A schizophrenia-related sensorimotor deficit links α3-containing GABAA receptors to a dopamine hyperfunction

  1. B. K. Yee*,
  2. R. Keist,
  3. L. von Boehmer,
  4. R. Studer,
  5. D. Benke,
  6. N. Hagenbuch*,
  7. Y. Dong,
  8. R. C. Malenka,
  9. J.-M. Fritschy,
  10. H. Bluethmann§,
  11. J. Feldon*,
  12. H. Möhler,,, and
  13. U. Rudolph
  1. Institute of Pharmacology and Toxicology, University of Zürich, Winterthurerstrasse 190, CH-8057 Zürich, Switzerland; *Laboratory of Behavioral Neurobiology and Department of Chemistry and Applied Biosciences and Collegium Helveticum, Swiss Federal Institute of Technology Zürich, Schorenstrasse 16, CH-8603 Schwerzenbach, Switzerland; Nancy Pritzker Laboratory, Department of Psychiatry and Behavioral Sciences, Stanford University School of Medicine, MSLS P104, Stanford, CA 94305-5485; and §Roche Center for Medical Genomics, CH-4070 Basel, Switzerland

  1. Communicated by Eugene Roberts, Beckman Research Institute of the City of Hope, Duarte, CA, October 6, 2005 (received for review September 5, 2005)

Abstract

Overactivity of the dopaminergic system in the brain is considered to be a contributing factor to the development and symptomatology of schizophrenia. Therefore, the GABAergic control of dopamine functions was assessed by disrupting the gene encoding the α3 subunit of the GABAA receptor. α3 knockout (α3KO) mice exhibited neither an obvious developmental defect nor apparent morphological brain abnormalities, and there was no evidence for compensatory up-regulation of other major GABAA-receptor subunits. Anxiety-related behavior in the elevated-plus-maze test was undisturbed, and the anxiolytic-like effect of diazepam, which is mediated by α2-containing GABAA receptors, was preserved. As a result of the loss of α3 GABAA receptors, the GABA-induced whole-cell current recorded from midbrain dopamine neurons was significantly reduced. Spontaneous locomotor activity was slightly elevated in α3KO mice. Most notably, prepulse inhibition of the acoustic startle reflex was markedly attenuated in the α3KO mice, pointing to a deficit in sensorimotor information processing. This deficit was completely normalized by treatment with the antipsychotic D2-receptor antagonist haloperidol. The amphetamine-induced hyperlocomotion was not altered in α3KO mice compared with WT mice. These results suggest that the absence of α3-subunit-containing GABAA receptors induces a hyperdopaminergic phenotype, including a severe deficit in sensorimotor gating, a common feature among psychiatric conditions, including schizophrenia. Hence, agonists acting at α3-containing GABAA receptors may constitute an avenue for an effective treatment of sensorimotor-gating deficits in various psychiatric conditions.

Footnotes

  • To whom correspondence should be addressed. E-mail: mohler{at}pharma.unizh.ch.

  • Author contributions: B.K.Y., H.M., and U.R. designed research; B.K.Y., R.K., L.v.B., R.S., D.B., N.H., Y.D., J.-M.F., H.B., and U.R. performed research; B.K.Y., R.K., L.v.B., R.S., D.B., N.H., Y.D., R.C.M., J.-M.F., J.F., H.M., and U.R. analyzed data; and B.K.Y., R.C.M., J.-M.F., J.F., H.M., and U.R. wrote the paper.

  • Conflict of interest statement: No conflicts declared.

  • Abbreviations: α3KO, α3 knockout; PPI, prepulse inhibition.

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  1. Published online before print November 11, 2005, doi: 10.1073/pnas.0508752102 PNAS November 22, 2005 vol. 102 no. 47 17154-17159
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