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Sex differences in response to amphetamine in adult Long-Evans rats performing a delay-discounting task

机译:成年Long-Evans大鼠执行延迟折扣任务后对苯丙胺的反应性别差异

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摘要

The use of animal models to investigate experimental questions about impulsive behavior can provide valuable insight into problems that affect human health. The delay-discounting paradigm involves subjects choosing between smaller reinforcers delivered immediately and larger reinforcers that are delivered after a delay. This is an important experimental paradigm for examining impulsive choice in both laboratory species and humans. However, a shortcoming of previously published delay-discounting studies in animals is that typically only males were studied, reducing the applicability of these studies to human populations. In the present study, both female and male adult Long-Evans rats were trained to perform a delay-discounting task, with delays of 0, 5, 10, 20 and 40 s before delivery of the larger reinforcer. Because dopaminergic signaling is important in mediating this task, the effects of d-amphetamine and the dopamine receptor antagonist, cis-flupenthixol, on task performance were then examined. The main experimental measure was percent larger-reinforcer choice, which was defined as the percentage of experimental trials at each delay in which the delayed, larger reinforcer was chosen. There was not a sex difference in percent larger-reinforcer choice during baseline performance of the task. However, d-amphetamine administration disrupted choice in females, as evidenced by < 80% larger-reinforcer choice in half of the females, but none of the males, at 0.5 mg/kg. d-Amphetamine also differentially altered the latency to choose between immediate versus delayed reinforcers in females compared to males. In contrast, cis-flupenthixol did not have a sex-related effect on percent larger-reinforcer choice. These findings parallel the sex differences in response to amphetamine seen in human delay-discounting studies and underscore the importance of evaluating sex-based differences in baseline performance and in response to pharmacologic agents when utilizing animal models.
机译:使用动物模型调查有关冲动行为的实验问题可以为影响人类健康的问题提供有价值的见解。延迟折扣范例涉及对象在立即交付的较小增强器和延迟之后交付的较大增强器之间进行选择。这是检查实验室物种和人类冲动选择的重要实验范式。但是,以前发表的动物延迟折扣研究的一个缺点是通常只对雄性动物进行研究,从而降低了这些研究对人群的适用性。在本研究中,成年的Long-Evans雌性和雄性大鼠均经过训练以执行延迟折扣任务,延迟期为0、5、10、20和40 s,然后再交付较大的增强器。由于多巴胺能信号传导在介导这项任务中很重要,因此,我们考察了d-苯异丙胺和多巴胺受体拮抗剂顺式氟戊醇对任务执行的影响。主要的实验方法是选择较大的增强剂,该百分比定义为每次延迟的实验试验的百分比,其中选择了延迟的较大增强剂。在任务的基准执行期间,较大型钢筋的选择百分比没有性别差异。然而,d-苯丙胺的给药干扰了雌性的选择,0.5毫克/千克的一半雌性中<80%的增强剂选择证明了这一点,而雄性中没有一种。与男性相比,d-苯丙胺还差异性地改变了女性在立即或延迟补强之间选择的潜伏期。相比之下,顺氟哌丁醇对大剂量补强剂的选择没有性别相关的影响。这些发现与在人类延迟折扣研究中看到的对安非他明的反应中的性别差异相似,并强调了在使用动物模型时评估基于基线的性能和药理剂反应中基于性别的差异的重要性。

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