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Structural studies of the N-terminal fragments of the WW domain: Insights into co-translational folding of a beta-sheet protein

机译:WW域N末端片段的结构研究:深入了解β-折叠蛋白的共翻译折叠

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摘要

Nascent proteins fold co-translationally because the folding speed and folding pathways are limited by the rate of ribosome biosynthesis in the living cell. In addition, though full-length proteins can fold all their residues during the folding process, nascent proteins initially fold only with the N-terminal residues. However, the transient structure and the co-translational folding pathway are not well understood. Here we report the atomic structures of a series of N-terminal fragments of the WW domain with increasing amino acid length. Unexpectedly, the structures indicate that the intermediate-length fragments take helical conformations even though the full-length protein has no helical regions. The circular dichroism spectra and theoretical calculations also support the crystallographic results. This suggests that the short-range interactions are more decisive in the structure formation than the long-range interactions for short nascent proteins. In the course of the peptide extension, the helical structure change to the structure mediated by the long-range interactions at a particular polypeptide length. Our results will provide unique information for elucidating the nature of co-translational folding.
机译:新生蛋白质共翻译折叠,因为折叠速度和折叠途径受到活细胞中核糖体生物合成速率的限制。另外,尽管全长蛋白质可以在折叠过程中折叠其所有残基,但新生蛋白质最初仅与N末端残基折叠。但是,暂时的结构和共翻译折叠途径尚不十分清楚。在这里,我们报道了随着氨基酸长度的增加,WW结构域的一系列N末端片段的原子结构。出乎意料的是,该结构表明,即使全长蛋白没有螺旋区,中等长度的片段也具有螺旋构象。圆二色性光谱和理论计算也支持晶体学结果。这表明,短程相互作用比短新生蛋白的长程相互作用对结构形成的决定性作用更大。在肽延伸的过程中,螺旋结构改变为由在特定多肽长度的远程相互作用介导的结构。我们的结果将提供独特的信息,以阐明共翻译折叠的性质。

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