Shaw Alice T, Yeap Beow Y, Mino-Kenudson Mari, Digumarthy Subba R, Costa Daniel B, Heist Rebecca S, Solomon Benjamin, Stubbs Hannah, Admane Sonal, McDermott Ultan, Settleman Jeffrey, Kobayashi Susumu, Mark Eugene J, Rodig Scott J, Chirieac Lucian R, Kwak Eunice L, Lynch Thomas J, Iafrate A John
Department of Pathology, Massachusetts General Hospital, Warren 501c, 55 Fruit St, Boston, MA 02114, USA.
J Clin Oncol. 2009 Sep 10;27(26):4247-53. doi: 10.1200/JCO.2009.22.6993. Epub 2009 Aug 10.
The EML4-ALK fusion oncogene represents a novel molecular target in a small subset of non-small-cell lung cancers (NSCLC). To aid in identification and treatment of these patients, we examined the clinical characteristics and treatment outcomes of patients who had NSCLC with and without EML4-ALK.
Patients with NSCLC were selected for genetic screening on the basis of two or more of the following characteristics: female sex, Asian ethnicity, never/light smoking history, and adenocarcinoma histology. EML4-ALK was identified by using fluorescent in situ hybridization for ALK rearrangements and was confirmed by immunohistochemistry for ALK expression. EGFR and KRAS mutations were determined by DNA sequencing.
Of 141 tumors screened, 19 (13%) were EML4-ALK mutant, 31 (22%) were EGFR mutant, and 91 (65%) were wild type (WT/WT) for both ALK and EGFR. Compared with the EGFR mutant and WT/WT cohorts, patients with EML4-ALK mutant tumors were significantly younger (P < .001 and P = .005) and were more likely to be men (P = .036 and P = .039). Patients with EML4-ALK-positive tumors, like patients who harbored EGFR mutations, also were more likely to be never/light smokers compared with patients in the WT/WT cohort (P < .001). Eighteen of the 19 EML4-ALK tumors were adenocarcinomas, predominantly the signet ring cell subtype. Among patients with metastatic disease, EML4-ALK positivity was associated with resistance to EGFR tyrosine kinase inhibitors (TKIs). Patients in the EML4-ALK cohort and the WT/WT cohort showed similar response rates to platinum-based combination chemotherapy and no difference in overall survival.
EML4-ALK defines a molecular subset of NSCLC with distinct clinical characteristics. Patients who harbor this mutation do not benefit from EGFR TKIs and should be directed to trials of ALK-targeted agents.
EML4-ALK融合致癌基因是一小部分非小细胞肺癌(NSCLC)中的一种新型分子靶点。为了帮助识别和治疗这些患者,我们研究了伴有和不伴有EML4-ALK的NSCLC患者的临床特征和治疗结果。
根据以下两个或更多特征选择NSCLC患者进行基因筛查:女性、亚洲人种、从不/轻度吸烟史和腺癌组织学类型。通过荧光原位杂交检测ALK重排来鉴定EML4-ALK,并通过免疫组织化学检测ALK表达进行确认。通过DNA测序确定EGFR和KRAS突变。
在筛查的141个肿瘤中,19个(13%)为EML4-ALK突变型,31个(22%)为EGFR突变型,91个(65%)ALK和EGFR均为野生型(WT/WT)。与EGFR突变型和WT/WT队列相比,EML4-ALK突变型肿瘤患者明显更年轻(P < .001和P = .005)且更可能为男性(P = .036和P = .039)。与WT/WT队列中的患者相比,EML4-ALK阳性肿瘤患者与携带EGFR突变的患者一样,也更可能从不/轻度吸烟(P < .001)。19个EML4-ALK肿瘤中有18个为腺癌,主要是印戒细胞亚型。在转移性疾病患者中,EML4-ALK阳性与对EGFR酪氨酸激酶抑制剂(TKIs)耐药相关。EML4-ALK队列和WT/WT队列中的患者对铂类联合化疗的反应率相似,总生存期无差异。
EML4-ALK定义了具有独特临床特征的NSCLC分子亚群。携带这种突变的患者不能从EGFR TKIs中获益,应接受ALK靶向药物试验。
