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原发性干燥综合征白种人的HLA标记物与临床特征

HLA markers and clinical characteristics in Caucasians with primary Sjögren's syndrome.

作者信息

Bolstad A I, Wassmuth R, Haga H J, Jonsson R

机构信息

Broegelmann Research Laboratory, University of Bergen, Germany.

出版信息

J Rheumatol. 2001 Jul;28(7):1554-62.

Abstract

OBJECTIVE

To explore the association between HLA genotypes and clinical and immunological characteristics in Caucasians with primary Sjögren's syndrome (pSS).

METHODS

HLA genotyping for DRB1, DQA1 and DQB1 was carried out in 62 single case patients with pSS and 64 healthy controls. The specific amino acid residues at DQA1 position 34 (DQalpha-34Q) and DQB1 position 26 (DQbeta-26L) in addition to the DQ-DI (AA59-AA69) motif were deterrmined. Subsequently, the relative contribution of individual HLA markers to clinical and immunologic characteristics of pSS was assessed by group comparisons.

RESULTS

No significant associations were seen between HLA markers and histopathological or clinical features of pSS. Significant positive associations with HLA Class II markers were restricted to the formation of different autoantibodies. Formation of an anti-Ro/SSA and anti-La/SSB autoantibody response was positively associated with DRB103, DQB102 and DRB103/DRB115-DQB102/DQB10602 heterozygosity. Patients positive for anti-La/SSB also showed a strong positive anti-La/SSB association with DQA1*0501. Considering the contribution of individual DQA1 and DQB1 amino acids and sequence motifs to the formation of anti-Ro/SSA and anti-La/SSB autoantibodies, a dose dependent positive influence was detected for DQalpha-34Q and DQbeta-26L. For DQbeta-DI, the largest difference between patients and controls was seen for the presence of a single copy of this motif after selecting patients with either anti-Ro/SSA or anti-La/SSB autoantibodies.

CONCLUSION

The association of HLA Class II markers with pSS may concern the anti-Ro/La response rather than the disease itself. The strongest contributors to the formation of an anti-Ro/La response included components of the DRB103-DQB102-DQA10501 haplotype also encompassing the transethnically-associated DQbeta-DI motif. In addition, the dose dependent contribution of DQalpha-34Q and DQbeta-26L argue for a recessive contribution of HLA-DQ to the formation of an anti-Ro/La response. Given the prominent associations with DRB103 and the complex dose dependent interactions at HLA-DQ, a joint contribution of HLA-DR and DQ is likely to be relevant for the formation of anti-Ro/La autoantibodies in patients with pSS.

摘要

目的

探讨原发性干燥综合征(pSS)白种人中HLA基因型与临床及免疫学特征之间的关联。

方法

对62例pSS单病例患者和64例健康对照进行DRB1、DQA1和DQB1的HLA基因分型。除了DQ-DI(AA59-AA69)基序外,还确定了DQA1第34位(DQα-34Q)和DQB1第26位(DQβ-26L)的特定氨基酸残基。随后,通过组间比较评估个体HLA标记物对pSS临床和免疫特征的相对贡献。

结果

未发现HLA标记物与pSS的组织病理学或临床特征之间存在显著关联。与HLA II类标记物的显著正相关仅限于不同自身抗体的形成。抗Ro/SSA和抗La/SSB自身抗体反应的形成与DRB103、DQB102以及DRB103/DRB115-DQB102/DQB10602杂合性呈正相关。抗La/SSB阳性的患者也显示出DQA1*0501与抗La/SSB之间有很强的正相关。考虑到个体DQA1和DQB1氨基酸及序列基序对抗Ro/SSA和抗La/SSB自身抗体形成的贡献,检测到DQα-34Q和DQβ-26L具有剂量依赖性的正向影响。对于DQβ-DI,在选择抗Ro/SSA或抗La/SSB自身抗体的患者后,患者与对照之间最大的差异在于该基序单拷贝的存在情况。

结论

HLA II类标记物与pSS的关联可能涉及抗Ro/La反应而非疾病本身。抗Ro/La反应形成的最强贡献因素包括DRB103-DQB102-DQA10501单倍型的组成部分,该单倍型还包含跨种族相关的DQβ-DI基序。此外,DQα-34Q和DQβ-26L的剂量依赖性贡献表明HLA-DQ对抗Ro/La反应的形成具有隐性贡献。鉴于与DRB103的显著关联以及HLA-DQ处复杂的剂量依赖性相互作用,HLA-DR和DQ的共同作用可能与pSS患者抗Ro/La自身抗体的形成相关。

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