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通过过表达Nurr1使大鼠胚胎神经前体细胞向多巴胺能神经元分化。

Dopaminergic neuronal differentiation from rat embryonic neural precursors by Nurr1 overexpression.

作者信息

Kim Ju-Yeon, Koh Hyun Chul, Lee Ji-Yeon, Chang Mi-Yoon, Kim You-Chan, Chung Hee-Yong, Son Hyeon, Lee Yong-Sung, Studer Lorenz, McKay Ron, Lee Sang-Hun

机构信息

Department of Biochemistry, and Institute of Mental Health, Hanyang University, Seoul, Korea.

出版信息

J Neurochem. 2003 Jun;85(6):1443-54. doi: 10.1046/j.1471-4159.2003.01780.x.

Abstract

In vitro expanded CNS precursors could provide a renewable source of dopamine (DA) neurons for cell therapy in Parkinson's disease. Functional DA neurons have been derived previously from early midbrain precursors. Here we demonstrate the ability of Nurr1, a nuclear orphan receptor essential for midbrain DA neuron development in vivo, to induce dopaminergic differentiation in naïve CNS precursors in vitro. Independent of gestational age or brain region of origin, Nurr1-induced precursors expressed dopaminergic markers and exhibited depolarization-evoked DA release in vitro. However, these cells were less mature and secreted lower levels of DA than those derived from mesencephalic precursors. Transplantation of Nurr1-induced DA neuron precursors resulted in limited survival and in vivo differentiation. No behavioral improvement in apomorphine-induced rotation scores was observed. These results demonstrate that Nurr1 induces dopaminergic features in naïve CNS precursors in vitro. However, additional factors will be required to achieve in vivo function and to unravel the full potential of neural precursors for cell therapy in Parkinson's disease.

摘要

体外扩增的中枢神经系统前体细胞可为帕金森病的细胞治疗提供可再生的多巴胺(DA)神经元来源。功能性DA神经元此前已从早期中脑前体细胞中获得。在此,我们证明了Nurr1(一种对体内中脑DA神经元发育至关重要的核孤儿受体)在体外诱导幼稚中枢神经系统前体细胞向多巴胺能分化的能力。与胎龄或起源脑区无关,Nurr1诱导的前体细胞表达多巴胺能标记物,并在体外表现出去极化诱发的DA释放。然而,这些细胞比从中脑前体细胞衍生而来的细胞成熟度更低,DA分泌水平也更低。移植Nurr1诱导的DA神经元前体细胞导致有限的存活和体内分化。未观察到阿扑吗啡诱导的旋转评分有行为改善。这些结果表明,Nurr1在体外诱导幼稚中枢神经系统前体细胞具有多巴胺能特性。然而,需要其他因素来实现体内功能,并揭示神经前体细胞在帕金森病细胞治疗中的全部潜力。

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