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关于将dTDP - D - 葡萄糖转化为dTDP - L - 鼠李糖的酶的结构视角。

A structural perspective on the enzymes that convert dTDP-d-glucose into dTDP-l-rhamnose.

作者信息

Dong C, Beis K, Giraud M-F, Blankenfeldt W, Allard S, Major L L, Kerr I D, Whitfield C, Naismith J H

机构信息

Centre for Biomolecular Science, The University, St. Andrews KY16 9ST, UK.

出版信息

Biochem Soc Trans. 2003 Jun;31(Pt 3):532-6. doi: 10.1042/bst0310532.

Abstract

Bacteria have a rich collection of biochemical pathways for the synthesis of complex metabolites. These conversions often involve chemical reactions that are hard to reproduce in the laboratory. An area of considerable interest is in the manipulation and synthesis of carbohydrates. In contrast with amino acids, carbohydrates are densely functionalized (each carbon atom is attached to at least one heteroatom) and this holds out the prospect of discovering novel enzyme mechanisms. The results from the study of the biosynthetic dTDP-L-rhamnose pathway are discussed. dTDP-L-rhamnose is a key intermediate in many pathogenic bacteria, as it is the donor for L-rhamnose, which is found in the cell wall of important human pathogens, such as Mycobacteria tuberculosis and Salmonella typhimurium. All four enzymes have been structurally characterized; in particular, the acquisition of structural data on substrate complexes was extremely useful. The structural data have guided site-directed-mutagenesis studies that have been used to test mechanistic hypotheses. The results shed light on three classes of enzyme mechanism: nucleotide condensation, short-chain dehydrogenase activity and epimerization.

摘要

细菌拥有丰富的生物化学途径来合成复杂的代谢产物。这些转化过程通常涉及在实验室中难以重现的化学反应。一个备受关注的领域是碳水化合物的操纵和合成。与氨基酸不同,碳水化合物具有密集的官能团化(每个碳原子至少连接一个杂原子),这为发现新的酶机制带来了希望。本文讨论了生物合成dTDP-L-鼠李糖途径的研究结果。dTDP-L-鼠李糖是许多致病细菌中的关键中间体,因为它是L-鼠李糖的供体,L-鼠李糖存在于重要人类病原体(如结核分枝杆菌和鼠伤寒沙门氏菌)的细胞壁中。所有四种酶都已进行了结构表征;特别是,底物复合物结构数据的获取非常有用。这些结构数据指导了定点诱变研究,这些研究已被用于检验机制假说。研究结果揭示了三类酶机制:核苷酸缩合、短链脱氢酶活性和差向异构化。

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