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丝氨酸蛋白酶自转运β-结构域保守残基在载体结构域加工和β-桶组装中的重要性。

Importance of conserved residues of the serine protease autotransporter beta-domain in passenger domain processing and beta-barrel assembly.

机构信息

Department of Biological Sciences, California State Polytechnic University, Pomona, CA 91709, USA.

出版信息

Infect Immun. 2010 Aug;78(8):3516-28. doi: 10.1128/IAI.00390-10. Epub 2010 Jun 1.

Abstract

Serine protease autotransporters of the family Enterobacteriaceae (SPATE) comprise a family of virulence proteins secreted by enteric Gram-negative bacteria via the autotransporter secretion pathway. A SPATE polypeptide contains a C-terminal translocator domain that inserts into the bacterial outer membrane as a beta-barrel structure and mediates secretion of the passenger domain to the extracellular environment. In the present study, we examined the role of conserved residues located in the SPATE beta-barrel-forming region in passenger domain secretion. Thirty-nine fully conserved residues in Tsh were mutated by single-residue substitution, and defects in their secretion phenotypes were assessed by cell fractionation and immunochemistry. A total of 22 single mutants exhibited abnormal phenotypes in different cellular compartments. Most mutants affecting secretion are charged residues with side chains pointing into the beta-barrel interior. Seven mutants showed notable abnormalities in processing (constructs with the E1231A, E1249A, and R1374A mutations) and beta-barrel assembly or insertion into the outer membrane (constructs with the G1158Y, F1360A, Y1375A, and F1377A mutations). The phenotypes of the beta-barrel assembly/insertion mutants and the presence of a processed Tsh passenger domain in the periplasm support the possibility that the translocator domain must undergo extensive folding prior to insertion into the outer membrane. Results from double-mutation experiments further demonstrate that F1360 and F1377 affect beta-barrel insertion/assembly at different times. In light of these new data, a more refined model for the mechanism of SPATE secretion is presented.

摘要

肠杆菌科丝氨酸蛋白酶自转运体(SPATE)家族由一组通过自转运体分泌途径分泌的肠道革兰氏阴性细菌的毒力蛋白组成。SPATE 多肽包含一个 C 端转运子结构域,该结构域插入细菌外膜作为β-桶结构,并介导载体结构域分泌到细胞外环境中。在本研究中,我们研究了位于 SPATE β-桶形成区域的保守残基在载体结构域分泌中的作用。Tsh 中的 39 个完全保守残基通过单残基取代发生突变,并通过细胞分级分离和免疫化学评估它们在分泌表型中的缺陷。共有 22 个单突变体在不同的细胞区室中表现出异常表型。大多数影响分泌的突变体是带电荷的残基,其侧链指向β-桶内部。7 个突变体在加工(E1231A、E1249A 和 R1374A 突变的构建体)和β-桶组装或插入外膜(G1158Y、F1360A、Y1375A 和 F1377A 突变的构建体)方面表现出明显异常。β-桶组装/插入突变体的表型以及周质中存在加工的 Tsh 载体结构域支持这样一种可能性,即转运子结构域在插入外膜之前必须经历广泛的折叠。双突变实验的结果进一步表明,F1360 和 F1377 在不同时间影响β-桶插入/组装。鉴于这些新数据,提出了一种更精细的 SPATE 分泌机制模型。

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