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Detection of common and less frequent EGFR mutations in cytological samples of lung cancer

机译:检测肺癌细胞学样本中常见和较不常见的EGFR突变

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Objective: Lung cancer represents the leading cause of cancer death. EGFR mutations, detected in 10-40% of lung adenocarcinomas, are an essential key to therapeutic management. EGFR-activated mutations comprise mainly deletions in exon 19 and point mutations in exon 21. Although histology is the traditional method of detection, we investigated the role of cytology in EGFR mutations. Study Design: A total of 774 lung cancers were studied for EGFR mutations (676 histological and 98 cytological samples), including 424 adenocarcinomas, 326 non-small cell lung carcinomas not otherwise specified, and 24 squamous cell carcinomas. Results: We had a total of 164 (21.2%) cases of mutations. Common mutations were short in-frame deletions in exon 19 (53.7%) and single-nucleotide substitutions in exon 21 (34.1%); less frequent mutations included single-nucleotide substitutions in exon 18 (3.7%) and in-frame insertions/deletions in exon 20 (8.5%). Histologically, EGFR mutations in exons 19 and 21 occurred in 19.4% and in exons 18 and 20 in 2.2%, while the rates cytologically were 13.3% for exons 19 and 21 and 5.1% for exons 18 and 20. Conclusions: The sensitivity for the detection of EGFR mutations in cytological samples overlaps histology, so the use of cytological material constitutes an adequate approach for treatment selection in patients with locally advanced or metastatic lung cancer.
机译:目的:肺癌是癌症死亡的主要原因。在10%至40%的肺腺癌中检测到的EGFR突变是治疗管理的关键。 EGFR激活的突变主要包括第19外显子的缺失和第21外显子的点突变。尽管组织学是传统的检测方法,但我们调查了细胞学在EGFR突变中的作用。研究设计:共对774例EGFR突变的肺癌进行了研究(676例组织学和98例细胞学样本),包括424例腺癌,326例未另行指明的非小细胞肺癌和24例鳞状上皮癌。结果:我们总共有164例(21.2%)突变案例。常见的突变是第19外显子的短框内缺失(53.7%)和第21外显子的单核苷酸取代(34.1%)。频率较低的突变包括第18外显子的单核苷酸取代(3.7%)和第20外显子的框内插入/缺失(8.5%)。组织学上,第19和21外显子的EGFR突变发生率为19.4%,第18和20外显子的EGFR突变发生率为2.2%,而第19和21外显子的细胞学发生率为13.3%,第18和20外显子发生率为5.1%。细胞学样品中EGFR突变的检测与组织学重叠,因此使用细胞学材料构成局部晚期或转移性肺癌患者治疗选择的适当方法。

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