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Coculture of Embryonic Ventricular Myocytes and Mouse Embryonic Stem Cell Enhance Intercellular Signaling by Upregulation of Connexin43

机译:胚胎心室肌细胞和小鼠胚胎干细胞的共培养通过连接蛋白43的上调增强细胞间信号传导。

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biBackground /i/bStem cell therapy has been proposed as a potential treatment strategy for ischemic cardiomyopathy in recent years. A variety of stem cells or stem cell-derived cells can potentially be used for transplantation. Despite improved cardiac function after treatment, one of the major problems is the poor integration between host and donor cells which can lead to post-transplantation arrhythmia and poor long-term outcome. biMethods /i/bIn the present study, we cocultured murine embryonic stem cells (mES) with murine embryonic ventricular myocytes (mEVs) in hanging drops to assess the cellular interaction and function of mES-derived cardiomyocytes under these conditions. biResults /i/bWe found that when mEVs are added to a culture system of embryonic stem cells, the number of spontaneously beating areas in embryoid bodies (EBs) increases, intercellular gap junction communication is enhanced by upregulation of Cx43 expression at the mid-developmental stage and Cx43 is distributed more orderly between cardiomyocytes. biConclusions /i/bOur findings suggest mES-derived cardiomyocytes are able to form effective signaling pathways through coculture with mEVs which is important for providing more functional grafts for cardiac cell therapy by improving the integration between transplanted and host cells.
机译:近年来,已经提出了 背景 干细胞疗法作为缺血性心肌病的潜在治疗策略。多种干细胞或干细胞衍生的细胞可潜在地用于移植。尽管治疗后心脏功能得到改善,但主要问题之一是宿主细胞与供体细胞之间的整合不良,这可能导致移植后心律失常和长期预后不良。 方法 在本研究中,我们将鼠胚胎干细胞(mES)与鼠胚胎心室肌细胞(mEVs)一起悬滴培养,以评估mES-的细胞相互作用和功能在这些条件下衍生的心肌细胞。 结果 我们发现,当将mEV添加到胚胎干细胞的培养系统中时,胚状体(EB)中自发搏动区域的数量增加,细胞间间隙连接通讯开始在发育中期通过Cx43表达的上调而增强,并且Cx43在心肌细胞之间更有序地分布。 结论 我们的研究结果表明,mES衍生的心肌细胞能够通过与mEV共培养形成有效的信号通路,这对于通过改善两者之间的整合为心脏细胞治疗提供更多功能性移植物至关重要移植和宿主细胞。

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