首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Trafficking of ODV-E66 is mediated via a sorting motif and other viral proteins: Facilitated trafficking to the inner nuclear membrane.
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Trafficking of ODV-E66 is mediated via a sorting motif and other viral proteins: Facilitated trafficking to the inner nuclear membrane.

机译:ODV-E66的贩运通过排序基序和其他病毒蛋白介导:促进向内核膜的贩运。

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The N-terminal 33 aa of the envelope protein ODV-E66 are sufficient to traffic fusion proteins to intranuclear membranes and the ODV envelope during infection with Autographa californica nucleopolyhedrovirus. This sequence has two distinct features: (i) an extremely hydrophobic sequence of 18 aa and (ii) positively charged amino acids close to the C-terminal end of the hydrophobic sequence. In the absence of infection, this sequence is sufficient to promote protein accumulation at the inner nuclear membrane. Covalent cross-linking results show that the lysines of the motif are proximal to FP25K and/or BV/ODV-E26 during transit from the endoplasmic reticulum to the nuclear envelope. We propose that the 33 aa comprise a signature for sorting proteins to the inner nuclear membrane (sorting motif) and that, unlike other resident proteins of the inner nuclear membrane, ODV-E66 and sortingmotif fusions do not randomly diffuse from their site of insertion at the endoplasmic reticulum to the nuclear envelope and viral-induced intranuclear membranes. Rather, during infection, trafficking is mediated by protein-protein interactions.
机译:包膜蛋白ODV-E66的N末端33aa足以在融合加利福尼亚州卷柏核多角体病毒感染期间将融合蛋白运输至核内膜和ODV包膜。该序列具有两个不同的特征:(i)18个氨基酸的极疏水序列和(ii)靠近疏水序列C端的带正电荷的氨基酸。在没有感染的情况下,该序列足以促进蛋白质在内核膜上的积累。共价交联结果表明,在从内质网转移到核膜的过程中,基序的赖氨酸与FP25K和/或BV / ODV-E26接近。我们建议33 aa包含一个将蛋白分类到内核膜的特征(分类基序),并且与内核膜的其他常驻蛋白不同,ODV-E66和sortingmotif融合体不会从其插入位点随机扩散内质网到核膜和病毒诱导的核内膜。相反,在感染过程中,贩运是由蛋白质与蛋白质的相互作用介导的。

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