Impaired Inactivation Gate Stabilization Predicts Increased Persistent Current for an Epilepsy-Associated SCN1A Mutation

doi:10.1523/JNEUROSCI.3378-06.2006

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The Journal of Neuroscience, October 25, 2006, 26(43):10958-10966; doi:10.1523/JNEUROSCI.3378-06.2006

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Neurobiology of Disease
Impaired Inactivation Gate Stabilization Predicts Increased Persistent Current for an Epilepsy-Associated SCN1A Mutation
Kristopher M. Kahlig,¹ Sunita N. Misra,² and Alfred L. George, Jr¹^,2
¹Division of Genetic Medicine, Department of Medicine, and ²Department of Pharmacology, Vanderbilt University, Nashville, Tennessee 37232-0275
Correspondence should be addressed to Dr. Alfred L. George Jr, Division of Genetic Medicine, 529 Light Hall, Vanderbilt University, 2215 Garland Avenue, Nashville, TN 37232-0275. Email: al.george{at}vanderbilt.edu
Mutations in SCN1A (encoding the neuronal voltage-gated sodiumchannel ${alpha}$ ₁ subunit, Na_V1.1, or SCN1A) are associated with geneticepilepsy syndromes including generalized epilepsy with febrileseizures plus (GEFS+) and severe myoclonic epilepsy of infancy.Here, we present the formulation and use of a computationalmodel for SCN1A to elucidate molecular mechanisms underlyingthe increased persistent sodium current exhibited by the GEFS+mutant R1648H. Our model accurately reproduces all experimentallymeasured SCN1A whole-cell biophysical properties including biphasicwhole-cell current decay, channel activation, and entry intoand recovery from fast and slow inactivation. The model predictsthat SCN1A open-state inactivation results from a two-step processthat can be conceptualized as initial gate closure, followedby recruitment of a mechanism ("latch") to stabilize the inactivatedstate. Selective impairment of the second latching step resultsin an increase in whole-cell persistent current similar to thatobserved for the GEFS+ mutant R1648H. These results providea deeper level of understanding of mutant SCN1A dysfunctionin an inherited epilepsy syndrome, which will enable more precisecomputational studies of abnormal neuronal activity in epilepsyand may help guide new targeted therapeutic strategies.

Key words: sodium channel; GEFS+; Markov model; SCN1A; epilepsy; computational neuroscience

Received June 6, 2006; revised Sept. 11, 2006; accepted Sept. 11, 2006.

Correspondence should be addressed to Dr. Alfred L. George Jr, Division of Genetic Medicine, 529 Light Hall, Vanderbilt University, 2215 Garland Avenue, Nashville, TN 37232-0275. Email: al.george{at}vanderbilt.edu

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