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首页> 外文期刊>Journal of Cell Science >The integrin alphavbeta6 is critical for keratinocyte migration on both its known ligand, fibronectin, and on vitronectin.
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The integrin alphavbeta6 is critical for keratinocyte migration on both its known ligand, fibronectin, and on vitronectin.

机译:整联蛋白αvbeta6对于角质形成细胞在其已知配体,纤连蛋白和玻连蛋白上的迁移至关重要。

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The integrin alphavbeta6 is expressed on a variety of epithelial cells during dynamic processes including organogenesis, tissue injury and malignant transformation. However, because of the lack of tools to specifically inhibit the function of this integrin, little is known about its effects on cell behavior. To directly examine the role of this integrin in cell migration, we used keratinocytes derived from wild-type mice or mice expressing a null mutation in the beta6 subunit (beta6-/-) to perform migration assays in vitro. Migration on the known alphavbeta6 ligand, fibronectin was reduced in keratinocytes from beta6-/- mice. Interestingly, keratinocytes from beta6-/- mice also demonstrated markedly reduced migration on vitronectin, a protein not previously known to be a ligand for alphavbeta6. An anti-alphavbeta6 monoclonal antibody 10D5, generated by immunization of beta6-/- mice with murine keratinocytes, inhibited adhesion and migration of wild-type keratinocyte on both vitronectin and fibronectin to levels similar to those seen with keratinocytes from beta6-/- mice. alphavbeta6-mediated migration on both ligands was dramatically augmented by treatment with phorbol myrisate acetate (PMA) or with hepatocyte growth factor, and augmentation of migration by either stimulus could be abolished by the PKC inhibitor GF109203X, suggesting a critical role for PKC in enhancement of alphavbeta6-mediated cell migration.
机译:在包括器官发生,组织损伤和恶性转化在内的动态过程中,整联蛋白αvbeta6在多种上皮细胞上表达。但是,由于缺乏专门抑制这种整合素功能的工具,因此人们对其作用的了解甚少。为了直接检查这种整合素在细胞迁移中的作用,我们使用了源自野生型小鼠或在beta6亚基(beta6-/-)中表达无效突变的小鼠的角质形成细胞,以进行体外迁移实验。在已知的alphavbeta6配体上,纤连蛋白的迁移在beta6-/-小鼠的角质形成细胞中减少。有趣的是,来自beta6-/-小鼠的角质形成细胞也显示出在玻连蛋白上的迁移明显减少,玻连蛋白是一种以前未知的αvbeta6配体蛋白。通过用鼠类角质形成细胞免疫β6-/-小鼠产生的抗αvβ6单克隆抗体10D5抑制了野生型角质形成细胞在玻连蛋白和纤连蛋白上的粘附和迁移,其水平与从β6-/-小鼠角质形成细胞观察到的水平相似。醋酸佛波豆蔻酸酯乙酸酯(PMA)或肝细胞生长因子治疗可显着增强alphavbeta6介导的两种配体上的迁移,而PKC抑制剂GF109203X则可消除任一刺激下的迁移,这提示PKC在增强CV的关键作用alphavbeta6介导的细胞迁移。

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