Interleukin-12p40 deficiency attenuates myocardial ferroptosis in doxorubicin-induced chronic cardiomyopathy by inhibiting Th17 differentiation and interleukin-17A production.

IF 10.2 1区医学 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS

Cardiovascular Research Pub Date : 2024-09-19 DOI:10.1093/cvr/cvae208

Jishou Zhang,Wen Ding,Zheng Yin,Siqi Liu,Mengmeng Zhao,Yao Xu,Jianfang Liu,Wei Pan,Shanshan Peng,Cheng Wei,Zihui Zheng,Juan-Juan Qin,Jun Wan,Menglong Wang

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引用次数: 0

Abstract

AIMS Interleukin (IL)-12p40 is a common subunit of the bioactive cytokines IL-12 and IL-23, and it also has its own intrinsic functional activity. However, its role in doxorubicin-induced chronic cardiomyopathy (DICCM) as well as the underlying mechanisms are still unknown. METHODS AND RESULTS In this study, we used IL-12p40-knockout mice, IL-23p19-knockout mice, Rag1-knockout mice, a ferroptosis inhibitor, recombinant IL-12 (rIL-12), rIL-23, rIL-12p40, rIL-12p80, and anti-IL17A to investigate the effects of IL-12p40 on DICCM and elucidate the underlying mechanisms. We found that myocardial ferroptosis were increased in DICCM and that the inhibition of ferroptosis protected against DICCM. The expression of IL-12p40 was upregulated, and IL-12p40 was predominantly expressed by CD4+ T cells in the hearts of mice with DICCM. IL-12p40 knockout attenuated cardiac dysfunction, fibrosis and ferroptosis in DICCM, and similar results were observed in the context of CD4+ T cell IL-12p40 deficiency in Rag1-/- mice. Treatment with rIL-23, but not rIL-12, rIL-12p40 monomer or rIL-12p80, abolished the protective effects of IL-12p40 knockout. Moreover, rIL-23 treatment and IL-23p19 knockout exacerbated and ameliorated DICCM, respectively. IL-12p40 knockout might protect against DICCM by inhibiting Th17 differentiation and IL-17A production but not Th1, Th2 and Treg differentiation. Neutralizing IL-17A with an antibody also attenuated cardiac dysfunction, fibrosis and ferroptosis. The IL-12p40/Th17/IL-17A axis might promote cardiomyocyte ferroptosis by activating TNF receptor-associated factor 6 (TRAF6)/mitogen-activated protein kinase (MAPK)/P53 signaling in DICCM. CONCLUSIONS Interleukin-12p40 deficiency protects against DICCM by inhibiting Th17 differentiation and the production of IL-17A, which plays critical roles in cardiomyocyte ferroptosis in DICCM via activating TRAF6/MAPK/P53 signaling. Our study may provide novel insights for the identification of therapeutic targets for treating DICCM in the clinic.

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白细胞介素-12p40的缺乏可通过抑制Th17分化和白细胞介素-17A的产生，减轻多柔比星诱发的慢性心肌病的心肌铁变态反应。

目的白细胞介素（IL）-12p40是生物活性细胞因子IL-12和IL-23的共同亚基，同时也具有自身固有的功能活性。然而，它在多柔比星诱导的慢性心肌病（DICCM）中的作用及其内在机制尚不清楚。方法和结果在本研究中，我们利用 IL-12p40 基因敲除小鼠、IL-23p19 基因敲除小鼠、Rag1 基因敲除小鼠、铁突变抑制剂、重组 IL-12 (rIL-12)、rIL-23、rIL-12p40、rIL-12p80 和抗 IL17A 来研究 IL-12p40 对 DICCM 的影响并阐明其潜在机制。我们发现，在 DICCM 中心肌铁蛋白沉积增加，而抑制铁蛋白沉积可防止 DICCM 的发生。在 DICCM 小鼠的心脏中，IL-12p40 的表达上调，并且 IL-12p40 主要由 CD4+ T 细胞表达。IL-12p40基因敲除减轻了DICCM的心脏功能障碍、纤维化和铁蛋白沉着，在Rag1-/-小鼠CD4+ T细胞IL-12p40缺乏的情况下也观察到了类似的结果。使用 rIL-23 而非 rIL-12、rIL-12p40 单体或 rIL-12p80 治疗可消除 IL-12p40 基因敲除的保护作用。此外，rIL-23 处理和 IL-23p19 基因敲除分别加剧和改善了 DICCM。IL-12p40基因敲除可能通过抑制Th17分化和IL-17A的产生，而不是Th1、Th2和Treg分化来保护DICCM。用抗体中和 IL-17A 还能减轻心脏功能障碍、纤维化和铁质沉着。在 DICCM 中，IL-12p40/Th17/IL-17A 轴可能会通过激活 TNF 受体相关因子 6（TRAF6）/丝裂原活化蛋白激酶（MAPK）/P53 信号转导来促进心肌细胞铁变态反应。IL-17A通过激活TRAF6/MAPK/P53信号在DICCM的心肌细胞铁凋亡中发挥关键作用。我们的研究可能会为临床上确定治疗 DICCM 的靶点提供新的见解。

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来源期刊

Cardiovascular Research 医学-心血管系统

CiteScore

21.50

自引率

3.70%

发文量

547

审稿时长

1 months

期刊介绍： Cardiovascular Research Journal Overview: International journal of the European Society of Cardiology Focuses on basic and translational research in cardiology and cardiovascular biology Aims to enhance insight into cardiovascular disease mechanisms and innovation prospects Submission Criteria: Welcomes papers covering molecular, sub-cellular, cellular, organ, and organism levels Accepts clinical proof-of-concept and translational studies Manuscripts expected to provide significant contribution to cardiovascular biology and diseases