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首页> 外文期刊>Stem cell research >Hepatocyte-like cells derived from human amniotic epithelial, bone marrow, and adipose stromal cells display enhanced functionality when cultured on decellularized liver substrate
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Hepatocyte-like cells derived from human amniotic epithelial, bone marrow, and adipose stromal cells display enhanced functionality when cultured on decellularized liver substrate

机译:衍生自人羊膜上皮,骨髓和脂肪基质细胞的肝细胞样细胞在脱细胞肝基质上培养时显示出增强的功能

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Transplantation of primary hepatocytes has been used in treatments for various liver pathologies and end-stage liver disease. However, shortage of donor tissue and the inability of hepatocyte proliferation in vitro have lead to alternative methods such as stem cell-derived hepatocyte-like cells (HLCs). Mesenchymal stromal/stem cells, and amniotic epithelial cells were isolated from human bone marrow (BM-MSCs), lipoaspirates (ASCs), and amniotic tissue (AECs) respectively. All cells were differentiated into HLCs on plates coated with Type I collagen or Porcine Liver Extracellular Matrix (PLECM-AA) matrix. Flow cytometry of BM-MSCs and ASCs, and AECs showed high expression of MSC-specific and embryonic stem cell markers respectively. All cell types differentiated into osteocytes, chondrocytes, and adipocytes. All cell type-derived HLCs presented the typical cuboidal primary hepatocyte morphology on PLECM-AA and fewer vacuoles (AECs) compared to HLCs cultured on type I collagen. Gene analysis of all cell type-derived HLCs cultured on PLECM-AA revealed higher upregulation of genes involved in drug transportation and metabolism compared to HLCs cultured on type I collagen. Although, HLCs cultured on PLECM-AA displayed some hepatocyte-related function and bioactivity, overall gene expression was lower compared to that of primary hepatocytes suggesting that caution should be taken when considering using HLCs to replace total hepatocyte functionality.
机译:原发性肝细胞的移植已用于治疗各种肝脏病理和终末期肝病。然而,供体组织的短缺和体外肝细胞增殖的不稳定导致替代方法,例如干细胞衍生的肝细胞样细胞(HLC)。分别从人骨髓(BM-MSCs),脂孢子物(ASCS)和羊膜组织(AECS)中分离间充质基质/干细胞和羊皮上皮细胞。将所有细胞与涂有I型胶原蛋白或猪肝细胞外基质(PLECM-AA)基质的平板上的HLC分化为HLC。 BM-MSCs和ASC的流式细胞术,AECs分别显示出高表达MSC特异性和胚胎干细胞标志物。所有细胞类型分为骨细胞,软骨细胞和脂肪细胞。与I型胶原蛋白培养的HLC相比,所有细胞类型衍生的HLC呈现典型的立方​​体初级肝细胞形态和较少的液压渣(AECS)。与在I型胶原蛋白上培养的HLC相比,对PLECM-AA培养的所有细胞类型衍生HLC的基因分析显示出涉及药物运输和代谢的基因更高。尽管,在PLECM-AA上培养的HLC显示出一些肝细胞相关的功能和生物活性,但与原发性肝细胞相比,总体基因表达较低,表明应在考虑使用HLC替代总肝细胞官能度时注意谨慎。

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