Genetic variations in low-to-medium-affinity Fcγ receptors and autoimmune neutropenia in early childhood in a Danish cohort

IF 2.3 4区 医学 Q3 GENETICS & HEREDITY International Journal of Immunogenetics Pub Date : 2023-02-08 DOI:10.1111/iji.12614
Kirstine Kløve-Mogensen, Rudi Steffensen, Tania Nicole Masmas, Andreas Glenthøj, Christina Friis Jensen, Thure Mors Haunstrup, Paul Ratcliffe, Petter Höglund, Henrik Hasle, Kaspar René Nielsen
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引用次数: 0

Abstract

Autoimmune neutropenia (AIN) in early childhood is caused by autoantibodies directed against antigens on the neutrophil membrane and is a frequent cause of neutropenia in children. Association of AIN with Fcγ receptor (FCGR) 3B variants is well described. In this study, we investigate genetic variations in the FCGR locus and copy number variation of FCGR3B. A total of 130 antibody-positive AIN patients, 64 with specific anti-HNA-1a antibodies and 66 with broad-reacting anti-FcγRIIIb antibodies, were genotyped with a multiplex ligation probe assay and compared with healthy controls. Positive findings were confirmed with real-time q-PCR. We determined copy numbers of the FCGR2 and FCGR3 genes and the following SNPs: FCGR2A Q62W (rs201218628), FCGR2A H166R (rs1801274), FCGR2B I232T (rs1050501), FCGR3A V176F (rs396991), haplotypes for FCGR2B/C promoters (rs3219018/rs780467580), FCGR2C STOP/ORF and HNA-1 genotypes in FCGR3B (rs447536, rs448740, rs52820103, rs428888 and rs2290834). Generally, associations were antibody specific, with all associations being representative of the anti-HNA-1a-positive group, while the only association found in the anti-FcγRIIIb group was with the HNA-1 genotype. An increased risk of AIN was observed for patients with one copy of FCGR3B; the HNA genotypes HNA-1a, HNA-1aa or HNA-1aac; the FCGR2A 166H and FCGR2B 232I variations; and no copies of FCGR2B 2B.4. A decreased risk was observed for HNA genotype HNA-1bb; FCGR2A 166R; FCGR2B 232T; and one copy of FCGR2B promoter 2B.4. We conclude that in our Danish cohort, there was a strong association between variation in the FCGR locus and AIN. The findings of different genetic associations between autoantibody groups could indicate the presence of two different disease entities and disease heterogeneity.

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在丹麦队列中,儿童早期低至中等亲和力Fcγ受体和自身免疫性中性粒细胞减少症的遗传变异
儿童早期自身免疫性中性粒细胞减少症(AIN)是由针对中性粒细胞膜上抗原的自身抗体引起的,是儿童中性粒细胞减少症的常见原因。AIN与Fcγ受体(FCGR) 3B变异的关联已被很好地描述。在本研究中,我们研究了FCGR位点的遗传变异和FCGR3B的拷贝数变异。采用多重连接探针法对130例抗体阳性的AIN患者进行基因分型,其中64例具有特异性的抗hna -1a抗体,66例具有广谱反应的抗fc - γ riiib抗体。real-time q-PCR证实阳性结果。我们测定了FCGR2和FCGR3基因的拷贝数和以下snp: FCGR2A Q62W (rs201218628)、FCGR2A H166R (rs1801274)、FCGR2B I232T (rs1050501)、FCGR3A V176F (rs396991)、FCGR2B/C启动子单倍型(rs3219018/rs780467580)、FCGR3B中STOP/ORF和HNA-1基因型(rs447536、rs448740、rss52820103、rs428888和rs2290834)。一般来说,关联是抗体特异性的,所有的关联都代表了抗rna -1阳性组,而抗fc γ riiib组中发现的唯一关联与rna -1基因型有关。携带一个FCGR3B拷贝的患者发生AIN的风险增加;基因型为:HNA-1a、HNA-1aa、HNA-1aac;FCGR2A 166H和FCGR2B 232I型号;没有FCGR2B 2B.4的副本。HNA-1bb基因型患者患病风险降低;FCGR2A 166 r;FCGR2B 232吨;FCGR2B启动子2B.4拷贝一份。我们得出结论,在我们的丹麦队列中,FCGR位点的变异与AIN之间存在很强的相关性。自身抗体组之间不同遗传关联的发现可能表明存在两种不同的疾病实体和疾病异质性。
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来源期刊
CiteScore
4.70
自引率
0.00%
发文量
48
审稿时长
6-12 weeks
期刊介绍: The International Journal of Immunogenetics (formerly European Journal of Immunogenetics) publishes original contributions on the genetic control of components of the immune system and their interactions in both humans and experimental animals. The term ''genetic'' is taken in its broadest sense to include studies at the evolutionary, molecular, chromosomal functional and population levels in both health and disease. Examples are: -studies of blood groups and other surface antigens- cell interactions and immune response- receptors, antibodies, complement components and cytokines- polymorphism- evolution of the organisation, control and function of immune system components- anthropology and disease associations- the genetics of immune-related disease: allergy, autoimmunity, immunodeficiency and other immune pathologies- All papers are seen by at least two independent referees and only papers of the highest quality are accepted.
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