心肌纤维化的治疗靶点：当前和新兴方法的综合综述。

Cardiovascular & hematological disorders drug targets Pub Date : 2025-09-02 DOI:10.2174/011871529X365096250827101044

Ankita Wal, Anurag Rawat, Rakesh Verma, Azhar Rasheed, Uttam Prasad Panigrahy, Anwesha Das, Amin Gasmi

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摘要

导读：心血管疾病（cvd）仍然是全球死亡的主要原因，超过其他慢性疾病。与心血管疾病相关的死亡人数，特别是在年轻人群中出现了惊人的上升，这加强了研究工作，以更好地了解该疾病及其并发症。其中，心肌纤维化在心功能障碍和心力衰竭的发展中起着核心作用。鉴于其多因素的性质，需要不同的治疗策略来有效地控制其进展。方法：使用PubMed、Scopus、Elsevier和ClinicalTrials.gov等数据库进行全面的文献综述。仅包括同行评议的、专注于心肌纤维化分子机制和治疗策略的英语研究。不相关、非英语和非同行评议的资料被排除在外。从选定的临床前和临床研究的数据进行定性综合。结果：心肌纤维化是由多种病理条件引起的，包括缺血、高脂血症和遗传疾病，这些病理条件促进了心脏重构的不适应。尽管RAAS抑制剂和β受体阻滞剂等传统治疗方法可以缓解症状，但它们并不能阻止疾病的进展。最近的证据表明，多种分子途径参与纤维化的发展，为探索替代治疗靶点提供了机会。讨论：由于其复杂的病理生理，心肌纤维化不能单药治疗。抗tgf -β药物与SGLT2抑制剂和MMP抑制剂等新疗法一起成为有希望的候选药物。此外，再生方法，如干细胞和基因治疗，提供了未来的途径，尽管技术和安全挑战伴随着它们。结论：心肌纤维化仍然是心力衰竭的关键因素，目前的治疗方法不足以逆转其进程。针对不同分子机制的多方面治疗方法是改善临床结果的关键。持续的转化研究对于将新兴疗法从实验室推向临床至关重要。

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Therapeutic Targets for Myocardial Fibrosis: A Comprehensive Review of Current and Emerging Approaches.

Introduction: Cardiovascular disorders (CVDs) remain the leading cause of global mortality, surpassing other chronic illnesses. An alarming rise in CVD-related deaths, particularly among younger populations, has intensified research efforts to better understand the disease and its complications. Among these, myocardial fibrosis plays a central role in the development of cardiac dysfunction and heart failure. Given its multifactorial nature, diverse therapeutic strategies are required to manage its progression effectively.

Methods: A comprehensive literature review was conducted using databases such as PubMed, Scopus, Elsevier, and ClinicalTrials.gov. Only peer-reviewed, English-language studies focusing on molecular mechanisms and therapeutic strategies for myocardial fibrosis were included. Irrelevant, non-English, and non-peer-reviewed sources were excluded. Data from selected preclinical and clinical investigations were qualitatively synthesized.

Results: Myocardial fibrosis arises from various pathological conditions, including ischemia, hyperlipidemia, and genetic disorders, which promote maladaptive cardiac remodeling. Although traditional treatments such as RAAS inhibitors and β-blockers offer symptomatic relief, they do not halt disease progression. Recent evidence suggests that multiple molecular pathways are involved in the development of fibrosis, opening opportunities to explore alternative therapeutic targets.

Discussion: Due to its complex pathophysiology, myocardial fibrosis cannot be addressed by monotherapy alone. Anti-TGF-β agents have emerged as promising candidates, alongside newer therapies like SGLT2 inhibitors and MMP inhibitors. Additionally, regenerative approaches, such as stem cell and gene therapy, offer future avenues, though technical and safety challenges accompany them.

Conclusion: Myocardial fibrosis remains a critical contributor to heart failure, and current treatments are insufficient to reverse its course. A multifaceted therapeutic approach targeting different molecular mechanisms holds the key to improved clinical outcomes. Continued translational research is crucial for advancing emerging therapies from bench to bedside.

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Cardiovascular & hematological disorders drug targets

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