NPA7:一种抑制心脏氧化应激的双受体激活肽。
NPA7: A Dual Receptor Activating Peptide That Inhibits Cardiac Oxidative Stress.
作者信息
Ma Xiaoyu, Malsawmzuali Joute Chawngvawr, Moroni Dante G, Ma Xiao, Zheng Ye, Pan Shuchong, Wang Ying, Sangaralingham S Jeson, Burnett John C
机构信息
Cardiorenal Research Laboratory, Department of Cardiovascular Medicine (Xiaoyu Ma, J.C.M., D.G.M., Xiao Ma, Y.Z., S.P., Y.W., S.J.S., J.C.B.), Mayo Clinic, Rochester, MN.
Department of Physiology and Biomedical Engineering (S.J.S., J.C.B.), Mayo Clinic, Rochester, MN.
出版信息
Hypertension. 2025 Mar;82(3):463-475. doi: 10.1161/HYPERTENSIONAHA.124.23579. Epub 2025 Jan 8.
BACKGROUND
Cardiomyocyte oxidative stress significantly contributes to the progression of hypertension-induced heart failure, highlighting the need for targeted therapies. We developed a novel peptide, NPA7, that coactivates the GC-A (guanylyl cyclase A)/cGMP and MasR (Mas receptor)/cAMP pathway. This study aimed to test NPA7's ability to inhibit oxidative stress by modulating the p62 (Sequestosome 1)-KEAP1 (Kelch-like ECH-associated protein 1)-NRF2 (nuclear factor erythroid 2-related factor 2) pathway in human cardiomyocytes (HCMs) and a rat model of hypertension.
METHODS
Oxidative stress was induced in HCMs using HO with phosphate-buffered saline or NPA7 treatment. Intracellular reactive oxygen species levels were assessed via dihydroethidium staining. Western blotting analysis measured p62, KEAP1, and NRF2 protein levels, while GSH/GSSG (glutathione/glutathione disulfide) ratios and antioxidant gene expression were analyzed. HCMs were transfected with small interfering RNA targeting GC-A, MasR, or p62 before NPA7 and HO treatment. In vivo, spontaneously hypertensive rats received saline or NPA7, with normotensive Wistar Kyoto rats as control and cardiac oxidative stress, KEAP1 protein levels, NOX2 (NADPH oxidase 2), and p67 (NADPH oxidase subunit p67-phox) mRNA levels were measured.
RESULTS
NPA7 reduced HO-induced reactive oxygen species levels and increased GSH/GSSG ratio in HCMs. Silencing GC-A (guanylyl cyclase A receptor) and MasR (Mas receptor) reversed NPA7's effects. NPA7 activated the KEAP1-NRF2 pathway, enhancing NRF2's antioxidant target gene expression. In p62 knockdown HCMs, NPA7-induced KEAP1 degradation and NRF2 activation were diminished. Reactive oxygen species levels were elevated in spontaneously hypertensive rat versusWistar Kyoto rats' hearts, however, NPA7 treatment reduced myocardial reactive oxygen species, suppressed KEAP1 protein, and decreased NOX2 and p67 mRNA levels.
CONCLUSIONS
NPA7 exhibits antioxidant properties in HCMs and spontaneously hypertensive rat hearts by targeting GC-A and MasR through the p62-KEAP1-NRF2 pathway, supporting a novel therapeutic approach against cardiovascular disease-related oxidative stress.
背景
心肌细胞氧化应激在高血压性心力衰竭的进展中起重要作用,这凸显了靶向治疗的必要性。我们研发了一种新型肽NPA7,它可共同激活GC-A(鸟苷酸环化酶A)/cGMP和MasR(Mas受体)/cAMP信号通路。本研究旨在测试NPA7通过调节人心肌细胞(HCMs)和高血压大鼠模型中的p62(聚集体蛋白1)-KEAP1(类kelch结构域蛋白1)-NRF2(核因子红细胞2相关因子2)信号通路来抑制氧化应激的能力。
方法
使用HO联合磷酸盐缓冲盐水或NPA7处理诱导HCMs产生氧化应激。通过二氢乙锭染色评估细胞内活性氧水平。蛋白质免疫印迹分析检测p62、KEAP1和NRF2蛋白水平,同时分析谷胱甘肽/谷胱甘肽二硫化物(GSH/GSSG)比值和抗氧化基因表达。在NPA7和HO处理前,用靶向GC-A、MasR或p62的小干扰RNA转染HCMs。在体内,自发性高血压大鼠接受盐水或NPA7处理,以正常血压的Wistar Kyoto大鼠作为对照,测量心脏氧化应激、KEAP1蛋白水平、NOX2(烟酰胺腺嘌呤二核苷酸磷酸氧化酶2)和p67(烟酰胺腺嘌呤二核苷酸磷酸氧化酶亚基p67-氧化型辅酶Ⅱ)mRNA水平。
结果
NPA7降低了HO诱导的HCMs活性氧水平,并提高了GSH/GSSG比值。沉默GC-A(鸟苷酸环化酶A受体)和MasR(Mas受体)可逆转NPA7的作用。NPA7激活了KEAP1-NRF2信号通路,增强了NRF2的抗氧化靶基因表达。在p62基因敲低的HCMs中,NPA7诱导的KEAP1降解和NRF2激活减弱。与Wistar Kyoto大鼠心脏相比,自发性高血压大鼠心脏中的活性氧水平升高,然而,NPA7处理降低了心肌活性氧水平,抑制了KEAP1蛋白表达,并降低了NOX2和p67 mRNA水平。
结论
NPA7通过p62-KEAP1-NRF2信号通路靶向GC-A和MasR,在HCMs和自发性高血压大鼠心脏中表现出抗氧化特性,为心血管疾病相关氧化应激提供了一种新的治疗方法。
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