TY - JOUR
T1 - A serine elastase inhibitor reduces inflammation and fibrosis and preserves cardiac function after experimentally-induced murine myocarditis
AU - Lee, Jong K.
AU - Zaidi, Syed H.E.
AU - Liu, Peter
AU - Dawood, Fayez
AU - Cheah, Alexander Y.L.
AU - Wen, Wen Hu
AU - Saiki, Yuriko
AU - Rabinovitch, Marlene
N1 - Funding Information:
Acknowledgments We thank J. Jowlabar and S. Taylor for secretarial assistance and C. Coulber, S. Ciura, E. Sitarz and K. Aitken for technical assistance. We also thank the staff of the Animal Care Facility at The Toronto Hospital General Division for their support with animal care, and members of the Department of Pathology at The Hospital for Sick Children for preparing the specimens for microscopy. This work was supported by a grants #74026 and T-2373 from the Heart and Stroke
Funding Information:
Foundation of Ontario and from the Medical Research Council of Canada.
PY - 1998/12
Y1 - 1998/12
N2 - In viral myocarditis, inflammation and destruction of cardiac myocytes leads to fibrosis, causing progressive impairment in cardiac function. Here we show the etiologic importance of serine elastase activity in the pathophysiology of acute viral myocarditis and the therapeutic efficacy of an elastase inhibitor. In DBA/2 mice inoculated with the encephalomyocarditis virus, a more than 150% increase in myocardial serine elastase activity is observed. This is suppressed by a selective serine elastase inhibitor, ZD0892, which is biologically effective after oral administration. Mice treated with this compound had little evidence of microvascular constriction and obstruction associated with myocarditis-induced ischemia reperfusion injury, much less inflammation and necrosis, only mild fibrosis and myocardial collagen deposition, and normal ventricular function, compared with the infected nontreated group.
AB - In viral myocarditis, inflammation and destruction of cardiac myocytes leads to fibrosis, causing progressive impairment in cardiac function. Here we show the etiologic importance of serine elastase activity in the pathophysiology of acute viral myocarditis and the therapeutic efficacy of an elastase inhibitor. In DBA/2 mice inoculated with the encephalomyocarditis virus, a more than 150% increase in myocardial serine elastase activity is observed. This is suppressed by a selective serine elastase inhibitor, ZD0892, which is biologically effective after oral administration. Mice treated with this compound had little evidence of microvascular constriction and obstruction associated with myocarditis-induced ischemia reperfusion injury, much less inflammation and necrosis, only mild fibrosis and myocardial collagen deposition, and normal ventricular function, compared with the infected nontreated group.
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U2 - 10.1038/3973
DO - 10.1038/3973
M3 - Article
C2 - 9846575
AN - SCOPUS:0031728050
SN - 1078-8956
VL - 4
SP - 1383
EP - 1391
JO - Nature Medicine
JF - Nature Medicine
IS - 12
ER -