中国非小细胞肺癌患者中存在涉及外显子19和21的表皮生长因子受体双重激活突变。
Epidermal growth factor receptor double activating mutations involving both exons 19 and 21 exist in Chinese non-small cell lung cancer patients.
作者信息
Zhang G-C, Lin J-Y, Wang Z, Zhou Q, Xu C-R, Zhu J-Q, Wang K, Yang X-N, Chen G, Yang J-J, Huang Y-J, Liao R-Q, Wu Y-L
机构信息
Cancer Center, Sun Yat-Sen University, and Lung Cancer Research Institute, Guangdong Provincial People's Hospital, Dong Chuan Road, Guangzhou 510080, People's Republic of China.
出版信息
Clin Oncol (R Coll Radiol). 2007 Sep;19(7):499-506. doi: 10.1016/j.clon.2007.04.006. Epub 2007 May 29.
AIMS
It has been shown that the introduction of a second mutation into the already mutated epidermal growth factor receptor (EGFR) in non-small cell lung cancer (NSCLC) will alter the sensitivity to tyrosine kinase inhibitors (TKIs). EGFR double activating mutations involving both exons 19 and 21 were previously detected in Asian patients, but the sensitivity to TKIs had not yet been characterised. Our objective was to profile the status of EGFR double mutations in Chinese NSCLC patients and to further ascertain the biological properties.
MATERIALS AND METHODS
In total, 145 NSCLC tumour samples from unselected Chinese NSCLC patients were sequenced to screen mutations in exons 18, 19 and 21 of EGFR. Five patients were detected to harbour the delE746-A750+L858R double activating mutations. Subcloning experiments were carried out, expression vectors inserted with corresponding full-length EGFR were constructed, and in vitro transient transfections were performed in 293T cells. Whole cell lysates were collected to assess the sensitivity to TKIs using immunoblotting.
RESULTS
All five patients had adenocarcinoma. The frequency of double mutations was 3.4% (5/145). Three patients received and responded to gefitinib treatment. Subcloning experiments showed that all the subclones were either wild type or double mutated. At a concentration of TKIs of 0.1 microM, the autophosphorylation of the double mutant was inhibited greater than that of either single mutated EGFR. However, the difference disappeared when the concentration increased to 1 microM.
CONCLUSIONS
delE746-A750+L858R double activating EGFR mutations exist in Chinese NSCLC patients and both locate on the same allele. These patients tend to respond well to TKIs and the sensitivity to TKIs of this double mutated EGFR is enhanced compared with either single mutant. Nonetheless, the alteration in downstream signal transduction of the double mutant remains to be determined.
目的
研究表明,在非小细胞肺癌(NSCLC)中,已发生突变的表皮生长因子受体(EGFR)引入第二个突变会改变对酪氨酸激酶抑制剂(TKIs)的敏感性。此前在亚洲患者中检测到涉及外显子19和21的EGFR双重激活突变,但对TKIs的敏感性尚未明确。我们的目的是分析中国NSCLC患者中EGFR双重突变的状态,并进一步确定其生物学特性。
材料与方法
对145例未经选择的中国NSCLC患者的肿瘤样本进行测序,以筛查EGFR外显子18、19和21的突变。检测到5例患者携带delE746 - A750 + L858R双重激活突变。进行亚克隆实验,构建插入相应全长EGFR的表达载体,并在293T细胞中进行体外瞬时转染。收集全细胞裂解物,采用免疫印迹法评估对TKIs的敏感性。
结果
所有5例患者均为腺癌。双重突变的频率为3.4%(5/145)。3例患者接受吉非替尼治疗并产生反应。亚克隆实验表明,所有亚克隆均为野生型或双重突变型。在TKIs浓度为0.1微摩尔时,双重突变体的自磷酸化抑制程度大于单突变EGFR。然而,当浓度增加到1微摩尔时,差异消失。
结论
中国NSCLC患者中存在delE746 - A750 + L858R双重激活EGFR突变,且均位于同一等位基因上。这些患者对TKIs往往反应良好,与单突变相比,这种双重突变EGFR对TKIs的敏感性增强。尽管如此,双重突变体下游信号转导的改变仍有待确定。
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