Behavioral, biological, and chemical perspectives on atypical agents targeting the dopamine transporter

Reith, Maarten E. A.; Blough, Bruce E.; Hong, Weijun; Jones, Kymry T.; Schmitt, Kyle C.; Baumann, Michael H.; Partilla, John S.; Rothman, Richard B.; Katz, Jonathan L.

doi:10.1016/j.drugalcdep.2014.12.005

Cited by 115 publications

(127 citation statements)

References 132 publications

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“…The correlation among those effects is greater than that for behavioral effects and affinities at the other monoamine transporters (Ritz et al, 1987), suggesting that behavioral effects of cocaine-like drugs are attributable to actions at the DAT (Kuhar et al, 1991). However, an increasing number of DAT inhibitors are being found with effects different from those of cocaine (Reith et al, 2015).…”

Section: Discussionmentioning

confidence: 86%

“…Contrary to the DAT hypothesis, several groups of compounds with DAT affinity have in vivo or in vitro effects that are distinct from those of standard DAT inhibitors such as cocaine (reviewed by Reith et al, 2015). These "atypical" DAT inhibitors include benztropine (BZT) and its analogs, which consist of the tropane ring of cocaine and the diphenylether moiety common to the piperazine class of DA uptake inhibitors such as GBR 12909 (Van der Zee et al, 1980).…”

Section: Introductionmentioning

confidence: 99%

“…However, several studies have suggested that antagonist actions at M 1 sites contribute minimally if at all to the atypical effects of BZT analogs (see review by Reith et al, 2015). More recently, it has been suggested that compounds with sigma receptor (sR) antagonist effects along with their affinity for the DAT will exhibit atypical DAT inhibitory effects similar to BZT .…”

Section: Introductionmentioning

confidence: 99%

“…Another potential mechanism for atypical actions of DAT inhibitors is the stabilization of cytosol-facing conformations resulting from ligand binding (see review by Reith et al, 2015). For example, Loland et al (2008) proposed a correlation between conformational states stabilized with DAT binding and the behavioral effects of a diverse group of DAT ligands.…”

Section: Introductionmentioning

confidence: 99%

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2-Substituted 3 -Aryltropane Cocaine Analogs Produce Atypical Effects without Inducing Inward-Facing Dopamine Transporter Conformations

Hong

Kopajtic

et al. 2016

Journal of Pharmacology and Experimental Therapeutics

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Previous structure-activity relationship studies indicate that a series of cocaine analogs, 3b-aryltropanes with 2b-diarylmethoxy substituents, selectively bind to the dopamine transporter (DAT) with nanomolar affinities that are 10-fold greater than the affinities of their corresponding 2a-enantiomers. The present study compared these compounds to cocaine with respect to locomotor effects in mice, and assessed their ability to substitute for cocaine (10 mg/kg, i.p.) in rats trained to discriminate cocaine from saline. Despite nanomolar DAT affinity, only the 2b-Ph 2 COCH 2 -3b-4-ClPh analog fully substituted for cocaine-like discriminative effects. Whereas all of the 2b compounds increased locomotion, only the 2b-(4-ClPh)PhCOCH 2 -3b-4-Cl-Ph analog had cocaine-like efficacy. None of the 2a-substituted compounds produced either of these cocaine-like effects. To explore the molecular mechanisms of these drugs, their effects on DAT conformation were probed using a cysteine-accessibility assay. Previous reports indicate that cocaine binds with substantially higher affinity to the DAT in its outward (extracellular)-compared with inward-facing conformation, whereas atypical DAT inhibitors, such as benztropine, have greater similarity in affinity to these conformations, and this is postulated to explain their divergent behavioral effects. All of the 2b-and 2a-substituted compounds tested altered cysteine accessibility of DAT in a manner similar to cocaine. Furthermore, molecular dynamics of in silico inhibitor-DAT complexes suggested that the 2-substituted compounds reach equilibrium in the binding pocket in a cocaine-like fashion. These behavioral, biochemical, and computational results show that aryltropane analogs can bind to the DAT and stabilize outward-facing DAT conformations like cocaine, yet produce effects that differ from those of cocaine.

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Section: Discussionmentioning

confidence: 86%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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2-Substituted 3 -Aryltropane Cocaine Analogs Produce Atypical Effects without Inducing Inward-Facing Dopamine Transporter Conformations

Hong

Kopajtic

et al. 2016

Journal of Pharmacology and Experimental Therapeutics

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“…Given that cocaine self-administration behavior is sensitive to fast changes in extracellular DA, the slow-onset long-lasting increase in DA produced by CTDP-32476 may underlie the reduction in cocaine self-administration observed in the present study. Another possibility is that CTDP-32476 may act as other atypical DAT inhibitors such as GBR-12909, benztropine, or modafinil-that induce a 'closed' or inwardfacing conformation upon binding to the DAT (Loland et al, 2008;Reith et al, 2015). Because cocaine has higher binding affinity for the more 'open' conformation, a compound inducing a 'closed' conformation would be more likely to attenuate cocaine binding to the DAT and thus be less effective as a DAT inhibitor.…”

Section: Discussionmentioning

confidence: 99%

CTDP-32476: A Promising Agonist Therapy for Treatment of Cocaine Addiction

Song²,

et al. 2016

Neuropsychopharmacol

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Agonist-replacement therapies have been successfully used for treatment of opiate and nicotine addiction, but not for cocaine addiction. One of the major obstacles is the cocaine-like addictive potential of the agonists themselves. We report here an atypical dopamine (DA) transporter (DAT) inhibitor, CTDP-32476, that may have translational potential for treating cocaine addiction. In vitro ligand-binding assays suggest that CTDP-32476 is a potent and selective DAT inhibitor and a competitive inhibitor of cocaine binding to the DAT. Systemic administration of CTDP-32476 alone produced a slow-onset, long-lasting increase in extracellular nucleus accumbens DA, locomotion, and brain-stimulation reward. Drug-naive rats did not self-administer CTDP-32476. In a substitution test, cocaine self-administration rats displayed a progressive reduction in CTDP-32476 self-administration with an extinction pattern of drug-taking behavior, suggesting significantly lower addictive potential than cocaine. Pretreatment with CTDP-32476 inhibited cocaine self-administration, cocaineassociated cue-induced relapse to drug seeking, and cocaine-enhanced extracellular DA in the nucleus accumbens. These findings suggest that CTDP-32476 is a unique DAT inhibitor that not only could satisfy 'drug hunger' through its slow-onset long-lasting DAT inhibitor action, but also render subsequent administration of cocaine ineffectual-thus constituting a novel and unique compound with translational potential as an agonist therapy for treatment of cocaine addiction.

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Amine Transporters

Reith¹

2020

Encyclopedia of Life Sciences

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Amine transporters in plasma membranes of nerve cells mediate the transport of dopamine, (nor)adrenaline and serotonin. These transporters are members of the larger Na + ‐ and Cl − ‐dependent neurotransmitter transporter family. All three transporters have been cloned, and the bacterial leucine transporter was the first prototypical structure available; this was followed by crystals of the drosophila dopamine transporter and the human serotonin transporter. Amine transporters are implicated in psychiatric disorders, such as attention‐deficit/hyperactivity disorder, schizophrenia, Parkinson disease, suicidal and aggressive‐impulsive behaviour, and are involved in affective disorders including depression. Amine transporters are important targets for psychostimulant drugs as well as antidepressants. Key Concepts Amine transporters in plasma membranes of nerve cells mediate the transport of dopamine, noradrenaline, adrenaline and serotonin through cotransport with Na + towards the cytosol where the Na + concentration is low. Amine uptake is best described by the alternating access model; accordingly, the transporter protein moves back and forth between outward‐ and inward‐facing conformations. Amine transporters are organised in multimeric structures, that is, oligomers consisting of varying numbers of protomers. How oligomerisation affects the function of each protomer is not fully understood. In addition to a primary central binding site for substrate and drugs, amine transporters have an extracellular vestibule, accommodating with appreciable flexibility varying small‐molecule allosteric ligands. Transporter polymorphisms and variants have been associated with increased risk for psychiatric diseases; a number of DAT variants, one‐point mutations, are known to cause parkinsonian symptoms starting at infancy in a hereditary recessive fashion. In addition to allosteric modulators, atypical inhibitors and releasers targeting amine transporters are subject of intense research.

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Behavioral, biological, and chemical perspectives on atypical agents targeting the dopamine transporter

Cited by 115 publications

References 132 publications

2-Substituted 3 -Aryltropane Cocaine Analogs Produce Atypical Effects without Inducing Inward-Facing Dopamine Transporter Conformations

2-Substituted 3 -Aryltropane Cocaine Analogs Produce Atypical Effects without Inducing Inward-Facing Dopamine Transporter Conformations

CTDP-32476: A Promising Agonist Therapy for Treatment of Cocaine Addiction

Amine Transporters

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