Complexin 1 knockout mice exhibit marked deficits in social behaviours but appear to be cognitively normal

doi:10.1093/hmg/ddm181

Human Molecular Genetics Advance Access published online on July 24, 2007
Human Molecular Genetics, doi:10.1093/hmg/ddm181

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Complexin 1 knockout mice exhibit marked deficits in social behaviours but appear to be cognitively normal

Cheney J. G. Drew¹, Rachel J. Kyd¹ and A. Jennifer Morton¹^,*

¹ Department of Pharmacology, University Of Cambridge, Tennis Court Road, Cambridge, CB2 1PD, United Kingdom

^* Author for Correspondence Dr. A. J. Morton, Department Of Pharmacology, University Of Cambridge, Tennis Court Road, Cambridge, CB2 1PD, United Kingdom. Telephone: +44 1223 334057, Fax: +44 1223 334100 E-mail: ajm41{at}cam.ac.uk

Received April 26, 2007; Revised July 6, 2007; Accepted July 6, 2007

Complexins are presynaptic proteins that modulate neurotransmitterrelease. Abnormal expression of complexin 1 (Cplx1) is seenin several neurodegenerative and psychiatric disorders in whichdisturbed social behaviour is commonplace. These include Parkinsons'sdisease, Alzheimer's disease, schizophrenia, major depressiveillness and bipolar disorder. We wondered if changes in Cplx1expression contribute to the psychiatric components of the diseasesin which Cplx1 is dysregulated. To investigate this we examinedthe cognitive and social behaviours of complexin 1 knockoutmice (Cplx1^-/-) mice. Cplx1^-/- mice have a profound ataxia thatlimits their ability to perform co-ordinated motor tasks. Nevertheless,when we taught juvenile Cplx1^-/- mice to swim they showed noevidence of cognitive impairment in the two-choice swim tank.By contrast, although olfactory discrimination in Cplx1^-/- micewas normal, Cplx1^-/- mice failed in the social transmissionof food preference task, another cognitive paradigm. This wasdue to abnormal social interactions rather than cognitive impairments,increased anxiety or neophobia. When we tested social behaviourdirectly, Cplx1^-/- mice failed to demonstrate a preference forsocial novelty. Further, in a resident-intruder paradigm maleCplx1^-/- mice failed to show the aggressive behaviour that istypical of wild-type males towards an intruder mouse. Togetherour results show that in addition to the severe motor and exploratorydeficits already described, Cplx1^-/- mice have pronounced deficitsin social behaviours. Abnormalities in complexin 1 levels inthe brain may therefore contribute to the psycho-social aspectsof human diseases in which this protein is dysregulated.

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