首页> 外文期刊>Oncogene >REPS2|[sol]|POB1 is downregulated during human prostate cancer progression and inhibits growth factor signalling in prostate cancer cells
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REPS2|[sol]|POB1 is downregulated during human prostate cancer progression and inhibits growth factor signalling in prostate cancer cells

机译:REPS2 | [sol] | POB1在人类前列腺癌进展过程中被下调,并抑制前列腺癌细胞中的生长因子信号传导

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During progression of prostate cancer, cellular changes occur, leading to a transition from androgen-dependent to androgen-independent growth. One aspect of this transition is a switch from androgens to growth factors, like epidermal growth factor (EGF), as primary regulators of proliferation. We examined the involvement of REPS2/POB1 in this process. REPS2/POB1 is an EH domain-containing protein, reported to be involved in signalling via RalBP1 and to play a role in endocytosis of EGF receptors. Furthermore, the protein is relatively highly expressed in androgen-dependent as compared to androgen-independent human prostate cancer cell lines and xenografts. Next to the known REPS2/POB1 protein, an open reading frame encoding REPS2/POB1, with 139 additional amino-acid residues at the NH2-terminus, was cloned and found to be expressed in prostate cancer cells. Overexpression, by transient transfection, of both forms of REPS2/POB1 in prostate cancer cell lines, induced apoptosis within 48h. At shorter time intervals after transfection, signalling towards a TPA response element luciferase reporter was found to be inhibited. From these experiments, it is concluded that REPS2/POB1, through its influence on the Ral signalling pathway, is involved in growth factor signalling. Decreased expression of REPS2/POB1 during progression of prostate cancer may therefore result in loss of control of growth factor signalling and consequently in loss of control of cell proliferation.
机译:在前列腺癌的进展过程中,发生细胞变化,导致从雄激素依赖性生长转变为非雄激素依赖性生长。这种转变的一方面是从雄激素向生长因子(如表皮生长因子(EGF))的转变,这是增殖的主要调节剂。我们检查了REPS2 / POB1在此过程中的参与。 REPS2 / POB1是一种含EH结构域的蛋白质,据报道参与RalBP1的信号传导,并在EGF受体的内吞作用中发挥作用。此外,与非雄激素依赖性人前列腺癌细胞系和异种移植物相比,该蛋白质在雄激素依赖性中相对较高地表达。在已知的REPS2 / POB1蛋白旁边,克隆了一个编码REPS2 / POB1的开放阅读框,在NH2末端带有139个其他氨基酸残基,并在前列腺癌细胞中表达。通过瞬时转染两种形式的REPS2 / POB1在前列腺癌细胞系中的过表达,在48小时内诱导了细胞凋亡。转染后的较短时间间隔内,发现向TPA反应元件荧光素酶报告基因的信号被抑制。从这些实验可以得出结论,REPS2 / POB1通过其对Ral信号通路的影响而参与了生长因子信号通路。因此,REPS2 / POB1在前列腺癌进展过程中的表达降低可能导致生长因子信号传导的控制丧失,并因此导致细胞增殖的控制丧失。

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