Center for Health Research, Kaiser Permanente Northwest, Portland, Oregon, 3800 North Interstate Avenue, Portland, OR 97227.
Am J Cancer Res. 2011 May 15;1(5):650-62.
Pharmacogenetic testing can help identify patients with metastatic colorectal cancer more likely to respond to anti-EGFR therapy. We systematically reviewed the benefits and harms of EGFR-related pharmacogenetic testing of molecular targets downstream to KRAS in the treatment of metastatic colorectal cancer. We searched five electronic databases from January 2000 through November 2010, and conducted separate grey literature and conference abstracts searches. Two reviewers independently assessed all articles for relevance and quality. We identified 27 studies, primarily fair- to marginal-quality, small retrospective, and single-arm cohort studies with significant overlap in patient populations. We identified seven studies that studied BRAF in independent patient populations, one that studied NRAS, four that studied PIK3CA, eight that studied PTEN expression, and five that studied AKT expression. The best evidence for BRAF, NRAS, and PIK3CA comes from the largest retrospective study (n=649) of chemorefractory patients from seven European countries. In this study, BRAF mutation was present in 6.5% of KRAS wild-type tumors. Only 8.3% of persons with BRAF mutations, compared to 38% of persons without BRAF mutations (p=0.0012), responded to chemotherapy with cetuximab. Clinical sensitivity and the false positive fraction (1- specificity) were estimated at 9.8% (95% CI 6.3, 14.5) and 1.6% (95% CI 0.2, 5.6), respectively. BRAF mutation was also associated with worse median progression-free survival (absolute difference 18 weeks, p<0.0001), and overall survival (absolute difference 28 weeks, p<0.0001). In the only study comparing outcomes in persons who did (n=227) and did not (n=332) receive cetuximab with combination chemotherapy, those with BRAF mutation had worse survival outcomes regardless of whether or not they received cetuximab. Although NRAS and PIK3CA exon 20 mutations were also associated with worse outcomes compared to persons without these mutations, evidence is based on a small number of identified mutations. Evidence for protein expression of PTEN and AKT is more sparse and limited by variable methods for assessing protein expression. Low-quality evidence addressing clinical validity of pharmacogenetic testing in metastatic colorectal cancer patients suggests that BRAF mutations are associated with poorer treatment response and survival outcomes, although this association may be independent of treatment with EGFR inhibitors.
药物遗传学检测可帮助识别转移性结直肠癌患者中更可能对抗 EGFR 治疗有反应者。我们系统地评价了 EGFR 相关的下游分子靶点 KRAS 后药物遗传学检测在转移性结直肠癌治疗中的获益和危害。我们从 2000 年 1 月至 2010 年 11 月检索了 5 个电子数据库,并对灰色文献和会议摘要进行了单独检索。2 位评价者独立地对所有文章的相关性和质量进行了评价。我们发现了 27 项研究,主要为质量中等至较差、回顾性小样本和单臂队列研究,患者人群有显著重叠。我们发现了 7 项研究独立于患者人群研究 BRAF,1 项研究 NRAS,4 项研究 PIK3CA,8 项研究 PTEN 表达,5 项研究 AKT 表达。关于 BRAF、NRAS 和 PIK3CA 的最佳证据来自于来自 7 个欧洲国家的对化疗耐药患者的最大的回顾性研究(n=649)。在该研究中,BRAF 突变见于 6.5%的 KRAS 野生型肿瘤中。只有 8.3%的 BRAF 突变者,而非 38%的无 BRAF 突变者(p=0.0012)对含 cetuximab 的化疗有反应。临床敏感性和假阳性率(1-特异性)估计值分别为 9.8%(95%CI 6.3,14.5)和 1.6%(95%CI 0.2,5.6)。BRAF 突变也与更差的中位无进展生存期(绝对差异 18 周,p<0.0001)和总生存期(绝对差异 28 周,p<0.0001)相关。在唯一一项研究中,比较了那些接受(n=227)和未接受(n=332) cetuximab 联合化疗者的结局,无论是否接受 cetuximab,BRAF 突变者的生存结局更差。尽管 NRAS 和 PIK3CA 外显子 20 突变也与无这些突变者相比更差的结局相关,但证据基于少数鉴定的突变。关于 PTEN 和 AKT 蛋白表达的证据更稀疏,并且受到评估蛋白表达的可变方法的限制。关于转移性结直肠癌患者药物遗传学检测的临床有效性的低质量证据提示,BRAF 突变与更差的治疗反应和生存结局相关,尽管这种关联可能独立于 EGFR 抑制剂的治疗。
