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Forced Expression of Keratin 16 Alters the Adhesion, Differentiation, and Migration of Mouse Skin Keratinocytes

机译:角蛋白16的强制表达会改变粘附力, 小鼠皮肤角质形成细胞的分化和迁移

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摘要

Injury to the skin results in an induction of keratins K6, K16, and K17 concomitant with activation of keratinocytes for reepithelialization. Forced expression of human K16 in skin epithelia of transgenic mice causes a phenotype that mimics several aspects of keratinocyte activation. Two types of transgenic keratinocytes, with forced expression of either human K16 or a K16-C14 chimeric cDNA, were analyzed in primary culture to assess the impact of K16 expression at a cellular level. High K16-C14-expressing and low K16-expressing transgenic keratinocytes behave similar to wild type in all aspects tested. In contrast, high K16-expressing transgenic keratinocytes show alterations in plating efficiency and calcium-induced differentiation, but proliferate normally. Migration of keratinocytes is reduced in K16 transgenic skin explants compared with controls. Finally, a subset of high K16-expressing transgenic keratinocytes develops major changes in the organization of keratin filaments in a time- and calcium concentration-dependent manner. These changes coincide with alterations in keratin content while the steady-state levels of K16 protein remain stable. We conclude that forced expression of K16 in progenitor skin keratinocytes directly impacts properties such as adhesion, differentiation, and migration, and that these effects depend upon determinants contained within its carboxy terminus.
机译:皮肤损伤导致角蛋白K6,K16和K17的诱导,并伴随着角质形成细胞的活化而重新上皮。人类K16在转基因小鼠皮肤上皮细胞中的强制表达导致表型模仿角质形成细胞活化的几个方面。在原代培养中分析了两种类型的强制表达人K16或K16-C14嵌合cDNA的转基因角质形成细胞,以评估K16表达在细胞水平上的影响。在所有测试的方面,高表达K16-C14和低表达K16的转基因角质形成细胞的行为与野生型相似。相反,高表达K16的转基因角质形成细胞在铺板效率和钙诱导的分化中表现出变化,但正常增殖。与对照组相比,K16转基因皮肤外植体中角质形成细胞的迁移减少。最后,高表达K16的转基因角质形成细胞的一个子集,以时间和钙浓度依赖性的方式,在角蛋白丝组织的发展方面发生了重大变化。这些变化与角蛋白含量的变化相吻合,而K16蛋白的稳态水平保持稳定。我们得出结论,祖先皮肤角质形成细胞中K16的强制表达直接影响诸如粘附,分化和迁移等特性,并且这些影响取决于其羧基末端所含的决定簇。

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