Identification of Highly Specific Diversity-Oriented Synthesis-Derived Inhibitors of Clostridium difficile.

ACS Infect Dis

Authors	Jeremy Duvall Leanne Bedard Adel Naylor-Olsen Abigail Manson Joshua Bittker Wenye Sun Mark Fitzgerald Zhenmin He Maurice Lee Jean-Charles Marie Giovanni Muncipinto Diane Rush Deming Xu Huisheng Xu Mingliang Zhang Ashlee Earl Michelle Palmer Michael Foley Joseph Vacca Christina Scherer
Keywords	Animals Female Mice Gene Expression Survival Analysis Species Specificity Anti-Bacterial Agents Mice, Inbred C57BL Bacterial Proteins Drug Design Microbial Sensitivity Tests Structure-Activity Relationship Gram-Negative Bacteria Gram-Positive Bacteria Pyrroles Amino Acid Isomerases Quinolines Phenylurea Compounds Clostridium difficile Enterocolitis, Pseudomembranous Heterocyclic Compounds, 2-Ring
Abstract	In 2013, the Centers for Disease Control highlighted Clostridium difficile as an urgent threat for antibiotic-resistant infections, in part due to the emergence of highly virulent fluoroquinolone-resistant strains. Limited therapeutic options currently exist, many of which result in disease relapse. We sought to identify molecules specifically targeting C. difficile in high-throughput screens of our diversity-oriented synthesis compound collection. We identified two scaffolds with apparently novel mechanisms of action that selectively target C. difficile while having little to no activity against other intestinal anaerobes; preliminary evidence suggests that compounds from one of these scaffolds target the glutamate racemase. In vivo efficacy data suggest that both compound series may provide lead optimization candidates.
Year of Publication	2017
Journal	ACS Infect Dis
Volume	3
Issue	5
Pages	349-359
Date Published	2017 05 12
ISSN	2373-8227
DOI	10.1021/acsinfecdis.6b00206
PubMed ID	28215073
PubMed Central ID	PMC5509442
Links
Grant list	HHSN272200900018C / AI / NIAID NIH HHS / United States U19 AI110818 / AI / NIAID NIH HHS / United States