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利用氢键模式对(β/α)8蛋白中的β桶进行比对。

Alignment of beta-barrels in (beta/alpha)8 proteins using hydrogen-bonding pattern.

作者信息

Sergeev Y, Lee B

机构信息

Laboratory of Molecular Biology, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892.

出版信息

J Mol Biol. 1994 Nov 25;244(2):168-82. doi: 10.1006/jmbi.1994.1717.

Abstract

A multiple alignment procedure for aligning the beta-sheet residues of the (beta/alpha)8-barrel structures is described. It uses a two-dimensional numbering scheme which is based on the covalent and hydrogen-bonding pattern of the beta-sheet. Two different scoring functions were used: one measured the sequence and topological similarity and the other the root-mean-square deviation of the coordinates of the matched residues. The procedure was applied to obtain multiple alignments of the beta-barrels of ten (beta/alpha)8-barrel proteins of known structure. Two kinds of alignments were derived: one in which the beta-strand numbering was preserved and another in which the beta-strands were allowed to be cyclically permuted. It is shown that-preservation of the beta-strand numbering corresponds to aligning only the layer structure of the beta-barrels. In order to obtain the optimal rotational alignment of the barrels as well, the beta-strands must be allowed to be renumbered. Although the 2-fold or 4-fold rotational symmetry of the beta-barrels makes it difficult to obtain unique rotational alignment of the barrels, the results of the alignment indicate that the beta-strands in the beta-barrel of enolase, xylose isomerase, taka-amylase, and possibly fructose biphosphate aldolase, must be cyclically permuted in order to be optimally aligned to those of the other proteins, which include triose phosphate isomerase, the alpha-subunit of tryptophan synthetase, flavocytochrome b2, ribulose-1, 5-biphosphate carboxylase/oxygenase, and glycolate oxidase.

摘要

本文描述了一种用于比对(β/α)8桶状结构中β折叠残基的多重比对程序。它使用了一种基于β折叠的共价和氢键模式的二维编号方案。使用了两种不同的评分函数:一种衡量序列和拓扑相似性,另一种衡量匹配残基坐标的均方根偏差。该程序被应用于获得十个已知结构的(β/α)8桶状蛋白的β桶的多重比对。得到了两种比对结果:一种是保留β链编号,另一种是允许β链进行循环置换。结果表明,保留β链编号仅对应于比对β桶的层结构。为了也获得桶状结构的最佳旋转比对,必须允许β链重新编号。尽管β桶的2重或4重旋转对称性使得难以获得桶状结构的唯一旋转比对,但比对结果表明,烯醇化酶、木糖异构酶、高峰淀粉酶以及可能的果糖二磷酸醛缩酶的β桶中的β链必须进行循环置换,以便与其他蛋白质的β链进行最佳比对,这些蛋白质包括磷酸丙糖异构酶、色氨酸合成酶的α亚基、黄素细胞色素b2、核酮糖-1,5-二磷酸羧化酶/加氧酶和乙醇酸氧化酶。

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