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SIAE Rare Variants in Juvenile Idiopathic Arthritis and Primary Antibody Deficiencies

机译:SIAE少年特发性关节炎和一抗缺乏的罕见变异

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摘要

Sialic acid acetylesterase (SIAE) deficiency was suggested to lower the levels of ligands for sialic acid-binding immunoglobulin-like receptors, decreasing the threshold for B-cell activation. In humans, studies of rare heterozygous loss-of-function mutations in SIAE gene in common autoimmune diseases, including juvenile idiopathic arthritis (JIA), yielded inconsistent results. Considering the distinct pathogenesis of the two main subtypes of JIA, autoinflammatory systemic (sJIA) and autoimmune oligo/polyarticular (aJIA), and a predisposition to autoimmunity displayed by patients and families with primary antibody deficiencies (PADs), the aim of our study was to analyze whether SIAE rare variants are associated with both the phenotype of JIA and the autoimmunity risk in families with PADs. A cohort of 69 patients with JIA, 117 healthy children, 54 patients, and family members with PADs were enrolled in the study. Three novel SIAE variants (p.Q343P, p.Y495X, and c.1320+33T>C) were found only in patients with aJIA but interestingly also in their healthy relatives without autoimmunity, while none of PAD patients or their relatives carried SIAE defects. Our results show that SIAE rare variants are not causative of autoimmunity as single defects.
机译:有人建议唾液酸乙酰酯酶(SIAE)缺乏会降低结合唾液酸的免疫球蛋白样受体的配体水平,从而降低B细胞活化的阈值。在人类中,对常见的自身免疫性疾病(包括幼年特发性关节炎(JIA))中SIAE基因罕见的杂合功能丧失突变的研究产生了不一致的结果。考虑到JIA的两种主要亚型的独特发病机理,即自身炎症性全身性(sJIA)和自身免疫性寡/多关节(aJIA),以及患有原发性抗体缺乏症(PAD)的患者和家庭对自身免疫的倾向,我们的研究目的是分析SIAE罕见变体是否与PAA家族的JIA表型和自身免疫风险相关。这项研究共纳入了69名JIA患者,117名健康儿童,54名患者以及PAD家族成员。仅在患有aJIA的患者中发现了三个新颖的SIAE变体(p.Q343P,p.Y495X和c.1320 + 33T> C),有趣的是,在没有自身免疫的健康亲戚中也发现了PAD患者或其亲属均未携带SIAE缺陷。我们的结果表明,SIAE罕见变体不是单一缺陷导致自身免疫性的原因。

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