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首页> 外文期刊>Nucleic Acids Research >Molecular determinants of HIV-1 NCp7 chaperone activity in maturation of the HIV-1 dimerization initiation site
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Molecular determinants of HIV-1 NCp7 chaperone activity in maturation of the HIV-1 dimerization initiation site

机译:HIV-1二聚化起始位点成熟中HIV-1 NCp7伴侣活性的分子决定因素。

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Human immunodeficiency virus genome dimeriza-tion is initiated through an RNA-RNA kissing interaction formed via the dimerization initiation site (DIS) loop sequence, which has been proposed to be converted to a more thermodynamically stable linkage by the viral p7 form of the nucleocapsid protein (NC). Here, we systematically probed the role of specific amino acids of NCp7 in its chaperone activity in the DIS conversion using 2-aminopurine (2-AP) fluorescence and nuclear magnetic resonance spectroscopy. Through comparative analysis of NCp7 mutants, the presence of positively charged residues in the N-terminus was found to be essential for both helix destabilization and strand transfer functions. It was also observed that the presence and type of the Zn finger is important for NCp7 chaperone activity, but not the order of the Zn fingers. Swapping single aromatic residues between Zn fingers had a significant effect on NCp7 activity; however, these mutants did not exhibit the same activity as mutantsin which the order of the Zn fingers was changed, indicating a functional role for other flanking residues. RNA chaperone activity is further correlated with NCp7 structure and interaction with RNA through comparative analysis of nuclear magnetic resonance spectra of NCp7 variants, and complexes of these proteins with the DIS dimer.
机译:人类免疫缺陷病毒基因组二聚化是通过二聚化起始位点(DIS)环序列形成的RNA-RNA接吻相互作用来启动的,该相互作用已被建议通过病毒衣壳蛋白的p7形式转化为更热力学稳定的连接(NC)。在这里,我们使用2-氨基嘌呤(2-AP)荧光和核磁共振波谱系统研究了NCp7特定氨基酸在其伴侣分子活性中的DIS转化作用。通过对NCp7突变体的比较分析,发现N末端带正电荷的残基对于螺旋去稳定和链转移功能都是必不可少的。还观察到,锌指的存在和类型对于NCp7分子伴侣活性很重要,但对锌指的顺序并不重要。在锌指之间交换单个芳族残基对NCp7活性有重要影响;然而,这些突变体没有表现出与突变体相同的活性,而锌指的顺序发生了改变,这表明其他侧翼残基具有功能性作用。通过对NCp7变体的核磁共振谱以及这些蛋白与DIS二聚体的复合物进行比较分析,RNA伴侣活性进一步与NCp7结构和与RNA的相互作用相关。

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