The First Affiliated Hospital, Shantou University Medical College, Shantou, China.
Department of Pharmacology, Shantou University Medical College, Shantou, China.
J Cell Mol Med. 2024 Jan;28(2):e18049. doi: 10.1111/jcmm.18049. Epub 2023 Nov 21.
Derangement of redox condition largely contributes to cardiac ischemia/reperfusion (I/R) injury. FoxO1 is a transcription factor which transcripts a series of antioxidants to antagonize I/R-induced oxidative myocardial damage. N-n-butyl haloperidol iodide (F ) is a derivative derived from haloperidol structural modification with potent capacity of inhibiting oxidative stress. This investigation intends to validate whether cardio-protection of F is dependent on FoxO1 using an in vivo mouse I/R model and if so, to further elucidate the molecular regulating mechanism. This study initially revealed that F preconditioning led to a profound reduction in I/R injury, which was accompanied by attenuated oxidative stress and upregulation of antioxidants (SOD2 and catalase), nuclear FoxO1 and phosphorylation of AMPK. Furthermore, inactivation of FoxO1 with AS1842856 abolished the cardio-protective effect of F . Importantly, we identified F -mediated nuclear accumulation of FoxO1 is dependent on AMPK, as blockage of AMPK with compound C induced nuclear exit of FoxO1. Collectively, our data uncover that F pretreatment exerts significant protection against post ischemic myocardial injury by its regulation of AMPK/FoxO1 pathway, which may provide a new avenue for treating ischemic disease.
氧化还原状态的紊乱在很大程度上导致了心脏缺血/再灌注(I/R)损伤。FoxO1 是一种转录因子,它转录一系列抗氧化剂来拮抗 I/R 诱导的氧化心肌损伤。N-正丁基哈尔丙醇碘化物(F)是一种从哈尔丙醇结构修饰而来的衍生物,具有很强的抑制氧化应激的能力。本研究旨在利用体内小鼠 I/R 模型验证 F 的心脏保护作用是否依赖于 FoxO1,如果是,进一步阐明其分子调节机制。本研究首先揭示了 F 预处理导致 I/R 损伤的显著减少,这伴随着氧化应激的减弱和抗氧化剂(SOD2 和过氧化氢酶)、核 FoxO1 和 AMPK 磷酸化的上调。此外,用 AS1842856 使 FoxO1 失活消除了 F 的心脏保护作用。重要的是,我们确定 F 介导的 FoxO1 的核积累依赖于 AMPK,因为用化合物 C 阻断 AMPK 会诱导 FoxO1 的核输出。总之,我们的数据揭示了 F 预处理通过调节 AMPK/FoxO1 通路对缺血后心肌损伤发挥显著的保护作用,这可能为治疗缺血性疾病提供了新的途径。
