Another cause of the neuronal cascade of death. Get your researcher involved.
http://www.ncbi.nlm.nih.gov/pubmed/23269317
Abstract
The migration of
polymorphonuclear granulocytes (PMN) into the brain parenchyma and
release of their abundant proteases are considered the main causes of
neuronal cell death and reperfusion injury following ischemia. Yet,
therapies targeting PMN egress have been largely ineffective. To address
this discrepancy we investigated the temporo-spatial localization of
PMNs early after transient ischemia in a murine transient middle
cerebral artery occlusion (tMCAO) model and human stroke specimens.
Using specific markers that distinguish PMN (Ly6G) from
monocytes/macrophages (Ly6C) and that define the cellular and basement
membrane boundaries of the neurovascular unit (NVU), histology and
confocal microscopy revealed that virtually no PMNs entered the
infarcted CNS parenchyma. Regardless of tMCAO duration, PMNs were mainly
restricted to luminal surfaces or perivascular spaces of cerebral
vessels. Vascular PMN accumulation showed no spatial correlation with
increased vessel permeability, enhanced expression of endothelial cell
adhesion molecules, platelet aggregation or release of neutrophil
extracellular traps. Live cell imaging studies confirmed that oxygen and
glucose deprivation followed by reoxygenation fail to induce PMN
migration across a brain endothelial monolayer under flow conditions in
vitro. The absence of PMN infiltration in infarcted brain tissues was
corroborated in 25 human stroke specimens collected at early time points
after infarction. Our observations identify the NVU rather than the
brain parenchyma as the site of PMN action after CNS ischemia and
suggest reappraisal of targets for therapies to reduce reperfusion
injury after stroke.
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