1. Puerarin protects against heart failure induced by pressure overload through mitigation of ferroptosis
- Author
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Sudan Xu, Xiaoqian Chen, Chunxia Zhao, Hongkun Li, Yu Ding, and Bei Liu
- Subjects
Male ,0301 basic medicine ,Programmed cell death ,Iron Overload ,Vasodilator Agents ,Biophysics ,Apoptosis ,Blood Pressure ,Pharmacology ,Biochemistry ,Cell Line ,Rats, Sprague-Dawley ,Lipid peroxidation ,03 medical and health sciences ,chemistry.chemical_compound ,0302 clinical medicine ,Puerarin ,Isoprenaline ,Ventricular Dysfunction ,medicine ,Animals ,Myocyte ,Myocytes, Cardiac ,Viability assay ,Molecular Biology ,Heart Failure ,Pressure overload ,Cell Biology ,Isoflavones ,Rats ,030104 developmental biology ,chemistry ,030220 oncology & carcinogenesis ,medicine.drug - Abstract
Heart failure (HF) is the end stage of cardiovascular disease and is characterized by the loss of myocytes caused by cell death. Puerarin has been found to improve HF clinically, and animal study findings have confirmed its anti-cell-death properties. However, the underlying mechanisms remain unclear, especially with respect to the impact on ferroptosis, a newly defined mechanism of iron-dependent non-apoptotic cell death in HF. Here, ferroptosis-like cell death was observed in erastin- or isoprenaline (ISO)-treated H9c2 myocytes in vitro and in rats with aortic banding inducing HF, characterized by reduced cell viability with increased lipid peroxidation and labile iron pool. Interestingly, the increased iron overload and lipid peroxidation observed in either rats with HF or H9c2 cells incubated with ISO were significantly blocked by puerarin administration. These results provide compelling evidence that puerarin plays a role in inhibiting myocyte loss during HF, partly through ferroptosis mitigation, suggesting a new mechanism of puerarin as a potential therapy for HF.
- Published
- 2018
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