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纹状体前脑啡肽原基因表达在急性而非慢性帕金森病猴中上调:对间接纹状体苍白球回路在帕金森病症状学中作用的启示。

Striatal preproenkephalin gene expression is upregulated in acute but not chronic parkinsonian monkeys: implications for the contribution of the indirect striatopallidal circuit to parkinsonian symptomatology.

作者信息

Schneider J S, Decamp E, Wade T

机构信息

Department of Pathology, Anatomy, and Cell Biology, Thomas Jefferson University, Philadelphia, Pennsylvania 19107, USA.

出版信息

J Neurosci. 1999 Aug 1;19(15):6643-9. doi: 10.1523/JNEUROSCI.19-15-06643.1999.

Abstract

This study examined the extent of striatal dopamine (DA) denervation and coincident expression of preproenkephalin (PPE) mRNA in monkeys made parkinsonian by 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) administration. Some animals (n = 4) became moderately parkinsonian after receiving large doses of MPTP over short periods of time and were symptomatic for only a short period of time (1-3 months; acute parkinsonian group). Other animals became moderately parkinsonian after receiving either escalating doses of MPTP over long periods (4-6 months; n = 5) or a high dose of MPTP over a short period (<1 month; n = 1) and remained symptomatic for an extended period (>8 months; chronic parkinsonian group). Despite similar symptomatology and similar degrees of striatal DA denervation at the time of their deaths, only acute parkinsonian animals had significantly increased PPE expression in sensorimotor striatal regions. PPE expression in chronic parkinsonian animals was either not changed or significantly decreased in most striatal regions. These findings suggest that the duration and not the extent of striatal DA denervation is a critical factor in modulating changes in striatal PPE expression. Furthermore, these results question the role of increased activity in the enkephalin-containing indirect striatopallidal pathway in the expression of parkinsonian symptoms.

摘要

本研究检测了通过给予1-甲基-4-苯基-1,2,3,6-四氢吡啶(MPTP)而患帕金森病的猴子纹状体多巴胺(DA)去神经支配的程度以及前脑啡肽原(PPE)mRNA的同步表达情况。一些动物(n = 4)在短时间内接受大剂量MPTP后出现中度帕金森病症状,且仅在短时间内(1 - 3个月;急性帕金森病组)有症状。其他动物在长时间内接受递增剂量的MPTP(4 - 6个月;n = 5)或在短时间内接受高剂量MPTP(<1个月;n = 1)后出现中度帕金森病症状,并在较长时间内(>8个月;慢性帕金森病组)仍有症状。尽管在死亡时它们有相似的症状学表现和相似程度的纹状体DA去神经支配,但只有急性帕金森病动物在感觉运动纹状体区域有显著增加的PPE表达。慢性帕金森病动物的PPE表达在大多数纹状体区域要么没有变化,要么显著降低。这些发现表明,纹状体DA去神经支配的持续时间而非程度是调节纹状体PPE表达变化的关键因素。此外,这些结果对含脑啡肽的间接纹状体苍白球通路活性增加在帕金森病症状表达中的作用提出了质疑。

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