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In vivo effects of chemotherapy on oncogenic pathways in colorectal cancer

机译:化疗对大肠癌致癌途径的体内作用

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摘要

Patients with advanced colorectal cancer often are treated with systemic cytotoxic therapy using fluorouracil (5‐FU), oxaliplatin, irinotecan, and FOLFOX or FOLFIRI combination protocols. Additionally, signaling pathways that are active in colorectal cancer can be therapeutically targeted. Herein, we examined whether chemotherapy impacts on WNT, MAPK and NOTCH signaling pathways in xenograft models of colon cancer. Furthermore, we tested whether combining chemotherapy with MAPK and NOTCH inhibition has superior therapeutic effects. We show that colon cancer cells with high WNT, MAPK and NOTCH activity are variably affected but generally persist in xenograft tumors under different chemotherapeutic regimens, indicating limited effects of cytotoxic therapy on oncogenic signaling pathways. Although these results provided a rationale to additionally target pathway activity, we found no significant increase in therapy response when combining MAPK and NOTCH inhibition with fluorouracil chemotherapy. We attribute this finding to a decrease in tumor cell proliferation upon MAPK and NOTCH inhibition, resulting in reduced effectiveness of cytotoxic treatment. Therapeutic benefits of combining chemotherapy with targeting of oncogenic signaling pathways must therefore be critically evaluated for patients with colorectal cancer.
机译:患有晚期大肠癌的患者通常接受系统性细胞毒性治疗,使用氟尿嘧啶(5-FU),奥沙利铂,伊立替康和FOLFOX或FOLFIRI联合治疗方案。另外,可以在治疗上靶向在结肠直肠癌中活跃的信号传导途径。在这里,我们检查了化学疗法是否对结肠癌异种移植模型中的WNT,MAPK和NOTCH信号通路产生影响。此外,我们测试了化学疗法结合MAPK和NOTCH抑制是否具有更好的治疗效果。我们显示具有高WNT,MAPK和NOTCH活性的结肠癌细胞受到不同程度的影响,但在不同的化疗方案下通常会在异种移植肿瘤中持续存在,这表明细胞毒性疗法对致癌信号通路的作用有限。尽管这些结果为进一步靶向通路活性提供了理论依据,但我们发现将MAPK和NOTCH抑制与氟尿嘧啶化疗联合使用时,治疗反应无​​明显增加。我们将此发现归因于MAPK和NOTCH抑制后肿瘤细胞增殖的减少,导致细胞毒性治疗的有效性降低。因此,对于结直肠癌患者,必须严格评估将化学疗法与靶向致癌信号通路相结合的治疗益处。

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