基底硬度与细胞因子TGF-β1协同作用对肝细胞表型的影响
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国家自然科学基金资助项目(30870608),国家111计划资助项目(B0623)


Synergistic effects from substrate stiffness and cytokine TGF-β1 on phenotypic transformation of hepatocytes
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    摘要:

    目的 通过建立与肝组织生理和病理硬度相当的体外培养模型,探讨基底硬度和TGF-β1协同作用对肝细胞表型变化的影响。方法 采用免疫荧光显微观测技术及Western Blotting等试验方法,研究肝细胞在不同硬度梯度的聚丙烯酰胺基底膜上的细胞形态调整、运动变化特征、骨架构象以及整合素、E-钙粘素、白蛋白和alpha-平滑肌动蛋白表达的差别,并通过图像分析软件对上述结果进行定量分析。结果3.6 kPa基底膜上单个分散细胞运动变形活跃,但群体细胞极化变小,肌动蛋白沿皮质下呈环状排列,E-钙粘素和白蛋白表达高,整合素和alpha-平滑肌动蛋白的表达水平较低,加药组与对照组变化趋势一致;30 kPa基底膜上细胞运动变形欠活跃,加药组与对照组相比,E-钙粘素和白蛋白表达均下调,alpha-平滑肌动蛋白表达上调;30 kPa与3.6 kPa对照组相比、30 kPa与3.6 kPa加药组相比,E-钙粘素及白蛋白表达均下调(P<0.05),alpha-平滑肌肌动蛋白的表达上调(P<0.05)。10 kPa基底膜上对照组和加药组与30 kPa和3.6 kPa对照组和加药组相比,均无显著性差异。结论基底硬度增加可诱导肝细胞表型转化,并促进TGF-β1对肝细胞代谢行为的影响。

    Abstract:

    Objective To explore the synergistic effects of substrate stiffness and cytokine TGF-β1 on phenotypic transformation of hepatocytes by establishing an in vitro culture model with the substrate stiffness that is relevant to hepatic cells physiologically and pathologically. Methods Immunofluorescence and Western blotting were adopted to observe the morphological adjustment, motion characteristics, cytoskeleton arrangement of hepatocytes on polyacrylamide substrates with different stiffness, as well as the changes in expression of integrin and phenotypic markers E-cadherin, albumin and alpha-smooth muscle actin (α-SMA). Image analysis software was also used for quantitative study on the obtained data. Results On the 3.6 kPa substrates, the scattered single cells were actively deformed and relocated, but the bulk cell population had little change in polarization and microfilament organization. Muscle actin was assembled as cortical ring in cell periphery. There was more abundant expression of E-cadherin and albumin, but less expression of integrin and α-SMA in TGF-β1 treated group as compared to the control group. On the 30 kPa substrates, the motion and deformation of cells were not so active, and expression of both E-cadherin and albumin in TGF-β1 treated group was decreased, while that of α-SMA was increased as compared to the control group. For 30 kPa and 3.6 kPa control groups and 30 kPa and 3.6 kPa TGF-β1 treated groups, expression of both E-cadherin and albumin was reduced (P<0.05), but that of alpha-SMA was increased (P<0.05), while no significant differences were found in both 10 kPa control group and TGF-β1 treated group, as well as in 30 kPa and 3.6 kPa control groups and TGF-β1 treated groups. Conclusions The increase of substrate stiffness can induce transformation of hepatocyte phenotype and promote the influence of TGF-beta 1 on behavior of hepatocyte metabolism.

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王红兵,徐以娟,徐秋华,于光磊,邹小兵,杨力,白洁,杨雨,张持.基底硬度与细胞因子TGF-β1协同作用对肝细胞表型的影响[J].医用生物力学,2012,27(6):661-667

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  • 收稿日期:2011-12-13
  • 最后修改日期:2012-02-17
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