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首页> 外文期刊>Cancer research: The official organ of the American Association for Cancer Research, Inc >A novel lung metastasis signature links Wnt signaling with cancer cell self-renewal and epithelial-mesenchymal transition in basal-like breast cancer.
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A novel lung metastasis signature links Wnt signaling with cancer cell self-renewal and epithelial-mesenchymal transition in basal-like breast cancer.

机译:一种新型的肺转移信号将Wnt信号与基底样乳腺癌中的癌细胞自我更新和上皮间质转化联系起来。

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摘要

The establishment of metastasis depends on the ability of cancer cells to acquire a migratory phenotype combined with their capacity to recreate a secondary tumor in a distant tissue. In epithelial cancers, such as those of the breast, the epithelial-mesenchymal transition (EMT) is associated with basal-like breast cancers, generates cells with stem-like properties, and enables cancer cell dissemination and metastasis. However, the molecular mechanism(s) that connects stem cell-like characteristics with EMT has yet to be defined. Using an orthotopic model of human breast cancer metastasis to lung, we identified a poor prognosis gene signature, in which several components of the wnt signaling pathway were overexpressed in early lung metastases. The wnt genes identified in this signature were strongly associated with human basal-like breast cancers. We found that inhibiting wnt signaling through LRP6 reduced the capacity of cancer cells to self-renew and seed tumors in vivo. Furthermore, inhibition of wnt signaling resulted in the reexpression of breast epithelial differentiation markers and repression of EMT transcription factors SLUG and TWIST. Collectively, these results provide a molecular link between self-renewal, EMT, and metastasis in basal-like breast cancers.
机译:转移的建立取决于癌细胞获得迁移表型的能力及其在远处组织中再形成继发性肿瘤的能力。在诸如乳腺癌的上皮癌中,上皮-间质转化(EMT)与基底样乳腺癌相关,产生具有干样性质的细胞,并使癌细胞能够扩散和转移。然而,将干细胞样特征与EMT相联系的分子机制尚待确定。使用人类乳腺癌向肺转移的原位模型,我们确定了不良的预后基因特征,其中在早期肺转移中过度表达了wnt信号通路的几个组成部分。此签名中鉴定出的wnt基因与人类基底样乳腺癌密切相关。我们发现抑制通过LRP6的wnt信号传导会降低癌细胞自我更新和在体内播种肿瘤的能力。此外,对wnt信号的抑制导致乳腺上皮分化标记物的重新表达以及EMT转录因子SLUG和TWIST的表达受到抑制。总的来说,这些结果在基底样乳腺癌的自我更新,EMT和转移之间提供了分子联系。

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