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Stem cell grafting improves both motor and cognitive impairments in a genetic model of Parkinson’s disease the aphakia mouse

机译:干细胞嫁接改善了帕金森病的遗传模型中的电动机和认知障碍北曲棍鼠

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摘要

Stem cell-based cell replacement of lost midbrain dopamine (mDA) neurons is a potential therapy for Parkinson’s disease (PD). Toward this goal, it is critical to optimize various aspects of cell transplantation and to assess functional recovery through behavioral tests in validated animal model(s) of PD. At present, cell transplantation studies are being done almost exclusively in neurotoxin-based animal models, because few genetic models of PD exhibit robust mDA neuronal loss. Here, we used a genetic model of PD, the aphakia mouse, which demonstrates selective degeneration of mDA neurons in the substantia nigra. We systematically investigated the functional effects of transplanting embryonic stem cell derived cells at different stages of in vitro differentiation; embryoid body (EB), neural progenitor (NP), and neuronal differentiated (ND) stages. We found that transplantation of NP cells yielded the best outcomes for both survival and behavioral improvement while transplantation of EB and ND cells resulted in high teratoma-like tumor formation and poor survival, respectively. In behavioral paradigms specific to basal ganglia, the NP cells group prominently improved motor behavioral defects 1 and 2 months post transplantation. Furthermore, we found that NP cells transplantation also improved cognitive impairments of aphakia mice, as examined by the passive avoidance task. Importantly, these graft-induced functional improvements well correlated with survival of tyrosine hydroxylase-positive DA neurons. Taken together, we propose that the aphakia mouse can serve as a novel and useful platform for cell transplantation studies to assess both neurological and cognitive improvements and that NP stage cells represent an optimal stage for transplantation.
机译:失去中脑多巴胺(mDA)神经元的干细胞为基础的细胞置换是帕金森氏病(PD)的潜在疗法。为了实现此目标,至关重要的是优化细胞移植的各个方面,并通过在经过验证的PD动物模型中进行行为测试来评估功能恢复。目前,细胞移植研究几乎完全在基于神经毒素的动物模型中进行,因为很少有PD的遗传模型表现出强大的mDA神经元丢失。在这里,我们使用了无晶状体小鼠PD的遗传模型,该模型显示了黑质中mDA神经元的选择性变性。我们系统地研究了在体外分化的不同阶段移植胚胎干细胞衍生细胞的功能效应。胚状体(EB),神经祖细胞(NP)和神经元分化(ND)阶段。我们发现,NP细胞的移植对于生存和行为改善均产生了最佳结果,而EB和ND细胞的移植分别导致了畸胎瘤样肿瘤的形成和较差的存活。在特定于基底神经节的行为范例中,NP细胞组在移植后1和2个月显着改善了运动行为缺陷。此外,我们发现,通过被动回避任务可以检查出,NP细胞移植还可以改善无晶状体小鼠的认知障碍。重要的是,这些移植物诱导的功能改善与酪氨酸羟化酶阳性DA神经元的存活密切相关。两者合计,我们建议无晶状体小鼠可以用作细胞移植研究的新型和有用的平台,以评估神经和认知的改善,并且NP阶段细胞代表了移植的最佳阶段。

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