Wang Hongxia, Ayala Julio C, Benitez Jorge A, Silva Anisia J
Morehouse School of Medicine Department of Microbiology, Biochemistry and Immunology, Atlanta, Georgia, United States of America; State Key Laboratory for Infectious Disease Prevention and Control, and National Institute for Communicable Disease Control and Prevention, Chinese Center for Disease Control and Prevention, Changping, Beijing, China.
University of Alabama at Birmingham Department of Microbiology, Birmingham, Alabama, United States of America.
PLoS One. 2015 Feb 13;10(2):e0118295. doi: 10.1371/journal.pone.0118295. eCollection 2015.
The histone-like nucleoid structuring protein (H-NS) functions as a transcriptional silencer by binding to AT-rich sequences at bacterial promoters. However, H-NS repression can be counteracted by other transcription factors in response to environmental changes. The identification of potential toxic factors, the expression of which is prevented by H-NS could facilitate the discovery of new regulatory proteins that may contribute to the emergence of new pathogenic variants by anti-silencing. Vibrio cholerae hns mutants of the El Tor biotype exhibit altered virulence, motility and environmental stress response phenotypes compared to wild type. We used an RNA-seq analysis approach to determine the basis of the above hns phenotypes and identify new targets of H-NS transcriptional silencing. H-NS affected the expression of 18% of all predicted genes in a growth phase-dependent manner. Loss of H-NS resulted in diminished expression of numerous genes encoding methyl-accepting chemotaxis proteins as well as chemotaxis toward the attractants glycine and serine. Deletion of hns also induced an endogenous envelope stress response resulting in elevated expression of rpoE encoding the extracytoplamic sigma factor E (σE). The RNA-seq analysis identified new genes directly repressed by H-NS that can affect virulence and biofilm development in the El Tor biotype cholera bacterium. We show that H-NS and the quorum sensing regulator HapR silence the transcription of the vieSAB three-component regulatory system in El Tor biotype V. cholerae. We also demonstrate that H-NS directly represses the transcription of hlyA (hemolysin), rtxCA (the repeat in toxin or RTX), rtxBDE (RTX transport) and the biosynthesis of indole. Of these genes, H-NS occupancy at the hlyA promoter was diminished by overexpression of the transcription activator HlyU. We discuss the role of H-NS transcriptional silencing in phenotypic differences exhibited by V. cholerae biotypes.
类组蛋白核仁结构蛋白(H-NS)通过与细菌启动子处富含AT的序列结合,发挥转录沉默因子的作用。然而,在环境变化时,H-NS的抑制作用可被其他转录因子抵消。鉴定那些表达受H-NS抑制的潜在毒性因子,有助于发现新的调控蛋白,这些蛋白可能通过抗沉默作用促进新的致病变体的出现。与野生型相比,霍乱弧菌El Tor生物型的hns突变体表现出毒力、运动性和环境应激反应表型的改变。我们采用RNA测序分析方法来确定上述hns表型的基础,并鉴定H-NS转录沉默的新靶点。H-NS以生长阶段依赖的方式影响所有预测基因中18%的基因表达。H-NS的缺失导致许多编码甲基接受趋化蛋白的基因表达减少,以及对吸引剂甘氨酸和丝氨酸的趋化性降低。hns的缺失还诱导了内源性包膜应激反应,导致编码胞质外σ因子E(σE)的rpoE表达升高。RNA测序分析鉴定出了受H-NS直接抑制的新基因,这些基因可影响El Tor生物型霍乱菌的毒力和生物膜形成。我们发现,H-NS和群体感应调节因子HapR使El Tor生物型霍乱弧菌中vieSAB三组分调节系统的转录沉默。我们还证明,H-NS直接抑制hlyA(溶血素)、rtxCA(毒素重复序列或RTX)、rtxBDE(RTX转运)的转录以及吲哚的生物合成。在这些基因中,转录激活因子HlyU的过表达减少了H-NS在hlyA启动子处的结合。我们讨论了H-NS转录沉默在霍乱弧菌不同生物型所表现出的表型差异中的作用。
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