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与年龄相关的黑质神经元功能衰退与恒河猴的运动障碍相关。

Age-related declines in nigral neuronal function correlate with motor impairments in rhesus monkeys.

作者信息

Emborg M E, Ma S Y, Mufson E J, Levey A I, Taylor M D, Brown W D, Holden J E, Kordower J H

机构信息

Research Center for Brain Repair and Department of Neurological Sciences, Rush Presbyterian Medical Center, Chicago, Illinois 60612, USA.

出版信息

J Comp Neurol. 1998 Nov 16;401(2):253-65.

PMID:9822152
Abstract

Although the role of dopamine dysfunction is well established in Parkinson's disease, the effect of nigrostriatal degeneration on motor performance during normal aging is less well understood. In this study, aged rhesus monkeys (25-27 years old) displayed significant impairments relative to young (3-5 years old) cohorts in motor function as assessed on a fine motor task and home cage activity. Additionally, the clinical motor function of aged monkeys was impaired relative to young monkeys as assessed on a clinical rating scale. Unbiased stereologic measurements of the substantia nigra revealed a significant age-related loss of tyrosine hydroxylase-immunoreactive (TH-ir; 50.3%) and dopamine transporter-immunoreactive (DAT-ir; 33.2%) nigral neurons. The monkeys performance on the fine motor task and on the clinical rating scale was correlated with TH-ir neuronal counts. The number of DAT-ir nigral neurons was correlated with activity and clinical rating scale scores. Our results suggest that age-related motor impairments in nonhuman primates are associated with spontaneous decreases in TH-ir and DAT-ir nigral cells. The correlation of motor deficits with the loss of TH-ir and DAT-ir nigral neurons suggests that aged nonhuman primates may provide a useful model for mimicking changes seen in human aging and early Parkinson's disease.

摘要

虽然多巴胺功能障碍在帕金森病中的作用已得到充分证实,但黑质纹状体变性在正常衰老过程中对运动表现的影响却鲜为人知。在本研究中,与年轻(3 - 5岁)猴群相比,老年恒河猴(25 - 27岁)在精细运动任务和笼内活动中评估的运动功能方面表现出显著损伤。此外,根据临床评分量表评估,老年猴的临床运动功能相对于年轻猴有所受损。对黑质进行无偏立体测量显示,酪氨酸羟化酶免疫反应阳性(TH-ir;50.3%)和多巴胺转运体免疫反应阳性(DAT-ir;33.2%)的黑质神经元出现与年龄相关的显著减少。猴在精细运动任务和临床评分量表上的表现与TH-ir神经元计数相关。DAT-ir黑质神经元的数量与活动及临床评分量表得分相关。我们的结果表明,非人灵长类动物中与年龄相关的运动损伤与TH-ir和DAT-ir黑质细胞的自发减少有关。运动缺陷与TH-ir和DAT-ir黑质神经元丢失之间的相关性表明,老年非人灵长类动物可能为模拟人类衰老和早期帕金森病中所见变化提供一个有用的模型。

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