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全基因组分析β-桶状膜蛋白中的序列基序和反基序:丙氨酸-酪氨酸二分法和伴侣蛋白结合基序

Sequence motifs and antimotifs in beta-barrel membrane proteins from a genome-wide analysis: the Ala-Tyr dichotomy and chaperone binding motifs.

作者信息

Jackups Ronald, Cheng Sarah, Liang Jie

机构信息

Department of Bioengineering,SEO, MC-063, University of Illinois at Chicago, 851 S. Morgan Street, Room 218, Chicago, IL 60607-7052, USA.

出版信息

J Mol Biol. 2006 Oct 20;363(2):611-23. doi: 10.1016/j.jmb.2006.07.095. Epub 2006 Aug 15.

DOI:10.1016/j.jmb.2006.07.095
PMID:16973175
Abstract

Beta-barrel membrane proteins are found in the outer membrane of gram-negative bacteria, mitochondria, and chloroplasts. Although sequence motifs have been studied in alpha-helical membrane proteins and have been shown to play important roles in their assembly, it is not clear whether over-represented motifs and under-represented anti-motifs exist in beta-barrel membrane proteins. We have developed probabilistic models to identify sequence motifs of residue pairs on the same strand separated by an arbitrary number of residues. A rigorous statistical model is essential for this study because of the difficulty associated with the short length of the strands and the small amount of structural data. By comparing to the null model of exhaustive permutation of residues within the same beta-strand, propensity values of sequence patterns of two residues and p-values measuring statistical significance are calculated exactly by several analytical formulae we have developed or by enumeration. We find that there are characteristic sequence motifs and antimotifs in transmembrane (TM) beta-strands. The amino acid Tyr plays an important role in several such motifs. We find a general dichotomy consisting of favorable Aliphatic-Tyr sequence motifs and unfavorable Tyr-Aliphatic antimotifs. Tyr is also part of a terminal motif, YxF, which is likely to be important for chaperone binding. Our results also suggest several experiments that can help to elucidate the mechanisms of in vitro and in vivo folding of beta-barrel membrane proteins.

摘要

β-桶状膜蛋白存在于革兰氏阴性菌的外膜、线粒体和叶绿体中。虽然已经对α-螺旋膜蛋白中的序列基序进行了研究,并且已证明它们在其组装过程中发挥重要作用,但尚不清楚β-桶状膜蛋白中是否存在过度代表的基序和代表性不足的反基序。我们开发了概率模型来识别同一条链上被任意数量的残基隔开的残基对的序列基序。由于与链的短长度和少量结构数据相关的困难,严格的统计模型对于本研究至关重要。通过与同一条β链内残基的穷举排列的空模型进行比较,我们开发的几个解析公式或通过枚举精确计算两个残基的序列模式的倾向值和测量统计显著性的p值。我们发现在跨膜(TM)β链中存在特征性的序列基序和反基序。氨基酸酪氨酸在几个这样的基序中起重要作用。我们发现了一种普遍的二分法,由有利的脂肪族-酪氨酸序列基序和不利的酪氨酸-脂肪族反基序组成。酪氨酸也是末端基序YxF的一部分,这可能对伴侣蛋白结合很重要。我们的结果还提出了一些实验,这些实验有助于阐明β-桶状膜蛋白在体外和体内折叠的机制。

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