4.1 Article Proceedings Paper

Dual Dopamine/Serotonin Releasers: Potential Treatment Agents for Stimulant Addiction

Journal

EXPERIMENTAL AND CLINICAL PSYCHOPHARMACOLOGY
Volume 16, Issue 6, Pages 458-474

Publisher

AMER PSYCHOLOGICAL ASSOC
DOI: 10.1037/a0014103

Keywords

alcohol; amphetamine; cocaine; dopamine; serotonin; transporter

Funding

  1. Intramural NIH HHS [Z01 DA000119-16] Funding Source: Medline
  2. NIDA NIH HHS [R01 DA12970, R01 DA012970, R01 DA012970-08] Funding Source: Medline

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Agonist therapy for cocaine and methamphetamine addiction involves administration of stimulant-like medications (e.g., monoamine releasers) to reduce withdrawal symptoms and prevent relapse. A significant problem with this strategy is that many candidate medications possess abuse liability because of activation of mesolimbic dopamine (DA) neurons in the brain. One way to reduce DA-mediated abuse liability of candidate drugs is to add in serotonin (5-HT) releasing properties, since substantial evidence shows that 5-HT neurons provide an inhibitory influence over mesolimbic DA neurons. This article addresses several key issues related to the development of dual DA/5-HT releasers for the treatment of substance use disorders. First, the authors briefly summarize the evidence supporting a dual deficit in DA and 5-HT function during withdrawal from chronic cocaine or alcohol abuse. Second, the authors discuss data demonstrating that 5HT release can dampen DA-mediated stimulant effects, and the antistimulant role of 5-HT2C receptors is considered. Next, the mechanisms underlying potential adverse effects of 5-HT releasers are described. Finally, the authors discuss recently published data with PAL-287, a novel nonamphetamine DA/5-HT releasing agent that suppresses cocaine self-administration but lacks positive reinforcing properties. It is concluded that DA/5-HT releasers could be useful therapeutic adjuncts for the treatment of cocaine and alcohol addictions, as well as for obesity, attention-deficit disorder, and depression.

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