TNF-α 抑制剂改善人源化小鼠的免疫相关性关节炎和肺炎。
TNF-α inhibitor ameliorates immune-related arthritis and pneumonitis in humanized mice.
机构信息
Department of Clinical Immunology, National Translational Science Center for Molecular Medicine & Department of Cell Biology, PLA Specialized Research Institute of Rheumatoid & Immunology, Xijing Hospital, The Fourth Military Medical University, Xi'an, China.
National Center for International Research of Bio-targeting Theranostics, Guangxi Key Laboratory of Bio-targeting Theranostics, Collaborative Innovation Center for Targeting Tumor Diagnosis and Therapy, Guangxi Talent Highland of Bio-targeting Theranostics, Guangxi Medical University, Nanning, China.
出版信息
Front Immunol. 2022 Aug 9;13:955812. doi: 10.3389/fimmu.2022.955812. eCollection 2022.
OBJECTIVES
This study aimed at establishing a mouse model of immune-related adverse in humanized BALB/c-hPD1/hCTLA4 mice to investigate their potential pathogenesis and explore therapeutic targets for immune-related arthritis and pneumonitis.
METHODS
Humanized BALB/c-hPD1/hCTLA4 mice were injected with vehicle or collagen-specific antibodies (CA) and immune checkpoint inhibitors (ICI, ipilimumab, anti-human CTLA-4; and nivolumab, anti-human PD-1), and some mice were treated with anti-TNF-α antibody, leading to the control, collagen antibody-induced arthritis (CAIA), CAIA+ICI and treatment groups. The severity of clinical arthritis and pneumonitis in mice was monitored longitudinally and the pathological changes in the joints and lungs were histologically analyzed and the contents of lung hydroxyproline were measured. The frequency of different subsets of T cells was analyzed by flow cytometry and multiplex immunofluorescency.
RESULTS
Compared with the control, the ICI group of mice developed the delayed onset of moderate degrees of arthritis while the CAIA+ICI group of mice exhibited the early onset of severe arthritis. Treatment with ICI caused severe pneumonitis, especially in the mice with CA. Flow cytometry analysis indicated a significantly higher frequency of splenic TNF-αCD4 and TNF-αCD8 T cells, but not other subsets of T cells tested, in the CAIA+ICI group of mice, relative to that in other groups of mice. Treatment with anti-TNF-α significantly mitigated the severity of arthritis and pneumonitis as well as deposition of collagen in lung of mice. The treatment also decreased the frequency of TNF-αCD4 and TNF-αCD8 T cells as well as effector memory T cells in the periphery lymph orangs and lungs of mice.
CONCLUSIONS
We successfully established a humanized mouse model of ICI-related severe arthritis and pneumonitis with a higher frequency of TNF-α T cells, which were significantly mitigated by anti-TNF-α treatment. Conceptually, ICI treatment can induce multiple autoimmune-like diseases in autoimmune-prone individuals and TNF-α T cells may be therapeutic targets for intervention of immune-related arthritis and pneumonitis.
目的
本研究旨在建立人源化 BALB/c-hPD1/hCTLA4 小鼠的免疫相关性不良反应模型,以探讨其潜在发病机制,并为免疫相关性关节炎和间质性肺炎探索治疗靶点。
方法
向人源化 BALB/c-hPD1/hCTLA4 小鼠注射载体或胶原特异性抗体(CA)和免疫检查点抑制剂(ICI,伊匹单抗,抗人 CTLA-4;纳武单抗,抗人 PD-1),部分小鼠接受抗 TNF-α 抗体治疗,由此分为对照组、胶原抗体诱导性关节炎(CAIA)组、CAIA+ICI 组和治疗组。纵向监测小鼠的临床关节炎和间质性肺炎严重程度,对关节和肺的组织病理学变化进行分析,并测量肺羟脯氨酸含量。通过流式细胞术和多重免疫荧光分析 T 细胞不同亚群的频率。
结果
与对照组相比,ICI 组小鼠出现迟发性中度关节炎,而 CAIA+ICI 组小鼠出现早发性严重关节炎。ICI 治疗引起严重的间质性肺炎,特别是在有 CA 的小鼠中。流式细胞术分析表明,与其他组小鼠相比,CAIA+ICI 组小鼠脾脏 TNF-αCD4 和 TNF-αCD8 T 细胞频率显著升高,而其他测试的 T 细胞亚群无明显差异。抗 TNF-α 治疗显著减轻了关节炎和间质性肺炎的严重程度以及肺胶原沉积。治疗还降低了外周淋巴结和肺中 TNF-αCD4 和 TNF-αCD8 T 细胞以及效应记忆 T 细胞的频率。
结论
我们成功建立了一种人源化小鼠模型,其具有 ICI 相关严重关节炎和间质性肺炎,且 TNF-α T 细胞频率较高,抗 TNF-α 治疗可显著缓解。从概念上讲,ICI 治疗可在自身免疫倾向个体中诱导多种自身免疫样疾病,TNF-α T 细胞可能是干预免疫相关性关节炎和间质性肺炎的治疗靶点。
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