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两种金(I)-N-杂环卡宾配合物对A2780人卵巢癌细胞的抗增殖作用:一项比较蛋白质组学研究

Antiproliferative effects of two gold(I)-N-heterocyclic carbene complexes in A2780 human ovarian cancer cells: a comparative proteomic study.

作者信息

Magherini Francesca, Fiaschi Tania, Valocchia Elisa, Becatti Matteo, Pratesi Alessandro, Marzo Tiziano, Massai Lara, Gabbiani Chiara, Landini Ida, Nobili Stefania, Mini Enrico, Messori Luigi, Modesti Alessandra, Gamberi Tania

机构信息

Department of Experimental and Clinical Biomedical Sciences "Mario Serio", University of Florence, Florence, Italy.

Department of Chemistry "Ugo Schiff", University of Florence, Florence, Italy.

出版信息

Oncotarget. 2018 Jun 15;9(46):28042-28068. doi: 10.18632/oncotarget.25556.

DOI:10.18632/oncotarget.25556
PMID:29963261
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6021324/
Abstract

Au(NHC) and Au(NHC), a monocarbene gold(I) complex and the corresponding bis(carbene) complex, are two structurally related compounds, endowed with cytotoxic properties against several cancer cell lines. Herein, we explore the molecular and cellular mechanisms at the basis of their cytotoxicity in A2780 human ovarian cancer cells. Through a comparative proteomic analysis, we demonstrated that the number of modulated proteins is far larger in Au(NHC)-treated than in Au(NHC)-treated A2780 cells. Both gold compounds mainly affected proteins belonging to the following functional classes: protein synthesis, metabolism, cytoskeleton and stress response and chaperones. Particularly, Au(NHC) gave rise to an evident upregulation of several glycolytic enzymes. Moreover, only Au(NHC) triggered a net impairment of respiration and a metabolic shift towards glycolysis, suggesting that mitochondria are relevant cellular targets. We also found that both carbenes, similarly to the gold(I) compound auranofin, caused a strong inhibition of the seleno-enzyme thioredoxin reductase (TrxR). In conclusion, we highlighted that coordination of two carbene ligands to the same gold(I) center greatly enhances the antiproliferative effects of the resulting compound in comparison to the monocarbene derivative. Moreover, TrxR inhibition and metabolic impairment seem to play a major role in the Au(NHC) cytotoxicity. Overall, these antiproliferative effects were also confirmed on other two human ovarian cancer cell lines ( SKOV3 and IGROV1).

摘要

单卡宾金(I)配合物Au(NHC)和相应的双卡宾配合物Au(NHC)是两种结构相关的化合物,对多种癌细胞系具有细胞毒性。在此,我们探究了它们在A2780人卵巢癌细胞中产生细胞毒性的分子和细胞机制。通过比较蛋白质组学分析,我们证明,与用Au(NHC)处理的A2780细胞相比,用Au(NHC)处理的细胞中被调节的蛋白质数量要多得多。两种金化合物主要影响以下功能类别的蛋白质:蛋白质合成、代谢、细胞骨架以及应激反应和伴侣蛋白。特别地,Au(NHC)导致几种糖酵解酶明显上调。此外,只有Au(NHC)引发了呼吸的净损伤以及代谢向糖酵解的转变,这表明线粒体是相关的细胞靶点。我们还发现,与金(I)化合物金诺芬类似,两种卡宾均强烈抑制硒酶硫氧还蛋白还原酶(TrxR)。总之,我们强调,与单卡宾衍生物相比,两个卡宾配体与同一个金(I)中心的配位极大地增强了所得化合物的抗增殖作用。此外,TrxR抑制和代谢损伤似乎在Au(NHC)的细胞毒性中起主要作用。总体而言,这些抗增殖作用在另外两种人卵巢癌细胞系(SKOV3和IGROV1)中也得到了证实。

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