首页> 美国卫生研究院文献>Frontiers in Behavioral Neuroscience >5-HT1B receptor agonist enhances breakpoint for cocaine on a progressive ratio (PR) schedule during maintenance of self-administration in female rats but reduces breakpoint for sucrose
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5-HT1B receptor agonist enhances breakpoint for cocaine on a progressive ratio (PR) schedule during maintenance of self-administration in female rats but reduces breakpoint for sucrose

机译:5-HT1B 受体激动剂在维持雌性大鼠自我给药期间以渐进比率 (PR) 时间表提高可卡因的断点但降低蔗糖的断点

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摘要

Background: Previous research showed that the 5-HT1B receptor agonist CP94253 enhanced cocaine reinforcement rate during maintenance of daily self-administration (SA), but inhibited reinforcement rate after 21 days of abstinence in male rats. Here we examined whether female rats show similar effects of CP94253 during maintenance as males across estrous cycle phases.Methods: Female rats trained on a fixed ratio 5 (FR5) cocaine reinforcement schedule were tested for the effects of CP94253 (5.6 mg/kg, s.c.) on cocaine reinforcement rate during each phase of the estrous cycle, with access to either low (0.075 and 0.1875) or high (0.375 and 0.75) cocaine doses available for 1 h sequentially in descending dose order. Other female and male rats trained on a progressive ratio (PR) schedule of cocaine or sucrose reinforcement were tested for CP94253 (0, 3.2, 5.6, and 10 mg/kg, s.c.) effects on reinforcement rate in 3-h sessions. CP94253 effects on responding during sucrose cue-reactivity were also examined post-abstinence.Results: Regardless of sex, CP94253 enhanced breakpoints on the PR schedule during maintenance of cocaine SA but attenuated breakpoints for sucrose reinforcement and decreased responding during sucrose cue-reactivity. FR results showed that CP94253 attenuated cocaine reinforcement rate during all estrous cycle phases except metestrus.Conclusions: Overall, we suggest that CP94253 increased incentive motivation for cocaine during maintenance of SA in female and male rats, yet decreased motivation for sucrose. We also suggest that 5-HT1BRs modulate motivation similarly across sexes except when females are in metestrus.
机译:背景: 既往研究表明,5-HT1B 受体激动剂CP94253增强雄性大鼠维持日常自我给药 (SA) 期间的可卡因强化率,但抑制了雄性大鼠戒断 21 天后的强化率。在这里,我们检查了雌性大鼠在维持期间是否表现出与雄性大鼠在发情周期阶段相似的 CP94253 效果。方法:测试以固定比例 5 (FR5) 可卡因强化计划训练的雌性大鼠在发情周期的每个阶段CP94253 (5.6 mg/kg, sc) 对可卡因强化率的影响,可获得低 (0.075 和 0.1875) 或高 (0.375 和 0.75) 可卡因剂量剂量 1 小时。在 3 小时疗程中,测试了以可卡因或蔗糖强化的渐进比率 (PR) 方案训练的其他雌性和雄性大鼠对 CP94253 (0、3.2、5.6 和 10 mg/kg,sc.c.) 对强化率的影响。还检查了戒断后对蔗糖提示反应性反应的CP94253影响。结果: 无论性别如何,CP94253 在可卡因 SA 维持期间增强了 PR 计划的断点,但减弱了蔗糖强化的断点,并在蔗糖提示反应性期间降低了反应。FR 结果显示,CP94253 在除 metestrus 外的所有发情周期阶段均减弱了可卡因强化率。结论: 总体而言,我们认为CP94253雌性和雄性大鼠维持 SA 期间可卡因的激励动机增加,但对蔗糖的动机降低。我们还表明,5-HT1BRs 在两性之间对动机的调节相似,除非女性处于 metestrus 中。

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