Bacillus cereus extracellular vesicles act as shuttles for biologically active multicomponent enterotoxins

Tanja Buchacher, Astrid Digruber, Markus Kanzler, Giorgia Del Favero, Monika Ehling-Schulz (Corresponding author)

Publications: Contribution to journalArticlePeer Reviewed

Abstract

Background: Extracellular vesicles (EVs) from Gram-positive bacteria have gained considerable importance as a novel transport system of virulence factors in host–pathogen interactions. Bacillus cereus is a Gram-positive human pathogen, causing gastrointestinal toxemia as well as local and systemic infections. The pathogenicity of enteropathogenic B. cereus has been linked to a collection of virulence factors and exotoxins. Nevertheless, the exact mechanism of virulence factor secretion and delivery to target cells is poorly understood. Results: Here, we investigate the production and characterization of enterotoxin-associated EVs from the enteropathogenic B. cereus strain NVH0075-95 by using a proteomics approach and studied their interaction with human host cells in vitro. For the first time, comprehensive analyses of B. cereus EV proteins revealed virulence-associated factors, such as sphingomyelinase, phospholipase C, and the three-component enterotoxin Nhe. The detection of Nhe subunits was confirmed by immunoblotting, showing that the low abundant subunit NheC was exclusively detected in EVs as compared to vesicle-free supernatant. Cholesterol-dependent fusion and predominantly dynamin-mediated endocytosis of B. cereus EVs with the plasma membrane of intestinal epithelial Caco2 cells represent entry routes for delivery of Nhe components to host cells, which was assessed by confocal microscopy and finally led to delayed cytotoxicity. Furthermore, we could show that B. cereus EVs elicit an inflammatory response in human monocytes and contribute to erythrocyte lysis via a cooperative interaction of enterotoxin Nhe and sphingomyelinase. Conclusion: Our results provide insights into the interaction of EVs from B. cereus with human host cells and add a new layer of complexity to our understanding of multicomponent enterotoxin assembly, offering new opportunities to decipher molecular processes involved in disease development. [MediaObject not available: see fulltext.]

Original languageEnglish
Article number112
JournalCell communication and signaling
Volume21
Issue number1
DOIs
Publication statusPublished - 15 May 2023

Austrian Fields of Science 2012

  • 106052 Cell biology
  • 106002 Biochemistry

Keywords

  • 3D-SIM microscopy
  • Bacillus cereus
  • Extracellular vesicles
  • Host–pathogen interaction
  • Multicomponent toxin
  • Non-hemolytic enterotoxin
  • SMase

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