首页> 外文期刊>Brazilian Journal of Medical and Biological Research >Expression of E-cadherin, Snail and Hakai in epithelial cells isolated from the primary tumor and from peritumoral tissue of invasive ductal breast carcinomas
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Expression of E-cadherin, Snail and Hakai in epithelial cells isolated from the primary tumor and from peritumoral tissue of invasive ductal breast carcinomas

机译:E-cadherin,Snail和Hakai在浸润性导管癌原发肿瘤和癌旁组织分离的上皮细胞中的表达

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Epithelial intercellular cohesion, mainly mediated by E-cadherin (CDH1) expression and function, may be deregulated during cancer cell invasion of adjacent tissues and lymphatic and vascular channels. CDH1 expression is down-modulated in invasive lobular breast carcinomas but its regulation in invasive ductal carcinomas (IDC) is less clear. CDH1 expression is repressed by transcription factors such as Snail (SNAI1) and its product is degraded after Hakai ubiquitination. We compared CDH1, SNAI1 and HAKAI mRNA expression in IDC and paired adjacent normal breast tissue and evaluated its relation with node metastasis and circulating tumor cells. Matched tumor/peritumoral and blood samples were collected from 30 patients with early IDC. Epithelial cells from each compartment (tumor/peritumoral) were recovered by an immunomagnetic method and gene expression was determined by real time RT-PCR. There were no differences in CDH1, SNAI1 and HAKAI mRNA expression between tumor and corresponding peritumoral samples and no differential tumoral gene expression according to nodal involvement. Another 30 patients with a long-term follow-up (at least 5 years) and a differential prognosis (good or poor, as defined by breast cancer death) had E-cadherin and Snail protein detected by immunohistochemistry in tumor samples. In this group, E-cadherin-positive expression, but not Snail, may be associated with a better prognosis. This is the first report simultaneously analyzing CDH1, SNAI1 and HAKAI mRNA expression in matched tumor and peritumoral samples from patients with IDC. However, no clear pattern of their expression could distinguish the invasive tumor compartment from its adjacent normal tissue.
机译:上皮细胞间凝聚力主要由E-钙黏着蛋白(CDH1)的表达和功能介导,在癌细胞侵袭邻近组织以及淋巴和血管通道时可能会受到调节。 CDH1表达在浸润性小叶型乳腺癌中被下调,但其在浸润性导管癌(IDC)中的调控尚不清楚。 Hakai泛素化后,转录因子如Snail(SNAI1)抑制CDH1表达,其产物被降解。我们比较了IDC和配对的正常乳腺组织中CDH1,SNAI1和HAKAI mRNA的表达,并评估了其与淋巴结转移和循环肿瘤细胞的关系。从30例早期IDC患者中收集匹配的肿瘤/腹膜和血液样本。通过免疫磁性方法从每个区室(肿瘤/周膜)中回收上皮细胞,并通过实时RT-PCR确定基因表达。肿瘤和相应的肿瘤周围样品之间的CDH1,SNAI1和HAKAI mRNA表达没有差异,并且根据淋巴结受累情况也没有差异的肿瘤基因表达。另有30名经过长期随访(至少5年)且预后不同(根据乳腺癌死亡定义为好或差)的患者,通过免疫组织化学方法在肿瘤样本中检测到E-钙黏着蛋白和Snail蛋白。在这一组中,E-cadherin阳性表达而非Snail可能与更好的预后相关。这是第一份同时分析来自IDC患者的匹配肿瘤和肿瘤周围样品中CDH1,SNAI1和HAKAI mRNA表达的报告。但是,没有明确的表达方式可以将浸润性肿瘤区隔与其相邻的正常组织区分开。

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