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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Modelling Parkinson-like neurodegeneration via osmotic minipump delivery of MPTP and probenecid.
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Modelling Parkinson-like neurodegeneration via osmotic minipump delivery of MPTP and probenecid.

机译:通过渗透微型泵的MPTP和丙磺舒模拟帕金森样神经变性。

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摘要

Mouse models of MPTP intoxication have been used extensively to explore the molecular mechanisms of Parkinson's disease. However, these models present some limitations since; (i) Dopaminergic (DA) cell death occurs rapidly in contrast to the presumably slow evolution of the disease process. (ii) Some of the key histological features of the disease such as Lewy body like inclusions and long-term inflammatory changes are lacking. Fornai et al. [Proc. Natl Acad. Sci. USA 102 (2005), 3413] suggested that continuous delivery of MPTP with Alzet osmotic minipumps may possibly circumvent these problems. Our results show, however, that MPTP infusion via Alzet osmotic minipumps (40 mg/kg/day) produces only a transient depletion in striatal dopamine (DA) without causing dopaminergic cell loss in the substantia nigra. Neuronal cell loss occurred, however, if MPTP was infused concomitantly with probenecid, an uricosuric agent which potentiates the effects of the toxin injected via the i.p. route. Even under these conditions, dopaminergic cell loss was moderate (-25%) and other neurodegenerative changes characteristic of Parkinson's disease remained undetectable.
机译:MPTP中毒的小鼠模型已广泛用于探索帕金森氏病的分子机制。但是,由于这些模型存在一些限制, (i)与疾病过程的缓慢发展相反,多巴胺能(DA)细胞死亡迅速发生。 (ii)缺乏该病的一些关键组织学特征,如路易体,如内含物和长期的炎症变化。 Fornai等。 [过程Natl Acad。科学USA 102(2005),3413]建议用Alzet渗透微型泵连续输送MPTP可能可以避免这些问题。然而,我们的结果表明,通过Alzet渗透微型泵(40 mg / kg /天)输注MPTP只会在纹状体多巴胺(DA)中产生短暂消耗,而不会引起黑质中的多巴胺能细胞损失。但是,如果将MPTP与丙磺舒(一种抗尿酸药物,可增强经腹膜内注射毒素的作用)同时注入MPTP,则会发生神经元细胞丢失。路线。即使在这些条件下,多巴胺能细胞损失也是中等程度的(-25%),帕金森氏病的其他神经退行性变化特征仍未检出。

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