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首页> 外文期刊>Cellular Physiology and Biochemistry >Cardiac Myocytes Derived from Murine Reprogrammed Fibroblasts: Intact Hormonal Regulation, Cardiac Ion Channel Expression and Development of Contractility
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Cardiac Myocytes Derived from Murine Reprogrammed Fibroblasts: Intact Hormonal Regulation, Cardiac Ion Channel Expression and Development of Contractility

机译:鼠重编程成纤维细胞衍生的心肌细胞:完整的激素调节,心脏离子通道表达和收缩力的发展。

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Aims: Induced pluripotent stem (iPS) cells have a developmental potential similar to that of blastocyst-derived embryonic stem (ES) cells and may serve as an autologous source of cells for tissue repair, in vitro disease modelling and toxicity assays. Here we aimed at generating iPS cell-derived cardiomyocytes (CMs) and comparing their molecular and functional characteristics with CMs derived from native murine ES cells. Methods and Results: Beating cardiomyocytes were generated using a mass culture system from murine N10 and O9 iPS cells as well as R1 and D3 ES cells. Transcripts of the mesoderm specification factor T-brachyury and non-atrial cardiac specific genes were expressed in differentiating iPS EBs. Using immunocytochemistry to determine the expression and intracellular organisation of cardiac specific structural proteins we demonstrate strong similarity between iPS-CMs and ES-CMs. In line with a previous study electrophysiological analyses showed that hormonal response to beta-adrenergic and muscarinic receptor stimulation was intact. Action potential (AP) recordings suggested that most iPS-CMs measured up to day 23 of differentiation are of ventricular-like type. Application of lidocaine, Cs+, SEA0400 and verapamil+nifedipine to plated iPS-EBs during multielectrode array (MEA) measurements of extracellular field potentials and intracellular sharp electrode recordings of APs revealed the presence of I-Na, I-f, I-NCX, and I-CaL, respectively, and suggested their involvement in cardiac pacemaking, with I-CaL being of major importance. Furthermore, iPS-CMs developed and conferred force to avitalized ventricular tissue that was responsive to adrenergic stimulation. Conclusions: Our data demonstrate that the cardiogenic potential of iPS cells is comparable to that of ES cells and that iPS-CMs possess all fundamental functional elements of a typical cardiac cell, including spontaneous beating, hormonal regulation, cardiac ion channel expression and contractility. Therefore, iPS-CMs can be regarded as a potentially valuable source of cells for in vitro studies and cellular cardiomyoplasty. Copyright
机译:目的:诱导多能干(iPS)细胞具有与囊胚来源的胚胎干(ES)细胞相似的发展潜力,并可作为组织修复,体外疾病建模和毒性测定的自体细胞来源。在这里,我们旨在生成iPS细胞来源的心肌细胞(CM),并将其分子和功能特征与天然鼠ES细胞衍生的CM进行比较。方法和结果:使用大规模培养系统从鼠的N10和O9 iPS细胞以及R1和D3 ES细胞中产生搏动的心肌细胞。中胚层特异性因子T-brachyury和非心房性心脏特异性基因的转录物在分化iPS EB中表达。使用免疫细胞化学确定心脏特异性结构蛋白的表达和细胞内组织,我们证明了iPS-CM和ES-CM之间的强相似性。与先前的研究一致,电生理分析表明,激素对β-肾上腺素和毒蕈碱受体刺激的反应是完整的。动作电位(AP)记录表明,直到分化的第23天,大多数iPS-CM都是心室样类型的。在多电极阵列(MEA)对APs的细胞外场电势和细胞内尖电极记录的多电极阵列(MEA)测量中,利多卡因,Cs +,SEA0400和维拉帕米+硝苯地平在平板iPS-EB上的应用表明,存在I-Na,If,I-NCX和I -CaL,并建议它们参与心脏起搏,其中I-CaL是最重要的。此外,iPS-CM发育并赋予了对肾上腺素能刺激有反应的无活性心室组织力。结论:我们的数据表明,iPS细胞的心源性潜力与ES细胞相当,并且iPS-CM具有典型心脏细胞的所有基本功能要素,包括自发搏动,激素调节,心脏离子通道表达和收缩力。因此,iPS-CMs可被认为是用于体外研究和细胞心肌成形术的潜在有价值的细胞来源。版权

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