Comparing the Characteristics of Microglia Preparations Generated Using Different Human iPSC-Based Differentiation Methods to Model Neurodegenerative Diseases.

IF 3.9 4区 医学 Q2 NEUROSCIENCES
Ye Man Tang, Nisha S Pulimood, Stefano Stifani
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引用次数: 2

Abstract

As the resident immune cells of the healthy nervous system, homeostatic microglia can rapidly become activated in response to injury/disease. Dysregulated microglia activation is a hallmark of nervous system disorders including neurodegenerative diseases such as amyotrophic lateral sclerosis (ALS) and Alzheimer's disease. The elucidation of the biological and pathological roles of microglia has recently benefitted from the development of microglia-like cells using human induced pluripotent stem cell (iPSC)-based approaches. The success of iPSC-derived microglia preparations as a disease-relevant model system depends on their representation of the in vivo spatial and temporal heterogeneity of microglia under pathological conditions. Little is currently known about the potential of human iPSC-derived microglia generated using different methods for the study of neurodegenerative diseases. We compared the transcriptomes of human iPSC-derived microglia generated using two frequently used in vitro differentiation methods to determine whether separate strategies can generate microglia with distinct transcriptional signatures in vitro. We show that microglia derived using different differentiation methods display distinct maturation characteristics after equivalent times in culture. We also reveal that iPSC-derived microglia preparations generated using these two methods are composed of different subpopulations with transcriptomic signatures resembling those of in vivo regionally distinct microglia subtypes, specifically white-matter and gray-matter microglia. These findings highlight the need to better characterize the subtype composition of each microglia preparation prior to its use to model neurodegenerative diseases.

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比较不同人类ipsc分化方法生成的小胶质细胞制剂的特征,以模拟神经退行性疾病。
作为健康神经系统的常驻免疫细胞,稳态小胶质细胞可以在损伤/疾病反应中迅速被激活。小胶质细胞激活失调是神经系统疾病的标志,包括神经退行性疾病,如肌萎缩侧索硬化症(ALS)和阿尔茨海默病。近年来,基于人类诱导多能干细胞(iPSC)的小胶质细胞样细胞的发展使小胶质细胞的生物学和病理学作用得到了阐明。ipsc衍生的小胶质细胞制剂作为疾病相关模型系统的成功取决于它们在病理条件下对小胶质细胞在体内空间和时间异质性的表征。目前,人们对不同方法产生的人类ipsc衍生小胶质细胞用于神经退行性疾病研究的潜力知之甚少。我们比较了使用两种常用的体外分化方法生成的人类ipsc衍生的小胶质细胞的转录组,以确定不同的策略是否可以在体外产生具有不同转录特征的小胶质细胞。我们发现,使用不同分化方法获得的小胶质细胞在同等培养时间后表现出不同的成熟特征。我们还发现,使用这两种方法生成的ipsc衍生的小胶质细胞制剂由不同的亚群组成,其转录组特征类似于体内区域不同的小胶质细胞亚型,特别是白质和灰质小胶质细胞。这些发现强调了在用于神经退行性疾病模型之前,需要更好地表征每种小胶质细胞制剂的亚型组成。
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来源期刊
ASN NEURO
ASN NEURO NEUROSCIENCES-
CiteScore
7.70
自引率
4.30%
发文量
35
审稿时长
>12 weeks
期刊介绍: ASN NEURO is an open access, peer-reviewed journal uniquely positioned to provide investigators with the most recent advances across the breadth of the cellular and molecular neurosciences. The official journal of the American Society for Neurochemistry, ASN NEURO is dedicated to the promotion, support, and facilitation of communication among cellular and molecular neuroscientists of all specializations.
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