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A Model System for Studying the Transcriptomic and Physiological Changes Associated with Mammalian Host-Adaptation by Leptospira interrogans Serovar Copenhageni

机译:研究与钩端螺旋体Serovar Copenhageni的哺乳动物宿主适应相关的转录组和生理变化的模型系统。

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摘要

Leptospirosis, an emerging zoonotic disease with worldwide distribution, is caused by spirochetes belonging to the genus Leptospira. More than 500,000 cases of severe leptospirosis are reported annually, with >10% of these being fatal. Leptospires can survive for weeks in suitably moist conditions before encountering a new host. Reservoir hosts, typically rodents, exhibit little to no signs of disease but shed large numbers of organisms in their urine. Transmission occurs when mucosal surfaces or abraded skin come into contact with infected urine or urine-contaminated water or soil. In humans, leptospires can cause a variety of clinical manifestations, ranging from asymptomatic or mild fever to severe icteric (Weil's) disease and pulmonary haemorrhage. Currently, little is known about how Leptospira persist within a reservoir host. Prior in vitro studies have suggested that leptospires alter their transcriptomic and proteomic profiles in response to environmental signals encountered during mammalian infection. However, no study has examined gene expression by leptospires within a mammalian host-adapted state. To obtain a more faithful representation of how leptospires respond to host-derived signals, we used RNA-Seq to compare the transcriptome of L. interrogans cultivated within dialysis membrane chambers (DMCs) implanted into the peritoneal cavities of rats with that of organisms grown in vitro. In addition to determining the relative expression levels of “core” housekeeping genes under both growth conditions, we identified 166 genes that are differentially-expressed by L. interrogans in vivo. Our analyses highlight physiological aspects of host adaptation by leptospires relating to heme uptake and utilization. We also identified 11 novel non-coding transcripts that are candidate small regulatory RNAs. The DMC model provides a facile system for studying the transcriptional and antigenic changes associated with mammalian host-adaption, selection of targets for mutagenesis, and the identification of previously unrecognized virulence determinants.
机译:钩端螺旋体病是一种新兴的人畜共患病,分布在世界各地,是由钩端螺旋体属的螺旋体引起的。每年报告超过500,000例严重钩端螺旋体病病例,其中10%以上是致命的。钩端螺旋体可以在适当的潮湿条件下存活数周,然后再遇到新的寄主。水库寄主,通常是啮齿动物,几乎没有或没有疾病迹象,但尿液中有大量生物体脱落。当粘膜表面或磨损的皮肤与受感染的尿液或尿液污染的水或土壤接触时,就会发生传播。在人类中,钩端螺旋体会导致多种临床表现,从无症状或轻度发烧到严重的黄疸(Weil's)病和肺出血。目前,关于钩端螺旋体如何在水库宿主中持续存在的了解很少。先前的体外研究表明,钩端螺旋体响应哺乳动物感染期间遇到的环境信号而改变其转录组和蛋白质组学特征。然而,尚无研究检查钩端螺旋体在哺乳动物宿主适应状态下的基因表达。为了更真实地描述钩端螺旋体如何响应宿主来源的信号,我们使用RNA-Seq比较了植入大鼠腹膜腔内的透析膜腔(DMC)中培养的问号乳杆菌的转录组,以及其生长的生物体。体外。除了确定两种生长条件下“核心”持家基因的相对表达水平外,我们还鉴定了166个在体内被问号李斯特菌差异表达的基因。我们的分析突出了钩端螺旋体与血红素摄取和利用有关的宿主适应的生理方面。我们还确定了11个新颖的非编码转录本,它们是候选的小调控RNA。 DMC模型为研究与哺乳动物宿主适应相关的转录和抗原变化,诱变靶标的选择以及以前无法识别的毒力决定因素的鉴定提供了一个简便的系统。

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