Laboratorio de Farmacología Molecular, Department of Pharmaceutical and Toxicological Chemistry, Faculty of Chemical Sciences and Pharmacy, Universidad de Chile, Santiago, Chile; Department of Pharmacology, Faculty of Medicine, Universidad Autónoma de Madrid, Madrid, Spain; Ph.D. Programme in Pharmacology and Physiology, Doctoral School, Universidad Autónoma de Madrid, Madrid, Spain; Advanced Center for Chronic diseases (ACCDiS), Faculty of Chemical Sciences and Pharmacy, Universidad de Chile, Santiago, Chile.
Department of Pharmacology, Faculty of Medicine, Universidad Autónoma de Madrid, Madrid, Spain; Ph.D. Programme in Pharmacology and Physiology, Doctoral School, Universidad Autónoma de Madrid, Madrid, Spain; Instituto de Investigaciones Sanitarias (IdiPAZ), Madrid, Spain.
Biochim Biophys Acta Mol Basis Dis. 2022 Nov 1;1868(11):166525. doi: 10.1016/j.bbadis.2022.166525. Epub 2022 Aug 18.
Cardiac fibroblasts (CFs) undergo senescence in reaction to different stressors, leading to a poor prognosis of cardiac disease. Doxorubicin (Doxo) is an antineoplastic drug with strong cardiotoxic effects, which induces IL-1β secretion and thus, triggers a potent pro-inflammatory response. Doxo induces CFs senescence; however, the mechanisms are not fully understood. Different pharmacological strategies have been used to eliminate senescent cells by inducing their apoptosis or modifying their secretome. However, Resolvin E1 (RvE1), a lipid derivative resolutive mediator with potent anti-inflammatory effects has not been used before to prevent CFs senescence. CFs were isolated from adult male C57BL/6J mice and subsequently stimulated with Doxo, in the presence or absence of RvE1. Senescence-associated β-galactosidase activity (SA-β-gal), γ-H2A.X, p53, p21, and senescence-associated secretory phenotype (SASP) were evaluated. The involvement of the NLRP3 inflammasome/interleukin-1 receptor (IL-1R) signaling pathway on CFs senescence was studied using an NLRP3 inhibitor (MCC950) and an endogenous IL-1R antagonist (IR1A). Doxo is able to trigger CFs senescence, as evidenced by an increase of γ-H2A.X, p53, p21, and SA-β-gal, and changes in the SASP profile. These Doxo effects were prevented by RvE1. Doxo triggers IL-1β secretion, which was dependent on NLRP3 activation. Doxo-induced CFs senescence was partially blocked by MCC950 and IR1A. In addition, IL-1β also triggered CFs senescence, as evidenced by the increase of γ-H2A.X, p53, p21, SA-β-gal activity, and SASP. All these effects were also prevented by RvE1 treatment. CONCLUSION: These data show the anti-senescent role of RvE1 in Doxo-induced CFs senescence, which could be mediated by reducing IL-1β secretion.
心肌成纤维细胞(CFs)在应对不同应激源时会发生衰老,导致心脏疾病预后不良。多柔比星(Doxo)是一种具有强烈心脏毒性的抗肿瘤药物,可诱导 IL-1β 分泌,从而引发强烈的促炎反应。多柔比星诱导 CFs 衰老;然而,其机制尚不完全清楚。已经使用了不同的药理学策略来通过诱导细胞凋亡或修饰其分泌组来消除衰老细胞。然而,具有强大抗炎作用的脂质衍生分辨介质 Resolvin E1(RvE1)以前尚未用于预防 CFs 衰老。从成年雄性 C57BL/6J 小鼠中分离出 CFs,然后用 Doxo 刺激,存在或不存在 RvE1 的情况下。评估衰老相关β-半乳糖苷酶活性(SA-β-gal)、γ-H2A.X、p53、p21 和衰老相关分泌表型(SASP)。使用 NLRP3 抑制剂(MCC950)和内源性 IL-1R 拮抗剂(IR1A)研究 NLRP3 炎性体/白细胞介素-1 受体(IL-1R)信号通路对 CFs 衰老的影响。Doxo 能够触发 CFs 衰老,这表现为 γ-H2A.X、p53、p21 和 SA-β-gal 的增加以及 SASP 谱的变化。这些 Doxo 作用被 RvE1 阻止。Doxo 触发 IL-1β 的分泌,这依赖于 NLRP3 的激活。MCC950 和 IR1A 部分阻断了 Doxo 诱导的 CFs 衰老。此外,IL-1β 也引发了 CFs 衰老,这表现为 γ-H2A.X、p53、p21、SA-β-gal 活性和 SASP 的增加。所有这些作用也被 RvE1 处理所阻止。结论:这些数据显示 RvE1 在 Doxo 诱导的 CFs 衰老中的抗衰老作用,这可能是通过减少 IL-1β 分泌来介导的。
