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Differentiation of human‐induced pluripotent stem cell under flow conditions to mature hepatocytes for liver tissue engineering

机译:流动条件下人诱导多能干细胞的分化对肝组织工程成熟肝细胞

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Abstract Hepatic differentiation of human‐induced pluripotent stem cells (hiPSCs) under flow conditions in a 3D scaffold is expected to be a major step forward for construction of bioartificial livers. The aims of this study were to induce hepatic differentiation of hiPSCs under perfusion conditions and to perform functional comparisons with fresh human precision‐cut liver slices (hPCLS), an excellent benchmark for the human liver in vivo. The majority of the mRNA expression of CYP isoenzymes and transporters and the tested CYP activities, Phase II metabolism, and albumin, urea, and bile acid synthesis in the hiPSC‐derived cells reached values that overlap those of hPCLS, which indicates a higher degree of hepatic differentiation than observed until now. Differentiation under flow compared with static conditions had a strong inducing effect on Phase II metabolism and suppressed AFP expression but resulted in slightly lower activity of some of the Phase I metabolism enzymes. Gene expression data indicate that hiPSCs differentiated into both hepatic and biliary directions. In conclusion, the hiPSC differentiated under flow conditions towards hepatocytes express a wide spectrum of liver functions at levels comparable with hPCLS indicating excellent future perspectives for the development of a bioartificial liver system for toxicity testing or as liver support device for patients.
机译:摘要在三维支架内流动条件下,人诱导多能干细胞(hiPSCs)的肝分化有望成为构建生物人工肝的一个重要步骤。本研究的目的是在灌注条件下诱导HIPSC的肝脏分化,并与新鲜人精确切割肝脏切片(hPCLS)进行功能比较,hPCLS是人体肝脏在体内的一个极好的基准。在hiPSC衍生细胞中,CYP同功酶和转运体的大部分mRNA表达以及检测的CYP活性、II期代谢、白蛋白、尿素和胆汁酸合成达到了与hPCLS重叠的值,这表明肝脏分化程度比目前观察到的更高。与静态条件相比,流动条件下的分化对II期代谢有强烈的诱导作用,并抑制AFP的表达,但导致一些I期代谢酶的活性稍低。基因表达数据表明hiPSCs分化为肝脏和胆汁方向。总之,在流向肝细胞的流动条件下分化的hiPSC在与hPCLS相当的水平上表达了广泛的肝功能,这表明了开发用于毒性试验的生物人工肝系统或作为患者肝脏支持装置的良好前景。

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