钩端螺旋体外膜蛋白 LipL41 对于急性钩端螺旋体病并非必需,但需要一种小的伴侣蛋白 lep 来实现稳定表达。
Leptospiral outer membrane protein LipL41 is not essential for acute leptospirosis but requires a small chaperone protein, lep, for stable expression.
机构信息
Department of Microbiology, Monash University, Clayton, Victoria, Australia.
出版信息
Infect Immun. 2013 Aug;81(8):2768-76. doi: 10.1128/IAI.00531-13. Epub 2013 May 20.
Abstract
Leptospirosis is a worldwide zoonosis caused by pathogenic Leptospira spp., but knowledge of leptospiral pathogenesis remains limited. However, the development of mutagenesis systems has allowed the investigation of putative virulence factors and their involvement in leptospirosis. LipL41 is the third most abundant lipoprotein found in the outer membranes of pathogenic leptospires and has been considered a putative virulence factor. LipL41 is encoded on the large chromosome 28 bp upstream of a small open reading frame encoding a hypothetical protein of unknown function. This gene was named lep, for LipL41 expression partner. In this study, lipL41 was found to be cotranscribed with lep. Two transposon mutants were characterized: a lipL41 mutant and a lep mutant. In the lep mutant, LipL41 protein levels were reduced by approximately 90%. Lep was shown through cross-linking and coexpression experiments to bind to LipL41. Lep is proposed to be a molecular chaperone essential for the stable expression of LipL41. The roles of LipL41 and Lep in the pathogenesis of Leptospira interrogans were investigated; surprisingly, neither of these two unique proteins was essential for acute leptospirosis.
摘要
钩端螺旋体病是一种由致病性钩端螺旋体引起的世界性人畜共患病,但对钩端螺旋体病的发病机制仍知之甚少。然而,诱变系统的发展使得对潜在的毒力因子及其在钩端螺旋体病中的作用的研究成为可能。LipL41 是在外膜中发现的第三丰富的脂蛋白,被认为是一种潜在的毒力因子。LipL41 编码在大染色体 28bp 上游的一个小开放阅读框,编码一个未知功能的假设蛋白。该基因被命名为 lep,用于 LipL41 表达伙伴。在这项研究中,发现 lipL41 与 lep 共转录。对两个转座子突变体进行了表征:lipL41 突变体和 lep 突变体。在 lep 突变体中,LipL41 蛋白水平降低了约 90%。通过交联和共表达实验表明 Lep 与 LipL41 结合。提出 Lep 是稳定表达 LipL41 所必需的分子伴侣。研究了 LipL41 和 Lep 在钩端螺旋体病发病机制中的作用;令人惊讶的是,这两种独特的蛋白质在急性钩端螺旋体病中都不是必需的。
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