Novel Seizure Phenotype and Sleep Disruptions in Knock-In Mice with Hypersensitive {alpha}4* Nicotinic Receptors

doi:10.1523/JNEUROSCI.3597-05.2005

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The Journal of Neuroscience, December 7, 2005, 25(49):11396-11411; doi:10.1523/JNEUROSCI.3597-05.2005

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Neurobiology of Disease
Novel Seizure Phenotype and Sleep Disruptions in Knock-In Mice with Hypersensitive ${alpha}$ 4^* Nicotinic Receptors
Carlos Fonck,¹ Bruce N. Cohen,¹ Raad Nashmi,¹ Paul Whiteaker,³ Daniel A. Wagenaar,² Nivalda Rodrigues-Pinguet,¹ Purnima Deshpande,¹ Sheri McKinney,¹ Steven Kwoh,¹ Jose Munoz,¹ Cesar Labarca,¹ Allan C. Collins,³ Michael J. Marks,³ and Henry A. Lester¹
Divisions of ¹Biology and ²Physics, Mathematics, and Astronomy, California Institute of Technology, Pasadena, California 91125, and ³Institute for Behavioral Genetics, University of Colorado at Boulder, Boulder, Colorado 80309

A leucine to alanine substitution (L9'A) was introduced in theM2 region of the mouse ${alpha}$ 4 neuronal nicotinic acetylcholine receptor(nAChR) subunit. Expressed in Xenopus oocytes, ${alpha}$ 4(L9'A) ${beta}$ 2 nAChRswere $≥$ 30-fold more sensitive than wild type (WT) to both AChand nicotine. We generated knock-in mice with the L9'A mutationand studied their cellular responses, seizure phenotype, andsleep-wake cycle. Seizure studies on ${alpha}$ 4-mutated animals are relevantto epilepsy research because all known mutations linked to autosomaldominant nocturnal frontal lobe epilepsy (ADNFLE) occur in theM2 region of ${alpha}$ 4or ${beta}$ 2 subunits. Thalamic cultures and synaptosomesfrom L9'A mice were hypersensitive to nicotine-induced ion flux.L9'A mice were $~$ 15-fold more sensitive to seizures elicited bynicotine injection than their WT littermates. Seizures in L9'Amice differed qualitatively from those in WT: L9'A seizuresstarted earlier, were prevented by nicotine pretreatment, lackedEEG spike-wave discharges, and consisted of fast repetitivemovements. Nicotine-induced seizures in L9'A mice were partial,whereas WT seizures were generalized. When L9'A homozygous micereceived a 10 mg/kg nicotine injection, there was temporal andphenomenological separation of mutant and WT-like seizures:an initial seizure $~$ 20 s after injection was clonic and showedno EEG changes. A second seizure began 3-4 min after injection,was tonic-clonic, and had EEG spike-wave activity. No spontaneousseizures were detected in L9'A mice during chronic video/EEGrecordings, but their sleep-wake cycle was altered. Our findingsshow that hypersensitive ${alpha}$ 4^* nicotinic receptors in mice mediatechanges in the sleep-wake cycle and nicotine-induced seizuresresembling ADNFLE.

Key words: epilepsy; ADNFLE; nicotinic receptors; sleep disorders; ${alpha}$ 4 ${beta}$ 2; nicotine

Received Feb 9, 2005; revised October 18, 2005; accepted October 21, 2005.

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