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首页> 外文期刊>Romanian Journal of Morphology and Embryology >Hyperplastic polyps and serrated adenomas: precancerous lesions with mixed immunophenotype
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Hyperplastic polyps and serrated adenomas: precancerous lesions with mixed immunophenotype

机译:增生性息肉和锯齿状腺瘤:混合免疫表型的癌前病变

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Our immunohistochemical study wants to be a contribution to clarifying the adenoma-carcinoma sequence and serrated pathway of colorectal carcinogenesis. Thus, we performed immunohistochemical analysis of hyperplastic polyps (HP), serrated adenomas (SA), and classical adenomas (tubular adenomas - TA and tubulovillous adenomas - TVA) and carcinomas developed from adenomas (CA) using expression of p53, Ki-67, c-myc, APC, MSH2 and Ets-1 proteins. Because of correlation of the expression of these proteins, we propose several immunophenotypes, which show modifications along the known carcinogenetic mechanisms. Along the adenoma-carcinoma sequence we noted an increase in the expression of p53, Ki-67, c-myc and Ets-1, and a decrease in APC expression. The majority of TAs and TVAs are characterized by p53+/Ki-67+, p53+/c-myc+, p53+/APC+, and Ets-/p53+, Ets-/Ki-67+ immunophenotypes. The majority of HPs and SAs are Ets-/p53-, Ets-/Ki-67+, Ets-/c-myc+, APC+/MSH2-. In approximately 1/3 of the hyperplastic polyps and serrated adenomas, we noted that the decrease in expression of MSH2 is associated with an increase in the expression of p53, c-myc, Ki-67, and Ets-1. Thus, we can conclude that a group of hyperplastic polyps and serrated adenomas display similar immunohistochemical characteristics to tubular and tubulovillous adenomas, which delineates a group of precancerous lesions that can develop via mixed carcinogenic pathways.
机译:我们的免疫组化研究希望为阐明腺癌-癌序列和结直肠癌发生的锯齿状途径做出贡献。因此,我们使用了p53,Ki-67, c-myc,APC,MSH2和Ets-1蛋白。由于这些蛋白质表达的相关性,我们提出了几种免疫表型,它们沿已知的致癌机理显示出修饰。沿着腺瘤-癌序列,我们注意到p53,Ki-67,c-myc和Ets-1的表达增加,而APC的表达减少。大多数TA和TVA的特征是p53 + / Ki-67 +,p53 + / c-myc +,p53 + / APC +和Ets- / p53 +,Ets- / Ki-67 +免疫表型。大多数HP和SA是Ets- / p53-,Ets- / Ki-67 +,Ets- / c-myc +,APC + / MSH2-。在大约1/3的增生性息肉和锯齿状腺瘤中,我们注意到MSH2表达的降低与p53,c-myc,Ki-67和Ets-1的表达增加有关。因此,我们可以得出结论,一组增生性息肉和锯齿状腺瘤显示出与肾小管和微管腺瘤相似的免疫组织化学特征,这描绘了一组可以通过混合致癌途径发展的癌前病变。

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