Anomalous Dopamine Release Associated with a Human Dopamine Transporter Coding Variant

Mazei-Robison, Michelle S.; Bowton, Erica; Holy, Marion; Schmudermaier, Martin; Freissmuth, Michael; Sitte, Harald H.; Galli, Aurelio; Blakely, Randy D.

doi:10.1523/jneurosci.0473-08.2008

Cited by 120 publications

(174 citation statements)

References 31 publications

(38 reference statements)

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“…As noted in the prior publication, these mice reproduce normally and display no overt sensorimotor deficits. Our previous heterologous expression studies demonstrated no impact of the DAT Val559 substitution on total or cell surface expression, inward DA transport, or sensitivity to psychostimulants (8,58). Consistent with these findings, striatal extracts from DAT Val559 animals demonstrate normal transporter protein levels (Fig.…”

Section: Resultssupporting

confidence: 81%

“…The key phenotypes found for DAT Val559 in transfected cells are ADE and a loss of AMPH-induced DA release (13,58). Evidence of ADE in vivo arises from both our striatal microdialysis studies that demonstrate a significant elevation of basal extracellular DA levels and our findings of elevated presynaptic D2 modulation of vesicular DA release that can be normalized with D2R antagonist (raclopride) treatments.…”

Section: Discussionmentioning

confidence: 72%

“…6F), suggesting that the enhanced darting speeds of DAT Val559 animals reflects a specific reaction to imminent handling. Our studies of AMPH action on DAT Val559-transfected cells demonstrated that the drug inhibits both DA uptake and ADE (58), but lacks the ability to produce DAT-mediated DA efflux (69). Moreover, our studies of AMPH effects on somatodendritic D2R-dependent IPSCs and on DA release in terminal fields revealed significantly blunted responses.…”

Section: Dat Val559 Mice Demonstrate Conditional Hyperactivity and Blmentioning

confidence: 71%

“…Often, such variation is confined to a single, and sometimes small, pedigree, compelling the demonstration of functional perturbations in vitro and in vivo to make conclusions as to possible disease associations. Our efforts to date have uncovered multiple rare SLC6A3 coding variants in screens of ADHD subjects, with two of these, A559V and R615C, demonstrating altered function after heterologous expression (58,77). Here, we present the first opportunity, to our knowledge, to explore the impact of diseaseassociated, rare DAT variation in vivo.…”

Section: Discussionmentioning

confidence: 94%

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The rare DAT coding variant Val559 perturbs DA neuron function, changes behavior, and alters in vivo responses to psychostimulants

Mergy¹,

Gowrishankar²,

Gresch

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

105

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Despite the critical role of the presynaptic dopamine (DA) transporter (DAT, SLC6A3) in DA clearance and psychostimulant responses, evidence that DAT dysfunction supports risk for mental illness is indirect. Recently, we identified a rare, nonsynonymous Slc6a3 variant that produces the DAT substitution Ala559Val in two male siblings who share a diagnosis of attention-deficit hyperactivity disorder (ADHD), with other studies identifying the variant in subjects with bipolar disorder (BPD) and autism spectrum disorder (ASD). Previously, using transfected cell studies, we observed that although DAT Val559 displays normal total and surface DAT protein levels, and normal DA recognition and uptake, the variant transporter exhibits anomalous DA efflux (ADE) and lacks capacity for amphetamine (AMPH)-stimulated DA release. To pursue the significance of these findings in vivo, we engineered DAT Val559 knock-in mice, and here we demonstrate in this model the presence of elevated extracellular DA levels, altered somatodendritic and presynaptic D2 DA receptor (D2R) function, a blunted ability of DA terminals to support depolarization and AMPHevoked DA release, and disruptions in basal and psychostimulant-evoked locomotor behavior. Together, our studies demonstrate an in vivo functional impact of the DAT Val559 variant, providing support for the ability of DAT dysfunction to impact risk for mental illness.T he neurotransmitter dopamine (DA) plays a key role in regulating brain circuits that control reward, attention, and locomotor activity (1-3), Accordingly, dopaminergic dysfunction is believed to contribute to several neuropsychiatric disorders including Parkinson's disease (4), bipolar disorder (BPD) (5), drug abuse and addiction (6), and attention-deficit hyperactivity disorder (ADHD) (7,8). The presynaptic DA transporter (DAT) is the primary mechanism for terminating DA signaling at the synapse (9) and is the primary target for several psychostimulant drugs including cocaine (COC), methylphenidate (MPH), and amphetamine (AMPH). COC and MPH are DAT antagonists, elevating extracellular DA levels by preventing DAT-mediated DA reuptake (10). AMPH actions are more complex (11). AMPH is structurally similar to DA and, as a result, is transported by DAT, competing with DA during the reuptake process. AMPH also induces DAT-mediated nonvesicular release, also termed "DA efflux," a process that involves the actions of intracellular signaling proteins such as CamKIIα (12-16) and , alterations in interactions with DAT-associated proteins and phospholipids (12,14,20), and changes in DAT phosphorylation (12,16,(21)(22)(23)) that biases the transporter toward an efflux-competent mechanism. Despite their mechanistic differences, MPH and AMPH both rapidly elevate DA in the CNS and are components of the most frequently prescribed medications for ADHD, Ritalin and Adderall, respectively. The DA modulatory actions of MPH and AMPH reinforce hypotheses derived from brain imaging studies (24) and the analysis of common genetic variation (25-30)...

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Section: Resultssupporting

confidence: 81%

Section: Discussionmentioning

confidence: 72%

Section: Dat Val559 Mice Demonstrate Conditional Hyperactivity and Blmentioning

confidence: 71%

Section: Discussionmentioning

confidence: 94%

See 2 more Smart Citations

The rare DAT coding variant Val559 perturbs DA neuron function, changes behavior, and alters in vivo responses to psychostimulants

Mergy¹,

Gowrishankar²,

Gresch

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

105

View full text Add to dashboard Cite

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“…Transporter-expressing cell lines allow the characterization of psychoactive compounds (Tatsumi et al, 1997) and are also a useful tool for discovering psychoactive therapeutic drugs (Bang-Andersen et al, 2011). Furthermore, in vitro experiments with transfected cells formed the basis for many genetic mutations that were later engineered in mice, which now serve for in vivo investigations of psychoactive drugs or as preclinical models of mental disorders (Henry et al, 2006;Mazei-Robison et al, 2008;Prasad et al, 2005). For example, in vitro experiments allowed the construction of a transgenic mouse model with a 5-hydroxytryptamine (5-HT [serotonin]) transporter (SERT) mutation for the in vivo assessment of SERT-mediated effects of antidepressants or cocaine (Prosser et al, 2014;Thompson et al, 2011) or to shed light on functional abnormalities of the DAT variant Val559, which is being investigated as a potential mouse model of attention-deficit hyperactivity disorder (Mergy et al, 2014).…”

Section: Methods For Studying Transporter and Receptor Pharmacology Imentioning

confidence: 99%

Interactions of Cathinone NPS with Human Transporters and Receptors in Transfected Cells

Simmler

Liechti

2016

Neuropharmacology of New Psychoactive Substances (NPS)

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Pharmacological assays carried out in transfected cells have been very useful for describing the mechanism of action of cathinone new psychoactive substances (NPS). These in vitro characterizations provide fast and reliable information on psychoactive substances soon after they emerge for recreational use. Well-investigated comparator compounds, such as methamphetamine, 3,4-methylenedioxymethamphetamine, cocaine, and lysergic acid diethylamide, should always be included in the characterization to enhance the translation of the in vitro data into clinically useful information. We classified cathinone NPS according to their pharmacology at monoamine transporters and receptors. Cathinone NPS are monoamine uptake inhibitors and most induce transportermediated monoamine efflux with weak to no activity at pre-or postsynaptic receptors. Cathinones with a nitrogen-containing pyrrolidine ring emerged as NPS that are extremely potent transporter inhibitors but not monoamine releasers. Cathinones exhibit clinically relevant differences in relative potencies at serotonin vs. dopamine transporters. Additionally, cathinone NPS have more dopaminergic vs. serotonergic properties compared with their non-β-keto amphetamine analogs, suggesting more stimulant and reinforcing properties. In conclusion, in vitro pharmacological assays in heterologous expression systems help to predict the psychoactive and toxicological effects of NPS.

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Computational modeling of the N-terminus of the human dopamine transporter and its interaction with PIP₂ -containing membranes

et al. 2015

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The dopamine transporter (DAT) is a transmembrane protein belonging to the family of Neurotransmitter:Sodium Symporters (NSS). Members of the NSS are responsible for the clearance of neurotransmitters from the synaptic cleft, and for their translocation back into the presynaptic nerve terminal. The DAT contains long intracellular N- and C-terminal domains that are strongly implicated in the transporter function. The N-terminus (N-term), in particular, regulates the reverse transport (efflux) of the substrate through DAT. Currently, the molecular mechanisms of the efflux remain elusive in large part due to lack of structural information on the N-terminal segment. Here we report a computational model of the N-term of the human DAT (hDAT), obtained through an ab initio structure prediction, in combination with extensive atomistic molecular dynamics (MD) simulations in the context of a lipid membrane. Our analysis reveals that whereas the N-term is a highly dynamic domain, it contains secondary structure elements that remain stable in the long MD trajectories of interactions with the bilayer (totaling >2.2 µs). Combining MD simulations with continuum mean-field modeling we found that the N-term engages with lipid membranes through electrostatic interactions with the charged lipids PIP2 (phosphatidylinositol 4,5-Biphosphate) or PS (phosphatidylserine) that are present in these bilayers. We identify specific motifs along the N-term implicated in such interactions and show that differential modes of N-term/membrane association result in differential positioning of the structured segments on the membrane surface. These results will inform future structure-based studies that will elucidate the mechanistic role of the N-term in DAT function.

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Anomalous Dopamine Release Associated with a Human Dopamine Transporter Coding Variant

Cited by 120 publications

References 31 publications

The rare DAT coding variant Val559 perturbs DA neuron function, changes behavior, and alters in vivo responses to psychostimulants

The rare DAT coding variant Val559 perturbs DA neuron function, changes behavior, and alters in vivo responses to psychostimulants

Interactions of Cathinone NPS with Human Transporters and Receptors in Transfected Cells

Computational modeling of the N-terminus of the human dopamine transporter and its interaction with PIP₂ -containing membranes

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Anomalous Dopamine Release Associated with a Human Dopamine Transporter Coding Variant

Cited by 120 publications

References 31 publications

The rare DAT coding variant Val559 perturbs DA neuron function, changes behavior, and alters in vivo responses to psychostimulants

The rare DAT coding variant Val559 perturbs DA neuron function, changes behavior, and alters in vivo responses to psychostimulants

Interactions of Cathinone NPS with Human Transporters and Receptors in Transfected Cells

Computational modeling of the N-terminus of the human dopamine transporter and its interaction with PIP2 -containing membranes

Contact Info

Product

Resources

About

Computational modeling of the N-terminus of the human dopamine transporter and its interaction with PIP₂ -containing membranes