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Association of HLA-dependent islet autoimmunity with systemic antibody responses to intestinal commensal bacteria in children

机译:HLA依赖性胰岛自身免疫的关联与儿童的全身性抗体反应

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Microbiome sequence analyses have suggested that changes in gut bacterial composition are associated with autoimmune disease in humans and animal models. However, little is known of the mechanisms through which the gut microbiota influences autoimmune responses to distant tissues. Here, we evaluated systemic antibody responses against cultured human gut bacterial strains to determine whether observed patterns of anticommensal antibody (ACAb) responses are associated with type 1 diabetes (T1 D) in two cohorts of pediatric study participants. In the first cohort, ACAb responses in sera collected from participants within 6 months of T1D diagnosis were compared with age-matched healthy controls and also with patients with recent onset Crohn's disease. ACAb responses against multiple bacterial species discriminated among these three groups. In the second cohort, we asked whether ACAb responses present before diagnosis were associated with later T1 D development and with HLA genotype in participants who were discordant for subsequent progression to diabetes. Serum IgG2 antibodies against Roseburia faecis and against a bacterial consortium were associated with future T1 D diagnosis in an HLA DR3/DR4 haplotype-dependent manner. These analyses reveal associations between antibody responses to intestinal microbes and HLA-DR genotype and islet autoantibody specificity and with a future diagnosis of T1 D. Further, we present a platform to investigate antibacterial antibodies in biological fluids that is applicable to studies of autoimmune diseases and responses to therapeutic interventions.
机译:微生物组序列分析表明,肠道细菌组成的变化与人类和动物模型中的自身免疫性疾病有关。然而,几乎不知道肠道微生物群会影响遥远组织的自身免疫反应的机制。在这里,我们评估了针对培养的人肠道细菌菌株的全身性抗体反应,以确定观察到的抗妇女抗体(ACAB)反应是否与两个小儿研究参与者中的1型糖尿病(T1 D)相关。在第一个队列中,将参与者在T1D诊断后6个月内收集的血清中的ACAB反应与年龄匹配的健康对照组以及最近发作Crohn病的患者进行了比较。 ACAB针对这三组的多种细菌物种的反应。在第二个队列中,我们询问诊断前的ACAB反应是否与后来的T1 D发育和HLA基因型有关,而HLA基因型与随后进展为糖尿病的参与者中是否与HLA基因型有关。针对Roseburia Faecis和对细菌联盟的血清IgG2抗体与HLA DR3/DR4单倍型依赖性的方式与未来的T1 D诊断有关。这些分析揭示了对肠道微生物的抗体反应与HLA-DR基因型和胰岛自身抗体特异性的关联,以及与T1 D的未来诊断之间的关联。此外,我们提出了一个平台,用于研究生物流体中抗菌抗体的平台,该平台适用于适用于自身免疫性疾病和自身免疫性疾病研究的平台。对治疗干预措施的反应。

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