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Preclinical evidence for combining the 5‐ HT 2C HT 2C 2C receptor agonist lorcaserin and varenicline as a treatment for nicotine dependence

机译:结合5-HT 2C HT 2C 2C受体激动剂Lorcaserin和Varenicline作为尼古丁依赖的治疗方法的临床前验证

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Abstract Varenicline, a nicotinic acetylcholine receptor partial agonist, is used to treat nicotine dependence. Lorcaserin, a 5‐HT 2C receptor agonist has been approved in some countries to treat obesity. Based on preclinical and preliminary clinical evidence, lorcaserin may have potential to treat nicotine dependence. These experiments examined in rats the effects of combining varenicline (0.5 or 1?mg/kg) and lorcaserin (0.3, 0.6 and 1?mg/kg) on nicotine self‐administration, reinstatement of nicotine seeking, responding for food and impulsive action. Both drugs alone reduced nicotine self‐administration. Combining varenicline and 0.6 mg/kg lorcaserin reduced responding to a greater extent than either drug alone. In a relapse model, extinguished nicotine seeking was reinstated by a priming injection of nicotine and nicotine‐associated cues. Reinstatement was reduced by varenicline (1?mg/kg) and by lorcaserin (0.3?mg/kg). Combining lorcaserin (0.3?mg/kg) with varenicline (0.5 or 1?mg/kg) reduced reinstatement to a greater degree than either drug alone. Both drugs had minimal effects on responding for food, alone or in combination. In the five‐choice serial reaction time test, varenicline (0.5 or 1?mg/kg) increased impulsivity, measured as increased premature responding. This effect was reduced by lorcaserin (0.3?mg/kg). Plasma levels of varenicline or lorcaserin were not altered by co‐administration of the other drug. Varenicline and lorcaserin have additive effects on nicotine self‐administration, and on nicotine seeking. Lorcaserin prevents impulsivity induced by varenicline. This pattern of effects suggests that co‐administration of varenicline and lorcaserin has potential as a treatment for nicotine dependence that may exceed the value of either drug alone.
机译:摘要varenicline,一种烟碱乙酰胆碱受体部分激动剂,用于治疗尼古丁依赖。 Lorcaserin,一个5-HT 2C受体激动剂已被批准在一些国家来治疗肥胖症。基于临床前和初步临床证据,Lorcaserin可能有可能治疗尼古丁依赖。这些实验在大鼠中检查了组合瓦尼尼线(0.5或1×mg / kg)和洛杉矶(0.3,0.6和1μg/ kg)对尼古丁自我给药,恢复尼古丁寻求的影响,应对食物和冲动作用的影响。只有两种药物都会减少尼古丁自我给药。结合varenicline和0.6 mg / kg Lorcaserin比单独的药物更大程度地降低响应。在复发模型中,通过引发尼古丁和尼古丁相关的提示恢复熄灭的尼古丁寻求。血管线(1×mg / kg)和洛根塞序(0.3×mg / kg)减少恢复。将Lorcaserin(0.3×mg / kg)与varenicline(0.5或1×mg / kg)结合在一起比单独的药物更大的程度。两种药物对单独或组合应对食物的影响很小。在五项选择的连续反应时间测试中,脉冲线(0.5或1×mg / kg)增加冲动,测量为较高的过早响应。 Lorcaserin(0.3μmg/ kg)减少了这种效果。通过共同施用其他药物,不会改变血浆水平或洛根氏素。 varenicline和lorcaserin对尼古丁自我给药以及尼古丁寻求的添加剂。 Lorcaserin防止脉冲线诱导的冲动。这种效果模式表明,樟树和洛氏菌蛋白的共同施用具有诸如尼古丁依赖性的治疗可能超过两种药物的价值。

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