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Highly efficient differentiation of functional hepatocytes from human induced pluripotent stem cells

机译:从人诱导的多能干细胞中高效分化出功能性肝细胞

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Human induced pluripotent stem cells (hiPSCs)hold great potential for useinregenerative medicine, novel drug development, and disease progression/developmental studies. Here, we report highly efficient differentiation of hiPSCs toward a relatively homogeneous population of functional hepa-tocytes. hiPSC-derived hepatocytes (hiHs) not only showed a high expression of hepatocyte-specific proteins and liver-specific functions, but they also developed a functional biotransformation system including phase I and II metabolizing enzymes and phase III transporters. Nuclear receptors, which are critical for regulating the expression of metabolizing enzymes, were also expressed in hiHs. hiHs also responded to different compounds/inducers ofcytochrome P450 as mature hepatocytes do. To follow up on this observation, we analyzed the drug metabolizing capacity of hiHs in real time using a novel ultraperformance liquid chromatography-tandem mass spectrometry. We found that, like freshly isolated primary human hepatocytes, the seven major metabolic pathways of the drug bufuralol were found in hiHs. In addition, transplanted hiHs engrafted, integrated, and proliferated in livers of an immune-deficient mouse model, and secreted human albumin, indicating that hiHs also function in vivo. In conclusion, we have generated a method for the efficient generation of hepatocytes from induced pluripotent stem cells in vitro and in vivo, and it appears that the cells function similarly to primary human hepatocytes, including developing a complete metabolic function. These results represent asignificant step toward using patient/disease-specific hepatocytes for cell-based therapeutics as well as for pharmacology and toxicology studies.
机译:人诱导的多能干细胞(hiPSC)在再生医学,新药开发和疾病进展/发展研究中具有巨大潜力。在这里,我们报道了hiPSCs向功能肝细胞相对同质群体的高效分化。 hiPSC衍生的肝细胞(hiHs)不仅显示出肝细胞特异性蛋白的高表达和肝特异性功能,而且还开发了一种功能性生物转化系统,包括I和II期代谢酶和III期转运蛋白。在hiHs中也表达了对调节代谢酶表达至关重要的核受体。与成熟的肝细胞一样,hiHs对细胞色素P450的不同化合物/诱导物也有反应。为了跟踪该观察结果,我们使用新型超高效液相色谱-串联质谱实时分析了hiHs的药物代谢能力。我们发现,像新鲜分离的原代人肝细胞一样,bufuralol的七个主要代谢途径在hiHs中被发现。此外,移植的hiHs在免疫缺陷小鼠模型的肝脏中移植,整合和增殖,并分泌人白蛋白,表明hiHs在体内也起作用。总之,我们已经产生了一种在体外和体内从诱导的多能干细胞中高效产生肝细胞的方法,看来这些细胞的功能与人类原代肝细胞相似,包括发展出完整的代谢功能。这些结果代表了将患者/疾病特异性肝细胞用于基于细胞的治疗以及药理学和毒理学研究的重要一步。

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