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丝状血凝素的分泌信号,一种典型的双伙伴分泌底物。

Secretion signal of the filamentous haemagglutinin, a model two-partner secretion substrate.

作者信息

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

机构信息

INSERM U629, 1 rue Calmette, F-59019 Lille Cedex, France.

出版信息

Mol Microbiol. 2006 Jul;61(2):368-82. doi: 10.1111/j.1365-2958.2006.05242.x. Epub 2006 Jun 12.

DOI:10.1111/j.1365-2958.2006.05242.x
PMID:16771844
Abstract

The sorting of proteins to their proper subcellular compartment requires specific addressing signals that mediate interactions with ad hoc transport machineries. In Gram-negative bacteria, the widespread two-partner secretion (TPS) pathway is dedicated to the secretion of large, mostly virulence-related proteins. The secreted TpsA proteins carry a characteristic 250-residue-long N-terminal 'TPS domain' essential for secretion, while their TpsB transporters are pore-forming proteins that specifically recognize their respective TpsA partners and mediate their translocation across the outer membrane. However, the nature of the secretion signal has not been elucidated yet. The whooping cough agent Bordetella pertussis secretes its major adhesin filamentous haemagglutinin (FHA) via the TpsB transporter FhaC. In this work, we show specific interactions between an N-terminal fragment of FHA containing the TPS domain and FhaC by using two different techniques, an overlay assay and a pull-down of the complex. FhaC recognizes only non-native conformations of the TPS domain, corroborating the model that in vivo, periplasmic FHA is not yet folded. By generating single amino acid substitutions, we have identified interaction determinants forming the secretion signal. They are found unexpectedly far into the TPS domain and include both conserved and variable residues, which most likely explains the specificity of the TpsA-TpsB interaction. The N-terminal domain of FhaC is involved in the FHA-FhaC interaction, in agreement with its proposed function and periplasmic localization.

摘要

将蛋白质分选到其合适的亚细胞区室需要特定的寻址信号,这些信号介导与特定运输机制的相互作用。在革兰氏阴性细菌中,广泛存在的双伙伴分泌(TPS)途径专门用于分泌大型的、大多与毒力相关的蛋白质。分泌的TpsA蛋白带有一个对分泌至关重要的特征性250个残基长的N端“TPS结构域”,而它们的TpsB转运蛋白是形成孔道的蛋白质,能特异性识别各自的TpsA伙伴并介导它们跨外膜的转运。然而,分泌信号的本质尚未阐明。百日咳病原体百日咳博德特氏菌通过TpsB转运蛋白FhaC分泌其主要黏附素丝状血凝素(FHA)。在这项研究中,我们通过两种不同技术,即覆盖分析和复合物下拉实验,展示了含有TPS结构域的FHA N端片段与FhaC之间的特异性相互作用。FhaC仅识别TPS结构域的非天然构象,这证实了体内周质FHA尚未折叠的模型。通过产生单氨基酸替换,我们确定了构成分泌信号的相互作用决定因素。它们意外地位于TPS结构域的深处,包括保守和可变残基,这很可能解释了TpsA - TpsB相互作用的特异性。FhaC的N端结构域参与FHA - FhaC相互作用,与其提出的功能和周质定位一致。

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