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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >An examination of d-amphetamine self-administration in pedunculopontine tegmental nucleus-lesioned rats.
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An examination of d-amphetamine self-administration in pedunculopontine tegmental nucleus-lesioned rats.

机译:对小足蛇形被膜被膜损伤的大鼠进行d-苯异丙胺自我给药的检查。

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The pedunculopontine tegmental nucleus (PPTg) has long been suggested to have a role in reward-related behaviour, and there is particular interest in its possible role in drug reward systems. Previous work found increased i.v. self-administration (IVSA) of d-amphetamine following PPTg lesions when training had included both operant pre-training and priming injections. The present study examined the effect of excitotoxin lesions of the PPTg on d-amphetamine IVSA under three training conditions. Naive: no previous experience of d-amphetamine or operant responding. Pre-trained: given operant training with food before lesion surgery took place. Primed: given single non-contingent d-amphetamine infusion (0.1 mg/0.l ml) at the start of each session. Rats in all conditions were given either ibotenate or phosphate buffer control lesions of the PPTg before d-amphetamine (0.1 mg/0.1 ml infusion) IVSA training took place. Rats received eight sessions of training under a fixed ratio (FR2) schedule of d-amphetamineIVSA, followed by four sessions under a progressive ratio (PR5) schedule. In the naive condition, PPTg-lesioned rats were attenuated in their responding under FR2, and took significantly fewer infusions under PR5 than the control group. Under FR2 in the pre-trained condition, there was no difference between PPTg excitotoxin and control lesioned rats; however, PPTg-lesioned rats took significantly fewer infusions under the PR5 schedule. In the primed condition, there were no differences between PPTg-lesioned and control rats under either FR2 or PR5 schedules. These data demonstrate that operant training prior to PPTg lesion surgery corrects some, but not all, of the deficits seen in the naive condition. PPTg-lesioned rats in both naive and pre-trained conditions showed reduced responding for d-amphetamine under a PR5 schedule. These deficits are overcome by priming with d-amphetamine. We suggest that alterations in striatal dopamine activity following PPTg lesions underlie these effects.
机译:长期以来,人们提出了人足桥骨被盖核(PPTg)在与奖励有关的行为中起作用,并且人们对其在药物奖励系统中的可能作用特别感兴趣。发现以前的工作增加了i.v. PPTg损伤后,当训练同时包括手术前训练和初免注射时,d-苯异丙胺的自我管理(IVSA)。本研究在三种训练条件下研究了PPTg的兴奋毒素损伤对d-苯异丙胺IVSA的影响。天真:没有d-苯异丙胺或操作员响应的经验。预先培训:在进行病变手术之前,先对食物进行操作培训。灌注:在每个疗程开始时进行一次非特效d-苯异丙胺输注(0.1 mg / 0.1 ml)。在进行d-苯异丙胺(0.1 mg / 0.1 ml输注)IVSA训练之前,在所有条件下的大鼠均接受了PPTg的ibotenate或磷酸盐缓冲液对照损伤。大鼠在d-苯丙胺IVSA固定比例(FR2)时间表下接受了八次训练,然后在渐进比例(PR5)时间表下接受了四次训练。在幼稚的条件下,PPTg损伤的大鼠在FR2下的反应减弱,并且在PR5下的输注量明显少于对照组。在FR2的预训练条件下,PPTg兴奋性毒素与对照组大鼠无差异。然而,根据PR5时间表,PPTg损伤的大鼠的输注量明显减少。在致敏条件下,在FR2或PR5方案下,PPTg损伤的大鼠与对照组之间没有差异。这些数据表明,在进行PPTg病变手术之前进行操作性训练可以纠正一些(但不是全部)幼稚状态下的缺陷。 PPRg损伤的大鼠在幼稚和预先训练的条件下,在PR5时间表下对d-苯异丙胺的反应均降低。这些缺陷可以通过用d-苯异丙胺引发来克服。我们建议,PPTg损伤后纹状体多巴胺活性的改变是这些作用的基础。

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