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LipL32是钩端螺旋体属和海鞘假交替单胞菌的一种细胞外基质相互作用蛋白。

LipL32 is an extracellular matrix-interacting protein of Leptospira spp. and Pseudoalteromonas tunicata.

作者信息

Hoke David E, Egan Suhelen, Cullen Paul A, Adler Ben

机构信息

Australian Bacterial Pathogenesis Program, Australian Research Council Centre of Excellence in Structural and Functional Microbial Genomics, Department of Microbiology, Monash University, VIC 3800, Australia.

出版信息

Infect Immun. 2008 May;76(5):2063-9. doi: 10.1128/IAI.01643-07. Epub 2008 Feb 19.

Abstract

LipL32 is the major outer membrane protein in pathogenic Leptospira. It is highly conserved throughout pathogenic species and is expressed in vivo during human infection. While these data suggest a role in pathogenesis, a function for LipL32 has not been defined. Outer membrane proteins of gram-negative bacteria are the first line of molecular interaction with the host, and many have been shown to bind host extracellular matrix (ECM). A search for leptospiral ECM-interacting proteins identified the major outer membrane protein, LipL32. To verify this finding, recombinant LipL32 was expressed in Escherichia coli and was found to bind Matrigel ECM and individual components of ECM, including laminin, collagen I, and collagen V. Likewise, an orthologous protein found in the genome of Pseudoalteromonas tunicata strain D2 was expressed and found to be functionally similar and immunologically cross-reactive. Lastly, binding activity was mapped to the C-terminal 72 amino acids. These studies show that LipL32 and an orthologous protein in P. tunicata are immunologically cross-reactive and function as ECM-interacting proteins via a conserved C-terminal region.

摘要

LipL32是致病性钩端螺旋体中的主要外膜蛋白。它在所有致病物种中高度保守,并且在人类感染期间在体内表达。虽然这些数据表明其在发病机制中起作用,但LipL32的功能尚未明确。革兰氏阴性菌的外膜蛋白是与宿主进行分子相互作用的第一道防线,并且许多已被证明可结合宿主细胞外基质(ECM)。对钩端螺旋体ECM相互作用蛋白的搜索鉴定出主要外膜蛋白LipL32。为了验证这一发现,重组LipL32在大肠杆菌中表达,并发现其可结合基质胶ECM以及ECM的各个成分,包括层粘连蛋白、I型胶原蛋白和V型胶原蛋白。同样,在海单胞菌属被膜菌D2菌株基因组中发现的一种直系同源蛋白也被表达,并且发现其功能相似且具有免疫交叉反应性。最后,结合活性定位于C末端的72个氨基酸。这些研究表明,LipL32和海单胞菌属被膜菌中的一种直系同源蛋白具有免疫交叉反应性,并通过保守的C末端区域作为ECM相互作用蛋白发挥作用。

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