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Elevated dopamine D1 receptor availability in striatum of Göttingen minipigs after electroconvulsive therapy

机译:电痉挛治疗后哥廷根小型猪纹状体中多巴胺D1受体的利用率升高

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摘要

Electroconvulsive therapy (ECT), a direct form of brain stimulation, is an effective antidepressant. We hypothesized that the beneficial effects of ECT are mediated by increased dopaminergic neurotransmission, in which the baseline activity of D1 receptors may predict the response to ECT. We established a novel model of brain stimulation in Göttingen minipigs based on the protocol of ECT applied in humans. With positron emission tomography (PET), we determined a measure of dopaminergic neurotransmission with the dopamine D1 receptor antagonist [11C]. Seven minipigs were anesthetized and completed PET at baseline, prior to the onset of ECT treatment, and at 24–48 h and 8–10 days after the end of a clinical course of ECT, consisting of 10 ECT sessions over a 3.5-week period. In all pigs, the binding of [11C] to striatal D1 receptors had increased by 24–48 h after ECT, and in most, binding returned towards baseline at 8–10 days. Increased binding was observed in inverse proportion to baseline binding rates. Increased binding to dopamine D1 receptors suggests facilitation of dopaminergic neurotransmission, which may contribute to the therapeutic effects of ECT. Importantly, the baseline binding capacity of D1 receptors predicts the magnitude of increased binding, up to a maximum binding capacity.
机译:电惊厥疗法(ECT)是大脑刺激的一种直接形式,是一种有效的抗抑郁药。我们假设ECT的有益作用是由多巴胺能神经传递增加介导的,其中D1受体的基线活性可以预测对ECT的反应。我们基于适用于人类的ECT协议建立了哥廷根小型猪的新型脑刺激模型。通过正电子发射断层扫描(PET),我们确定了使用多巴胺D1受体拮抗剂[ 11 C]进行多巴胺能神经传递的方法。麻醉七只小猪,并在ECT治疗开始之前的基线,以及ECT临床过程结束后的24–48–h和8–10天,完成PET,包括3.5周内的10次ECT疗程。在所有猪中,[ 11 C]与纹状体D1受体的结合在ECT后增加了24–48 h,并且大多数情况下,结合在8–10天回到基线。观察到结合增加与基线结合速率成反比。与多巴胺D1受体的结合增加表明促进多巴胺能神经传递,这可能有助于ECT的治疗作用。重要的是,D1受体的基线结合能力可预测结合增加的幅度,直至最大结合能力。

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