Abstract

A scientific search for therapeutically useful compounds in combating psychostimulant abuse and addiction has been in progress for decades, with no clinically available agents to date. A major hindrance toward this goal has been the limited information on the structure and function of the plasma membrane monoamine transporter proteins. Pharmacological and behavioral studies indicate that the dopamine transporter protein (DAT) is the brain receptor chiefly responsible for the reward/reinforcing properties of cocaine and the amphetamines. The serotonin transporter protein (SERT) also plays a key role in the mood-altering effects of these drugs, especially in the case of amphetamines such as MDMA (""""""""ecstasy""""""""). The DAT and SERT are responsible for termination of neurotransmission by uptake of the monoamine neurotransmitter from the neuronal synapse. The long-term objective of this application is to understand how cocaine and the amphetamines interact with the DAT and SERT, which entails mapping the DAT and SERT binding pockets of these drugs at the level of the amino acid residue. This level of resolution may now be a possibility, as the recently published X-ray crystal structure of the LeuTAa transporter protein, homologous in sequence to the DAT and SERT, can serve as a template for creation of 3-dimensional DAT and SERT computer models. The two specific aims of this proposal are to create LeuTAa-based 3-D DAT and SERT models, and use the models to identify and characterize via site-directed mutagenesis and pharmacology the DAT and SERT residues key in substrate (e.g., dopamine, serotonin, various amphetamines) and inhibitor (e.g., cocaine, methylphenidate) recognition. The resultant pharmacologic data will be used to refine the molecular models to the point that they can be employed in in silico screening of structural libraries containing hundreds of thousands of """"""""small molecule"""""""" compounds in the search for novel DAT and SERT ligands.
These specific aims will be addressed by DAT and SERT computer-aided molecular modeling to identify logical mutagenesis targets, site-directed mutagenesis of the cDNAs encoding the DAT and SERT proteins, transfecting mammalian cell lines with wildtype or mutant DAT or SERT cDNAs, assaying transfected cells for binding and uptake of radiolabeled DAT or SERT ligands, inhibition of radioligand binding or uptake with non-radioactive competing DAT or SERT ligands, and assessment of cell surface expression of the transporter proteins via immunoblotting techniques. Results from the proposed experiments should reveal specific insights as to how cocaine and the amphetamines exert their effects via these monoamine transporters, as well as information on DAT recognition of drugs with less abuse potential such as benztropine and methylphenidate and SERT recognition of antidepressant drugs. Elucidating at the amino acid residue level the mechanisms of discriminating abused and non-abused substrates and inhibitors should provide a blueprint for rational design of medications that block cocaine and amphetamine actions without in turn carrying the potential for abuse and addiction. Additionally, these studies may lead to therapeutics for other DAT- or SERT-related conditions including depression, anxiety disorders, attention deficit hyperactivity disorder, migraine, narcolepsy and Parkinson's disease. The proposed dopamine transporter (DAT) and serotonin transporter (SERT) studies tease apart binding requirements for psychostimulants of low abuse potential (benztropine and methylphenidate) and high abuse potential (cocaine and methamphetamine), and should even allow discrimination of monoamine transporter recognition mechanisms for cocaine, methamphetamine and MDMA (""""""""ecstasy""""""""). Exploring exactly how specific DAT and SERT protein components contribute to recognition of abused and non-abused drugs should provide a blueprint for designing medications that block actions of cocaine and the amphetamines without in turn carrying the potential for abuse and addiction. Additionally, these studies may lead to therapeutics for other DAT- or SERT-related conditions including depression, anxiety disorders, attention deficit hyperactivity disorder, migraine, narcolepsy and Parkinson's disease. ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Academic Research Enhancement Awards (AREA) (R15)
Project #
2R15DA016604-03A1
Application #
7305399
Study Section
Neurotransporters, Receptors, and Calcium Signaling Study Section (NTRC)
Program Officer
Rapaka, Rao
Project Start
2003-08-01
Project End
2010-07-31
Budget Start
2007-08-01
Budget End
2010-07-31
Support Year
3
Fiscal Year
2007
Total Cost
$179,019
Indirect Cost

  Institution

Name
Duquesne University
Department
Pharmacology
Type
Schools of Pharmacy
DUNS #
004501193
City
Pittsburgh
State
PA
Country
United States
Zip Code
15282

  Publications

Lapinsky, David J; Aggarwal, Shaili; Nolan, Tammy L et al. (2012) (±)-2-(N-tert-Butylamino)-3'-[(125)I]-iodo-4'-azidopropiophenone: a dopamine transporter and nicotinic acetylcholine receptor photoaffinity ligand based on bupropion (Wellbutrin, Zyban). Bioorg Med Chem Lett 22:523-6
Lapinsky, David J; Yarravarapu, Nageswari; Nolan, Tammy L et al. (2012) Evolution of a Compact Photoprobe for the Dopamine Transporter Based on (±)-threo-Methylphenidate. ACS Med Chem Lett 3:378-382
Lapinsky, David J; Velagaleti, Ranganadh; Yarravarapu, Nageswari et al. (2011) Azido-iodo-N-benzyl derivatives of threo-methylphenidate (Ritalin, Concerta): Rational design, synthesis, pharmacological evaluation, and dopamine transporter photoaffinity labeling. Bioorg Med Chem 19:504-12
Indarte, Martín; Liu, Yi; Madura, Jeffry D et al. (2010) Receptor-Based Discovery of a Plasmalemmal Monoamine Transporter Inhibitor via High Throughput Docking and Pharmacophore Modeling. ACS Chem Neurosci 1:223-233
Lapinsky, David J; Aggarwal, Shaili; Huang, Yurong et al. (2009) A novel photoaffinity ligand for the dopamine transporter based on pyrovalerone. Bioorg Med Chem 17:3770-4
Indarte, Martin; Madura, Jeffry D; Surratt, Christopher K (2008) Dopamine transporter comparative molecular modeling and binding site prediction using the LeuT(Aa) leucine transporter as a template. Proteins 70:1033-46
Ukairo, Okechukwu T; Ramanujapuram, Suneetha; Surratt, Christopher K (2007) Fluctuation of the dopamine uptake inhibition potency of cocaine, but not amphetamine, at mammalian cells expressing the dopamine transporter. Brain Res 1131:68-76
Ukairo, Okechukwu T; Bondi, Corry D; Newman, Amy Hauck et al. (2005) Recognition of benztropine by the dopamine transporter (DAT) differs from that of the classical dopamine uptake inhibitors cocaine, methylphenidate, and mazindol as a function of a DAT transmembrane 1 aspartic acid residue. J Pharmacol Exp Ther 314:575-83
Surratt, Christopher K; Ukairo, Okechukwu T; Ramanujapuram, Suneetha (2005) Recognition of psychostimulants, antidepressants, and other inhibitors of synaptic neurotransmitter uptake by the plasma membrane monoamine transporters. AAPS J 7:E739-51