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Alterations in membrane potential promote neonatal cardiomyocyte proliferation

机译:膜电位的改变促进新生儿心肌细胞增殖

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Zebrafish and newt heart regeneration has been demonstrated to be the result of cardiomyocyte proliferation, which has suggested the feasibility of maintaining the proliferation capacity of native mammalian neonatal cardiomyocytes. Recent experiments demonstrating that stem cells are highly depolarized while terminally differentiated cells are hyperpolarized have indicated a potential role of membrane potential in maintaining a proliferative phenotype. In this study, we used titrated potassium gluconate and ouabain to depolarize primary neonatal rat cardiomyocytes and demonstrated the concomitant proliferative effect between postpartum day 3 (P3) and post partum day 7 (P7). After isolation, the cells were cultured for one day in normal media and before replacing the media with titrated depolarizing agents for four days. The effect of depolarization was validated by DiBAC, a slow-acting voltage-sensitive fluorescence dye. Total nuclei count and cardiomyocyte percentage were evaluated by microscopic cytometry. Cell cycle was analyzed by propidium iodide on flow cytometry. Both treatment groups had a dose dependent effect on cardiomyocyte percentage and induced proliferation at specific range of concentrations before eventually reaching toxic levels. A study of cell cycle showed increased populations of non-G0/G1 phase cardiomyocytes with treatment. Conclusion: We concluded that the control of membrane potential could modulate the proliferation of neonatal rat cardiomyocytes.
机译:斑马鱼和new的心脏再生已被证明是心肌细胞增殖的结果,这表明维持天然哺乳动物新生儿心肌细胞增殖能力的可行性。最近的实验表明干细胞高度去极化,而终末分化细胞超极化,表明膜电位在维持增殖表型中的潜在作用。在这项研究中,我们使用滴定的葡萄糖酸钾和哇巴因对新生鼠的心肌细胞去极化,并证明了产后第3天(P3)和产后第7天(P7)的并发增殖作用。分离后,将细胞在正常培养基中培养一天,然后用滴定的去极化剂替换培养基四天。去极化作用已通过DiBAC(一种缓慢作用的电压敏感荧光染料)进行了验证。通过显微细胞术评估总核数和心肌细胞百分比。在流式细胞仪上通过碘化丙啶分析细胞周期。两个治疗组对心肌细胞的百分比均具有剂量依赖性,并在特定浓度范围内诱导增殖,直至最终达到毒性水平。细胞周期研究显示,经过治疗,非G0 / G1期心肌细胞数量增加。结论:我们得出结论,膜电位的控制可以调节新生大鼠心肌细胞的增殖。

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