Selected Contribution: Tryptase-induced PAR-2-mediated [Ca2+]i signaling in
human airway smooth muscle cells.
Berger, Patrick, J. Manuel Tunon-De-Lara, Jean-Pierre Savineau, and Roger Marthan.
Laboratoire de Physiologie Cellulaire Respiratoire, Inserm E9937, Université
Bordeaux 2, 33076 Bordeaux, France
APStracts 8:0256A, 2001.
Tryptase, the major mast cell product, is considered to play an important role in airway
inflammation and hyperresponsiveness. Tryptase produces different, sometimes opposite,
effects on airway responsiveness (bronchoprotection and/or airway contraction). This
study was designed to examine the effect of human lung tryptase and activation of
protease-activated receptor (PAR)-2 by synthetic activated peptide (AP) SLIGKV-NH2
on Ca2+ signaling in human airway smooth muscle (HASM) cells.
Immunocytochemistry revealed that PAR-2 was expressed by HASM cells. Tryptase
(7.5-30 mU/ml) induced a concentration-dependent transient relative rise in cytoplasmic
Ca2+ concentration ([Ca2+]i) that reached 207 ± 32 nM (n = 10) measured by indo 1
spectrofluorometry. The protease inhibitors leupeptin or benzamidine (100 µM) abolished
tryptase-induced [Ca2+]i increase. Activation of PAR-2 by AP (1-100 µM) also induced
a concentration-dependent transient rise in [Ca2+]i, whereas the reverse peptide produced
no effect. There was a homologous desensitization of the [Ca2+]i response on repeated
stimulation with tryptase or AP. U-73122, a specific phospholipase C (PLC) antagonist,
xestospongin, an inositol trisphosphate (IP3) receptor antagonist, or thapsigargin, a
sarcoplamic Ca2+-ATPase inhibitor, abolished tryptase-induced [Ca2+]i response,
whereas Ca2+ removal, in the additional presence of EGTA, had no effect. Calphostin C,
a protein kinase C inhibitor, increased PAR-2 [Ca2+]i response. Our results indicate that
tryptase activates a [Ca2+]i response, which appears PAR-2 mediated in HASM cells.
Signal transduction implicates the intracellular Ca2+ store via PLC activation and thus
via the IP3 pathway. This study provides evidence that tryptase, which is increasingly
recognized as an important mediator in airway inflammation and hyperresponsiveness, is
also a potent direct agonist at the site of airway smooth muscle.
Received 2 March 2001; accepted in final form 27 April 2001
APS Manuscript Number A208-1.
Article publication pending J Appl Physiol
ISSN 1080-4757 Copyright 2001 The American Physiological Society.
Published in APStracts on 18 June 2001