Point mutant mice with hypersensitive α4 nicotinic receptors show dopaminergic deficits and increased anxiety

Cesar Labarca; Johannes Schwarz; Purnima Deshpande; Sigrid Schwarz; Mark W. Nowak; Carlos Fonck; Raad Nashmi; Paulo Kofuji; Hong Dang; Wenmei Shi; Melihat Fidan; Baljit S. Khakh; Zhoufeng Chen; Barbara J. Bowers; Jim Boulter; Jeanne M. Wehner; Henry A. Lester

doi:10.1073/pnas.041582598

Point mutant mice with hypersensitive α4 nicotinic receptors show dopaminergic deficits and increased anxiety

Cesar Labarca, Johannes Schwarz, Purnima Deshpande, Sigrid Schwarz, Mark W. Nowak, Carlos Fonck, Raad Nashmi, Paulo Kofuji, Hong Dang, Wenmei Shi, Melihat Fidan, Baljit S. Khakh, Zhoufeng Chen, Barbara J. Bowers, Jim Boulter, Jeanne M. Wehner, Henry A. Lester

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Abstract

Knock-in mice were generated that harbored a leucine-to-serine mutation in the α4 nicotinic receptor near the gate in the channel pore. Mice with intact expression of this hypersensitive receptor display dominant neonatal lethality. These mice have a severe deficit of dopaminergic neurons in the substantia nigra, possibly because the hypersensitive receptors are continuously activated by normal extracellular choline concentrations. A strain that retains the neo selection cassette in an intron has reduced expression of the hypersensitive receptor and is viable and fertile. The viable mice display increased anxiety, poor motor learning, excessive ambulation that is eliminated by very low levels of nicotine, and a reduction of nigrostriatal dopaminergic function upon aging. These knock-in mice provide useful insights into the pathophysiology of sustained nicotinic receptor activation and may provide a model for Parkinson's disease.

Original language	English
Pages (from-to)	2786-2791
Number of pages	6
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	98
Issue number	5
DOIs	https://doi.org/10.1073/pnas.041582598
State	Published - Feb 27 2001

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Labarca, C., Schwarz, J., Deshpande, P., Schwarz, S., Nowak, M. W., Fonck, C., Nashmi, R., Kofuji, P., Dang, H., Shi, W., Fidan, M., Khakh, B. S., Chen, Z., Bowers, B. J., Boulter, J., Wehner, J. M., & Lester, H. A. (2001). Point mutant mice with hypersensitive α4 nicotinic receptors show dopaminergic deficits and increased anxiety. Proceedings of the National Academy of Sciences of the United States of America, 98(5), 2786-2791. https://doi.org/10.1073/pnas.041582598

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title = "Point mutant mice with hypersensitive α4 nicotinic receptors show dopaminergic deficits and increased anxiety",

abstract = "Knock-in mice were generated that harbored a leucine-to-serine mutation in the α4 nicotinic receptor near the gate in the channel pore. Mice with intact expression of this hypersensitive receptor display dominant neonatal lethality. These mice have a severe deficit of dopaminergic neurons in the substantia nigra, possibly because the hypersensitive receptors are continuously activated by normal extracellular choline concentrations. A strain that retains the neo selection cassette in an intron has reduced expression of the hypersensitive receptor and is viable and fertile. The viable mice display increased anxiety, poor motor learning, excessive ambulation that is eliminated by very low levels of nicotine, and a reduction of nigrostriatal dopaminergic function upon aging. These knock-in mice provide useful insights into the pathophysiology of sustained nicotinic receptor activation and may provide a model for Parkinson's disease.",

author = "Cesar Labarca and Johannes Schwarz and Purnima Deshpande and Sigrid Schwarz and Nowak, {Mark W.} and Carlos Fonck and Raad Nashmi and Paulo Kofuji and Hong Dang and Wenmei Shi and Melihat Fidan and Khakh, {Baljit S.} and Zhoufeng Chen and Bowers, {Barbara J.} and Jim Boulter and Wehner, {Jeanne M.} and Lester, {Henry A.}",

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doi = "10.1073/pnas.041582598",

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Labarca, C, Schwarz, J, Deshpande, P, Schwarz, S, Nowak, MW, Fonck, C, Nashmi, R, Kofuji, P, Dang, H, Shi, W, Fidan, M, Khakh, BS, Chen, Z, Bowers, BJ, Boulter, J, Wehner, JM & Lester, HA 2001, 'Point mutant mice with hypersensitive α4 nicotinic receptors show dopaminergic deficits and increased anxiety', Proceedings of the National Academy of Sciences of the United States of America, vol. 98, no. 5, pp. 2786-2791. https://doi.org/10.1073/pnas.041582598

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T1 - Point mutant mice with hypersensitive α4 nicotinic receptors show dopaminergic deficits and increased anxiety

AU - Labarca, Cesar

AU - Schwarz, Johannes

AU - Deshpande, Purnima

AU - Schwarz, Sigrid

AU - Nowak, Mark W.

AU - Fonck, Carlos

AU - Nashmi, Raad

AU - Kofuji, Paulo

AU - Dang, Hong

AU - Shi, Wenmei

AU - Fidan, Melihat

AU - Khakh, Baljit S.

AU - Chen, Zhoufeng

AU - Bowers, Barbara J.

AU - Boulter, Jim

AU - Wehner, Jeanne M.

AU - Lester, Henry A.

PY - 2001/2/27

Y1 - 2001/2/27

N2 - Knock-in mice were generated that harbored a leucine-to-serine mutation in the α4 nicotinic receptor near the gate in the channel pore. Mice with intact expression of this hypersensitive receptor display dominant neonatal lethality. These mice have a severe deficit of dopaminergic neurons in the substantia nigra, possibly because the hypersensitive receptors are continuously activated by normal extracellular choline concentrations. A strain that retains the neo selection cassette in an intron has reduced expression of the hypersensitive receptor and is viable and fertile. The viable mice display increased anxiety, poor motor learning, excessive ambulation that is eliminated by very low levels of nicotine, and a reduction of nigrostriatal dopaminergic function upon aging. These knock-in mice provide useful insights into the pathophysiology of sustained nicotinic receptor activation and may provide a model for Parkinson's disease.

AB - Knock-in mice were generated that harbored a leucine-to-serine mutation in the α4 nicotinic receptor near the gate in the channel pore. Mice with intact expression of this hypersensitive receptor display dominant neonatal lethality. These mice have a severe deficit of dopaminergic neurons in the substantia nigra, possibly because the hypersensitive receptors are continuously activated by normal extracellular choline concentrations. A strain that retains the neo selection cassette in an intron has reduced expression of the hypersensitive receptor and is viable and fertile. The viable mice display increased anxiety, poor motor learning, excessive ambulation that is eliminated by very low levels of nicotine, and a reduction of nigrostriatal dopaminergic function upon aging. These knock-in mice provide useful insights into the pathophysiology of sustained nicotinic receptor activation and may provide a model for Parkinson's disease.

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Point mutant mice with hypersensitive α4 nicotinic receptors show dopaminergic deficits and increased anxiety

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