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色氨酸合酶通道受损突变体的动力学特性

Kinetic characterization of channel impaired mutants of tryptophan synthase.

作者信息

Anderson K S, Kim A Y, Quillen J M, Sayers E, Yang X J, Miles E W

机构信息

Yale University School of Medicine, Department of Pharmacology, New Haven, Connecticut 06520, USA.

出版信息

J Biol Chem. 1995 Dec 15;270(50):29936-44. doi: 10.1074/jbc.270.50.29936.

Abstract

Tryptophan synthase, an alpha 2 beta 2 tetrameric complex, is a classic example of an enzyme that is thought to "channel" a metabolic intermediate (indole) from the active site of the alpha subunit to the active site of the beta subunit. The solution of the three-dimensional structure of the enzyme from Salmonella typhimurium provided physical evidence for a 25-A hydrophobic tunnel which connects the alpha and beta active sites (Hyde, C. C., Ahmed, S. A., Padlan, E. A., Miles, E. W., and Davies, D. R. (1988) J. Biol. Chem. 263, 17857-17871). Using rapid reaction kinetics, we have previously established that indole is indeed channeled and have identified three essential kinetic features which govern efficient channeling. In the current study we have probed the necessity of these features by using site-directed mutagenesis to alter these requirements. We now report the kinetic characterization of two mutants which contain substitutions to block or restrict the tunnel (beta C170F and beta C170W). Preliminary kinetic and structural evidence of a restricted tunnel in the beta C170W has been provided (Schlichting, I., Yang, X. W., Miles, E. W., Kim, A. Y., and Anderson, K. S. (1994) J. Biol. Chem. 269, 26591-26593). The rapid kinetic analysis of these mutant proteins shows that these mutations interfere with efficient channeling of the indole metabolite such that indole can be observed in single enzyme turnover of the physiologically relevant alpha beta reaction. In addition, the beta C170W mutant appears to be impaired in alpha beta intersubunit communication.

摘要

色氨酸合成酶是一种α₂β₂四聚体复合物,是一种典型的酶,被认为能将代谢中间体(吲哚)从α亚基的活性位点“输送”到β亚基的活性位点。鼠伤寒沙门氏菌中该酶三维结构的解析为连接α和β活性位点的一条25埃的疏水通道提供了物理证据(海德,C.C.,艾哈迈德,S.A.,帕德兰,E.A.,迈尔斯,E.W.,和戴维斯,D.R.(1988年)《生物化学杂志》263卷,17857 - 17871页)。我们之前利用快速反应动力学确定吲哚确实是被输送的,并确定了控制有效输送的三个关键动力学特征。在当前研究中,我们通过定点诱变改变这些要求来探究这些特征的必要性。我们现在报告两个突变体的动力学特征,这两个突变体含有用于阻断或限制通道的取代(βC170F和βC170W)。已提供βC170W中通道受限的初步动力学和结构证据(施利希廷,I.,杨,X.W.,迈尔斯,E.W.,金,A.Y.,和安德森,K.S.(1994年)《生物化学杂志》269卷,26591 - 26593页)。对这些突变蛋白的快速动力学分析表明,这些突变干扰了吲哚代谢物的有效输送,以至于在生理相关的αβ反应的单酶周转中可以观察到吲哚。此外,βC170W突变体在αβ亚基间通讯方面似乎受损。

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