PCM1 is necessary for focal ciliary integrity and is a candidate for severe schizophrenia

Author:

Monroe Tanner O.ORCID,Garrett Melanie E.,Kousi Maria,Rodriguiz Ramona M.,Moon Sungjin,Bai Yushi,Brodar Steven C.,Soldano Karen L.,Savage Jeremiah,Hansen Thomas F.,Muzny Donna M.,Gibbs Richard A.,Barak Lawrence,Sullivan Patrick F.,Ashley-Koch Allison E.ORCID,Sawa AkiraORCID,Wetsel William C.ORCID,Werge ThomasORCID,Katsanis NicholasORCID

Abstract

AbstractThe neuronal primary cilium and centriolar satellites have functions in neurogenesis, but little is known about their roles in the postnatal brain. We show that ablation of pericentriolar material 1 in the mouse leads to progressive ciliary, anatomical, psychomotor, and cognitive abnormalities. RNAseq reveals changes in amine- and G-protein coupled receptor pathways. The physiological relevance of this phenotype is supported by decreased available dopamine D2 receptor (D2R) levels and the failure of antipsychotic drugs to rescue adult behavioral defects. Immunoprecipitations show an association with Pcm1 and D2Rs. Finally, we sequence PCM1 in two human cohorts with severe schizophrenia. Systematic modeling of all discovered rare alleles by zebrafish in vivo complementation reveals an enrichment for pathogenic alleles. Our data emphasize a role for the pericentriolar material in the postnatal brain, with progressive degenerative ciliary and behavioral phenotypes; and they support a contributory role for PCM1 in some individuals diagnosed with schizophrenia.

Funder

U.S. Department of Health & Human Services | NIH | Center for Information Technology

U.S. Department of Health & Human Services | National Institutes of Health

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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