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首页> 外文期刊>Applied immunohistochemistry and molecular morphology: AIMM >Combination of Napsin A and TTF-1 Immunohistochemistry Helps in Differentiating Primary Lung Adenocarcinoma From MetastaticCarcinoma in the Lung
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Combination of Napsin A and TTF-1 Immunohistochemistry Helps in Differentiating Primary Lung Adenocarcinoma From MetastaticCarcinoma in the Lung

机译:Napsin A和TTF-1免疫组织化学的组合有助于区分原发性肺腺癌和转移性肺癌

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Differentiation of primary from metastatic adenocarcinoma in the lung can be challenging, and it demands sensitive and specific biomarkers, especially when the tissue for diagnosis is limited. Thyroid transcription factor-1 (TTF-1) has been considered a reliable marker for adenocarcinoma of lung origin. However, several recent studies have shown that TTF-1 immunostaining is also positive in adenocarcinomas arising in different organs including colon, endometrium, endocervix, and ovary. In addition, approximately 20% of lung primary adenocarcinomas are negative for TTF-1 immunostaining, and napsin A immunostaining has slightly higher sensitivity in detecting lung primary adenocarcinoma. We performed TTF-1 and napsin A immunostaining on 120 cases of primary lung adenocarcinomas and 37 cases of metastatic carcinomas in the lung. The results showed that 95 (79.2%) of 120 lung primary adenocarcinomas showed napsin A(+)/TTF-l(+) double-positive immunostaining pattern. TTF-1 (-)apsin A(+), TTF-1 (+)/ napsin A(-), and TTF-1 (-)apsin A(-) were seen in 8.3%, 3.3%, and 9.2% lung primary adenocarcinomas, respectively. Eight (21.6%) of the 37 metastatic carcinomas were positive for TTF-1 and they include clear-cell renal cell carcinomas completely negative for napsin A although napsin A was detected in 12 (80.0%) of 15 primary papillary and 3 (33.3%) of 9 primary clear-cell renal cell carcinomas. All renal epithelial neoplasms were TTF-1 negative. These findings indicate that double napsin A and TTF-1-positive immunostaining is highly specific for lung primary adenocarcinoma and the combination of these 2 biomarkers is warranted to help segregating primary lung adenocarcinoma from metastatic carcinoma in the lung.
机译:肺中原发性和转移性腺癌的区分可能具有挑战性,并且需要敏感和特异性的生物标志物,尤其是在诊断组织有限的情况下。甲状腺转录因子-1(TTF-1)被认为是肺源性腺癌的可靠标记。但是,最近的一些研究表明,TTF-1免疫染色在不同器官(包括结肠,子宫内膜,子宫颈内膜和卵巢)产生的腺癌中也呈阳性。此外,大约20%的肺原发性腺癌对TTF-1免疫染色呈阴性,而napsin A免疫染色在检测肺原发性腺癌中具有更高的敏感性。我们对120例原发性肺腺癌和37例肺转移癌进行了TTF-1和napsin A免疫染色。结果表明,在120例肺原发性腺癌中,有95例(79.2%)显示出了Naps A(+)/ TTF-1(+)双阳性免疫染色模式。分别以8.3%,3.3%和9.2%的比率看到TTF-1(-)/纸巾A(+),TTF-1(+)/纸巾A(-)和TTF-1(-)/纸巾A(-) %分别为肺原发性腺癌。在37例转移性癌中,有8例(21.6%)对TTF-1呈阳性,尽管对15例原发性乳头状癌中有12例(80.0%)和3例(33.3%)检出了Naps A,但其中的Npsin A完全阴性。 )的9种原发性透明细胞肾细胞癌。所有肾上皮肿瘤均为TTF-1阴性。这些发现表明,双napps A和TTF-1阳性免疫染色对肺原发性腺癌具有高度特异性,这两种生物标记物的结合可确保将原发性肺腺癌与肺转移癌区分开。

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