The antivirulent Staphylococcal sRNA SprC regulates CzrB efflux pump to adapt its response to zinc toxicity
- Simon Raynaud1,
- Marc Hallier1,2,
- Stéphane Dréano3,
- Brice Felden1,4,
- Yoann Augagneur1 and
- Hélène Le Pabic1
- 1Inserm, BRM (Bacterial RNAs and Medicine)—UMR_S 1230, Université de Rennes, 35000 Rennes, France
- 2Université de Rennes, QCPS (Quality Control in Protein Synthesis), IGDR UMR CNRS 6290, F-35042 Rennes, France
- 3Université de Rennes, CNRS UMR 6290 IGDR, BIOSIT, Molecular Bases of Tumorigenesis: VHL Disease Team, 35043 Rennes, France
- Corresponding authors: yoann.augagneur{at}univ-rennes.fr, helene.lepabic{at}univ-rennes.fr
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Handling editor: Jörg Vogel
Abstract
Bacterial regulatory RNAs (sRNAs) are important players to control gene expression. In Staphylococcus aureus, SprC is an antivirulent trans-acting sRNA known to base-pair with the major autolysin atl mRNA, preventing its translation. Using MS2-affinity purification coupled with RNA sequencing, we looked for its sRNA-RNA interactome and identified 14 novel mRNA targets. In vitro biochemical investigations revealed that SprC binds two of them, czrB and deoD, and uses a single accessible region to regulate its targets, including Atl translation. Unlike Atl regulation, the characterization of the SprC-czrB interaction pinpointed a destabilization of the czrAB cotranscript, leading to a decrease of the mRNA level that impaired CzrB zinc efflux pump expression. On a physiological standpoint, we showed that SprC expression is detrimental to combat against zinc toxicity. In addition, phagocyctosis assays revealed a significant, but moderate, increase of czrB mRNA levels in a sprC-deleted mutant, indicating a functional link between SprC and czrB upon internalization in macrophages, and suggesting a role in resistance to both oxidative and zinc bursts. Altogether, our data uncover a novel pathway in which SprC is implicated, highlighting the multiple strategies used by S. aureus to balance virulence using an RNA regulator.
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Article is online at http://www.rnajournal.org/cgi/doi/10.1261/rna.080122.124.
- Received June 7, 2024.
- Accepted July 24, 2024.
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