KRAS 基因突变和微卫星不稳定性：两个影响结直肠癌预后的早期肿瘤发展的遗传标志物。

KRAS mutation and microsatellite instability: two genetic markers of early tumor development that influence the prognosis of colorectal cancer.

机构信息

Department of Surgery, Memorial Sloan-Kettering Cancer Center, New York, USA.

出版信息

Ann Surg Oncol. 2010 Feb;17(2):416-24. doi: 10.1245/s10434-009-0713-0. Epub 2009 Oct 8.

DOI:10.1245/s10434-009-0713-0

PMID:19813061

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4380015/

Abstract

INTRODUCTION

We examined two genetic markers established early in colorectal tumor development, microsatellite instability (MSI) and mutation of the KRAS proto-oncogene, to see if these genetic changes influence metastatic disease progression and survival.

PATIENTS AND METHODS

MSI and KRAS mutation status were assessed in 532 primary adenocarcinomas (stage I-IV) from patients treated by colon resection. Median follow-up was 4.1 years (range 0-13.3 years) overall, 5.4 years for survivors.

RESULTS

MSI and KRAS mutation were detected in 12 and 36% of cases, respectively. MSI was more common in early-stage disease (I, 15%; II, 21%; III, 10%; IV, 2%; P = 0.0001). Prevalence of KRAS mutation did not vary with stage (I, 36%; II, 34%; III, 35%; IV, 40%; P = ns). Disease-specific survival was far superior for MSI tumors than for microsatellite stability (MSS) tumors (5-year survival 92 vs. 59%, P < 0.0001). KRAS mutation was a marker of poor survival (5-year survival 55 vs. 68%, P = 0.0002). Using Cox regression analysis MSI, KRAS mutation, and stage were strong independent predictors of survival in the entire patient population. A high-mortality group with MSS/KRAS-mutant tumors was identified within the stage I and II cohort.

CONCLUSIONS

MSI and KRAS mutation provide fundamental genetic signatures influencing tumor behavior across patient subsets and stages of tumor development.

摘要

简介

我们研究了两种在结直肠肿瘤早期发展中确立的遗传标记物，微卫星不稳定性（MSI）和 KRAS 原癌基因突变，以观察这些遗传变化是否影响转移性疾病的进展和生存。

患者和方法

评估了 532 例接受结肠切除术治疗的原发性腺癌（I-IV 期）患者的 MSI 和 KRAS 突变状态。总体中位随访时间为 4.1 年（范围 0-13.3 年），幸存者为 5.4 年。

结果

分别在 12%和 36%的病例中检测到 MSI 和 KRAS 突变。MSI 在早期疾病（I 期，15%；II 期，21%；III 期，10%；IV 期，2%；P=0.0001）中更为常见。KRAS 突变的发生率与分期无关（I 期，36%；II 期，34%；III 期，35%；IV 期，40%；P=ns）。MSI 肿瘤的疾病特异性生存率远高于微卫星稳定性（MSS）肿瘤（5 年生存率 92% vs. 59%，P<0.0001）。KRAS 突变是预后不良的标志物（5 年生存率 55% vs. 68%，P=0.0002）。使用 Cox 回归分析，MSI、KRAS 突变和分期是整个患者群体生存的强有力独立预测因子。在 I 期和 II 期队列中确定了具有 MSS/KRAS 突变肿瘤的高死亡率组。

结论

MSI 和 KRAS 突变提供了影响肿瘤行为的基本遗传特征，跨越了患者亚组和肿瘤发展阶段。

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