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Exiguolysin, a Novel Thermolysin (M4) Peptidase from . | LitMetric

Exiguolysin, a Novel Thermolysin (M4) Peptidase from .

Microorganisms

Biofilm Research Group, School of Pharmacy, Queen's University Belfast, Medical Biology Centre, 97 Lisburn Road, Belfast BT9 7BL, UK.

Published: November 2024

AI Article Synopsis

  • This study investigates exiguolysin, a new thermolysin-like enzyme produced by a marine isolate, showing optimal activity at 37 °C and pH 3, with significant stability at 50 °C.
  • The enzyme, identified as a 32 kDa metalloprotease in the M4 family, requires metal ions for activity and selectively acts on specific substrates, with a notable inhibition of thrombin-induced PAR-1 activation in PC-3 cells.
  • The research highlights the potential industrial applications of exiguolysin and its role as a possible virulence factor, marking the first detailed analysis of such a peptidase in its genus.

Article Abstract

This study details a comprehensive biochemical and structural characterization of exiguolysin, a novel thermolysin-like, caseinolytic peptidase secreted by a marine isolate of strain BW26. Exiguolysin demonstrated optimal proteolytic activity at 37 °C and pH 3, retaining 85% activity at 50 °C, highlighting its potential stability under broad reaction conditions. SDS-PAGE and LC-MS analysis identified the enzyme as a 32 kDa M4-family metalloprotease. Exiguolysin activity was inhibited by 1,10-phenanthroline, confirming its dependence on metal ions for activity. Zymographic analysis and substrate specificity assays revealed selective hydrolysis of matrix metalloproteinase (MMP) substrates but no activity against elastase substrates. Analysis of the predicted gene sequence and structural predictions using AlphaFold identified the presence and position of HEXXH and Glu-Xaa-Xaa-Xaa-Asp motifs, crucial for zinc binding and catalytic activity, characteristic of 'Glu-zincins' and members of the M4 peptidase family. High-throughput screening of a 20 × 20 -alpha mercaptoamide dipeptide inhibitor library against exiguolysin identified SH-CH-CO-Met-Tyr-NH as the most potent inhibitor, with a i of 1.95 μM. Notably, exiguolysin selectively inhibited thrombin-induced PAR-1 activation in PC-3 cells, potentially indicating a potential mechanism of virulence in modulating PAR-1 signalling during infection by disarming PARs. This is the first detailed characterization of a peptidase of the M4 (thermolysin) family in the genus which may have industrial application potential and relevance as a putative virulence factor.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11596557PMC
http://dx.doi.org/10.3390/microorganisms12112311DOI Listing

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