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通过部分结构化状态共翻译折叠血影蛋白结构域。

Cotranslational folding of spectrin domains via partially structured states.

机构信息

Department of Biochemistry and Biophysics Stockholm University, Stockholm, Sweden.

Department of Chemistry, University of Cambridge, Cambridge, UK.

出版信息

Nat Struct Mol Biol. 2017 Mar;24(3):221-225. doi: 10.1038/nsmb.3355. Epub 2017 Jan 23.

Abstract

How do the key features of protein folding, elucidated from studies on native, isolated proteins, manifest in cotranslational folding on the ribosome? Using a well-characterized family of homologous α-helical proteins with a range of biophysical properties, we show that spectrin domains can fold vectorially on the ribosome and may do so via a pathway different from that of the isolated domain. We use cryo-EM to reveal a folded or partially folded structure, formed in the vestibule of the ribosome. Our results reveal that it is not possible to predict which domains will fold within the ribosome on the basis of the folding behavior of isolated domains; instead, we propose that a complex balance of the rate of folding, the rate of translation and the lifetime of folded or partly folded states will determine whether folding occurs cotranslationally on actively translating ribosomes.

摘要

蛋白质折叠的关键特征是如何从对天然分离蛋白质的研究中阐明的?在核糖体上共翻译折叠中又是如何表现的?我们使用一系列具有不同生物物理特性的同源α-螺旋蛋白家族,表明 spectrin 结构域可以在核糖体上进行矢量折叠,并且可能通过与分离结构域不同的途径进行折叠。我们使用 cryo-EM 揭示了在核糖体前庭中形成的折叠或部分折叠结构。我们的结果表明,不能仅仅根据分离结构域的折叠行为来预测哪些结构域将在核糖体中折叠;相反,我们提出折叠速度、翻译速度和折叠或部分折叠状态的寿命之间的复杂平衡将决定折叠是否在活跃翻译的核糖体上共翻译发生。

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