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Conformational Transition of Membrane-Associated Terminally Acylated HIV-1 Nef

机译:膜相关的末端酰化的HIV-1 Nef的构象转变。

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摘要

Many proteins are posttranslationally modified by acylation targeting them to lipid membranes. While methods such as X-ray crystallography and nuclear magnetic resonance are available to determine the structure of folded proteins in solution, the precise position of folded domains relative to a membrane remains largely unknown. We used neutron and X-ray reflection methods to measure the displacement of the core domain of HIV Nef from lipid membranes upon insertion of the N-terminal myristate group. Nef is one of several HIV-1 accessory proteins and an essential factor in AIDS progression. Upon insertion of the myristate and residues from the N-terminal arm, Nef transitions from a closed-toopen conformation that positions the core domain 70 ? from the lipid headgroups. This work rules out previous speculation that the Nef core remains closely associated with the membrane to optimize interactions with the cytoplasmic domain of MHC-1.
机译:许多蛋白质通过酰化作用将其靶向脂质膜进行翻译后修饰。尽管可以使用诸如X射线晶体学和核磁共振的方法来确定溶液中折叠蛋白的结构,但是折叠域相对于膜的精确位置仍然未知。我们使用中子和X射线反射方法来测量插入N末端肉豆蔻酸酯基团后,HIV Nef核心域从脂质膜的移位。 Nef是几种HIV-1辅助蛋白之一,也是AIDS进展的重要因素。在插入肉豆蔻酸酯和来自N-末端臂的残基时,Nef从定位核心结构域70→70的封闭-开放构象转变。来自脂类头基。这项工作排除了以前的推测,即Nef核心仍然与膜紧密结合,以优化与MHC-1胞质域的相互作用。

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