TY - JOUR
T1 - Diverse stage-dependent effects of glucocorticoids in a murine model of viral myocarditis
AU - Nakamura, Hiroshi
AU - Kunitsugu, Ichiro
AU - Fukuda, Keiichi
AU - Matsuzaki, Masunori
AU - Sano, Motoaki
N1 - Funding Information:
This study was supported, in part, by grants from the Idiopathic Cardiomyopathy Research Group of the Ministry of Health and Welfare of Japan .
PY - 2013/3
Y1 - 2013/3
N2 - Background: The effects of glucocorticoids on viral myocarditis are contentious. The aim of the present study was to determine whether there is a " window of opportunity" for glucocorticoid treatment in a mouse model of acute viral myocarditis induced by Coxsackie group B3 virus (CVB3). Methods: A/J (H-2a) mice were randomly assigned to one of four experimental groups: (1) viral infection without dexamethasone (DEX) treatment; (2) treatment with 0.75. mg/kg, i.p., DEX each day for 5 days prior to viral infection; (3) 0.75. mg/kg, i.p., DEX treatment for 5 days immediately after viral infection; and (4) 0.75. mg/kg, i.p., DEX treatment for 5 days starting on day 7 after infection. Results: DEX administration before or immediately after viral infection improved survival and attenuated left ventricular dilatation, systolic dysfunction, fibrosis, and infiltration of immune cells in the post-infectious heart. In contrast, late administration of DEX reduced survival (as determined on day 14), and was associated with sustained increases in cardiac tumor necrosis factor-α and interferon-γ levels. The beneficial effects of early DEX administration on survival were completely abrogated by coadministration of a selective cyclooxygenase (COX)-2 inhibitor (NS-398; 5. mg/kg per day, p.o.). Notably, the virus titer in the post-infectious heart was significantly suppressed by DEX, but coadministration of NS-398 at the time of viral infection abolished the suppressive effects of DEX and, in fact, increased virus titers. Conclusions: Early administration of DEX is beneficial in the treatment of fulminant viral myocarditis, whereas late administration of DEX is harmful. The beneficial effects of DEX on survival were completely abolished by simultaneous administration of a selective COX-2 inhibitor. Hence, we speculate that a direct action of DEX on cardiomyocytes, rather than anti-inflammatory effects of DEX on immune cells, confers resistance to myocardial damage induced by viral infection.
AB - Background: The effects of glucocorticoids on viral myocarditis are contentious. The aim of the present study was to determine whether there is a " window of opportunity" for glucocorticoid treatment in a mouse model of acute viral myocarditis induced by Coxsackie group B3 virus (CVB3). Methods: A/J (H-2a) mice were randomly assigned to one of four experimental groups: (1) viral infection without dexamethasone (DEX) treatment; (2) treatment with 0.75. mg/kg, i.p., DEX each day for 5 days prior to viral infection; (3) 0.75. mg/kg, i.p., DEX treatment for 5 days immediately after viral infection; and (4) 0.75. mg/kg, i.p., DEX treatment for 5 days starting on day 7 after infection. Results: DEX administration before or immediately after viral infection improved survival and attenuated left ventricular dilatation, systolic dysfunction, fibrosis, and infiltration of immune cells in the post-infectious heart. In contrast, late administration of DEX reduced survival (as determined on day 14), and was associated with sustained increases in cardiac tumor necrosis factor-α and interferon-γ levels. The beneficial effects of early DEX administration on survival were completely abrogated by coadministration of a selective cyclooxygenase (COX)-2 inhibitor (NS-398; 5. mg/kg per day, p.o.). Notably, the virus titer in the post-infectious heart was significantly suppressed by DEX, but coadministration of NS-398 at the time of viral infection abolished the suppressive effects of DEX and, in fact, increased virus titers. Conclusions: Early administration of DEX is beneficial in the treatment of fulminant viral myocarditis, whereas late administration of DEX is harmful. The beneficial effects of DEX on survival were completely abolished by simultaneous administration of a selective COX-2 inhibitor. Hence, we speculate that a direct action of DEX on cardiomyocytes, rather than anti-inflammatory effects of DEX on immune cells, confers resistance to myocardial damage induced by viral infection.
KW - Cytokines
KW - Drug therapy
KW - Myocarditis
KW - Prostaglandins
KW - Viruses
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U2 - 10.1016/j.jjcc.2012.11.006
DO - 10.1016/j.jjcc.2012.11.006
M3 - Article
C2 - 23415923
AN - SCOPUS:84875257973
SN - 0914-5087
VL - 61
SP - 237
EP - 242
JO - Journal of Cardiology
JF - Journal of Cardiology
IS - 3
ER -