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Opiate and cocaine addiction: from bench to clinic and back to the bench.

机译:阿片和可卡因成瘾:从板凳到诊所再到板凳。

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摘要

This review primarily focuses on our recent findings in bidirectional translational research on opiate and cocaine addictions. First, we present neurobiological and molecular studies on endogenous opioid systems (e.g. proopiomelanocortin, mu opioid receptor, dynorphin, and kappa opioid receptor), brain stress-responsive systems (e.g. orexin, arginine vasopressin, V1b receptor, and corticotropin-releasing factor), hypothalamic-pituitary-adrenal axis, and neurotransmitters (especially dopamine), in response to both chronic cocaine or opiate exposure and to drug withdrawal, using several newly developed animal models and molecular approaches. The second aspect is human molecular genetic association investigations including hypothesis-driven studies and genome-wide array studies, to define particular systems involved in vulnerability to develop specific addictions, and response to pharmacotherapy.
机译:这篇综述主要集中在我们最近对鸦片和可卡因成瘾的双向转化研究中的发现。首先,我们对内源性阿片系统(例如proopiomelanocortin,μ阿片受体,强啡肽和kappa阿片受体),脑应激反应系统(例如食欲素,精氨酸加压素,V1b受体和促肾上腺皮质激素释放因子)进行神经生物学和分子研究,下丘脑-垂体-肾上腺轴和神经递质(特别是多巴胺),使用几种新近开发的动物模型和分子方法,对慢性可卡因或鸦片暴露以及戒断药物都有反应。第二个方面是人类分子遗传协会研究,包括假设驱动的研究和全基因组阵列研究,以定义参与发展特定成瘾性和对药物疗法反应的脆弱性的特定系统。

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