Prostacyclin receptor agonists induce DUSP1 to inhibit pulmonary artery smooth muscle cell proliferation.

H. Maruyama, S. Sakai, L. Dewachter, C. Dewachter, B. Rondelet, R. Naeije, M. Ieda
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引用次数: 1

Abstract

AIMS Upregulated p38MAPK signaling is implicated in the accelerated proliferation of pulmonary artery smooth muscle cells (PA-SMCs) and the pathogenesis of pulmonary artery remodeling observed in pulmonary arterial hypertension (PAH). Previously, we reported that after endothelin-1 (ET-1) pretreatment, bone morphogenetic protein 2 (BMP2) activates p38MAPK signaling and accelerates PA-SMC proliferation. The activity of p38MAPK signaling is tightly regulated by the inactivation of dual-specificity phosphatase 1 (DUSP1). Activated p38MAPK induces DUSP1 expression, forming a negative feedback loop. Prostacyclin IP receptor agonists (prostacyclin and selexipag) are used to treat PAH. In this study, we aimed to verify whether IP receptor agonists affect DUSP1 expression and accelerate the proliferation of PA-SMCs. MAIN METHODS PA-SMCs were treated with BMP2, ET-1, prostacyclin, and MRE-269, an active metabolite of selexipag, either alone or in combination. We quantified mRNA expressions using real-time quantitative polymerase chain reaction. Pulmonary artery specimens and PA-SMCs were obtained during lung transplantation in patients with PAH. KEY FINDINGS Both prostacyclin and MRE-269 increased DUSP1 expression. Combined treatment with BMP2 and ET-1 induced cyclin D1 and DUSP1 expression and increased PA-SMC proliferation. MRE-269 attenuated BMP2/ET-1-induced cell proliferation. ET-1 increased DUSP1 expression in PA-SMCs from control patients but not in PA-SMCs from patients with PAH. SIGNIFICANCE This study showed that the p38MAPK/DUSP1 negative feedback loop is impaired in PAH, contributing to unregulated p38MAPK activation and PA-SMC hyperplasia. IP receptor agonist MRE-269 increases DUSP1 expression and inhibit p38MAPK-mediated PA-SMC proliferation. Future elucidation of the detailed mechanism underlying reduced DUSP1 expression would be informative for PAH treatment.
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前列环素受体激动剂诱导DUSP1抑制肺动脉平滑肌细胞增殖。
aim调控的p38MAPK信号与肺动脉高压(PAH)中肺动脉平滑肌细胞(PA-SMCs)的加速增殖和肺动脉重塑的发病机制有关。此前,我们报道了内皮素-1 (ET-1)预处理后,骨形态发生蛋白2 (bone morphogenetic protein 2, BMP2)激活p38MAPK信号,加速PA-SMC增殖。p38MAPK信号的活性受到双特异性磷酸酶1 (DUSP1)失活的严格调控。激活的p38MAPK诱导DUSP1表达,形成负反馈循环。前列环素IP受体激动剂(前列环素和selexipag)用于治疗PAH。在本研究中,我们旨在验证IP受体激动剂是否会影响DUSP1的表达并加速PA-SMCs的增殖。主要方法分别用BMP2、ET-1、前列环素和selexipag活性代谢物MRE-269单独或联合治疗spa - smcs。我们使用实时定量聚合酶链反应定量mRNA表达。肺动脉标本和PA-SMCs在PAH患者肺移植过程中获得。主要发现:前列环素和MRE-269均可增加DUSP1的表达。BMP2和ET-1联合治疗可诱导cyclin D1和DUSP1的表达,增加PA-SMC的增殖。MRE-269减弱BMP2/ et -1诱导的细胞增殖。ET-1增加了对照组患者的PA-SMCs中DUSP1的表达,而在PAH患者的PA-SMCs中则没有。本研究表明p38MAPK/DUSP1负反馈回路在PAH中受损,导致p38MAPK激活不调节和PA-SMC增生。IP受体激动剂MRE-269增加DUSP1表达,抑制p38mapk介导的PA-SMC增殖。未来阐明DUSP1表达减少的详细机制将为PAH的治疗提供信息。
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