4.7 Article

An Aniline-Substituted Bile Salt Analog Protects both Mice and Hamsters from Multiple Clostridioides difficile Strains

期刊

出版社

AMER SOC MICROBIOLOGY
DOI: 10.1128/AAC.01435-21

关键词

antibiotic-associated diarrhea; bacterial spores; bile salts; Clostridioides difficile; prophylaxis; spore germination

资金

  1. National Institutes of Health (NIH) [R01-AI109139, GM103440, GR08954]
  2. NASA under Nevada Space grant [NNX15AI02H]
  3. NASA [NNX15AI02H, 803929] Funding Source: Federal RePORTER

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Clostridioides difficile infection (CDI) is the major cause of antibiotic-associated diarrhea. Hypervirulent strains have led to increased CDI rates, and standard treatments are becoming less effective. The bile salt analog CaPA was found to be a better antigerminant than CamSA against different C. difficile strains, and it showed efficacy in preventing CDI in mice and hamsters.
Clostridioides difficile infection (CDI) is the major identifiable cause of antibiotic-associated diarrhea. The emergence of hypervirulent C. difficile strains has led to increases in both hospital- and community-acquired CDI. Furthermore, the rate of CDI relapse from hypervirulent strains can reach up to 25%. Thus, standard treatments are rendered less effective, making new methods of prevention and treatment more critical. Previously, the bile salt analog CamSA (cholic acid substituted with maminosulfonic acid) was shown to inhibit spore germination in vitro and protect mice and hamsters from C. difficile strain 630. Here, we show that CamSA was less active in preventing spore germination by other C. difficile ribotypes, including the hypervirulent strain R20291. The strain-specific in vitro germination activity of CamSA correlated with its ability to prevent CDI in mice. Additional bile salt analogs were screened for in vitro germination inhibition activity against strain R20291, and the most active compounds were tested against other strains. An aniline-substituted bile salt analog, CaPA (cholic acid substituted with phenylamine), was found to be a better antigerminant than CamSA against eight different C. difficile strains. In addition, CaPA was capable of reducing, delaying, or preventing murine CDI signs with all strains tested. CaPA-treated mice showed no obvious toxicity and showed minor effects on their gut microbiome. CaPA's efficacy was further confirmed by its ability to prevent CDI in hamsters infected with strain 630. These data suggest that C. difficile spores respond to germination inhibitors in a strain-dependent manner. However, careful screening can identify antigerminants with broad CDI prophylaxis activity.

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