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肺腺癌中表皮生长因子受体突变特异性免疫组化抗体

Epidermal growth factor receptor mutation-specific immunohistochemical antibodies in lung adenocarcinoma.

作者信息

Allo Ghassan, Bandarchi Bizhan, Yanagawa Naoki, Wang Ami, Shih Warren, Xu Jing, Dalby Morgan, Nitta Hiroaki, To Christine, Liu Ni, Sykes Jenna, Tsao Ming S

机构信息

Department of Pathology, Princess Margaret Cancer Centre, University Health Network, Toronto, ON, Canada; Department of Laboratory Medicine and Pathobiology, University of Toronto, Toronto, ON, Canada.

出版信息

Histopathology. 2014 May;64(6):826-39. doi: 10.1111/his.12331. Epub 2014 Jan 29.

DOI:10.1111/his.12331
PMID:24251405
Abstract

AIMS

We investigated the sensitivity and specificity of two novel Epidermal growth factor receptor (EGFR) mutation-specific antibodies in the detection of the most common EGFR mutations in lung adenocarcinoma.

METHODS AND RESULTS

A total of 241 resected lung adenocarcinoma specimens and six resected post-neoadjuvant gefitinib adenocarcinomas were analysed for EGFR mutation using mass spectrometry, fragment analysis and direct PCR sequencing platforms. Tissue arrays and/or full sections of these cases were evaluated using immunohistochemistry with two novel antibodies (clones SP125 and SP111) and two previously reported antibodies (clones 43B2 and 6B6), specific for L858R or 15-nucleotide exon-19 deletion EGFR mutations. SP125 antibody detected EGFR L858R mutation with a sensitivity of 76% and positive predictive value of 73%. SP111 antibody stained the 15-nucleotide EGFR exon-19 deletions with a sensitivity of 83% and a positive predictive value of 94%. Pretreatment with gefitinib did not affect antibody performance. Full-section immunohistochemical staining detected heterogeneous mutant EGFR proteins expression in tumours, and revealed L858R mutation in the non-neoplastic bronchial epithelium adjacent to EGFR L858R-carrying carcinomas in three of 16 (19%) cases.

CONCLUSIONS

Immunohistochemistry using EGFR mutant-specific antibodies may be useful in shortening the diagnostic time of lung adenocarcinoma with most common EGFR mutations, especially in samples with low tumour cellularity.

摘要

目的

我们研究了两种新型表皮生长因子受体(EGFR)突变特异性抗体在检测肺腺癌中最常见EGFR突变时的敏感性和特异性。

方法与结果

使用质谱、片段分析和直接PCR测序平台对总共241例切除的肺腺癌标本和6例新辅助吉非替尼治疗后切除的腺癌标本进行EGFR突变分析。使用两种新型抗体(克隆号SP125和SP111)和两种先前报道的抗体(克隆号43B2和6B6)进行免疫组织化学评估,这些抗体对L858R或15个核苷酸的外显子19缺失EGFR突变具有特异性,对这些病例的组织芯片和/或全切片进行评估。SP125抗体检测EGFR L858R突变的敏感性为76%,阳性预测值为73%。SP111抗体对15个核苷酸的EGFR外显子19缺失进行染色,敏感性为83%,阳性预测值为94%。吉非替尼预处理不影响抗体性能。全切片免疫组织化学染色检测到肿瘤中EGFR突变蛋白表达存在异质性,并在16例(19%)病例中的3例中,在携带EGFR L858R的癌旁非肿瘤性支气管上皮中发现了L858R突变。

结论

使用EGFR突变特异性抗体的免疫组织化学可能有助于缩短诊断最常见EGFR突变的肺腺癌的时间,尤其是在肿瘤细胞含量低的样本中。

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