IL1RAP Blockade With a Monoclonal Antibody Reduces Cardiac Inflammation and Preserves Heart Function in Viral and Autoimmune Myocarditis.

IF 7.8 1区 医学 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS
Diego A Lema, Gabriel Jakobsson, Abdel Daoud, David Elias, Monica V Talor, Sara Rattik, Caitríona Grönberg, Hannah Kalinoski, Elin Jaensson Gyllenbäck, Nadan Wang, David Liberg, Alexandru Schiopu, Daniela Čiháková
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引用次数: 0

Abstract

Background: Currently, there are no therapies targeting specific pathogenic pathways in myocarditis. IL (interleukin)-1 blockade has shown promise in preclinical studies and case reports. We hypothesized that blockade of IL1RAP (IL-1 receptor accessory protein), a shared subunit of the IL-1, IL-33, and IL-36 receptors, could be more efficient than IL-1 blockade alone.

Methods: We induced coxsackievirus B3 (CVB3)-mediated or experimental autoimmune myocarditis (EAM) in BALB/c mice, followed by treatment with an Fc (fragment crystallizable)-modified mIgG2a mouse anti-mouse IL1RAP monoclonal antibody (mCAN10). Myocarditis severity and immune infiltration were assessed by histology and flow cytometry. Cardiac function was measured by echocardiography. We used spatial transcriptomics (Visium 10× Genomics) to compare the gene expression landscape in the hearts of mCAN10-treated versus control mice.

Results: IL1RAP blockade reduced CVB3 and EAM severity. In EAM, the treatment prevented deterioration of cardiac function, measured on day 42 post-disease induction (left ventricular ejection fraction: 56.5% versus 51.0% in isotype controls [P=0.002] and versus 51.4% in mice treated with anti-IL-1β antibodies alone [P=0.003]; n=10-11 mice per group). In the CVB3 model, mCAN10 did not impede viral clearance from the heart and significantly lowered the numbers of CD4+ (cluster of differentiation 4) T cells (P=0.025), inflammatory Ly6C+CCR2+ (lymphocyte antigen 6 complex, locus C/C-C motif chemokine receptor 2) monocytes (P=0.038), neutrophils (P=0.001) and eosinophils (P<0.001) infiltrating the myocardium. The spatial transcriptomic analysis revealed reduced canonical IL-1 signaling and chemokine expression in cardiac immune foci in CVB3-infected mice treated with IL1RAP blockade.

Conclusions: Blocking IL1RAP reduces acute CVB3 myocarditis and EAM severity and preserves cardiac function in EAM. We conclude that IL1RAP blockade is a potential therapeutic strategy in viral and autoimmune myocarditis.

用单克隆抗体阻断 IL1RAP 可减轻病毒性和自身免疫性心肌炎的心脏炎症并保护心脏功能
背景:目前,还没有针对心肌炎特定致病途径的疗法。IL(白细胞介素)-1 阻断剂在临床前研究和病例报告中显示出了前景。我们假设,阻断 IL1RAP(IL-1 受体附属蛋白)(IL-1、IL-33 和 IL-36 受体的共享亚基)可能比单独阻断 IL-1 更有效:方法:我们诱导 BALB/c 小鼠患柯萨奇病毒 B3(CVB3)介导的或实验性自身免疫性心肌炎(EAM),然后用 Fc(可结晶片段)修饰的 mIgG2a 小鼠抗小鼠 IL1RAP 单克隆抗体(mCAN10)治疗。心肌炎的严重程度和免疫浸润通过组织学和流式细胞术进行评估。心脏功能通过超声心动图进行测量。我们使用空间转录组学(Visium 10× Genomics)比较了经 mCAN10 处理的小鼠与对照组小鼠心脏的基因表达情况:结果:IL1RAP阻断降低了CVB3和EAM的严重程度。结果:IL1RAP阻断降低了CVB3和EAM的严重程度,在EAM中,治疗防止了心脏功能的恶化(在疾病诱导后第42天测量的左心室射血分数为56.5%,而对照组为51.0%):56.5%对51.0%[P=0.002],对51.4%[P=0.003];每组10-11只小鼠)。在 CVB3 模型中,mCAN10 不会阻碍病毒从心脏清除,并能显著降低 CD4+(分化群 4)T 细胞(P=0.025)、炎性 Ly6C+CCR2+(淋巴细胞抗原 6 复合物,C/C-C 矩阵趋化因子受体 2)单核细胞(P=0.038)、中性粒细胞(P=0.001)和嗜酸性粒细胞(PConclusions:阻断 IL1RAP 可降低急性 CVB3 心肌炎和 EAM 的严重程度,并保护 EAM 的心脏功能。我们得出结论:阻断 IL1RAP 是病毒性和自身免疫性心肌炎的一种潜在治疗策略。
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来源期刊
Circulation: Heart Failure
Circulation: Heart Failure 医学-心血管系统
CiteScore
12.90
自引率
3.10%
发文量
271
审稿时长
6-12 weeks
期刊介绍: Circulation: Heart Failure focuses on content related to heart failure, mechanical circulatory support, and heart transplant science and medicine. It considers studies conducted in humans or analyses of human data, as well as preclinical studies with direct clinical correlation or relevance. While primarily a clinical journal, it may publish novel basic and preclinical studies that significantly advance the field of heart failure.
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