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The C34 Peptide Fusion Inhibitor Binds to the Six-Helix Bundle Core Domain of HIV-1 gp41 by Displacement of the C-Terminal Helical Repeat Region

机译:C34肽融合剂抑制剂通过C末端螺旋重复区域的位移与HIV-1 GP41的六螺旋束核心结构域结合

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摘要

The conformational transition of the core domain of HIV-1 gp41 from a prehairpin intermediate to a six-helix bundle is responsible for virus-cell fusion. Several inhibitors which target the N-heptad repeat helical coiled-coil trimer that is fully accessible in the prehairpin intermediate have been designed. One such inhibitor is the peptide C34 derived from the C-heptad repeat of gp41 that forms the exterior of the six-helix bundle. Here, using a variety of biophysical techniques, including dye tagging, size-exclusion chromatography combined with multiangle light scattering, double electron-electron resonance EPR spectroscopy, and circular dichroism, we investigate the binding of C34 to two six-helix bundle mimetics comprising N- and C-heptad repeats either without (core(SP)) or with (core(SP)) a short spacer connecting the two. In the case of core(SP), C34 directly exchanges with the C-heptad repeat. For cores, up to two molecules of C34 bind the six-helix bundle via displacement of the C-heptad repeat. These results suggest that fusion inhibitors such as C34 can target a continuum of transitioning conformational states from the prehairpin intermediate to the six-helix bundle prior to the occurrence of irreversible fusion of viral and target cell membranes.
机译:HIV-1GP41的核心结构域从预发素素中间体到六螺旋束的构象过渡是病毒细胞融合的原因。已经设计了几种靶向前一家中间体中可接近的N-庚隙重复螺旋卷绕式线圈三边形的抑制剂。一种这样的抑制剂是衍生自GP41的C-庚隙重复的肽C34,其形成六螺旋束的外部。在这里,使用多种生物物理技术,包括染料标记,尺寸排阻色谱法与多聚光散射相结合,双电子 - 电子共振EPR光谱和圆形二色性,我们研究了C34至两种六螺旋束模拟物的结合 - 并且C-庚段重复(核心(SP))或(核心(SP))连接两者的短垫片。在核心(SP)的情况下,C34直接与C-eptad重复交换。对于核心,最多两个C34分子通过C-庚隙重复的位移绑定六螺旋束。这些结果表明,诸如C34之类的融合抑制剂可以在发生病毒和靶细胞膜的不可逆融合之前从预发素中间体到六螺旋束的连续转换一致状态。

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