首页> 美国卫生研究院文献>American Journal of Physiology - Lung Cellular and Molecular Physiology >Bioengineering the Lung: Molecules Materials Matrix Morphology and Mechanics: Fibroblast engraftment in the decellularized mouse lung occurs via a β1-integrin-dependent FAK-dependent pathway that is mediated by ERK and opposed by AKT
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Bioengineering the Lung: Molecules Materials Matrix Morphology and Mechanics: Fibroblast engraftment in the decellularized mouse lung occurs via a β1-integrin-dependent FAK-dependent pathway that is mediated by ERK and opposed by AKT

机译:肺的生物工程:分子材料基质形态和力学:成纤维细胞植入去细胞小鼠肺中的过程是通过ERK介导且受AKT阻断的β1整合素依赖性FAK依赖性途径发生的

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摘要

Creation of bioartificial organs has been enhanced by the development of strategies involving decellularized mammalian lung. Because fibroblasts critically support lung function through a number of mechanisms, study of these cells in the context of the decellularized lung has the potential to improve the structure and function of tissue-engineered lungs. We characterized the engraftment and survival of a mouse fibroblast cell line in decellularized rat lung slices and found a time-dependent increase in cell numbers assessed by hematoxylin and eosin staining, cell proliferation assessed by Ki67 staining, and minimal cell death assessed by TUNEL staining. We developed a repopulation index to allow quantification of cell survival that accounts for variation in cell density throughout the seeded scaffold. We then applied this method to the study of mouse lung scaffolds and found that decellularization of presliced mouse lungs produced matrices with preserved alveolar architecture and proteinaceous components including fibronectin, collagens I and IV, laminin, and elastin. Treatment with a β1-integrin-neutralizing antibody significantly reduced the repopulation index after 24 h of culture. Treatment with focal adhesion kinase (FAK) inhibitor and extracellular signal-regulated kinase (ERK) inhibitor further reduced initial repopulation scores while treatment with AKT inhibitor increased initial scores. Rho-associated kinase inhibitor had no discernible effect. These data indicate that initial adhesion and survival of mouse fibroblasts in the decellularized mouse lung occur in a β1-integrin-dependent, FAK/ERK-dependent manner that is opposed by AKT.
机译:通过开发涉及脱细胞的哺乳动物肺的策略,生物人工器官的创造得到了增强。由于成纤维细胞通过多种机制关键性地支持肺功能,因此在脱细胞肺的背景下研究这些细胞具有改善组织工程化肺的结构和功能的潜力。我们表征了小鼠去纤维化大鼠肺切片中成纤维细胞系的移植和存活,并发现了苏木精和曙红染色评估的细胞数量随时间的增加,Ki67染色评估了细胞增殖,TUNEL染色评估了最小的细胞死亡。我们开发了一个重新种群指数,以量化细胞存活率,从而说明整个播种支架中细胞密度的变化。然后,我们将这种方法应用于小鼠肺支架的研究,发现预先切开的小鼠肺的脱细胞化产生了具有保留的肺泡结构和蛋白质成分(包括纤连蛋白,I型和IV型胶原,层粘连蛋白和弹性蛋白)的基质。用β1-整合素中和抗体处理可显着降低培养24小时后的再种群指数。用粘着斑激酶(FAK)抑制剂和细胞外信号调节激酶(ERK)抑制剂治疗可进一步降低初始再种群得分,而用AKT抑制剂治疗可提高初始得分。 Rho相关的激酶抑制剂没有明显的作用。这些数据表明,脱细胞的小鼠肺中小鼠成纤维细胞的初始粘附和存活以与AKT相对的β1整合素依赖性,FAK / ERK依赖性方式发生。

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