Exploring the Inhibitory Potential of the Antiarrhythmic Drug Amiodarone Against Toxins TcdA and TcdB

Overview

Journal Gut Microbes

Specialties Gastroenterology
Microbiology

Date 2023 Sep 26

PMID 37749884

Authors

Judith Schumacher

Astrid Nienhaus

Sebastian Heber

Jauheni Matylitsky

Esteban Chaves-Olarte

Cesar Rodriguez

Holger Barth

Panagiotis Papatheodorou

Affiliations

Soon will be listed here.

Abstract

The intestinal pathogen is the leading cause of antibiotic-associated diarrhea and pseudomembranous colitis in humans. The symptoms of -associated diseases (CDADs) are directly associated with the pathogen's toxins TcdA and TcdB, which enter host cells and inactivate Rho and/or Ras GTPases by glucosylation. Membrane cholesterol is crucial during the intoxication process of TcdA and TcdB, and likely involved during pore formation of both toxins in endosomal membranes, a key step after cellular uptake for the translocation of the glucosyltransferase domain of both toxins from endosomes into the host cell cytosol. The licensed drug amiodarone, a multichannel blocker commonly used in the treatment of cardiac dysrhythmias, is also capable of inhibiting endosomal acidification and, as shown recently, cholesterol biosynthesis. Thus, we were keen to investigate with cultured cells and human intestinal organoids, whether amiodarone preincubation protects from TcdA and/or TcdB intoxication. Amiodarone conferred protection against both toxins independently and in combination as well as against toxin variants from the clinically relevant, epidemic strain NAP1/027. Further mechanistic studies suggested that amiodarone's mode-of-inhibition involves also interference with the translocation pore of both toxins. Our study opens the possibility of repurposing the licensed drug amiodarone as a novel pan-variant antitoxin therapeutic in the context of CDADs.

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