Author:
Salopek-Sondi Branka,Vukelić Bojana,Špoljarić Jasminka,Šimaga Šumski,Vujaklija Dušica,Makarević Janja,Jajčanin Nina,Abramić Marija
Abstract
AbstractHuman dipeptidyl peptidase III (DPP III) is a member of the metallopeptidase family M49 with an implied role in the pain-modulatory system and endogenous defense against oxidative stress. Here, we report the heterologous expression of human DPP III and the site-directed mutagenesis results which demonstrate a functional role for Tyr318at the active site of this enzyme. The substitution of Tyr318to Phe decreasedkcatby two orders of magnitude without altering the binding affinity of substrate, or of a competitive hydroxamate inhibitor designed to interact with S1 and S2 subsites. The results indicate that the conserved tyrosine could be involved in transition state stabilization during the catalytic action of M49 peptidases.
Subject
Clinical Biochemistry,Molecular Biology,Biochemistry
Cited by
22 articles.
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