Mice lacking the inducible nitric oxide synthase gene exhibited a 28% reduction in infarct volume and significantly improved neurological deficits 96 hours after focal cerebral ischemia.
Does a null mutation of the iNOS gene reduce ischemic brain damage and neurological deficits in mice following middle cerebral artery occlusion?
iNOS gene knockout reduces delayed ischemic brain damage and neurological deficits, suggesting iNOS inhibition as a potential therapeutic strategy for secondary progression of ischemic brain injury.
p-value: p=<0.01
Inducible nitric oxide synthase (iNOS), an enzyme that produces toxic amounts of nitric oxide, is expressed in a number of brain pathologies, including cerebral ischemia. We used mice with a null mutation of the iNOS gene to study the role of iNOS in ischemic brain damage. Focal cerebral ischemia was produced by occlusion of the middle cerebral artery (MCA). In wild-type mice, iNOS mRNA expression in the post-ischemic brain begun between 24 and 48 hr peaked at 96 hr and subsided 7 d after MCA occlusion. iNOS mRNA induction was associated with expression of iNOS protein and enzymatic activity. In contrast, mice lacking the iNOS gene did not express iNOS message or protein after MCA occlusion. The infarct and the motor deficits produced by MCA occlusion were smaller in iNOS knockouts than in wild-type mice (p < 0.05). Such reduction in ischemic damage and neurological deficits was observed 96 hr after ischemia but not at 24 hr, when iNOS is not yet expressed in wild-type mice. The decreased susceptibility to cerebral ischemia in iNOS knockouts could not be attributed to differences in the degree of ischemia or vascular reactivity between wild-type and knockout mice. These findings indicate that iNOS expression is one of the factors contributing to the expansion of the brain damage that occurs in the post-ischemic period. iNOS inhibition may provide a novel therapeutic strategy targeted specifically at the secondary progression of ischemic brain injury.
Iadecola et al. (Mon,) conducted a other in Focal cerebral ischemia. iNOS gene knockout vs. Wild-type mice was evaluated on Infarct volume 96 hours after middle cerebral artery occlusion (p=<0.01). Mice lacking the inducible nitric oxide synthase gene exhibited a 28% reduction in infarct volume and significantly improved neurological deficits 96 hours after focal cerebral ischemia.