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The prevalent KRAS exon 2 c.35 G>A mutation in metastatic colorectal cancer patients: A biomarker of worse prognosis and potential benefit of bevacizumab-containing intensive regimens?

机译:转移性结直肠癌患者中普遍存在的KRAS外显子2 c.35 G> A突变:含贝伐单抗强化治疗的预后较差和潜在获益的生物标志物?

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摘要

Bevacizumab-containing chemotherapy differently predict increased efficacy in KRAS exon 2 mutant and wild-type metastatic colorectal cancer (MCRC) patients. Mutant compared to wild-type status did not significantly affect progression-free survival (PFS) and overall survival (OS) in patients fit for first line bevacizumab-containing FIr-B/FOx regimen, and after progression. In patients unfit for intensive regimens, mutant status significantly affected PFS, while not OS. Codon 12 KRAS mutations differentially affect GTPase function, and confer worse clinical behaviour. Prognostic relevance of the prevalent c.35 G. >. A KRAS mutation was retrospectively evaluated. Fit c.35 G. >. A mutant patients showed significantly worse OS compared to wild-type and to other mutant. After progression and in unfit patients, c.35 G. >. A mutation affected significantly worse PFS and OS. c.35 G. >. A mutant status does not significantly affect worse PFS in patients fit for first line FIr-B/FOx, and it may depend upon effectiveness of anti-VEGF-containing intensive regimen.
机译:含贝伐单抗的化学疗法不同地预测KRAS外显子2突变和野生型转移性结直肠癌(MCRC)患者的疗效增加。与野生型状态相比,突变体对一线含贝伐单抗FIr-B / FOx方案的患者以及进展后的无进展生存期(PFS)和总生存期(OS)均无显着影响。在不适合强化治疗的患者中,突变状态会显着影响PFS,而不会影响OS。密码子12 KRAS突变差异影响GTPase功能,并赋予较差的临床行为。普遍存在的c.35 G.>的预后相关性。回顾性评估KRAS突变。适合c.35 G.与野生型和其他突变型相比,突变型患者显示出明显更差的OS。进展后和不适的患者,c.35 G.>。突变会严重影响PFS和OS。约35G。突变状态不会明显影响适合一线FIr-B / FOx的患者的较差PFS,这可能取决于含抗VEGF强化治疗方案的有效性。

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