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首页> 外文期刊>Antioxidants and redox signalling >A Curcumin Derivative That Inhibits Vinyl Carbamate-Induced Lung Carcinogenesis via Activation of the Nrf2 Protective Response
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A Curcumin Derivative That Inhibits Vinyl Carbamate-Induced Lung Carcinogenesis via Activation of the Nrf2 Protective Response

机译:姜黄素衍生物通过激活Nrf2保护反应抑制氨基甲酸乙烯酯诱导的肺癌发生。

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Aims: Lung cancer has a high worldwide morbidity and mortality. The employment of chemopreventive agents is effective to reduce lung cancer. Nuclear factor erythroid 2-related factor 2 (Nrf2) mitigates insults from both exogenous and endogenous sources and thus has been verified as a target for chemoprevention. Curcumin has long been recognized as a chemopreventive agent, but poor bioavailability and weak Nrf2 induction have prohibited clinical application. Thus, we have developed new curcumin derivatives and tested their Nrf2 induction. Results: Based on curcumin, we synthesized curcumin analogs with five carbon linkages and established a structure-activity relationship for Nrf2 induction. Among these derivatives, bis[2-hydroxybenzylidene]acetone (BHBA) was one of the most potent Nrf2 inducers with minimal toxicity and improved pharmacological properties and was thus selected for further investigation. BHBA activated the Nrf2 pathway in the canonical Keap1-Cys151-dependent manner. Furthermore, BHBA was able to protect human lung epithelial cells against sodium arsenite [As(III)]-induced cytotoxicity. More importantly, in an in vivo vinyl carbamate-induced lung cancer model in A/J mice, preadministration of BHBA significantly reduced lung adenocarcinoma, while curcumin failed to show any effects even at high doses. Innovation: The curcumin derivative, BHBA, is a potent inducer of Nrf2. It was demonstrated to protect against As(III) toxicity in lung epithelial cells in an Nrf2-dependent manner. Furthermore, compared with curcumin, BHBA displayed improved chemopreventive activities in a carcinogen-induced lung cancer model. Conclusion: Taken together, our results demonstrate that BHBA, a curcumin analog with improved Nrf2-activating and chemopreventive activities both in vitro and in vivo, could be developed into a chemoprotective pharmacological agent. Antioxid. Redox Signal. 23, 651-664.
机译:目的:肺癌在世界范围内具有很高的发病率和死亡率。使用化学预防剂可有效减少肺癌。核因子红系2相关因子2(Nrf2)减轻了来自外源和内源性来源的侵害,因此已被证实是化学预防的目标。姜黄素长期以来一直被认为是一种化学预防剂,但是生物利用度差和Nrf2诱导能力弱已经禁止了临床应用。因此,我们开发了新的姜黄素衍生物并测试了它们的Nrf2诱导作用。结果:基于姜黄素,我们合成了具有五个碳键的姜黄素类似物,并建立了Nrf2诱导的结构-活性关系。在这些衍生物中,双[2-羟基亚苄基]丙酮(BHBA)是最有效的Nrf2诱导剂之一,具有最小的毒性和改善的药理特性,因此被选择作进一步研究。 BHBA以典型的Keap1-Cys151依赖性方式激活Nrf2途径。此外,BHBA能够保护人肺上皮细胞免受亚砷酸钠[As(III)]诱导的细胞毒性作用。更重要的是,在体内氨基甲酸乙烯基酯诱发的A / J小鼠肺癌模型中,预先给予BHBA可以显着减少肺腺癌,而姜黄素即使在高剂量下也没有表现出任何作用。创新:姜黄素衍生物BHBA是Nrf2的有效诱导剂。它被证明可以以Nrf2依赖的方式抵抗肺上皮细胞的As(III)毒性。此外,与姜黄素相比,BHBA在致癌物诱发的肺癌模型中显示出更高的化学预防活性。结论:综上所述,我们的结果表明BHBA是一种姜黄素类似物,在体外和体内均具有改善的Nrf2活化和化学预防活性,可以开发为化学保护药理剂。抗氧化。氧化还原信号。 23,651-664。

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