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Structure-based mechanism for Na+/melibiose symport by MelB

机译:MelB的Na + /近等速共生的基于结构的机制

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摘要

The bacterial melibiose permease (MelB) belongs to the glycoside–pentoside–hexuronide:cation symporter family, a part of the major facilitator superfamily (MFS). Structural information regarding glycoside–pentoside–hexuronide:cation symporter family transporters and other Na+-coupled permeases within MFS has been lacking, although a wealth of biochemical and biophysical data are available. Here we present the three-dimensional crystal structures of Salmonella typhimurium MelBSt in two conformations, representing an outward partially occluded and an outward inactive state of MelBSt. MelB adopts a typical MFS fold and contains a previously unidentified cation-binding motif. Three conserved acidic residues form a pyramidal-shaped cation-binding site for Na+, Li+ or H+, which is in close proximity to the sugar-binding site. Both cosubstrate-binding sites are mainly contributed by the residues from the amino-terminal domain. These two structures and the functional data presented here provide mechanistic insights into Na+/melibiose symport. We also postulate a structural foundation for the conformational cycling necessary for transport catalysed by MFS permeases in general.
机译:细菌melibiose通透酶(MelB)属于糖苷-戊糖苷-己糖苷:阳离子同向转运蛋白家族,是主要促进子超家族(MFS)的一部分。尽管缺乏大量的生化和生物物理数据,但关于MFS中糖苷-戊糖苷-己糖苷:阳离子转运蛋白家族转运蛋白和其他Na + 偶联渗透酶的结构信息仍然缺乏。在这里,我们以两种构象展示鼠伤寒沙门氏菌MelBSt的三维晶体结构,分别代表MelBSt的向外部分被阻塞和向外处于非活性状态。 MelB采用典型的MFS折叠,并包含一个以前无法识别的阳离子结合基序。三个保守的酸性残基形成Na + ,Li + 或H + 的金字塔形阳离子结合位点,与糖结合位点。两个共底物结合位点主要由氨基末端结构域的残基贡献。此处介绍的这两个结构和功能数据为Na + /微共生对称运动提供了机械方面的见识。我们还为一般由MFS渗透酶催化的运输所必需的构象循环提供了结构基础。

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