AI Article Synopsis

  • Research suggests that six proteases in a pathogen's operon are linked to its virulence, with SplA, B, D, and E showing unique substrate preferences while SplF's characteristics were previously unclear.
  • The study establishes a method for expressing the SplF protease and investigates its substrate specificity using peptide libraries, highlighting its preference for long aliphatic sidechains and aromatic residues.
  • A high-resolution crystal structure of SplF was created to explain its substrate specificity, revealing that this operon contains a distinct extracellular proteolytic system compared to other known Spl proteases.

Article Abstract

Accumulating evidence suggests that six proteases encoded in the operon of a dangerous human pathogen, , may play a role in virulence. Interestingly, SplA, B, D, and E have complementary substrate specificities while SplF remains to be characterized in this regard. Here, we describe the prerequisites of a heterologous expression system for active SplF protease and characterize the enzyme in terms of substrate specificity and its structural determinants. Substrate specificity of SplF is comprehensively profiled using combinatorial libraries of peptide substrates demonstrating strict preference for long aliphatic sidechains at the P1 subsite and significant selectivity for aromatic residues at P3. The crystal structure of SplF was provided at 1.7 Å resolution to define the structural basis of substrate specificity of SplF. The obtained results were compared and contrasted with the characteristics of other Spl proteases determined to date to conclude that the operon encodes a unique extracellular proteolytic system.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7926377PMC
http://dx.doi.org/10.3390/ijms22042220DOI Listing

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