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溶质会改变膜转运蛋白中的构象转变。

Solutes modify a conformational transition in a membrane transport protein.

作者信息

Kim Miyeon, Xu Qi, Fanucci Gail E, Cafiso David S

机构信息

Department of Chemistry and Biophysics Program, University of Virginia, Charlottesville, 22904-4319, USA.

出版信息

Biophys J. 2006 Apr 15;90(8):2922-9. doi: 10.1529/biophysj.105.078246. Epub 2006 Jan 27.

Abstract

The bacterial outer-membrane vitamin B(12) transporter, BtuB, undergoes a dramatic order-to-disorder transition in its N-terminal energy-coupling motif (Ton box) upon substrate binding. Here, site-directed spin labeling (SDSL) is used to show that a range of solutes prevents this conformational change when ligand is bound to BtuB, resulting in a more ordered Ton box structure. For each solute examined, the data indicate that solutes effectively block this conformational transition through an osmotic mechanism. The molecular weight dependence of this solute effect has been examined for a series of polyethylene glycols, and a sharp molecular weight cutoff is observed. This cutoff indicates that solutes are preferentially excluded from a cavity within the protein as well as the protein surface. Furthermore, the sensitivity of the conformational change to solution osmolality is consistent with a structural model predicted by SDSL. When the Ton box is unfolded by detergents or mutations (rather than by ligand binding), solutes, such as polyethylene glycols and salts, also induce a more structured compacted conformation. These results suggest that conformational changes in this class of outer membrane transporters, which involve modest energy differences and changes in hydration, may be modulated by a range of solutes, including solutes typically used in protein crystallization.

摘要

细菌外膜维生素B12转运蛋白BtuB在底物结合时,其N端能量偶联基序(Ton盒)会发生从有序到无序的显著转变。本文采用定点自旋标记(SDSL)技术表明,当配体与BtuB结合时,一系列溶质可阻止这种构象变化,从而形成更有序的Ton盒结构。对于所研究的每种溶质,数据表明溶质通过渗透机制有效阻断了这种构象转变。已对一系列聚乙二醇研究了这种溶质效应的分子量依赖性,并观察到明显的分子量截止值。该截止值表明溶质优先被排除在蛋白质内部的空腔以及蛋白质表面之外。此外,构象变化对溶液渗透压的敏感性与SDSL预测的结构模型一致。当Ton盒通过去污剂或突变(而非配体结合)展开时,聚乙二醇和盐等溶质也会诱导形成更具结构的紧密构象。这些结果表明,这类外膜转运蛋白的构象变化涉及适度的能量差异和水合作用变化,可能会受到包括蛋白质结晶中常用溶质在内的一系列溶质的调节。

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