Similar Neurons, Opposite Adaptations: Psychostimulant Experience Differentially Alters Firing Properties in Accumbens Core versus Shell

doi:10.1523/JNEUROSCI.3028-09.2009

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The Journal of Neuroscience, September 30, 2009, 29(39):12275-12283; doi:10.1523/JNEUROSCI.3028-09.2009

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Behavioral/Systems/Cognitive
Similar Neurons, Opposite Adaptations: Psychostimulant Experience Differentially Alters Firing Properties in Accumbens Core versus Shell
Saïd Kourrich¹^,2^,3 and Mark J. Thomas¹^,2^,3
Departments of ¹Neuroscience and ²Psychology and ³Institute of Human Genetics, University of Minnesota, Minneapolis, Minnesota 55455
Correspondence should be addressed to Dr. Mark J. Thomas, University of Minnesota, 6-145 Jackson Hall, 321 Church Street SE, Minneapolis, MN 55455. Email: tmhomas{at}umn.edu
The principal components of neuronal excitability include synapticand intrinsic membrane parameters. While recent studies indicatethat cocaine exposure can induce widespread changes in synapticfunction in the neural circuits for reward, intrinsic firingproperties have received much less attention. Using whole-cellrecording in ex vivo brain slices from cocaine-treated mice,we studied the intrinsic firing characteristics of medium-spinyprojection neurons of the nucleus accumbens—a key nodein the circuit that controls reward-directed behavior. Our datademonstrate that repeated in vivo cocaine (5 x 15 mg/kg, i.p.,once daily, 5 d) induces opposite changes in neurons of thetwo main subdivisions of the accumbens, the shell and the core.While shell neurons exhibit an initial depression in firingcapacity (1–3 d abstinence) that persists for at least2 weeks, core neurons exhibit increased firing capacity duringearly abstinence (1–3 d) that declines to basal levelswithin 2 weeks. Shared adaptations between addictive drugs maymediate core processes of addiction. We find that amphetamineexposure (5 x 5 mg/kg, i.p., once daily, 5 d) that induced asimilar degree of locomotor sensitization as cocaine also inducedan indistinguishable pattern of NAc intrinsic plasticity. Finally,we provided evidence that opposite regulation of A-type potassiumcurrent is an important factor in this bidirectional intrinsicplasticity for both cocaine and amphetamine. We propose thata persistent disparity in core/shell excitability might be animportant mediator of the changes in reward circuit activitythat drive drug-seeking behavior in animal models of addiction.

Received June 25, 2009; revised Aug. 21, 2009; accepted Aug. 25, 2009.

Correspondence should be addressed to Dr. Mark J. Thomas, University of Minnesota, 6-145 Jackson Hall, 321 Church Street SE, Minneapolis, MN 55455. Email: tmhomas{at}umn.edu