自由喂养与限食大鼠基底和D-1多巴胺受体激动剂刺激下尾壳核和伏隔核神经肽基因表达的比较

Sandra L. Haberny , Kenneth D. Carr
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引用次数: 32

摘要

行为学研究表明,慢性食物限制增强了中枢注射精神兴奋剂和直接多巴胺受体激动剂的奖励和运动激活作用。最近,研究表明,相对于自由喂养(AL)大鼠,在限食(FR)大鼠中,脑室内注射D-1 DA受体激动剂SKF-82958可增强运动激活作用,并增加纹状体ERK 1/2 MAP激酶、CaM激酶II、CREB和c-fos的激活。表达D-1 DA受体的纹状体神经元共表达dynorphin和P物质,并且已知CREB将D-1 DA受体刺激与preprodynorphin (ppD)基因表达偶联。本研究的目的是在体外注射SKF-82958 (20 μg) 3小时后,利用实时定量RT-PCR检测纹状神经肽基因表达,以检测FR可能的基因组影响。结果表明,在伏隔核(NAc)中,FR大鼠ppD和原纤裂蛋白(ppT) mRNA的基础水平低于AL大鼠。这可能反映了FR期间强直性DA传递的减少,在突触后D-1 DA受体介导的细胞信号传导代偿上调之前。然而,在SKF-82958刺激下,FR受试者的NAc中ppD和ppT mRNA水平高于AL受试者。在尾核-壳核(CPu)中也有类似的趋势。SKF-82958也增加了Nac中pre - proenkephalin (ppE) mRNA的表达,但没有增加CPu的表达,各组间差异无统计学意义。目前关于ppD和ppT的研究结果与先前的研究结果一致,即FR大鼠对急性D-1 DA激动剂攻击的行为和细胞反应增加。急性药物刺激下神经肽基因表达增加的功能后果仍有待研究,但可能包括反复药物暴露后出现的行为效应的调节,包括致敏、耐受性和成瘾。
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Comparison of basal and D-1 dopamine receptor agonist-stimulated neuropeptide gene expression in caudate-putamen and nucleus accumbens of ad libitum fed and food-restricted rats

Behavioral studies have demonstrated that chronic food restriction augments the rewarding and motor-activating effects of centrally injected psychostimulants and direct dopamine (DA) receptor agonists. Recently, it has been shown that intracerebroventricular (i.c.v.) injection of the D-1 DA receptor agonist, SKF-82958, produces an enhanced locomotor-activating effect as well as increased activation of striatal ERK 1/2 MAP kinase, CaM kinase II, CREB, and c-fos in food-restricted (FR) relative to ad libitum fed (AL) rats. Striatal neurons that express the D-1 DA receptor coexpress dynorphin and substance P, and CREB is known to couple D-1 DA receptor stimulation to preprodynorphin (ppD) gene expression. The purpose of the present study was to examine possible genomic consequences of FR using real-time quantitative RT-PCR to measure striatal neuropeptide gene expression 3 h after i.c.v. injection of SKF-82958 (20 μg). Results indicate that, in nucleus accumbens (NAc), basal levels of ppD and preprotachykinin (ppT) mRNA are lower in FR than AL rats. This may reflect a decrease in tonic DA transmission during FR which precedes the compensatory upregulation of postsynaptic D-1 DA receptor-mediated cell signaling. In response to SKF-82958 challenge, however, FR subjects displayed greater levels of ppD and ppT mRNA in NAc than did AL subjects. A similar trend was seen in caudate-putamen (CPu). SKF-82958 also increased preproenkephalin (ppE) mRNA in Nac, but not CPu, with no difference between feeding groups. The present findings regarding ppD and ppT are consistent with prior findings of increased behavioral and cellular responses to acute D-1 DA agonist challenge in FR rats. The functional consequences of increased neuropeptide gene expression in response to acute drug challenge remain to be investigated but may include modulation of behavioral effects that emerge with repeated drug exposure, including sensitization, tolerance, and addiction.

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