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High-throughput sequencing reveals suppressors of Vibrio cholerae rpoE mutations: One fewer porin is enough

Nucleic Acids Research, ISSN: 0305-1048, Vol: 37, Issue: 17, Page: 5757-5767
2009
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Analyses of suppressor mutations have been extremely valuable in understanding gene function. However, techniques for mapping suppressor mutations are not available for most bacterial species. Here, we used high-throughput sequencing technology to identify spontaneously arising suppressor mutations that enabled disruption of. rpoE (which encodes σ. ) in. Vibrio cholerae, the agent of cholera. The alternative sigma factor σ. , which is activated by envelope stress, promotes expression of factors that help preserve and/or restore cell envelope integrity. In. Escherichia coli, rpoE is an essential gene that can only be disrupted in the presence of additional suppressor mutations. Among a panel of independent. V. cholerae rpoE mutants, more than 75r% contain suppressor mutations that reduce production of OmpU, V. cholerae's principal outer membrane porin. OmpU appears to be a key determinant of. V. cholerae's requirement for and production of σ. . Such dependence upon a single factor contrasts markedly with regulation of σ. in. E. coli, in which numerous factors contribute to its activation and none is dominant. We also identified a suppressor mutation that differs from all previously described suppressors in that it elevates, rather than reduces, σ. 's activity. Finally, analyses of a panel of. rpoE mutants shed light on the mechanisms by which suppressor mutations may arise in. V. cholerae. © 2009 The Author(s).

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