Reinforced Spatial Alternation as an Animal Model of Obsessive-Compulsive Disorder (OCD): Investigation of 5-HT 2C and 5-HT 1D Receptor Involvement in OCD Pathophysiology

This study introduces a laboratory model of compulsive behavior based on persistence in the context of rewarded spatial alternation. Rats were screened for spontaneous persistence during T-maze reinforced alternation. Experiment 1: One high and one low spontaneous persistence group ( n = 8) received...

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Bibliographic Details
Published inBiological psychiatry (1969) Vol. 57; no. 10; pp. 1176 - 1185
Main Authors Tsaltas, Eleftheria, Kontis, Dimitris, Chrysikakou, Sofia, Giannou, Haralambos, Biba, Angeliki, Pallidi, Stella, Christodoulou, Angeliki, Maillis, Antonis, Rabavilas, Andreas
Format Journal Article
LanguageEnglish
Published Elsevier Inc 2005
Subjects
5HT receptors
animal model
fluoxetine
mCPP
naratriptan
OCD
OCD
naratriptan
fluoxetine
mCPP
5HT receptors
animal model
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Summary:This study introduces a laboratory model of compulsive behavior based on persistence in the context of rewarded spatial alternation. Rats were screened for spontaneous persistence during T-maze reinforced alternation. Experiment 1: One high and one low spontaneous persistence group ( n = 8) received 20 injections of fluoxetine, a matched pair saline, both followed by 4 days of meta-chlorophenylpiperazine (mCPP) challenge. Experiment 2: Five matched groups of rats ( n = 9) received pretreatment (20 injections) with fluoxetine, mCPP, desipramine, diazepam or saline, followed by 4 days of mCPP challenge (fluoxetine in mCPP group). After washout, animals received 2 days of naratriptan, followed by another 2-day mCPP challenge. In both experiments mCPP significantly increased persistence in saline controls. Fluoxetine also acutely increased persistence scores: after a gradual return to baseline, these scores showed tolerance to mCPP. Experiment 1: This pattern was significant in high but not low initial persistence groups. Experiment 2: Fluoxetine and mCPP showed cross-tolerance. Neither desipramine nor diazepam protected against mCPP challenge. Persistence scores returned to baseline during washout and naratriptan and were thereafter increased by another mCPP challenge in all but the fluoxetine and mCPP groups, suggesting 5-HT 2C receptor mediation. This model is based on spontaneous persistence behavior showing pharmacological responses concordant with those of compulsive symptomatology.
ISSN:0006-3223
1873-2402
DOI:10.1016/j.biopsych.2005.02.020