PLoS ONE (Jan 2011)

Expression and genetic loss of function analysis of the HAT/DESC cluster proteases TMPRSS11A and HAT.

  • Katiuchia Uzzun Sales,
  • John P Hobson,
  • Rebecca Wagenaar-Miller,
  • Roman Szabo,
  • Amber L Rasmussen,
  • Alexandra Bey,
  • Maham F Shah,
  • Alfredo A Molinolo,
  • Thomas H Bugge

DOI
https://doi.org/10.1371/journal.pone.0023261
Journal volume & issue
Vol. 6, no. 8
p. e23261

Abstract

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Genome mining at the turn of the millennium uncovered a new family of type II transmembrane serine proteases (TTSPs) that comprises 17 members in humans and 19 in mice. TTSPs phylogenetically belong to one of four subfamilies: matriptase, hepsin/TMPRSS, corin and HAT/DESC. Whereas a wealth of information now has been gathered as to the physiological functions of members of the hepsin/TMPRSS, matriptase, and corin subfamilies of TTSPs, comparatively little is known about the functions of the HAT/DESC subfamily of proteases. Here we perform a combined expression and functional analysis of this TTSP subfamily. We show that the five human and seven murine HAT/DESC proteases are coordinately expressed, suggesting a level of functional redundancy. We also perform a comprehensive phenotypic analysis of mice deficient in two of the most widely expressed HAT/DESC proteases, TMPRSS11A and HAT, and show that the two proteases are dispensable for development, health, and long-term survival in the absence of external challenges or additional genetic deficits. Our comprehensive expression analysis and generation of TMPRSS11A- and HAT-deficient mutant mouse strains provide a valuable resource for the scientific community for further exploration of the HAT/DESC subfamily proteases in physiological and pathological processes.