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丝状血凝素分泌结构域的晶体结构及其对双伙伴分泌途径的影响。

The crystal structure of filamentous hemagglutinin secretion domain and its implications for the two-partner secretion pathway.

作者信息

Clantin Bernard, Hodak Hélène, Willery Eve, Locht Camille, Jacob-Dubuisson Françoise, Villeret Vincent

机构信息

Institut Fédératif de Recherche du Centre National de la Recherche Scientifique 3, Lille Cedex, France.

出版信息

Proc Natl Acad Sci U S A. 2004 Apr 20;101(16):6194-9. doi: 10.1073/pnas.0400291101. Epub 2004 Apr 12.

Abstract

Filamentous hemagglutinin (FHA), the major 230-kDa adhesin of the whooping cough agent Bordetella pertussis, is one of the most efficiently secreted proteins in Gram-negative bacteria. FHA is secreted by means of the two-partner secretion (TPS) pathway. Several important human, animal, and plant pathogens also secrete adhesins and other virulence factors by using this mode of secretion. A TPS system is composed of two separate proteins, with TpsA the secreted protein and TpsB its associated specific outermembrane transporter. All TPS-secreted proteins contain a distinctive N-proximal module essential for secretion, the TPS domain. We report here the 1.7- A structure of a functionally secreted 30-kDa N-terminal fragment of FHA. It reveals that the TPS domain folds into a beta-helix, with three extrahelical motifs, a beta-hairpin, a four-stranded beta-sheet, and an N-terminal capping, mostly formed by the nonconserved regions of the TPS domain. The structure thus explains why the TPS domain is able to initiate folding of the beta-helical motifs that form the central domain of the adhesin, because it is itself a beta-helical scaffold. It also contains less conserved extrahelical regions most likely involved in specific properties, such as the recognition of the outer-membrane transporter. This structure is representative of the TPS domains found so far in >100 secreted proteins from pathogenic bacteria. It also provides a mechanistic insight into how protein folding may be linked to secretion in the TPS pathway.

摘要

丝状血凝素(FHA)是百日咳杆菌的主要230 kDa黏附素,是革兰氏阴性菌中分泌效率最高的蛋白质之一。FHA通过双组分分泌(TPS)途径分泌。几种重要的人类、动物和植物病原体也通过这种分泌方式分泌黏附素和其他毒力因子。TPS系统由两种独立的蛋白质组成,其中TpsA是分泌蛋白,TpsB是其相关的特异性外膜转运蛋白。所有TPS分泌的蛋白质都含有一个对分泌至关重要的独特N端模块,即TPS结构域。我们在此报告了FHA功能分泌的30 kDa N端片段的1.7 Å结构。结果表明,TPS结构域折叠成一个β螺旋,带有三个螺旋外基序,一个β发夹、一个四链β片层和一个N端帽,主要由TPS结构域的非保守区域形成。因此,该结构解释了TPS结构域为何能够启动形成黏附素中央结构域的β螺旋基序的折叠,因为它本身就是一个β螺旋支架。它还包含最有可能参与特定特性(如外膜转运蛋白识别)的保守性较低的螺旋外区域。这种结构代表了迄今为止在来自致病细菌的100多种分泌蛋白中发现的TPS结构域。它还为蛋白质折叠如何与TPS途径中的分泌相联系提供了机制上的见解。

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