Trace Amine-Associated Receptor 1 Modulates Dopaminergic Activity

Lindemann, Lothar; Meyer, Claas A.; Jeanneau, Karine; Bradaı̈a, Amyaouch; Ozmen, Laurence; Bluethmann, Horst; Bettler, Bernhard; Wettstein, Joseph G.; Borroni, Edilio; Moreau, Jean‐Luc; Hoener, Marius C.

doi:10.1124/jpet.107.132647

Cited by 290 publications

(433 citation statements)

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“…Taar1 − / − mice also display greater locomotor stimulation to amphetamine and MA (Achat-Mendes et al, 2012;Lindemann et al, 2008;Wolinsky et al, 2007), consistent with the idea that TAAR1 function is important for counteracting some MA effects. However, the role of TAAR1 function in sensitivity to aversive effects of MA has not been examined.…”

Section: Introductionsupporting

confidence: 62%

“…However, Taar1 is within the QTL interval, and it modulates monoamine levels by altering transporter function in mice and primates (Miller, 2011(Miller, ,2012Revel et al, 2011;Miller, 2008,2009). Furthermore, Taar1 − / − mice exhibit lower basal levels and greater amphetamine-induced release of DA in the striatum, compared with +/+ mice (Lindemann et al, 2008;Wolinsky et al, 2007). Similarly, MAHDR mice, which carry the non-functional version of the TAAR1, also exhibit lower resting DA tone in the NAcc and medial prefrontal cortex (mPFC), and higher MA-induced DA release in the mPFC, but not in the NAcc (Lominac et al, 2014).…”

Section: Taar1 and Methamphetamine Intakementioning

confidence: 99%

“…Trace amines, such as p-tyramine, β-phenylethylamine, octopamine, and tryptamine, interact with this G protein-coupled receptor (Borowsky et al, 2001;Bunzow et al, 2001;Lindemann et al, 2005;Wolinsky et al, 2007), and TAAR1 modulates monoamine activity, in part, through regulation of neurotransmitter availability and disposition (Revel et al, 2011;Xie and Miller, 2008). TAAR1 agonists reduce endogenous firing of dopaminergic (DA), noradrenergic (NE), and serotonergic (5-HT) neurons, and Taar1 knockout (− / − ) mice exhibit greater amphetamine-induced release of these neurotransmitters in the striatum, compared with wild-type (+/+) littermates (Lindemann et al, 2008;Wolinsky et al, 2007).…”

Section: Introductionmentioning

confidence: 99%

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Trace Amine-Associated Receptor 1 Regulation of Methamphetamine Intake and Related Traits

Harkness

Shi

Janowsky

et al. 2015

Neuropsychopharmacol

148

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Continued methamphetamine (MA) use is dependent on a positive MA experience and is likely attenuated by sensitivity to the aversive effects of MA. Bidirectional selective breeding of mice for high (MAHDR) or low (MALDR) voluntary consumption of MA demonstrates a genetic influence on MA intake. Quantitative trait locus (QTL) mapping identified a QTL on mouse chromosome 10 that accounts for greater than 50% of the genetically-determined differences in MA intake in the MAHDR and MALDR lines. The trace amine-associated receptor 1 gene (Taar1) is within the confidence interval of the QTL and encodes a receptor (TAAR1) that modulates monoamine neurotransmission and at which MA serves as an agonist. We demonstrate the existence of a non-functional allele of Taar1 in the DBA/2J mouse strain, one of the founder strains of the selected lines, and show that this non-functional allele co-segregates with high MA drinking and with reduced sensitivity to MA-induced conditioned taste aversion (CTA) and hypothermia. The functional Taar1 allele, derived from the other founder strain, C57BL/6J, segregates with low MA drinking and heightened sensitivity to MA-induced CTA and hypothermia. A role for TAAR1 in these phenotypes is corroborated in Taar1 transgenic mice: Taar1 knockout mice consume more MA and exhibit insensitivity to MA-induced CTA and hypothermia, compared with Taar1 wild-type mice. These are the first data to show that voluntary MA consumption is, in part, regulated by TAAR1 function. Behavioral and physiological studies indicate that TAAR1 function increases sensitivity to aversive effects of MA, and may thereby protect against MA use.

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Section: Introductionsupporting

confidence: 62%

Section: Taar1 and Methamphetamine Intakementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Trace Amine-Associated Receptor 1 Regulation of Methamphetamine Intake and Related Traits

Harkness

Shi

Janowsky

et al. 2015

Neuropsychopharmacol

148

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“…However, because TAs not only activate TAAR1 but also influence the activity of TAAR4, DA transporters, adrenergic, as well as serotonin receptors it was difficult to assign specific physiological functions to TAAR1 (1, 6). With the availability of Taar1 knockout mice (7,8) it became clear that TAAR1 can inhibit DA neurons in the VTA via a receptor-mediated pathway. The genetic absence of TAAR1 clearly increased the spontaneous firing rate of DA neurons but the underlying signaling mechanism remained unclear (7).…”

mentioning

confidence: 99%

“…With the availability of Taar1 knockout mice (7,8) it became clear that TAAR1 can inhibit DA neurons in the VTA via a receptor-mediated pathway. The genetic absence of TAAR1 clearly increased the spontaneous firing rate of DA neurons but the underlying signaling mechanism remained unclear (7). Taar1 knockout mice also display behavioral and neurochemical signs of DA supersensitivity, a feature thought to relate to positive symptoms of schizophrenia (8).…”

mentioning

confidence: 99%

The selective antagonist EPPTB reveals TAAR1-mediated regulatory mechanisms in dopaminergic neurons of the mesolimbic system

Bradaı̈a

Trube

Stalder

et al. 2009

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

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Trace amine-associated receptor 1 (TAAR1) is a G protein-coupled receptor (GPCR) that is nonselectively activated by endogenous metabolites of amino acids. TAAR1 is considered a promising drug target for the treatment of psychiatric and neurodegenerative disorders. However, no selective ligand to identify TAAR1-specific signaling mechanisms is available yet. Here we report a selective TAAR1 antagonist, EPPTB, and characterize its physiological effects at dopamine (DA) neurons of the ventral tegmental area (VTA). We show that EPPTB prevents the reduction of the firing frequency of DA neurons induced by p-tyramine (p-tyr), a nonselective TAAR1 agonist. When applied alone, EPPTB increases the firing frequency of DA neurons, suggesting that TAAR1 either exhibits constitutive activity or is tonically activated by ambient levels of endogenous agonist(s). We further show that EPPTB blocks the TAAR1-mediated activation of an inwardly rectifying K ؉ current. When applied alone, EPPTB induces an apparent inward current, suggesting the closure of tonically activated K ؉ channels. Importantly, these EPPTB effects were absent in Taar1 knockout mice, ruling out off-target effects. We additionally found that both the acute application of EPPTB and the constitutive genetic lack of TAAR1 increase the potency of DA at D2 receptors in DA neurons. In summary, our data support that TAAR1 tonically activates inwardly rectifying K ؉ channels, which reduces the basal firing frequency of DA neurons in the VTA. We hypothesize that the EPPTB-induced increase in the potency of DA at D2 receptors is part of a homeostatic feedback mechanism compensating for the lack of inhibitory TAAR1 tone.desensitization ͉ dopamine supersensitivity ͉ Kir3 ͉ trace amines ͉ VTA T race amines (TAs) such as p-tyr, ␤-phenylethylamine, octopamine, and tryptamine are metabolites of amino acids that are found at low concentrations in the brain (1). Because of their structural similarity to classical biogenic amines, TAs were for a long time believed to modulate neurotransmission by displacing biogenic amines from vesicular stores or by acting on transporters in an amphetamine-like manner. It was not until TAs were found to bind to members of a family of GPCRs, the TAassociated receptors (TAARs), that receptor-mediated mechanisms were evoked (2-5). While several TAARs were identified, only TAAR1 and, to a lesser extent, TAAR4 respond to typical TAs (5). TAs such as p-tyr and ␤-phenylethylamine activate human, mouse, and rat TAAR1 with EC 50 values of 0.2-1.7 M. Other TAs (octopamine, tryptamine), classical biogenic amines, and amphetamine-related psychostimulants have much reduced potency and efficacy at TAAR1.TA binding to TAAR1 engages G s -type G proteins that activate adenylyl cyclases (1). However, because TAs not only activate TAAR1 but also influence the activity of TAAR4, DA transporters, adrenergic, as well as serotonin receptors it was difficult to assign specific physiological functions to TAAR1 (1, 6). With the availability of Taar1 knockout mice (7,8) ...

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2014

Drug Discovery for the Treatment of Addiction

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Trace Amine-Associated Receptor 1 Modulates Dopaminergic Activity

Cited by 290 publications

References 35 publications

Trace Amine-Associated Receptor 1 Regulation of Methamphetamine Intake and Related Traits

Trace Amine-Associated Receptor 1 Regulation of Methamphetamine Intake and Related Traits

The selective antagonist EPPTB reveals TAAR1-mediated regulatory mechanisms in dopaminergic neurons of the mesolimbic system

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