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CD4 T cell differentiation in type 1 diabetes

机译:1型糖尿病的CD4 T细胞分化

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Susceptibility to type 1 diabetes is associated strongly with human leucocyte antigen (HLA) genes, implicating T cells in disease pathogenesis. In humans, CD8 T cells predominantly infiltrate the islets, yet their activation and propagation probably requires CD4 T cell help. CD4 T cells can select from several differentiation fates following activation, and this choice has profound consequences for their subsequent cytokine production and migratory potential. In turn, these features dictate which other immune cell types T cells interact with and influence, thereby determining downstream effector functions. Obtaining an accurate picture of the type of CD4 T cell differentiation associated with a particular immune-mediated disease therefore constitutes an important clue when planning intervention strategies. Early models of T cell differentiation focused on the dichotomy between T helper type 1 (Th1) and Th2 responses, with type 1 diabetes (T1D) being viewed mainly as a Th1-mediated pathology. However, several additional fate choices have emerged in recent years, including Th17 cells and follicular helper T cells. Here we revisit the issue of T cell differentiation in autoimmune diabetes, highlighting new evidence from both mouse models and patient samples. We assess the strengths and the weaknesses of the Th1 paradigm, review the data on interleukin (IL)-17 production in type 1 diabetes and discuss emerging evidence for the roles of IL-21 and follicular helper T cells in this disease setting. A better understanding of the phenotype of CD4 T cells in T1D will undoubtedly inform biomarker development, improve patient stratification and potentially reveal new targets for therapeutic intervention.
机译:1型糖尿病的易感性与人类白细胞抗原(HLA)基因密切相关,在疾病发病机理中涉及T细胞。在人类中,CD8 T细胞主要渗入胰岛,但其活化和增殖可能需要CD4 T细胞的帮助。 CD4 T细胞可以在激活后从几种分化命运中进行选择,这种选择对其随后的细胞因子产生和迁移潜力具有深远的影响。反过来,这些特征决定了T细胞与哪些其他免疫细胞类型相互作用并影响,从而确定下游效应子功能。因此,在计划干预策略时,获得与特定免疫介导疾病相关的CD4 T细胞分化类型的准确图片就成为了重要线索。 T细胞分化的早期模型集中于T辅助型1(Th1)和Th2反应之间的二分法,其中1型糖尿病(T1D)主要被视为Th1介导的病理。但是,近年来出现了其他几种命运选择,包括Th17细胞和滤泡辅助性T细胞。在这里,我们重新审视自身免疫性糖尿病中T细胞分化的问题,强调了来自小鼠模型和患者样品的新证据。我们评估了Th1范例的优缺点,回顾了1型糖尿病中白介素(IL)-17产生的数据,并讨论了IL-21和滤泡辅助性T细胞在这种疾病中的作用的新证据。更好地了解T1D中CD4 T细胞的表型无疑将为生物标记物的开发,改善患者分层以及潜在地揭示治疗干预的新目标提供依据。

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