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DREAM消融选择性地改变了四氢大麻酚引起的位置厌恶和镇痛作用,但吗啡的动机和镇痛作用保持不变。

DREAM ablation selectively alters THC place aversion and analgesia but leaves intact the motivational and analgesic effects of morphine.

作者信息

Cheng Hai-Ying M, Laviolette Steven R, van der Kooy Derek, Penninger Josef M

机构信息

Departments of Medical Biophysics and Immunology, University of Toronto, 610 University Avenue, Toronto, Ontario, Canada M5G 2M9.

出版信息

Eur J Neurosci. 2004 Jun;19(11):3033-41. doi: 10.1111/j.0953-816X.2004.03435.x.

Abstract

DREAM (downstream regulatory element antagonistic modulator) is a novel transcriptional repressor for the prodynorphin gene, and genetic deletion of DREAM in mice results in a phenotype of ongoing analgesia by virtue of its effect on opioid gene expression. In the present study, we evaluated the motivational effects of opioids (morphine), cannabinoids [Delta(9)-tetrahydrocannabinol (THC)] and cocaine in mice lacking the dream gene (dream(-/-)). The aversive effects of THC were potentiated in dream(-/-) mice in a kappa-opioid receptor-dependent fashion, whereas morphine reward and the aversive effects of morphine withdrawal remained intact. The rewarding and aversive effects of cocaine were likewise unperturbed in dream(-/-) mice. Moreover, the aversive properties of lithium chloride and naloxone were unaffected by the absence of DREAM, indicating that the effect of DREAM on THC-induced dysphoria is not due to a general involvement in the behavioral response to aversive stimuli. Additionally, physical dependence to morphine and the locomotor-sensitizing effects of cocaine were unaltered in these animals. Finally, whereas the absence of DREAM reduced the analgesic efficacy of THC, morphine analgesia was unaffected in dream(-/-) mice.

摘要

DREAM(下游调节元件拮抗调节剂)是前强啡肽基因的一种新型转录抑制因子,小鼠体内DREAM基因的缺失因其对阿片类基因表达的影响而导致持续镇痛的表型。在本研究中,我们评估了阿片类药物(吗啡)、大麻素[Δ⁹-四氢大麻酚(THC)]和可卡因对缺乏dream基因(dream⁻/⁻)的小鼠的动机效应。THC的厌恶效应在dream⁻/⁻小鼠中以κ-阿片受体依赖性方式增强,而吗啡奖赏和吗啡戒断的厌恶效应保持不变。可卡因的奖赏和厌恶效应在dream⁻/⁻小鼠中同样未受干扰。此外,氯化锂和纳洛酮的厌恶特性不受DREAM缺失的影响,这表明DREAM对THC诱导的烦躁不安的影响并非由于其普遍参与对厌恶刺激的行为反应。另外,这些动物对吗啡的身体依赖性和可卡因的运动致敏作用未改变。最后,虽然DREAM的缺失降低了THC的镇痛效果,但吗啡镇痛在dream⁻/⁻小鼠中未受影响。

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