Hyperphosphate-Induced Myocardial Hypertrophy through the GATA-4/NFAT-3 Signaling Pathway Is Attenuated by ERK Inhibitor Treatment

Chao-Min Wang; Che-Yi Chou; Chih-Yang Huang; Chiu-Ching Huang; Chiz-Chung Chang; Dennis Jine-Yuan Hsieh; Gwo-Ping Jong; I-Kuan Wang; Shih-Yi Lin; Yao-Lung Liu

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Hyperphosphate-Induced Myocardial Hypertrophy through the GATA-4/NFAT-3 Signaling Pathway Is Attenuated by ERK Inhibitor Treatment

机译：通过ERK抑制剂治疗可减轻通过GATA-4 / NFAT-3信号通路引起的高磷酸盐诱导的心肌肥大。

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>Background/Aims: Numerous epidemiological studies have associated elevated serum phosphorus levels with cardiovascular disease and the risk of death in the general population as well as in chronic kidney disease (CKD) and dialysis patients. In this study, we explored whether elevated phosphate conditions induce cardiac hypertrophy and attempted to identify the molecular and cellular mechanisms in the hypertrophic response. Methods: H9c2 myocardial cells were incubated in high-phosphate conditions to induce hypertrophy. Pathological hypertrophic responses were measured in terms of cell size, arrangement of actin filaments, and hypertrophy markers such as atrial natriuretic peptide (ANP) and B-type natriuretic peptide (BNP) in myocardial cells. Several transcriptional factors involved in cardiac hypertrophy development were measured to investigate the molecular pathways involved in elevated phosphate-induced cardiac hypertrophy. Results: High-phosphate conditions induced cellular hypertrophy, marked by increased cell size, reorganization of actin filaments, and upregulation of both ANP and BNP in H9c2 cells. Both upstream calcineurin and downstream transcription factors, including GATA-4 and NFAT-3, were significantly increased under hyperphosphate conditions. Moreover, both MEK1/2 and ERK1/2 expression increased significantly, and cellular hypertrophy was markedly attenuated by U0126, an ERK1/2 inhibitor. Conclusions: These results suggest that hyperphosphate conditions induce myocardial hypertrophy through the ERK signaling pathway in H9c2 cells. Our findings provide a link between the hyperphosphate-induced response and the ERK/NFAT-3 signaling pathway that mediates the development of cardiac hypertrophy. In view of the potent and selective activity of the ERK inhibitor U0126, this agent warrants further investigation as a candidate for preventing hyperphosphate-induced cardiac hypertrophy in CKD and dialysis patients.

机译：> 背景/目标：众多流行病学研究表明，血清磷水平升高与心血管疾病以及普通人群和慢性肾脏疾病的死亡风险相关（ CKD）和透析患者。在这项研究中，我们探讨了磷酸盐水平升高是否会诱发心脏肥大，并试图确定肥大性反应中的分子和细胞机制。方法： H9c2心肌细胞在高磷酸盐条件下孵育以诱导肥大。根据细胞大小，肌动蛋白丝的排列以及心肌细胞中的肥大标志物（如心钠素和B型肥大素）来测量病理性肥大反应。测量了参与心脏肥大发展的几种转录因子，以研究参与磷酸盐诱导的心脏肥大升高的分子途径。结果：高磷酸盐条件诱导细胞肥大，其特征是细胞大小增加，肌动蛋白丝重组，H9c2细胞中ANP和BNP均上调。在高磷酸盐条件下，上游钙调磷酸酶和下游转录因子（包括GATA-4和NFAT-3）均显着增加。此外，MEK1 / 2和ERK1 / 2的表达均显着增加，并且细胞肥大被ERK1 / 2抑制剂U0126显着减弱。结论：这些结果表明，高磷酸盐血症可通过H9c2细胞中的ERK信号通路诱导心肌肥大。我们的发现提供了高磷酸盐诱导的反应与介导心脏肥大发展的ERK / NFAT-3信号通路之间的联系。鉴于ERK抑制剂U0126的强效和选择性活性，该药物作为预防高磷酸盐血症引起的CKD和透析患者心脏肥大的候选药物值得进一步研究。

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《Cardiorenal medicine》 |2015年第2期|共10页
作者
Chao-Min Wang; Che-Yi Chou; Chih-Yang Huang; Chiu-Ching Huang; Chiz-Chung Chang; Dennis Jine-Yuan Hsieh; Gwo-Ping Jong; I-Kuan Wang; Shih-Yi Lin; Yao-Lung Liu;
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中图分类心脏、血管（循环系）疾病;
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入库时间 2022-08-18 06:17:22

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6. Hyperphosphate-Induced Myocardial Hypertrophy through the GATA-4/NFAT-3 Signaling Pathway Is Attenuated by ERK Inhibitor Treatment [O] . Yao-Lung Liu, Chiu-Ching Huang, Chiz-Chung Chang, 2015

机译：通过ERK抑制剂治疗减弱了通过GATA-4 / NFAT-3信号通路引起的高磷酸盐诱导的心肌肥大。
7. Hyperphosphate-Induced Myocardial Hypertrophy through the GATA-4/NFAT-3 Signaling Pathway Is Attenuated by ERK Inhibitor Treatment [O] . Yao-Lung Liu, Chiu-Ching Huang, Chiz-Chung Chang, 2015

机译：通过ERK抑制剂治疗衰减通过GATA-4 / NFAT-3信号传导途径的超磷酸诱导的心肌肥厚

Hyperphosphate-Induced Myocardial Hypertrophy through the GATA-4/NFAT-3 Signaling Pathway Is Attenuated by ERK Inhibitor Treatment

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