首页> 外文期刊>European journal of immunogenetics: official journal of the British Society for Histocompatibility and Immunogenetics >Nationwide collaborative study of HLA class II associations with distinct types of juvenile chronic arthritis (JCA) in Greece.
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Nationwide collaborative study of HLA class II associations with distinct types of juvenile chronic arthritis (JCA) in Greece.

机译:在希腊进行的HLA II类协会与不同类型的青少年慢性关节炎(JCA)的全国性合作研究。

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摘要

The aim of this study was to investigate the association of different groups and subgroups of juvenile chronic arthritis (JCA) with HLA class II (DR, DP, DQ) alleles and/or haplotypes. Groups and subgroups were mainly distinguished on the basis of the type of onset, the course and complications of the disease, and some predefined disease markers according to the criteria proposed by the ILAR Standing Committee (Chile, 1994). On the basis of these criteria the following five JCA groups and their subgroups were included in the study: (1) define systemic onset (n = 25) and systemic progressing to persistent arthritis (n = 14); (2) JCA of oligoarthritis onset (O-JCA, n = 124) and of oligoarthritis onset and course (n = 98), O-JCA of early (< 6 years) or late (> 6 years) onset (EOO-JCA n = 71 and LOO-JCA n = 44), O-JCA with ANA positive (n = 69) or negative (n = 55) and O-JCA progressing to extended arthritis (n = 22); (3) JCA of polyarthritis onset (P-JCA) with rheumatic factor (RF) negative (n = 29), and P-JCA RF negative with antinuclear antibodies (ANA) positive (n = 13) or negative (n = 16); (4) JCA complicated with chronic anterior uveitis (CAU, n = 32); (5) juvenile psoriatic arthritis (n = 20). To assess the HLA allele frequencies in the above 223 Greek children with JCA, these frequencies were compared to those of 98 age-matched and 250 adult controls. The main findings were the following. A common HLA-DRB1* allele was not involved in the JCA groups and subgroups studied; on the other hand, the DQA1*0501 allele was found to be associated with different JCA groups/subgroups (O-JCA, P-JCA RF-negative ANA-positive, JCA with CAU), probably suggesting a closer relationship of this locus with the immunogenetic background of JCA. The DPB1*0201 allele was associated with the development of either EOO-JCA or CAU. Susceptibility to CAU was stronger when the DPB1*0201 was combined with the presence of DRB1*13. Another allele, DQB1*0301, was also associated with O-JCA and CAU. Finally, no specific HLA class II allele was found to be related to the presence of ANA or psoriatic lesions or to the severity of the arthritis. Our findings suggest that the wide clinical and laboratory spectrum of JCA is associated with an immunogenetic background that is linked with HLA alleles of more than one locus. Some of them, such as the DPB1*0201 allele, confer susceptibility to certain clinical onsets and courses or complications of the disease. The rapidly advancing techniques of typing of DNA profiles may lead to more definite conclusions.
机译:这项研究的目的是调查少年慢性关节炎(JCA)的不同组和亚组与HLA II类(DR,DP,DQ)等位基因和/或单倍型的关系。主要根据疾病的发作类型,病程和并发症以及根据ILAR常务委员会提出的标准(智利,1994年)确定的一些预定义疾病标志来区分组和亚组。根据这些标准,以下五个JCA组及其亚组被纳入研究:(1)定义全身性发作(n = 25)和全身性进展为持续性关节炎(n = 14); (2)少关节炎(O-JCA,n = 124)和少关节炎和病程(n = 98),早期(<6岁)或晚期(> 6年)O-JCA(EOO-JCA)的JCA n = 71,LOO-JCA n = 44),ANA阳性(n = 69)或阴性(n = 55)的O-JCA,而O-JCA则发展为扩展性关节炎(n = 22); (3)风湿因子(RF)阴性(n = 29)的多关节炎发作(P-JCA)的JCA,而抗核抗体(ANA)阳性(n = 13)或阴性(n = 16)的P-JCA RF阴性; (4)JCA并发慢性前葡萄膜炎(CAU,n = 32); (5)少年银屑病关节炎(n = 20)。为了评估上述223名希腊JCA儿童的HLA等位基因频率,将这些频率与98位年龄匹配的儿童和250位成人对照的频率进行了比较。主要发现如下。常见的HLA-DRB1 *等位基因未参与所研究的JCA组和亚组。另一方面,发现DQA1 * 0501等位基因与不同的JCA组/亚组(O-JCA,P-JCA RF阴性ANA阳性,JCA与CAU)相关,可能表明该基因座与JCA的免疫遗传背景。 DPB1 * 0201等位基因与EOO-JCA或CAU的发展有关。当DPB1 * 0201与DRB1 * 13结合使用时,对CAU的敏感性更强。另一个等位基因DQB1 * 0301也与O-JCA和CAU相关。最后,没有发现特定的HLA II类等位基因与ANA或牛皮癣病变的存在或关节炎的严重程度有关。我们的发现表明,JCA的广泛临床和实验室谱系与免疫遗传背景有关,该背景与一个以上基因座的HLA等位基因有关。其中一些,例如DPB1 * 0201等位基因,对某些临床发作,病程或并发症具有敏感性。 DNA配置文件类型的快速发展技术可能会得出更明确的结论。

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