Discovery of potent, selective, orally active, nonpeptide inhibitors of human mast cell chymase

Michael N. Greco; Michael J. Hawkins; Eugene T. Powell; Harold R. Almond; Lawrence De Garavilla; Jeffrey Hall; Lisa K. Minor; Yuanping Wang; Thomas W. Corcoran; Enrico Di Cera; Angelene M. Cantwell; Savvas N. Savvides; Bruce P. Damiano; Bruce E. Maryanoff

Journal Article

Discovery of potent, selective, orally active, nonpeptide inhibitors of human mast cell chymase

Journal of Medicinal Chemistry (2007) 50(8) 1727-1730

DOI: 10.1021/jm0700619

59Citations

30Readers

Get full text

Abstract

A series of β-carboxamido-phosphon(in)ic acids (2) was identified as a new structural motif for obtaining potent inhibitors of human mast cell chymase. For example, 1-naphthyl derivative 5f had an IC50 value of 29 nM and (E)-styryl derivative 6g had an IC50 value of 3.5 nM. An X-ray structure for 5f·chymase revealed key interactions within the enzyme active site. Compound 5f was selective for inhibiting chymase versus eight serine proteases. Compound 6h was orally bioavailable in rats (F = 39%), and orally efficacious in a hamster model of inflammation. © 2007 American Chemical Society.

Cite

CITATION STYLE

APA

Greco, M. N., Hawkins, M. J., Powell, E. T., Almond, H. R., De Garavilla, L., Hall, J., … Maryanoff, B. E. (2007). Discovery of potent, selective, orally active, nonpeptide inhibitors of human mast cell chymase. Journal of Medicinal Chemistry, 50(8), 1727–1730. https://doi.org/10.1021/jm0700619

Discovery of potent, selective, orally active, nonpeptide inhibitors of human mast cell chymase

Abstract

Cite

Register to see more suggestions