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INFLAMMATION, CYTOKINES, AND TEMPERATURE REGULATION
Department of Biochemistry and Molecular Biology, University of Barcelona, E-08028 Barcelona, Spain
Submitted 20 September 2002 ; accepted in final form 28 March 2003
Acute, high-intensity stress induces necrotic lesions in the heart. We
found that restraint-and-cold (4°C) exposure (RCE) raises plasma lactate
dehydrogenase (LDH), creatine kinase (CK), and transaminase activity in a
time-dependent manner, with a peak value 7 h after stimulus cessation. At 24
h, signs of necrotic lesions were observed in paraffin sections stained with
hematoxylineosin: focal accumulation of mononuclear cells in subendocardial
areas of the left ventricle wall and focal hemorrhage in papillary muscles. In
contrast, intermale fighting (IF) did not increase plasma CK activity,
although LDH and transaminase activities did increase. In IF, no histological
evidence of heart injury was observed. Because IF, but not RCE, increased
plasma epidermal growth factor (EGF) concentration by
1,000-fold, we
hypothesized that EGF receptor (ErbB1) activation may protect the heart
against stress-induced injury. To examine this hypothesis, we injected the
ErbB1 tyrosine kinase inhibitor tyrphostin AG-1478 (25 mg/kg ip) immediately
before mice were exposed to IF. After 3 h, plasma activities of LDH-1 and CK
increased. Plasma enzyme activities were as low in control mice (injected with
vehicle alone) as in nonfighting mice. In the last experiment, we injected EGF
(0.25 mg/kg ip) 20 min before exposing mice to RCE. After 7 h, plasma LDH-1
and CK activities were significantly lower in these animals than in mice
injected with vehicle. The effect required ErbB1 activation, because
simultaneous administration of AG-1478 completely abolished the effect of
exogenous EGF. We conclude that activated ErbB1, by endogenous or exogenous
ligands, may protect the heart against stress-induced injury.
aggressive behavior; mitogen-activated protein kinase; alanine aminotransferase; aspartate aminotransferase; corticosterone
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