在不同血统中，HLA - B∗08:01∼DRB1∗03:01（DR3）和HLA - DQA∗01:02（DR2）通过低补体C4水平增加患青少年型系统性红斑狼疮的风险。

Across ancestries, HLA-B∗08:01∼DRB1∗03:01 (DR3) and HLA-DQA∗01:02 (DR2) increase the risk to develop juvenile-onset systemic lupus erythematosus through low complement C4 levels.

作者信息

Renaudineau Yves, Charras Amandine, Natoli Valentina, Congy-Jolivet Nicolas, Haldenby Sam, Liu Xuan, Fang Yongxiang, Smith Eve Md, Beresford Michael W, Hedrich Christian M

机构信息

Immunology Department Laboratory, Referral Medical Biology Laboratory, Institut Fédératif de Biologie, Toulouse University Hospital Centre, France.

INFINITy, Toulouse Institute for Infectious and Inflammatory Diseases, INSERM U1291, CNRS U5051, University Toulouse III, Toulouse, France.

出版信息

J Transl Autoimmun. 2025 Jan 7;10:100268. doi: 10.1016/j.jtauto.2025.100268. eCollection 2025 Jun.

DOI:10.1016/j.jtauto.2025.100268

PMID:39896198

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11786776/

Abstract

OBJECTIVE

Systemic lupus erythematosus (SLE) is a systemic autoimmune/inflammatory disease with a strong genetic component. Genetic burden is higher in children when compared to patients with adult-onset SLE, contributing to earlier disease expression and more severe phenotypes. The human leukocyte antigen (HLA) cluster on chromosome 6p21.3 is among the most variable genomic regions, representing a major risk-factor for SLE in adults. Its impact on juvenile-onset (j)SLE remains largely unstudied.

METHODS

High-resolution sequencing of HLA class I (A, B, C), class II (DRB1, DQA1, DQB1) and class III (complement ) was undertaken in the multi-ancestral UK JSLE Cohort including participants of Caucasian (n = 151, 48.8 %), Asian (n = 108, 35.0 %) and African/Caribbean (n = 50, 16.2 %) descent. Considering ancestral variation, clinical associations were tested at the level of alleles (2-field resolution), associated HLA protein sequences (antigen binding domains, 4-field resolution), and extended haplotypes (DRh).

RESULTS

Although important ancestral recombination was reported for HLA-DR2 and -DR3 haplotypes, risk associated with jSLE was conserved at related alleles (DR2h: DRB1∗15:01, DQA∗01:02, DQB1∗06:02; DR3h: C∗07:02 [Asian], B∗08:01, rs9332730 [Asian], DRB1∗03:01). HLA-DR7 haplotypes (DRB1∗07:01, OR = 0.44, 95 % CI:0.27-0.72, p = 0.0004; DQA1∗02:01, OR = 0.34, 95 % CI:0.21-0.56, p = 1.8 × 10) protect Asians from jSLE development. Among 23 clinical variables recorded, the main association was found between low levels of complement C4 in Caucasian carriers of HLA-DR3h. This was not the case in Asians due to recombination with HLA-C∗07:02 and integration of the rs9332730 minor allele. Low C4 serum levels associated with HLA-DQA1∗01:02 (DR2h) in Caucasians after excluding HLA-DR3h carriers from the analysis. An association between low white blood cell counts and HLA-A∗03:01P was observed across ancestries.

CONCLUSION

Genetic variation in the cluster associates with organ domain involvement (hematological) and complement levels in jSLE. Lupus-associated haplotypes vary between ancestral groups, underscoring the importance of multi-ancestral approaches to genetic studies in SLE and other autoimmune/inflammatory diseases.

摘要

目的

系统性红斑狼疮（SLE）是一种具有强烈遗传成分的全身性自身免疫/炎症性疾病。与成人发病的SLE患者相比，儿童的遗传负担更高，这导致疾病更早出现且表型更严重。位于6号染色体p21.3上的人类白细胞抗原（HLA）簇是基因组中变异最大的区域之一，是成人SLE的主要危险因素。其对青少年发病（j）SLE的影响在很大程度上仍未得到研究。

方法

对多祖先的英国JSLE队列进行了HLA I类（A、B、C）、II类（DRB1、DQA1、DQB1）和III类（补体）的高分辨率测序，该队列包括白种人（n = 151，48.8%）、亚洲人（n = 108，35.0%）和非洲/加勒比人（n = 50，16.2%）后裔的参与者。考虑到祖先变异，在等位基因水平（2字段分辨率）、相关的HLA蛋白序列（抗原结合域，4字段分辨率）和扩展单倍型（DRh）水平上测试临床关联。

结果

尽管报告了HLA - DR2和 - DR3单倍型存在重要的祖先重组，但与jSLE相关的风险在相关等位基因（DR2h：DRB1∗15:01、DQA∗01:02、DQB1∗06:02；DR3h：C∗07:02[亚洲人]、B∗08:01、rs9332730[亚洲人]、DRB1∗03:01）中是保守的。HLA - DR7单倍型（DRB1∗07:01，OR = 0.44，95%CI：0.27 - 0.72，p = 0.0004；DQA1∗02:01，OR = 0.34，95%CI：0.21 - 0.56，p = 1.8×10）可保护亚洲人不发生jSLE。在记录的23个临床变量中，主要关联发现于HLA - DR3h的白种人携带者中补体C4水平较低。在亚洲人中并非如此，因为与HLA - C∗07:02发生了重组且整合了rs9332730次要等位基因。在排除HLA - DR3h携带者后，白种人中低C4血清水平与HLA - DQA1∗01:02（DR2h）相关。在所有祖先群体中均观察到低白细胞计数与HLA - A∗03:01P之间存在关联。