Affiliation:
1. National Research Laboratory of Molecular Microbiology and Toxicology, Department of Agricultural Biotechnology, and Center for Food Safety and Toxicology, Seoul National University, Seoul, South Korea
2. Infection and Immunity Research Laboratory, Metabolic Regulation Research Center, Korea Research Institute of Bioscience and Biotechnology, Daejeon, South Korea
3. Department of Chemistry, Sejong University, Seoul, South Korea
Abstract
ABSTRACT
Pathogenic
Vibrio
species cause diseases in diverse marine animals reared in aquaculture. Since their pathogenesis, persistence, and survival in marine environments are regulated by quorum sensing (QS), QS interference has attracted attention as a means to control these bacteria in aquatic settings. A few QS inhibitors of
Vibrio
species have been reported, but detailed molecular mechanisms are lacking. Here, we identified a novel, potent, and selective
Vibrio
QS inhibitor, named QStatin [1-(5-bromothiophene-2-sulfonyl)-1H-pyrazole], which affects
Vibrio harveyi
LuxR homologues, the well-conserved master transcriptional regulators for QS in
Vibrio
species. Crystallographic and biochemical analyses showed that QStatin binds tightly to a putative ligand-binding pocket in SmcR, the LuxR homologue in
V. vulnificus
, and changes the flexibility of the protein, thereby altering its transcription regulatory activity. Transcriptome analysis revealed that QStatin results in SmcR dysfunction, affecting the expression of SmcR regulon required for virulence, motility/chemotaxis, and biofilm dynamics. Notably, QStatin attenuated representative QS-regulated phenotypes in various
Vibrio
species, including virulence against the brine shrimp (
Artemia franciscana
). Together, these results provide molecular insights into the mechanism of action of an effective, sustainable QS inhibitor that is less susceptible to resistance than other antimicrobial agents and useful in controlling the virulence of
Vibrio
species in aquacultures.
IMPORTANCE
Yields of aquaculture, such as penaeid shrimp hatcheries, are greatly affected by vibriosis, a disease caused by pathogenic
Vibrio
infections. Since bacterial cell-to-cell communication, known as quorum sensing (QS), regulates pathogenesis of
Vibrio
species in marine environments, QS inhibitors have attracted attention as alternatives to conventional antibiotics in aquatic settings. Here, we used target-based high-throughput screening to identify QStatin, a potent and selective inhibitor of
V. harveyi
LuxR homologues, which are well-conserved master QS regulators in
Vibrio
species. Structural and biochemical analyses revealed that QStatin binds tightly to a putative ligand-binding pocket on SmcR, the LuxR homologue in
V. vulnificus
, and affects expression of QS-regulated genes. Remarkably, QStatin attenuated diverse QS-regulated phenotypes in various
Vibrio
species, including pathogenesis against brine shrimp, with no impact on bacterial viability. Taken together, the results suggest that QStatin may be a sustainable antivibriosis agent useful in aquacultures.
Funder
National Research Foundation of Korea
Ministry of Agriculture, Food and Rural Affairs
Korea Research Institute of Bioscience and Biotechnology
Publisher
American Society for Microbiology
Cited by
42 articles.
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