Porphyromonas gingivalis Cysteine Proteinase Inhibition by κ-Casein Peptides

Author:

Toh Elena C. Y.1,Dashper Stuart G.1,Huq N. Laila1,Attard Troy J.1,O'Brien-Simpson Neil M.1,Chen Yu-Yen1,Cross Keith J.1,Stanton David P.1,Paolini Rita A.1,Reynolds Eric C.1

Affiliation:

1. Oral Health Cooperative Research Centre, Melbourne Dental School, and The Bio21 Institute of Molecular Science and Biotechnology, The University of Melbourne, 720 Swanston Street, Victoria 3010, Australia

Abstract

ABSTRACT Porphyromonas gingivalis is a major pathogen associated with chronic periodontitis, an inflammatory disease of the supporting tissues of the teeth. The Arg-specific (RgpA/B) and Lys-specific (Kgp) cysteine proteinases of P. gingivalis are major virulence factors for the bacterium. In this study κ-casein(109-137) was identified in a chymosin digest of casein as an inhibiting peptide of the P. gingivalis proteinases. The peptide was synthesized and shown to inhibit proteolytic activity associated with P. gingivalis whole cells, purified RgpA-Kgp proteinase-adhesin complexes, and purified RgpB proteinase. The peptide κ-casein(109-137) exhibited synergism with Zn(II) against both Arg- and Lys-specific proteinases. The active region for inhibition was identified as κ-casein(117-137) using synthetic peptides. Kinetic studies revealed that κ-casein(109-137) inhibits in an uncompetitive manner. A molecular model based on the uncompetitive action and its synergistic ability with Zn(II) was developed to explain the mechanism of inhibition. Preincubation of P. gingivalis with κ-casein(109-137) significantly reduced lesion development in a murine model of infection.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology

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