The Phage Mu Middle Promoter Pm Contains a Partial UP Element

Ma, Ji; Howe, Michael J. A.

doi:10.1534/g3.114.013607

Cited by 1 publication

(1 citation statement)

References 33 publications

(58 reference statements)

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“…It is known that Mu is a temperate bacteriophage of E. coli K-12 and several other enteric bacteria [15]. There are three phases of transcription during the lytic development of bacteriophage Mu: early, middle, and late [16]. The initiation of the middle transcription from Pm requires the phage-encoded activator, Mor [15], which is a sequence-specific DNA-binding protein that promotes transcription activation via interactions with the C-terminal domains of the α and σ subunits of the bacterial RNA polymerase [17].…”

Section: Introductionmentioning

confidence: 99%

The Response Regulator VC1795 of Vibrio Pathogenicity Island-2 Contributes to Intestinal Colonization by Vibrio cholerae

Yan,

Liu,

Xue

et al. 2023

IJMS

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Vibrio cholerae is an intestinal pathogen that can cause severe diarrheal disease. The disease has afflicted millions of people since the 19th century and has aroused global concern. The Vibrio Pathogenicity Island-2 (VPI-2) is a 57.3 kb region, VC1758–VC1809, which is present in choleragenic V. cholerae. At present, little is known about the function of VC1795 in the VPI-2 of V. cholerae. In this study, the intestinal colonization ability of the ΔVC1795 strain was significantly reduced compared to that of the wild-type strain, and the colonization ability was restored to the wild-type strain after VC1795 gene replacement. This result indicated that the VC1795 gene plays a key role in the intestinal colonization and pathogenicity of V. cholerae. Then, we explored the upstream and downstream regulation mechanisms of the VC1795 gene. Cyclic adenylate receptor protein (CRP) was identified as being located upstream of VC1795 by a DNA pull-down assay and electrophoretic mobility shift assays (EMSAs) and negatively regulating the expression of VC1795. In addition, the results of Chromatin immunoprecipitation followed by sequencing (ChIP-seq), EMSAs, and Quantitative Real-Time Polymerase Chain Reaction (qRT-PCR) indicated that VC1795 directly negatively regulates the expression of its downstream gene, VC1794. Furthermore, by using qRT-PCR, we hypothesized that VC1795 indirectly positively regulates the toxin-coregulated pilus (TCP) cluster to influence the colonization ability of V. cholerae in intestinal tracts. In short, our findings support the key regulatory role of VC1795 in bacterial pathogenesis as well as lay the groundwork for the further determination of the complex regulatory network of VC1795 in bacteria.

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