Vibrio cholerae virulence is blocked by chitosan oligosaccharide-mediated inhibition of ChsR activity

Vibrio cholerae causes cholera, an important cause of death worldwide. A fuller understanding of how virulence is regulated offers the potential for developing virulence inhibitors, regarded as efficient therapeutic alternatives for cholera treatment. Here we show using competitive infections of wil...

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Veröffentlicht in:Nature microbiology 2024-11, Vol.9 (11), p.2909-2922
Hauptverfasser: Liu, Yutao, Wu, Jialin, Liu, Ruiying, Li, Fan, Xuan, Leyan, Wang, Qian, Li, Dan, Chen, XinTong, Sun, Hao, Li, Xiaoya, Jin, Chen, Huang, Di, Li, Linxing, Tang, Guosheng, Liu, Bin
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Sprache:eng
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Zusammenfassung:Vibrio cholerae causes cholera, an important cause of death worldwide. A fuller understanding of how virulence is regulated offers the potential for developing virulence inhibitors, regarded as efficient therapeutic alternatives for cholera treatment. Here we show using competitive infections of wild-type and mutant bacteria that the regulator of chitosan utilization, ChsR, increases V. cholerae virulence in vivo. Mechanistically, RNA sequencing, chromatin immunoprecipitation with sequencing and molecular biology approaches revealed that ChsR directly upregulated the expression of the virulence regulator, TcpP, which promoted expression of the cholera toxin and the toxin co-regulated pilus, in response to low O 2 levels in the small intestine. We also found that chitosan degradation products inhibit the ChsR– tcpP promoter interaction. Consistently, administration of chitosan oligosaccharide, particularly when delivered via sodium alginate microsphere carriers, reduced V. cholerae intestinal colonization and disease severity in mice by blocking the chsR -mediated pathway. These data reveal the potential of chitosan oligosaccharide as supplemental therapy for cholera treatment and prevention. The chitosan utilization regulator, ChsR, positively regulates Vibrio cholerae virulence factor expression, which can be inhibited therapeutically by chitosan oligosaccharide administration in mice.
ISSN:2058-5276
2058-5276
DOI:10.1038/s41564-024-01823-6