Medium- and short-chain dehydrogenase/reductase gene and protein families

生物化学 辅因子 NAD+激酶 生物 活动站点 脱氢酶 结合位点 序列母题 共识序列 氧化还原酶 保守序列 沃克图案 肽序列 核苷酸 化学 立体化学 基因 ATP酶 ATP水解
作者
K.L. Kavanagh,Hans Jörnvall,Bengt Persson,Udo Oppermann
出处
期刊:Cellular and Molecular Life Sciences [Springer Nature]
卷期号:65 (24) 被引量:786
标识
DOI:10.1007/s00018-008-8588-y
摘要

Short-chain dehydrogenases/reductases (SDRs) constitute a large family of NAD(P)(H)-dependent oxidoreductases, sharing sequence motifs and displaying similar mechanisms. SDR enzymes have critical roles in lipid, amino acid, carbohydrate, cofactor, hormone and xenobiotic metabolism as well as in redox sensor mechanisms. Sequence identities are low, and the most conserved feature is an α/β folding pattern with a central beta sheet flanked by 2–3 α-helices from each side, thus a classical Rossmannfold motif for nucleotide binding. The conservation of this element and an active site, often with an Asn-Ser-Tyr-Lys tetrad, provides a platform for enzymatic activities encompassing several EC classes, including oxidoreductases, epimerases and lyases. The common mechanism is an underlying hydride and proton transfer involving the nicotinamide and typically an active site tyrosine residue, whereas substrate specificity is determined by a variable C-terminal segment. Relationships exist with bacterial haloalcohol dehalogenases, which lack cofactor binding but have the active site architecture, emphasizing the versatility of the basic fold in also generating hydride transfer-independent lyases. The conserved fold and nucleotide binding emphasize the role of SDRs as scaffolds for an NAD(P)(H) redox sensor system, of importance to control metabolic routes, transcription and signalling.
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