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首页> 外文期刊>International Journal of Clinical and Experimental Pathology >β-catenin expression in benign and malignant pleural disorders
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β-catenin expression in benign and malignant pleural disorders

机译:β-catenin在良,恶性胸膜疾病中的表达

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摘要

Benign and malignant pleural processes display a large and overlapping spectrum of morphological appearances, and can be difficult to distinguish, histologically, from each other. β-catenin, a participant in the wingless-type (Wnt) transduction pathway, is involved in the pathogenesis of malignant mesothelioma and has received limited evaluation for its ability to serve as a diagnostic aid for distinguishing between individual pleural disorders. We performed immunohistochemistry for β-catenin on 10 pleural malignant mesotheliomas, 10 examples of mesothelial hyperplasia and 18 cases of organizing pleuritis. Although differences were noted in staining intensity between the mesothelioma and mesothelial hyperplasia groups, extensiveness and cellular location were similar. Staining intensity (mean +/− s.d.) in mesotheliomas (2.00 +/− 0.67) was significantly less intense than in mesothelial hyperplasia cases (3.00 +/− 0.00) (p=0.0005). Stromal cell staining was cytoplasmic in all cases, and endothelial cell staining was membranous, submembranous and cytoplasmic. Nuclear expression of β-catenin was not observed in any of the cases studied. This lack of nuclear staining in the stromal cells of organizing pleuritis differs markedly from the previously reported high frequencies of nuclear β-catenin expression in other pleural spindle cell proliferations (desmoid tumors and solitary fibrous tumors). In summary, the current study adds to previous work indicating a role for β-catenin in the genesis of pleural conditions including organizing pleuritis, mesothelial hyperplasia and malignant mesothelioma. Although IHC for β-catenin does not appear to be conclusive for separating benign from malignant mesothelial proliferations, it may be valuable for assisting in the differential diagnosis of mesothelial and spindle cell proliferations in the pleura.
机译:良性和恶性胸膜过程显示出较大且重叠的形态学外观谱,并且可能难以在组织学上彼此区分。 &#x003b2-catenin是无翼型(Wnt)转导途径的参与者,参与了恶性间皮瘤的发病机理,并且由于其作为区分各种胸膜疾病的诊断手段的能力而受到了有限的评价。我们对10例胸膜恶性间皮瘤,10例间皮增生和18例组织性胸膜炎进行了β -catenin的免疫组化分析。尽管注意到间皮瘤组和间皮增生组之间的染色强度存在差异,但广泛性和细胞位置相似。中皮瘤(2.00 + /#02222; 0.67)中的染色强度(平均值)比间皮增生病例(3.00 + /#02212; 0.00)的强度显着降低(p = 0.0005)。在所有情况下,基质细胞染色均为细胞质,内皮细胞染色为膜,亚膜和细胞质。在所研究的任何案例中均未观察到β -catenin的核表达。组织性胸膜炎的基质细胞中这种核染色的缺乏与先前报道的其他胸膜梭形细胞增殖(类胶质瘤和孤立性纤维性肿瘤)中核-catenin表达的高频率明显不同。总而言之,当前的研究增加了以前的工作,表明β-连环蛋白在包括组织性胸膜炎,间皮增生和恶性间皮瘤在内的胸膜疾病发生中的作用。尽管IHC对于-catenin的分离对于良性和恶性间皮增生似乎不是结论性的,但可能有助于鉴别胸膜间皮和梭形细胞增生。

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