Literature DB >> 24140929

Long-term impacts of adolescent risperidone treatment on behavioral responsiveness to olanzapine and clozapine in adulthood.

Jing Qiao1, Qinglin Zhang, Ming Li.   

Abstract

This preclinical study investigated how a short-term risperidone treatment in adolescence impacts antipsychotic response to olanzapine and clozapine in adulthood. Antipsychotic effect was indexed by a drug's suppressive effect on avoidance responding in a rat conditioned avoidance response (CAR) model. Male adolescent Sprague-Dawley rats were first treated with risperidone (1.0mg/kg, sc) or sterile water and tested in the CAR model for 5 consecutive days from postnatal days P 40 to 44. After they became adults (~P 80-84), they were switched to olanzapine (0.5mg/kg, sc), clozapine (5.0mg/kg, sc) or vehicle treatment and tested for avoidance for 5days. During the adolescent period, repeated risperidone treatment produced a persistent inhibition of avoidance response. Throughout the 5days of adulthood drug testing, rats previously treated with risperidone in adolescence made significantly fewer avoidance responses than the vehicle ones when they all were switched to olanzapine, indicating a risperidone-induced enhancement of behavioral sensitivity to olanzapine. In contrast, when switched to clozapine, rats previously treated with risperidone made significantly more avoidance responses than the vehicle rats, indicating a risperidone-induced decrease of behavioral sensitivity to clozapine. Performance in the prepulse inhibition of acoustic startle response in adulthood was not altered by adolescent risperidone treatment. Collectively, adolescent risperidone exposure induced a long-term change in behavioral sensitivity to other atypical antipsychotic drugs, with the specific direction of change (i.e., increase or decrease) dependent on the drug to be switched to. These long-lasting changes are likely mediated by drug-induced neuroplastic changes and may also have significant clinical implications for antipsychotic treatment of chronic patients with an early onset of psychotic symptoms.
© 2013.

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Keywords:  % PPI; 5′-Bromo-2-deoxyuridine; Adolescence; BrdU; CAR; CLZ; CLZ 5.0; CS; Clozapine; Conditioned avoidance response; DA; FDA; Food and Drug Administration; GABA; OLZ; OLZ 0.5; Olanzapine; P; PCP; PFC; PPI; RIS; RIS 1.0; Risperidone; Sensitization; US; VEH; clozapine; clozapine 5.0 mg/kg; conditioned avoidance response; conditioned stimulus; dopamine; gamma amino butyric acid; olanzapine; olanzapine 0.5 mg/kg; percent prepulse inhibition; phencyclidine; postnatal; prefrontal cortex; prepulse inhibition; risperidone; risperidone 1.0 mg/kg; sc; subcutaneously; unconditioned stimulus; vehicle

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Year:  2013        PMID: 24140929      PMCID: PMC3859461          DOI: 10.1016/j.pnpbp.2013.10.005

Source DB:  PubMed          Journal:  Prog Neuropsychopharmacol Biol Psychiatry        ISSN: 0278-5846            Impact factor:   5.067


  54 in total

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2.  Repeated effects of the neurotensin receptor agonist PD149163 in three animal tests of antipsychotic activity: assessing for tolerance and cross-tolerance to clozapine.

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4.  Differential effects of intermittent versus continuous haloperidol treatment throughout adolescence on haloperidol sensitization and social behavior in adulthood.

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5.  Maternal immune activation and repeated maternal separation alter offspring conditioned avoidance response learning and antipsychotic response in male rats.

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Review 6.  Antipsychotic-induced sensitization and tolerance: Behavioral characteristics, developmental impacts, and neurobiological mechanisms.

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  6 in total

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