小鼠纹状体A(1) 腺苷能受体对乙醇诱导的运动不协调的调节作用
Modulation of ethanol-induced motor incoordination by mouse striatal A(1) adenosinergic receptor.
作者信息
Dar M S
机构信息
Department of Pharmacology, The Brody School of Medicine, East Carolina University, Greenville, NC 27858, USA.
出版信息
Brain Res Bull. 2001 Jul 1;55(4):513-20. doi: 10.1016/s0361-9230(01)00552-4.
We have demonstrated that ethanol-induced motor incoordination is modulated by cerebellar adenosine A(1) receptor. This study represents an extension into another important brain motor area, the striatum that, unlike cerebellum, has high density of both A(1) and A(2A) receptors. Direct intra-striatal micro-infusion of Ro15-4513 (0.05, 0.5, 1 ng), a partial inverse-agonist of benzodiazepine, significantly and nearly dose-dependently attenuated ethanol-induced motor incoordination indicating mediation of ethanol's motor incoordination by striatum. Intra-striatal A(1)-selective agonist N(6)-cyclohexyladenosine (CHA; 1, 2, 4 ng), A(1) = A(2A) non-selective agonist, 5'-N-ethylcarboxamidoadenosine (NECA; 1.5, 3, 6 ng), and A(1)-selective antagonist 8-cyclopentyl-1,3-dipropylxanthine (DPCPX; 25, 50, 100 ng) dose-dependently accentuated and attenuated, respectively, ethanol-induced motor incoordination, strongly suggesting modulation by striatal adenosine A(1) receptor. Intra-striatal DPCPX significantly antagonized not only ethanol-induced motor incoordination but also its potentiation by intra-striatal CHA, R-(+)-N(6)-(2-phenylisopropyladenosine) (R-PIA), or NECA. No change in motor coordination occurred after the highest dose of CHA, R-PIA, or NECA followed by saline. Similarly, the highest intra-striatal dose of Ro15-4513 or DPCPX neither altered motor coordination or locomotor activity indicating relative selectivity of interaction with ethanol. Nearly 25-fold higher dose of A(2A)-selective agonist, CGS-21680, compared to CHA was necessary to produce a comparable potentiation of ethanol's motor incoordination perhaps suggesting a lack of or less significant striatal A(2A) involvement. Intra-striatal pertussis toxin (0.5 microg) pre-treatment markedly attenuated ethanol-induced motor incoordination as well as its potentiation by intra-striatal CHA. These results support that striatum is one of the brain motor areas mediating the motor impairing effects of acute ethanol and that the latter's modulation occurs via A(1)-selective receptors coupled to pertussis toxin-sensitive G proteins.
我们已经证明,乙醇诱导的运动不协调受小脑腺苷A(1)受体调节。本研究将范围扩展至另一个重要的脑运动区域——纹状体,与小脑不同,纹状体中A(1)和A(2A)受体的密度都很高。直接向纹状体内微量注射Ro15 - 4513(0.05、0.5、1纳克),一种苯二氮䓬类的部分反向激动剂,能显著且几乎呈剂量依赖性地减轻乙醇诱导的运动不协调,表明纹状体介导了乙醇的运动不协调作用。向纹状体内注射A(1)选择性激动剂N(6)-环己基腺苷(CHA;1、2、4纳克)、A(1)=A(2A)非选择性激动剂5'-N-乙基羧酰胺腺苷(NECA;1.5、3、6纳克)以及A(1)选择性拮抗剂8-环戊基-1,3-二丙基黄嘌呤(DPCPX;25、50、100纳克),分别呈剂量依赖性地增强和减弱乙醇诱导的运动不协调,强烈提示纹状体腺苷A(1)受体参与了调节。向纹状体内注射DPCPX不仅显著拮抗了乙醇诱导的运动不协调,还拮抗了纹状体内注射CHA、R-(+)-N(6)-(2-苯异丙基腺苷)(R-PIA)或NECA对其产生的增强作用。在注射最高剂量的CHA、R-PIA或NECA后再注射生理盐水,运动协调性没有变化。同样,纹状体内注射Ro15 - 4513或DPCPX的最高剂量既未改变运动协调性也未改变运动活性,表明其与乙醇相互作用具有相对选择性。与CHA相比,产生与乙醇运动不协调相当增强作用所需的A(2A)选择性激动剂CGS-21680的剂量要高近25倍,这可能表明纹状体中A(2A)的参与较少或不显著。向纹状体内预先注射百日咳毒素(0.5微克)可显著减轻乙醇诱导的运动不协调以及纹状体内注射CHA对其的增强作用。这些结果支持纹状体是介导急性乙醇运动损害作用的脑运动区域之一,且乙醇的调节作用是通过与百日咳毒素敏感的G蛋白偶联的A(1)选择性受体实现的。
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