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Proteome-wide survey of the autoimmune target repertoire in autoimmune polyendocrine syndrome type 1

机译:蛋白质组范围的自身免疫性多内分泌综合征1型自身免疫性靶标库的调查

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摘要

Autoimmune polyendocrine syndrome type 1 (APS1) is a monogenic disorder that features multiple autoimmune disease manifestations. It is caused by mutations in the Autoimmune regulator (AIRE) gene, which promote thymic display of thousands of peripheral tissue antigens in a process critical for establishing central immune tolerance. We here used proteome arrays to perform a comprehensive study of autoimmune targets in APS1. Interrogation of established autoantigens revealed highly reliable detection of autoantibodies, and by exploring the full panel of more than 9000 proteins we further identified MAGEB2 and PDILT as novel major autoantigens in APS1. Our proteome-wide assessment revealed a marked enrichment for tissue-specific immune targets, mirroring AIRE’s selectiveness for this category of genes. Our findings also suggest that only a very limited portion of the proteome becomes targeted by the immune system in APS1, which contrasts the broad defect of thymic presentation associated with AIRE-deficiency and raises novel questions what other factors are needed for break of tolerance.
机译:1型自身免疫性多内分泌综合征(APS1)是一种单基因疾病,具有多种自身免疫性疾病表现。它是由自身免疫调节剂(AIRE)基因的突变引起的,该突变在建立中枢免疫耐受的关键过程中促进了成千上万个外周组织抗原的胸腺显示。我们在这里使用蛋白质组芯片对APS1中的自身免疫靶标进行全面研究。对已建立的自身抗原的询问揭示了对自身抗体的高度可靠的检测,并且通过探索全部9000多种蛋白质,我们进一步鉴定了MAGEB2和PDILT是APS1中的新型主要自身抗原。我们对整个蛋白质组进行的评估表明,组织特异性免疫靶点明显富集,这反映了AIRE对此类基因的选择性。我们的发现还表明,蛋白质组中只有非常有限的一部分会被APS1中的免疫系统靶向,这与与AIRE缺乏症相关的胸腺呈象的广泛缺陷形成了鲜明对比,并提出了新的问题,即打破耐受性还需要其他哪些因素。

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