首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >The iron-regulated metastasis suppressor, Ndrg-1: identification of novel molecular targets.
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The iron-regulated metastasis suppressor, Ndrg-1: identification of novel molecular targets.

机译:铁调节的转移抑制剂Ndrg-1:新分子靶标的鉴定。

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摘要

A recently identified metastasis suppressor, N-myc downstream regulated gene-1 (Ndrg-1), has been shown to reduce the invasion and metastasis of breast, colon, prostate and pancreatic cancer. Among its many functions, Ndrg-1 is involved in modulating differentiation, proliferation and angiogenesis. However, knowledge of the molecular targets of Ndrg-1 is limited. The current study has focused on examining the functions of Ndrg-1 in a number of different cancer cell models including prostate, colon, lung and pancreatic cancer to elucidate the known pleiotropic nature of this protein. Furthermore, the potential gene targets of Ndrg-1 were analyzed using whole genome gene array revealing a substantial number of genes whose expression was affected by this metastasis suppressor. Significantly, Ndrg-1 up-regulated thiamine triphosphatase (Thtpa) expression in three of the four cell models. Thtpa is known to decrease the levels of the energy currency molecule, thiamine triphosphate, suggesting a potential pathway for the anti-proliferative effects of Ndrg-1. Furthermore, Ndrg-1 reduced the protein levels of cathepsin C which plays a role in invasion, indicating a potential mechanism of its anti-metastatic role in pancreatic cancer cells. These findings provide a potential link between the observed functions of Ndrg-1 and its molecular targets, further demonstrating its anti-metastatic effect.
机译:最近发现的一种转移抑制因子,N-myc下游调节基因1(Ndrg-1),可以减少乳腺癌,结肠癌,前列腺癌和胰腺癌的侵袭和转移。在其许多功能中,Ndrg-1参与调节分化,增殖和血管生成。但是,有关Ndrg-1分子靶标的知识是有限的。当前的研究集中在检查Ndrg-1在许多不同的癌细胞模型中的功能,包括前列腺癌,结肠癌,肺癌和胰腺癌,以阐明该蛋白的已知多效性。此外,使用全基因组基因阵列分析了Ndrg-1的潜在基因靶标,揭示了其表达受此转移抑制因子影响的大量基因。重要的是,在四个细胞模型中的三个中,Ndrg-1上调了硫胺素三磷酸酶(Thtpa)的表达。已知Thtpa会降低能量货币分子硫胺素三磷酸的水平,这暗示了Ndrg-1的抗增殖作用的潜在途径。此外,Ndrg-1降低了组织蛋白酶C的蛋白水平,该蛋白在侵袭中起作用,表明其在胰腺癌细胞中具有抗转移作用的潜在机制。这些发现为观察到的Ndrg-1的功能与其分子靶标之间提供了潜在的联系,进一步证明了其抗转移作用。

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