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Histological types and significance of bronchial epithelial dysplasia

机译:支气管上皮异常增生的组织学类型及其意义

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Pulmonary epithelium is known to undergo a preneoplastic process prior to the development of lung carcinoma. Squamous dysplasia and atypical adenomatous hyperplasia have been identified and classified as preinvasive lesions of squamous cell carcinoma and peripheral pulmonary adenocarcinoma, respectively. However, these commonly recognized preinvasive lesions do not completely explain the development of all histological types of lung carcinoma. By examining 114 resection lung specimens, we concluded that there are four histological patterns of bronchial epithelial dysplasia based on morphological features (basal cell dysplasia, columnar cell dysplasia, bronchial epithelial dysplasia with transitional differentiation, and squamous dysplasia). The histological patterns were further characterized by immunohistochemistry. Basal cell dysplasia was focally positive for cytokeratin (CK) 17 and 10/13; columnar cell dysplasia was generally positive for CK7, 8, and 18; bronchial epithelial dysplasia with transitional differentiation had a heterogeneous immunoprofile, while squamous dysplasia was positive for CK10/13 and focally positive for CK17. Various degrees of abnormal expression of p53 and Ki-67 were found in the different types of bronchial epithelial dysplasia. The cases were divided into three groups based on degree and extent of bronchial epithelial dysplasia. By Crosstabs McNemar test, the Mann–Whitney U-test (for two independent groups), the Kruskal–Wallis one-way nonparametric ANOVA (for >2 independent groups) and Spearman correlation analysis, the degree and extent of bronchial epithelial dysplasia was shown to be positively correlated with the incidence of bronchogenic carcinoma and multifocal primary lung carcinoma (P<0.05). These findings indicated the following: (1) bronchial epithelium can develop various patterns of dysplasia with abnormal/ambiguous cell differentiation and abnormal expressions of p53 and Ki-67. Thus, these bronchial epithelial dysplastic lesions may represent a preneoplastic process. (2) The degree of bronchial epithelial dysplasia may significantly predispose individuals to bronchogenic carcinoma and multifocal primary lung carcinoma.
机译:已知肺上皮在肺癌发生之前会经历肿瘤前过程。鳞状上皮不典型增生和非典型腺瘤样增生已被确定为鳞状细胞癌和周围性肺腺癌的浸润前病变。但是,这些公认的浸润前病变不能完全解释所有组织学类型肺癌的发展。通过检查114例切除的肺标本,我们得出结论,根据形态学特征,支气管上皮发育异常有四种组织学模式(基底细胞发育异常,柱状细胞发育异常,伴有过渡分化的支气管上皮发育异常和鳞状增生)。通过免疫组织化学进一步表征组织学模式。基底细胞发育异常的细胞角蛋白(CK)17和10/13呈局灶性阳性; CK7、8和18的柱状细胞发育异常通常为阳性;具有过渡分化的支气管上皮异型增生具有异质性免疫特征,而鳞状异型增生对CK10 / 13呈阳性,而对CK17呈局灶性阳性。在不同类型的支气管上皮发育异常中发现了不同程度的p53和Ki-67异常表达。根据支气管上皮发育不良的程度和程度将病例分为三组。通过Crosstabs McNemar检验,Mann-Whitney U检验(用于两个独立组),Kruskal-Wallis单向非参数方差分析(用于两个以上独立组)和Spearman相关分析,显示了支气管上皮异型增生的程度和程度与支气管癌和多灶性原发性肺癌的发生率呈正相关(P <0.05)。这些发现表明以下几点:(1)支气管上皮细胞可发展为各种异常增生,具有异常/模糊的细胞分化以及p53和Ki-67的异常表达。因此,这些支气管上皮异常增生性病变可能代表了一个肿瘤前过程。 (2)支气管上皮异常增生的程度可能使个体更易患支气管癌和多灶性原发性肺癌。

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