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首页> 外文期刊>Applied immunohistochemistry and molecular morphology: AIMM >Novel markers of pancreatic adenocarcinoma in fine-needle aspiration: mesothelin and prostate stem cell antigen labeling increases accuracy in cytologically borderline cases.
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Novel markers of pancreatic adenocarcinoma in fine-needle aspiration: mesothelin and prostate stem cell antigen labeling increases accuracy in cytologically borderline cases.

机译:细针穿刺术中胰腺腺癌的新标志物:间皮素和前列腺干细胞抗原标记可提高细胞学临界病例的准确性。

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摘要

The interpretation of pancreas fine-needle aspiration (FNA) is extremely difficult given the cytologic overlap of neoplastic and reactive processes. Using serial analysis of gene expression, we have discovered 2 new markers of pancreatic adenocarcinoma, mesothelin and prostate stem cell antigen (PSCA), and confirmed their specificity by immunohistochemical labeling. Here we evaluate the potential contribution of immunohistochemical labeling of mesothelin and PSCA to the interpretation of pancreas FNAs. Thirty pancreas FNAs with follow-up data were reviewed. Unstained cell block sections from these aspirates labeled for mesothelin and PSCA using immunohistochemistry were compared with initial cytologic diagnoses and with follow-up diagnoses. On follow-up, 19 patients proved to have cancer, and 11 did not. Initial cytologic diagnosis of malignancy correlated with carcinoma on follow-up in 12 of 12 cases, and initial benign cytologic diagnosis correlated with benign follow-up in 8 of 9 cases (sensitivity,92%; specificity, 100%). Six of the 9 patients with suspicious cytology were found to have a carcinoma on follow-up. PSCA labeling was present in 16 of the 19 patients who ultimately were proven to have carcinoma; PSCA labeling was absent in 10 of the 11 lesions proven to be benign (sensitivity, 84%; specificity, 91%). Mesothelin labeling was present in 13 of the 19 patients who ultimately were proven to have carcinoma; mesothelin labeling was absent in 10 of the 11 lesions proven to be benign (sensitivity, 68%; specificity, 91%). Five of the 6 cytologically suspicious cases with malignant follow-up labeled for either PSCA or mesothelin (83%), and 2 of the 6 cases labeled for both markers. None of the 3 suspicious cases with benign follow-up labeled for either PSCA or mesothelin. Increasingly, molecular techniques are identifying potential cancer markers that may have diagnostic utility. In this study, immunohistochemical labeling for 2 of these markers, PSCA and mesothelin, appears highly specific for pancreatic adenocarcinoma in FNA specimens and useful in categorizing cytologically suspicious lesions.
机译:鉴于肿瘤性和反应性过程的细胞学重叠,对胰腺细针抽吸术(FNA)的解释极为困难。使用基因表达的系列分析,我们发现了2种胰腺腺癌,间皮素和前列腺干细胞抗原(PSCA)的新标记,并通过免疫组织化学标记证实了它们的特异性。在这里,我们评估间皮素和PSCA的免疫组织化学标记对胰腺FNAs解释的潜在贡献。回顾了三十例胰腺FNA,并进行了随访。将使用免疫组织化学标记了间皮素和PSCA的这些抽吸物中未染色的细胞块与初始细胞学诊断和后续诊断进行了比较。在随访中,有19名患者被证明患有癌症,而11名没有。最初的细胞学诊断为恶性肿瘤与癌症相关的随访12例中有12例,并且最初的良性细胞学诊断与良性肿瘤相关的9例中的8例(敏感性,92%;特异性,100%)。在9例可疑细胞学患者中,有6例在随访中发现癌症。 19名最终被证实患有癌症的患者中有16名存在PSCA标记。经证实是良性的11个病变中有10个没有PSCA标记(敏感性为84%;特异性为91%)。在19例最终被证实患有癌症的患者中,有13例存在间皮素标记。经证实是良性的11个病变中有10个没有间皮素标记(敏感性为68%;特异性为91%)。在6例细胞学可疑病例中,有5例被标记为PSCA或间皮素的恶性随访中有5例(占83%),在6例同时标记有两种标记物的病例中有2例。 3例可疑病例均未标明PSCA或间皮素。分子技术越来越多地识别出可能具有诊断用途的潜在癌症标志物。在这项研究中,其中两种标记物PSCA和间皮素的免疫组化标记似乎对FNA标本中的胰腺腺癌具有高度特异性,可用于对细胞学可疑病变进行分类。

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