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Assessment of EGFR Mutation Status in Lung Adenocarcinoma by Immunohistochemistry Using Antibodies Specific to the Two Major Forms of Mutant EGFR

机译:使用两种主要形式的突变EGFR特异性抗体通过免疫组织化学评估肺腺癌中EGFR突变状态

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摘要

EGFR mutations are the best predictors of response to EGFR kinase inhibitors in lung adenocarcinoma. We evaluated two mutation-specific monoclonal antibodies for the detection of EGFR mutations by immunohistochemistry (IHC), generated respectively against the L858R mutant and the exon 19 mutant with the common 15bp/5AA deletion. These two mutations account for approximately 90% of all EGFR mutations. IHC staining performed on 218 paraffin-embedded lung adenocarcinomas was assessed on a 0 to 3+ scale, and positivity cutoffs of 1+ and 2+ were compared. All cases were studied by standard molecular methods for these two mutations, and selected cases were also studied using higher sensitivity molecular assays. The EGFR L858R mutant antibody showed a sensitivity of 95% and a positive predictive value (PPV) of 99% with a positivity cutoff of 1+ and a sensitivity of 76% and a PPV of 100% with a positivity cutoff of 2+. The EGFR exon 19 mutant–specific antibody showed reduced sensitivity for exon 19 deletions other than 15bp. A positivity cutoff of 1+ resulted in a sensitivity of 85% and a PPV of 99%, whereas a 2+ cutoff gave a sensitivity of 67% and a PPV of 100%. IHC with EGFR mutant–specific antibodies could be used as a screen to identify most candidates for EGFR inhibitors.
机译:EGFR突变是肺腺癌中对EGFR激酶抑制剂反应的最佳预测指标。我们评估了两种突变特异性单克隆抗体,用于通过免疫组织化学(IHC)检测EGFR突变,分别针对L858R突变体和具有常见15bp / 5AA缺失的外显子19突变体生成。这两个突变约占所有EGFR突变的90%。在0至3+的等级上评估了对218种石蜡包埋的肺腺癌的IHC染色,并比较了1+和2+的阳性截止值。所有病例均通过标准分子方法对这两个突变进行了研究,并使用更高灵敏度的分子分析对选定病例进行了研究。 EGFR L858R突变型抗体显示出95%的敏感性和99%的阳性预测值(PPV),阳性截止值为1+,灵敏度为76%,PPV为100%,阳性截止值为2+。 EGFR外显子19突变体特异性抗体显示出对15bp以外的19外显子缺失的敏感性降低。阳性截断值为1+时,灵敏度为85%,PPV为99%,而阳性截断值为2+时,灵敏度为67%,PPV为100%。带有EGFR突变体特异性抗体的IHC可以用作鉴定大多数EGFR抑制剂候选药物的筛选。

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