Novel Macrocyclic NLRP3 Inhibitors

化学 组合化学 立体化学
作者
Stefanie Mesch,Jonathan Shannon,D.O. Miller,Angus M. MacLeod,Léa Bouché,Heather J. Johnston,Kim L. Matthews,Axel Paehler,Stuart Best,Wolfgang Guba,Thomas A. Alanine,Reena Halai,Lorna Charge,Susan C. Garside,Stephen Thom,Celia A. Incerti‐Pradillos,Christopher McPherson,Jokin Carrillo,Stephen A. St-Gallay,Philippe Rigo
出处
期刊:Journal of Medicinal Chemistry [American Chemical Society]
被引量:1
标识
DOI:10.1021/acs.jmedchem.4c01376
摘要

Aberrant activation of NLRP3 due to persistent tissue damage, misfolded proteins or crystal deposits has been linked to multiple chronic inflammatory disorders such as cryopyrin-associated periodic syndrome (CAPS), neurodegenerative diseases, gouty arthritis, and numerous others. Hence, there has been an increasing interest in NLRP3 inhibitors as therapeutics. A first generation of NLRP3 inhibitors bearing a sulfonylurea core such as MCC950 (developed by Pfizer) were discovered by phenotypic screening, however their mode of action was only elucidated later. Based on MCC950, second-generation inhibitors were developed, aiming to overcome some liabilities such as moderate potency and drug induced liver injury. During the optimization of these (second-generation) inhibitors, conformational studies led to the design of novel macrocycles. Here we report the discovery and optimization of this class of NLRP3 inhibitors.
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