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三维自组装肽基质增强类胚体的形成及其神经元分化。

Three-dimensional self-assembling peptide matrix enhances the formation of embryoid bodies and their neuronal differentiation.

作者信息

Li Qianqian, Chow King L, Chau Ying

机构信息

Department of Chemical and Biomolecular Engineering, The Hong Kong University of Science and Technology, Clear Water Bay, Kowloon, Hong Kong, Republic of China.

出版信息

J Biomed Mater Res A. 2014 Jun;102(6):1991-2000. doi: 10.1002/jbm.a.34876. Epub 2013 Jul 30.

Abstract

We have tailored the properties of a self-assembling peptide (SAP) matrix to direct embryonic stem cells towards neuronal differentiation by adopting a three-dimensional (3D) culture, matching mechanical strength with that of neural tissue, and incorporating fixed laminin-derived pentapeptide signals (IKVAV). We report here that such a matrix alone can induce mouse embryonic stem (ES) cells to first develop into embryoid body (EB) and increase their propensity for subsequent neuronal differentiation. Embryoid bodies were observed by day 5 of culture in SAP matrix. βIII-tubulin as an early neuronal commitment marker was more prominently detected in cells cultured in the matrix containing IKVAV signals. Interestingly, ES-derived cells did not display distinct neuron morphology within the 3D culture; however, 55 ± 10% of those cells within IKVAV conjugated matrix and 38 ± 6% of those within base matrix displayed higher potential towards neuronal differentiation after 7 days. When retrieved and recultured on a tissue culture plate, they exhibited extended neurite outgrowths and networks in the absence of any additional neuronal differentiation growth factor. The up-regulated expression of neuronal development markers (MAP2 and MeCP2) and the down-regulation of glial marker (GFAP) support that further neuronal differentiation takes place upon reculture. The results showed that an artificial matrix composed of designer SAPs could prompt the formation of EB and provides the cues favoring neuronal differentiation of ES cells.

摘要

我们通过采用三维(3D)培养方式,使自组装肽(SAP)基质的特性与神经组织的机械强度相匹配,并掺入固定的层粘连蛋白衍生五肽信号(IKVAV),从而引导胚胎干细胞向神经元分化。我们在此报告,这样的基质 alone 就能诱导小鼠胚胎干(ES)细胞首先发育成胚状体(EB),并增加其随后神经元分化的倾向。在 SAP 基质中培养 5 天时观察到了胚状体。作为早期神经元定向标志物的βIII -微管蛋白在含有 IKVAV 信号的基质中培养的细胞中检测更为显著。有趣的是,ES 来源的细胞在 3D 培养中未显示出明显的神经元形态;然而,7 天后,IKVAV 偶联基质中的那些细胞中有 55±10%以及基础基质中的那些细胞中有 38±6%显示出更高的神经元分化潜能。当将它们取出并重新培养在组织培养板上时,在没有任何额外神经元分化生长因子的情况下,它们表现出延长的神经突生长和网络形成。神经元发育标志物(MAP2 和 MeCP2)的上调表达以及胶质标志物(GFAP)的下调表达支持了重新培养后进一步的神经元分化发生。结果表明,由定制的 SAP 组成的人工基质可以促使 EB 的形成,并提供有利于 ES 细胞神经元分化的线索。

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