AKAP1 in Renal Patients with AHF to Reduce Ferroptosis of Cardiomyocyte

Yifeng Fang, Junpeng Xu, Ruofei Huang
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Abstract

Background: This study mainly investigated the mechanism and effects of AKAP1 in renal patients with acute heart failure (AHF). Methods: Patients with renal patients with AHF and normal volunteers were collected. The left anterior descending arteries (LAD) of mice were ligated to induce myocardial infarction. Results: AKAP1 messenger RNA (mRNA) expression was found to be down-regulated in renal patients with AHF. The serum levels of AKAP1 mRNA expression were negatively correlated with collagen I/III in patients. AKAP1 mRNA and protein expression in the heart tissue of mice with AHF were also found to be down-regulated in a time-dependent manner. Short hairpin (Sh)-AKAP1 promotes AHF in a mouse model. AKAP1 up-regulation reduces reactive oxygen species (ROS)-induced oxidative stress in an In Vitro model. AKAP1 up-regulation also reduces ROS-induced lipid peroxidation ferroptosis in an In Vitro model. AKAP1 induces NDUFS1 expression to increase GPX4 activity levels. AKAP1 protein interlinked with the NDUFS1 protein. Up-regulation of the AKAP1 gene reduced NDUFS1 ubiquitination, while down-regulation of the AKAP1 gene increased NDUFS1 ubiquitination in a model. In vivo imaging showed that the sh-AKAP1 virus reduced NDUFS1 expression in the heart of a mouse model. Conclusions: AKAP1 reduced ROS-induced lipid peroxidation ferroptosis through the inhibition of ubiquitination of NDUFS by mitochondrial damage in model of renal patients with AHF, suggest a novel target for AHF treatment.
AKAP1 在 AHF 肾病患者中减少心肌细胞的铁突变
研究背景本研究主要探讨AKAP1在急性心力衰竭(AHF)肾病患者中的作用机制。研究方法收集急性心力衰竭肾病患者和正常志愿者。结扎小鼠左前降支动脉(LAD)诱发心肌梗死。结果发现AHF肾病患者的AKAP1信使RNA(mRNA)表达下调。患者血清中 AKAP1 mRNA 的表达水平与胶原 I/III 呈负相关。研究还发现,AHF 小鼠心脏组织中的 AKAP1 mRNA 和蛋白表达也呈时间依赖性下调。短发夹(Sh)-AKAP1 可促进小鼠模型中的 AHF。在体外模型中,AKAP1上调可降低活性氧(ROS)诱导的氧化应激。在体外模型中,上调 AKAP1 还能减少 ROS 诱导的脂质过氧化铁中毒。AKAP1 可诱导 NDUFS1 的表达,从而提高 GPX4 的活性水平。AKAP1 蛋白与 NDUFS1 蛋白相互连接。在一个模型中,上调 AKAP1 基因可减少 NDUFS1 泛素化,而下调 AKAP1 基因可增加 NDUFS1 泛素化。体内成像显示,sh-AKAP1 病毒减少了小鼠模型心脏中 NDUFS1 的表达。结论在 AHF 肾病模型中,AKAP1 通过抑制线粒体损伤对 NDUFS 的泛素化,减少了 ROS 诱导的脂质过氧化铁中毒,为 AHF 治疗提供了一个新靶点。
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