Reversal of Subchronic PCP-Induced Deficits in Attentional Set Shifting in Rats by Sertindole and a 5-HT6 Receptor Antagonist: Comparison Among Antipsychotics

Rodefer, Joshua S.; Nguyen, Tuyet N.; Karlsson, Jens-Jakob; Arnt, Jørn

doi:10.1038/sj.npp.1301654

Cited by 114 publications

(115 citation statements)

References 65 publications

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“…In contrast, Rodefer and colleagues subsequently found that clozapine and risperidone to be ineffective in reversing the PCP-induced deficit, however sertindole and the selective 5-HT 6 (SB-271046) and 5-HT 2A (M100907) receptor antagonists did attenuate the PCP-induced impairment (Rodefer et al, 2008), which is similar to our findings using reversal learning paradigm (Idris et al 2010). This same dosing regime was shown again in male hooded-Lister rats to produce deficits in the EDS phase; an effect which was ameliorated by sertindole and the anti-narcoleptic drug modafinil but not by risperidone or haloperidol (Goetghebeur and Dias, 2009).…”

Section: Attentional Set-shiftingsupporting

confidence: 86%

Animal models of cognitive dysfunction and negative symptoms of schizophrenia: Focus on NMDA receptor antagonism

Neill

Barnes

Cook

et al. 2010

Pharmacology & Therapeutics

473

322

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Cognitive deficits in schizophrenia remain an unmet clinical need. Improved understanding of the neuro-and psychopathology of these deficits depends on the availability of carefully validated animal models which will assist the development of novel therapies. There is much evidence that at least some of the pathology and symptomatology (particularly cognitive and negative symptoms) of schizophrenia results from a dysfunction of the glutamatergic system which may be modelled in animals through the use of NMDA receptor antagonists. The current review examines the validity of this model in rodents. We review the ability of acute and sub-chronic treatment with three non-competitive NMDA antagonists; phencyclidine (PCP), ketamine and MK801 (dizocilpine) to produce cognitive disturbances of relevance to schizophrenia in rodents and their subsequent reversal by first-and second-generation antipsychotic drugs. Effects of NMDA receptor antagonists on the performance of rodents in behavioural tests assessing the various domains of cognition and negative symptoms are examined: novel object recognition for visual memory, reversal learning and attentional set shifting for problem solving and reasoning, 5-choice serial reaction time for attention and speed of processing; in addition to effects on social behaviour and neuropathology. The evidence strongly supports the use of NMDA receptor antagonists to model cognitive deficit and negative symptoms of schizophrenia as well as certain pathological disturbances seen in the illness. This will facilitate the evaluation of much-needed novel therapies for improved therapy of cognitive deficits and negative symptoms in schizophrenia.

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Section: Attentional Set-shiftingsupporting

confidence: 86%

Animal models of cognitive dysfunction and negative symptoms of schizophrenia: Focus on NMDA receptor antagonism

Neill

Barnes

Cook

et al. 2010

Pharmacology & Therapeutics

473

322

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“…The D 1 antagonist used in these studies (SCH23390) has affinity for both D 1 and 5HT 2A receptors. However, the observation that systemic blockade of 5HT 2A receptors with M100907 produces no apparent impairment in set-shifting (Rodefer et al, 2008) suggests that the effects of SCH23390 reported here are likely attributable to actions on NAc D 1 receptors.…”

Section: A Selective Role For Nac D 1 Receptors In Strategy Set-shiftingmentioning

confidence: 53%

Ventral Striatal Dopamine Modulation of Different Forms of Behavioral Flexibility

Haluk

Floresco

2009

Neuropsychopharmacol

182

174

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Different forms of behavioral flexibility are facilitated by interactions between separate regions of the prefrontal cortex and their striatal outputs. However, the contribution of ventral striatal dopamine (DA) to these functions is unclear. The present study assessed the involvement of DA receptors in the nucleus accumbens (NAc) core on either between-or within-strategy shifts using operant chamberbased tasks. Strategy set-shifting required rats initially to learn a visual-cue discrimination and, on the following day, shift to using an egocentric spatial response strategy to obtain reward. For reversal learning, rats were initially trained on a response discrimination and then required to select the opposite lever to receive food reward. Intra-NAc microinfusions of D 1 (SCH23390) but not D 2 (eticlopride) receptor antagonists impaired set-shifting, disrupting the maintenance of a new strategy. Conversely, supranormal activation of D 2 (quinpirole) but not D 1 (SKF81297) receptors also impaired set-shifting, inducing perseverative deficits. However, only infusions of the D 2 agonist impaired reversal learning, but did so without disrupting initial response learning. Thus, mesoaccumbens DA, acting on D 1 receptors, selectively facilitates complex forms of flexibility requiring shifts between different strategies, but does not appear to contribute to simpler forms of flexibility entailing shifts of specific stimulus-reward associations. In contrast, abnormal increases in D 2 receptor activity cause a more general impairment in behavioral flexibility. These findings suggest that deficits in these forms of executive functioning observed in disorders linked to dysfunction of the DA system may be attributable in part to aberrant increases or decreases in mesoaccumbens DA activity.

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“…It has been reported that haloperidol is ineffective whereas risperidone, olanzapine, and clozapine show nonsignificant trends toward improved ED-shift performance, and other antipsychotics, sertindole, and quetiapine show full reversal (Rodefer et al, 2008;Goetghebeur and Dias, 2009;Nikiforuk and Popik, 2012). In addition, studies of selective 5-HT receptor subtype antagonists indicate that the 5-HT 2A antagonist M100907 has borderline effects similar to risperidone whereas a 5-HT 6 antagonist [SB-271046, 5-chloro-N-[4-methoxy-3-(1-piperazinyl) phenyl]-3-methylbenzo[b]thiophene-2-sulfonamide hydrochloride] and 5-HT 7 antagonist [SB-269970, (R)-3-{2-[2-(4-methylpiperidin-1-yl)ethyl]pyrrolidin-1-ylsulfonyl}phenol] replicate the profile of sertindole (Rodefer et al, 2008;Nikiforuk et al, 2013). Therefore, the effect of brexpiprazole in this model would be associated with its potent 5-HT 2A and modest 5-HT 6 receptor antagonist activity (Maeda et al, 2014).…”

Section: Discussionmentioning

confidence: 99%

“…Subchronic PCP treatment is known to impair cognitive performance in various tests (Rodefer et al, 2008;Neill et al, 2010). Two tests were selected for characterization of brexpiprazole and aripiprazole in the present studies: NOR and ID-ED.…”

Section: Brexpiprazole Reverses Cognitive Deficits Induced By Subchromentioning

confidence: 99%

“…These latter strains have been shown to acquire cognitive tests faster and more reliably (Andrews et al, 1995). For this reason, the NOR test was validated using LH rats Redrobe et al, 2010), and the ID-ED test was validated with either LH (Goetghebeur and Dias, 2009) or LE rats (Rodefer et al, 2008). However, only the LE rat strain was available in the People's Republic of China, so it was selected for use in the ID-ED test.…”

Section: Subjectsmentioning

confidence: 99%

See 1 more Smart Citation

Brexpiprazole II: Antipsychotic-Like and Procognitive Effects of a Novel Serotonin-Dopamine Activity Modulator

Maeda¹,

Lerdrup²,

Sugino³

et al. 2014

J Pharmacol Exp Ther

Self Cite

108

116

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Brexpiprazole piperazin-1-yl]butoxy}quinolin-2(1H)-one) is a novel serotonin-dopamine activity modulator with partial agonist activity at serotonin 1A (5-HT 1A ) and D 2/3 receptors, combined with potent antagonist effects on 5-HT 2A , a 1B -, and a 2C -adrenergic receptors. Brexpiprazole inhibited conditioned avoidance response (ED 50 = 6.0 mg/kg), apomorphine-or D-amphetamine-induced hyperactivity (ED 50 = 2.3 and 0.90, respectively), and apomorphine-induced stereotypy (ED 50 = 2.9) in rats at clinically relevant D 2 receptor occupancies. Brexpiprazole also potently inhibited apomorphine-induced eye blinking in monkeys. The results suggest that brexpiprazole has antipsychotic potential. Brexpiprazole induced catalepsy (ED 50 = 20) well above clinically relevant D 2 receptor occupancies, suggesting a low risk for extrapyramidal side effects. Subchronic treatment with phencyclidine (PCP) induced cognitive impairment in both novel object recognition (NOR) and attentional set-shifting (ID-ED) tests in rats. Brexpiprazole reversed the PCP-induced cognitive impairment in the NOR test at 1.0 and 3.0 mg/kg, and in the ID-ED test at 1.0 mg/kg. However, aripiprazole (10 mg/kg) was ineffective in both tests, despite achieving relevant D 2 occupancies. In the NOR test,

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Reversal of Subchronic PCP-Induced Deficits in Attentional Set Shifting in Rats by Sertindole and a 5-HT6 Receptor Antagonist: Comparison Among Antipsychotics

Cited by 114 publications

References 65 publications

Animal models of cognitive dysfunction and negative symptoms of schizophrenia: Focus on NMDA receptor antagonism

Animal models of cognitive dysfunction and negative symptoms of schizophrenia: Focus on NMDA receptor antagonism

Ventral Striatal Dopamine Modulation of Different Forms of Behavioral Flexibility

Brexpiprazole II: Antipsychotic-Like and Procognitive Effects of a Novel Serotonin-Dopamine Activity Modulator

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