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Direct interaction between the hepatitis B virus core and envelope proteins analyzed in a cellular context

机译:在细胞背景下分析乙型肝炎病毒核心与包络蛋白之间的直接相互作用

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Hepatitis B virus (HBV) production requires intricate interactions between the envelope and core proteins. Analyses of mutants of these proteins have made it possible to map regions involved in the formation and secretion of virions. Tests of binding between core and envelope peptides have also been performed in cell-free conditions, to study the interactions potentially underlying these mechanisms. We investigated the residues essential for core-envelope interaction in a cellular context in more detail, by transiently producing mutant or wild-type L, S, or core proteins separately or in combination, in Huh7 cells. The colocalization and interaction of these proteins were studied by confocal microscopy and co-immunoprecipitation, respectively. The L protein was shown to constitute a molecular platform for the recruitment of S and core proteins in a perinuclear environment. Several core amino acids were found to be essential for direct interaction with L, including residue Y132, known to be crucial for capsid formation, and residues L60, L95, K96 and I126. Our results confirm the key role of L in the tripartite core-S-L interaction and identify the residues involved in direct core-L interaction. This model may be valuable for studies of the potential of drugs to inhibit HBV core-envelope interaction.
机译:乙型肝炎病毒(HBV)生产需要包围和核心蛋白之间复杂的相互作用。这些蛋白质的突变体的分析使得可以映射参与中的形成和分泌的区域。在无细胞条件下也进行了核心和包膜肽之间的结合的测试,以研究可能潜在地潜在的这些机制的相互作用。我们研究了细胞上下文中的核心包络相互作用所必需的残留物,更详细地通过瞬时产生突变或野生型L,S或核心蛋白在HUH7细胞中。通过共聚焦显微镜和共免疫沉淀研究了这些蛋白质的分层化和相互作用。显示L蛋白质在治疗核环境中募集S和核心蛋白的分子平台。发现几个核酸氨基酸对于与L的直接相互作用是必不可少的,包括残基Y132,已知是衣壳形成至关重要,以及残基L60,L95,K96和I126。我们的结果证实了L在三方核心-S-L相互作用中的关键作用,并识别直接核心互动中涉及的残留物。该模型对于研究药物抑制HBV核心包络相互作用的潜力可能是有价值的。

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