹病毒密切相关的猪甲型疱疹病毒假狂犬病病毒(PRV)的病毒糖蛋白gB和gD能够驱动可能在感染的单核细胞表面形成的抗体-抗原复合物的内在化,从而保护这些细胞免受抗体介导的有效裂解。我们早先发现gB在此内化过程中依赖于其胞质结构域中的内吞基序。在这里,我们报道PRV gD蛋白在其胞质结构域中还包含功能性内吞作用基序(YRLL),可在感染初期从细胞表面驱动gD自发内吞,并与gB中的内吞作用基序协同起作用,从而有助于有效PRV感染的单核细胞中抗体-抗原复合物的内在化。

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