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酵母和人类在将末端三肽识别为过氧化物酶体靶向信号1方面存在差异,这是由于它们的受体Pex5p对同源信号及其相邻残基的亲和力不同。

The difference in recognition of terminal tripeptides as peroxisomal targeting signal 1 between yeast and human is due to different affinities of their receptor Pex5p to the cognate signal and to residues adjacent to it.

作者信息

Lametschwandtner G, Brocard C, Fransen M, Van Veldhoven P, Berger J, Hartig A

机构信息

Institut fuer Biochemie und Molekulare Zellbiologie der Universitaet Wien and Ludwig Boltzmann-Forschungsstelle fuer Biochemie, Vienna Biocenter, Dr. Bohrgasse 9, A-1030 Wien, Austria.

出版信息

J Biol Chem. 1998 Dec 11;273(50):33635-43. doi: 10.1074/jbc.273.50.33635.

Abstract

Pex5p is the receptor for the peroxisomal targeting signal 1 (PTS1) that consists of a C-terminal tripeptide (consensus (S/A/C)(K/R/H)(L/M)). Hexadecapeptides recognized by Pex5p from Homo sapiens and Saccharomyces cerevisiae were identified by screening a two-hybrid peptide library, and the targeting ability of the peptides was demonstrated using the green fluorescent protein as reporter. The PTS1 receptors recognized in a species-specific manner a broad range of C-terminal tripeptides, and these are reported herein. In addition, residues upstream of the tripeptide influenced the strength of the interaction in the two-hybrid system as well as in an in vitro competition assay. In peptides interacting with the human protein, hydrophobic residues were found with high frequency especially at positions -2 and -5, whereas peptides interacting with S. cerevisiae Pex5p were more hydrophilic and frequently contained arginine at position -2. In instances where the terminal tripeptide deviated from the consensus, upstream residues exerted a greater influence on the ability of the hexadecapeptides to bind Pex5p.

摘要

Pex5p是过氧化物酶体靶向信号1(PTS1)的受体,PTS1由一个C端三肽(共有序列为(S/A/C)(K/R/H)(L/M))组成。通过筛选双杂交肽库,鉴定了来自人类和酿酒酵母的被Pex5p识别的十六肽,并使用绿色荧光蛋白作为报告基因证明了这些肽的靶向能力。PTS1受体以物种特异性方式识别广泛的C端三肽,本文对此进行了报道。此外,三肽上游的残基在双杂交系统以及体外竞争试验中影响相互作用的强度。在与人类蛋白相互作用的肽中,疏水残基尤其是在-2和-5位出现的频率很高,而与酿酒酵母Pex5p相互作用的肽更具亲水性,并且在-2位经常含有精氨酸。在末端三肽偏离共有序列的情况下,上游残基对十六肽结合Pex5p的能力影响更大。

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