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通过正向编程产生人内嗅星状细胞样细胞显示出Foxp1在重编程中的重要作用。

Production of human entorhinal stellate cell-like cells by forward programming shows an important role of Foxp1 in reprogramming.

作者信息

Bergmann Tobias, Liu Yong, Skov Jonathan, Mogus Leo, Lee Julie, Pfisterer Ulrich, Handfield Louis-Francois, Asenjo-Martinez Andrea, Lisa-Vargas Irene, Seemann Stefan E, Lee Jimmy Tsz Hang, Patikas Nikolaos, Kornum Birgitte Rahbek, Denham Mark, Hyttel Poul, Witter Menno P, Gorodkin Jan, Pers Tune H, Hemberg Martin, Khodosevich Konstantin, Hall Vanessa Jane

机构信息

Group of Brain Development and Disease, Department of Veterinary and Animal Sciences, Faculty of Health and Medical Sciences, University of Copenhagen, Frederiksberg, Denmark.

Novo Nordisk Foundation Center for Stem Cell Research, DanStem University of Copenhagen, Copenhagen, Denmark.

出版信息

Front Cell Dev Biol. 2022 Aug 15;10:976549. doi: 10.3389/fcell.2022.976549. eCollection 2022.

Abstract

Stellate cells are principal neurons in the entorhinal cortex that contribute to spatial processing. They also play a role in the context of Alzheimer's disease as they accumulate Amyloid beta early in the disease. Producing human stellate cells from pluripotent stem cells would allow researchers to study early mechanisms of Alzheimer's disease, however, no protocols currently exist for producing such cells. In order to develop novel stem cell protocols, we characterize at high resolution the development of the porcine medial entorhinal cortex by tracing neuronal and glial subtypes from mid-gestation to the adult brain to identify the transcriptomic profile of progenitor and adult stellate cells. Importantly, we could confirm the robustness of our data by extracting developmental factors from the identified intermediate stellate cell cluster and implemented these factors to generate putative intermediate stellate cells from human induced pluripotent stem cells. Six transcription factors identified from the stellate cell cluster including , , , , , were overexpressed using a forward programming approach to produce neurons expressing a unique combination of , , and BCL11B observed in stellate cells. Further analyses of the individual transcription factors led to the discovery that is critical in the reprogramming process and omission of and enhances neuron conversion. Our findings contribute not only to the profiling of cell types within the developing and adult brain's medial entorhinal cortex but also provides proof-of-concept for using scRNAseq data to produce entorhinal intermediate stellate cells from human pluripotent stem cells .

摘要

星状细胞是内嗅皮质中的主要神经元,有助于空间处理。它们在阿尔茨海默病的背景中也发挥作用,因为它们在疾病早期就会积累β淀粉样蛋白。从多能干细胞中产生人类星状细胞将使研究人员能够研究阿尔茨海默病的早期机制,然而,目前还没有产生此类细胞的方案。为了开发新的干细胞方案,我们通过追踪从妊娠中期到成年大脑的神经元和神经胶质亚型,以高分辨率表征猪内侧内嗅皮质的发育,以确定祖细胞和成年星状细胞的转录组谱。重要的是,我们可以通过从鉴定出的中间星状细胞簇中提取发育因子来确认我们数据的稳健性,并利用这些因子从人类诱导多能干细胞中生成假定的中间星状细胞。使用正向编程方法过表达从星状细胞簇中鉴定出的六个转录因子,包括 、 、 、 、 、 ,以产生表达在星状细胞中观察到的 、 、 和BCL11B独特组合的神经元。对单个转录因子的进一步分析发现, 在重编程过程中至关重要,而省略 和 可增强神经元转化。我们的研究结果不仅有助于对发育中和成年大脑内侧内嗅皮质内的细胞类型进行分析,还为利用单细胞RNA测序数据从人类多能干细胞中产生内嗅中间星状细胞提供了概念验证。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/77e8/9420913/4cd1f172eac1/fcell-10-976549-g001.jpg

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