Regenerative Medicine for the Aging Brain.

Enliven. Journal of stem cell research & regenerative medicine Pub Date : 2014-01-01 DOI:10.18650/2379-5751.11001

M. López-León, P. Reggiani, C. Hereñú, R. Goya

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引用次数: 15

Abstract

In the central nervous system, cholinergic and dopaminergic (DA) neurons are among the cells most susceptible to the deleterious effects of age. Thus, the basal forebrain cholinergic system is known to undergo moderate neurodegenerative changes during normal aging as well as severe atrophy in Alzheimer's disease (AD). Parkinson's disease (PD), a degeneration of nigro-striatal DA neurons is the most conspicuous reflection of the vulnerability of DA neurons to age. In this context, cell reprogramming offers novel therapeutic possibilities for the treatment of these devastating diseases. In effect, the generation of induced pluripotent stem cells (iPSCs) from somatic cells demonstrated that adult mammalian cells can be reprogrammed to a pluripotent state by the overexpression of a few embryonic transcription factors (TF). This discovery fundamentally widened the research horizon in the fields of disease modeling and regenerative medicine. Although it is possible to re-differentiate iPSCs to specific somatic cell types, the tumorigenic potential of contaminating iPSCs that failed to differentiate, increases the risk for clinical application of somatic cells generated by this procedure. Therefore, reprogramming approaches that bypass the pluripotent stem cell state are being explored. A method called lineage reprogramming has been recently documented. It consists of the direct conversion of one adult cell type into another by transgenic expression of multiple lineage-specific TF or microRNAs. Another approach, termed direct reprogramming, features several advantages such as the use of universal TF system and the ability to generate a rejuvenated multipotent progenitor cell population, able to differentiate into specific cell types in response to a specific differentiation factors. These novel approaches offer a new promise for the treatment of pathologies associated with the loss of specific cell types as for instance, nigral DA neurons (in PD) or basal forebrain cholinergic neurons in the early stages of AD. The above topics are reviewed here.

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衰老大脑的再生医学。

在中枢神经系统中，胆碱能和多巴胺能(DA)神经元是最容易受到年龄有害影响的细胞。因此，已知基底前脑胆碱能系统在正常衰老过程中经历中度神经退行性改变，以及阿尔茨海默病(AD)的严重萎缩。帕金森病(PD)，黑纹状体DA神经元的变性是DA神经元易受年龄影响的最明显反映。在这种情况下，细胞重编程为治疗这些毁灭性疾病提供了新的治疗可能性。事实上，体细胞诱导多能干细胞(iPSCs)的产生表明，成年哺乳动物细胞可以通过过度表达一些胚胎转录因子(TF)而被重编程为多能状态。这一发现从根本上拓宽了疾病建模和再生医学领域的研究视野。虽然有可能将iPSCs重新分化为特定的体细胞类型，但污染未能分化的iPSCs的致瘤性潜力增加了该过程产生的体细胞的临床应用风险。因此，绕过多能干细胞状态的重编程方法正在被探索。最近有一种方法被称为谱系重编程。它包括通过转基因表达多个谱系特异性TF或microrna将一种成年细胞类型直接转化为另一种。另一种方法，称为直接重编程，具有几个优点，如使用通用TF系统和产生返老还衰的多能祖细胞群的能力，能够根据特定的分化因子分化为特定的细胞类型。这些新方法为治疗与特定细胞类型丧失相关的病理提供了新的希望，例如，PD中的黑质DA神经元或AD早期阶段的基底前脑胆碱能神经元。在此回顾上述主题。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Enliven. Journal of stem cell research & regenerative medicine

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