对难治性抗表皮生长因子受体(EGFR)治疗的结直肠癌患者循环肿瘤DNA中的克隆选择模式进行表征。
Characterizing the patterns of clonal selection in circulating tumor DNA from patients with colorectal cancer refractory to anti-EGFR treatment.
作者信息
Morelli M P, Overman M J, Dasari A, Kazmi S M A, Mazard T, Vilar E, Morris V K, Lee M S, Herron D, Eng C, Morris J, Kee B K, Janku F, Deaton F L, Garrett C, Maru D, Diehl F, Angenendt P, Kopetz S
机构信息
Department of Gastrointestinal Medical Oncology.
Department of Gastrointestinal Medical Oncology; Clinical Cancer Prevention.
出版信息
Ann Oncol. 2015 Apr;26(4):731-736. doi: 10.1093/annonc/mdv005. Epub 2015 Jan 26.
INTRODUCTION
KRAS and EGFR ectodomain-acquired mutations in patients with metastatic colorectal cancer (mCRC) have been correlated with acquired resistance to anti-EGFR monoclonal antibodies (mAbs). We investigated the frequency, co-occurrence, and distribution of acquired KRAS and EGFR mutations in patients with mCRC refractory to anti-EGFR mAbs using circulating tumor DNA (ctDNA).
PATIENTS AND METHODS
Sixty-two post-treatment plasma and 20 matching pretreatment archival tissue samples from KRAS (wt) mCRC patients refractory to anti-EGFR mAbs were evaluated by high-sensitivity emulsion polymerase chain reaction for KRAS codon 12, 13, 61, and 146 and EGFR 492 mutations.
RESULTS
Plasma analyses showed newly detectable EGFR and KRAS mutations in 5/62 [8%; 95% confidence interval (CI) 0.02-0.18] and 27/62 (44%; 95% CI 0.3-0.56) samples, respectively. KRAS codon 61 and 146 mutations were predominant (33% and 11%, respectively), and multiple EGFR and/or KRAS mutations were detected in 11/27 (41%) cases. The percentage of mutant allele reads was inversely correlated with time since last treatment with EGFR mAbs (P = 0.038). In the matching archival tissue, these mutations were detectable as low-allele-frequency clones in 35% of patients with plasma mutations after treatment with anti-EGFR mAbs and correlated with shorter progression-free survival (PFS) compared with the cases with no new mutations (3.0 versus 8.0 months, P = 0.0004).
CONCLUSION
Newly detected KRAS and/or EGFR mutations in plasma ctDNA from patients refractory to anti-EGFR treatment appear to derive from rare, pre-existing clones in the primary tumors. These rare clones were associated with shorter PFS in patients receiving anti-EGFR treatment. Multiple simultaneous mutations in KRAS and EGFR in the ctDNA and the decline in allele frequency after discontinuation of anti-EGFR therapy in a subset of patients suggest that several resistance mechanisms can co-exist and that relative clonal burdens may change over time. Monitoring treatment-induced genetic alterations by sequencing ctDNA could identify biomarkers for treatment screening in anti-EGFR-refractory patients.
引言
转移性结直肠癌(mCRC)患者中KRAS和表皮生长因子受体(EGFR)胞外域获得性突变与抗EGFR单克隆抗体(mAb)获得性耐药相关。我们使用循环肿瘤DNA(ctDNA)研究了对抗EGFR mAb难治的mCRC患者中获得性KRAS和EGFR突变的频率、共现情况及分布。
患者与方法
对62例抗EGFR mAb难治的KRAS(野生型)mCRC患者治疗后的血浆样本以及20例匹配的治疗前存档组织样本进行高灵敏度乳液聚合酶链反应,检测KRAS密码子12、13、61和146以及EGFR 492突变。
结果
血浆分析显示,分别在5/62(8%;95%置信区间[CI] 0.02 - 0.18)和27/62(44%;95% CI 0.3 - 0.56)的样本中检测到新的可检测到的EGFR和KRAS突变。KRAS密码子61和146突变占主导(分别为33%和11%),11/27(41%)的病例中检测到多个EGFR和/或KRAS突变。突变等位基因读数百分比与上次使用EGFR mAb治疗后的时间呈负相关(P = 0.038)。在匹配的存档组织中,抗EGFR mAb治疗后,35%血浆突变患者中这些突变可作为低等位基因频率克隆被检测到,与无新突变的病例相比,其无进展生存期(PFS)更短(3.0个月对8.0个月,P = 0.0004)。
结论
抗EGFR治疗难治患者血浆ctDNA中新检测到的KRAS和/或EGFR突变似乎源自原发肿瘤中罕见的、预先存在的克隆。这些罕见克隆与接受抗EGFR治疗患者的较短PFS相关。ctDNA中KRAS和EGFR同时发生多个突变以及部分患者停用抗EGFR治疗后等位基因频率下降,提示多种耐药机制可能共存,且相对克隆负担可能随时间变化。通过对ctDNA进行测序监测治疗诱导的基因改变,可为抗EGFR难治患者的治疗筛选鉴定生物标志物。
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