首页> 外文期刊>Journal of the American Society for Mass Spectrometry >Mass spectrometric characterization of glycosylation of hepatitis C virus E2 envelope glycoprotein reveals extended microheterogeneity of N-glycans
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Mass spectrometric characterization of glycosylation of hepatitis C virus E2 envelope glycoprotein reveals extended microheterogeneity of N-glycans

机译:丙型肝炎病毒E2包膜糖蛋白糖基化的质谱表征揭示了N-聚糖的微异质性扩展

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Hepatitis C virus (HCV) causes acute and chronic liver disease in humans, including chronic hepatitis, cirrhosis, and hepatocellular carcinoma. The polyprotein encoded in the HCV genome is co- and post-translationally processed by host and viral peptidases, generating the structural proteins Core, E1, E2, and p7, and five nonstructural proteins. The two envelope proteins E1 and E2 are heavily glycosylated. Studying the glycan moieties attached to the envelope E2 glycoprotein is important because the N-linked glycans on E2 envelope protein are involved in the interaction with some human neutralizing antibodies, and may also have a direct or indirect effect on protein folding. In the present study, we report the mass spectrometric characterization of the glycan moieties attached to the E2 glycoprotein. The mass spectrometric analysis clearly identified the nature, composition, and microheterogeneity of the sugars attached to the E2 glycopeptides. All 11 sites of glycosylation on E2 protein were characterized, and the majority of these sites proved to be occupied by high mannose glycans. However, complex type oligosaccharides, which have not been previously identified, were exclusively observed at two N-linked sites, and their identity and heterogeneity were determined.
机译:丙型肝炎病毒(HCV)引起人类的急性和慢性肝病,包括慢性肝炎,肝硬化和肝细胞癌。 HCV基因组中编码的多蛋白由宿主和病毒肽酶进行共翻译和翻译后加工,生成结构蛋白Core,E1,E2和p7,以及五个非结构蛋白。两个包膜蛋白E1和E2被高度糖基化。研究与包膜E2糖蛋白连接的聚糖部分很重要,因为E2包膜蛋白上的N-连接聚糖参与与某些人中和抗体的相互作用,并且也可能对蛋白质折叠产生直接或间接影响。在本研究中,我们报告了与E2糖蛋白相连的聚糖部分的质谱表征。质谱分析清楚地确定了与E2糖肽相连的糖的性质,组成和微异质性。表征了E2蛋白上所有11个糖基化位点,这些位点中的大多数被证明被高甘露糖聚糖占据。但是,以前未发现的复杂类型的寡糖仅在两个N-连接位点观察到,并确定了它们的同一性和异质性。

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