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Role of the Orbitofrontal Cortex and Dorsal Striatum in Regulating the Dose-Related Effects of Self-Administered Cocaine

机译:眶额皮质和背侧纹状体在调节可卡因剂量相关效应中的作用

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摘要

Little is known regarding which neural systems regulate dose-related changes in responding maintained by self-administered cocaine. This empirical question is important because elucidating neural systems engaged in this process could provide clues for effectively treating cocaine addiction. It has been suggested that different cocaine doses represent reinforcers of differing magnitudes, implicating the dorsal striatum or orbitofrontal cortex as important. Rats were trained to self-administer 1.0 mg/kg cocaine under a fixed-interval based second-order schedule. Next, cocaine unit doses (0.1–3.0 mg/kg) were each non-systematically available for a 5-day block of sessions. Tests (1-hr) were conducted on day 3 (vehicle) and day 5 (100 μg lidocaine) of each block. Lidocaine inactivation of the lateral dorsal striatum had no effect on dose-related responding or cocaine intake. In contrast, when doses along the ascending limb were available for self-administration, lidocaine inactivation of the lateral orbitofrontal cortex caused reductions in responding and cocaine intake, resulting in overall flattening of dose-response curves. This included reductions during the entire 1-hr test sessions and during the interval immediately following the first cocaine infusion of test sessions. Lidocaine inactivation of the lateral orbitofrontal cortex did not alter responding during the first cocaine-free interval of test sessions, but increased the latency to the first infusion. Collectively, the findings suggest that when the amount of experience with different cocaine unit doses is limited to a few sessions, the lateral orbitofrontal cortex regulates the dose-related effects of self-administered cocaine, likely by processing information pertaining to the reinforcing value of each unit dose.
机译:关于哪种神经系统调节由自我管理的可卡因维持的反应中剂量相关变化知之甚少。这个经验性问题很重要,因为阐明参与此过程的神经系统可以提供有效治疗可卡因成瘾的线索。有人建议,不同剂量的可卡因代表不同强度的加强剂,暗示背纹状体或眶额皮质很重要。训练大鼠以固定间隔的二阶时间表自我给药1.0 mg / kg可卡因。接下来,在为期5天的疗程中,非全身均可使用可卡因单位剂量(0.1-3.0 mg / kg)。在每个区块的第3天(车辆)和第5天(100μg利多卡因)进行测试(1小时)。利多卡因使背侧外侧纹状体失活对剂量相关反应或可卡因摄入量没有影响。相反,当沿上肢的剂量可自行给药时,利多卡因使眶额叶外侧皮质失活会导致反应和可卡因的摄入减少,从而导致剂量反应曲线总体趋于平坦。这包括在整个1小时的测试期间以及首次注入可卡因之后的时间间隔内的减少。在第一个无可卡因间隔的测试期间,外侧眶额皮质的利多卡因失活没有改变反应,但增加了第一次输注的潜伏期。总的来说,研究结果表明,当可卡因单位剂量的使用经验仅限于几次疗程时,眼眶额叶皮层可能调节可卡因的剂量相关作用,这可能是通过处理与每种可卡因的增值有关的信息来进行的。单位剂量。

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