Endothelial ILK induces cardioprotection by preventing coronary microvascular dysfunction and endothelial-to-mesenchymal transition.

IF 7.5 1区 医学 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS
P Reventun, S Sánchez-Esteban, A Cook-Calvete, M Delgado-Marín, C Roza, S Jorquera-Ortega, I Hernandez, L Tesoro, L Botana, J L Zamorano, C Zaragoza, M Saura
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Abstract

Endothelial dysfunction is an early event in coronary microvascular disease. Integrin-linked kinase (ILK) prevents endothelial nitric oxide synthase (eNOS) uncoupling and, thus, endothelial dysfunction. However, the specific role of endothelial ILK in cardiac function remains to be fully elucidated. We hypothesised that endothelial ILK plays a crucial role in maintaining coronary microvascular function and contractile performance in the heart. We generated an endothelial cell-specific ILK conditional knock-out mouse (ecILK cKO) and investigated cardiovascular function. Coronary endothelial ILK deletion significantly impaired cardiac function: ejection fraction, fractional shortening and cardiac output decreased, whilst left ventricle diastolic internal diameter decreased and E/A and E/E' ratios increased, indicating not only systolic but also diastolic dysfunction. The functional data correlated with extensive extracellular matrix remodelling and perivascular fibrosis, indicative of adverse cardiac remodelling. Mice with endothelial ILK deletion suffered early ischaemic-like events with ST elevation and transient increases in cardiac troponins, which correlated with fibrotic remodelling. In addition, ecILK cKO mice exhibited many features of coronary microvascular disease: reduced cardiac perfusion, impaired coronary flow reserve and arterial remodelling with patent epicardial coronary arteries. Moreover, endothelial ILK deletion induced a moderate increase in blood pressure, but the antihypertensive drug Losartan did not affect microvascular remodelling whilst only partially ameliorated fibrotic remodelling. The plasma miRNA profile reveals endothelial-to-mesenchymal transition (endMT) as an upregulated pathway in endothelial ILK conditional KO mice. Our results show that endothelial cells in the microvasculature in endothelial ILK conditional KO mice underwent endMT. Moreover, endothelial cells isolated from these mice and ILK-silenced human microvascular endothelial cells underwent endMT, indicating that decreased endothelial ILK contributes directly to this endothelial phenotype shift. Our results identify ILK as a crucial regulator of microvascular endothelial homeostasis. Endothelial ILK prevents microvascular dysfunction and cardiac remodelling, contributing to the maintenance of the endothelial cell phenotype.

Abstract Image

内皮ILK通过防止冠状动脉微血管功能障碍和内皮-间质转化诱导心脏保护。
内皮功能障碍是冠状动脉微血管疾病的早期事件。整合素连接激酶(ILK)可防止内皮一氧化氮合酶(eNOS)解偶联,从而防止内皮功能障碍。然而,内皮细胞ILK在心功能中的具体作用仍有待充分阐明。我们假设内皮细胞ILK在维持心脏冠状动脉微血管功能和收缩性能方面起着至关重要的作用。我们制造了内皮细胞特异性ILK条件敲除小鼠(ecILK cKO)并研究了心血管功能。冠状动脉内皮ILK缺失显著损害心功能:射血分数、分数缩短和心输出量降低,左心室舒张内径减小,E/A和E/E′比值升高,表明不仅有收缩期功能障碍,还有舒张期功能障碍。功能数据与广泛的细胞外基质重构和血管周围纤维化相关,表明不良的心脏重构。内皮细胞ILK缺失的小鼠出现早期缺血样事件,伴有ST段抬高和心脏肌钙蛋白的短暂性增加,这与纤维化重构相关。此外,ecILK cKO小鼠表现出冠状动脉微血管疾病的许多特征:心脏灌注减少,冠状动脉血流储备受损,动脉重构伴心外膜冠状动脉未闭。此外,内皮ILK缺失诱导血压适度升高,但降压药氯沙坦不影响微血管重构,仅部分改善纤维化重构。血浆miRNA谱显示内皮-间质转化(endMT)在内皮ILK条件下的KO小鼠中是一个上调的途径。我们的研究结果表明,内皮ILK条件下的KO小鼠微血管内皮细胞发生了endMT。此外,从这些小鼠和ILK沉默的人微血管内皮细胞分离的内皮细胞发生了endMT,表明内皮ILK的减少直接导致了内皮表型的转变。我们的研究结果确定ILK是微血管内皮稳态的关键调节因子。内皮ILK可防止微血管功能障碍和心脏重构,有助于维持内皮细胞表型。
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来源期刊
Basic Research in Cardiology
Basic Research in Cardiology 医学-心血管系统
CiteScore
16.30
自引率
5.30%
发文量
54
审稿时长
6-12 weeks
期刊介绍: Basic Research in Cardiology is an international journal for cardiovascular research. It provides a forum for original and review articles related to experimental cardiology that meet its stringent scientific standards. Basic Research in Cardiology regularly receives articles from the fields of - Molecular and Cellular Biology - Biochemistry - Biophysics - Pharmacology - Physiology and Pathology - Clinical Cardiology
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