| Literature DB >> 15781396 |
Julian Levell1, Peter Astles, Paul Eastwood, Jennifer Cairns, Olivier Houille, Suzanne Aldous, Gregory Merriman, Brian Whiteley, James Pribish, Mark Czekaj, Guyan Liang, Sebastien Maignan, Jean-Pierre Guilloteau, Alain Dupuy, Jane Davidson, Trevor Harrison, Andrew Morley, Simon Watson, Garry Fenton, Clive McCarthy, Joseph Romano, Rose Mathew, Darren Engers, Michael Gardyan, Keith Sides, Jennifer Kwong, Joseph Tsay, Sam Rebello, Liduo Shen, Jie Wang, Yongyi Luo, Odessa Giardino, Heng-Keang Lim, Keith Smith, Henry Pauls.
Abstract
Tryptase is a serine protease found almost exclusively in mast cells. It has trypsin-like specificity, favoring cleavage of substrates with an arginine (or lysine) at the P1 position, and has optimal catalytic activity at neutral pH. Current evidence suggests tryptase beta is the most important form released during mast cell activation in allergic diseases. It is shown to have numerous pro-inflammatory cellular activities in vitro, and in animal models tryptase provokes broncho-constriction and induces a cellular inflammatory infiltrate characteristic of human asthma. Screening of in-house inhibitors of factor Xa (a closely related serine protease) identified beta-amidoester benzamidines as potent inhibitors of recombinant human betaII tryptase. X-ray structure driven template modification and exchange of the benzamidine to optimize potency and pharmacokinetic properties gave selective, potent and orally bioavailable 4-(3-aminomethyl phenyl)piperidinyl-1-amides.Entities:
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Year: 2005 PMID: 15781396 DOI: 10.1016/j.bmc.2005.02.014
Source DB: PubMed Journal: Bioorg Med Chem ISSN: 0968-0896 Impact factor: 3.641