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不同来源的人诱导多能干细胞的体内肝脏再生潜力。

In vivo liver regeneration potential of human induced pluripotent stem cells from diverse origins.

机构信息

Sidney Kimmel Comprehensive Cancer Center, Johns Hopkins University School of Medicine, Baltimore, MD 21231, USA.

出版信息

Sci Transl Med. 2011 May 11;3(82):82ra39. doi: 10.1126/scitranslmed.3002376.

Abstract

Human induced pluripotent stem cells (iPSCs) are a potential source of hepatocytes for liver transplantation to treat end-stage liver disease. In vitro differentiation of human iPSCs into hepatic cells has been achieved using a multistage differentiation protocol, but whether these cells are functional and capable of engrafting and regenerating diseased liver tissue is not clear. We show that human iPSC-derived hepatic cells at various differentiation stages can engraft the liver in a mouse transplantation model. Using the same differentiation and transplantation protocols, we also assessed the ability of human iPSCs derived from each of the three developmental germ layer tissues (that is, ectoderm, mesoderm, and endoderm) to regenerate mouse liver. These iPSC lines, with similar but distinct global DNA methylation patterns, differentiated into multistage hepatic cells with an efficiency similar to that of human embryonic stem cells. Human hepatic cells at various differentiation stages derived from iPSC lines of different origins successfully repopulated the liver tissue of mice with liver cirrhosis. They also secreted human-specific liver proteins into mouse blood at concentrations comparable to that of proteins secreted by human primary hepatocytes. Our results demonstrate the engraftment and liver regenerative capabilities of human iPSC-derived multistage hepatic cells in vivo and suggest that human iPSCs of distinct origins and regardless of their parental epigenetic memory can efficiently differentiate along the hepatic lineage.

摘要

人诱导多能干细胞(iPSCs)是肝移植治疗终末期肝病的潜在肝细胞来源。已经使用多步分化方案实现了将人 iPSC 体外分化为肝细胞,但这些细胞是否具有功能以及是否能够植入和再生病变的肝组织尚不清楚。我们表明,各种分化阶段的人 iPSC 衍生的肝细胞可以在小鼠移植模型中植入肝脏。使用相同的分化和移植方案,我们还评估了源自三个发育胚层组织(即外胚层、中胚层和内胚层)的每个组织的人 iPSC 再生小鼠肝脏的能力。这些 iPSC 系具有相似但不同的全基因组 DNA 甲基化模式,分化为多阶段肝细胞的效率与人类胚胎干细胞相似。源自不同来源的 iPSC 系的各种分化阶段的人肝细胞成功地将肝硬化小鼠的肝组织重新填充。它们还将人特异性肝蛋白分泌到小鼠血液中,其浓度与人原代肝细胞分泌的蛋白相当。我们的结果证明了人 iPSC 衍生的多阶段肝细胞在体内的植入和肝再生能力,并表明具有不同来源和与其亲本表观遗传记忆无关的人 iPSC 可以沿着肝系有效地分化。

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