免疫检查点抑制剂通过MerTK切割，通过抑制巨噬细胞的efferocytic诱导心脏损伤

IF 4.7 2区医学 Q2 IMMUNOLOGY

International immunopharmacology Pub Date : 2025-02-11 DOI:10.1016/j.intimp.2025.114263

Yu Zhang , Zhenzhu Cao , Huihui Jia , Yuting Feng , Xuan Sun , Han Wu , Biao Xu , Zhonghai Wei

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引用次数: 0

摘要

癌症免疫疗法是一种行之有效的治疗各种类型癌症的方法。然而，其临床应用通常受到心血管不良事件的限制。免疫检查点抑制剂（ICIs）可诱导多种形式的心脏毒性，心肌炎是最致命的并发症。其发生的潜在机制仍然难以捉摸。因此，本研究旨在阐明程序性死亡-1 （PD-1）抑制剂对小鼠心肌炎发展的影响。骨髓上皮-生殖酪氨酸激酶（MerTK）受体位于巨噬细胞表面，在吞噬调节中起关键作用。我们通过给6周龄正常雄性BALB/c小鼠注射PD-1抑制剂和心肌肌钙蛋白I肽片段，建立小鼠自身免疫性心肌炎模型，导致小鼠血清可溶性MerTK （SolMer）水平升高，MerTK- cd68双阳性巨噬细胞数量减少，并伴有心脏损伤。在体外，PD-1抑制剂通过MKK3/P38 MAPK通路，促进分解素和金属蛋白酶17 （ADAM17）介导的MerTK脱落，形成SolMer，导致巨噬细胞表面MerTK表达下调。这导致了胞浆功能的抑制和组织修复功能的损害，最终导致了心肌炎的发展。TAPI-0抑制ADAM17的活性，SB203580抑制P38 MAPK的磷酸化。两种抑制剂都有效地恢复了PD-1抑制剂诱导的efferocytosis的抑制作用。在体外，敲除RAW264.7巨噬细胞表面的PD-1受体，然后用PD-1抑制剂刺激该通路，未引起进一步的显著改变。综上所述，PD-1抑制剂通过与巨噬细胞表面的PD-1受体结合，激活MKK3/P38 MAPK/ADAM17通路，诱导巨噬细胞中MerTK的脱落，导致efferocytosis受损。阐明这一分子机制有望改善癌症患者的预后和治疗策略。

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Immune checkpoint inhibitor induces cardiac injury by impairing efferocytosis of macrophages via MerTK cleavage

Cancer immunotherapy is a well-established therapeutic approach for various types of cancer. However, its clinical utility is usually limited by cardiovascular adverse events. Immune Checkpoint Inhibitors (ICIs) can induce diverse forms of cardiotoxicity, with myocarditis being the most fatal complication. The underlying mechanism of its occurrence remains elusive. Therefore, this study aims to elucidate the impact of programmed death-1 (PD-1) inhibitor on myocarditis development in mice. Myeloid-epithelial-reproductive tyrosine kinase (MerTK) receptors, located on the surface of macrophages, play a pivotal role in phagocytic regulation. We established a mouse model of autoimmune myocarditis by injecting 6-week-old normal male BALB/c mice with PD-1 inhibitor and cardiac troponin I peptide fragments, which resulted in elevated levels of serum soluble MerTK (SolMer) and reduced numbers of MerTK-CD68 double-positive macrophages, accompanied by cardiac injury in mice. In vitro, PD-1 inhibitor promotes a disintegrin and metalloproteinase17 (ADAM17)-mediated shed of the MerTK, forming SolMer, through MKK3/P38 MAPK pathway, leading to downregulation of MerTK expression on the macrophage surface. This results in the inhibition of efferocytosis and impairment of tissue repair function, ultimately contributing to myocarditis development. TAPI-0 inhibited the activity of ADAM17, while SB203580 inhibited the phosphorylation of P38 MAPK. Both inhibitors effectively restored the inhibition of efferocytosis induced by the PD-1 inhibitor. In vitro, when the PD-1 receptor on the surface of RAW264.7 macrophages was knocked down and then stimulated with a PD-1 inhibitor, no further significant alterations in the pathway were elicited. In conclusion, the PD-1 inhibitor induces the shedding of MerTK in macrophages by binding to the PD-1 receptor on the surface of macrophages and activating the MKK3/P38 MAPK/ADAM17 pathway, leading to impaired efferocytosis. Elucidation of this molecular mechanism holds promise for improved prognosis and therapeutic strategies in cancer patients.

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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.