代谢型谷氨酸受体5(mGlu5)拮抗剂MPEP与代谢型谷氨酸受体2/3(mGlu2/3)拮抗剂LY341495对大鼠尼古丁自我给药及尼古丁戒断相关奖赏缺陷的交互作用。
Interactive effects of the mGlu5 receptor antagonist MPEP and the mGlu2/3 receptor antagonist LY341495 on nicotine self-administration and reward deficits associated with nicotine withdrawal in rats.
作者信息
Liechti Matthias E, Markou Athina
机构信息
Department of Psychiatry, School of Medicine, University of California, San Diego, La Jolla, CA 92093, USA.
出版信息
Eur J Pharmacol. 2007 Jan 12;554(2-3):164-74. doi: 10.1016/j.ejphar.2006.10.011. Epub 2006 Oct 17.
Stimulatory actions of nicotine on mesocorticolimbic dopamine transmission are partly mediated by nicotine-induced glutamate release acting on ionotropic and metabotropic glutamate (mGlu) receptors. Because both presynaptic inhibitory mGlu2/3 and postsynaptic excitatory mGlu5 receptors provide potential targets for treatment of aspects of nicotine dependence, we examined interacting effects of mGlu5 (2-methyl-6-(phenylethynyl)-pyridine, MPEP) and mGlu2/3 (LY341495) receptor antagonists on nicotine self-administration and brain reward threshold elevations associated with spontaneous nicotine withdrawal in rats. We hypothesized that increasing glutamate transmission by blocking presynaptic inhibitory mGlu2/3 autoreceptors would antagonize MPEP-induced decreases in nicotine self-administration. We also hypothesized that blocking postsynaptic actions of glutamate on mGlu5 receptors would exacerbate nicotine withdrawal-induced reward deficits, and that this effect would be attenuated by co-administration of the mGlu2/3 receptor antagonist LY341495. MPEP selectively decreased nicotine, but not food, self-administration in rats. LY341495 slightly decreased both nicotine and food self-administration. Co-administration of LY341495 with MPEP attenuated the effectiveness of MPEP in decreasing nicotine intake, although MPEP was still effective. Spontaneous nicotine withdrawal induced somatic signs of withdrawal and reward threshold elevations indicating reward deficits. MPEP increased somatic signs and reward deficits in both nicotine- and saline-withdrawing rats. Thus, while mGlu5 receptor antagonists may be therapeutically useful in decreasing tobacco smoking, they worsen nicotine withdrawal. Co-administration of LY341495 reduced MPEP-induced reward deficits in both nicotine- and saline-withdrawing rats. Thus, increasing glutamate transmission via mGlu2/3 autoreceptor blockade reduces the effects of mGlu5 receptor blockade on nicotine self-administration and MPEP-induced exacerbation of brain reward deficits associated with nicotine withdrawal.
尼古丁对中脑皮质边缘多巴胺传递的刺激作用部分是由尼古丁诱导的谷氨酸释放介导的,该释放作用于离子型和代谢型谷氨酸(mGlu)受体。由于突触前抑制性mGlu2/3受体和突触后兴奋性mGlu5受体都为治疗尼古丁依赖的某些方面提供了潜在靶点,我们研究了mGlu5(2-甲基-6-(苯乙炔基)-吡啶,MPEP)和mGlu2/3(LY341495)受体拮抗剂对大鼠尼古丁自我给药以及与自发尼古丁戒断相关的脑奖赏阈值升高的相互作用。我们假设,通过阻断突触前抑制性mGlu2/3自身受体来增加谷氨酸传递,会拮抗MPEP诱导的尼古丁自我给药减少。我们还假设,阻断谷氨酸对mGlu5受体的突触后作用会加剧尼古丁戒断诱导的奖赏缺陷,并且这种作用会因共同给予mGlu2/3受体拮抗剂LY341495而减弱。MPEP选择性降低大鼠的尼古丁自我给药,但不影响食物自我给药。LY341495略微降低了尼古丁和食物的自我给药。LY341495与MPEP共同给药减弱了MPEP降低尼古丁摄入量的有效性,尽管MPEP仍然有效。自发尼古丁戒断诱导了戒断的躯体症状和奖赏阈值升高,表明存在奖赏缺陷。MPEP增加了尼古丁戒断和生理盐水戒断大鼠的躯体症状和奖赏缺陷。因此,虽然mGlu5受体拮抗剂在减少吸烟方面可能具有治疗作用,但它们会加重尼古丁戒断症状。LY341495与MPEP共同给药减少了尼古丁戒断和生理盐水戒断大鼠中MPEP诱导的奖赏缺陷。因此,通过mGlu2/3自身受体阻断增加谷氨酸传递,可降低mGlu5受体阻断对尼古丁自我给药以及MPEP诱导的与尼古丁戒断相关的脑奖赏缺陷加剧的影响。
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