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Discovery of LFF571: an Investigational Agent for Clostridium Difficile Infection

Overview
Journal J Med Chem
Publisher American Chemical Society
Specialty Chemistry
Date 2012 Feb 10
PMID 22315981
Citations 44
Authors
Matthew J LaMarche
Jennifer A Leeds
Adam Amaral
Jason T Brewer
Simon M Bushell
Gejing Deng
Janetta M Dewhurst
Jian Ding
Joanne Dzink-Fox
Gabriel Gamber
Akash Jain
Kwangho Lee
Lac Lee
Troy Lister
David McKenney
Steve Mullin
Colin Osborne
Deborah Palestrant
Michael A Patane
Elin M Rann
Meena Sachdeva
Jian Shao
Stacey Tiamfook
Anna Trzasko
Lewis Whitehead
Aregahegn Yifru
Donghui Yu
Wanlin Yan
Qingming Zhu
Affiliations
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Abstract

Clostridium difficile (C. difficile) is a Gram positive, anaerobic bacterium that infects the lumen of the large intestine and produces toxins. This results in a range of syndromes from mild diarrhea to severe toxic megacolon and death. Alarmingly, the prevalence and severity of C. difficile infection are increasing; thus, associated morbidity and mortality rates are rising. 4-Aminothiazolyl analogues of the antibiotic natural product GE2270 A (1) were designed, synthesized, and optimized for the treatment of C. difficile infection. The medicinal chemistry effort focused on enhancing aqueous solubility relative to that of the natural product and previous development candidates (2, 3) and improving antibacterial activity. Structure-activity relationships, cocrystallographic interactions, pharmacokinetics, and efficacy in animal models of infection were characterized. These studies identified a series of dicarboxylic acid derivatives, which enhanced solubility/efficacy profile by several orders of magnitude compared to previously studied compounds and led to the selection of LFF571 (4) as an investigational new drug for treating C. difficile infection.

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