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A Single Kinase Generates the Majority of the Secreted Phosphoproteome

机译:单一激酶可产生大部分的分泌型磷酸化蛋白质组。

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摘要

The existence of extracellular phosphoproteins has been acknowledged for over a century. However, research in this area has been undeveloped largely because the kinases that phosphorylate secreted proteins have escaped identification. Fam20C is a kinase that phosphorylates S-x-E/pS motifs on proteins in milk and in the extracellular matrix of bones and teeth. Here, we show that Fam20C generates the majority of the extracellular phosphoproteome. Using CRISPR/Cas9 genome editing, mass spectrometry, and biochemistry, we identify more than 100 secreted phosphoproteins as genuine Fam20C substrates. Further, we show that Fam20C exhibits broader substrate specificity than previously appreciated. Functional annotations of Fam20C substrates suggest roles for the kinase beyond biomineralization, including lipid homeostasis, wound healing, and cell migration and adhesion. Our results establish Fam20C as the major secretory pathway protein kinase and serve as a foundation for new areas of investigation into the role of secreted protein phosphorylation in human biology and disease.
机译:细胞外磷蛋白的存在已经有一个多世纪的历史了。但是,该领域的研究尚未开发,主要是因为磷酸化分泌蛋白的激酶未能通过鉴定。 Fam20C是一种激酶,可磷酸化牛奶中以及骨骼和牙齿的细胞外基质中蛋白质上的S-x-E / pS基序。在这里,我们表明Fam20C生成大多数的细胞外磷酸化蛋白质组。使用CRISPR / Cas9基因组编辑,质谱和生物化学,我们确定了100多种分泌的磷蛋白作为真正的Fam20C底物。此外,我们表明Fam20C展示了比以前认可的更广泛的底物特异性。 Fam20C底物的功能注释表明该激酶在生物矿化作用之外的作用,包括脂质稳态,伤口愈合以及细胞迁移和粘附。我们的研究结果将Fam20C确立为主要的分泌途径蛋白激酶,并为研究分泌型蛋白磷酸化在人类生物学和疾病中的作用的新领域奠定了基础。

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