Molecular and Neuronal Substrate for the Selective Attenuation of Anxiety

Karin Löw; Florence Crestani; Ruth Keist; Dietmar Benke; Ina Brünig; Jack A. Benson; Jean‐Marc Fritschy; Thomas Rülicke; Horst Bluethmann; Hanns Möhler; Uwe Rudolph

doi:10.1126/science.290.5489.131

Molecular and Neuronal Substrate for the Selective Attenuation of Anxiety

Karin Löw(University of Zurich), Florence Crestani(University of Zurich), Ruth Keist(University of Zurich), Dietmar Benke(University of Zurich), Ina Brünig(University of Zurich), Jack A. Benson(University of Zurich), Jean‐Marc Fritschy(University of Zurich), Thomas Rülicke(University of Zurich), Horst Bluethmann(Roche (Switzerland)), Hanns Möhler(University of Zurich), Uwe Rudolph(University of Zurich)

Science

October 6, 2000

10.1126/science.290.5489.131

Cited by 939

Abstract

Benzodiazepine tranquilizers are used in the treatment of anxiety disorders. To identify the molecular and neuronal target mediating the anxiolytic action of benzodiazepines, we generated and analyzed two mouse lines in which the alpha2 or alpha3 GABAA (gamma-aminobutyric acid type A) receptors, respectively, were rendered insensitive to diazepam by a knock-in point mutation. The anxiolytic action of diazepam was absent in mice with the alpha2(H101R) point mutation but present in mice with the alpha3(H126R) point mutation. These findings indicate that the anxiolytic effect of benzodiazepine drugs is mediated by alpha2 GABAA receptors, which are largely expressed in the limbic system, but not by alpha3 GABAA receptors, which predominate in the reticular activating system.

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