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过氧化物酶体循环受体Pex5p的N端一半是一个天然未折叠结构域。

The N-terminal half of the peroxisomal cycling receptor Pex5p is a natively unfolded domain.

作者信息

Carvalho Andreia F, Costa-Rodrigues João, Correia Isabel, Costa Pessoa João, Faria Tiago Q, Martins Cristina L, Fransen Marc, Sá-Miranda Clara, Azevedo Jorge E

机构信息

Instituto de Biologia Molecular e Celular, Rua do Campo Alegre, 823, 4150-180 Porto, Portugal.

出版信息

J Mol Biol. 2006 Mar 3;356(4):864-75. doi: 10.1016/j.jmb.2005.12.002. Epub 2005 Dec 19.

Abstract

Targeting of most newly synthesised peroxisomal matrix proteins to the organelle requires Pex5p, the so-called PTS1 receptor. According to current models of peroxisomal biogenesis, Pex5p interacts with these proteins in the cytosol, transports them to the peroxisomal membrane and catalyses their translocation across the membrane. Presently, our knowledge on the structural details behind the interaction of Pex5p with the cargo proteins is reasonably complete. In contrast, information regarding the structure of the Pex5p N-terminal half (a region containing its peroxisomal targeting domain) is still limited. We have recently observed that the Stokes radius of this Pex5p domain is anomalously large, suggesting that this portion of the protein is either a structured elongated domain or that it adopts a low compactness conformation. Here, we address this issue using a combination of biophysical and biochemical approaches. Our results indicate that the N-terminal half of Pex5p is best described as a natively unfolded pre-molten globule-like domain. The implications of these findings on the mechanism of protein import into the peroxisome are discussed.

摘要

大多数新合成的过氧化物酶体基质蛋白靶向该细胞器需要Pex5p,即所谓的PTS1受体。根据目前过氧化物酶体生物发生的模型,Pex5p在细胞质中与这些蛋白相互作用,将它们转运到过氧化物酶体膜并催化它们跨膜转运。目前,我们对Pex5p与货物蛋白相互作用背后的结构细节的了解相当完整。相比之下,关于Pex5p N端一半(包含其过氧化物酶体靶向结构域的区域)结构的信息仍然有限。我们最近观察到该Pex5p结构域的斯托克斯半径异常大,这表明该蛋白的这一部分要么是一个结构化的延伸结构域,要么是它采用了低紧密性构象。在这里,我们结合生物物理和生化方法来解决这个问题。我们的结果表明,Pex5p的N端一半最好被描述为一个天然未折叠的类前熔球结构域。讨论了这些发现对蛋白质导入过氧化物酶体机制的影响。

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