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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Differential effects of dopamine and opioid receptor blockade on motivated Coca-Cola drinking behavior and associated changes in brain, skin and muscle temperatures.
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Differential effects of dopamine and opioid receptor blockade on motivated Coca-Cola drinking behavior and associated changes in brain, skin and muscle temperatures.

机译:多巴胺和阿片类受体阻断对脑,皮肤和肌肉温度的促进可口可乐饮用行为的差异影响。

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摘要

Although pharmacological blockade of both dopamine (DA) and opiate receptors has an inhibiting effect on appetitive motivated behaviors, it is still unclear which physiological mechanisms affected by these treatments underlie the behavioral deficit. To clarify this issue, we examined how pharmacological blockade of either DA (SCH23390+eticlopride at 0.2 mg/kg each) or opioid receptors (naloxone 1 mg/kg) affects motor activity and temperature fluctuations in the nucleus accumbens (NAcc), temporal muscle, and facial skin associated with motivated Coca-Cola drinking behavior in rats. In drug-free conditions, presentation of a cup containing 5 ml of Coca-Cola induced locomotor activation and rapid NAcc temperature increases, which both transiently decreased during drinking, and phasically increased again after the cup was emptied. Muscle temperatures followed this pattern, but increases were weaker and more delayed than those in the NAcc. Skin temperature rapidly dropped after cup presentation, remained at low levels during consumption, and slowly restored during post-consumption behavioral activation. By itself, DA receptor blockade induced robust decrease in spontaneous locomotion, moderate increases in brain and muscle temperatures, and a relative increase in skin temperatures, suggesting metabolic activation coupled with adynamia. Following this treatment (approximately 180 min), motor activation to cup presentation and Coca-Cola consumption were absent, but rats showed NAcc and muscle temperature increases following cup presentation comparable to control. Therefore, DA receptor blockade does not affect significantly central and peripheral autonomic responses to appetitive stimuli, but eliminates their behavior-activating effects, thus disrupting appetitive behavior and blocking consumption. Naloxone alone slightly decreased brain and muscle temperatures and increased skin temperatures, pointing at the enhanced heat loss and possible minor inhibition of basal metabolic activity. This treatment (approximately 60 min) had minimal effects on the latencies of drinking, but increased its total duration, with licking interrupted by pauses and retreats. This behavioral attenuation was coupled with weaker than in control locomotor activation and diminished temperature fluctuations in each recording location. Therefore, attenuation of normal behavioral and physiological responses to appetitive stimuli appears to underlie modest inhibiting effects of opiate receptor blockade on motivated behavior and consumption.
机译:虽然多巴胺(DA)和阿片受体的药理阻滞对食欲性促进行为的抑制作用,但仍然不清楚受这些治疗影响的哪种生理机制是行为赤字。为了澄清这一问题,我们研究了DA(SCH23390 + Itemlopridere)的药理学阻滞方式(每种0.2mg / kg)或阿片类药物(纳洛酮1mg / kg)影响核心尿嘧啶(Nacc),颞肌的运动活性和温度波动和大鼠Coca-Cola饮酒行为相关的面部皮肤。在无毒条件下,含有5ml可口可乐诱导的运动活化和快速Nacc温度的杯子的呈递增加,在饮用期间瞬时降低,并且在杯子清空后再次增加。肌肉气温遵循这种模式,但增加比NACC中的那些较弱,更延迟。在杯子呈现后,皮肤温度迅速下降,在消耗期间保持低水平,并且在消耗后行为激活期间缓慢恢复。本身,DA受体阻断诱导的自发运动诱导的稳健降低,脑和肌肉温度的中度增加,皮肤温度的相对增加,表明代谢激活与Adynamia相结合。在该处理(约180分钟)之后,不存在对杯呈递和可口可乐消费的电动机活化,但大鼠显示NACC和肌肉温度随着控制的杯子呈现而增加。因此,DA受体阻滞不影响对食欲刺激的显着中央和外周自主主义反应,而是消除了它们的行为激活效果,从而扰乱了满意行为和阻塞消耗。纳洛酮单独略微降低脑和肌肉温度,增加皮肤温度,指向增强的热量损失和对基础代谢活性的轻微抑制。这种治疗(约60分钟)对饮酒潜伏期的影响很小,但增加了总持续时间,而少睡眠中断并撤退。该行为衰减与每个记录位置中的控制运动位置激活和减少温度波动减少。因此,对食欲性刺激的正常行为和生理反应的衰减似乎是阿片受体阻断对促进行为和消费的适度抑制作用。

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