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首页> 外文期刊>BMC Clinical Pathology >Experiences from treatment-predictive KRAS testing; high mutation frequency in rectal cancers from females and concurrent mutations in the same tumor
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Experiences from treatment-predictive KRAS testing; high mutation frequency in rectal cancers from females and concurrent mutations in the same tumor

机译:具有治疗预测性的KRAS测试的经验;女性直肠癌的高突变频率以及同一肿瘤中的并发突变

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摘要

Background KRAS mutations represent key alterations in colorectal cancer development and lead to constitutive EGFR signaling. Since EGFR inhibition represents a therapeutic strategy in advanced colorectal cancer, KRAS mutation analysis has quickly been introduced as a treatment-predictive test. Methods We used a real-time PCR based method to determine KRAS mutations in 136 colorectal cancers with mutations identified in 53 (39%) tumors. Results KRAS mutations were significantly more often found in rectal cancer (21/38, 55%) than in colon cancer (32/98, 33%) (P = 0.02). This finding was explained by marked differences mutation rates in female patients who showed mutations in 33% of the colon cancers and in 67% of the rectal cancers (P = 0.01). Concurrent KRAS mutations were identified in three tumors; two colorectal cancers harbored Gly12Asp/Gly13Asp and Gly12Cys/Gly13Asp and a third tumor carried Gly12Cys/Gly12Asp in an adenomatous component and additionally acquired Gly12Val in the invasive component. Conclusion The demonstration of a particularly high KRAS mutation frequency among female rectal cancer patients suggests that this subset is the least likely to respond to anti-EGFR therapies, whereas the observation of concurrent KRAS mutations imply that repeated KRAS targeting may occur during tumor progression in a subset of colorectal cancers.
机译:背景KRAS突变代表结直肠癌发展中的关键变化,并导致组成型EGFR信号传导。由于EGFR抑制代表了晚期大肠癌的治疗策略,因此已迅速引入KRAS突变分析作为治疗预测性测试。方法我们使用基于实时PCR的方法确定136例大肠癌中的KRAS突变,其中53例(39%)肿瘤中发现了突变。结果KRAS突变在直肠癌(21 / 38,55%)中的发生率明显高于在结肠癌(32 / 98,33%)中的发生率(P = 0.02)。这一发现可以通过女性患者的显着差异突变率来解释,这些女性患者中33%的结肠癌和67%的直肠癌具有突变(P = 0.01)。在三个肿瘤中发现了同时发生的KRAS突变。两种结肠直肠癌分别带有Gly12Asp / Gly13Asp和Gly12Cys / Gly13Asp,第三种肿瘤的腺瘤成分带有Gly12Cys / Gly12Asp,侵袭性成分还带有Gly12Val。结论在女性直肠癌患者中特别高的KRAS突变频率表明,该亚群对抗EGFR疗法的反应可能性最小,而同时发生KRAS突变的观察结果表明,在肿瘤进展过程中可能反复进行KRAS靶向治疗。大肠癌的子集。

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