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RNA-Mediated Reprogramming of Primary Adult Human Dermal Fibroblasts into c-kit(+) Cardiac Progenitor Cells

机译:RNA介导的初级成年人类皮肤成纤维细胞重编程为c-kit(+)心脏祖细胞。

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摘要

Cardiovascular disease is the leading cause of death in the United States. Heart failure is a common, costly, and potentially fatal condition that is inadequately managed by pharmaceuticals. Cardiac repair therapies are promising alternative options. A potential cardiac repair therapy involves reprogramming human fibroblasts toward an induced cardiac progenitor-like state. We developed a clinically useful and safer reprogramming method by nonintegrative delivery of a cocktail of cardiac transcription factor-encoding mRNAs into autologous human dermal fibroblasts obtained from skin biopsies. Using this method, adult and neonatal dermal fibroblasts were reprogrammed into cardiac progenitor cells (CPCs) that expressed c-kit, Isl-1, and Nkx2.5. Furthermore, these reprogrammed CPCs differentiated into cardiomyocytes (CMs) in vitro as judged by increased expression of cardiac troponin T, -sarcomeric actinin, RyR2, and SERCA2 and displayed enhanced caffeine-sensitive calcium release. The ability to reprogram patient-derived dermal fibroblasts into c-kit(+) CPCs and differentiate them into functional CMs provides clinicians with a potential new source of CPCs for cardiac repair from a renewable source and an alternative therapy in the treatment of heart failure.
机译:在美国,心血管疾病是主要的死亡原因。心力衰竭是一种常见,昂贵且可能致命的疾病,无法通过药物加以管理。心脏修复疗法是有前途的替代选择。潜在的心脏修复疗法涉及将人成纤维细胞重编程为诱导的心脏祖细胞样状态。我们通过将心脏转录因子编码mRNA的混合物非整合递送至从皮肤活检获得的自体人类皮肤成纤维细胞中,开发了一种临床上有用且更安全的重编程方法。使用这种方法,将成年和新生儿的真皮成纤维细胞重新编程为表达c-kit,Isl-1和Nkx2.5的心脏祖细胞(CPC)。此外,根据心脏肌钙蛋白T,肌氨酸肌动蛋白,RyR2和SERCA2表达的增加判断,这些重新编程的CPC在体外分化为心肌细胞(CMs),并显示出增强的咖啡因敏感性钙释放。将患者来源的皮肤成纤维细胞重编程为c-kit(+)CPC并将其分化为功能性CM的能力为临床医生提供了潜在的CPC的新来源,可从可再生来源和替代疗法治疗心脏衰竭中进行心脏修复。

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