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首页> 外文期刊>Histochemistry and Cell Biology >Melanoma progression exhibits a significant impact on connexin expression patterns in the epidermal tumor microenvironment
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Melanoma progression exhibits a significant impact on connexin expression patterns in the epidermal tumor microenvironment

机译:黑色素瘤的进展对表皮肿瘤微环境中的连接蛋白表达模式有重要影响

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Melanoma depends on, interacts with and reacts to the stroma in which it is embedded, including fibroblasts, extracellular matrix, endothelial cells and immune cells. However, the impact of melanoma on the epidermal tumor microenvironment—the multilayered epithelium of the skin—is poorly understood. Gap junctions are essential for intercellular communication and involved in proliferation, differentiation and homeostasis of keratinocytes. We have shown previously that the gap junction proteins connexin 26 and 30 (Cx26 and Cx30) are induced in the epidermal tumor microenvironment of skin cancers including melanoma. This study compares the extent of Cx26, Cx30 and Cx43 expression in the epidermal microenvironment of melanocytic nevi and melanomas and its association with melanoma thickness, proliferative index of the tumor and its microenvironment, and with 5-year metastasis and survival. We found that induction of Cx26 and Cx30 cell–cell border expression in the epidermal tumor microenvironment correlates to malignancy. Importantly, there was a significant correlation of tumor thickness with the vertical epidermal Cx26 and Cx30 expression pattern and the horizontal Cx26 dissemination. Furthermore, horizontal Cx26 expression correlated with metastasis. Vertical epidermal expression patterns of Cx26 and Cx30 significantly correlated with the proliferative index in the epidermal tumor microenvironment but not with the proliferative index in the tumor. In contrast, Cx43 did not correlate with malignancy, thickness or proliferative index. In summary, here we show for the first time a significant association between the progression of melanoma and alterations in its epithelial tumor microenvironment. Keywords Cell–cell communication - Gap junctions - Cx26 - Cx30 - Skin cancer - Carcinogenesis N. K. Haass and D. Ripperger contributed equally to this paper.
机译:黑色素瘤取决于包埋在其中的基质,包括成纤维细胞,细胞外基质,内皮细胞和免疫细胞,并与之相互作用。然而,关于黑色素瘤对表皮肿瘤微环境(皮肤的多层上皮)的影响知之甚少。间隙连接对于细胞间的通讯是必不可少的,并且参与角质形成细胞的增殖,分化和稳态。以前我们已经表明,间隙连接蛋白连接蛋白26和30(Cx26和Cx30)在包括黑素瘤在内的皮肤癌的表皮肿瘤微环境中被诱导。这项研究比较了Cx26,Cx30和Cx43在黑素细胞痣和黑色素瘤的表皮微环境中的表达程度及其与黑色素瘤厚度,肿瘤及其微环境的增殖指数以及5年转移和生存的关系。我们发现表皮肿瘤微环境中Cx26和Cx30细胞间边界表达的诱导与恶性肿瘤相关。重要的是,肿瘤厚度与垂直表皮Cx26和Cx30表达模式以及水平Cx26分布之间存在显着相关性。此外,水平Cx26表达与转移相关。 Cx26和Cx30的垂直表皮表达模式与表皮肿瘤微环境中的增殖指数显着相关,但与肿瘤中的增殖指数无关。相反,Cx43与恶性,厚度或增殖指数无关。总之,这里我们首次显示了黑色素瘤的进展与其上皮肿瘤微环境改变之间的显着关联。关键词细胞间通讯-间隙连接-Cx26-Cx30-皮肤癌-致癌作用N. K. Haass和D. Ripperger同样为本文做出了贡献。

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