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黑色素聚集激素对奥氮平抑制雄性小鼠的运动活动是必需的。

Melanin-concentrating hormone is necessary for olanzapine-inhibited locomotor activity in male mice.

作者信息

Chee Melissa J S, Douris Nicholas, Forrow Avery B, Monnard Arnaud, Lu Shuangyu, Flaherty Stephen E, Adams Andrew C, Maratos-Flier Eleftheria

机构信息

Division of Endocrinology, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, MA 02115, USA.

Division of Endocrinology, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, MA 02115, USA.

出版信息

Eur Neuropsychopharmacol. 2015 Oct;25(10):1808-16. doi: 10.1016/j.euroneuro.2015.05.010. Epub 2015 Jun 3.

Abstract

Olanzapine (OLZ), an atypical antipsychotic, can be effective in treating patients with restricting type anorexia nervosa who exercise excessively. Clinical improvements include weight gain and reduced pathological hyperactivity. However the neuronal populations and mechanisms underlying OLZ actions are not known. We studied the effects of OLZ on hyperactivity using male mice lacking the hypothalamic neuropeptide melanin-concentrating hormone (MCHKO) that are lean and hyperactive. We compared the in vivo effects of systemic or intra-accumbens nucleus (Acb) OLZ administration on locomotor activity in WT and MCHKO littermates. Acute systemic OLZ treatment in WT mice significantly reduced locomotor activity, an effect that is substantially attenuated in MCHKO mice. Furthermore, OLZ infusion directly into the Acb of WT mice reduced locomotor activity, but not in MCHKO mice. To identify contributing neuronal mechanisms, we assessed the effect of OLZ treatment on Acb synaptic transmission ex vivo and in vitro. Intraperitoneal OLZ treatment reduced Acb GABAergic activity in WT but not MCHKO neurons. This effect was also seen in vitro by applying OLZ to acute brain slices. OLZ reduced the frequency and amplitude of GABAergic activity that was more robust in WT than MCHKO Acb. These findings indicate that OLZ reduced Acb GABAergic transmission and that MCH is necessary for the hypolocomotor effects of OLZ.

摘要

奥氮平(OLZ)是一种非典型抗精神病药物,对治疗过度运动的限制型神经性厌食症患者可能有效。临床改善包括体重增加和病理性多动减少。然而,OLZ作用的神经元群体和机制尚不清楚。我们使用缺乏下丘脑神经肽黑色素浓缩激素(MCHKO)的雄性小鼠(这些小鼠体型消瘦且多动)研究了OLZ对多动的影响。我们比较了全身或伏隔核(Acb)内注射OLZ对野生型(WT)和MCHKO同窝小鼠运动活动的体内效应。野生型小鼠急性全身注射OLZ可显著降低运动活动,而在MCHKO小鼠中这种效应明显减弱。此外,直接向野生型小鼠的Acb内注入OLZ可降低运动活动,但对MCHKO小鼠无效。为了确定相关的神经元机制,我们评估了OLZ治疗对离体和在体Acb突触传递的影响。腹腔注射OLZ可降低野生型而非MCHKO神经元的Acb GABA能活性。在急性脑片上应用OLZ也可在体外观察到这种效应。OLZ降低了GABA能活性的频率和幅度,野生型Acb中的这种作用比MCHKO Acb更明显。这些发现表明,OLZ降低了Acb GABA能传递,且MCH对于OLZ的运动减少效应是必需的。

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