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Targeting brain-adaptive cancer stem cells prohibits brain metastatic colonization of triple-negative breast cancer

机译:靶向脑适应性癌症干细胞禁止三阴性乳腺癌的脑转移定植

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摘要

Triple-negative breast cancer (TNBC) exhibits more traits possessed by cancer stem cells (CSC) than other breast cancer subtypes and is more likely to develop brain metastases. TNBC patients usually have shorter survival time after diagnosis of brain metastasis, suggesting an innate ability of TNBC tumor cells in adapting to the brain. In this study, we establish novel animal models to investigate early tumor adaptation in brain metastases by introducing both patient-derived and cell line-derived CSC-enriched brain metastasis tumorsphere cells into mice. We discovered astrocyte-involved tumor activation of protocadherin 7 (PCDH7)-PLCβ-Ca2+-CaMKII/S100A4 signaling as a mediator of brain metastatic tumor outgrowth. We further identified and evaluated the efficacy of a known drug, the selective PLC inhibitor edelfosine, in suppressing the PCDH7 signaling pathway to prohibit brain metastases in the animal models. The results of this study reveal a novel signaling pathway for brain metastases in TNBC and indicate a promising strategy of metastatic breast cancer prevention and treatment by targeting organ-adaptive cancer stem cells.
机译:与其他乳腺癌亚型相比,三阴性乳腺癌(TNBC)具有更多的癌症干细胞(CSC)特征,并且更有可能发生脑转移。 TNBC患者在诊断出脑转移后通常具有较短的生存时间,这表明TNBC肿瘤细胞具有先天适应大脑的能力。在这项研究中,我们建立了新颖的动物模型,通过将患者来源的和细胞系来源的CSC丰富的脑转移肿瘤球细胞引入小鼠体内来研究脑转移的早期肿瘤适应性。我们发现星形胶质细胞参与的原钙粘蛋白7(PCDH7)-PLCβ-Ca2+ -CaMKII / S100A4信号激活是脑转移性肿瘤生长的介质。我们进一步鉴定并评估了已知药物选择性PLC抑制剂edelfosine在抑制PCDH7信号通路以禁止动物模型中脑转移的功效。这项研究的结果揭示了TNBC中脑转移的新型信号传导途径,并表明了通过靶向器官适应性癌症干细胞来预防和治疗转移性乳腺癌的策略。

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