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小分子增强成人人类皮肤成纤维细胞重编程为背侧前脑前体细胞的过程。

Small Molecules Enhance Reprogramming of Adult Human Dermal Fibroblasts to Dorsal Forebrain Precursor Cells.

作者信息

Edwards Nicole, McCaughey-Chapman Amy, Combrinck Catharina, Geiger Johannes, Connor Bronwen

机构信息

Department of Pharmacology and Clinical Pharmacology, Centre for Brain Research, School of Medical Science, Faculty of Medical and Health Sciences, University of Auckland, Auckland, New Zealand.

Ethris GmbH, Munich, Germany.

出版信息

Stem Cells Dev. 2022 Feb;31(3-4):78-89. doi: 10.1089/scd.2021.0130. Epub 2022 Jan 21.

Abstract

The development of human cell-based platforms for disease modeling, drug discovery, and regenerative therapy relies on robust and practical methods to derive high yields of relevant neuronal subtypes. Direct reprogramming strategies have sought to provide a means of deriving human neurons that mitigate the low conversion efficiencies, and protracted timing of human embryonic stem cell and induced pluripotent stem cell-derived neuron specification in vitro. However, few studies have demonstrated the direct conversion of adult human fibroblasts into multipotent neural precursors with the capacity to differentiate into cortical neurons with high efficiency. In this study, we demonstrate a reprogramming strategy using chemically modified mRNA encoding the proneural genes and coupled with small molecule supplementation to enhance the derivation of human-induced dorsal forebrain precursors directly from adult human dermal fibroblasts (aHDFs). Through transcriptional and phenotypic analysis of lineage-specific precursor and cortical neuron markers, we have demonstrated that this combined strategy significantly enhances the direct derivation of dorsal forebrain precursors from aHDFs, which, after timely exposure to defined differentiation media, gives rise to high yields of functional glutamatergic neurons. We propose that this combined strategy provides a highly tractable and efficient human cell-based platform for disease modeling and drug discovery.

摘要

用于疾病建模、药物发现和再生治疗的基于人类细胞的平台的发展依赖于强大且实用的方法来获得高产量的相关神经元亚型。直接重编程策略试图提供一种获得人类神经元的方法,以减轻体外人类胚胎干细胞和诱导多能干细胞衍生神经元定向分化的低转化效率和漫长时间。然而,很少有研究证明成人人类成纤维细胞能直接转化为具有高效分化为皮质神经元能力的多能神经前体细胞。在本研究中,我们展示了一种重编程策略,即使用编码神经前体基因的化学修饰mRNA,并辅以小分子添加剂,以增强直接从成人人类皮肤成纤维细胞(aHDFs)衍生人类诱导的背侧前脑前体细胞。通过对谱系特异性前体细胞和皮质神经元标志物的转录和表型分析,我们证明了这种联合策略显著增强了从aHDFs直接衍生背侧前脑前体细胞的能力,这些前体细胞在及时暴露于特定分化培养基后,可产生高产量的功能性谷氨酸能神经元。我们认为,这种联合策略为疾病建模和药物发现提供了一个高度易处理且高效的基于人类细胞的平台。

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