首页> 外文OA文献 >Refining the diagnosis and EGFR status of non-small cell lung carcinoma in biopsy and cytologic material, using a panel of mucin staining, TTF-1, cytokeratin 5/6, and P63, and EGFR mutation analysis.
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Refining the diagnosis and EGFR status of non-small cell lung carcinoma in biopsy and cytologic material, using a panel of mucin staining, TTF-1, cytokeratin 5/6, and P63, and EGFR mutation analysis.

机译:使用一组粘蛋白染色,TTF-1,细胞角蛋白5/6和P63以及EGFR突变分析,完善活检和细胞学材料中非小细胞肺癌的诊断和EGFR状态。

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摘要

INTRODUCTION: The dichotomization of non-small cell carcinoma (NSCLC) subtype into squamous (SQCC) and adenocarcinoma (ADC) has become important in recent years and is increasingly required with regard to management. The aim of this study was to determine the utility of a panel of commercially available antibodies in refining the diagnosis on small biopsies and also to determine whether cytologic material is suitable for somatic EGFR genotyping in a prospectively analyzed series of patients undergoing investigation for suspected lung cancer. METHODS: Thirty-two consecutive cases of NSCLC were first tested using a panel comprising cytokeratin 5/6, P63, thyroid transcription factor-1, 34betaE12, and a D-PAS stain for mucin, to determine their value in refining diagnosis of NSCLC. After this test phase, two further pathologists independently reviewed the cases using a refined panel that excluded 34betaE12 because of its low specificity for SQCC, and refinement of diagnosis and concordance were assessed. Ten cases of ADC, including eight derived from cytologic samples, were sent for EGFR mutation analysis. RESULTS: There was refinement of diagnosis in 65% of cases of NSCLC to either SQCC or ADC in the test phase. This included 10 of 13 cases where cell pellets had been prepared from transbronchial needle aspirates. Validation by two further pathologists with varying expertise in lung pathology confirmed increased refinement and concordance of diagnosis. All samples were adequate for analysis, and they all showed a wild-type EGFR genotype. CONCLUSION: A panel comprising cytokeratin 5/6, P63, thyroid transcription factor-1, and a D-PAS stain for mucin increases diagnostic accuracy and agreement between pathologists when faced with refining a diagnosis of NSCLC to SQCC or ADC. These small samples, even cell pellets derived from transbronchial needle aspirates, seem to be adequate for EGFR mutation analysis.
机译:简介:近年来,将非小细胞癌(NSCLC)亚型分为鳞状(SQCC)和腺癌(ADC)变得很重要,并且在管理方面也越来越需要。这项研究的目的是确定一组可购得的抗体在完善小型活检诊断中的实用性,并确定细胞学材料是否适合接受前瞻性分析的一系列疑似肺癌患者的体表EGFR基因分型。方法:首先使用包含细胞角蛋白5/6,P63,甲状腺转录因子-1、34betaE12和D-PAS粘液染色的试剂盒对32例连续的NSCLC病例进行检测,以确定其在细化NSCLC诊断中的价值。在该测试阶段之后,另外两名病理学家使用经过精制的小组独立审查了病例,该小组排除了34betaE12,因为它对SQCC的特异性较低,并评估了诊断和一致性的细化程度。十例ADC,包括八例来自细胞学样本的ADC被送去进行EGFR突变分析。结果:在测试阶段中,有65%的NSCLC病例中SQCC或ADC的诊断有所改善。这包括13例中有10例由经支气管针抽吸物制备细胞沉淀的病例。由另外两名在肺病理学方面具有不同专长的病理学家进行的验证证实,诊断的细化程度和一致性得到了提高。所有样品均足以进行分析,并且均显示出野生型EGFR基因型。结论:包含细胞角蛋白5/6,P63,甲状腺转录因子-1和D-PAS粘液染色的检测组在将NSCLC诊断细化为SQCC或ADC时提高了诊断准确性,并提高了病理学家之间的一致性。这些小样本,甚至是从经支气管针吸出的细胞沉淀,似乎也足以进行EGFR突变分析。

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