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Direct binding of RalA to PKCη and its crucial role in morphological change during keratinocyte differentiation

机译:角质形成细胞分化期间RALA对PKCη的直接结合及其在形态变化中的关键作用

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During differentiation, keratinocytes undergo a dramatic shape change from small and round to large and flat, in addition to production of proteins necessary for the formation of epidermis. It has been shown that protein kinase C (PKC) η is crucial for keratinocyte differentiation. However, its role in this process has yet to be fully elucidated. Here, we show that catalytic activity is not necessary for enlarged and flattened morphology of human keratinocytes induced by overexpression of PKCη, although it is important for gene expression of the marker proteins. In addition, we identify the small G protein RalA as a binding partner of PKCη, which binds to the C1 domain, an indispensable region for the morphological change. The binding led activation of RalA and actin depolymerization associated with keratinocyte differentiation. siRNA techniques proved that RalA is involved in not only the keratinocyte differentiation induced by PKCη overexpression but also normal keratinocyte differentiation induced by calcium and cholesterol sulfate. These results provide a new insight into the molecular mechanism of cytoskeletal regulation leading to drastic change of cell shape.
机译:在分化期间,除了产生表皮形成所需的蛋白质之外,角质形成细胞除了产生蛋白质之外,异常形状从小和圆形变为大而扁平。已经表明,蛋白激酶C(PKC)η对于角蛋白细胞分化至关重要。然而,它在这个过程中的作用尚未完全阐明。在这里,我们表明,由于PKCH的过表达诱导的人角蛋白细胞的扩大和扁平形态而不是必需的催化活性,但对于标记蛋白的基因表达是重要的。此外,我们将小G蛋白RALA鉴定为PKCH的结合伴侣,其与C1结构域结合,是形态变化的不可或缺的区域。与角质形成细胞分化相关的RAA和肌动蛋白解聚的结合LED激活。 SiRNA技术证明,RAA不仅涉及PKCH过表达诱导的角质形成细胞分化,而且还涉及由钙和胆固醇硫酸钙诱导的正常角质形成细胞分化。这些结果对细胞骨骼调节的分子机制提供了新的洞察力,导致细胞形状的激烈变化。

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