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Ref-1对配对结构域中两个半胱氨酸残基的氧化还原修饰调节Pax-8的DNA结合活性。

Oxidoreductive modification of two cysteine residues in paired domain by Ref-1 regulates DNA-binding activity of Pax-8.

作者信息

Cao Xia, Kambe Fukushi, Ohmori Sachiko, Seo Hisao

机构信息

Division of Molecular and Cellular Adaptation, Department of Endocrinology and Metabolism, Research Institute of Environmental Medicine, Nagoya University, Furo-cho, Chikusa-ku, Japan.

出版信息

Biochem Biophys Res Commun. 2002 Sep 20;297(2):288-93. doi: 10.1016/s0006-291x(02)02196-4.

Abstract

We have reported reversible oxidoreductive regulation of DNA-binding activity of Pax-8: oxidation inhibits its binding and subsequent reduction restores the binding. Here, we show that Cys-45 and Cys-57 in the paired domain of rat Pax-8, which are conserved in all Pax members, are responsible for the redox regulation of its binding. Electrophoretic mobility shift assay using deletion mutants and mutants with substitution of cysteine with serine revealed that oxidation by diamide of either Cys-45 or Cys-57 loses the DNA binding of Pax-8. An intracellular oxidoreductive enzyme redox factor-1 (Ref-1) could reduce the oxidized Cys-45 or Cys-57 and restored the binding. Furthermore, reporter gene assay showed that transcriptional activity of wild-type Pax-8 was enhanced by co-expression of Ref-1. When the mutant with double substitutions of Cys-45 and Cys-57, which was insensitive to oxidation, was transfected, the basal transactivation level was much higher than that of wild-type Pax-8, while it was not enhanced by Ref-1. These results demonstrated that oxidoreductive modification of Cys-45 and Cys-57 via Ref-1 plays a role in redox regulation of Pax-8 in living cells.

摘要

我们曾报道过Pax-8的DNA结合活性存在可逆的氧化还原调节:氧化会抑制其结合,随后的还原则会恢复结合。在此,我们表明大鼠Pax-8配对结构域中的Cys-45和Cys-57在所有Pax成员中都是保守的,它们负责其结合的氧化还原调节。使用缺失突变体以及用丝氨酸替代半胱氨酸的突变体进行的电泳迁移率变动分析表明,用二硫苏糖醇氧化Cys-45或Cys-57会导致Pax-8失去DNA结合能力。一种细胞内氧化还原酶氧化还原因子-1(Ref-1)能够还原被氧化的Cys-45或Cys-57并恢复结合能力。此外,报告基因分析表明,Ref-1的共表达增强了野生型Pax-8的转录活性。当转染对氧化不敏感的Cys-45和Cys-57双取代突变体时,基础反式激活水平远高于野生型Pax-8,而Ref-1并未增强其活性。这些结果表明,通过Ref-1对Cys-45和Cys-57进行氧化还原修饰在活细胞中Pax-8的氧化还原调节中发挥作用。

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