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首页> 外文期刊>Asia-Pacific journal of clinical oncology >Prognostic significance of BRAF mutation alone and in combination with microsatellite instability in stage III colon cancer
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Prognostic significance of BRAF mutation alone and in combination with microsatellite instability in stage III colon cancer

机译:单独的BRAF突变的预后意义及其在III期结肠癌中微卫星不稳定性的影响

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摘要

Purpose The prognostic significance of biomarkers in colorectal cancer is still being defined. This study aimed to determine the prognostic significance of BRAF mutation alone and in combination with microsatellite instability (MSI), in stage III colon cancer. Methods Curatively resected stage III colon cancers were studied from a 33-year period. Clinicopathological data were collated (adjuvant chemotherapy, age, gender, obstruction, perforation, tumour location, grade, presence of mucin, nodal stage, extramural vascular, and perineural invasion). MSI status was established and molecular testing for BRAF (V600E) was performed. Four mutation categories were examined: "traditional" (microsatellite stable [MSS]/BRAF -ve), "presumed Lynch" (MSI/BRAF -ve), "sporadic MSI" (MSI/BRAF +ve), and "other BRAF" (MSS/BRAF +ve). These factors were correlated with cancer-specific survival. Results In total, 686 unselected cases met our inclusion criteria, of which 15.7% had a BRAF mutation and 13.8% showed MSI. In the adjusted analysis, neither BRAF mutation nor MSI mutation were independently prognostic. On univariate analysis, survival in presumed Lynch cancers was similar to traditional cancers (5-year survival: 62% and 61%, respectively). While there was no difference in cancer-specific survival between sporadic MSI and other BRAF, both these tumour group had poorer outcome when compared to traditional or presumed Lynch cancers. Adjusted analysis of the four groups, however, showed that none of the subgroups were independently prognostic. Conclusion BRAF-mutated cancers demonstrated a trend toward poorer outcomes, however, when adjusted for clinicopathological factors and chemotherapy, BRAF mutation was not found to be an independent prognostic biomarker in stage III colon cancer, even when combined with MSI.
机译:目的仍然定义了结直肠癌中生物标志物的预后意义。本研究旨在确定BRAF突变单独的预后意义,并与微卫星不稳定性(MSI)组合,III期结肠癌。方法从33年期间,研究了疗法切除阶段III阶段的结肠癌。临床病理数据被整理(佐剂化疗,年龄,性别,梗阻,穿孔,肿瘤位置,粘蛋白,节点阶段,越耳血管和麻痹侵袭)。建立了MSI状态,并进行了BRAF(V600E)的分子测试。检查了四个突变类别:“传统”(微卫星稳定[MSS] / BRAF -VE),“假定林奇”(MSI / BRAF -VE),“零星MSI”(MSI / BRAF + VE)和“其他BRAF” (MSS / BRAF + VE)。这些因素与癌症特异性的存活率相关。结果总计686例未选择的案件达到了纳入标准,其中15.7%具有BRAF突变,13.8%显示MSI。在调整后的分析中,BRAF突变和MSI突变都没有独立预后。关于单变量分析,假定林基癌症的生存与传统癌症相似(分别为5年生存:62%和61%)。虽然散发性MSI和其他BRAF之间的癌症特异性存活率没有差异,但与传统或推定的林基癌症相比,这两个肿瘤组都有较差的结果。然而,调整后的四组分析表明,没有一个亚组是独立的预后。结论BRAF-突变的癌症表现出较差的结果趋势,然而,在调整临床病理因素和化疗时,尚未发现BRAF突变是III阶段结肠癌的独立预后生物标志物,即使与MSI相结合。

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