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亚硒酸盐或碲酸盐联合金诺芬处理人类癌细胞会因氧化还原转移而增强细胞死亡。

Treatment of human cancer cells with selenite or tellurite in combination with auranofin enhances cell death due to redox shift.

机构信息

Dipartimento di Chimica Biologica, Università di Padova, 35121 Padova, Italy.

出版信息

Free Radic Biol Med. 2009 Sep 15;47(6):710-21. doi: 10.1016/j.freeradbiomed.2009.05.027. Epub 2009 May 29.

Abstract

Selenium is an essential trace element incorporated as selenocysteine in 25 human selenoproteins. Among them are thioredoxin reductases (TrxR) and glutathione peroxidases, all central proteins in the regulation of the cellular thiol redox state. In this paper the effects of selenite and tellurite treatment in human cancer cells are reported and compared. Our results show that both selenite and tellurite, at relatively low concentrations, are able to increase the expression of mitochondrial and cytosolic TrxR in cisplatin-sensitive (2008) and -resistant (C13*) phenotypes. We further investigated the cellular effects induced by selenite or tellurite in combination with the specific TrxR inhibitor auranofin. Selenite pretreatment induced a dramatic increase in auranofin cytotoxicity in both resistant and sensitive cells. Investigation of TrxR activity and expression levels as well as the cellular redox state demonstrated the involvement of TrxR inhibition and redox changes in selenite and auranofin combined action.

摘要

硒是一种必需的微量元素,以硒代半胱氨酸的形式存在于 25 个人类硒蛋白中。其中包括硫氧还蛋白还原酶(TrxR)和谷胱甘肽过氧化物酶,它们都是调节细胞硫醇氧化还原状态的核心蛋白。本文报道并比较了亚硒酸盐和碲酸盐处理人类癌细胞的效果。我们的结果表明,亚硒酸盐和碲酸盐在相对较低的浓度下,均能增加顺铂敏感(2008 型)和耐药(C13* 型)表型中线粒体和细胞质 TrxR 的表达。我们进一步研究了亚硒酸盐或碲酸盐与特异性 TrxR 抑制剂 aurafoin 联合作用诱导的细胞效应。亚硒酸盐预处理可显著增加两种耐药和敏感细胞中 aurafoin 的细胞毒性。对 TrxR 活性和表达水平以及细胞氧化还原状态的研究表明,TrxR 抑制和氧化还原变化参与了亚硒酸盐和 aurafoin 的联合作用。

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