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Structure of a protein phosphatase 2A holoenzyme: insights into B55-mediated Tau dephosphorylation.蛋白磷酸酶2A全酶的结构:对B55介导的 Tau 去磷酸化的见解
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寡聚半乳糖醛酸裂解酶的活性部位为细胞质寡聚半乳糖醛酸 β 消除提供了独特的见解。

The active site of oligogalacturonate lyase provides unique insights into cytoplasmic oligogalacturonate beta-elimination.

机构信息

Complex Carbohydrate Research Center, University of Georgia, Athens, Georgia 30602, USA.

出版信息

J Biol Chem. 2010 Dec 10;285(50):39029-38. doi: 10.1074/jbc.M110.153981. Epub 2010 Sep 17.

DOI:10.1074/jbc.M110.153981
PMID:20851883
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2998093/
Abstract

Oligogalacturonate lyases (OGLs; now also classified as pectate lyase family 22) are cytoplasmic enzymes found in pectinolytic members of Enterobacteriaceae, such as the enteropathogen Yersinia enterocolitica. OGLs utilize a β-elimination mechanism to preferentially catalyze the conversion of saturated and unsaturated digalacturonate into monogalacturonate and the 4,5-unsaturated monogalacturonate-like molecule, 5-keto-4-deoxyuronate. To provide mechanistic insights into the specificity of this enzyme activity, we have characterized the OGL from Y. enterocolitica, YeOGL, on oligogalacturonides and determined its three-dimensional x-ray structure to 1.65 Å. The model contains a Mn(2+) atom in the active site, which is coordinated by three histidines, one glutamine, and an acetate ion. The acetate mimics the binding of the uronate group of galactourono-configured substrates. These findings, in combination with enzyme kinetics and metal supplementation assays, provide a framework for modeling the active site architecture of OGL. This enzyme appears to contain a histidine for the abstraction of the α-proton in the -1 subsite, a residue that is highly conserved throughout the OGL family and represents a unique catalytic base among pectic active lyases. In addition, we present a hypothesis for an emerging relationship observed between the cellular distribution of pectate lyase folding and the distinct metal coordination chemistries of pectate lyases.

摘要

寡聚半乳糖醛酸裂解酶(OGLs;现在也被归类为果胶裂解酶家族 22)是存在于肠杆菌科果胶分解成员中的细胞质酶,如肠道病原体肠炎沙门氏菌。OGL 利用β消除机制优先催化饱和和不饱和二半乳糖醛酸转化为单半乳糖醛酸和 4,5-不饱和单半乳糖醛酸样分子,5-酮-4-脱氧尿苷酸。为了深入了解该酶活性的特异性,我们对肠炎沙门氏菌的 OGL(YeOGL)在寡聚半乳糖醛酸上的特性进行了表征,并确定了其三维 X 射线结构,分辨率为 1.65Å。该模型包含一个位于活性位点的 Mn(2+)原子,由三个组氨酸、一个谷氨酰胺和一个醋酸盐离子配位。醋酸盐模拟了半乳糖构型底物的醛酸基团的结合。这些发现,结合酶动力学和金属补充测定,为 OGL 的活性位点结构建模提供了一个框架。该酶似乎包含一个用于在-1 亚位点中提取α-质子的组氨酸,该残基在整个 OGL 家族中高度保守,代表了果胶活性裂解酶中独特的催化碱。此外,我们提出了一个假设,即观察到果胶裂解酶折叠的细胞分布与果胶裂解酶独特的金属配位化学之间存在新兴关系。