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首页> 外文期刊>Acta crystallographica. Section F, Structural biology communications >The ribosome and its role in protein folding: looking through a magnifying glass
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The ribosome and its role in protein folding: looking through a magnifying glass

机译:核糖体及其在蛋白质折叠中的作用:通过放大镜看

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Protein folding, a process that underpins cellular activity, begins co-translationally on the ribosome. During translation, a newly synthesized polypeptide chain enters the ribosomal exit tunnel and actively interacts with the ribosome elements - the r-proteins and rRNA that line the tunnel - prior to emerging into the cellular milieu. While understanding of the structure and function of the ribosome has advanced significantly, little is known about the process of folding of the emerging nascent chain (NC). Advances in cryoelectron microscopy are enabling visualization of NCs within the exit tunnel, allowing early glimpses of the interplay between the NC and the ribosome. Once it has emerged from the exit tunnel into the cytosol, the NC (still attached to its parent ribosome) can acquire a range of conformations, which can be characterized by NMR spectroscopy. Using experimental restraints within molecular-dynamics simulations, the ensemble of NC structures can be described. In order to delineate the process of co-translational protein folding, a hybrid structural biology approach is foreseeable, potentially offering a complete atomic description of protein folding as it occurs on the ribosome.
机译:蛋白质折叠,一个底层活性的过程,在核糖体上共同翻译。在翻译期间,新合成的多肽链进入核糖体出口隧道,并主动与核糖体元素相互作用 - 在出现进入细胞内部的隧道之前的R-蛋白和RRNA。虽然了解核糖体的结构和功能显着提出,但是关于新出现的新生链链(NC)的折叠过程很少。冷冻电子显微镜的进展在出口隧道内能够可视化NCS,允许早期瞥见NC和核糖体之间的相互作用。一旦从出口隧道出来进入胞质溶胶中,NC(仍然附着在其亲本核糖体)中就可以获得一系列构象,其可以通过NMR光谱表征。在分子动力学模拟中使用实验限制,可以描述NC结构的集合。为了描绘共转化蛋白折叠的过程,混合结构生物学方法可预见,可能提供蛋白质折叠的完全原子描述,因为它发生在核糖体上。

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