Cho Jeonghee, Bass Adam J, Lawrence Michael S, Cibulskis Kristian, Cho Ahye, Lee Shi-Nai, Yamauchi Mai, Wagle Nikhil, Pochanard Panisa, Kim Nayoung, Park Angela Kj, Won Jonghwa, Hur Hyung-Suk, Greulich Heidi, Ogino Shuji, Sougnez Carrie, Voet Douglas, Tabernero Josep, Jimenez Jose, Baselga Jose, Gabriel Stacey B, Lander Eric S, Getz Gad, Eck Michael J, Park Woong-Yang, Meyerson Matthew
Department of Medical Oncology, Dana-Farber Cancer Institute, Boston MA 02115, USA.
Mol Cancer. 2014 Jun 4;13:141. doi: 10.1186/1476-4598-13-141.
Inhibition of the activated epidermal growth factor receptor (EGFR) with either enzymatic kinase inhibitors or anti-EGFR antibodies such as cetuximab, is an effective modality of treatment for multiple human cancers. Enzymatic EGFR inhibitors are effective for lung adenocarcinomas with somatic kinase domain EGFR mutations while, paradoxically, anti-EGFR antibodies are more effective in colon and head and neck cancers where EGFR mutations occur less frequently. In colorectal cancer, anti-EGFR antibodies are routinely used as second-line therapy of KRAS wild-type tumors. However, detailed mechanisms and genomic predictors for pharmacological response to these antibodies in colon cancer remain unclear.
We describe a case of colorectal adenocarcinoma, which was found to harbor a kinase domain mutation, G724S, in EGFR through whole genome sequencing. We show that G724S mutant EGFR is oncogenic and that it differs from classic lung cancer derived EGFR mutants in that it is cetuximab responsive in vitro, yet relatively insensitive to small molecule kinase inhibitors. Through biochemical and cellular pharmacologic studies, we have determined that cells harboring the colon cancer-derived G719S and G724S mutants are responsive to cetuximab therapy in vitro and found that the requirement for asymmetric dimerization of these mutant EGFR to promote cellular transformation may explain their greater inhibition by cetuximab than small-molecule kinase inhibitors.
The colon-cancer derived G719S and G724S mutants are oncogenic and sensitive in vitro to cetuximab. These data suggest that patients with these mutations may benefit from the use of anti-EGFR antibodies as part of the first-line therapy.
使用酶促激酶抑制剂或西妥昔单抗等抗表皮生长因子受体(EGFR)抗体抑制活化的EGFR,是治疗多种人类癌症的有效方法。酶促EGFR抑制剂对具有体细胞激酶结构域EGFR突变的肺腺癌有效,而矛盾的是,抗EGFR抗体在EGFR突变较少发生的结肠癌和头颈癌中更有效。在结直肠癌中,抗EGFR抗体通常用作KRAS野生型肿瘤的二线治疗。然而,这些抗体在结肠癌中药物反应的详细机制和基因组预测指标仍不清楚。
我们描述了一例结肠腺癌病例,通过全基因组测序发现其EGFR中存在激酶结构域突变G724S。我们表明,G724S突变型EGFR具有致癌性,并且它与经典肺癌衍生的EGFR突变体不同,在于它在体外对西妥昔单抗有反应,但对小分子激酶抑制剂相对不敏感。通过生化和细胞药理学研究,我们确定携带结肠癌衍生的G719S和G724S突变体的细胞在体外对西妥昔单抗治疗有反应,并发现这些突变型EGFR不对称二聚化以促进细胞转化的需求可能解释了它们比小分子激酶抑制剂更易被西妥昔单抗抑制。
结肠癌衍生的G719S和G724S突变体具有致癌性,且在体外对西妥昔单抗敏感。这些数据表明,携带这些突变的患者可能受益于使用抗EGFR抗体作为一线治疗的一部分。
