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乙醇脱氢酶和多元醇脱氢酶都分为两种蛋白质类型,并且结构特性使每种类型中的不同酶活性相互关联。

Alcohol and polyol dehydrogenases are both divided into two protein types, and structural properties cross-relate the different enzyme activities within each type.

作者信息

Jörnvall H, Persson M, Jeffery J

出版信息

Proc Natl Acad Sci U S A. 1981 Jul;78(7):4226-30. doi: 10.1073/pnas.78.7.4226.

Abstract

Sorbitol dehydrogenase from sheep liver shows similarities to mammalian and yeast alcohol dehydrogenases. Comparisons based on peptides from segments of sorbitol dehydrogenase reveal that homologous regions with 38% identity include two ligands to the active site zinc atom in liver alcohol dehydrogenase, as well as further important residues. Similarities in in other regions are less extensive, exactly as they are between different alcohol dehydrogenases. In all aspects, sorbitol dehydrogenase appears as a typical member of the alcohol dehydrogenase family. On the other hand, alcohol dehydrogenase from Drosophila, which has a shorter subunit, is not closely related to either of these enzymes, except for a region that probably corresponds to the first part of the coenzyme binding domain in many dehydrogenases. Instead, Drosophila alcohol dehydrogenase in its supposed catalytic region shows similarities toward Klebsiella ribitol dehydrogenase, which also has a small subunit. It may be concluded that both alcohol and polyol dehydrogenases show two types of protein subunit, reflecting an early subdivision of polypeptide types into "long" and "short" subunits rather than into different enzymatic specificities or quaternary structures. The relationships explain known properties of all these enzymes and provide insight into functional mechanisms and evolutionary interpretations.

摘要

绵羊肝脏中的山梨醇脱氢酶与哺乳动物和酵母的醇脱氢酶有相似之处。基于山梨醇脱氢酶片段的肽段进行比较发现,具有38%同一性的同源区域包括肝脏醇脱氢酶活性位点锌原子的两个配体以及其他重要残基。其他区域的相似性则没那么广泛,这与不同醇脱氢酶之间的情况完全相同。在各个方面,山梨醇脱氢酶都表现为醇脱氢酶家族的典型成员。另一方面,果蝇的醇脱氢酶亚基较短,除了一个可能对应于许多脱氢酶辅酶结合域第一部分的区域外,它与这两种酶都没有密切关系。相反,果蝇醇脱氢酶在其假定的催化区域与同样具有小亚基的克雷伯氏菌核糖醇脱氢酶有相似之处。可以得出结论,醇脱氢酶和多元醇脱氢酶都有两种类型的蛋白质亚基,这反映了多肽类型早期分为“长”亚基和“短”亚基,而不是分为不同的酶特异性或四级结构。这些关系解释了所有这些酶的已知特性,并为功能机制和进化解释提供了见解。

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