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测序阐明了嗜肺军团菌感染过程中的转录反应,并鉴定了 70 种新型的小非编码 RNA。

Sequencing illustrates the transcriptional response of Legionella pneumophila during infection and identifies seventy novel small non-coding RNAs.

机构信息

UCD Conway Institute for Biomolecular and Biomedical Research, Dublin, Ireland.

出版信息

PLoS One. 2011 Mar 3;6(3):e17570. doi: 10.1371/journal.pone.0017570.

Abstract

Second generation sequencing has prompted a number of groups to re-interrogate the transcriptomes of several bacterial and archaeal species. One of the central findings has been the identification of complex networks of small non-coding RNAs that play central roles in transcriptional regulation in all growth conditions and for the pathogen's interaction with and survival within host cells. Legionella pneumophila is a gram-negative facultative intracellular human pathogen with a distinct biphasic lifestyle. One of its primary environmental hosts in the free-living amoeba Acanthamoeba castellanii and its infection by L. pneumophila mimics that seen in human macrophages. Here we present analysis of strand specific sequencing of the transcriptional response of L. pneumophila during exponential and post-exponential broth growth and during the replicative and transmissive phase of infection inside A. castellanii. We extend previous microarray based studies as well as uncovering evidence of a complex regulatory architecture underpinned by numerous non-coding RNAs. Over seventy new non-coding RNAs could be identified; many of them appear to be strain specific and in configurations not previously reported. We discover a family of non-coding RNAs preferentially expressed during infection conditions and identify a second copy of 6S RNA in L. pneumophila. We show that the newly discovered putative 6S RNA as well as a number of other non-coding RNAs show evidence for antisense transcription. The nature and extent of the non-coding RNAs and their expression patterns suggests that these may well play central roles in the regulation of Legionella spp. specific traits and offer clues as to how L. pneumophila adapts to its intracellular niche. The expression profiles outlined in the study have been deposited into Genbank's Gene Expression Omnibus (GEO) database under the series accession GSE27232.

摘要

第二代测序技术促使许多研究小组重新研究了几种细菌和古菌的转录组。其中一个中心发现是,鉴定出了复杂的小非编码 RNA 网络,这些 RNA 在所有生长条件下以及病原体与宿主细胞相互作用和在宿主细胞内存活中都发挥着核心作用。嗜肺军团菌是一种革兰氏阴性兼性胞内人类病原体,具有独特的二相生活方式。它的主要环境宿主之一是自由生活的变形虫棘阿米巴原虫,它对棘阿米巴原虫的感染类似于对人类巨噬细胞的感染。在这里,我们对嗜肺军团菌在指数和对数期生长以及在棘阿米巴原虫内复制和传播阶段的转录反应进行了测序分析。我们扩展了以前基于微阵列的研究,并揭示了大量非编码 RNA 支持的复杂调控结构的证据。可以鉴定出 70 多个新的非编码 RNA;其中许多似乎是菌株特异性的,并且具有以前未报道过的结构。我们发现了一组在感染条件下优先表达的非编码 RNA,并在嗜肺军团菌中鉴定出第二个 6S RNA 副本。我们表明,新发现的假定 6S RNA 以及许多其他非编码 RNA 都具有反义转录的证据。非编码 RNA 的性质和程度及其表达模式表明,这些可能在调节军团菌属特定性状方面发挥核心作用,并提供有关嗜肺军团菌如何适应其细胞内生态位的线索。该研究中概述的表达谱已被存入 Genbank 的基因表达综合数据库(GEO),系列注册号为 GSE27232。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/19eb/3048289/ad108180c69a/pone.0017570.g001.jpg

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