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装置植入后心脏适应的分子机制

Molecular Mechanisms of Cardiac Adaptation After Device Deployment.

作者信息

Romano Letizia Rosa, Plutino Paola, Lopes Giovanni, Quarta Rossella, Calvelli Pierangelo, Indolfi Ciro, Polimeni Alberto, Curcio Antonio

机构信息

Division of Cardiology, Annunziata Hospital, 87100 Cosenza, Italy.

Department of Pharmacy, Health and Nutritional Sciences, University of Calabria, 87036 Rende, Italy.

出版信息

J Cardiovasc Dev Dis. 2025 Jul 30;12(8):291. doi: 10.3390/jcdd12080291.

Abstract

Cardiac devices have transformed the management of heart failure, ventricular arrhythmias, ischemic cardiomyopathy, and valvular heart disease. Technologies such as cardiac resynchronization therapy (CRT), conduction system pacing, left ventricular assist devices (LVADs), and implantable cardioverter-defibrillators have contributed to abated global cardiovascular risk through action onto pathophysiological processes such as mechanical unloading, electrical resynchronization, or hemodynamic optimization, respectively. While their clinical benefits are well established, their long-term molecular and structural effects on the myocardium remain under investigation. Cardiac devices dynamically interact with myocardial and vascular biology, inducing molecular and extracellular matrix adaptations that vary by pathology. CRT enhances calcium cycling and reduces fibrosis, but chronic pacing may lead to pacing-induced cardiomyopathy. LVADs and Impella relieve ventricular workload yet alter sarcomeric integrity and mitochondrial function. Transcatheter valve therapies influence ventricular remodeling, conduction, and coronary flow. Understanding these remodeling processes is crucial for optimizing patient selection, device programming, and therapeutic strategies. This narrative review integrates the current knowledge on the molecular and structural effects of cardiac devices, highlighting their impact across different disease settings.

摘要

心脏设备已经改变了心力衰竭、室性心律失常、缺血性心肌病和心脏瓣膜病的治疗方式。诸如心脏再同步治疗(CRT)、传导系统起搏、左心室辅助装置(LVAD)和植入式心律转复除颤器等技术,分别通过作用于机械卸载、电再同步或血流动力学优化等病理生理过程,降低了全球心血管疾病风险。虽然它们的临床益处已得到充分证实,但其对心肌的长期分子和结构影响仍在研究中。心脏设备与心肌和血管生物学动态相互作用,诱导分子和细胞外基质适应,这种适应因病理情况而异。CRT可增强钙循环并减少纤维化,但长期起搏可能导致起搏诱导的心肌病。LVAD和Impella可减轻心室负荷,但会改变肌节完整性和线粒体功能。经导管瓣膜治疗会影响心室重塑、传导和冠状动脉血流。了解这些重塑过程对于优化患者选择、设备程控和治疗策略至关重要。这篇叙述性综述整合了关于心脏设备分子和结构影响的现有知识,强调了它们在不同疾病背景下的影响。

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