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Pathogen at the Gates: Human Cytomegalovirus Entry and Cell Tropism

机译:大门的病原体:人类巨细胞病毒进入和细胞趋向

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The past few years have brought substantial progress toward understanding how human cytomegalovirus (HCMV) enters the remarkably wide spectrum of cell types and tissues that it infects. Neuropilin-2 and platelet-derived growth factor receptor alpha (PDGFRα) were identified as receptors, respectively, for the trimeric and pentameric glycoprotein H/glycoprotein L (gH/gL) complexes that in large part govern HCMV cell tropism, while CD90 and CD147 were also found to play roles during entry. X-ray crystal structures for the proximal viral fusogen, glycoprotein B (gB), and for the pentameric gH/gL complex (pentamer) have been solved. A novel virion gH complex consisting of gH bound to UL116 instead of gL was described, and findings supporting the existence of a stable complex between gH/gL and gB were reported. Additional work indicates that the pentamer promotes a mode of cell-associated spread that resists antibody neutralization, as opposed to the trimeric gH/gL complex (trimer), which appears to be broadly required for the infectivity of cell-free virions. Finally, viral factors such as UL148 and US16 were identified that can influence the incorporation of the alternative gH/gL complexes into virions. We will review these advances and their implications for understanding HCMV entry and cell tropism.
机译:过去几年,在了解人类巨细胞病毒(HCMV)如何进入其感染的非常广泛的细胞类型和组织方面取得了实质性进展。对于三聚体和五聚体糖蛋白H /糖蛋白L(gH / gL)复合物,它们主要控制HCMV细胞的嗜性,而CD90和CD147分别被识别为Neuropilin-2和血小板衍生的生长因子受体α(PDGFRα)。也被发现在进入过程中扮演角色。解决了近端病毒融合蛋白,糖蛋白B(gB)和五聚体gH / gL复合物(pentamer)的X射线晶体结构。描述了一种新的病毒体gH复合物,该复合物由与UL116结合的gH代替gL组成,报道了支持gH / gL和gB之间存在稳定复合物的发现。额外的工作表明,五聚体促进了抗抗体中和的细胞相关扩散模式,这与三聚体gH / gL复合物(三聚体)相反,后者似乎是无细胞病毒体感染性的广泛要求。最后,确定了可以影响替代性gH / gL复合物掺入病毒粒子的病毒因子,例如UL148和US16。我们将回顾这些进展及其对理解HCMV进入和细胞嗜性的意义。

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