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原核生物中一类新型的维生素模块化转运蛋白。

A novel class of modular transporters for vitamins in prokaryotes.

作者信息

Rodionov Dmitry A, Hebbeln Peter, Eudes Aymerick, ter Beek Josy, Rodionova Irina A, Erkens Guus B, Slotboom Dirk J, Gelfand Mikhail S, Osterman Andrei L, Hanson Andrew D, Eitinger Thomas

机构信息

Burnham Institute for Medical Research, 10901 North Torrey Pines Road, La Jolla, CA 92037, USA.

出版信息

J Bacteriol. 2009 Jan;191(1):42-51. doi: 10.1128/JB.01208-08. Epub 2008 Oct 17.

Abstract

The specific and tightly controlled transport of numerous nutrients and metabolites across cellular membranes is crucial to all forms of life. However, many of the transporter proteins involved have yet to be identified, including the vitamin transporters in various human pathogens, whose growth depends strictly on vitamin uptake. Comparative analysis of the ever-growing collection of microbial genomes coupled with experimental validation enables the discovery of such transporters. Here, we used this approach to discover an abundant class of vitamin transporters in prokaryotes with an unprecedented architecture. These transporters have energy-coupling modules comprised of a conserved transmembrane protein and two nucleotide binding proteins similar to those of ATP binding cassette (ABC) transporters, but unlike ABC transporters, they use small integral membrane proteins to capture specific substrates. We identified 21 families of these substrate capture proteins, each with a different specificity predicted by genome context analyses. Roughly half of the substrate capture proteins (335 cases) have a dedicated energizing module, but in 459 cases distributed among almost 100 gram-positive bacteria, including numerous human pathogens, different and unrelated substrate capture proteins share the same energy-coupling module. The shared use of energy-coupling modules was experimentally confirmed for folate, thiamine, and riboflavin transporters. We propose the name energy-coupling factor transporters for the new class of membrane transporters.

摘要

众多营养物质和代谢产物跨细胞膜的特异性且严格受控的转运对所有生命形式都至关重要。然而,许多涉及的转运蛋白尚未被鉴定出来,包括各种人类病原体中的维生素转运蛋白,其生长严格依赖于维生素的摄取。对不断增加的微生物基因组集合进行比较分析并结合实验验证,能够发现此类转运蛋白。在此,我们采用这种方法在原核生物中发现了一类具有前所未有的结构的丰富的维生素转运蛋白。这些转运蛋白具有能量偶联模块,该模块由一个保守的跨膜蛋白和两个与ATP结合盒(ABC)转运蛋白相似的核苷酸结合蛋白组成,但与ABC转运蛋白不同的是,它们利用小的整合膜蛋白来捕获特定底物。我们鉴定出了21个此类底物捕获蛋白家族,每个家族通过基因组背景分析预测具有不同的特异性。大约一半的底物捕获蛋白(335例)具有专用的供能模块,但在分布于近100种革兰氏阳性菌(包括众多人类病原体)中的459例中,不同且不相关的底物捕获蛋白共享相同的能量偶联模块。叶酸、硫胺素和核黄素转运蛋白的能量偶联模块的共享使用已通过实验得到证实。我们为这类新的膜转运蛋白提出了“能量偶联因子转运蛋白”这一名称。

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