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新型小RNA的鉴定及伯氏考克斯氏体6S RNA的特性分析。

Identification of novel small RNAs and characterization of the 6S RNA of Coxiella burnetii.

作者信息

Warrier Indu, Hicks Linda D, Battisti James M, Raghavan Rahul, Minnick Michael F

机构信息

Division of Biological Sciences, University of Montana, Missoula, Montana, United States of America.

Department of Biology, Portland State University, Portland, Oregon, United States of America.

出版信息

PLoS One. 2014 Jun 20;9(6):e100147. doi: 10.1371/journal.pone.0100147. eCollection 2014.

Abstract

Coxiella burnetii, an obligate intracellular bacterial pathogen that causes Q fever, undergoes a biphasic developmental cycle that alternates between a metabolically-active large cell variant (LCV) and a dormant small cell variant (SCV). As such, the bacterium undoubtedly employs complex modes of regulating its lifecycle, metabolism and pathogenesis. Small RNAs (sRNAs) have been shown to play important regulatory roles in controlling metabolism and virulence in several pathogenic bacteria. We hypothesize that sRNAs are involved in regulating growth and development of C. burnetii and its infection of host cells. To address the hypothesis and identify potential sRNAs, we subjected total RNA isolated from Coxiella cultured axenically and in Vero host cells to deep-sequencing. Using this approach, we identified fifteen novel C. burnetii sRNAs (CbSRs). Fourteen CbSRs were validated by Northern blotting. Most CbSRs showed differential expression, with increased levels in LCVs. Eight CbSRs were upregulated (≥2-fold) during intracellular growth as compared to growth in axenic medium. Along with the fifteen sRNAs, we also identified three sRNAs that have been previously described from other bacteria, including RNase P RNA, tmRNA and 6S RNA. The 6S regulatory sRNA of C. burnetii was found to accumulate over log phase-growth with a maximum level attained in the SCV stage. The 6S RNA-encoding gene (ssrS) was mapped to the 5' UTR of ygfA; a highly conserved linkage in eubacteria. The predicted secondary structure of the 6S RNA possesses three highly conserved domains found in 6S RNAs of other eubacteria. We also demonstrate that Coxiella's 6S RNA interacts with RNA polymerase (RNAP) in a specific manner. Finally, transcript levels of 6S RNA were found to be at much higher levels when Coxiella was grown in host cells relative to axenic culture, indicating a potential role in regulating the bacterium's intracellular stress response by interacting with RNAP during transcription.

摘要

伯纳特柯克斯体是一种导致Q热的专性细胞内细菌病原体,经历双相发育周期,在代谢活跃的大细胞变体(LCV)和休眠的小细胞变体(SCV)之间交替。因此,这种细菌无疑采用复杂的模式来调节其生命周期、代谢和致病性。小RNA(sRNA)已被证明在控制几种致病细菌的代谢和毒力方面发挥重要的调节作用。我们假设sRNA参与调节伯纳特柯克斯体的生长发育及其对宿主细胞的感染。为了验证这一假设并鉴定潜在的sRNA,我们对从在无细胞环境中培养的以及在Vero宿主细胞中培养的柯克斯体中分离出的总RNA进行了深度测序。使用这种方法,我们鉴定出15种新的伯纳特柯克斯体sRNA(CbSR)。通过Northern印迹法验证了14种CbSR。大多数CbSR表现出差异表达,在LCV中水平升高。与在无细胞培养基中生长相比,8种CbSR在细胞内生长期间上调(≥2倍)。除了这15种sRNA,我们还鉴定出3种先前在其他细菌中描述过的sRNA,包括核糖核酸酶P RNA、转移信使RNA和6S RNA。发现伯纳特柯克斯体的6S调节性sRNA在对数生长期积累,在SCV阶段达到最高水平。6S RNA编码基因(ssrS)被定位到ygfA的5'非翻译区;这是真细菌中高度保守的连锁关系。预测的6S RNA二级结构具有在其他真细菌的6S RNA中发现的三个高度保守的结构域。我们还证明柯克斯体的6S RNA以特定方式与RNA聚合酶(RNAP)相互作用。最后,发现当柯克斯体在宿主细胞中生长时,6S RNA的转录水平相对于无细胞培养要高得多,表明其在转录过程中通过与RNAP相互作用来调节细菌的细胞内应激反应方面具有潜在作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f053/4064990/ba650a0958a3/pone.0100147.g001.jpg

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