J Clin Invest. 2014 Apr;124(4):1582-6. doi: 10.1172/JCI72763. Epub 2014 Feb 24.
Targeted cancer therapies often induce "outlier" responses in molecularly defined patient subsets. One patient with advanced-stage lung adenocarcinoma, who was treated with oral sorafenib, demonstrated a near-complete clinical and radiographic remission for 5 years. Whole-genome sequencing and RNA sequencing of primary tumor and normal samples from this patient identified a somatic mutation, ARAF S214C, present in the cancer genome and expressed at high levels. Additional mutations affecting this residue of ARAF and a nearby residue in the related kinase RAF1 were demonstrated across 1% of an independent cohort of lung adenocarcinoma cases. The ARAF mutations were shown to transform immortalized human airway epithelial cells in a sorafenib-sensitive manner. These results suggest that mutant ARAF is an oncogenic driver in lung adenocarcinoma and an indicator of sorafenib response.
靶向癌症疗法通常会在分子定义的患者亚组中引起“异常”反应。一名晚期肺腺癌患者接受索拉非尼口服治疗,5 年内临床和影像学完全缓解。对该患者的原发肿瘤和正常样本进行全基因组测序和 RNA 测序,发现了一个存在于肿瘤基因组中并高水平表达的体细胞突变 ARAF S214C。在独立的肺腺癌病例队列中,有 1%的病例显示出影响该 ARAF 残基和相关激酶 RAF1 附近残基的其他突变。研究表明,突变的 ARAF 以索拉非尼敏感的方式转化为永生化的人呼吸道上皮细胞。这些结果表明,突变的 ARAF 是肺腺癌的致癌驱动因子,也是索拉非尼反应的标志物。
