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帕金森病的细胞治疗。

Cell therapy in Parkinson's disease.

作者信息

Lindvall Olle, Björklund Anders

机构信息

Wallenberg Neuroscience Center and Lund Strategic Center for Stem Cell Biology and Cell Therapy, BMC A11, SE-221 84 Lund, Sweden.

出版信息

NeuroRx. 2004 Oct;1(4):382-93. doi: 10.1602/neurorx.1.4.382.

Abstract

The clinical studies with intrastriatal transplants of fetal mesencephalic tissue in Parkinson's disease (PD) patients have provided proof-of-principle for the cell replacement strategy in this disorder. The grafted dopaminergic neurons can reinnervate the denervated striatum, restore regulated dopamine (DA) release and movement-related frontal cortical activation, and give rise to significant symptomatic relief. In the most successful cases, patients have been able to withdraw L-dopa treatment after transplantation and resume an independent life. However, there are currently several problems linked to the use of fetal tissue: 1) lack of sufficient amounts of tissue for transplantation in a large number of patients, 2) variability of functional outcome with some patients showing major improvement and others modest if any clinical benefit, and 3) occurrence of troublesome dyskinesias in a significant proportion of patients after transplantation. Thus, neural transplantation is still at an experimental stage in PD. For the development of a clinically useful cell therapy, we need to define better criteria for patient selection and how graft placement should be optimized in each patient. We also need to explore in more detail the importance for functional outcome of the dissection and cellular composition of the graft tissue as well as of immunological mechanisms. Strategies to prevent the development of dyskinesias after grafting have to be developed. Finally, we need to generate large numbers of viable DA neurons in preparations that are standardized and quality controlled. The stem cell technology may provide a virtually unlimited source of DA neurons, but several scientific issues need to be addressed before stem cell-based therapies can be tested in PD patients.

摘要

帕金森病(PD)患者脑内纹状体移植胎儿中脑组织的临床研究为该疾病的细胞替代策略提供了原理证明。移植的多巴胺能神经元可重新支配去神经支配的纹状体,恢复调节性多巴胺(DA)释放及与运动相关的额叶皮质激活,并显著缓解症状。在最成功的病例中,患者在移植后能够停用左旋多巴治疗并恢复独立生活。然而,目前使用胎儿组织存在几个问题:1)大量患者缺乏足够用于移植的组织;2)功能结果存在变异性,一些患者有显著改善,而另一些患者即使有临床益处也很有限;3)相当一部分患者移植后出现麻烦的运动障碍。因此,神经移植在帕金森病中仍处于实验阶段。为了开发临床上有用的细胞疗法,我们需要为患者选择定义更好的标准,以及如何针对每个患者优化移植物植入。我们还需要更详细地探讨移植物组织的解剖结构和细胞组成以及免疫机制对功能结果的重要性。必须制定防止移植后运动障碍发生的策略。最后,我们需要在标准化和质量控制的制剂中生成大量有活力的多巴胺能神经元。干细胞技术可能提供几乎无限的多巴胺能神经元来源,但在基于干细胞的疗法能够在帕金森病患者中进行测试之前,需要解决几个科学问题。

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