Advances in the Differentiation of hiPSCs into Cerebellar Neuronal Cells.

IF 4.5 3区 医学 Q2 CELL & TISSUE ENGINEERING Stem Cell Reviews and Reports Pub Date : 2024-10-01 Epub Date: 2024-07-18 DOI:10.1007/s12015-024-10763-x
Yingxin Wang, Wenzhu Liu, Yichang Jiao, Yitong Yang, Didi Shan, Xinbo Ji, Rui Zhang, Zexin Zhan, Yao Tang, Dandan Guo, Chuanzhu Yan, Fuchen Liu
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Abstract

The cerebellum has historically been primarily associated with the regulation of precise motor functions. However, recent findings suggest that it also plays a pivotal role in the development of advanced cognitive functions, including learning, memory, and emotion regulation. Pathological changes in the cerebellum, whether congenital hereditary or acquired degenerative, can result in a diverse spectrum of disorders, ranging from genetic spinocerebellar ataxias to psychiatric conditions such as autism, and schizophrenia. While studies in animal models have significantly contributed to our understanding of the genetic networks governing cerebellar development, it is important to note that the human cerebellum follows a protracted developmental timeline compared to the neocortex. Consequently, employing animal models to uncover human-specific molecular events in cerebellar development presents significant challenges. The emergence of human induced pluripotent stem cells (hiPSCs) has provided an invaluable tool for creating human-based culture systems, enabling the modeling and analysis of cerebellar physiology and pathology. hiPSCs and their differentiated progenies can be derived from patients with specific disorders or carrying distinct genetic variants. Importantly, they preserve the unique genetic signatures of the individuals from whom they originate, allowing for the elucidation of human-specific molecular and cellular processes involved in cerebellar development and related disorders. This review focuses on the technical advancements in the utilization of hiPSCs for the generation of both 2D cerebellar neuronal cells and 3D cerebellar organoids.

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将 hiPSCs 分化为小脑神经元细胞的进展。
小脑历来主要与精确运动功能的调节有关。然而,最近的研究结果表明,小脑在高级认知功能(包括学习、记忆和情绪调节)的发展过程中也发挥着举足轻重的作用。小脑的病理变化,无论是先天遗传性的还是后天退化性的,都会导致各种不同的疾病,从遗传性脊髓小脑性共济失调到自闭症和精神分裂症等精神疾病。虽然动物模型研究极大地促进了我们对支配小脑发育的遗传网络的了解,但必须注意的是,与新皮质相比,人类小脑的发育时间较长。因此,利用动物模型来揭示小脑发育过程中的人类特异性分子事件是一项重大挑战。人类诱导多能干细胞(hiPSCs)的出现为创建基于人类的培养系统提供了一个宝贵的工具,使小脑生理学和病理学的建模和分析成为可能。重要的是,它们保留了其来源个体的独特遗传特征,从而可以阐明小脑发育和相关疾病所涉及的人类特异性分子和细胞过程。本综述重点介绍利用hiPSCs生成二维小脑神经元细胞和三维小脑器官组织的技术进展。
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来源期刊
Stem Cell Reviews and Reports
Stem Cell Reviews and Reports 医学-细胞生物学
CiteScore
9.30
自引率
4.20%
发文量
0
审稿时长
3 months
期刊介绍: The purpose of Stem Cell Reviews and Reports is to cover contemporary and emerging areas in stem cell research and regenerative medicine. The journal will consider for publication: i) solicited or unsolicited reviews of topical areas of stem cell biology that highlight, critique and synthesize recent important findings in the field. ii) full length and short reports presenting original experimental work. iii) translational stem cell studies describing results of clinical trials using stem cells as therapeutics. iv) papers focused on diseases of stem cells. v) hypothesis and commentary articles as opinion-based pieces in which authors can propose a new theory, interpretation of a controversial area in stem cell biology, or a stem cell biology question or paradigm. These articles contain more speculation than reviews, but they should be based on solid rationale. vi) protocols as peer-reviewed procedures that provide step-by-step descriptions, outlined in sufficient detail, so that both experts and novices can apply them to their own research. vii) letters to the editor and correspondence. In order to facilitate this exchange of scientific information and exciting novel ideas, the journal has created five thematic sections, focusing on: i) the role of adult stem cells in tissue regeneration; ii) progress in research on induced pluripotent stem cells, embryonic stem cells and mechanism governing embryogenesis and tissue development; iii) the role of microenvironment and extracellular microvesicles in directing the fate of stem cells; iv) mechanisms of stem cell trafficking, stem cell mobilization and homing with special emphasis on hematopoiesis; v) the role of stem cells in aging processes and cancerogenesis.
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