Dopamine signaling enriched striatal gene set predicts striatal dopamine synthesis and physiological activity in vivo

Author:

Sportelli LeonardoORCID,Eisenberg Daniel P.ORCID,Passiatore Roberta,D’Ambrosio EnricoORCID,Antonucci Linda A.,Bettina Jasmine S.,Chen Qiang,Goldman Aaron L.,Gregory Michael D.ORCID,Griffiths Kira,Hyde Thomas M.ORCID,Kleinman Joel E.ORCID,Pardiñas Antonio F.ORCID,Parihar MadhurORCID,Popolizio Teresa,Rampino Antonio,Shin Joo HeonORCID,Veronese MattiaORCID,Ulrich William S.,Zink Caroline F.,Bertolino Alessandro,Howes Oliver D.ORCID,Berman Karen F.,Weinberger Daniel R.ORCID,Pergola GiulioORCID

Abstract

AbstractThe polygenic architecture of schizophrenia implicates several molecular pathways involved in synaptic function. However, it is unclear how polygenic risk funnels through these pathways to translate into syndromic illness. Using tensor decomposition, we analyze gene co-expression in the caudate nucleus, hippocampus, and dorsolateral prefrontal cortex of post-mortem brain samples from 358 individuals. We identify a set of genes predominantly expressed in the caudate nucleus and associated with both clinical state and genetic risk for schizophrenia that shows dopaminergic selectivity. A higher polygenic risk score for schizophrenia parsed by this set of genes predicts greater dopamine synthesis in the striatum and greater striatal activation during reward anticipation. These results translate dopamine-linked genetic risk variation into in vivo neurochemical and hemodynamic phenotypes in the striatum that have long been implicated in the pathophysiology of schizophrenia.

Publisher

Springer Science and Business Media LLC

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