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Selection proliferation and differentiation of bone marrow-derived liver stem cells with a culture system containing cholestatic serum in vitro

机译:含胆汁淤积血清的培养系统对骨髓源性肝干细胞的选择增殖和分化

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摘要

AIM: To explore the feasibility of direct separation, selective proliferation and differentiation of the bone marrow-derived liver stem cells (BDLSC) from bone marrow cells with a culture system containing cholestatic serum in vitro.METHODS: Whole bone marrow cells of rats cultured in routine medium were replaced with conditioning selection media containing 20 mL/L, 50 mL/L, 70 mL/L, and 100 mL/L cholestatic sera, respectively, after they attached to the plates. The optimal concentration of cholestatic serum was determined according to the outcome of the selected cultures. Then the selected BDLSC were induced to proliferate and differentiate with the addition of hepatocyte growth factor (HGF). The morphology and phenotypic markers of BDLSC were characterized using immunohistochemistry, RT-PCR and electron microscopy. The metabolic functions of differentiated cells were also determined by glycogen staining and urea assay.RESULTS: Bone marrow cells formed fibroblast-like but not hepatocyte-like colonies in the presence of 20 mL/L cholestatic serum. In 70 mL/L cholestatic serum, BDLSC colonies could be selected but could not maintain good growth status. In 100 mL/L cholestatic serum, all of the bone marrow cells were unable to survive. A 50 mL/L cholestatic serum was the optimal concentration for the selection of BDLSC at which BDLSC could survive while the other populations of the bone marrow cells could not. The selected BDLSC proliferated and differentiated after HGF was added. Hepatocyte-like colony-forming units (H-CFU) then were formed. H-CFU expressed markers of embryonic hepatocytes (AFP, albumin and cytokeratin 8/18), biliary cells (cytokeratin 19), hepatocyte functional proteins (transthyretin and cytochrome P450-2b1), and hepatocyte nuclear factors (HNF-1α and HNF-3β). They also had glycogen storage and urea synthesis functions, two of the critical features of hepatocytes.CONCLUSION: The selected medium containing cholestatic serum can select BDLSC from whole bone marrow cells. It will be a new way to provide a readily available alternate source of cells for clinical hepatocyte therapy.
机译:目的:探讨含胆汁静息血清培养系统从骨髓细胞中直接分离,选择性增殖和分化骨髓源性肝干细胞(BDLSC)的可行性。方法:在体外培养的大鼠全骨髓细胞在将常规培养基附着到平板上后,分别用含有20 mL / L,50 mL / L,70 mL / L和100 mL / L胆汁抑制血清的条件选择培养基代替。根据所选培养物的结果确定胆汁淤积血清的最佳浓度。然后通过添加肝细胞生长因子(HGF)诱导所选的BDLSC增殖和分化。利用免疫组织化学,RT-PCR和电​​子显微镜对BDLSC的形态和表型标记进行了表征。结果:在20mL / L胆汁郁积的血清中,骨髓细胞形成了成纤维细胞样的集落,但没有形成肝细胞样的集落。在70 mL / L的胆汁​​淤积血清中,可以选择BDLSC菌落,但不能保持良好的生长状态。在100 mL / L的胆汁​​淤积血清中,所有骨髓细胞均无法存活。 50 mL / L的胆汁​​淤积血清是选择BDLSC的最佳浓度,在该浓度下BDLSC可以存活,而其他骨髓细胞则不能。加入HGF后,选定的BDLSC增殖并分化。然后形成肝细胞样集落形成单位(H-CFU)。 H-CFU表达了胚胎肝细胞(AFP,白蛋白和细胞角蛋白8/18),胆管细胞(细胞角蛋白19),肝细胞功能蛋白(运甲状腺素蛋白和细胞色素P450-2b1)和肝细胞核因子(HNF-1α和HNF-3β)的标志物)。它们还具有肝细胞的两个关键特征,即糖原存储和尿素合成功能。结论:所选的含胆汁抑制血清的培养基可以从整个骨髓细胞中选择BDLSC。这将是为临床肝细胞治疗提供随时可用的备用细胞来源的新方法。

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