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Abstract Infections by Clostridioides difficile , a bacterium that targets the large intestine (colon), impact a large number of people worldwide. Bacterial colonization is mediated by two exotoxins: toxins A and B. Short peptides that can be delivered to the gut and inhibit the biocatalytic activity of these toxins represent a promising therapeutic strategy to prevent and treat C. diff . infection. We describe an approach that combines a Pep tide B inding D esign (PepBD) algorithm, molecular-level simulations, a rapid screening assay to evaluate peptide:toxin binding, a primary human cell-based assay, and surface plasmon resonance (SPR) measurements to develop peptide inhibitors that block Toxin A in colon epithelial cells. One peptide, SA1, is found to block TcdA toxicity in primary-derived human colon (large intestinal) epithelial cells. SA1 binds TcdA with a K D of 56.1 ± 29.8 nM as measured by surface plasmon resonance (SPR).more » « less
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Durmusoglu, Deniz; Catella, Carly M; Purnell, Ethan F; Menegatti, Stefano; Crook, Nathan C (, Current Opinion in Physiology)null (Ed.)
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Chu, Wenning; Prodromou, Raphael; Day, Kevin N.; Schneible, John D.; Bacon, Kaitlyn B.; Bowen, John D.; Kilgore, Ryan E.; Catella, Carly M.; Moore, Brandyn D.; Mabe, Matthew D.; et al (, Journal of Chromatography A)null (Ed.)