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Published January 2013 | Accepted Version
Journal Article Open

Mice expressing the ADNFLE valine 287 leucine mutation of the Β2 nicotinic acetylcholine receptor subunit display increased sensitivity to acute nicotine administration and altered presynaptic nicotinic receptor function

O'Neill, Heidi C.
Laverty, Duncan C.
Patzlaff, Natalie E.
Cohen, Bruce N.
Fonck, Carlos
McKinney, Sheri
McIntosh, J. Michael
Lindstrom, Jon M.
Lester, Henry A. ORCID icon
Grady, Sharon R.
Marks, Michael J.

Abstract

Several mutations in α4 or β2 nicotinic receptor subunits are linked to autosomal dominant nocturnal frontal lobe epilepsy (ADNFLE). One such missense mutation in the gene encoding the β2 neuronal nicotinic acetylcholine receptor (nAChR) subunit (CHRNB2) is a valine-to-leucine substitution in the second transmembrane domain at position 287 (β2VL). Previous studies indicated that the β2VL mutation in mice alters circadian rhythm consistent with sleep alterations observed in ADNFLE patients (Xu et al., 2011). The current study investigates changes in nicotinic receptor function and expression that may explain the behavioral phenotype of β2VL mice. No differences in β2 mRNA expression were found between wild-type (WT) and heterozygous (HT) or homozygous mutant (MT) mice. However, antibody and ligand binding indicated that the mutation resulted in a reduction in receptor protein. Functional consequences of the β2VL mutation were assessed biochemically using crude synaptosomes. A gene-dose dependent increase in sensitivity to activation by acetylcholine and decrease in maximal nAChR-mediated [^3H]-dopamine release and ^(86)Rb efflux were observed. Maximal nAChR-mediated [^3H]-GABA release in the cortex was also decreased in the MT, but maximal [^3H]-GABA release was retained in the hippocampus. Behaviorally both HT and MT mice demonstrated increased sensitivity to nicotine-induced hypolocomotion and hypothermia. Furthermore, WT mice display only a tonic–clonic seizure (EEG recordable) 3 min after injection of a high dose of nicotine, while MT mice also display a dystonic arousal complex (non-EEG recordable) event 30 s after nicotine injection. Data indicate decreases in maximal response for certain measures are larger than expected given the decrease in receptor expression.

Additional Information

© 2012 Elsevier Inc. Received 25 July 2012. Received in revised form 26 September 2012. Accepted 24 October 2012. Available online 1 November 2012. The authors thank Jian Xuand Steve Heinemannatthe SalkInstitute, La Jolla, CA for initially supplying the β2VL mutant mice. This work was supported by grants R01 DA003194, R01 DA012242, P30 DA015663 and U19 DA019375 to MJM; R01 GM 103801 and R01 GM 48677 to JMM; R01 NS 11323 to JML

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Identifiers Funding Dates
Created:
August 22, 2023
Modified:
October 23, 2023