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Chronic valproate attenuates some but not all facets of mania-like behavior in mice

机译:慢性valproate衰减一些但不是全部在老鼠中的躁狂症行为的方面

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摘要

Bipolar Disorder (BD) mania is a psychiatric disorder with multifaceted symptoms. Development of targeted treatments for BD mania may benefit from animal models that mimic multiple symptoms, as opposed to hyperactivity alone. Using the reverse-translated multivariate exploratory paradigm, the Behavioral Pattern Monitor (BPM), we reported that patients with BD mania exhibit hyperactivity as well as increased specific exploration and more linear movements through space. This abnormal profile is also observed in mice with reduced function of the dopamine transporter (DAT) through either constitutive genetic (knockdown (KD)) or acute pharmacological (GBR12909) means. Here, we assessed the pharmacological predictive validity of these models by administering the BD-treatment valproic acid (VPA) for 28 days. After 28 days of 1.5% VPA- or regular-chow treatment, C57BL/6J mice received GBR12909 (9 mg/kg) or saline and were tested in the BPM. Similarly, DAT KD and WT littermates were treated with VPA-chow and tested in the BPM. GBR12909-treated and DAT KD mice on regular chow were hyperactive, exhibited increased specific exploration, and moved in straighter patterns compared to saline-treated and WT mice respectively. Chronic 1.5% VPA-chow treatment resulted in therapeutic concentrations of VPA and ameliorated hyperactivity in both models, while specific exploration and behavioral organization remained unaffected. Hence, the mania-like profile of mice with reduced functional DAT was partially attenuated by chronic VPA treatment, consistent with the incomplete symptomatic effect of VPA treatment in BD patients. Both DAT models may help to identify therapeutics that impact the full spectrum of BD mania.
机译:躁郁症(BD)躁狂症是一种具有多种症状的精神病。 BD躁狂症的靶向治疗方法的开发可能受益于模仿多种症状的动物模型,而不是单纯的过度活跃。我们使用反向翻译的多元探索范式,行为模式监控器(BPM),报道了BD躁狂症患者表现出活动亢进,以及特定的探查增加和在空间中更多的线性运动。在多巴胺转运蛋白(DAT)功能降低的小鼠中,也通过组成型遗传学(敲除(KD)(Knockdown)(KD))或急性药理学(GBR12909)手段观察到这种异常情况。在这里,我们通过给予BD治疗的丙戊酸(VPA)28天来评估这些模型的药理学预测有效性。在接受1.5%VPA或常规咀嚼的28天后,C57BL / 6J小鼠接受了GBR12909(9 mg / kg)或生理盐水,并在BPM中进行了测试。同样,将DAT KD和WT同窝仔用VPA-chow处理并在BPM中进行测试。与生理盐水处理和WT小鼠相比,GBR12909处理的DAT KD小鼠和DAT KD正常饮食小鼠活动过度,表现出更高的特异性探查,并且以更直的方式运动。在两种模型中,慢性1.5%VPA吞咽治疗均导致VPA的治疗浓度和改善的多动症,而特定的探索和行为组织仍然不受影响。因此,功能性DAT降低的小鼠的躁狂样特征通过慢性VPA治疗而部分减弱,这与BD患者中VPA治疗的不完全症状效应一致。两种DAT模型都可能有助于确定影响BD躁狂症全谱的疗法。

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