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大肠杆菌甘露醇转运蛋白IImtl的B结构域和C结构域之间构象偶联的热力学证据。

Thermodynamic evidence for conformational coupling between the B and C domains of the mannitol transporter of escherichia coli, enzyme IImtl.

作者信息

Meijberg W, Schuurman-Wolters G K, Robillard G T

机构信息

Groningen Biomolecular Sciences and Biotechnology Institute and the Department of Biochemistry, University of Groningen, Nijenborgh 4, 9747 AG Groningen, The Netherlands.

出版信息

J Biol Chem. 1998 Apr 3;273(14):7949-56. doi: 10.1074/jbc.273.14.7949.

Abstract

The transport across the cytoplasmic membrane and concomitant phosphorylation of mannitol in Escherichia coli is catalyzed by the mannitol-specific transport protein from the phosphoenolpyruvate-dependent phosphotransferase system, enzyme IImtl. Interactions between the cytoplasmic B and the membrane embedded C domain play an important role in the catalytic cycle of this enzyme, but the nature of this interaction is largely unknown. We have studied the thermodynamics of binding of (i) mannitol to enzyme IImtl, (ii) the substrate analog perseitol to enzyme IImtl, (iii) perseitol to phosphorylated enzyme IImtl, and (iv) mannitol to enzyme IImtl treated with trypsin to eliminate the cytoplasmic domains. Analysis of the heat capacity increment of these reactions showed that approximately 50-60 residues are involved in the binding of mannitol and perseitol, but far less in the phosphorylated state or after removal of the B domain. A model is proposed in which binding of mannitol leads to the formation of a contact interface between the two domains, either by folding of unstructured parts or by docking of preexisting surfaces, thus positioning the incoming mannitol close to the phosphorylation site on the B domain to facilitate the transfer of the phosphoryl group.

摘要

在大肠杆菌中,磷酸烯醇式丙酮酸依赖性磷酸转移酶系统的甘露醇特异性转运蛋白IImtl催化甘露醇穿过细胞质膜并伴随其磷酸化。细胞质B结构域与嵌入膜的C结构域之间的相互作用在该酶的催化循环中起重要作用,但这种相互作用的本质在很大程度上尚不清楚。我们研究了以下几种结合的热力学:(i)甘露醇与IImtl酶的结合;(ii)底物类似物卫矛醇与IImtl酶的结合;(iii)卫矛醇与磷酸化的IImtl酶的结合;(iv)甘露醇与用胰蛋白酶处理以去除细胞质结构域的IImtl酶的结合。对这些反应的热容增量分析表明,约50 - 60个残基参与甘露醇和卫矛醇的结合,但在磷酸化状态下或去除B结构域后参与结合的残基要少得多。提出了一个模型,其中甘露醇的结合通过非结构化部分的折叠或预先存在的表面对接导致两个结构域之间形成接触界面,从而将进入的甘露醇定位在靠近B结构域上的磷酸化位点,以促进磷酰基的转移。

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