Cancer cell death induced by phosphine gold(I) compounds targeting thioredoxin reductase

硫氧还蛋白还原酶 奥兰诺芬 硫氧还蛋白 化学 癌细胞 生物化学 谷胱甘肽 程序性细胞死亡 谷胱甘肽还原酶 金化合物 细胞凋亡 谷胱甘肽过氧化物酶 生物 癌症 类风湿性关节炎 遗传学 免疫学 组合化学
作者
Valentina Gandin,Aristi P. Fernandes,Maria Pia Rigobello,Barbara Dani,Francesca Sorrentino,Francesco Tisato,Mikael Björnstedt,Alberto Bindoli,Alberto Sturaro,R. Rella,Cristina Marzano
出处
期刊:Biochemical Pharmacology [Elsevier BV]
卷期号:79 (2): 90-101 被引量:233
标识
DOI:10.1016/j.bcp.2009.07.023
摘要

The thioredoxin system, composed of thioredoxin reductase (TrxR), thioredoxin (Trx), and NADPH (nicotinamide adenine dinucleotide phosphate), plays a central role in regulating cellular redox homeostasis and signaling pathways. TrxR, overexpressed in many tumor cells and contributing to drug resistance, has emerged as a new target for anticancer drugs. Gold complexes have been validated as potent TrxR inhibitors in vitro in the nanomolar range. In order to obtain potent and selective TrxR inhibitors, we have synthesized a series of linear, ‘auranofin-like’ gold(I) complexes all containing the [Au(PEt3)]+ synthon and the ligands: Cl−, Br−, cyanate, thiocyanate, ethylxanthate, diethyldithiocarbamate and thiourea. Phosphine gold(I) complexes efficiently inhibited cytosolic and mitochondrial TrxR at concentrations that did not affect the two related oxidoreductases glutathione reductase (GR) and glutathione peroxidase (GPx). The inhibitory effect of the redox proteins was also observed intracellularly in cancer cells pretreated with gold(I) complexes. Gold(I) compounds were found to induce antiproliferative effects towards several human cancer cells some of which endowed with cisplatin or multidrug resistance. In addition, they were able to activate caspase-3 and induce apoptosis observed as nucleosome formation and sub-G1 cell accumulation. The complexes with thiocyanate and xanthate ligands were particularly effective in inhibiting thioredoxin reductase and inducing apoptosis. Pharmacodynamic studies in human ovarian cancer cells allowed for the correlation of intracellular drug accumulation with TrxR inhibition that leads to the induction of apoptosis via the mitochondrial pathway.

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