首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Hepatitis B virus (HBV) envelope glycoproteins vary drastically in their sensitivity to glycan processing: Evidence that alteration of a single N-linked glycosylation site can regulate HBV secretion
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Hepatitis B virus (HBV) envelope glycoproteins vary drastically in their sensitivity to glycan processing: Evidence that alteration of a single N-linked glycosylation site can regulate HBV secretion

机译:乙型肝炎病毒(HBV)包膜糖蛋白对聚糖加工的敏感性差异很大:有证据表明单个N-联糖基化位点的改变可以调节HBV的分泌

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摘要

The role of N-linked glycosylation and glycan trimming in the function of glycoproteins remains a central question in biology. Hepatitis B virus specifies three glycoproteins (L, M, and S) that are derived from alternate translation of the same ORF. All three glycoproteins contain a common N-glycosylation site in the S domain while M possesses an additional N-glycosylation site at its amino terminus. In the presence of N-butyl-deoxnojirimycin (an inhibitor of α-glucosidase) virions and the M protein are surprisingly retained. Preliminary evidence suggests that the retained M protein is hyperglucosylated and localized to lysosomal vesicles. In contrast, the S and L proteins are secreted, and their glycosylation state is unaffected by the presence of the inhibitor. Site-directed mutagenesis provides evidence that virion secretion requires the glycosylation sequon in the pre-S2 domain of M. This highlights the potential role of the M protein oligosaccharide as a therapeutic target.
机译:N-联糖基化和聚糖修饰在糖蛋白功能中的作用仍然是生物学中的中心问题。乙型肝炎病毒指定了三种糖蛋白(L,M和S),这些糖蛋白来自同一ORF的交替翻译。所有这三种糖蛋白在S结构域中都有一个共同的N-糖基化位点,而M在其氨基末端具有一个额外的N-糖基化位点。在存在N-丁基-脱氧野oji霉素(α-葡萄糖苷酶的抑制剂)的情况下,病毒体和M蛋白出人意料地被保留。初步证据表明,保留的M蛋白被高糖基化并定位在溶酶体囊泡中。相反,S和L蛋白是分泌的,其糖基化状态不受抑制剂存在的影响。定点诱变提供证据表明病毒体分泌需要M的pre-S2结构域中的糖基化序列。这突出了M蛋白寡糖作为治疗靶标的潜在作用。

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