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研究药物成瘾和精神兴奋剂药物影响的转基因小鼠。

Transgenic mice in the study of drug addiction and the effects of psychostimulant drugs.

机构信息

Department of Biological Psychiatry, Tohoku University Graduate School of Medicine, Sendai, Japan.

出版信息

Ann N Y Acad Sci. 2010 Feb;1187:218-46. doi: 10.1111/j.1749-6632.2009.05276.x.

Abstract

The first transgenic models used to study addiction were based upon a priori assumptions about the importance of particular genes in addiction, including the main target molecules of morphine, amphetamine, and cocaine. This consequently emphasized the importance of monoamine transporters, opioid receptors, and monoamine receptors in addiction. Although the effects of opiates were largely eliminated by mu opioid receptor gene knockout, the case for psychostimulants was much more complex. Research using transgenic models supported the idea of a polygenic basis for psychostimulant effects and has associated particular genes with different behavioral consequences of psychostimulants. Phenotypic analysis of transgenic mice, especially gene knockout mice, has been instrumental in identifying the role of specific molecular targets of addictive drugs in their actions. In this article, we summarize studies that have provided insight into the polygenic determination of drug addiction phenotypes in ways that are not possible with other methods, emphasizing research into the effects of psychostimulant drugs in gene knockouts of the monoamine transporters and monoamine receptors.

摘要

用于研究成瘾的第一代转基因模型是基于对特定基因在成瘾中的重要性的先验假设,包括吗啡、安非他命和可卡因的主要靶分子。这就强调了单胺转运体、阿片受体和单胺受体在成瘾中的重要性。尽管阿片类药物的作用在很大程度上被 mu 阿片受体基因敲除所消除,但精神兴奋剂的情况要复杂得多。使用转基因模型的研究支持了精神兴奋剂作用的多基因基础的观点,并将特定基因与精神兴奋剂的不同行为后果联系起来。转基因小鼠,特别是基因敲除小鼠的表型分析,对于确定成瘾药物特定分子靶点在其作用中的作用至关重要。在本文中,我们总结了一些研究,这些研究以其他方法不可能的方式提供了对药物成瘾表型的多基因决定的深入了解,强调了对单胺转运体和单胺受体基因敲除的精神兴奋剂药物作用的研究。

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