Macrophage-derived VEGF-C reduces cardiac inflammation and prevents heart dysfunction in CVB3-induced viral myocarditis via remodeling cardiac lymphatic vessels

IF 4.8 2区医学 Q2 IMMUNOLOGY

International immunopharmacology Pub Date : 2024-10-14 DOI:10.1016/j.intimp.2024.113377

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引用次数: 0

Abstract

Background

Cardiac lymphatic vessels are important channels for cardiac fluid circulation and immune regulation. In myocardial infarction and chronic heart failure, promoting cardiac lymphangiogenesis is beneficial in reducing cardiac edema and inflammation. However, the specific involvement of cardiac lymphangiogenesis in viral myocarditis (VMC) has not been studied. Despite the recognized participation of macrophages in lymphangiogenesis, the contribution of macrophages to cardiac lymphangiogenesis in VMC is still unclear.

Methods

The male Balb/c mice with VMC were grouped according to the time to explore changes in inflammation, cardiac function and lymphangiogenesis. Adeno-associated virus (AAV) was used to determine the effect of cardiac lymphangiogenesis in VMC. Macrophage depletion and VEGF-C_C156S treatment were used to investigate the connection between macrophages and cardiac lymphangiogenesis.

Results

Cardiac inflammation and lymphatic vessel density were both upregulated, peaking on day 7 following CVB3 infection. After treatment with AAV-sVEGFR3, lymphangiogenesis was inhibited, leading to worsened cardiac dysfunction and aggravated inflammation. However, these effects were reversed by AAV-VEGF-C treatment. Furthermore, macrophages infiltrated the inflamed myocardium and secreted VEGF-C. In vitro, VEGF-C was upregulated when RAW264.7 cells were co-cultured with CVB3. Macrophage depletion in mice with VMC inhibited lymphangiogenesis, while supplementation with VEGF-C_C156S depressed it.

Conclusion

Collectively, these results indicate that activation of the VEGF-C/VEGFR3 axis exerts a protective effect in CVB3-induced VMC by resolving inflammation and alleviating cardiac dysfunction through increased lymphatic vasculature density, with macrophage-derived VEGF-C partially contributing to this effect.

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巨噬细胞源性 VEGF-C 通过重塑心脏淋巴管减轻 CVB3 病毒性心肌炎的心脏炎症并预防心脏功能障碍

背景心脏淋巴管是心脏体液循环和免疫调节的重要通道。在心肌梗死和慢性心力衰竭中，促进心脏淋巴管生成有利于减轻心脏水肿和炎症。然而，关于病毒性心肌炎（VMC）中心脏淋巴管生成的具体参与情况还没有研究。方法将患有病毒性心肌炎的雄性 Balb/c 小鼠按时间分组，探讨炎症、心脏功能和淋巴管生成的变化。使用腺相关病毒（AAV）测定 VMC 中心脏淋巴管生成的影响。结果心脏炎症和淋巴管密度均上调，在感染 CVB3 后第 7 天达到高峰。用 AAV-sVEGFR3 治疗后，淋巴管生成受到抑制，导致心脏功能障碍恶化和炎症加重。然而，AAV-VEGF-C 治疗可逆转这些影响。此外，巨噬细胞渗入发炎的心肌并分泌 VEGF-C。在体外，当 RAW264.7 细胞与 CVB3 共同培养时，VEGF-C 会上调。总之，这些结果表明，VEGF-C/VEGFR3 轴的激活对 CVB3 诱导的 VMC 有保护作用，它通过增加淋巴管密度来消除炎症和缓解心脏功能障碍，巨噬细胞衍生的 VEGF-C 在一定程度上促进了这一作用。

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

International immunopharmacology 医学-免疫学

CiteScore

8.40

自引率

3.60%

发文量

935

审稿时长

53 days

期刊介绍： International Immunopharmacology is the primary vehicle for the publication of original research papers pertinent to the overlapping areas of immunology, pharmacology, cytokine biology, immunotherapy, immunopathology and immunotoxicology. Review articles that encompass these subjects are also welcome. The subject material appropriate for submission includes: • Clinical studies employing immunotherapy of any type including the use of: bacterial and chemical agents; thymic hormones, interferon, lymphokines, etc., in transplantation and diseases such as cancer, immunodeficiency, chronic infection and allergic, inflammatory or autoimmune disorders. • Studies on the mechanisms of action of these agents for specific parameters of immune competence as well as the overall clinical state. • Pre-clinical animal studies and in vitro studies on mechanisms of action with immunopotentiators, immunomodulators, immunoadjuvants and other pharmacological agents active on cells participating in immune or allergic responses. • Pharmacological compounds, microbial products and toxicological agents that affect the lymphoid system, and their mechanisms of action. • Agents that activate genes or modify transcription and translation within the immune response. • Substances activated, generated, or released through immunologic or related pathways that are pharmacologically active. • Production, function and regulation of cytokines and their receptors. • Classical pharmacological studies on the effects of chemokines and bioactive factors released during immunological reactions.