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肉毒梭菌 C143S 硫胺素酶 I/硫胺素复合物的结构揭示了活性位点结构。

Structure of a Clostridium botulinum C143S thiaminase I/thiamin complex reveals active site architecture .

机构信息

Department of Chemistry and Chemical Biology, Cornell University , Ithaca, New York 14853, United States.

出版信息

Biochemistry. 2013 Nov 5;52(44):7830-9. doi: 10.1021/bi400841g. Epub 2013 Oct 25.

Abstract

Thiaminases are responsible for the degradation of thiamin and its metabolites. Two classes of thiaminases have been identified based on their three-dimensional structures and their requirements for a nucleophilic second substrate. Although the reactions of several thiaminases have been characterized, the physiological role of thiamin degradation is not fully understood. We have determined the three-dimensional X-ray structure of an inactive C143S mutant of Clostridium botulinum (Cb) thiaminase I with bound thiamin at 2.2 Å resolution. The C143S/thiamin complex provides atomic level details of the orientation of thiamin upon binding to Cb-thiaminase I and the identity of active site residues involved in substrate binding and catalysis. The specific roles of active site residues were probed by using site directed mutagenesis and kinetic analyses, leading to a detailed mechanism for Cb-thiaminase I. The structure of Cb-thiaminase I is also compared to the functionally similar but structurally distinct thiaminase II.

摘要

硫胺素酶负责硫胺素及其代谢物的降解。根据其三维结构和对亲核第二底物的要求,已经确定了两类硫胺素酶。尽管已经对几种硫胺素酶的反应进行了表征,但硫胺素降解的生理作用仍未完全理解。我们已经确定了结合硫胺素的产毒梭菌(Cb)硫胺素酶 I 的 C143S 无活性突变体的三维 X 射线结构,分辨率为 2.2Å。C143S/硫胺素复合物提供了硫胺素与 Cb-硫胺素酶 I 结合时的取向以及参与底物结合和催化的活性位点残基的原子水平细节。通过使用定点突变和动力学分析来探测活性位点残基的特定作用,从而为 Cb-硫胺素酶 I 提出了详细的机制。还将 Cb-硫胺素酶 I 的结构与功能相似但结构不同的硫胺素酶 II 进行了比较。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/caea/3883099/cb03d801d119/nihms529827f1.jpg

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