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多种蛋白酶的调控、顺序加工是鲍特菌丝状血凝素正确成熟和释放所必需的。

Regulated, sequential processing by multiple proteases is required for proper maturation and release of Bordetella filamentous hemagglutinin.

机构信息

Department of Microbiology and Immunology, School of Medicine, University of North Carolina - Chapel Hill, Chapel Hill, NC, 27599-7290, USA.

出版信息

Mol Microbiol. 2019 Sep;112(3):820-836. doi: 10.1111/mmi.14318. Epub 2019 Jun 19.

DOI:10.1111/mmi.14318
PMID:31152610
Abstract

Filamentous hemagglutinin (FHA) is a critically important virulence factor produced by Bordetella species that cause respiratory infections in humans and other animals. It is also a prototypical member of the widespread two partner secretion (TPS) pathway family of proteins. First synthesized as a ~370 kDa protein called FhaB, its C-terminal ~1,200 amino acid 'prodomain' is removed during translocation to the cell surface via the outer membrane channel FhaC. Here, we identify CtpA as a periplasmic protease that is responsible for the regulated degradation of the prodomain and for creation of an intermediate polypeptide that is cleaved by the autotransporter protease SphB1 to generate FHA. We show that the central prodomain region is required to initiate degradation of the prodomain and that CtpA degrades the prodomain after a third, unidentified protease (P3) first removes the extreme C-terminus of the prodomain. Stepwise proteolysis by P3, CtpA and SphB1 is required for maturation of FhaB, release of FHA into the extracellular milieu, and full function in vivo. These data support a substantially updated model for the mechanism of secretion, maturation and function of this model TPS protein.

摘要

丝状血凝素 (FHA) 是博德特氏菌属产生的一种重要的毒力因子,可引起人类和其他动物的呼吸道感染。它也是广泛存在的双伙伴分泌 (TPS) 途径家族蛋白的典型成员。首先合成的 FHA 是一种约 370 kDa 的蛋白质,称为 FhaB,其 C 端约 1200 个氨基酸的“前导区”在通过外膜通道 FhaC 转运到细胞表面时被去除。在这里,我们鉴定出 CtpA 是一种周质蛋白酶,负责调节前导区的降解,并产生一种中间多肽,该多肽被自转运体蛋白酶 SphB1 切割以生成 FHA。我们表明,中央前导区区域是启动前导区降解所必需的,并且 CtpA 在第三个未鉴定的蛋白酶 (P3) 首先去除前导区的极端 C 末端后降解前导区。P3、CtpA 和 SphB1 的逐步蛋白水解对于 FhaB 的成熟、FHA 释放到细胞外环境以及体内的完全功能都是必需的。这些数据支持对该模型 TPS 蛋白分泌、成熟和功能的机制进行了实质性更新的模型。

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