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

被引：5

作者：

Zhang, Jishou ^{[1
,2
,3
,4
]}

Ding, Wen ^{[1
,5
]}

Yin, Zheng ^{[1
,3
,4
]}

Liu, Siqi ^{[1
,3
,4
]}

Zhao, Mengmeng ^{[1
,3
,4
]}

Xu, Yao ^{[1
,3
,4
]}

Liu, Jianfang ^{[1
,3
,4
]}

Pan, Wei ^{[1
,3
,4
]}

Peng, Shanshan ^{[1
,3
,4
]}

Wei, Cheng ^{[1
,3
,4
]}

Zheng, Zihui ^{[1
,3
,4
]}

Qin, Juan-Juan ^{[1
,6
,7
]}

Wan, Jun ^{[1
,3
,4
]}

Wang, Menglong ^{[1
,3
,4
]}

机构：

[1] Wuhan Univ, Renmin Hosp, Dept Cardiol, 238 Jiefang Rd, Wuhan 430060, Peoples R China

[2] Zhejiang Univ, Affiliated Hosp 1, Sch Med, Dept Cardiol, Hangzhou, Peoples R China

[3] Wuhan Univ, Cardiovasc Res Inst, Wuhan, Peoples R China

[4] Hubei Key Lab Cardiol, Wuhan, Peoples R China

[5] Zhejiang Univ, Affiliated Hosp 1, Sch Med, Dept Radiol, Wuhan, Peoples R China

[6] Wuhan Univ, Zhongnan Hosp, Dept Geriatr, 169 Donghu Rd, Wuhan, Peoples R China

[7] Wuhan Univ, Ctr Hlth Aging, Sch Nursing, Wuhan, Peoples R China

来源：

CARDIOVASCULAR RESEARCH | 2024年 / 120卷 / 16期

基金：

中国国家自然科学基金;

关键词：

Interleukin; 12-p40; Doxorubicin-induced cardiotoxicity; Ferroptosis; Inflammation; Adaptive immunity; T lymphocyte differentiation; IL-12; P40; MONOMER; P53; INFLAMMATION; ACTIVATION; APOPTOSIS; CYTOKINE; MICE; NEUTRALIZATION; DYSFUNCTION; CELLS;

D O I：

10.1093/cvr/cvae208

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

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 signalling in DICCM.Conclusion 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 signalling. Our study may provide novel insights for the identification of therapeutic targets for treating DICCM in the clinic. Graphical Abstract

引用

页码：2117 / 2133

页数：17

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