首页> 外文期刊>The Journal of Clinical Investigation: The Official Journal of the American Society for Clinical Investigation >Genetic bias in immune responses to a cassette shared by different microorganisms in patients with rheumatoid arthritis.
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Genetic bias in immune responses to a cassette shared by different microorganisms in patients with rheumatoid arthritis.

机译:类风湿性关节炎患者对不同微生物共享的盒式磁带的免疫反应的遗传偏差。

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摘要

Rheumatoid arthritis (RA) is an autoimmune disease associated with HLA-DRbeta1 alleles which contain the QKRAA amino acid sequence in their third hypervariable region(s). The QKRAA sequence is also expressed by several human pathogens. We have shown previously that an Escherichia coli peptide encompassing QKRAA is a target of immune responses in RA patients. Here we address two questions: first, whether QKRAA may function as an "immunological cassette" with similar, RA-associated, immunogenic properties when expressed by other common human pathogens; and second, what is the influence of genetic background in the generation of these responses. We find that early RA patients have enhanced humoral and cellular immune responses to Epstein-Barr virus and Brucella ovis and Lactobacillus lactis antigens which contain the QKRAA sequence. These results suggest that the QKRAA sequence is an antigenic epitope on several different microbial proteins, and that RA patients recognize the immunological cassette on different backgrounds. ANOVA of immune responses to "shared epitope" antigens in monozygotic twin couples shows that, despite significantly elevated responses in affected individuals, a similarity between pairs is retained, thus suggesting a role played either by hereditary or shared environmental factors in the genesis or maintenance of these responses.
机译:类风湿性关节炎 (RA) 是一种与 HLA-DRbeta1 等位基因相关的自身免疫性疾病,HLA-DRbeta1 等位基因在其第三个高变区中含有 QKRAA 氨基酸序列。QKRAA序列也由几种人类病原体表达。我们之前已经证明,包含QKRAA的大肠杆菌肽是RA患者免疫反应的靶标。在这里,我们解决两个问题:首先,当其他常见的人类病原体表达时,QKRAA是否可以作为具有相似的RA相关免疫原性的“免疫盒”发挥作用;其次,遗传背景对这些反应的产生有什么影响。我们发现早期 RA 患者对含有 QKRAA 序列的 Epstein-Barr 病毒、绵羊布鲁氏菌和乳酸乳杆菌抗原的体液和细胞免疫反应增强。这些结果表明,QKRAA序列是几种不同微生物蛋白上的抗原表位,并且RA患者在不同背景下识别免疫盒。同卵双胞胎对“共享表位”抗原的免疫反应方差分析表明,尽管受影响个体的反应显着升高,但配对之间的相似性仍保留,因此表明遗传或共享环境因素在这些反应的发生或维持中发挥了作用。

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