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首页> 外文期刊>Psychopharmacology >Differential effects of nicotinic antagonists perfused into the nucleus accumbens or the ventral tegmental area on cocaine-induced dopamine release in the nucleus accumbens of mice.
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Differential effects of nicotinic antagonists perfused into the nucleus accumbens or the ventral tegmental area on cocaine-induced dopamine release in the nucleus accumbens of mice.

机译:尼古丁拮抗剂灌注到伏隔核或腹侧被盖区中对可卡因诱导的伏隔核中多巴胺释放的差异作用。

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摘要

RATIONALE: The mesolimbic dopamine (DA) system is considered a principal site for nicotine-cocaine interactions. OBJECTIVES AND METHODS: The aim of this paper is to study the effects of local perfusions (through the microdialysis cannula) of nicotinic acetylcholine receptor (nAChR) antagonists in the ventral tegmental area (VTA, where mesolimbic DA cell bodies are located) or nucleus accumbens (nAc, where mesolimbic DA nerve terminals project) on cocaine-elicited increase in DA levels in the nAc of mice using intracerebral microdialysis. RESULTS: Intra-nAc perfusion of mecamylamine (a nonselective central nicotinic antagonist) or coperfusion of methyllycaconitine (MLA, 10 nM) and dihydro-beta-erythroidine (DHbetaE, 10-100 muM) decreased cocaine-elicited increase in DA perfusate levels. In contrast, intra-nAc perfusion of MLA alone (a relatively selective antagonist of alpha7 subunit-containing nAChRs) increased, while DHbetaE (a relatively selective antagonist of heteromeric nAChR subtypes) did not alter, cocaine-elicited increase in DA perfusate levels. Intra-VTA perfusion of MLA (100 nM) or DHbetaE (100 micro M) significantly increased the cocaine-elicited increase of DA levels in the nAc or VTA, whereas DHbetaE and MLA coperfusion or mecamylamine perfusion had no significant effect. CONCLUSIONS: These results show that intra-nAc and intra-VTA perfusion of nAChR antagonists differentially affect cocaine-elicited increase in DA levels in a region and subtype-specific manner. This suggests that multiple cholinergicicotinic pathways influence the effects of cocaine on mesolimbic DA neurons in complex, and sometimes opposing, patterns.
机译:理由:中脑边缘多巴胺(DA)系统被认为是尼古丁与可卡因相互作用的主要部位。目的和方法:本文的目的是研究腹侧被盖区(VTA,中边缘边缘DA细胞体所在的位置)的烟碱乙酰胆碱受体(nAChR)拮抗剂的局部灌注(通过微透析插管)的影响。 (脑内,边缘中脑DA神经末梢突出的nAc)使用可卡因引起的使用脑内微透析的小鼠nAc的DA水平增加。结果:美卡明胺(非选择性中枢烟碱拮抗药)的nAc内灌注或甲基lycaconitine(MLA,10 nM)和dihydro-β-erythroidine(DHbetaE,10-100μM)的共同灌注降低了可卡因引起的DA灌注液水平的增加。相反,单独的MLA(含α7亚基的nAChRs的相对选择性拮抗剂)的nAc内灌注增加,而DHbetaE(异源nAChR亚型的相对选择性拮抗剂)没有改变,可卡因引起DA灌注液水平增加。 VLA内MLA(100 nM)或DHbetaE(100 micro M)的灌注显着增加了可卡因引起的nAc或VTA中DA水平的增加,而DHbetaE和MLA灌注或美卡明胺灌注没有明显作用。结论:这些结果表明,nAChR拮抗剂的nAc内和VTA内灌注以区域和亚型特异性方式差异影响可卡因引起的DA水平的升高。这表明,多种胆碱能/烟碱途径以复杂的,有时是相反的模式影响可卡因对中脑边缘DA神经元的作用。

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