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μ阿片受体信号传导与内吞作用的功能解离:对阿片类药物耐受性和成瘾生物学的影响。

Functional dissociation of mu opioid receptor signaling and endocytosis: implications for the biology of opiate tolerance and addiction.

作者信息

Whistler J L, Chuang H H, Chu P, Jan L Y, von Zastrow M

机构信息

Department of Cellular and Molecular Pharmacology, University of California, San Francisco, 94143, USA.

出版信息

Neuron. 1999 Aug;23(4):737-46. doi: 10.1016/s0896-6273(01)80032-5.

Abstract

Opiate analgesia, tolerance, and addiction are mediated by drug-induced activation of the mu opioid receptor. A fundamental question in addiction biology is why exogenous opiate drugs have a high liability for inducing tolerance and addiction while native ligands do not. Studies indicate that highly addictive opiate drugs such as morphine are deficient in their ability to induce the desensitization and endocytosis of receptors. Here, we demonstrate that this regulatory mechanism reveals an independent functional property of opiate drugs that can be distinguished from previously established agonist properties. Moreover, this property correlates with agonist propensity to promote physiological tolerance, suggesting a fundamental revision of our understanding of the role of receptor endocytosis in the biology of opiate drug action and addiction.

摘要

阿片类镇痛药、耐受性和成瘾性是由药物诱导的μ阿片受体激活介导的。成瘾生物学中的一个基本问题是,为什么外源性阿片类药物具有很高的诱导耐受性和成瘾性的倾向,而内源性配体却不会。研究表明,吗啡等高度成瘾的阿片类药物在诱导受体脱敏和内吞作用方面能力不足。在此,我们证明这种调节机制揭示了阿片类药物一种独立的功能特性,该特性可与先前确立的激动剂特性区分开来。此外,这种特性与激动剂促进生理耐受性的倾向相关,这表明我们对受体内吞作用在阿片类药物作用和成瘾生物学中的作用的理解需要进行根本性的修正。

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