首页> 外文期刊>Pigment cell & melanoma research >NDRG2 gene expression in B16F10 melanoma cells restrains melanogenesis via inhibition of Mitf expression
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NDRG2 gene expression in B16F10 melanoma cells restrains melanogenesis via inhibition of Mitf expression

机译:B16F10黑色素瘤细胞中NDRG2基因表达通过抑制Mitf表达来抑制黑色素生成

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摘要

NDRG2 (N-myc downstream-regulated gene 2) is a candidate tumor suppressor implicated in control of glioblastoma proliferation and dendritic cell differentiation. The microphthalmia-associated transcription factor (Mitf) plays a crucial role in the melanocyte lineage and in melanoma by controlling survival, differentiation, cell cycle entry and exit, and melanoma metastasis. Identifying upstream regulators of Mitf expression, therefore, remains a key issue. In this study, we aimed to assess whether the candidate tumor suppressor NDRG2 can modulate Mitf expression. Here, we show that NDRG2 acts to prevent cAMP and β-catenin-mediated activation of the Mitf promoter, thereby blocking melanogenesis via the downstream Mitf target genes Tyrosinase, Tyrp1 and Dct. The data suggest that NDRG2 impairs melanogenesis by interfering with both the TCF/β-catenin and cAMP/CREB pathways that are known to stimulate Mitf expression in melanocytes and have major implications for the role of NDRG2 in pigmentation and melanoma progression. Taken together, the results not only identify NDRG2 as a novel regulator of pigmentation, but also potentially a key factor in regulating melanoma progression via Mitf.
机译:NDRG2(N-myc下游调控基因2)是一种候选肿瘤抑制因子,可能与胶质母细胞瘤的增殖和树突状细胞的分化有关。小眼症相关转录因子(Mitf)通过控制存活,分化,细胞周期进入和退出以及黑素瘤转移,在黑素细胞谱系和黑素瘤中起关键作用。因此,确定Mitf表达的上游调节子仍然是关键问题。在这项研究中,我们旨在评估候选肿瘤抑制物NDRG2是否可以调节Mitf表达。在这里,我们表明NDRG2可以阻止cAMP和β-catenin介导的Mitf启动子的激活,从而通过下游Mitf目标基因酪氨酸酶,酪氨酸酶和Dct阻止黑色素生成。数据表明,NDRG2通过干扰TCF /β-catenin和cAMP / CREB途径而损害黑素生成,已知这两种途径可刺激黑素细胞中Mitf的表达,并对NDRG2在色素沉着和黑素瘤进展中的作用具有重要意义。两者合计,结果不仅将NDRG2鉴定为色素沉着的新型调节剂,而且还可能是通过Mitf调节黑色素瘤进展的关键因素。

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