首页> 外文OA文献 >Soluble Epstein-Barr Virus Glycoproteins gH, gL, and gp42 Form a 1:1:1 Stable Complex That Acts Like Soluble gp42 in B-Cell Fusion but Not in Epithelial Cell Fusion
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Soluble Epstein-Barr Virus Glycoproteins gH, gL, and gp42 Form a 1:1:1 Stable Complex That Acts Like Soluble gp42 in B-Cell Fusion but Not in Epithelial Cell Fusion

机译:可溶性爱泼斯坦-巴尔病毒糖蛋白gH,gL和gp42形成1:1:1稳定的复合物,其作用类似于B细胞融合而不是上皮细胞融合中的gp42

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摘要

Epstein-Barr virus (EBV) is a herpesvirus that infects cells by fusing its lipid envelope with the target cell membrane. The fusion process requires the actions of viral glycoproteins gH, gL, and gB for entry into epithelial cells and additionally requires gp42 for entry into B cells. To further study the roles of these membrane-associated glycoproteins, purified soluble forms of gp42, gH, and gL were expressed that lack the membrane-spanning regions. The soluble gH/gL protein complex binds to soluble gp42 with high affinity, forming a stable heterotrimer with 1:1:1 stoichiometry, and this complex is not formed by an N-terminally truncated variant of gp42. The effects of adding soluble gp42, gH/gL, and gH/gL/gp42 were examined with a virus-free cell-cell fusion assay. The results demonstrate that, in contrast to gp42, membrane fusion does not proceed with secreted gH/gL. The addition of soluble gH/gL does not inhibit or enhance B-cell or epithelial cell fusion when membrane-bound gH/gL, gB, and gp42 are present. However, the soluble gH/gL/gp42 complex does activate membrane fusion with B cells, similarly to soluble gp42, but it does not inhibit fusion with epithelial cells, as observed for gp42 alone. A gp42 peptide, derived from an N-terminal segment involved in gH/gL interactions, binds to soluble gH/gL and inhibits EBV-mediated epithelial cell fusion, mimicking gp42. These observations reveal distinct functional requirements for gH/gL and gp42 complexes in EBV-mediated membrane fusion.
机译:爱泼斯坦-巴尔病毒(EBV)是一种疱疹病毒,通过将其脂质包膜与靶细胞膜融合来感染细胞。融合过程需要病毒糖蛋白gH,gL和gB的作用才能进入上皮细胞,另外还需要gp42才能进入B细胞。为了进一步研究这些膜相关糖蛋白的作用,表达了缺乏跨膜区域的纯化可溶形式的gp42,gH和gL。可溶性gH / gL蛋白复合物以高亲和力与可溶性gp42结合,形成化学计量比为1:1:1的稳定的异源三聚体,并且该复合物不是由gp42的N端截短的变体形成。用无病毒的细胞-细胞融合测定法检查了添加可溶性gp42,gH / gL和gH / gL / gp42的效果。结果表明,与gp42相比,分泌的gH / gL不会进行膜融合。当存在膜结合的gH / gL,gB和gp42时,添加可溶性gH / gL不会抑制或增强B细胞或上皮细胞融合。但是,可溶性gH / gL / gp42复合物的确激活了与B细胞的膜融合,类似于可溶性gp42,但它不抑制与上皮细胞的融合,就像单独对gp42观察到的那样。源自参与gH / gL相互作用的N末端片段的gp42肽与可溶性gH / gL结合并抑制EBV介导的上皮细胞融合,与gp42相似。这些观察结果揭示了EBV介导的膜融合中gH / gL和gp42复合物的不同功能要求。

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