Signaling via the prostaglandin E2 receptor EP4 exerts neuronal and vascular protection in a mouse model of cerebral ischemia
Xibin Liang, … , Milton Merchant, Katrin Andreasson
Xibin Liang, … , Milton Merchant, Katrin Andreasson
Published October 3, 2011
Citation Information: J Clin Invest. 2011;121(11):4362-4371. https://doi.org/10.1172/JCI46279.
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Research Article Neuroscience

Signaling via the prostaglandin E2 receptor EP4 exerts neuronal and vascular protection in a mouse model of cerebral ischemia

Abstract

Stroke is the third leading cause of death in the United States. Fewer than 5% of patients benefit from the only intervention approved to treat stroke. Thus, there is an enormous need to identify new therapeutic targets. The role of inducible cyclooxygenase (COX-2) activity in stroke and other neurologic diseases is complex, as both activation and sustained inhibition can engender cerebral injury. Whether COX-2 induces cerebroprotective or injurious effects is probably dependent on which downstream prostaglandin receptors are activated. Here, we investigated the function of the PGE2 receptor EP4 in a mouse model of cerebral ischemia. Systemic administration of a selective EP4 agonist after ischemia reduced infarct volume and ameliorated long-term behavioral deficits. Expression of EP4 was robust in neurons and markedly induced in endothelial cells after ischemia-reperfusion, suggesting that neuronal and/or endothelial EP4 signaling imparts cerebroprotection. Conditional genetic inactivation of neuronal EP4 worsened stroke outcome, consistent with an endogenous protective role of neuronal EP4 signaling in vivo. However, endothelial deletion of EP4 also worsened stroke injury and decreased cerebral reperfusion. Systemic administration of an EP4 agonist increased levels of activated eNOS in cerebral microvessels, an effect that was abolished with conditional deletion of endothelial EP4. Thus, our data support the concept of targeting protective prostaglandin receptors therapeutically after stroke.

Authors

Xibin Liang, Lu Lin, Nathaniel S. Woodling, Qian Wang, Christoph Anacker, Tingting Pan, Milton Merchant, Katrin Andreasson

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Figure 5

Endothelial EP4 regulates CBF during reperfusion.

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Endothelial EP4 regulates CBF during reperfusion. (A) Measurement of rel...
(A) Measurement of relative CBF by LDF revealed a significant decrease in cerebral perfusion in male VECad-Cre-ERT2;EP4lox/lox mice compared with VECad-Cre-ERT2;EP4+/+ mice after 60 minutes of MCAo (effect of genotype, F1,22 = 4.769, P = 0.039; effect of time, F12,22 = 74.73, P < 0.001; effect of interaction, F12,22 = 2.168, P < 0.05). Heterozygous VECad-Cre-ERT2;EP4lox/+ values were intermediate between homozygous and control wild type values, but did not differ significantly from either EP4lox/lox or EP4+/+ genotypes. (B) MAP before, during, and after ischemia (60 minutes MCAo) did not show differences between genotypes. bf, before any surgery; CCA, common carotid artery ligation; ECA, external carotid artery ligation; ICA, internal carotid ligation. MAP units are mm Hg.