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首页> 外文期刊>Regenerative Therapy >A heparin-modified thermoresponsive surface with heparin-binding epidermal growth factor-like growth factor for maintaining hepatic functions in vitro and harvesting hepatocyte sheets
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A heparin-modified thermoresponsive surface with heparin-binding epidermal growth factor-like growth factor for maintaining hepatic functions in vitro and harvesting hepatocyte sheets

机译:具有肝素结合表皮生长因子样生长因子的肝素修饰的热敏表面,可在体外维持肝功能并收集肝细胞片

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A heparin-modified thermoresponsive surface bound with heparin-binding epidermal growth factor-like growth factor (HB-EGF) was designed to allow creation of transferrable and functional hepatocyte sheets. A heparin-modified thermoresponsive surface was prepared by covalently tethering heparin onto poly(N-isopropylacrylamide-co-2-carboxyisopropylacrylamide)-grafted tissue culture polystyrene surfaces (Heparin-IC). HB-EGFs were able to stably bind to heparin-IC via affinity interaction. The survival of primary rat hepatocytes was maintained through HB-EGF-bound heparin-IC (HB-EGF/heparin-IC). Moreover, cultured rat primary hepatocytes on HB-EGF/heparin-IC exhibited higher albumin-secretion than hepatocytes cultured on PIPAAm-grafted and collagen-coated surfaces with soluble HB-EGF in the culture medium, regardless of whether soluble EGF was added. These results suggested that HB-EGF/heparin-IC is able to effectively maintain hepatic function via continuous signaling of HB-EGF. After a 4-day cultivation, the cultured hepatocytes on HB-EGF/heparin-IC detached as a cell sheet with fibronectin and HB-EGF only after the temperature was lowered to 20 ^oC. In addition, higher expression of hepatocyte-specific genes (albumin, hepatocyte nuclear factor 4 alpha, coagulation factor VII, and coagulation factor IX) in hepatocyte sheets was detected on HB-EGF/heparin-IC than on a PIPAAm surface with soluble HB-EGF, indicating that HB-EGF/heparin-IC suppressed the dedifferentiation of cultured hepatocytes. Hence, heparin-modified thermoresponsive surfaces bound with HB-EGF facilitate the fabrication of transferrable hepatocyte sheets with intact hepatic functions and have the potential to provide an in vitro culture system using functional hepatocyte sheet tissues, which may serve as an effective hepatocyte-based tissue engineering platform for liver disease treatments.
机译:设计与肝素结合的表皮生长因子样生长因子(HB-EGF)结合的肝素修饰的热响应性表面,以允许创建可转移的功能肝细胞片。通过将肝素共价束缚在聚(N-异丙基丙烯酰胺-co-2-羧基异丙基丙烯酰胺)接枝的组织培养聚苯乙烯表面(Heparin-IC)上,制备肝素修饰的热响应性表面。 HB-EGF能够通过亲和相互作用与肝素-IC稳定结合。通过结合HB-EGF的肝素-IC(HB-EGF /肝素-IC)维持原代大鼠肝细胞的存活。此外,无论是否添加可溶性EGF,在HB-EGF /肝素-IC上培养的大鼠原代肝细胞均比在PIPAAm移植的胶原表面上培养的具有可溶性HB-EGF的肝细胞分泌更高的白蛋白分泌。这些结果表明,HB-EGF /肝素-IC能够通过HB-EGF的连续信号传导有效地维持肝功能。培养4天后,仅在温度降低至20℃后,在HB-EGF /肝素-IC上培养的肝细胞与纤连蛋白和HB-EGF分离为细胞片。此外,在HB-EGF /肝素-IC上检测到的肝细胞特异性基因(白蛋白,肝细胞核因子4α,凝血因子VII和凝血因子IX)的表达高于在可溶性HB-E的PIPAAm表面上的表达。 EGF,表明HB-EGF /肝素-IC抑制了培养的肝细胞的去分化。因此,与HB-EGF结合的肝素修饰的热响应表面促进了具有完整肝功能的可转移肝细胞片的制造,并有可能提供使用功能性肝细胞片组织的体外培养系统,该组织可以用作有效的基于肝细胞的组织肝病治疗的工程平台。

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