Oppermann Udo, Filling Charlotta, Hult Malin, Shafqat Naeem, Wu Xiaoqiu, Lindh Monica, Shafqat Jawed, Nordling Erik, Kallberg Yvonne, Persson Bengt, Jörnvall Hans
Department of Medical Biochemistry and Biophysics, Karolinska Institutet, SE-17177, Stockholm, Sweden.
Chem Biol Interact. 2003 Feb 1;143-144:247-53. doi: 10.1016/s0009-2797(02)00164-3.
Short-chain dehydrogenases/reductases (SDR) form a large, functionally heterogeneous protein family presently with about 3000 primary and about 30 3D structures deposited in databases. Despite low sequence identities between different forms (about 15-30%), the 3D structures display highly similar alpha/beta folding patterns with a central beta-sheet, typical of the Rossmann-fold. Based on distinct sequence motifs functional assignments and classifications are possible, making it possible to build a general nomenclature system. Recent mutagenetic and structural studies considerably extend the knowledge on the general reaction mechanism, thereby establishing a catalytic tetrad of Asn-Ser-Tyr-Lys residues, which presumably form the framework for a proton relay system including the 2'-OH of the nicotinamide ribose, similar to the mechanism found in horse liver ADH. Based on their cellular functions, several SDR enzymes appear as possible and promising pharmacological targets with application areas spanning hormone-dependent cancer forms or metabolic diseases such as obesity and diabetes, and infectious diseases.
短链脱氢酶/还原酶(SDR)构成了一个庞大的、功能异质的蛋白质家族,目前数据库中存有大约3000个一级结构和约30个三维结构。尽管不同形式之间的序列同一性较低(约15%-30%),但其三维结构显示出高度相似的α/β折叠模式,具有典型的Rossmann折叠中央β-折叠片层。基于不同的序列基序,可以进行功能分配和分类,从而有可能建立一个通用的命名系统。最近的诱变和结构研究极大地扩展了对一般反应机制的认识,从而确立了由天冬酰胺-丝氨酸-酪氨酸-赖氨酸残基组成的催化四联体,推测这构成了一个质子传递系统的框架,该系统包括烟酰胺核糖的2'-OH,类似于在马肝乙醇脱氢酶中发现的机制。基于其细胞功能,几种SDR酶似乎是可能且有前景的药理学靶点,其应用领域涵盖激素依赖性癌症类型或代谢疾病,如肥胖症和糖尿病,以及传染病。
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