Montefiore Medical Center, Bronx, NY 10461, USA.
Clin Colorectal Cancer. 2012 Jun;11(2):143-50. doi: 10.1016/j.clcc.2011.12.001. Epub 2012 Jan 28.
To identify novel genetic markers predictive of clinical benefit from epidermal growth factor receptor-directed antibody therapy in patients with metastatic colorectal cancer.
Seventy-six consecutive patients who received cetuximab or panitumumab, either alone or in combination with chemotherapy and with available tumor tissue were included. Tumor tissue was tested by pyrosequencing for mutations at known hot spots in the KRAS, BRAF, PIK3CA, PIK3R1, AKT1, and PTEN genes. PTEN promoter methylation status was analyzed by methylation-specific polymerase chain reaction, and expression was determined by immunohistochemistry (IHC). Forty-four patients had 4 weeks of therapy and were considered for clinical correlates.
Consistent with previous studies, KRAS gene mutations were associated with a shorter progression-free survival (PFS) and overall survival (OS). Among the patients with wild-type KRAS, preservation of PTEN expression and PIK3CA wild-type status was associated with improved OS (median OS, 80.4 vs. 32.5 weeks; hazard ratio, 0.33; P = .0008) and a trend toward improved PFS (median PFS, 24.8 vs. 15.2 weeks; hazard ratio, 0.51; P = .06), compared with PTEN-negative or PIK3CA-mutant tumors. PTEN methylation was more common in the metastatic samples than in the primary samples (P = .02). The simultaneous presence of methylation and mutation in the PTEN gene was associated with IHC negativity (P = .026).
In addition to KRAS mutation, loss of PTEN expression (by IHC) and PIK3CA mutation is likely to be predictive of a lack of benefit to anti-EGFR therapy in metastatic colorectal cancer. PTEN promoter methylation and mutation status was predictive of PTEN expression and may be used as an alternative means of predicting response to EGFR-targeted therapy.
鉴定预测转移性结直肠癌患者接受表皮生长因子受体定向抗体治疗临床获益的新型遗传标志物。
纳入 76 例连续接受西妥昔单抗或帕尼单抗治疗的患者,这些患者单独或联合化疗且有可用肿瘤组织。通过焦磷酸测序检测 KRAS、BRAF、PIK3CA、PIK3R1、AKT1 和 PTEN 基因中已知热点的突变。通过甲基化特异性聚合酶链反应分析 PTEN 启动子甲基化状态,并用免疫组织化学(IHC)检测表达。44 例患者接受了 4 周的治疗,并进行了临床相关性分析。
与既往研究一致,KRAS 基因突变与较短的无进展生存期(PFS)和总生存期(OS)相关。在 KRAS 野生型患者中,PTEN 表达和 PIK3CA 野生型状态的保留与 OS 改善相关(中位 OS,80.4 与 32.5 周;风险比,0.33;P =.0008),且 PFS 有改善趋势(中位 PFS,24.8 与 15.2 周;风险比,0.51;P =.06),与 PTEN 阴性或 PIK3CA 突变肿瘤相比。与原发样本相比,转移性样本中 PTEN 甲基化更为常见(P =.02)。PTEN 基因的同时存在甲基化和突变与 IHC 阴性相关(P =.026)。
除 KRAS 突变外,PTEN 表达缺失(通过 IHC)和 PIK3CA 突变可能是转移性结直肠癌患者抗 EGFR 治疗获益缺失的预测指标。PTEN 启动子甲基化和突变状态可预测 PTEN 表达,可作为预测 EGFR 靶向治疗反应的替代方法。
