Please use this identifier to cite or link to this item:
http://elar.urfu.ru/handle/10995/111556
Title: | Behavioral and Dopamine Transporter Binding Properties of the Modafinil Analog (S, S)-CE-158: Reversal of the Motivational Effects of Tetrabenazine and Enhancement of Progressive Ratio Responding |
Authors: | Rotolo, R. A. Kalaba, P. Dragacevic, V. Presby, R. E. Neri, J. Robertson, E. Yang, J. -H. Correa, M. Bakulev, V. Volkova, N. N. Pifl, C. Lubec, G. Salamone, J. D. |
Issue Date: | 2020 |
Publisher: | Springer Science and Business Media Deutschland GmbH Springer Science and Business Media LLC |
Citation: | Behavioral and Dopamine Transporter Binding Properties of the Modafinil Analog (S, S)-CE-158: Reversal of the Motivational Effects of Tetrabenazine and Enhancement of Progressive Ratio Responding / R. A. Rotolo, P. Kalaba, V. Dragacevic et al. // Psychopharmacology. — 2020. — Vol. 237. — Iss. 11. — P. 3459-3470. |
Abstract: | Rationale: Atypical dopamine (DA) transport blockers such as modafinil and its analogs may be useful for treating motivational symptoms of depression and other disorders. Previous research has shown that the DA depleting agent tetrabenazine can reliably induce motivational deficits in rats, as evidenced by a shift towards a low-effort bias in effort-based choice tasks. This is consistent with human studies showing that people with major depression show a bias towards low-effort activities. Objectives: Recent studies demonstrated that the atypical DA transport (DAT) inhibitor (S)-CE-123 reversed tetrabenazine-induced motivational deficits, increased progressive ratio (PROG) lever pressing, and increased extracellular DA in the nucleus accumbens. In the present studies, a recently synthesized modafinil analog, (S, S)-CE-158, was assessed in a series of neurochemical and behavioral studies in rats. Results: (S, S)-CE-158 demonstrated the ability to reverse the effort-related effects of tetrabenazine and increase selection of high-effort PROG lever pressing in rats tested on PROG/chow feeding choice task. (S, S)-CE-158 showed a high selectivity for inhibiting DAT compared with other monoamine transporters, and systemic administration of (S, S)-CE-158 increased extracellular DA in the nucleus accumbens during the behaviorally active time course, which is consistent with the effects of (S)-CE-123 and other DAT inhibitors that enhance high-effort responding. Conclusions: These studies provide an initial neurochemical characterization of a novel atypical DAT inhibitor, and demonstrate that this compound is active in models of effort-related choice. This research could contribute to the development of novel compounds for the treatment of motivational dysfunctions in humans. © 2020, Springer-Verlag GmbH Germany, part of Springer Nature. |
Keywords: | ANERGIA DEPRESSION DOPAMINE FATIGUE MODAFINIL MOTIVATION SYNTHESIS TRANSPORT 5 [[[(3 BROMOPHENYL)(PHENYL)METHYL]SULFINYL]METHYL]THIAZOLE ANTIDEPRESSANT AGENT CE 158 DOPAMINE TRANSPORTER TETRABENAZINE UNCLASSIFIED DRUG ADRENERGIC RECEPTOR AFFECTING AGENT DOPAMINE TRANSPORTER MODAFINIL PROTEIN BINDING TETRABENAZINE ADULT ANIMAL EXPERIMENT ANIMAL TISSUE ANTIDEPRESSANT ACTIVITY ARTICLE CAUDATE NUCLEUS CONTROLLED STUDY DECISION MAKING DOPAMINERGIC TRANSMISSION DRUG DETERMINATION DRUG EFFECT DRUG POTENCY DRUG PROTEIN BINDING DRUG STRUCTURE FEEDING IC50 IN VITRO STUDY MALE MOTIVATION NEUROCHEMISTRY NONHUMAN NUCLEUS ACCUMBENS PRIORITY JOURNAL PROTEIN EXPRESSION PUTAMEN RAT SCANNING ELECTRON MICROSCOPY SYSTEMIC THERAPY ANIMAL DOSE RESPONSE FEEDING BEHAVIOR HEK293 CELL LINE HUMAN METABOLISM PHYSIOLOGY SPRAGUE DAWLEY RAT ADRENERGIC UPTAKE INHIBITORS ANIMALS CHOICE BEHAVIOR DOPAMINE PLASMA MEMBRANE TRANSPORT PROTEINS DOSE-RESPONSE RELATIONSHIP, DRUG FEEDING BEHAVIOR HEK293 CELLS HUMANS MALE MODAFINIL NUCLEUS ACCUMBENS PROTEIN BINDING RATS RATS, SPRAGUE-DAWLEY TETRABENAZINE |
URI: | http://elar.urfu.ru/handle/10995/111556 |
Access: | info:eu-repo/semantics/openAccess |
SCOPUS ID: | 85089100938 |
WOS ID: | 000557112200001 |
PURE ID: | 14163499 |
ISSN: | 0033-3158 |
DOI: | 10.1007/s00213-020-05625-6 |
Sponsorship: | The authors would like to acknowledge Eurofins DiscoverX Corporation (Fremont, CA). |
Appears in Collections: | Научные публикации ученых УрФУ, проиндексированные в SCOPUS и WoS CC |
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