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Keap1, the cysteine-based mammalian intracellular sensor for electrophiles and oxidants

机译:Keap1,基于半胱氨酸的哺乳动物细胞内传感器,用于电子氧化剂和氧化剂

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摘要

The Kelch-like ECH associated protein 1 (Keap1) is a component of a Cullin3-based Cullin-RING E3 ubiquitin ligase (CRL) multisubunit protein complex. Within the CRL, homodimeric Keap1 functions as the Cullin3 adaptor, and importantly, it is also the critical component of the E3 ligase that performs the substrate recognition. The best-characterized substrate of Keap1 is transcription factor NF-E2 p45-related factor 2 (Nrf2), which orchestrates an elaborate transcriptional program in response to environmental challenges caused by oxidants, electrophiles and pro-inflammatory agents, allowing adaptation and survival under stress conditions. Keap1 is equipped with reactive cysteine residues that act as sensors for endogenously produced and exogenously encountered small molecules (termed inducers), which have a characteristic chemical signature, reactivity with sulfhydryl groups. Inducers modify the cysteine sensors of Keap1 and impair its ability to target Nrf2 for ubiquitination and degradation. Consequently, Nrf2 accumulates, enters the nucleus and drives the transcription of its target genes, which encode a large network of cytoprotective proteins. Here we summarize the early studies leading to the prediction of the existence of Keap1, followed by the discovery of Keap1 as the main negative regulator of Nrf2. We then describe the available structural information on Keap1, its assembly with Cullin3, and its interaction with Nrf2. We also discuss the multiple cysteine sensors of Keap1 that allow for detection of a wide range of endogenous and environmental inducers, and provide fine-tuning and tight control of the Keap1/Nrf2 stress-sensing response. (C) 2016 Published by Elsevier Inc.
机译:Kelch样Ech相关蛋白1(Keap1)是Cullin3的Cullin-Ring E3泛素连接酶(CRL)多管蛋白质复合物的组分。在CRL内,同源化Keap1用作Cullin3适配器,并且重要的是,它也是执行基板识别的E3连接酶的关键组件。 Keap1的最佳表征底物是转录因子NF-E2 P45相关因子2(NRF2),其响应于氧化剂,电子药物和促炎剂引起的环境挑战,允许在压力下进行适应和存活的环境挑战进行协调状况。 Keap1配备有反应性半胱氨酸残基,其充当内源性产生和外源遇到的小分子(称为诱导剂)的传感器,其具有特征化学特征,与巯基的反应性。诱导剂改变Keap1的半胱氨酸传感器,损害其靶向NRF2以普遍染色和降解的能力。因此,NRF2累积,进入细胞核并驱动其靶基因的转录,其编码大型细胞保护蛋白网络。在这里,我们总结了导致预测Keap1的存在的早期研究,然后发现Keap1作为NRF2的主要负调节剂。然后,我们用Cullin3描述Keap1的可用结构信息,以及与NRF2的相互作用。我们还讨论了Keap1的多个半胱氨酸传感器,其允许检测各种内源性和环境诱导剂,并提供Keap1 / NRF2应激感应响应的微调和紧密控制。 (c)2016年由elsevier公司发布

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