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The Journal of Neuroscience, November 21, 2007, 27(47):13012-13021; doi:10.1523/JNEUROSCI.3605-07.2007

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Neurobiology of Disease
Progressive Dendritic HCN Channelopathy during Epileptogenesis in the Rat Pilocarpine Model of Epilepsy

Sangwook Jung,1 Terrance D. Jones,1 Joaquin N. Lugo, Jr,4 Aaron H. Sheerin,3 John W. Miller,1,2 Raimondo D'Ambrosio,3 Anne E. Anderson,4 and Nicholas P. Poolos1,2

1Department of Neurology, 2Regional Epilepsy Center, and 3Department of Neurological Surgery, University of Washington, Seattle, Washington 98104, and 4Department of Pediatrics, Cain Foundation Laboratories, Baylor College of Medicine, Houston, Texas 77030

Correspondence should be addressed to Nicholas P. Poolos, Department of Neurology and Regional Epilepsy Center, University of Washington, Box 359745, 325 9th Avenue, Seattle, WA 98104. Email: npoolos{at}u.washington.edu

Ion channelopathy plays an important role in human epilepsy with a genetic cause and has been hypothesized to occur in epilepsy after acquired insults to the CNS as well. Acquired alterations of ion channel function occur after induction of status epilepticus (SE) in animal models of epilepsy, but it is unclear how they correlate with the onset of spontaneous seizures. We examined the properties of hyperpolarization-activated cation (HCN) channels in CA1 hippocampal pyramidal neurons in conjunction with video-EEG (VEEG) recordings to monitor the development of spontaneous seizures in the rat pilocarpine model of epilepsy. Our results showed that dendritic HCN channels were significantly downregulated at an acute time point 1 week postpilocarpine, with loss of channel expression and hyperpolarization of voltage-dependent activation. This downregulation progressively increased when epilepsy was established in the chronic period. Surprisingly, VEEG recordings during the acute period showed that a substantial fraction of animals were already experiencing recurrent seizures. Suppression of these seizures with phenobarbital reversed the change in the voltage dependence of Ih, the current produced by HCN channels, but did not affect the loss of HCN channel expression. These results suggest two mechanisms of HCN channel downregulation after SE, one dependent on and one independent of recurrent seizures. This early and progressive downregulation of dendritic HCN channel function increases neuronal excitability and may be associated with both the process of epileptogenesis and maintenance of the epileptic state.

Key words: HCN channel; epilepsy; pilocarpine; EEG; dendrites; Ih

Received Aug. 8, 2007; revised Oct. 11, 2007; accepted Oct. 12, 2007.

Correspondence should be addressed to Nicholas P. Poolos, Department of Neurology and Regional Epilepsy Center, University of Washington, Box 359745, 325 9th Avenue, Seattle, WA 98104. Email: npoolos{at}u.washington.edu




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