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首页> 外文期刊>Pharmacology, Biochemistry and Behavior >Continuous nicotine infusion reduces nicotine self-administration in rats with 23-h/day access to nicotine.
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Continuous nicotine infusion reduces nicotine self-administration in rats with 23-h/day access to nicotine.

机译:连续尼古丁输注会减少每天23小时接触尼古丁的大鼠的尼古丁自我给药。

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摘要

The effects of continuous nicotine infusion on nicotine self-administration (NSA) were studied in rats as a model of nicotine replacement therapy (NRT) in humans. A NSA model in which rats had 23-h/day access to nicotine was used to approximate nicotine access conditions in cigarette smokers. In order to estimate serum nicotine concentrations associated with NSA, arterial and venous serum nicotine concentrations were measured during a simulation of NSA. Nicotine was noncontingently administered as 30 doses/12 h of 0.03 mg/kg/inf or 60 doses/12 h of 0.01 mg/kg/inf daily. Venous serum nicotine concentrations were measured after the first nicotine dose of the day, and arterial and venous concentrations were measured after doses in the middle of the day. The range of mean concentrations measured was similar to those reported in cigarette smokers (venous concentrations 6-59 ng/ml, arterial concentrations 42-96 ng/ml). The effects of continuous nicotine infusion on NSA were studied by noncontingently administering nicotine at various rates via osmotic pump to animals self-administering nicotine (0.01 or 0.03 mg/kg/inf) during 23-h/day sessions. Continuous nicotine infusion at all infusion rates substantially suppressed NSA, but suppression was rate-related only for the 0.01-mg/kg/inf NSA unit dose. Nicotine infusion rates producing venous serum nicotine concentrations equaling or exceeding the peak venous levels associated with simulated NSA were more effective than lower infusion rates only at the lower NSA unit dose. The highest nicotine infusion rate had no sustained effect on food-maintained responding, demonstrating its specificity for suppression of NSA. These data provide a model for studying NRT in the rat.
机译:作为人类尼古丁替代疗法(NRT)的模型,在大鼠中研究了连续尼古丁输注对尼古丁自我给药(NSA)的影响。使用NSA模型(其中大鼠每天可使用尼古丁23小时)来近似吸烟者中尼古丁的摄入情况。为了估算与NSA相关的血清尼古丁浓度,在模拟NSA的过程中测量了动脉和静脉的血清尼古丁浓度。每天以0.03 mg / kg / inf的30剂量/ 12 h或0.01 mg / kg / inf的60剂量/ 12 h的剂量连续非尼古丁给药。在一天的第一个尼古丁剂量之后测量静脉血清尼古丁的浓度,在一天的中间剂量之后测量动脉和静脉的浓度。测量的平均浓度范围与吸烟者中报告的浓度相似(静脉浓度为6-59 ng / ml,动脉浓度为42-96 ng / ml)。在23小时/天的疗程中,通过渗透泵非连续性地对动物自我给药的尼古丁(0.01或0.03 mg / kg / inf)以不同的速率连续给药尼古丁,研究了连续尼古丁输注对NSA的影响。在所有输注速率下连续尼古丁输注均能显着抑制NSA,但抑制仅与0.01 mg / kg / inf NSA单位剂量相关。仅在较低的NSA单位剂量下,产生的静脉血清尼古丁浓度等于或超过与模拟NSA相关的峰值静脉水平的尼古丁输注速率比较低的输注速率更有效。最高的尼古丁输注速率对维持食物的反应没有持续的影响,表明其抑制NSA的特异性。这些数据为研究大鼠NRT提供了模型。

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