Repurposing Synthetic Acetaminophen Derivatives Containing a Benzothiazole Scaffold as an Alternative Therapy for Infectious Diarrhea Caused by Drug-Resistant Shigella Species

Author:

Pone Kamdem Boniface1ORCID,Pinlap Brice Rostan1ORCID,Noumboue Kouamou Bijou-Lafortune1,Youbi Kamche Aubin1ORCID,Kuate Boris Arnaud2,Tsemeugne Joseph2,Ngomo Orleans2,Mkounga Pierre2,Fekam Boyom Fabrice1ORCID

Affiliation:

1. Antimicrobial and Biocontrol Agents Unit (AmBcAU), Laboratory for Phytobiochemistry and Medicinal Plants Studies, Department of Biochemistry, Faculty of Science, University of Yaounde I, Yaounde P.O. Box 812, Cameroon

2. Department of Organic Chemistry, Faculty of Science, University of Yaounde I, Yaounde P.O. Box 812, Cameroon

Abstract

Diarrhea remains one of the leading causes of mortality worldwide, especially among children. Accumulated evidence has shown that Shigella species are the most prevalent bacteria responsible for diarrhea in developing countries. Antimicrobial therapy is necessary for Shigella infections; however, the development of resistance against current drugs justifies the pressing need to search for alternative medications. In this study, we have applied antibacterial phenotypic screening to identify potent anti-Shigella compounds across a broad chemical diversity, including selected acetaminophen derivatives containing a benzothiazole backbone, and their combination with certain antibiotics. As a result, two acetaminophen derivatives containing a benzothiazole backbone (4a and 4b) inhibited the growth of Shigella flexneri with a common MIC value of 12.5 µg/mL. These compounds were established through a time-kill kinetics study to be potentially bactericidal. Meanwhile, the 2-aminobenzothiazoles (1a and 1b) used for the synthesis of compounds 4 (a and b) were found to be poorly active (MIC: 100 µg/mL) against this pathogen. Combination studies of 4a and 4b with the least effective antibiotics (ceftriaxone and cotrimoxazole) demonstrated synergistic anti-Shigella activity with MIC values decreasing from 12.5 to 0.781 μg/ mL. The present study demonstrates that the azobenzothiazole dyes 4 (a and b) can be repurposed as potential anti-Shigella compounds, thus providing potential chemical pharmacophores for the discovery of drugs against infectious diarrhea caused by Shigella and other enteric pathogens, especially in developing countries.

Funder

YaBiNaPA

Seeding Labs’ Instrumental Access

Publisher

MDPI AG

Reference68 articles.

1. Yamada, T. (2009). Bacterial, viral, and toxic causes of diarrhea, gastroenteritis, and anorectal infections. Textbook of Gastroenterology, Blackwell. [5th ed.].

2. The World Health Organization (WHO) (2023, August 30). Diarrheal Disease. Available online: https://www.who.int/health-topics/diarrhoea#tab=tab_3.

3. Wood, J.D., Johnson Leonard, R., Ghishan Fayez, K., Kaunitz Jonathan, D., Merchant Juanita, L., and Said Hamid, M. (2012). Pathophysiology of diarrhea and its clinical implications. Physiology of the Gastronintestinal Tract, Elsevier Inc.. [5th ed.].

4. Evaluation of anti-diarrhoeal property of crude aqueous extract of Ocimum gratissimum L. (Labiatae) in rats;Ezekwesili;Biokemistri,2004

5. Shigellosis;Kotloff;Lancet,2018

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