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Flexibility in HIV-1 assembly subunits: Solution structure of the monomeric C-terminal domain of the capsid protein

机译:HIV-1装配亚基的灵活性:衣壳蛋白单体C末端结构域的溶液结构

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摘要

The protein CA forms the mature capsid of human immunodeficiency virus. Hexamerization of the N-terminal domain and dimerization of the C-terminal domain, CAC, occur during capsid assembly, and both domains constitute potential targets for anti- HIV inhibitors. CAC homodimerization occurs mainly through its second helix, and is abolished when its sole tryptophan is mutated to alanine. Previous thermodynamic data obtained with the dimeric and monomeric forms of CAC indicate that the structure of the mutant resembles that of a monomeric intermediate found in the folding and association reactions of CAC. We have solved the three- dimensional structure in aqueous solution of the monomeric mutant. The structure is similar to that of the subunits in the dimeric, nonmutated CAC, except the segment corresponding to the second helix, which is highly dynamic. At the end of this region, the polypeptide chain is bent to bury several hydrophobic residues and, as a consequence, the last two helices are rotated 90 degrees when compared to their position in dimeric CAC. The previously obtained thermodynamic data are consistent with the determined structure of the monomeric mutant. This extraordinary ability of CAC to change its structure may contribute to the different modes of association of CA during HIV assembly, and should be taken into account in the design of new drugs against this virus.
机译:蛋白质CA形成人免疫缺陷病毒的成熟衣壳。 N末端结构域的六聚体化和C末端结构域CAC的二聚化发生在衣壳组装过程中,并且两个结构域均构成抗HIV抑制剂的潜在靶标。 CAC同二聚化主要通过其第二个螺旋发生,并且当其唯一的色氨酸突变为丙氨酸时被废除。用CAC的二聚体和单体形式获得的先前热力学数据表明,突变体的结构类似于在CAC的折叠和缔合反应中发现的单体中间体的结构。我们已经解决了单体突变体在水溶液中的三维结构。该结构与二聚体非突变型CAC中的亚基相似,只是对应于第二个螺旋的片段是高度动态的。在该区域的末端,弯曲多肽链以掩埋几个疏水残基,结果,与它们在二聚体CAC中的位置相比,最后两个螺旋旋转了90度。先前获得的热力学数据与所确定的单体突变体的结构一致。 CAC改变其结构的非凡能力可能会导致在HIV组装过程中CA缔合的不同模式,并且在设计针对该病毒的新药时应予以考虑。

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