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首页> 外文期刊>Alcoholism: Clinical and experimental research >The alcohol deprivation effect in C57BL/6J mice is observed using operant self-administration procedures and is modulated by CRF-1 receptor signaling.
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The alcohol deprivation effect in C57BL/6J mice is observed using operant self-administration procedures and is modulated by CRF-1 receptor signaling.

机译:使用操作性自我给药程序可观察到C57BL / 6J小鼠的酒精剥夺作用,并受CRF-1受体信号传导调节。

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BACKGROUND: The alcohol deprivation effect (ADE) is characterized by transient excessive alcohol consumption upon reinstatement of ethanol following a period of ethanol deprivation. While this phenomenon has been observed in rats using both bottle drinking (consummatory behavior) and operant self-administration (consummatory and appetitive "ethanol-seeking" behavior) procedures, ADE studies in mice have primarily relied on bottle drinking measures. Furthermore, the neurochemical pathways that modulate the ADE are not well understood. Therefore, we determined whether the ADE can be observed in C57BL/6J mice using operant self-administration procedures and if expression of the ADE is modulated by the corticotropin releasing factor-1 (CRF-1) receptor. METHODS: C57BL/6J mice were trained in a 2-hour operant self-administration paradigm to lever press for 10% ethanol or water on separate response keys. Between operant sessions, mice had access to ethanol in their homecage. Once stable responding occurred, mice were deprived of ethanol for 4 days and were then retested with ethanol in the operant paradigm for 3 consecutive days. Next, to assess the role of the CRF-1 receptor, mice were given intraperitoneal (i.p.) injection (0, 10, or 20 mg/kg) of the CRF-1 receptor antagonist CP-154,526 30 minutes before ADE testing. Additional experiments assessed (i) ADE responding in which the alternate response lever was inactive, (ii) the effects of CP-154,526 on self-administration of a 1% sucrose solution following 4 days of deprivation, and (iii) ADE responding in which mice did not received i.p. injections throughout the experiment. RESULTS: Mice exhibited a significant increase in postdeprivation lever responding for ethanol with either a water reinforced or inactive alternate lever. Interestingly, i.p. injection of a 10 mg/kg dose of CP-154,526 protected against the ADE while not affecting lever responding for a sucrose solution. Finally, baseline and deprivation-induced increases of ethanol reinforced lever responding were greater in mice not given i.p. injections. CONCLUSIONS: The ADE in C57BL/6J mice can be modeled using the operant self-administration paradigm and increased ethanol self-administration associated with the ADE is modulated by CRF-1 receptor signaling.
机译:背景:酒精剥夺效应(ADE)的特征是在一段时间的乙醇剥夺之后,恢复乙醇后会短暂地过度消耗酒精。尽管已经在使用饮酒(消耗行为)和操作性自我管理(消耗性和食欲性的“寻求乙醇”行为)程序的大鼠中观察到了这种现象,但是在小鼠中进行的ADE研究主要依赖于饮酒措施。此外,调节ADE的神经化学途径还不太清楚。因此,我们确定是否可以使用操作性自我施用程序在C57BL / 6J小鼠中观察到ADE,以及ADE的表达是否受促肾上腺皮质激素释放因子1(CRF-1)受体调节。方法:C57BL / 6J小鼠在2小时的自我操作管理模式下接受训练,以分别按压10%的乙醇或水。在两次手术之间,小鼠可以在笼中接触乙醇。一旦出现稳定的反应,将小鼠剥夺乙醇4天,然后连续3天在操作范式中用乙醇重新测试。接下来,为了评估CRF-1受体的作用,在ADE测试前30分钟给小鼠腹膜内(i.p.)注射(0、10或20 mg / kg)CRF-1受体拮抗剂CP-154,526。其他实验评估(i)替代应答杠杆无效的ADE应答,(ii)剥夺4天后CP-154,526对1%蔗糖溶液自我给药的影响,以及(iii)ADE应答小鼠没有接受ip在整个实验过程中进行注射。结果:小鼠表现出剥夺后杠杆对乙醇的显着增加,无论是水强化还是无效的替代杠杆。有趣的是,注射10 mg / kg剂量的CP-154,526可以防止ADE,同时不影响蔗糖溶液的杠杆响应。最后,未给予腹膜内注射的小鼠基线和剥夺诱导的乙醇增强杠杆反应增加。注射。结论:C57BL / 6J小鼠的ADE可以使用操作性自我给药范例进行建模,而与ADE相关的乙醇自我给药的增加受CRF-1受体信号传导的调节。

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