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移植腹侧中脑的 A9 多巴胺神经元成分是帕金森病大鼠模型运动功能恢复的重要决定因素。

The A9 dopamine neuron component in grafts of ventral mesencephalon is an important determinant for recovery of motor function in a rat model of Parkinson's disease.

机构信息

Wallenberg Neuroscience Centre, Lund University, Lund, Sweden.

出版信息

Brain. 2010 Feb;133(Pt 2):482-95. doi: 10.1093/brain/awp328. Epub 2010 Jan 31.

Abstract

Grafts of foetal ventral mesencephalon, used in cell replacement therapy for Parkinson's disease, are known to contain a mix of dopamine neuronal subtypes including the A9 neurons of the substantia nigra and the A10 neurons of the ventral tegmental area. However, the relative importance of these subtypes for functional repair of the brain affected by Parkinson's disease has not been studied thoroughly. Here, we report results from a series of grafting experiments where the anatomical and functional properties of grafts either selectively lacking in A9 neurons, or with a typical A9/A10 composition were compared. The results show that the A9 component of intrastriatal grafts is of critical importance for recovery in tests on motor performance, in a rodent model of Parkinson's disease. Analysis at the histological level indicates that this is likely to be due to the unique ability of A9 neurons to innervate and functionally activate their target structure, the dorsolateral region of the host striatum. The findings highlight dopamine neuronal subtype composition as a potentially important parameter to monitor in order to understand the variable nature of functional outcome better in transplantation studies. Furthermore, the results have interesting implications for current efforts in this field to generate well-characterized and standardized preparations of transplantable dopamine neuronal progenitors from stem cells.

摘要

胎 ventral mesencephalon 移植物,用于帕金森病的细胞替代治疗,已知包含多巴胺神经元亚型的混合物,包括黑质的 A9 神经元和腹侧被盖区的 A10 神经元。然而,这些亚型对于受帕金森病影响的大脑的功能修复的相对重要性尚未得到充分研究。在这里,我们报告了一系列移植实验的结果,其中比较了选择性缺乏 A9 神经元的移植物或具有典型 A9/A10 组成的移植物的解剖学和功能特性。结果表明,纹状体内移植的 A9 成分对于帕金森病啮齿动物模型中运动性能测试的恢复至关重要。组织学水平的分析表明,这可能是由于 A9 神经元独特的支配和功能激活其靶结构(宿主纹状体的背外侧区域)的能力。这些发现强调了多巴胺神经元亚型组成作为一个潜在的重要参数,可以监测以更好地理解移植研究中功能结果的可变性质。此外,这些结果对于当前该领域的努力具有有趣的意义,即从干细胞中产生特征明确和标准化的可移植多巴胺神经元祖细胞制剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5755/2822634/625302f80df3/awp328f1.jpg

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