Synthesis of Muramyl‐δ‐Lactam in Spore Peptidoglycan of Clostridioides difficile

Author:

Kim Choon1,Lee Mijoon1,Birhanu Biruk T.1,Hesek Dusan1,Chang Mayland1,Mobashery Shahriar1ORCID

Affiliation:

1. Department of Chemistry and Biochemistry University of Notre Dame 354 McCourtney Hall Notre Dame IN 46556 USA

Abstract

AbstractClostridioides difficile is a spore‐forming human pathogen responsible for significant morbidity and mortality. Infections by this pathogen ensue dysbiosis of the intestinal tract, which leads to germination of the spores. The process of spore formation requires a transition for the cell‐wall peptidoglycan of the vegetative C. difficile to that of spores, which entails the formation of muramyl‐δ‐lactam. We describe a set of reactions for three recombinant C. difficile proteins, GerS, CwlD, and PdaA1, with the use of four synthetic peptidoglycan analogs. CwlD and PdaA1 excise the peptidoglycan stem peptide and the acetyl moiety of N‐acetyl muramate, respectively. The reaction of CwlD is accelerated in the presence of GerS. With the use of a suitable substrate, we document that PdaA1 catalyzes a novel zinc‐dependent transamidation/transpeptidation reaction, an unusual reaction that requires excision of the stem peptide as a pre‐requisite.

Publisher

Wiley

Subject

Organic Chemistry,Molecular Biology,Molecular Medicine,Biochemistry

Reference31 articles.

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3. I. Joana L. M. Aristides S. Mónica O. H. Adriano O. Mónica inClostridium difficile(Ed.: E. Shymaa) IntechOpen Rijeka 2017 p. Ch. 2.

4. Clostridioides difficile Biology: Sporulation, Germination, and Corresponding Therapies for C. difficile Infection

5. Peptidoglycan structure and architecture

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