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Brexpiprazole reduces hyperactivity, impulsivity, and risk-preference behavior in mice with dopamine transporter knockdown-a model of mania. | LitMetric

AI Article Synopsis

  • Bipolar disorder is characterized by episodes of depression and mania, leading to cognitive deficits like impulsivity and risky decision-making that current treatments don't fully address.
  • Brexpiprazole, a drug with serotonin and dopamine modulating effects, was tested in a mouse model to evaluate its impact on mania-related behaviors, specifically focusing on activity levels and decision-making in risk scenarios.
  • The study found that brexpiprazole reduced hyperactivity and impulsivity in mice with mania-like traits, suggesting it may be a promising treatment for managing symptoms of bipolar disorder and related impulsivity disorders.

Article Abstract

Rationale: Bipolar disorder (BD) is a unique mood disorder defined by periods of depression and mania. The defining diagnosis of BD is the presence of mania/hypomania, with symptoms including hyperactivity and risk-taking. Since current treatments do not ameliorate cognitive deficits such as risky decision-making, and impulsivity that can negatively affect a patient's quality of life, better treatments are needed.

Objectives: Here, we tested whether acute treatment with brexpiprazole, a serotonin-dopamine activity modulator with partial agonist activity at D and 5-HT receptors, would attenuate the BD mania-relevant behaviors of the dopamine transporter (DAT) knockdown mouse model of mania.

Methods: The effects of brexpiprazole on DAT knockdown and wild-type littermate mice were examined in the behavioral pattern monitor (BPM) and Iowa gambling task (IGT) to quantify activity/exploration and impulsivity/risk-taking behavior respectively.

Results: DAT knockdown mice exhibited hyper-exploratory behavior in the BPM and made fewer safe choices in the IGT. Brexpiprazole attenuated the mania-like hyper-exploratory phenotype and increased safe choices in risk-preferring DAT knockdown mice. Brexpiprazole also reduced safe choices in safe-preferring mice irrespective of genotype. Finally, brexpiprazole reduced premature (impulsive-like) responses in both groups of mice.

Conclusions: Consistent with earlier reports, DAT knockdown mice exhibited hyper-exploratory, risk-preferring, and impulsive-like profiles consistent with patients with BD mania in these tasks. These behaviors were attenuated after brexpiprazole treatment. These data therefore indicate that brexpiprazole could be a novel treatment for BD mania and/or risk-taking/impulsivity disorders, since it remediates some relevant behavioral abnormalities in this mouse model.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5391249PMC
http://dx.doi.org/10.1007/s00213-017-4543-7DOI Listing

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