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首页> 外文期刊>Virology >Impact of immune escape mutations and N-linked glycosylation on the secretion of hepatitis B virus virions and subviral particles: Role of the small envelope protein
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Impact of immune escape mutations and N-linked glycosylation on the secretion of hepatitis B virus virions and subviral particles: Role of the small envelope protein

机译:免疫逃生突变和N-连接的糖基化对乙型肝炎病毒病毒病毒病毒病毒和亚病毒颗粒的影响:小包络蛋白的作用

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摘要

Hepatitis B virus (HBV) expresses three co-terminal envelope proteins: large (L), middle (M), and small (S), with the S protein driving the secretion of both virions and subviral particles. Virion secretion requires N-linked glycosylation at N146 in the S domain but can be impaired by immune escape mutations. An M133T mutation creating a novel glycosylation site at N131could rescue virion secretion of N146Q mutant (loss of original glycosylation site) and immune escape mutants such as G145R. Here we demonstrate that other novel N-linked glycosylation sites could rescue virion secretion of the G145R and N146Q mutants to variable extents. Both G145R and N146Q mutations impaired vision secretion through the S protein. The M133T mutation restored vision secretion through the S protein, and could work in trans. Impaired virion secretion was not necessarily associated with a similar block in the secretion of subviral particles.
机译:乙型肝炎病毒(HBV)表达了三个共聚末端包膜蛋白:大(L),中间(M)和小(S),S蛋白质驱动病毒粒子和亚病毒颗粒的分泌。 病毒赛分泌在S结构域内的N146处需要N-连接的糖基化,但可以通过免疫逸出突变损害。 M133T突变在N131中产生新的糖基化位点,拯救N146Q突变体(原始糖基化位点的损失)和免疫逸出突变体如G145R。 在这里,我们证明了其他新的N-连接糖基化位点可以拯救将G145R和N146Q突变体的病毒中分泌到可变范围。 G145R和N146Q突变均通过S蛋白质损害视力分泌。 M133T突变通过S蛋白恢复视觉分泌,可以在反式中工作。 受损的病毒虫分泌不一定与亚病毒颗粒分泌中类似的嵌段相关。

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