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褪黑素给药通过高亲和力褪黑素受体发出的信号改变尼古丁偏好性消费。

Melatonin administration alters nicotine preference consumption via signaling through high-affinity melatonin receptors.

作者信息

Horton William J, Gissel Hannah J, Saboy Jennifer E, Wright Kenneth P, Stitzel Jerry A

机构信息

Institute for Behavioral Genetics, University of Colorado, 1480 30th Street, Boulder, CO, 80303, USA.

出版信息

Psychopharmacology (Berl). 2015 Jul;232(14):2519-30. doi: 10.1007/s00213-015-3886-1. Epub 2015 Feb 24.

Abstract

RATIONALE

While it is known that tobacco use varies across the 24-h day, the time-of-day effects are poorly understood. Findings from several previous studies indicate a potential role for melatonin in these time-of-day effects; however, the specific underlying mechanisms have not been well characterized. Understanding of these mechanisms may lead to potential novel smoking cessation treatments.

OBJECTIVE

The objective of this study is examine the role of melatonin and melatonin receptors in nicotine free-choice consumption

METHODS

A two-bottle oral nicotine choice paradigm was utilized with melatonin supplementation in melatonin-deficient mice (C57BL/6J) or without melatonin supplementation in mice proficient at melatonin synthesis (C3H/Ibg) compared to melatonin-proficient mice lacking both or one of the high-affinity melatonin receptors (MT1 and MT2; double-null mutant DM, or MT1 or MT2). Preference for bitter and sweet tastants also was assessed in wild-type and MT1 and MT2 DM mice. Finally, home cage locomotor monitoring was performed to determine the effect of melatonin administration on activity patterns.

RESULTS

Supplemental melatonin in drinking water significantly reduced free-choice nicotine consumption in C57BL/6J mice, which do not produce endogenous melatonin, while not altering activity patterns. Independently, genetic deletion of both MT1 and MT2 receptors in a melatonin-proficient mouse strain (C3H) resulted in significantly more nicotine consumption than controls. However, single genetic deletion of either the MT1 or MT2 receptor alone did not result in increased nicotine consumption. Deletion of MT1 and MT2 did not impact taste preference.

CONCLUSIONS

This study demonstrates that nicotine consumption can be affected by exogenous or endogenous melatonin and requires at least one of the high-affinity melatonin receptors. The fact that expression of either the MT1 or MT2 melatonin receptor is sufficient to maintain lower nicotine consumption suggests functional overlap and potential mechanistic explanations.

摘要

理论依据

虽然已知烟草使用在一天24小时内有所不同,但对一天中不同时间的影响了解甚少。先前几项研究的结果表明褪黑素在这些一天中不同时间的影响中可能发挥作用;然而,具体的潜在机制尚未得到充分表征。对这些机制的理解可能会带来潜在的新型戒烟治疗方法。

目的

本研究的目的是研究褪黑素和褪黑素受体在无尼古丁自由选择消费中的作用。

方法

采用双瓶口服尼古丁选择范式,在褪黑素缺乏的小鼠(C57BL/6J)中补充褪黑素,或在褪黑素合成能力强的小鼠(C3H/Ibg)中不补充褪黑素,并与缺乏高亲和力褪黑素受体(MT1和MT2;双缺失突变体DM,或MT1或MT2)之一或两者的褪黑素合成能力强的小鼠进行比较。还评估了野生型、MT1和MT2双缺失突变体小鼠对苦味和甜味剂的偏好。最后,进行笼内运动监测以确定褪黑素给药对活动模式的影响。

结果

在饮用水中补充褪黑素可显著降低不产生内源性褪黑素的C57BL/6J小鼠的自由选择尼古丁消费量,同时不改变活动模式。单独来看,在褪黑素合成能力强的小鼠品系(C3H)中,MT1和MT2受体的基因缺失导致尼古丁消费量显著高于对照组。然而,单独缺失MT1或MT2受体之一并未导致尼古丁消费量增加。MT1和MT2的缺失不影响味觉偏好。

结论

本研究表明,尼古丁消费可受外源性或内源性褪黑素影响,且需要至少一种高亲和力褪黑素受体。MT1或MT2褪黑素受体的表达足以维持较低的尼古丁消费量,这一事实表明存在功能重叠和潜在的机制解释。

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