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首页> 外文期刊>APMIS: Acta Pathologica, Microbiologica et Immunologica Scandinavica >Disturbed expression of E-cadherin, beta-catenin and tight junction proteins in colon carcinoma is unrelated to growth pattern and genetic polymorphisms.
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Disturbed expression of E-cadherin, beta-catenin and tight junction proteins in colon carcinoma is unrelated to growth pattern and genetic polymorphisms.

机译:E-钙粘蛋白,β-连环蛋白和紧密连接蛋白在结肠癌中的表达受干扰与生长模式和遗传多态性无关。

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Adhesion proteins are responsible for the structural integrity of epithelial tissue and in tumors this integrity is often lost, resulting in a disorganization of the tissue. In the present study the complexity of the invasive front of colon carcinomas was correlated with cell adhesion protein expression and with polymorphisms in their genes. A complexity index was constructed from 32 colon carcinomas using computer-assisted morphometry estimating fractal dimension and tumor cell clusters followed by tree analysis. Immunohistochemical staining of beta-catenin, E-cadherin, occludin and claudin 2 was used for assessment of protein expression. Genetic screening of tissue from the tumor invasion front with laser microdissection was performed using SSCP and DNA sequencing. Adhesion protein distribution was significantly disturbed in most carcinomas. A single mutation in the gene of beta-catenin was found but there was no correlation between protein expression and genetic polymorphism. Nor was there any correlation between the complexity of the invasive border and protein distribution or genetic alterations. The results indicate that the complexity of colon carcinoma invasion is not dependent on genetic derangements in the genes of adhesion proteins or the protein distribution. Rather, aberrations in the function of other proteins related to the adhesive proteins could be responsible.
机译:粘附蛋白负责上皮组织的结构完整性,在肿瘤中,这种完整性通常会丢失,从而导致组织混乱。在本研究中,结肠癌侵袭性前沿的复杂性与细胞粘附蛋白表达及其基因多态性相关。使用计算机辅助形态计量学估计分形维数和肿瘤细胞簇,然后通过树分析,从32个结肠癌构建复杂性指数。 β-catenin,E-cadherin,occludin和claudin 2的免疫组织化学染色用于评估蛋白表达。使用SSCP和DNA测序从肿瘤浸润前沿对组织进行遗传学筛选,并进行激光显微切割。在大多数癌症中,粘附蛋白的分布明显受到干扰。发现了β-catenin基因的单个突变,但蛋白表达与遗传多态性之间没有相关性。侵入性边界的复杂性与蛋白质分布或遗传改变之间也没有任何关联。结果表明,结肠癌侵袭的复杂性不依赖于粘附蛋白基因的遗传失序或蛋白分布。相反,与粘附蛋白有关的其他蛋白功能的异常可能是造成这种情况的原因。

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