Macrophages as key modulators of calcific aortic valve disease.

IF 2.8 3区医学 Q2 CARDIAC & CARDIOVASCULAR SYSTEMS

Frontiers in Cardiovascular Medicine Pub Date : 2025-09-24 eCollection Date: 2025-01-01 DOI:10.3389/fcvm.2025.1664067

Nervana Issa, Gérémy Blot, Alexandre Candellier, Cédric Boudot, Loïc Louvet, Saïd Kamel, Youssef Bennis, Lucie Hénaut

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Abstract

Calcific aortic valve disease (CAVD), defined by thickening, fibrosis, and mineralization of the aortic valve (AV) leaflets, is the most common valvular heart disease worldwide. This progressive remodeling gradually impairs valve opening, obstructing blood flow. Without intervention, the resulting aortic stenosis (AS) causes hemodynamic deterioration that ultimately leads to heart failure and death. To date, therapeutic options remain limited, making valve replacement the reference treatment. While valvular endothelial and interstitial cells have traditionally been considered the primary drivers of the osteogenic program underlying AV remodeling, recent evidence highlights a central role for macrophages, whose plasticity profoundly impacts the local microenvironment. In their inflammatory state, macrophages release cytokines, generate oxidative stress, and secrete Bone Morphogenetic Protein 2 (BMP2), which promotes the osteogenic transformation of valvular cells. The resulting calcium crystal deposition further amplifies macrophage-driven inflammation, creating a vicious cycle. Conversely, immunomodulatory macrophages can protect against CAVD by releasing pyrophosphate, a calcification inhibitor. However, these macrophages also secrete pro-fibrotic factors and may undergo myeloid-to-mesenchymal transition, processes that paradoxically contribute to AV fibrosis and mineralization. In addition, macrophages within the AV can differentiate into osteoclast-like cells, suggesting that a bone-like remodeling process occurs in the cardiovascular wall. This high phenotypic plasticity complicates our understanding of CAVD pathogenesis and highlights the need for deeper insight into macrophage functions to design effective preventive and therapeutic strategies. This review summarizes the mechanisms through which different macrophage subsets promote, prevent, or reverse AV remodeling, in both native and bioprosthetic contexts, and explores the therapeutic potential of targeting macrophages or their activity to slow AS progression.

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巨噬细胞作为钙化性主动脉瓣疾病的关键调节剂。

主动脉瓣钙化病（CAVD）是世界范围内最常见的瓣膜性心脏病，主要表现为主动脉瓣（AV）小叶增厚、纤维化和矿化。这种渐进式重塑逐渐损害了瓣膜的开放，阻碍了血液流动。如果不进行干预，由此产生的主动脉狭窄（AS）会导致血流动力学恶化，最终导致心力衰竭和死亡。迄今为止，治疗选择仍然有限，使瓣膜置换术作为参考治疗。虽然瓣膜内皮细胞和间质细胞传统上被认为是房颤重塑的成骨程序的主要驱动因素，但最近的证据强调了巨噬细胞的核心作用，其可塑性深刻影响局部微环境。在炎症状态下，巨噬细胞释放细胞因子，产生氧化应激，分泌骨形态发生蛋白2 (Bone Morphogenetic Protein 2, BMP2)，促进瓣膜细胞的成骨转化。由此产生的钙晶体沉积进一步放大了巨噬细胞驱动的炎症，形成了一个恶性循环。相反，免疫调节巨噬细胞可以通过释放焦磷酸盐（一种钙化抑制剂）来预防CAVD。然而，这些巨噬细胞也分泌促纤维化因子，并可能经历髓质向间质转化，这一过程矛盾地促进了AV纤维化和矿化。此外，AV内的巨噬细胞可分化为破骨细胞样细胞，提示心血管壁发生骨样重塑过程。这种高度的表型可塑性使我们对CAVD发病机制的理解复杂化，并强调需要更深入地了解巨噬细胞的功能，以设计有效的预防和治疗策略。本文综述了不同巨噬细胞亚群在天然和生物假体环境下促进、预防或逆转AV重塑的机制，并探讨了靶向巨噬细胞或其活性减缓AS进展的治疗潜力。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Frontiers in Cardiovascular Medicine Medicine-Cardiology and Cardiovascular Medicine

CiteScore

3.80

自引率

11.10%

发文量

3529

审稿时长

14 weeks

期刊介绍： Frontiers? Which frontiers? Where exactly are the frontiers of cardiovascular medicine? And who should be defining these frontiers? At Frontiers in Cardiovascular Medicine we believe it is worth being curious to foresee and explore beyond the current frontiers. In other words, we would like, through the articles published by our community journal Frontiers in Cardiovascular Medicine, to anticipate the future of cardiovascular medicine, and thus better prevent cardiovascular disorders and improve therapeutic options and outcomes of our patients.