Binding of the RNA Chaperone Hfq on Target mRNAs Promotes the Small RNA RyhB-Induced Degradation in Escherichia coli

David Lalaouna, Karine Prévost, Seongjin Park, Thierry Chénard, Marie-Pier Bouchard, Marie-Pier Caron, Carin K. Vanderpool, Jingyi Fei, Eric Massé

Research output: Contribution to journalArticlepeer-review

Abstract

Many RNA-RNA interactions depend on molecular chaperones to form and remain stable in living cells. A prime example is the RNA chaperone Hfq, which is a critical effector involved in regulatory interactions between small RNAs (sRNAs) and cognate target mRNAs in Enterobacteriaceae. While there is a great deal of in vitro biochemical evidence supporting the model that Hfq enhances rates or affinities of sRNA:mRNA interactions, there is little corroborating in vivo evidence. Here we used in vivo tools including reporter genes, co-purification assays, and super-resolution microscopy to analyze the role of Hfq in RyhB-mediated regulation, and we found that Hfq is often unnecessary for efficient RyhB:mRNA complex formation in vivo. Remarkably, our data suggest that a primary function of Hfq is to promote RyhB-induced cleavage of mRNA targets by RNase E. Moreover, our work indicates that Hfq plays a more limited role in dictating regulatory outcomes following sRNAs RybB and DsrA complex formation with specific target mRNAs. Our investigation helps evaluate the roles played by Hfq in some RNA-mediated regulation.
Original languageEnglish (US)
Article number64
JournalNon-coding RNA
Volume7
Issue number4
DOIs
StatePublished - Dec 2021

Keywords

  • small RNA (sRNA)
  • Hfg
  • RNase E
  • sRNA-induced degradation
  • super-resolution imaging
  • RNA chaperone
  • Hfg binding site
  • Hfq
  • Small RNA (sRNA)
  • Hfq binding site
  • SRNA-induced degradation
  • Super-resolution imaging

ASJC Scopus subject areas

  • Genetics
  • Molecular Biology
  • Biochemistry

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