Design and Optimization of Sulfone Pyrrolidine Sulfonamide Antagonists of Transient Receptor Potential Vanilloid-4 with in Vivo Activity in a Pulmonary Edema Model

Authors :: Brian G. Lawhorn
Brian Budzik
Karl F. Erhard
Huijie Li
Carla A. Donatelli
Kalindi Vaidya
Melissa H. Costell
Joseph E. Pero
John J. McAtee
Carl Brooks
Lorraine M. Posobiec
Larry J. Jolivette
Dennis A. Holt
Theresa J. Roethke
Stephen H. Eisennagel
Michael C. Fischer
Matthews Jay M
Arthur Shu
Brent W. Mccleland
Lamont Roscoe Terrell
Sender Matthew Robert
Katrina Rivera
David J. Behm
Israil Pendrak
Ralph A. Rivero
Xiaoping Xu
Edward J. Brnardic
Peng Li
Source :: Journal of medicinal chemistry. 61(24)
Publication Year :: 2018
Abstract: Pulmonary edema is a common ailment of heart failure patients and has remained an unmet medical need due to dose-limiting side effects associated with current treatments. Preclinical studies in rodents have suggested that inhibition of transient receptor potential vanilloid-4 (TRPV4) cation channels may offer an alternative—and potentially superior—therapy. Efforts directed toward small-molecule antagonists of the TRPV4 receptor have led to the discovery of a novel sulfone pyrrolidine sulfonamide chemotype exemplified by lead compound 6. Design elements toward the optimization of TRPV4 activity, selectivity, and pharmacokinetic properties are described. Activity of leading exemplars 19 and 27 in an in vivo model suggestive of therapeutic potential is highlighted herein.

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