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首页> 外文期刊>Nucleic acids research >Mapping the RNA binding sites for human immunodeficiency virus type-1 Gag and NC proteins within the complete HIV-1 and -2 untranslated leader regions
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Mapping the RNA binding sites for human immunodeficiency virus type-1 Gag and NC proteins within the complete HIV-1 and -2 untranslated leader regions

机译:在完整的HIV-1和-2非翻译前导区内定位人免疫缺陷病毒1型Gag和NC蛋白的RNA结合位点

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摘要

Encapsidation of HIV-1 genomic RNA is mediated by specific interactions between the RNA packaging signal and the Gag protein. During maturation of the virion, the Gag protein is processed into smaller fragments, including the nucleocapsid (NC) domain which remains associated with the viral genomic RNA. We have investigated the binding of glutathione-S-transferase (GST) Gag and NC fusion proteins from HIV-1, to the entire HIV-1 and -2 leader RNA encompassing the packaging signal. We have mapped the binding sites at conditions where only about two complexes are formed and find that GST-Gag and GST-NC fusion proteins bind specifically to discrete sites within the leader. Analysis of the HIV-1 leader indicated that GST-Gag strongly associates with the PSI stem-loop and to a lesser extent with regions near the primer binding site. GST-NC binds the same regions but with reversed preferences. The HIV-1 proteins also interact specifically with the 54-leader of HIV-2 and the major site of interaction mapped to a stem-loop, with homology to the HIV-1 PSI stem-loop structure. The different specificities of Gag and NC may reflect functionally distinct roles in the viral replication, and suggest that the RNA binding specificity of NC is modulated by its structural context.
机译:HIV-1基因组RNA的衣壳化是由RNA包装信号与Gag蛋白之间的特异性相互作用介导的。在病毒体成熟期间,Gag蛋白被加工成较小的片段,包括仍然与病毒基因组RNA关联的核衣壳(NC)域。我们已经研究了来自HIV-1的谷胱甘肽S-转移酶(GST)Gag和NC融合蛋白与包含包装信号的整个HIV-1和-2前导RNA的结合。我们已经在仅形成大约两个复合物的条件下定位了结合位点,发现GST-Gag和GST-NC融合蛋白特异性结合至前导区内的离散位点。对HIV-1前导序列的分析表明,GST-Gag与PSI茎环密切相关,并且在较小程度上与引物结合位点附近的区域相关。 GST-NC绑定相同的区域,但具有相反的首选项。 HIV-1蛋白还与HIV-2的54位前导蛋白特异性相互作用,并且主要相互作用位点定位于茎环,与HIV-1 PSI茎环结构具有同源性。 Gag和NC的不同特异性可能反映了病毒复制中功能上不同的角色,并表明NC的RNA结合特异性受其结构背景的调节。

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