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磷酸酮醇酶的晶体结构:硫胺素二磷酸依赖性脱水机制。

Crystal structures of phosphoketolase: thiamine diphosphate-dependent dehydration mechanism.

机构信息

Department of Biotechnology, The University of Tokyo, 1-1-1 Yayoi, Bunkyo-ku, Tokyo 113-8657, Japan.

出版信息

J Biol Chem. 2010 Oct 29;285(44):34279-87. doi: 10.1074/jbc.M110.156281. Epub 2010 Aug 24.

Abstract

Thiamine diphosphate (ThDP)-dependent enzymes are ubiquitously present in all organisms and catalyze essential reactions in various metabolic pathways. ThDP-dependent phosphoketolase plays key roles in the central metabolism of heterofermentative bacteria and in the pentose catabolism of various microbes. In particular, bifidobacteria, representatives of beneficial commensal bacteria, have an effective glycolytic pathway called bifid shunt in which 2.5 mol of ATP are produced per glucose. Phosphoketolase catalyzes two steps in the bifid shunt because of its dual-substrate specificity; they are phosphorolytic cleavage of fructose 6-phosphate or xylulose 5-phosphate to produce aldose phosphate, acetyl phosphate, and H(2)O. The phosphoketolase reaction is different from other well studied ThDP-dependent enzymes because it involves a dehydration step. Although phosphoketolase was discovered more than 50 years ago, its three-dimensional structure remains unclear. In this study we report the crystal structures of xylulose 5-phosphate/fructose 6-phosphate phosphoketolase from Bifidobacterium breve. The structures of the two intermediates before and after dehydration (α,β-dihydroxyethyl ThDP and 2-acetyl-ThDP) and complex with inorganic phosphate give an insight into the mechanism of each step of the enzymatic reaction.

摘要

硫胺素焦磷酸(ThDP)依赖性酶普遍存在于所有生物体中,并催化各种代谢途径中的必需反应。ThDP 依赖性磷酸酮醇酶在异型发酵细菌的中心代谢和各种微生物的戊糖分解代谢中起关键作用。特别是双歧杆菌,有益共生菌的代表,具有一种有效的糖酵解途径,称为双歧分流,其中每葡萄糖产生 2.5 摩尔的 ATP。由于其双底物特异性,磷酸酮醇酶催化双歧分流中的两个步骤;它们是果糖 6-磷酸或木酮糖 5-磷酸的磷酸解裂解,产生醛糖磷酸、乙酰磷酸和 H(2)O。磷酸酮醇酶反应不同于其他研究充分的 ThDP 依赖性酶,因为它涉及脱水步骤。尽管磷酸酮醇酶早在 50 多年前就被发现,但它的三维结构仍不清楚。在这项研究中,我们报告了短双歧杆菌的木酮糖 5-磷酸/果糖 6-磷酸磷酸酮醇酶的晶体结构。脱水前后的两种中间产物(α,β-二羟乙基 ThDP 和 2-乙酰-ThDP)和与无机磷酸的复合物的结构深入了解了酶反应的每一步的机制。

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