FYN 通过 STAT5/NOTCH2 信号节点促进基底型乳腺癌细胞的间质表型。

FYN promotes mesenchymal phenotypes of basal type breast cancer cells through STAT5/NOTCH2 signaling node.

机构信息

Department of Life Science, Research Institute for Natural Sciences, Hanyang University, Seoul, Korea.

Department of Radiation Oncology, Samsung Medical Center, Seoul, Korea.

出版信息

Oncogene. 2018 Apr;37(14):1857-1868. doi: 10.1038/s41388-017-0114-y. Epub 2018 Jan 19.

DOI:10.1038/s41388-017-0114-y

PMID:29348460

Abstract

Basal type breast cancer is the most aggressive and has mesenchymal features with a high metastatic ability. However, the signaling node that determines the basal type features in breast cancer remains obscure. Here, we report that FYN among SRC family kinases is required for the maintenance of basal type breast cancer subtype. Importantly, FYN enhanced NOTCH2 activation in basal type breast cancer cells through STAT5-mediated upregulation of Jagged-1 and DLL4 NOTCH ligands, thereby contributed to mesenchymal phenotypes. In addition, we found that high levels of FYN persist in basal type breast cancer cells by a positive feedback loop between FYN and STAT5. FYN interacted directly with STAT5 and increased p-STAT5 that further acts as a transcription factor for FYN. Taken together, our findings demonstrate a pivotal role of FYN and its downstream effectors in maintaining the basal type features in breast cancer.

摘要

基底样乳腺癌是最具侵袭性的，具有间充质特征和高转移能力。然而，决定乳腺癌基底样特征的信号节点仍然不清楚。在这里，我们报告 SRC 家族激酶中的 FYN 对于维持基底样乳腺癌亚型是必需的。重要的是，FYN 通过 STAT5 介导的 Jagged-1 和 DLL4 NOTCH 配体的上调增强了基底样乳腺癌细胞中的 NOTCH2 激活，从而有助于间充质表型。此外，我们发现，通过 FYN 和 STAT5 之间的正反馈回路，高表达的 FYN 持续存在于基底样乳腺癌细胞中。FYN 与 STAT5 直接相互作用，增加了 p-STAT5，后者进一步作为 FYN 的转录因子。总之，我们的研究结果表明 FYN 及其下游效应物在维持乳腺癌的基底样特征中起着关键作用。

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FYN 通过 STAT5/NOTCH2 信号节点促进基底型乳腺癌细胞的间质表型。

FYN promotes mesenchymal phenotypes of basal type breast cancer cells through STAT5/NOTCH2 signaling node.

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