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硫氧还蛋白折叠超家族中功能的分化:过氧化物氧还蛋白从硫氧还蛋白样祖先进化而来的证据。

Divergence of function in the thioredoxin fold suprafamily: evidence for evolution of peroxiredoxins from a thioredoxin-like ancestor.

作者信息

Copley Shelley D, Novak Walter R P, Babbitt Patricia C

机构信息

Department of Molecular, Cellular, and Developmental Biology, University of Colorado, Boulder, Colorado 80309, USA.

出版信息

Biochemistry. 2004 Nov 9;43(44):13981-95. doi: 10.1021/bi048947r.

Abstract

The thioredoxin fold is found in proteins that serve a wide variety of functions. Among these are peroxiredoxins, which catalyze the reduction of hydrogen peroxide and alkyl peroxides. Although the common structural fold shared by thioredoxins and peroxiredoxins suggests the possibility that they have evolved from a common progenitor, it has been difficult to examine this hypothesis in depth because pairwise sequence identities between proteins in these two superfamilies are statistically insignificant. Using the Shotgun program, we have found that sequences of reductases involved in maturation of cytochromes in certain bacteria bridge the sequences of thioredoxins and peroxiredoxins. Analysis of motifs found in a divergent set of thioredoxins, cytochrome maturation proteins, and peroxiredoxins provides further support for an evolutionary relationship between these proteins. Within the conserved motifs are specific residues that are characteristic of individual protein classes, and therefore are likely to be involved in the specific functions of those classes. We have used this information, in combination with existing structural and functional information, to gain new insight into the structure-function relationships in these proteins and to construct a model for the emergence of peroxiredoxins from a thioredoxin-like ancestor.

摘要

硫氧还蛋白折叠存在于具有多种功能的蛋白质中。其中包括过氧化物还原酶,它催化过氧化氢和烷基过氧化物的还原。尽管硫氧还蛋白和过氧化物还原酶共有的常见结构折叠表明它们可能由共同的祖先进化而来,但由于这两个超家族中蛋白质之间的成对序列同一性在统计学上不显著,因此很难深入研究这一假设。使用Shotgun程序,我们发现某些细菌中参与细胞色素成熟的还原酶序列连接了硫氧还蛋白和过氧化物还原酶的序列。对一组不同的硫氧还蛋白、细胞色素成熟蛋白和过氧化物还原酶中发现的基序进行分析,为这些蛋白质之间的进化关系提供了进一步的支持。在保守基序中存在特定的残基,这些残基是各个蛋白质类别的特征,因此可能参与这些类别的特定功能。我们结合现有的结构和功能信息,利用这些信息对这些蛋白质的结构-功能关系有了新的认识,并构建了一个从类似硫氧还蛋白的祖先中出现过氧化物还原酶的模型。

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