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Epithelial-to-mesenchymal transition: immunohistochemical investigation of related molecules in canine cutaneous epithelial tumours

机译:上皮 - 间充质转换:犬皮肤上皮肿瘤中相关分子的免疫组化研究

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Background - Epithelial-to-mesenchymal transition (EMT) is a multistep process, important in tumour invasion and metastasis, characterized by loss of epithelial markers, redistribution of p-catenin and gain of mesenchymal markers.Hyposthesis/Objectives - Our aim was to investigate the immunohistochemical aberrant expression of cytoker-atin, vimentin, survivin and heat shock protein 72 (Hsp72) in canine cutaneous epithelial tumours, to understand the association of expression of these molecules with features of malignancy and their role in the EMT phenotype.Methods - Ten canine squamous cell carcinomas (SCCs; one with lymph node metastasis), 30 canine hair follicle tumours (six pilomatricomas, eight infundibular keratinizing acanthomas, six trichoepitheliomas and 10 trichoblastomas) and five normal skin samples were investigated by immunohistochemistry using specific anti-vimentin, -cytokeratin, -survivin and -Hsp72 antibodies. A semi-quantitative method was used to analyse the results, as follows: 0 to <5%; >5 to <10%; >10 to <25%; and >25% of positive cells. Immunofluorescence was performed to investigate survivin-vimentin and survivin-Hsp72 colocalization in selected SCCs.Results - In malignant hair follicle tumours and SCCs, a reduced intensity of cytokeratin and increased survivin and Hsp72 expression were observed. In SCCs, loss of cytokeratin expression and vimentin immunolabelling, suggestive of the EMT phenotype, were evident in <5% of neoplastic cells in the front of tumour invasion. In the same areas, strong nuclear survivin and cytoplasmic Hsp72 staining was evident, often colocalizing. Only a few neoplastic cells in the front of tumour invasion showed vimentin-survivin colocalization.Conclusions and clinical importance - A possible simultaneous involvement of survivin and Hsp72 in tumour invasion and the multistep process of EMT of cutaneous epithelial tumours of dogs is suggested.
机译:背景 - 上皮 - 间质转化(EMT)是一个多步骤的过程,在肿瘤侵袭和转移,其特征在于上皮标记,β-连环蛋白和间充质markers.Hyposthesis /目标的增益的再分配的损失重要 - 我们的目的是调查十 - cytoker-ATIN,波形蛋白,存活蛋白和热休克蛋白72(Hsp72的)在犬皮肤上皮肿瘤,了解这些分子与恶性肿瘤的特征和它们在EMT phenotype.Methods作用的表达关联的免疫组化表达异常犬鳞状细胞癌(SCC的;一个与淋巴结转移),30个犬毛囊肿瘤(6个pilomatricomas,八个漏斗部角化acanthomas,六个trichoepitheliomas和10个trichoblastomas)和五个正常皮肤样品通过免疫组织化学使用特异性抗波形蛋白,研究 - 细胞角蛋白,-survivin和-Hsp72抗体。用半定量方法来分析结果,如下所示:0至<5%; > 5至<10%; > 10至<25%;和>阳性细胞的25%。免疫荧光进行调查存活蛋白波形蛋白和存活蛋白的Hsp72共定位在选定SCCs.Results - 在恶性毛囊肿瘤和SCC的,细胞角蛋白的减少的强度和增加的存活和Hsp72的表达中观察到。在SCC中,细胞角蛋白的表达和波形蛋白免疫标记,该EMT表型暗示,损失均在肿瘤侵袭的前肿瘤细胞的<5%明显。在同一地区,强大的核生存和胞质Hsp72的染色明显,往往colocalizing。只有在肿瘤侵犯的前几个肿瘤细胞呈波形蛋白生存colocalization.Conclusions及临床意义 - 肿瘤的侵袭和生存的Hsp72的可能同时参与和狗的皮肤上皮性肿瘤的EMT的多步骤的过程提出了建议。

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