TY - JOUR
T1 - Expression of a mitogen-inducible cyclooxygenase in brain neurons
T2 - Regulation by synaptic activity and glucocorticoids
AU - Yamagata, Kanato
AU - Andreasson, Katrin I.
AU - Kaufmann, Walter E.
AU - Barnes, Carol A.
AU - Worley, Paul F.
N1 - Funding Information:
We thank Daniel Nathans and Anthony Lanahan for advice and support in the differential cloning project, C. D. Stevenson and C. Rao for technical assistancewith portions of the electrophysiological procedures, and Darla Rodgers for secretarial assistance. This work was supported by grants AG09219, EY08900, EY09374 (P. F. W.), MH00897 (C. A. B.), and HD00992 (K. I. A.), by a grant from the W. M. Keck foundation (P. F.W.), and by the Krieger Mind/Brain Institute. W. E. K. a Merck Clinician-Scientist.
PY - 1993/8
Y1 - 1993/8
N2 - Prostaglandins play important and diverse roles in the CNS. The first step in prostaglandin synthesis involves enzymatic oxidation of arachidonic acid, which is catalyzed by prostaglandin H(PGH) synthase, also referred to as cyclooxygenase. We have cloned an inducible form of this enzyme from rat brain that is nearly identical to a murine, mitogen-inducible cyclooxygenase identified from fibroblasts. Our studies indicate that this gene, here termed COX-2, is expressed throughout the forebrain in discrete populations of neurons and is enriched in the cortex and hippocampus. Neuronal expression is rapidly and transiently induced by seizures or NMDA-dependent synaptic activity. No expression is detected in glia or vascular endothelial cells. Basal expression of COX-2 appears to be regulated by natural synaptic activity in the developing and adult brain. Both basal and induced expression of COX-2 are inhibited by glucocorticoids, consistent with COX-2 regulation in peripheral tissues. Our studies indicate that COX-2 expression may be important in regulating prostaglandin signaling in brain. The marked inducibility in neurons by synaptic stimuli suggests a role in activity-dependent plasticity.
AB - Prostaglandins play important and diverse roles in the CNS. The first step in prostaglandin synthesis involves enzymatic oxidation of arachidonic acid, which is catalyzed by prostaglandin H(PGH) synthase, also referred to as cyclooxygenase. We have cloned an inducible form of this enzyme from rat brain that is nearly identical to a murine, mitogen-inducible cyclooxygenase identified from fibroblasts. Our studies indicate that this gene, here termed COX-2, is expressed throughout the forebrain in discrete populations of neurons and is enriched in the cortex and hippocampus. Neuronal expression is rapidly and transiently induced by seizures or NMDA-dependent synaptic activity. No expression is detected in glia or vascular endothelial cells. Basal expression of COX-2 appears to be regulated by natural synaptic activity in the developing and adult brain. Both basal and induced expression of COX-2 are inhibited by glucocorticoids, consistent with COX-2 regulation in peripheral tissues. Our studies indicate that COX-2 expression may be important in regulating prostaglandin signaling in brain. The marked inducibility in neurons by synaptic stimuli suggests a role in activity-dependent plasticity.
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U2 - 10.1016/0896-6273(93)90192-T
DO - 10.1016/0896-6273(93)90192-T
M3 - Article
C2 - 8352945
AN - SCOPUS:0027290813
SN - 0896-6273
VL - 11
SP - 371
EP - 386
JO - Neuron
JF - Neuron
IS - 2
ER -