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Mu-opiate receptors measured by positron emission tomography are increased in temporal lobe epilepsy

✍ Scribed by Dr. J. James Frost; Helen S. Mayberg; Robert S. Fisher; Kenneth H. Douglass; Robert F. Dannals; Jonathan M. Links; Alan A. Wilson; Hayden T. Ravert; Arthur E. Rosenbaum; Solomon H. Snyder; Henry N. Wagner Jr.


Publisher
John Wiley and Sons
Year
1988
Tongue
English
Weight
743 KB
Volume
23
Category
Article
ISSN
0364-5134

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✦ Synopsis


Neurochemical studies in animal models of epilepsy have demonstrated the importance of multiple neurotransmitters and their receptors in mediating seizures. The role of opiate receptors and endogenous opioid peptides in seizure mechanisms is well developed and is the basis for measuring opiate receptors in patients with epilepsy. Patients with complex partial seizures due to unilateral temporal seizure foci were studied by positron emission tomography using "C-carfentanil to measure mu-opiate receptors and "F-fluoro-deoxy-D-glucose to measure glucose utilization. Opiate receptor binding is greater in the temporal neocortex on the side of the electrical focus than on the opposite side. Modeling studies indicate that the increase in binding is due to an increase in affinity or the number of unoccupied receptors. No significant asymmetry of "C-carfentanil binding was detected in the amygdala or hippocampus. Glucose utilization correlated inversely with "C-carfentanil binding in the temporal neocortex. Increased opiate receptors in the temporal neocortex may represent a tonic anticonvulsant system that limits the spread of electrical activity from other temporal lobe structures.