EGFR autophosphorylation but not protein score correlates with histologic and molecular subtypes in lung adenocarcinoma.

Judit Moldvay, Tamás Barbai, Krisztina Bogos, Violetta Piurko, János Fillinger, Helmut H Popper, József Tímár
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引用次数: 2

Abstract

Established clinicopathologic characteristics of non-small cell lung cancer patients define a subgroup responding better to EGFR-TK inhibitors: adenocarcinoma histology, ethnicity, sex, smoking status, presence of activating EGFR mutation, and/or K-RAS wild type. However, EGFR mutation does not automatically lead to increased activity of the protein influenced by several factors. As adenocarcinoma can be further divided into histologic subclasses, we compared adenocarcinomas without lepidic growth pattern (NLAC) to those characterized by pure or predominant lepidic growth (LAC) for EGFR protein expression and autophosphorylation activity (Y1173), as determined by immunohistochemistry. This pretarget therapy cohort comprised a total of 110 surgically operated patients of stage I non-small cell lung cancer: 49 NLAC and 61 LAC variants. The LAC group had a significantly better prognosis and the incidence of phospho-EGFR-positive tumors was significantly higher compared with NLAC. Patient sex did not influence EGFR activity, but the incidence of pEGFR-positive tumors was significantly lower among smoker patients. There was no statistically significant difference in EGFR or KRAS mutation frequencies between the 2 groups. In NLAC, pEGFR-positive tumors occurred exclusively among EGFR-mutant/K-RAS wild-type tumors. On the contrary, in LAC tumors, pEGFR-positive tumors were similarly frequent in the EGFR or K-RAS mutant groups indicating an interesting feedback activation of EGFR signaling in K-RAS mutant tumors. Our data also indicate that EGFR mutation leads to EGFR autophosphorylation only in a small fraction of adenocarcinoma patients, which might have clinical significance.

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EGFR自磷酸化与肺腺癌的组织学和分子亚型相关,但与蛋白评分无关。
非小细胞肺癌患者的既定临床病理特征定义了一个对EGFR- tk抑制剂反应更好的亚组:腺癌组织学、种族、性别、吸烟状况、激活EGFR突变的存在和/或K-RAS野生型。然而,EGFR突变不会自动导致受多种因素影响的蛋白质活性增加。由于腺癌可以进一步划分为组织学亚类,我们比较了没有鳞状生长模式(NLAC)的腺癌和具有鳞状生长模式(LAC)的腺癌的EGFR蛋白表达和自磷酸化活性(Y1173),这是由免疫组织化学测定的。该预靶向治疗队列共包括110例手术治疗的I期非小细胞肺癌患者:49例NLAC和61例LAC变体。LAC组预后明显好于NLAC组,且磷酸化egfr阳性肿瘤发生率明显高于NLAC组。患者性别对EGFR活性没有影响,但吸烟患者中pegfr阳性肿瘤的发生率明显较低。两组间EGFR、KRAS突变频率差异无统计学意义。在NLAC中,pegfr阳性肿瘤仅发生在egfr突变/K-RAS野生型肿瘤中。相反,在LAC肿瘤中,pegfr阳性肿瘤在EGFR或K-RAS突变组中同样频繁,这表明在K-RAS突变肿瘤中EGFR信号的有趣反馈激活。我们的数据还表明,EGFR突变仅在一小部分腺癌患者中导致EGFR自磷酸化,这可能具有临床意义。
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期刊介绍: Diagnostic Molecular Pathology focuses on providing clinical and academic pathologists with coverage of the latest molecular technologies, timely reviews of established techniques, and papers on the applications of these methods to all aspects of surgical pathology and laboratory medicine. It publishes original, peer-reviewed contributions on molecular probes for diagnosis, such as tumor suppressor genes, oncogenes, the polymerase chain reaction (PCR), and in situ hybridization. Articles demonstrate how these highly sensitive techniques can be applied for more accurate diagnosis.
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