Ageing Affects Thymopoiesis and Experimental Autoimmune Encephalomyelitis Development in a Strain-Dependent Manner.

IF 2.2 4区 医学 Q3 ENDOCRINOLOGY & METABOLISM
Neuroimmunomodulation Pub Date : 2023-01-01 Epub Date: 2023-11-10 DOI:10.1159/000535150
Zorica Stojić-Vukanić, Marija Petrušić, Ivan Pilipović, Gordana Leposavić
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引用次数: 0

Abstract

Introduction: Considering significance of mechanisms of central tolerance for development of autoimmune diseases, including experimental autoimmune encephalomyelitis (EAE), and suppressive influence of circulating proinflammatory cytokines and alterations in brain-thymus communication, characteristic for the central nervous system (CNS) autoimmune diseases, on thymopoiesis, the study interogated putative strain-based thymus-related specificities relevant for the opposite effects of ageing on susceptibility of Dark Agouti (DA) and Albino Oxford (AO) rats to EAE.

Methods: Quantitative and qualitative changes in thymopoiesis including underlying mechanisms were examined using flow cytometry and RT-qPCR quantification of mRNAs for molecules relevant for integrity of stroma and T-cell development, respectively.

Results: With ageing, differently from DA rats, in AO rats the surface density of CD90, a negative regulator of selection threshold, on thymocytes undergoing lineage commitment was upregulated (consistent with TGF-β expression downregulation), whereas the generation of natural CD4+CD25+Foxp3+ regulatory T cells (nTregs) was impaired reflecting differences in thymic expression of cytokines supporting their development. Additionally, specifically in old AO rats, in whom EAE development depends on IL-17-producing CD8+ T cells, their thymic differentiation was augmented, reflecting augmented thymic IL-4 expression. In turn, differently from old DA rats developing self-limiting EAE, in age-matched AO rats developing EAE of prolonged duration, EAE development led to impaired generation of nTregs and accumulation of proinflammatory, cytotoxic CD28-CD4+ T cells in the periphery.

Discussion: The study indicates that strain differences in age-related changes in the efficacy of central tolerance, in addition to enhanced thymic generation of CD8+ T cells prone to differentiate into IL-17-producing cells, could partly explain the opposite effect of ageing on DA and AO rat susceptibility to EAE induction. Additionally, it suggested that EAE development leading to a less efficient thymic output of CD4+ cells and nTregs in old AO rats than their DA counterparts could contribute to prolonged EAE duration in AO compared with DA rats.

Conclusion: The study warns to caution when designing therapeutic interventions to enhance thymic activity in genetically diverse populations, e.g., humans, and interpreting their outcomes. Furthermore, it indicates that CNS autoimmune pathology may additionally worsen thymic involution and age-related immune changes.

衰老以菌株依赖的方式影响胸腺功能和EAE的发展。
作品简介:考虑中枢耐受机制在自身免疫性疾病(包括实验性自身免疫性脑脊髓炎(EAE))发展中的重要性,以及循环促炎细胞因子和脑-胸腺通讯特征改变对中枢神经系统(CNS)自身免疫性疾病的抑制作用,该研究旨在确定基于菌株的胸腺相关特异性,这些特异性可能与衰老对黑鼠(DA)和牛津白化(AO)大鼠对EAE的易感性的相反影响有关。方法:分别使用流式细胞术和RT-qPCR对基质完整性和t细胞发育相关分子的mrna进行定量和定性检测,包括潜在的机制。结果:与DA大鼠不同,随着年龄的增长,AO大鼠胸腺细胞进行谱系承诺的CD90(选择阈值的负调节因子)表面密度上调(与TGF-β表达下调一致),而天然CD4+CD25+Foxp3+ t调节细胞(nTregs)的生成受损,反映了支持其发育的胸腺细胞因子表达的差异。此外,特别是在老年AO大鼠中,EAE的发展依赖于产生il -17的CD8+ T细胞,它们的胸腺分化增强,反映了胸腺IL-4表达增强。反过来,与发生自限性EAE的老年DA大鼠不同,在发生EAE的年龄匹配的AO大鼠中,EAE的发展导致外周nTregs的产生和促炎、细胞毒性CD28-CD4+ T细胞的积累受损。讨论:研究表明,除了胸腺中CD8+ T细胞易于分化为产生il -17的细胞外,与年龄相关的中枢耐受性变化的品系差异可以部分解释衰老对DA和AO大鼠对EAE诱导的易感性的相反影响。此外,这表明EAE的发展导致老年AO大鼠的CD4+细胞和ntreg的胸腺输出效率低于DA大鼠,这可能导致AO大鼠的EAE持续时间比DA大鼠长。结论:该研究警告说,在设计治疗干预措施以增强遗传多样性人群(如人类)的胸腺活动时要谨慎,并解释其结果。此外,这表明中枢神经系统自身免疫病理可能会加重胸腺退化和年龄相关的免疫变化。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Neuroimmunomodulation
Neuroimmunomodulation 医学-免疫学
CiteScore
3.60
自引率
4.20%
发文量
35
审稿时长
>12 weeks
期刊介绍: The rapidly expanding area of research known as neuroimmunomodulation explores the way in which the nervous system interacts with the immune system via neural, hormonal, and paracrine actions. Encompassing both basic and clinical research, ''Neuroimmunomodulation'' reports on all aspects of these interactions. Basic investigations consider all neural and humoral networks from molecular genetics through cell regulation to integrative systems of the body. The journal also aims to clarify the basic mechanisms involved in the pathogenesis of the CNS pathology in AIDS patients and in various neurodegenerative diseases. Although primarily devoted to research articles, timely reviews are published on a regular basis.
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