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首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >C-Src-mediated phosphorylation of δ-catenin increases its protein stability and the ability of inducing nuclear distribution of β-catenin
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C-Src-mediated phosphorylation of δ-catenin increases its protein stability and the ability of inducing nuclear distribution of β-catenin

机译:C-Src介导的δ-catenin磷酸化增加其蛋白质稳定性并诱导β-catenin的核分布

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摘要

Although δ-catenin was first considered as a brain specific protein, strong evidence of δ-catenin overexpression in various cancers, including prostate cancer, has been accumulated. Phosphorylation of δ-catenin by Akt and GSK3β has been studied in various cell lines. However, tyrosine phosphorylation of δ-catenin in prostate cancer cells remains unknown. In the current study, we demonstrated that Src kinase itself phosphorylates δ-catenin on its tyrosine residues in prostate cancer cells and further illustrated that Y1073, Y1112 and Y1176 of δ-catenin are predominant sites responsible for tyrosine phosphorylation mediated by c-Src. Apart from c-Src, other Src family kinases, including Fgr, Fyn and Lyn, can also phosphorylate δ-catenin. We also found that c-Src-mediated Tyr-phosphorylation of δ-catenin increases its stability via decreasing its affinity to GSK3β and enhances its ability of inducing nuclear distribution of β-catenin through interrupting the integrity of the E-cadherin. Taken together, these results indicate that c-Src can enhance the oncogenic function of δ-catenin in prostate cancer cells.
机译:尽管δ-catenin首先被认为是一种大脑特异性蛋白,但是δ-catenin在包括前列腺癌在内的各种癌症中过表达的强有力证据已经得到了积累。已经在各种细胞系中研究了Akt和GSK3β对δ-catenin的磷酸化作用。然而,前列腺癌细胞中δ-连环蛋白的酪氨酸磷酸化仍然未知。在当前的研究中,我们证明了Src激酶本身会在前列腺癌细胞的酪氨酸残基上磷酸化δ-catenin,并进一步说明δ-catenin的Y1073,Y1112和Y1176是负责c-Src介导的酪氨酸磷酸化的主要位点。除c-Src外,其他Src家族激酶(包括Fgr,Fyn和Lyn)也可以使δ-catenin磷酸化。我们还发现,c-Src介导的δ-catenin的Tyr磷酸化可通过降低其对GSK3β的亲和力来提高其稳定性,并通过中断E-cadherin的完整性来增强其诱导β-catenin核分布的能力。综上,这些结果表明,c-Src可以增强δ-catenin在前列腺癌细胞中的致癌功能。

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