Reprogramming rat astrocytes into neurons using small molecules for cell replacement following intracerebral hemorrhage

Brain Science Advances Pub Date : 2021-09-01 DOI:10.26599/BSA.2021.9050009

Yang-yang Feng, Shuang Bai, Gaigai Li, H. Nie, Shiling Chen, Chao Pan, Ping Zhang, Yingxin Tang, Na Liu, Zhouping Tang

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引用次数: 3

Abstract

Astrocytes are promising source cells to replace neurons lost to disease owing to a shared lineage and capacities for dedifferentiation and proliferation under pathological conditions. Reprogramming of astrocytes to neurons has been achieved by transcription factor modulation, but reprogramming in vitro or in vivo using small‐molecule drugs may have several advantages for clinical application. For instance, small molecules can be extensively characterized for efficacy, toxicity, and tumorigenicity in vitro; induce rapid initiation and subsequent reversal of transdifferentiation upon withdrawal, and obviate the need for exogenous gene transfection. Here we report a new astrocyte–neuron reprogramming strategy using a combination of small molecules (0.5 mM valproic acid, 1 μM RepSox, 3 μM CHIR99021, 2 μM I‐BET151, 10 μM ISX‐9, and 10 μM forskolin). Treatment with this drug combination gradually reduced expression levels of astroglial marker proteins (glial fibrillary acidic protein and S100), transiently enhanced expression of the neuronal progenitor marker doublecortin, and subsequently elevated expression of the mature neuronal marker NeuN in primary astrocyte cultures. These changes were accompanied by transition to a neuron‐like morphological phenotype and expression of multiple neuronal transcription factors. Further, this drug combination induced astrocyte‐to‐neuron transdifferentiation in a culture model of intracerebral hemorrhage (ICH) and upregulated many transdifferentiation‐associated signaling molecules in ICH model rats. In culture, the drug combination also reduced ICH model‐associated oxidative stress, apoptosis, and pro‐inflammatory cytokine production. Neurons derived from small‐molecule reprogramming of astrocytes in adult Sprague–Dawley rats demonstrated long‐term survival and maintenance of neuronal phenotype. This small‐molecule‐induced astrocyte‐to‐neuron transdifferentiation method may be a promising strategy for neuronal replacement therapy.

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脑出血后用小分子细胞替代将大鼠星形胶质细胞重新编程为神经元

星形胶质细胞是一种很有前途的来源细胞，可以取代因疾病而失去的神经元，因为它们有着共同的谱系和在病理条件下去分化和增殖的能力。星形胶质细胞向神经元的重新编程已经通过转录因子调节实现，但使用小分子药物在体外或体内重新编程可能具有临床应用的几个优势。例如，小分子可以在体外广泛表征其功效、毒性和致瘤性；在退出时诱导转分化的快速启动和随后的逆转，并且不需要外源基因转染。在这里，我们报道了一种新的星形细胞-神经元重编程策略，使用小分子（0.5 mM丙戊酸、1μM RepSox、3μM CHIR99021、2μM I‐BET151、10μM ISX‐9和10μM毛喉素）的组合。该药物组合的治疗逐渐降低了星形胶质细胞标志物蛋白（胶质原纤维酸性蛋白和S100）的表达水平，短暂增强了神经元祖细胞标志物双皮质素的表达，随后在原代星形细胞培养物中提高了成熟神经元标志物NeuN的表达。这些变化伴随着向神经元样形态表型的转变和多种神经元转录因子的表达。此外，该药物组合在脑出血（ICH）培养模型中诱导星形胶质细胞到神经元的转分化，并在ICH模型大鼠中上调许多转分化相关的信号分子。在培养中，药物组合还减少了ICH模型相关的氧化应激、细胞凋亡和促炎细胞因子的产生。成年Sprague-Dawley大鼠星形胶质细胞小分子重编程产生的神经元表现出神经元表型的长期存活和维持。这种小分子诱导的星形细胞到神经元的转分化方法可能是一种很有前途的神经元替代治疗策略。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Brain Science Advances

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10 weeks