Axon initial segment dysfunction in a mouse model of genetic epilepsy with febrile seizures plus
Verena C. Wimmer, … , Heinz Beck, Steven Petrou
Verena C. Wimmer, … , Heinz Beck, Steven Petrou
Published July 12, 2010
Citation Information: J Clin Invest. 2010;120(8):2661-2671. https://doi.org/10.1172/JCI42219.
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Research Article Neuroscience

Axon initial segment dysfunction in a mouse model of genetic epilepsy with febrile seizures plus

Abstract

Febrile seizures are a common childhood seizure disorder and a defining feature of genetic epilepsy with febrile seizures plus (GEFS+), a syndrome frequently associated with Na+ channel mutations. Here, we describe the creation of a knockin mouse heterozygous for the C121W mutation of the β1 Na+ channel accessory subunit seen in patients with GEFS+. Heterozygous mice with increased core temperature displayed behavioral arrest and were more susceptible to thermal challenge than wild-type mice. Wild-type β1 was most concentrated in the membrane of axon initial segments (AIS) of pyramidal neurons, while the β1(C121W) mutant subunit was excluded from AIS membranes. In addition, AIS function, an indicator of neuronal excitability, was substantially enhanced in hippocampal pyramidal neurons of the heterozygous mouse specifically at higher temperatures. Computational modeling predicted that this enhanced excitability was caused by hyperpolarized voltage activation of AIS Na+ channels. This heat-sensitive increased neuronal excitability presumably contributed to the heightened thermal seizure susceptibility and epileptiform discharges seen in patients and mice with β1(C121W) subunits. We therefore conclude that Na+ channel β1 subunits modulate AIS excitability and that epilepsy can arise if this modulation is impaired.

Authors

Verena C. Wimmer, Christopher A. Reid, Suzanne Mitchell, Kay L. Richards, Byron B. Scaf, Bryan T. Leaw, Elisa L. Hill, Michel Royeck, Marie-Therese Horstmann, Brett A. Cromer, Philip J. Davies, Ruwei Xu, Holger Lerche, Samuel F. Berkovic, Heinz Beck, Steven Petrou

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Figure 7

Modeling suggests that wild-type β1 subunits reduce the voltage-dependent opening of AIS Na+ channels.

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Modeling suggests that wild-type β1 subunits reduce the voltage-dependen...
(A) Comparison of first APs elicited by current injection into a neuron model an AIS/soma Na+ conductance ratio of 15. APs are aligned at threshold as defined for the physiological data. Shifts in AIS Na+ channel V1/2 from 0 to –15 mV are color-coded green to black. V1/2 of the soma was held constant. Time bar: 1 ms; Vm bar: 50 mV. (B) Second derivative of the voltage traces shown in A, illustrating AIS-specific changes in AP initiation (cf. Figure 6, D and E). Traces are aligned to the second peak in the second derivative to more clearly demonstrate changes in peak acceleration and axo-somatic delay. (CE) Influence of changes in V1/2 of AIS relative Na+ current density (AIS/soma Na+ conductance ratios between 2 and 15) on Vm and acceleration reflecting AIS AP initiation (C), somatic AP generation (D), and axo-somatic delay, calculated as the temporal separation of the 2 peaks in the second derivative (E).