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PIK3CA mutations confer resistance to first-line chemotherapy in colorectal cancer

机译:Pik3CA突变赋予抗直肠癌的一线化学疗法

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Chemotherapy represents an important treatment option for colorectal cancer (CRC), but only half of the patients benefit from these regimens. We explored the potential predicting value and mechanism of PIK3CA mutation in CRC chemotherapy. CRC specimens from 440 patients were retrospectively collected and examined with a fluorescence PCR-based method. The correlation of first-line chemotherapy response and PIK3CA mutation was evaluated according to follow-up and medical records. The underlying mechanism of PIK3CA mutation in chemotherapy resistance was assessed with CRC tumors and primary cells. The mutation frequency of the PIK3CA gene in CRC patients was 9.55%, which was correlated with late TNM staging and lower histological grade. The CRC patients with PIK3A mutation showed worse response to first-line chemotherapy than those without PIK3CA mutation. PIK3A mutation tumor cells showed poor sensitivity to first-line chemotherapy in vitro and in vivo. PIK3CA mutation induced PI3K/Akt signaling activation to increase LGR5+ CRC stem cells survival and proliferation, from which lead to chemotherapy resistance. Furthermore, PIK3CA mutation/LGR5+ expression was an independent detrimental factor for CRC patients. Our findings indicated that PIK3CA mutation induced PI3K/Akt activation contributed to CRC stem cells survival and proliferation, from which cells further resistance to chemotherapy. PIK3CA mutation/LGR5+ expression was a potential biomarker for monitoring chemotherapy resistance in CRC.
机译:化疗代表了结直肠癌(CRC)的重要治疗选择,但只有一半的患者受益于这些方案。我们探讨了CRC化疗中PIK3CA突变的潜在预测价值和机制。回顾性收集来自440名患者的CRC标本,并用基于荧光PCR的方法检查并检查。根据后续和医疗记录评价一线化疗反应和PIK3CA突变的相关性。用CRC肿瘤和原代细胞评估化疗抗性中PIK3CA突变的潜在机制。 CRC患者中PIK3CA基因的突变频率为9.55%,与晚期TNM分期和较低的组织学等级相关。 PIK3A突变的CRC患者对第一线化学疗法的响应较差,而不是没有PIK3CA突变的响应。 Pik3A突变肿瘤细胞对体外和体内的一线化疗敏感性差。 PIK3CA突变诱导PI3K / AKT信号激活,以增加LGR5 + CRC干细胞存活和增殖,从此导致化疗抗性。此外,PIK3CA突变/ LGR5 +表达是CRC患者的独立性不利因素。我们的研究结果表明,PIK3CA突变诱导的PI3K / AKT活化有助于CRC干细胞存活和增殖,从中进一步抵抗化疗。 PIK3CA突变/ LGR5 +表达是用于监测CRC中化疗抗性的潜在生物标志物。

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