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黑色素瘤细胞的膜γ-谷氨酰转肽酶活性:对细胞过氧化氢生成、细胞表面蛋白巯基氧化及核因子κB激活状态的影响

Membrane gamma-glutamyl transpeptidase activity of melanoma cells: effects on cellular H(2)O(2) production, cell surface protein thiol oxidation and NF-kappa B activation status.

作者信息

Maellaro E, Dominici S, Del Bello B, Valentini M A, Pieri L, Perego P, Supino R, Zunino F, Lorenzini E, Paolicchi A, Comporti M, Pompella A

机构信息

Department of Pathophysiology & Experimental Medicine, University of Siena, Italy.

出版信息

J Cell Sci. 2000 Aug;113 ( Pt 15):2671-8. doi: 10.1242/jcs.113.15.2671.

Abstract

The metabolism of glutathione by membrane-bound &ggr;-glutamyl transpeptidase (GGT) has been recently recognized as a basal source of hydrogen peroxide in the extracellular space. Significant levels of GGT activity are expressed by malignant tumours, and in melanoma cell lines they were found to correlate with the malignant behaviour. As hydrogen peroxide and other oxidants can affect signal transduction pathways at several levels, the present study was aimed to verify: (i) the occurrence of GGT-dependent production of hydrogen peroxide in melanoma cells; (ii) the effects of GGT-dependent prooxidant reactions on known redox-sensitive cellular targets, i.e. protein thiols, the nuclear transcription factor NF-kappa B and p53. Two melanoma Me665/2 cell clones, exhibiting traces of (clone 2/21) or high (clone 2/60) GGT activity, were studied. The occurrence of GGT-dependent production of hydrogen peroxide was apparent in 2/60 cells, in which it was accompanied by lower levels of cell surface protein thiols. In 2/60 cells, GGT expression was also associated with higher levels of NF-kappa B activation, as compared to GGT-poor 2/21 cell clone. Indeed, stimulation or inhibition of GGT activity in 2/60 cells resulted in progressive activation or inactivation of NF-kappa B, respectively. An analysis of the p53 gene product indicated lack of protein expression in 2/60 cells, whereas a mutant protein was highly expressed in 2/21 cells. Taken together, these results indicate that the expression of GGT activity can provide melanoma cells with an additional source of hydrogen peroxide, and that such prooxidant reactions are capable to modify protein thiols at the cell surface level. In addition, GGT expression results in an up-regulation of the transcription factor NF-kappa B, which could explain the higher metastatic behaviour reported for GGT-rich melanoma cells as compared to their GGT-poor counterparts.

摘要

膜结合γ-谷氨酰转肽酶(GGT)介导的谷胱甘肽代谢最近被认为是细胞外空间中过氧化氢的一个基础来源。恶性肿瘤会表达显著水平的GGT活性,并且在黑色素瘤细胞系中,人们发现其与恶性行为相关。由于过氧化氢和其他氧化剂可在多个水平影响信号转导通路,本研究旨在验证:(i)黑色素瘤细胞中是否存在GGT依赖性的过氧化氢生成;(ii)GGT依赖性的促氧化反应对已知的氧化还原敏感细胞靶点的影响,即蛋白质硫醇、核转录因子NF-κB和p53。研究了两个黑色素瘤Me665/2细胞克隆,其中一个(克隆2/21)GGT活性极低,另一个(克隆2/60)GGT活性高。在2/60细胞中明显存在GGT依赖性的过氧化氢生成,同时其细胞表面蛋白质硫醇水平较低。与GGT含量低的2/21细胞克隆相比,在2/60细胞中,GGT表达还与更高水平的NF-κB激活相关。实际上,对2/60细胞中GGT活性的刺激或抑制分别导致NF-κB的逐渐激活或失活。对p53基因产物的分析表明,2/60细胞中缺乏蛋白质表达,而突变蛋白在2/21细胞中高表达。综上所述,这些结果表明,GGT活性的表达可为黑色素瘤细胞提供额外的过氧化氢来源,并且这种促氧化反应能够在细胞表面水平修饰蛋白质硫醇。此外,GGT表达导致转录因子NF-κB上调,这可以解释与GGT含量低的黑色素瘤细胞相比,GGT含量高的黑色素瘤细胞具有更高转移行为的原因。

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