白鸟 (2024-02-29 22:33):
#paper Double-Negative T (DNT) Cells in Patients with Systemic Lupus Erythematosus doi:10.3390/biomedicines12010166 这篇小型综述收集和总结SLE患者DNT细胞群基础研究的初步证据,分析最相关的临床研究,DNT细胞在SLE免疫发病机制中的作用。 1.SLE疾病概述; 2.临床表现:存在大量且多变的自身抗体产生有关,抗dsDNA抗体,导致免疫介导的器官损伤; 3.主要的免疫致病机制:胞吞作用缺陷(即自身抗原的清除减少,补体因子)、细胞凋亡缺陷(这也会导致B细胞自我耐受性的丧失), I 型干扰素的不适当激活等,原因复杂; 4.SLE 患者中DNT细胞百分比会增加,尤其是活动期的患者; 5.双阴性T (DNT) 细胞是一群罕见的T淋巴细胞亚群,不表达CD4和CD8,但表达 αβ 或 γδ T细胞受体 (TCR)。 6.DNT的产生:分胸腺依赖型(负选择逃逸)和胸腺非依赖型(可能来自活化的外周淋巴细胞,在特定情况下失去CD4或CD8标记物的表达),确切的个体发育过程尚未完全阐明。 7.人SLE与其他自免疾病比较,动物模型狼疮鼠结果比较,目前缺系统论证,实验证据比较分散: 证据1: DNT细胞可能源自自身反应性CD8+T细胞,特别是自身免疫疾病。 实验模型证据:DNT细胞可以表现出炎症和免疫调节(抗炎或抑制)功能。
IF:3.900Q1 Biomedicines, 2024-Jan-12. DOI: 10.3390/biomedicines12010166 PMID: 38255272
Double-Negative T (DNT) Cells in Patients with Systemic Lupus Erythematosus
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Abstract:
Double-negative T (DNT) cells are a rare and unconventional T-lymphocyte subpopulation lacking both CD4 and CD8 markers. Their immunopathological roles and clinical relevance have yet to be elucidated. Beyond autoimmune lymphoproliferative syndrome (ALPS), these cells may also play a role in rheumatic disorders, including systemic lupus erythematosus (SLE); indeed, these two diseases share several autoimmune manifestations (including nephritis). Moreover, one of the main experimental murine models used to investigate lupus, namely the MRL/lpr mouse, is characterized by an expansion of DNT cells, which can support the production of pathogenic autoantibodies and/or modulate the immune response in this context. However, lupus murine models are not completely consistent with their human SLE counterpart, of course. In this mini review, we summarize and analyze the most relevant clinical studies investigating the DNT cell population in SLE patients. Overall, based on the present literature review and analysis, DNT cell homeostasis seems to be altered in patients with SLE. Indeed, most of the available clinical studies (which include both adults and children) reported an increased DNT cell percentage in SLE patients, especially during the active phases, even though no clear correlation with disease activity and/or inflammatory parameters has been clearly established. Well-designed, standardized, and longitudinal clinical studies focused on DNT cell population are needed, in order to further elucidate the actual contribution of these cells in SLE pathogenesis and their interactions with other immune cells (also implicated and/or altered in SLE, such as basophils), and clarify whether their expansion and/or immunophenotypic aspects may have any immunopathological relevance (and, then, represent potential disease markers and, in perspective, even therapeutic targets) or are just an unspecific epiphenomenon of autoimmunity.
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