Endothelial epoxyeicosatrienoic acid release is intact in aldosterone excess

IF 4.9 2区 医学 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS Atherosclerosis Pub Date : 2024-09-05 DOI:10.1016/j.atherosclerosis.2024.118591
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Abstract

Background and aims

Endothelial dysfunction (ED) is considered to be a major driver of the increased incidence of cardiovascular disease in primary aldosteronism (PA). The functionality of the epoxyeicosatrienoic acid (EET) pathway, involving the release of beneficial endothelium-derived lipid mediators, in PA is unknown. Evidence suggests this pathway to be disturbed in various models of experimental hypertension.

We therefore assessed EET production in primary human coronary artery endothelial cells exposed to aldosterone excess and measured circulating EET in patients with PA.

Methods

We used qPCR to investigate changes in the expression levels of essential genes for the synthesis and degradation of EET, calcium imaging to address the functional impact on overall endothelial function, as well as mass spectrometry to determine endothelial synthetic capacity to release EET upon stimulation. RNA-seq was performed to gain further mechanistic insights. Eicosanoid concentrations in patient's plasma were also determined by mass spectrometry.

Results

Aldosterone, while eliciting proinflammatory VCAM1 expression and disturbed calcium response to acetylcholine, did not negatively affect stimulated release of endothelial EET. Likewise, no differences were observed in eicosanoid concentrations in plasma from patients with PA when compared to essential hypertensive controls.

However, an inhibitor of soluble epoxide hydrolase abrogated aldosterone-mediated VCAM1 induction and led to a normalized endothelial calcium response probably by restoring expression of CHRNE.

Conclusion

EET release appears intact despite aldosterone excess. Epoxide hydrolase inhibition may revert aldosterone-induced functional changes in endothelial cells. These findings indicate a potential new therapeutic principle to address ED, which should be explored in future preclinical and clinical trials.

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内皮环氧二十碳三烯酸的释放在醛固酮过量时保持不变
背景和目的内皮功能障碍(ED)被认为是原发性醛固酮增多症(PA)心血管疾病发病率增加的主要原因。环二十碳三烯酸(EET)途径涉及释放有益的内皮衍生脂质介质,但其在 PA 中的功能尚不清楚。因此,我们评估了暴露于醛固酮过量的原代人类冠状动脉内皮细胞的 EET 生成情况,并测量了 PA 患者的循环 EET。方法:我们使用 qPCR 来研究 EET 合成和降解的重要基因表达水平的变化,使用钙成像来研究对整体内皮功能的影响,并使用质谱法来确定内皮在受到刺激时释放 EET 的合成能力。为了进一步了解机理,还进行了 RNA-seq 分析。结果醛固酮虽然会引起促炎性 VCAM1 表达和对乙酰胆碱的钙反应紊乱,但不会对内皮 EET 的刺激释放产生负面影响。然而,可溶性环氧化物水解酶抑制剂可减轻醛固酮介导的 VCAM1 诱导,并可能通过恢复 CHRNE 的表达而导致内皮钙反应正常化。环氧化物水解酶抑制可恢复醛固酮诱导的内皮细胞功能变化。这些发现揭示了一种潜在的新治疗原理,可用于治疗 ED,应在未来的临床前和临床试验中加以探索。
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来源期刊
Atherosclerosis
Atherosclerosis 医学-外周血管病
CiteScore
9.80
自引率
3.80%
发文量
1269
审稿时长
36 days
期刊介绍: Atherosclerosis has an open access mirror journal Atherosclerosis: X, sharing the same aims and scope, editorial team, submission system and rigorous peer review. Atherosclerosis brings together, from all sources, papers concerned with investigation on atherosclerosis, its risk factors and clinical manifestations. Atherosclerosis covers basic and translational, clinical and population research approaches to arterial and vascular biology and disease, as well as their risk factors including: disturbances of lipid and lipoprotein metabolism, diabetes and hypertension, thrombosis, and inflammation. The Editors are interested in original or review papers dealing with the pathogenesis, environmental, genetic and epigenetic basis, diagnosis or treatment of atherosclerosis and related diseases as well as their risk factors.
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