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可卡因自我给药过程中神经活动的波动:脑温记录提供的线索。

Fluctuations in neural activity during cocaine self-administration: clues provided by brain thermorecording.

作者信息

Kiyatkin E A, Brown P L

机构信息

Behavioral Neuroscience Branch, Intramural Research Program, National Institute on Drug Abuse, 5500 Nathan Shock Drive, Baltimore, MD 21224, USA.

出版信息

Neuroscience. 2003;116(2):525-38. doi: 10.1016/s0306-4522(02)00711-x.

Abstract

Since metabolic neural activity is accompanied by heat release, measurement of local brain temperature offers a method for assessing alterations in neural activity. This approach, continuous monitoring of local brain (ventral tegmental area, ventral striatum, and hippocampus) and body (temporal muscle) temperature, was used to study intravenous cocaine self-administration in trained rats. The first self-administration of a session was preceded by a strong temperature increase that continued after the drug infusion. After peaking at the time of the second self-administration, temperature plateaued (+0.7 degrees C) with biphasic fluctuations (+/-0.10-0.15 degrees C) around each subsequent self-administration. Temperature gradually increased before and for 30-50 s after the lever-press, but then abruptly decreased to a minimum at 180-240 s, when it began to increase to reach another peak immediately after the next lever-press. Doubling the dose of injected cocaine significantly potentiated the post-cocaine temperature decrease and increased time to the next lever-press. In contrast to drug-reinforced lever-presses, temperatures phasically increased after non-reinforced lever-presses and at the end of a session when the lever was blocked and the rat was hyperactive, trying to reach the inaccessible lever. While temperature changes in each recording location were generally correlative, the initial temperature elevation was stronger in all brain structures than in muscle and ventral striatum was the structure that showed the most pronounced and consistent temperature fluctuations. These data suggest a generalized brain activation associated with cocaine-seeking and cocaine-taking behavior with its phasic fluctuations around individual drug self-injections. While the initial component of brain activation preceding the first lever-press for cocaine is internally determined and closely related to behavioral search, subsequent biphasic fluctuations in neural activity associated with repeated drug intakes appear to be drug-mediated. Cocaine-induced potentiation of monoamine transmission is a possible factor for gradual increases in neural activity that drive cocaine seeking, while a rapid, brain concentration-dependent action on Na(+) transport (local anesthetic action) is the most probable factor determining an abrupt, transient cessation of neural activation associated with cocaine reward.

摘要

由于代谢性神经活动伴随着热量释放,测量局部脑温提供了一种评估神经活动变化的方法。这种方法,即连续监测局部脑(腹侧被盖区、腹侧纹状体和海马体)和身体(颞肌)温度,被用于研究训练有素的大鼠静脉注射可卡因自我给药的情况。在一次给药过程中,首次自我给药之前会出现强烈的体温升高,这种升高在药物注射后仍会持续。在第二次自我给药时达到峰值后,体温会趋于平稳(升高0.7摄氏度),随后每次自我给药时都会出现双相波动(±0.10 - 0.15摄氏度)。在杠杆按压前及按压后30 - 50秒内体温会逐渐升高,但随后会在180 - 240秒时突然降至最低,然后在下一次杠杆按压后立即开始升高并达到另一个峰值。将注射可卡因的剂量加倍会显著增强可卡因注射后的体温下降,并延长至下一次杠杆按压的时间。与药物强化的杠杆按压不同,在非强化杠杆按压后以及在实验结束时,当杠杆被阻挡且大鼠过度活跃试图够到够不着的杠杆时,体温会出现相位性升高。虽然每个记录位置的温度变化通常具有相关性,但所有脑结构中的初始体温升高都比肌肉中的更强,并且腹侧纹状体是显示出最明显和一致的温度波动的结构。这些数据表明,与寻求可卡因和服用可卡因行为相关的是一种全身性的脑激活,且在每次个体药物自我注射时会出现相位性波动。虽然在首次按压杠杆获取可卡因之前的脑激活初始成分是由内部决定的,并且与行为搜索密切相关,但与重复药物摄入相关的神经活动随后的双相波动似乎是由药物介导的。可卡因诱导的单胺传递增强是驱动可卡因寻求行为的神经活动逐渐增加的一个可能因素,而对钠(+)转运的快速、脑浓度依赖性作用(局部麻醉作用)是决定与可卡因奖赏相关的神经激活突然、短暂停止的最可能因素。

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