
Bioorganic and Medicinal Chemistry Letters p. 1069 - 1074 (1999)
Update date:2022-07-29
Topics:
Augeri, David J.
Janowick, Dave
Kalvin, Douglas
Sullivan, Gerry
Larsen, John
Dickman, Daniel
Ding, Hong
Cohen, Jerry
Lee, Jang
Warner, Robert
Kovar, Peter
Cherian, Sajeev
Saeed, Badr
Zhang, Haichao
Tahir, Steve
Ng, Shi-Chung
Sham, Hing
Rosenberg, Saul H.
Potent and orally bioavailable nonthiol-containing inhibitors of protein farnesyltransferase are described. Oral bioavailability was achieved by replacement of the pyridyl ether moiety of 1 with a 2-substituted furan ether to give 4. Potency was regained with 2,5-disubstituted furan ethers while maintaining the bioavailability inherent in 4. p-Chlorophenylfuran ether 24 is 0.7 nM in vitro (FTase) and is 32% bioavailable in the mouse, 30% bioavailable in rats, and 21% bioavailable in dogs.
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