Antagonists of human CCR5 receptor containing 4-(pyrazolyl)piperidine side chains. Part 2: Discovery of potent, selective, and orally bioavailable compounds

Authors :: Salvatore J. Siciliano
Karen Holmes
Jeffrey J. Hale
Dong-Ming Shen
Shrenik K. Shah
Christopher A. Willoughby
Michael D. Miller
Anthony Carella
Lorraine Malkowitz
Julie A. DeMartino
Kathy Lyons
Min Shu
James V. Pivnichny
Emilio A. Emini
William A. Schleif
Gloria Y. Kwei
Martin S. Springer
Gwen Carver
Renee Danzeisen
Sandra L. Gould
Joseph Kessler
Daria J. Hazuda
Sander G. Mills
Christopher L. Lynch
Janet Lineberger
Kevin T. Chapman
Source :: Bioorganicmedicinal chemistry letters. 14(4)
Publication Year :: 2003
Abstract: Modifications of the alkyl acetic acid portion and the phenyl on pyrrolidine in our lead pyrazole compound 1 afforded the isopropyl compound 9. This compound is a potent CCR5 antagonist showing good in vitro antiviral activity against HIV-1, an excellent selectivity profile, and good oral bioavailability in three animal species. During this investigation, a new method for the preparation of alpha-(pyrrolidin-1-yl)-alpha,alpha-dialkyl acetic acid from a pyrrolidine and alpha-bromo-alpha,alpha-dialkyl acetic acid using silver triflate was discovered. This allowed us to prepare compounds such as 24 and 25 for the first time. A novel Pd-mediated N-dealkylation of alpha-(pyrrolidin-1-yl)acetic acid was also uncovered.

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