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使用单细胞红外光谱法研究全反式维甲酸(ATRA)和合成类视黄醇类似物(EC19和EC23)对人多能干细胞分化的作用。

The action of all-trans-retinoic acid (ATRA) and synthetic retinoid analogues (EC19 and EC23) on human pluripotent stem cells differentiation investigated using single cell infrared microspectroscopy.

作者信息

Clemens Graeme, Flower Kevin R, Henderson Andrew P, Whiting Andrew, Przyborski Stefan A, Jimenez-Hernandez Melody, Ball Francis, Bassan Paul, Cinque Gianfelice, Gardner Peter

机构信息

Manchester Institute of Biotechnology, Manchester University, 131 Princess Street, Manchester, M1 7DN, UK.

出版信息

Mol Biosyst. 2013 Apr 5;9(4):677-92. doi: 10.1039/c3mb25505k.

Abstract

All trans-retinoic acid (ATRA) is widely used to direct the differentiation of cultured stem cells. When exposed to the pluripotent human embryonal carcinoma (EC) stem cell line, TERA2.cl.SP12, ATRA induces ectoderm differentiation and the formation of neuronal cell types. We have previously generated synthetic analogues of retinoic acid (EC23 and EC19) which also induce the differentiation of EC cells. Even though EC23 and EC19 have similar chemical structures, they have differing biochemical effects in terms of EC cell differentiation. EC23 induces neuronal differentiation in a manner similar to ATRA, whereas EC19 directs the cells to form epithelial-like derivatives. Previous MALDI-TOF MS analysis examined the response of TERA2.cl.SP12 cells after exposure to ATRA, EC23 and EC19 and further demonstrated the similarly in the effect of ATRA and EC23 activity whilst responses to EC19 were very different. In this study, we show that Fourier Transform Infrared Micro-Spectroscopy (FT-IRMS) coupled with appropriate scatter correction and multivariate analysis can be used as an effective tool to further investigate the differentiation of human pluripotent stem cells and monitor the alternative affects different retinoid compounds have on the induction of differentiation. FT-IRMS detected differences between cell populations as early as 3 days of compound treatment. Populations of cells treated with different retinoid compounds could easily be distinguished from one another during the early stages of cell differentiation. These data demonstrate that FT-IRMS technology can be used as a sensitive screening technique to monitor the status of the stem cell phenotype and progression of differentiation along alternative pathways in response to different compounds.

摘要

全反式维甲酸(ATRA)被广泛用于指导培养的干细胞分化。当暴露于多能性人类胚胎癌(EC)干细胞系TERA2.cl.SP12时,ATRA诱导外胚层分化并形成神经元细胞类型。我们之前已经合成了维甲酸的类似物(EC23和EC19),它们也能诱导EC细胞分化。尽管EC23和EC19具有相似的化学结构,但它们在EC细胞分化方面具有不同的生化效应。EC23以类似于ATRA的方式诱导神经元分化,而EC19则引导细胞形成上皮样衍生物。先前的基质辅助激光解吸电离飞行时间质谱(MALDI-TOF MS)分析检测了TERA2.cl.SP12细胞在暴露于ATRA、EC23和EC19后的反应,进一步证明了ATRA和EC23活性效应的相似性,而对EC19的反应则非常不同。在本研究中,我们表明,傅里叶变换红外显微光谱(FT-IRMS)结合适当的散射校正和多变量分析可以用作进一步研究人类多能干细胞分化并监测不同类视黄醇化合物对诱导分化的替代影响的有效工具。FT-IRMS早在化合物处理3天时就检测到细胞群体之间的差异。在细胞分化的早期阶段,用不同类视黄醇化合物处理的细胞群体很容易相互区分。这些数据表明,FT-IRMS技术可以用作一种灵敏的筛选技术,以监测干细胞表型的状态以及响应不同化合物沿着替代途径的分化进程。

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