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短篇综述:探索 ARSACS:理解小脑退行性变的模型。

Short Review: Investigating ARSACS: models for understanding cerebellar degeneration.

机构信息

Stem Cells Therapies in Neurodegenerative Diseases Lab, Research Center "Principe Felipe", Valencia, Spain.

Unit of Genetics and Genomics of Neuromuscular and Neurodegenerative Disorders and Service of Genomics and Translational Genetics, Research Center "Principe Felipe", Valencia, Spain.

出版信息

Neuropathol Appl Neurobiol. 2019 Oct;45(6):531-537. doi: 10.1111/nan.12540. Epub 2019 Mar 11.

Abstract

Autosomal recessive spastic ataxia of Charlevoix-Saguenay (ARSACS) is an early-onset neurodegenerative disease that includes progressive cerebellar dysfunction. ARSACS is caused by an autosomal recessive loss-of-function mutation in the SACS gene, which encodes for SACSIN. Although animal models are still necessary to investigate the role of SACSIN in the pathology of this disease, more reliable human cellular models need to be generated to better understand the cerebellar pathophysiology of ARSACS. The discovery of human induced pluripotent stem cells (hiPSC) has permitted the derivation of patient-specific cells. These cells have an unlimited self-renewing capacity and the ability to differentiate into different neural cell types, allowing studies of disease mechanism, drug discovery and cell replacement therapies. In this study, we discuss how the hiPSC-derived cerebellar organoid culture offers novel strategies for targeting the pathogenic mutations related to ARSACS. We also highlight the advantages and challenges of this 3D cellular model, as well as the questions that still remain unanswered.

摘要

常染色体隐性痉挛性共济失调型小脑性共济失调(ARSACS)是一种早发性神经退行性疾病,包括进行性小脑功能障碍。ARSACS 是由 SACS 基因的常染色体隐性功能丧失突变引起的,该基因编码 SACSIN。尽管仍然需要动物模型来研究 SACSIN 在该疾病病理中的作用,但需要生成更可靠的人类细胞模型,以更好地理解 ARSACS 的小脑病理生理学。人类诱导多能干细胞(hiPSC)的发现使得能够衍生出患者特异性细胞。这些细胞具有无限的自我更新能力和分化为不同神经细胞类型的能力,从而可以研究疾病机制、药物发现和细胞替代疗法。在本研究中,我们讨论了 hiPSC 衍生的小脑类器官培养如何为靶向与 ARSACS 相关的致病突变提供新的策略。我们还强调了这种 3D 细胞模型的优势和挑战,以及仍然存在的未解决的问题。

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