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首页> 外文期刊>Oncogene >Downregulation of CCN3 expression as a potential mechanism for melanoma progression
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Downregulation of CCN3 expression as a potential mechanism for melanoma progression

机译:CCN3表达下调是黑色素瘤进展的潜在机制

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Coculture of human melanocytes with keratinocytes upregulates CCN3, a matricellular protein critical to maintenance of normal homeostasis of melanocytes in the skin. CCN3 affects two fundamental features of melanocyte physiology: it inhibits melanocyte proliferation and stimulates their adhesion to the basement membrane. Here we report that expression of CCN3 is downregulated in advanced melanomas. Aggressive melanoma cell lines did not respond to treatment with CCN3 inducers, such as interleukin-1β (IL-1β), while less aggressive melanoma cell lines responded similarly to melanocytes. Immunostaining analyses revealed that CCN3 was present in melanoma cells close to the epidermal–dermal interface, but not in melanoma cells that had invaded deep into the dermis or had metastasized to lymph nodes. Contrary to our expectations, overexpression of CCN3 in 1205Lu metastatic melanoma cells did not affect their adhesion to collagen IV. However, CCN3 decreased the transcription and activation of matrix metalloproteinases and suppressed the invasion of 1205Lu melanoma cells. These results suggest that the lack of CCN3 in advanced melanoma cells contributes to their invasive phenotype. Whereas major matricellular proteins, such as osteopontin, tenascin or secreted protein acidic and rich in cysteine (SPARC), are strongly upregulated in melanoma cells; CCN3 is the first member of this family that is downregulated.
机译:人黑素细胞与角质形成细胞的共培养可上调CCN3,这是一种母体细胞蛋白,对于维持皮肤中黑素细胞的正常稳态至关重要。 CCN3影响黑素细胞生理学的两个基本特征:它抑制黑素细胞增殖并刺激其与基底膜的粘附。在这里我们报告在晚期黑素瘤中CCN3的表达下调。侵袭性黑色素瘤细胞系对CCN3诱导剂(如白介素-1β(IL-1β))的治疗无反应,而侵略性黑色素瘤细胞系对黑素细胞的反应相似。免疫染色分析表明,CCN3存在于靠近表皮-真皮界面的黑色素瘤细胞中,但不存在于侵入真皮深层或转移至淋巴结的黑色素瘤细胞中。与我们的预期相反,CCN3在1205Lu转移性黑色素瘤细胞中的过表达并不影响其与胶原IV的粘附。然而,CCN3减少了基质金属蛋白酶的转录和激活,并抑制了1205Lu黑色素瘤细胞的侵袭。这些结果表明,晚期黑素瘤细胞中缺乏CCN3有助于其侵袭性表型。黑色素瘤细胞中主要的基质细胞蛋白,例如骨桥蛋白,腱糖蛋白或酸性且富含半胱氨酸的分泌蛋白(SPARC)强烈上调; CCN3是该家族中第一个被下调的成员。

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