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Effect of ROCK inhibitor Y-27632 on normal and variant human embryonic stem cells (hESCs) in vitro: Its benefits in hESC expansion

机译:ROCK抑制剂Y-27632对正常和变异人类胚胎干细胞(hESCs)的体外影响:其对hESC扩增的益处

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The Rho associated coiled coil protein kinase (ROCK) dependent signaling pathway plays an important role in numerous physiological functions such as cell proliferation, adhesion, migration and inflammation. Human embryonic stem cells (hESCs) undergo differentiation and poor survival after single cell dissociation in culture thus limiting their expansion for cell based therapies. We evaluated the role of the selective ROCK inhibitor Y-27632 on hESC colonies and disassociated single hESCs from two different hESC lines. Karyotypically normal hESCs (HES3) and variant hESCs (BG01V) were treated with Y-27632 at 5, 10 and 20 μM concentrations for 72 h and its effects on hESC self renewal, colony morphology, cell cycle and pluripotency were evaluated. Increased cell proliferation of both HES3 and BG01V were observed for all three concentrations compared to untreated controls following passaging of cell clusters or dissociated single cells and some of these increases were statistically significant. Cell cycle assay demonstrated normal cell cycle progression with no peaks evident of apoptosis. No morphological differentiation was evident following treatment with the highest concentration of Y-27632 (20 μM) and the stemness related genes continued to be highly expressed in both HES3 and BG01V cells compared to untreated controls. The results confirmed that Y-27632 is a useful agent that aids in the expansion of undifferentiated hESC numbers for downstream applications in regenerative medicine.
机译:Rho相关的卷曲螺旋蛋白激酶(ROCK)依赖性信号通路在许多生理功能(例如细胞增殖,粘附,迁移和炎症)中起重要作用。人类胚胎干细胞(hESCs)在培养中的单细胞解离后经历分化和较差的存活,因此限制了它们在基于细胞的疗法中的扩展。我们评估了选择性ROCK抑制剂Y-27632对hESC集落和来自两个不同hESC系的分离的单个hESC的作用。用Y-27632在5、10和20μM浓度下处理核型正常的hESC(HES3)和变异的hESC(BG01V)72小时,并评估其对hESC自我更新,菌落形态,细胞周期和多能性的影响。与未处理的对照相比,在细胞簇或解离的单细胞传代后,所有三种浓度的HES3和BG01V的细胞增殖均增加,其中一些增加具有统计学意义。细胞周期分析表明细胞周期正常进行,没有明显的凋亡峰。与未处理的对照组相比,用最高浓度的Y-27632(20μM)处理后,没有形态学分化,并且与干性相关的基因在HES3和BG01V细胞中继续高表达。结果证实,Y-27632是有用的试剂,有助于扩大未分化的hESC数,用于再生医学的下游应用。

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