RAS/PIK3CA/BRAF肿瘤突变作为转移性结直肠癌患者一线贝伐单抗化疗反应预测指标的回顾性研究。
Retrospective study of RAS/PIK3CA/BRAF tumor mutations as predictors of response to first-line chemotherapy with bevacizumab in metastatic colorectal cancer patients.
作者信息
Nakayama Izuma, Shinozaki Eiji, Matsushima Tomohiro, Wakatsuki Takeru, Ogura Mariko, Ichimura Takashi, Ozaka Masato, Takahari Daisuke, Suenaga Mitsukuni, Chin Keisho, Mizunuma Nobuyuki, Yamaguchi Kensei
机构信息
Department of Gastroenterology, Cancer Institute Hospital of the Japanese Foundation for Cancer Research, 3-8-31 Ariake, Koto-ku, Tokyo, 135-8550, Japan.
出版信息
BMC Cancer. 2017 Jan 9;17(1):38. doi: 10.1186/s12885-016-2994-6.
BACKGROUND
After analysis of minor RAS mutations (KRAS exon 3, 4/NRAS) in the FIRE-3 and PRIME studies, an expanded range of RAS mutations were established as a negative predictive marker for the efficacy of anti-EGFR antibody treatment. BRAF and PIK3CA mutations may be candidate biomarkers for anti-EGFR targeted therapies. However, it remains unknown whether RAS/PIK3CA/BRAF tumor mutations can predict the efficacy of bevacizumab in metastatic colorectal cancer. We assessed whether selection according to RAS/PIK3CA/BRAF mutational status could be beneficial for patients treated with bevacizumab as first-line treatment for metastatic colorectal cancer.
METHODS
Of the 1001 consecutive colorectal cancer patients examined for RAS, PIK3CA, and BRAF tumor mutations using a multiplex kit (Luminex®), we studied 90 patients who received combination chemotherapy with bevacizumab as first-line treatment for metastatic colorectal cancer. The objective response rate (ORR) and progression-free survival (PFS) were evaluated according to mutational status.
RESULTS
The ORR was higher among patients with wild-type tumors (64.3%) compared to those with tumors that were only wild type with respect to KRAS exon 2 (54.8%), and the differences in ORR between patients with wild-type and mutant-type tumors were greater when considering only KRAS exon 2 mutations (6.8%) rather than RAS/PIK3CA/BRAF mutations (18.4%). There were no statistically significant differences in ORR or PFS between all wild-type tumors and tumors carrying any of the mutations. Multivariate analysis revealed that liver metastasis and RAS and BRAF mutations were independent negative factors for disease progression after first-line treatment with bevacizumab.
CONCLUSIONS
Patient selection according to RAS/PIK3CA/BRAF mutations could help select patients who will achieve a better response to bevacizumab treatment. We found no clinical benefit of restricting combination therapy with bevacizumab for metastatic colorectal cancer patients with EGFR-wild type tumors.
背景
在对FIRE-3和PRIME研究中的小RAS突变(KRAS外显子3、4/NRAS)进行分析后,确定了更广泛的RAS突变范围作为抗表皮生长因子受体(EGFR)抗体治疗疗效的阴性预测标志物。BRAF和PIK3CA突变可能是抗EGFR靶向治疗的候选生物标志物。然而,RAS/PIK3CA/BRAF肿瘤突变是否能预测贝伐单抗在转移性结直肠癌中的疗效仍不清楚。我们评估了根据RAS/PIK3CA/BRAF突变状态进行选择是否对接受贝伐单抗作为转移性结直肠癌一线治疗的患者有益。
方法
在使用多重试剂盒(Luminex®)检测RAS、PIK3CA和BRAF肿瘤突变的1001例连续结直肠癌患者中,我们研究了90例接受贝伐单抗联合化疗作为转移性结直肠癌一线治疗的患者。根据突变状态评估客观缓解率(ORR)和无进展生存期(PFS)。
结果
野生型肿瘤患者的ORR(64.3%)高于仅KRAS外显子2为野生型的肿瘤患者(54.8%),当仅考虑KRAS外显子2突变(6.8%)而非RAS/PIK3CA/BRAF突变(18.4%)时,野生型和突变型肿瘤患者之间的ORR差异更大。所有野生型肿瘤与携带任何一种突变的肿瘤之间的ORR或PFS无统计学显著差异。多变量分析显示,肝转移以及RAS和BRAF突变是贝伐单抗一线治疗后疾病进展的独立负性因素。
结论
根据RAS/PIK3CA/BRAF突变进行患者选择有助于挑选出对贝伐单抗治疗反应更好的患者。我们发现,对于EGFR野生型肿瘤的转移性结直肠癌患者,限制使用贝伐单抗联合治疗并无临床益处。
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