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Characterization of HIV-1 resistance to a fusion inhibitor, N36, derived from the gp41 amino-terminal heptad repeat.

机译:HIV-1对融合抑制剂N36(源自gp41氨基末端七肽重复序列)的抗性特征。

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摘要

A transmembrane glycoprotein of HIV-1, gp41, plays a central role in membrane fusion of HIV-1 and host cells. Peptides derived from the amino- and carboxyl-terminal heptad repeat (N-HR and C-HR, respectively) of gp41 inhibit this fusion. The mechanism of resistance to enfuvirtide, a C-HR-derived peptide, is well defined; however the mechanism of resistance to N-HR-derived peptides remains unclear. We characterized an HIV-1 isolate resistant to the N-HR-derived peptide, N36. This HIV-1 acquired a total of four amino acid substitutions, D36G, N126K and E137Q in gp41, and P183Q in gp120. Among these substitutions, N126K and/or E137Q conferred resistance to not only N36, but also C34, which is the corresponding C-HR-derived peptide fusion inhibitor. We performed crystallographic and biochemical analysis of the 6-helix bundle formed by synthetic gp41-derived peptides containing the N126K/E137Q substitutions. The structure of the 6-helix bundle with N126K/E137Q was identical to that in wild-type HIV-1 except for the presence of a new hydrogen bond. Denaturing experiments revealed that the stability of the 6-helix bundle of N126K/E137Q is greater than in the wild-type. These results suggest that the stabilizing effect of N126K/E137Q provides resistance to N36 and C34.
机译:HIV-1的跨膜糖蛋白gp41在HIV-1与宿主细胞的膜融合中起核心作用。来自gp41氨基末端和羧基末端七肽重复序列的肽(分别为N-HR和C-HR)抑制了这种融合。对恩夫韦肽(一种C-HR衍生肽)的抗性机制已明确定义;然而,对N-HR衍生肽的抗性机制仍不清楚。我们表征了对N-HR衍生肽N36具有抗性的HIV-1分离株。该HIV-1总共获得了四个氨基酸取代,gp41中的D36G,N126K和E137Q,gp120中的P183Q。在这些取代中,N126K和/或E137Q不仅赋予对N36的抗性,还赋予对相应C-HR衍生肽融合抑制剂C34的抗性。我们对包含N126K / E137Q取代的合成gp41衍生肽形成的6螺旋束进行了晶体学和生化分析。 N126K / E137Q的6螺旋束的结构与野生型HIV-1相同,只是存在新的氢键。变性实验表明,N126K / E137Q的6螺旋束的稳定性高于野生型。这些结果表明,N126K / E137Q的稳定作用提供了对N36和C34的抗性。

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