Clostridium perfringens type B and D strains produce epsilon-toxin (ETX). Our 2011 study (mBio 2:e00275-11, 2011, https://doi.org/10.1128/mBio.00275-11) reported that the Agr quorum-sensing (QS) system regulates ETX production by type D strain CN3718. However, subsequent studies have brought that conclusion into question. For example, we reported in 2012 (Infect Immun 80:3008-3017, 2012, https://doi.org/10.1128/IAI.00438-12) that the Agr-like QS system is not required for wild-type ETX production levels by two type B strains. Consequently, we reexamined whether the Agr-like QS system regulates ETX production in type D strains by using Targetron insertional mutagenesis to construct new null mutants of two type D strains, CN3718 and CN2068. Western blotting showed that both mutants still produce wild-type ETX levels. However, the newly constructed mutants of both type D strains produced reduced amounts of alpha-toxin, and this effect was reversible by complementation, which confirms loss of functional AgrB production by these mutants since alpha-toxin production is known to be regulated by AgrB. Coupled with the previously published results for type B strains, these new findings indicate the Agr-like QS system is not usually necessary for C. perfringens to produce wild-type ETX levels. Since epsilon-toxin (ETX) is necessary for the virulence of C. perfringens type D and, likely, type B strains, understanding the regulation of ETX production is important. In 2011, we reported that an null mutant of type D strain CN3718 produces less ETX than its wild-type parent. However, when new mutants were constructed in type D strains CN3718 and C2068, ETX production was unaffected. Those newly constructed mutants produced less alpha-toxin, and this phenotype was reversible by complementation, confirming construction of null mutants since alpha-toxin production is regulated by AgrB. Coupled with previous results for type B strains, these new type D results support the conclusion that the Agr QS is not usually necessary for wild-type ETX production levels.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9040827PMC
http://dx.doi.org/10.1128/mbio.00496-22DOI Listing

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