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Beta-cell Specific Autoantibodies: Are they Just an Indicator of Type 1 Diabetes?

机译:β细胞特异性自身抗体:它们只是1型糖尿病的指标吗?

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摘要

Background: Autoantibodies (AAbs) against islet autoantigens (AAgs) are used for type 1 diabetes (T1D) diagnosis and prediction. Islet-specific AAbs usually appear early in life and may fluctuate in terms of number and titer sometimes for over 20 years before T1D develops. Whereas their predictive power is high for pediatric subjects with high genetic risk who rapidly progress to multiple AAb positivity, they are less reliable for children with low genetic risk, single AAb positivity and slow disease progression. Objective: It is unknown how AAbs develop and whether they are involved in T1D pathogenesis. So far an increase in AAb number seems to only indicate AAg spreading and progression towards clinical T1D. The goal of this review is to shed light on the possible involvement of AAbs in T1D development. Method: We thoroughly review the current literature and discuss possible mechanisms of AAb development and the roles they may play in disease pathogenesis. Results: Genetic and environmental factors instigate changes at the molecular and cellular levels that promote AAb development. Although direct involvement of AAbs in T1D is less clear, autoreactive B cells are clearly involved in various immune and autoimmune responses via antigen presentation, im-munoregulation and cytokine production.
机译:背景:针对胰岛自身抗原 (AAgs) 的自身抗体 (AAbs) 用于 1 型糖尿病 (T1D) 的诊断和预测。胰岛特异性 AAb 通常出现在生命早期,在 T1D 发生之前,胰岛特异性 AAb 的数量和滴度可能会波动,有时持续 20 多年。虽然它们对具有高遗传风险且迅速进展为多发 AAb 阳性的儿科受试者具有很高的预测能力,但对于遗传风险低、单 AAb 阳性和疾病进展缓慢的儿童,它们的可靠性较低。目的:尚不清楚AAbs是如何发展的,以及它们是否参与T1D的发病机制。到目前为止,AAb 数量的增加似乎仅表明 AAg 扩散并进展为临床 T1D。本综述的目的是阐明AAbs可能参与T1D开发。方法:我们全面回顾了目前的文献,并讨论了AAb发展的可能机制及其在疾病发病机制中可能发挥的作用。结果:遗传和环境因素在分子和细胞水平上引发变化,促进AAb的发育。虽然 AAbs 直接参与 T1D 不太清楚,但自身反应性 B 细胞通过抗原呈递、免疫调节和细胞因子产生明显参与各种免疫和自身免疫反应。

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