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口服抗原可减轻或加重炎性关节炎动物模型中的病理状况,这取决于给药时间。

Orally administered antigen can reduce or exacerbate pathology in an animal model of inflammatory arthritis dependent upon the timing of administration.

作者信息

Meehan Gavin R, Scales Hannah E, McInnes Iain B, Brewer James M, Garside Paul

机构信息

School of Infection and Immunity, University of Glasgow, Glasgow, UK.

出版信息

Immunother Adv. 2022 Sep 13;2(1):ltac020. doi: 10.1093/immadv/ltac020. eCollection 2022.

Abstract

Currently, treatments for rheumatoid arthritis (RA) are focussed on management of disease symptoms rather than addressing the cause of disease, which could lead to remission and cure. Central to disease development is the induction of autoimmunity through a breach of self-tolerance. Developing approaches to re-establish antigen specific tolerance is therefore an important emerging area of RA research. A crucial step in this research is to employ appropriate animal models to test prospective antigen specific immunotherapies. In this short communication, we evaluate our previously developed model of antigen specific inflammatory arthritis in which ovalbumin-specific T cell receptor transgenic T cells drive breach of tolerance to endogenous antigens to determine the impact that the timing of therapy administration has upon disease progression. Using antigen feeding to induce tolerance we demonstrate that administration prior to articular challenge results in a reduced disease score as evidenced by pathology and serum antibody responses. By contrast, feeding antigen after initiation of disease had the opposite effect and resulted in the exacerbation of pathology. These preliminary data suggest that the timing of antigen administration may be key to the success of tolerogenic immunotherapies. This has important implications for the timing of potential tolerogenic therapies in patients.

摘要

目前,类风湿性关节炎(RA)的治疗主要集中在疾病症状的管理上,而非针对疾病的病因,而病因才是实现缓解和治愈的关键。疾病发展的核心是通过自我耐受的破坏引发自身免疫。因此,开发重新建立抗原特异性耐受的方法是类风湿性关节炎研究中一个重要的新兴领域。这项研究的关键一步是采用合适的动物模型来测试前瞻性的抗原特异性免疫疗法。在这篇简短的通讯中,我们评估了我们之前开发的抗原特异性炎性关节炎模型,其中卵清蛋白特异性T细胞受体转基因T细胞驱动对内源性抗原的耐受破坏,以确定治疗给药时机对疾病进展的影响。通过抗原喂食诱导耐受,我们证明在关节攻击前给药会使疾病评分降低,病理和血清抗体反应均可证明这一点。相比之下,在疾病开始后喂食抗原则产生相反的效果,导致病理加重。这些初步数据表明,抗原给药时机可能是耐受性免疫疗法成功的关键。这对于患者潜在耐受性疗法的给药时机具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f454/9579813/d2b04af86c85/ltac020_fig3.jpg

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