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      Circadian rhythms: Of owls, larks and alarm clocks

      Nature
      Springer Science and Business Media LLC

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          Mania-like behavior induced by disruption of CLOCK.

          Circadian rhythms and the genes that make up the molecular clock have long been implicated in bipolar disorder. Genetic evidence in bipolar patients suggests that the central transcriptional activator of molecular rhythms, CLOCK, may be particularly important. However, the exact role of this gene in the development of this disorder remains unclear. Here we show that mice carrying a mutation in the Clock gene display an overall behavioral profile that is strikingly similar to human mania, including hyperactivity, decreased sleep, lowered depression-like behavior, lower anxiety, and an increase in the reward value for cocaine, sucrose, and medial forebrain bundle stimulation. Chronic administration of the mood stabilizer lithium returns many of these behavioral responses to wild-type levels. In addition, the Clock mutant mice have an increase in dopaminergic activity in the ventral tegmental area, and their behavioral abnormalities are rescued by expressing a functional CLOCK protein via viral-mediated gene transfer specifically in the ventral tegmental area. These findings establish the Clock mutant mice as a previously unrecognized model of human mania and reveal an important role for CLOCK in the dopaminergic system in regulating behavior and mood.
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            An hPer2 Phosphorylation Site Mutation in Familial Advanced Sleep Phase Syndrome

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              Stability, Precision, and Near-24-Hour Period of the Human Circadian Pacemaker

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                Author and article information

                Journal
                Nature
                Nature
                Springer Science and Business Media LLC
                0028-0836
                1476-4687
                March 2009
                March 11 2009
                March 2009
                : 458
                : 7235
                : 142-144
                Article
                10.1038/458142a
                19279605
                c2ae06fa-31cb-44bb-9c83-e2c8edc92bc7
                © 2009

                http://www.springer.com/tdm

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