Literature DB >> 29739866

Region-Specific Regulation of Presynaptic Dopamine Homeostasis by D2 Autoreceptors Shapes the In Vivo Impact of the Neuropsychiatric Disease-Associated DAT Variant Val559.

Raajaram Gowrishankar1,2, Paul J Gresch2,3, Gwynne L Davis1,2, Rania M Katamish2, Justin R Riele1, Adele M Stewart1,2, Roxanne A Vaughan4, Maureen K Hahn2,3, Randy D Blakely5,2,3.   

Abstract

Disruptions of dopamine (DA) signaling contribute to a broad spectrum of neuropsychiatric disorders, including attention-deficit hyperactivity disorder (ADHD), addiction, bipolar disorder, and schizophrenia. Despite evidence that risk for these disorders derives from heritable variation in DA-linked genes, a better understanding is needed of the molecular and circuit context through which gene variation drives distinct disease traits. Previously, we identified the DA transporter (DAT) variant Val559 in subjects with ADHD and established that the mutation supports anomalous DAT-mediated DA efflux (ADE). Here, we demonstrate that region-specific contributions of D2 autoreceptors (D2AR) to presynaptic DA homeostasis dictate the consequences of Val559 expression in adolescent male mice. We show that activation of D2ARs in the WT dorsal striatum (DS), but not ventral striatum (VS), increases DAT phosphorylation and surface trafficking. In contrast, the activity of tyrosine hydroxylase (TH) is D2AR-dependent in both regions. In the DS but not VS of Val559 mice, tonic activation of D2ARs drives a positive feedback loop that promotes surface expression of efflux-prone DATs, raising extracellular DA levels and overwhelming DAT-mediated DA clearance capacity. Whereas D2ARs that regulate DAT are tonically activated in the Val559 DS, D2ARs that regulate TH become desensitized, allowing maintenance of cytosolic DA needed to sustain ADE. Together with prior findings, our results argue for distinct D2AR pools that regulate DA synthesis versus DA release and inactivation and offer a clear example of how the penetrance of gene variation can be limited to a subset of expression sites based on differences in intersecting regulatory networks.SIGNIFICANCE STATEMENT Altered dopamine (DA) signaling has been linked to multiple neuropsychiatric disorders. In an effort to understand and model disease-associated DAergic disturbances, we previously screened the DA transporter (DAT) in subjects with attention-deficit hyperactivity disorder (ADHD) and identified multiple, functionally impactful, coding variants. One of these variants, Val559, supports anomalous DA efflux (ADE) and in transgenic mice leads to changes in locomotor patterns, psychostimulant sensitivity, and impulsivity. Here, we show that the penetrance of Val559 ADE is dictated by region-specific differences in how presynaptic D2-type autoreceptors (D2ARs) constrain DA signaling, biasing phenotypic effects to dorsal striatal projections. The Val559 model illustrates how the impact of genetic variation underlying neuropsychiatric disorders can be shaped by the differential engagement of synaptic regulatory mechanisms.
Copyright © 2018 the authors 0270-6474/18/385303-11$15.00/0.

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Keywords:  dopamine; dopamine D2 autoreceptor; dopamine transporter; neuropsychiatric disorders

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Year:  2018        PMID: 29739866      PMCID: PMC5990980          DOI: 10.1523/JNEUROSCI.0055-18.2018

Source DB:  PubMed          Journal:  J Neurosci        ISSN: 0270-6474            Impact factor:   6.167


  79 in total

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9.  SLC6A3 coding variant Ala559Val found in two autism probands alters dopamine transporter function and trafficking.

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4.  Dopamine transporter trafficking and Rit2 GTPase: Mechanism of action and in vivo impact.

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5.  Conditional, inducible gene silencing in dopamine neurons reveals a sex-specific role for Rit2 GTPase in acute cocaine response and striatal function.

Authors:  Carolyn G Sweeney; Patrick J Kearney; Rita R Fagan; Lindsey A Smith; Nicholas C Bolden; Rubing Zhao-Shea; Iris V Rivera; Jenya Kolpakova; Jun Xie; Guangping Gao; Andrew R Tapper; Gilles E Martin; Haley E Melikian
Journal:  Neuropsychopharmacology       Date:  2019-07-05       Impact factor: 7.853

Review 6.  In Situ Regulated Dopamine Transporter Trafficking: There's No Place Like Home.

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7.  Role of RGS12 in the differential regulation of kappa opioid receptor-dependent signaling and behavior.

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8.  Serotonin transporter inhibition and 5-HT2C receptor activation drive loss of cocaine-induced locomotor activation in DAT Val559 mice.

Authors:  Adele Stewart; Gwynne L Davis; Paul J Gresch; Rania M Katamish; Rodeania Peart; Maximilian J Rabil; Raajaram Gowrishankar; F Ivy Carroll; Maureen K Hahn; Randy D Blakely
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9.  Novelty-induced hyperactivity and suppressed cocaine induced locomotor activation in mice lacking threonine 53 phosphorylation of dopamine transporter.

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  9 in total

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