Different CprABC amino acid sequences affect nisin A susceptibility in Clostridioides difficile isolates

Clinical isolates of Clostridioides difficile sometimes exhibit multidrug resistance and cause diarrhea after antibiotic administration. Metronidazole and vancomycin are often used as therapeutic agents, but resistance to these antibiotics has been found clinically. Therefore, the development of alt...

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Autores principales: Ide, Noriaki, Kawada-Matsuo, Miki, Le, Mi Nguyen-Tra, Hisatsune, Junzo, Nishi, Hiromi, Hara, Toshinori, Kitamura, Norikazu, Kashiyama, Seiya, Yokozaki, Michiya, Kawaguchi, Hiroyuki, Ohge, Hiroki, Sugai, Motoyuki, Komatsuzawa, Hitoshi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9858009/
https://www.ncbi.nlm.nih.gov/pubmed/36662820
http://dx.doi.org/10.1371/journal.pone.0280676
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author Ide, Noriaki
Kawada-Matsuo, Miki
Le, Mi Nguyen-Tra
Hisatsune, Junzo
Nishi, Hiromi
Hara, Toshinori
Kitamura, Norikazu
Kashiyama, Seiya
Yokozaki, Michiya
Kawaguchi, Hiroyuki
Ohge, Hiroki
Sugai, Motoyuki
Komatsuzawa, Hitoshi
author_facet Ide, Noriaki
Kawada-Matsuo, Miki
Le, Mi Nguyen-Tra
Hisatsune, Junzo
Nishi, Hiromi
Hara, Toshinori
Kitamura, Norikazu
Kashiyama, Seiya
Yokozaki, Michiya
Kawaguchi, Hiroyuki
Ohge, Hiroki
Sugai, Motoyuki
Komatsuzawa, Hitoshi
author_sort Ide, Noriaki
collection PubMed
description Clinical isolates of Clostridioides difficile sometimes exhibit multidrug resistance and cause diarrhea after antibiotic administration. Metronidazole and vancomycin are often used as therapeutic agents, but resistance to these antibiotics has been found clinically. Therefore, the development of alternative antimicrobial agents is needed. Nisin A, produced by Lactococcus lactis, has been demonstrated to be effective against C. difficile infection. In this study, we evaluated the susceptibility of 11 C. difficile clinical isolates to nisin A and found that they could be divided into 2 groups: high and low susceptibility. Since CprABC and DltDABC, which are responsible for nisin A efflux and cell surface charge, respectively, have been reported to be related to nisin A susceptibility, we investigated the expression of cprA and dltA among the 11 strains. cprA expression in all strains was induced by nisin A, but dltA expression was not. The expression levels of both genes did not correlate with nisin A susceptibility in these clinical isolates. To evaluate cell surface charge, we performed a cytochrome C binding assay and found no relationship between charge and nisin A susceptibility. Then, we determined the whole genome sequence of each clinical isolate and carried out phylogenetic analysis. The 11 isolates separated into two major clusters, which were consistent with the differences in nisin A susceptibility. Furthermore, we found common differences in several amino acids in the sequences of CprA, CprB, and CprC between the two clusters. Therefore, we speculated that the different amino acid sequences of CprABC might be related to nisin A susceptibility. In addition, C. difficile strains could be divided in the same two groups based on susceptibility to epidermin and mutacin III, which are structurally similar to nisin A. These results suggest that genotypic variations in C. difficile strains confer different susceptibilities to bacteriocins.
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spelling pubmed-98580092023-01-21 Different CprABC amino acid sequences affect nisin A susceptibility in Clostridioides difficile isolates Ide, Noriaki Kawada-Matsuo, Miki Le, Mi Nguyen-Tra Hisatsune, Junzo Nishi, Hiromi Hara, Toshinori Kitamura, Norikazu Kashiyama, Seiya Yokozaki, Michiya Kawaguchi, Hiroyuki Ohge, Hiroki Sugai, Motoyuki Komatsuzawa, Hitoshi PLoS One Research Article Clinical isolates of Clostridioides difficile sometimes exhibit multidrug resistance and cause diarrhea after antibiotic administration. Metronidazole and vancomycin are often used as therapeutic agents, but resistance to these antibiotics has been found clinically. Therefore, the development of alternative antimicrobial agents is needed. Nisin A, produced by Lactococcus lactis, has been demonstrated to be effective against C. difficile infection. In this study, we evaluated the susceptibility of 11 C. difficile clinical isolates to nisin A and found that they could be divided into 2 groups: high and low susceptibility. Since CprABC and DltDABC, which are responsible for nisin A efflux and cell surface charge, respectively, have been reported to be related to nisin A susceptibility, we investigated the expression of cprA and dltA among the 11 strains. cprA expression in all strains was induced by nisin A, but dltA expression was not. The expression levels of both genes did not correlate with nisin A susceptibility in these clinical isolates. To evaluate cell surface charge, we performed a cytochrome C binding assay and found no relationship between charge and nisin A susceptibility. Then, we determined the whole genome sequence of each clinical isolate and carried out phylogenetic analysis. The 11 isolates separated into two major clusters, which were consistent with the differences in nisin A susceptibility. Furthermore, we found common differences in several amino acids in the sequences of CprA, CprB, and CprC between the two clusters. Therefore, we speculated that the different amino acid sequences of CprABC might be related to nisin A susceptibility. In addition, C. difficile strains could be divided in the same two groups based on susceptibility to epidermin and mutacin III, which are structurally similar to nisin A. These results suggest that genotypic variations in C. difficile strains confer different susceptibilities to bacteriocins. Public Library of Science 2023-01-20 /pmc/articles/PMC9858009/ /pubmed/36662820 http://dx.doi.org/10.1371/journal.pone.0280676 Text en © 2023 Ide et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Ide, Noriaki
Kawada-Matsuo, Miki
Le, Mi Nguyen-Tra
Hisatsune, Junzo
Nishi, Hiromi
Hara, Toshinori
Kitamura, Norikazu
Kashiyama, Seiya
Yokozaki, Michiya
Kawaguchi, Hiroyuki
Ohge, Hiroki
Sugai, Motoyuki
Komatsuzawa, Hitoshi
Different CprABC amino acid sequences affect nisin A susceptibility in Clostridioides difficile isolates
title Different CprABC amino acid sequences affect nisin A susceptibility in Clostridioides difficile isolates
title_full Different CprABC amino acid sequences affect nisin A susceptibility in Clostridioides difficile isolates
title_fullStr Different CprABC amino acid sequences affect nisin A susceptibility in Clostridioides difficile isolates
title_full_unstemmed Different CprABC amino acid sequences affect nisin A susceptibility in Clostridioides difficile isolates
title_short Different CprABC amino acid sequences affect nisin A susceptibility in Clostridioides difficile isolates
title_sort different cprabc amino acid sequences affect nisin a susceptibility in clostridioides difficile isolates
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9858009/
https://www.ncbi.nlm.nih.gov/pubmed/36662820
http://dx.doi.org/10.1371/journal.pone.0280676
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