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Publication Date:
June 2005
ISSN:
1437-4315
DOI:
10.1515/BC.2004.064

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Biological Chemistry

Editor-in-Chief: Brüne, Bernhard

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Characterisation of a highly specific, endogenous inhibitor of cysteine protease from Staphylococcus epidermidis, a new member of the staphostatin family

G. Dubin / J. Stec-Niemczyk / T. Dylag / J. Silberring / A. Dubin / J. Potempa

Citation Information: Biological Chemistry. Volume 385, Issue 6, Pages 543–546, ISSN (Print) 1431-6730, DOI: 10.1515/BC.2004.064, June 2005

Publication History:
Published Online:
2005-06-01

Abstract

Staphostatins, a novel family of cysteine protease inhibitors with a unique mechanism of action and distinct protein fold has recently been discovered. In this report we describe the properties of Staphylococcus epidermidis staphostatin A (EcpB), a new member of the family. As for other staphostatins, the recombinant S. epidermidis staphostatin A exerted very narrow inhibitory specificity, limited to cysteine protease from the same species. The closely related proteases from S. aureus cleaved the inhibitor at the reactive site peptide bond and inactivated it. The EcpB homologue, S. aureus staphostatin A (ScpB), was also susceptible to proteolytic cleavage at the same site by nontarget cysteine proteases. Conversely, S. aureus staphostatin B (SspC) was resistant to such proteolysis. The difference in the susceptibility of individual inhibitors to proteolytic cleavage at the reactive site suggests subtle variations in the mechanism of interaction with cysteine proteases.

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