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Engineered heart tissue graft derived from somatic cell nuclear transferred embryonic stem cells improve myocardial performance in infarcted rat heart

机译:从体细胞核移植的胚胎干细胞衍生的工程心脏组织移植物改善了梗塞大鼠心脏的心肌性能

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摘要

The concept of regenerating diseased myocardium by implanting engineered heart tissue (EHT) is intriguing. Yet it was limited by immune rejection and difficulties to be generated at a size with contractile properties. Somatic cell nuclear transfer is proposed as a practical strategy for generating autologous histocompatible stem (nuclear transferred embryonic stem [NT-ES]) cells to treat diseases. Nevertheless, it is controversial as NT-ES cells may pose risks in their therapeutic application. EHT from NT-ES cell-derived cardiomyocytes was generated through a series of improved techniques in a self-made mould to keep the EHTs from contraction and provide static stretch simultaneously. After 7 days of static and mechanical stretching, respectively, the EHTs were implanted to the infarcted rat heart. Four weeks after transplantation, the suitability of EHT in heart muscle repair after myocardial infarction was evaluated by histological examination, echocardiography and multielectrode array measurement. The results showed that large (thickness/diameter, 2–4 mm/10 mm) spontaneously contracting EHTs was generated successfully. The EHTs, which were derived from NT-ES cells, inte grated and electrically coupled to host myocardium and exerted beneficial effects on the left ventricular function of infarcted rat heart. No teratoma formation was observed in the rat heart implanted with EHTs for 4 weeks. NT-ES cells can be used as a source of seeding cells for cardiac tissue engineering. Large contractile EHT grafts can be constructed in vitro with the ability to survive after implantation and improve myocardial performance of infarcted rat hearts.
机译:通过植入工程心脏组织(EHT)再生患病心肌的概念很有趣。然而,它受到免疫排斥和难以产生具有收缩特性的大小的限制。提出将体细胞核转移作为一种产生自体组织相容性干细胞(核转移的胚胎干[NT-ES])以治疗疾病的实用策略。然而,这是有争议的,因为NT-ES细胞可能会在其治疗应用中带来风险。 NT-ES细胞来源的心肌细胞的EHT是通过一系列改良技术在自制模具中生成的,以防止EHT收缩并同时提供静态拉伸。分别在静态和机械拉伸7天后,将EHTs植入梗塞的大鼠心脏。移植后四周,通过组织学检查,超声心动图和多电极阵列测量评估EHT在心肌梗死后心肌修复中的适用性。结果表明,成功生成了大(厚度/直径,2-4 mm / 10 mm)自发收缩的EHT。源自NT-ES细胞的EHT整合并电耦合至宿主心肌,并对梗塞大鼠心脏的左心室功能产生有益作用。在植入EHT的大鼠心脏中,连续4周未观察到畸胎瘤形成。 NT-ES细胞可以用作心脏组织工程的种子细胞来源。可以体外构建大型可收缩的EHT移植物,使其具有在植入后存活并改善梗死大鼠心脏的心肌性能的能力。

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