| Literature DB >> 15893930 |
Jon Bondebjerg1, Henrik Fuglsang, Kirsten Rosendal Valeur, Dorte Wissing Kaznelson, Johnny Arnsdorf Hansen, René Orup Pedersen, Berit Olsen Krogh, Bo Skaaning Jensen, Conni Lauritzen, Gitte Petersen, John Pedersen, Lars Naerum.
Abstract
Human dipeptidyl peptidase I (hDPPI, cathepsin C, EC 3.4.14.1) is a novel putative drug target for the treatment of inflammatory diseases. Using 1 as a starting point (IC50>10 microM), we have improved potency by more than 500-fold and successfully identified novel inhibitors of DPPI via screening of a one-bead-two-compounds library of semicarbazide derivatives. Selected compounds were shown to inhibit intracellular DPPI in RBL-2H3 cells. These compounds were further characterized for adverse effects on HepG2 cells (cytotoxicity and viability) and their metabolic stability in rat liver microsomes was estimated. One of the most potent inhibitors, 8 (IC50=31+/-3 nM; Ki=45+/-2 nM, competitive inhibition), is selective for DPPI over other cysteine and serine proteases, has a half-life of 24 min in rat liver microsomes, shows approximately 50% inhibition of intracellular DPPI at 20 microM and is noncytotoxic.Entities:
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Year: 2005 PMID: 15893930 DOI: 10.1016/j.bmc.2005.04.048
Source DB: PubMed Journal: Bioorg Med Chem ISSN: 0968-0896 Impact factor: 3.641