Abstract
Sarcoidosis is a multiorgan inflammatory disorder with heritability estimates up to 66%. Previous studies have shown the major histocompatibility complex (MHC) region to be associated with sarcoidosis, suggesting a functional role for antigen-presenting molecules and immune mediators in the disease pathogenesis. To detect variants predisposing to sarcoidosis and to identify genetic differences between patient subgroups, we studied four genes in the MHC Class III region (LTA, TNF, AGER, BTNL2) and HLA-DRA with tag-SNPs and their relation to HLA-DRB1 alleles. We present results from a joint analysis of four study populations (Finnish, Swedish, Dutch, and Czech). Patients with sarcoidosis (n = 805) were further subdivided based on the disease activity and the presence of Löfgren’s syndrome. In a joint analysis, seven SNPs were associated with non-Löfgren sarcoidosis (NL; the strongest association with rs3177928, P = 1.79E−07, OR = 1.9) and eight with Löfgren’s syndrome [Löfgren syndrome (LS); the strongest association with rs3129843, P = 3.44E−12, OR = 3.4] when compared with healthy controls (n = 870). Five SNPs were associated with sarcoidosis disease course (the strongest association with rs3177928, P = 0.003, OR = 1.9). The high linkage disequilibrium (LD) between SNPs and an HLA-DRB1 challenged the result interpretation. When the SNPs and HLA-DRB1 alleles were analyzed together, independent association was observed for four SNPs in the HLA-DRA/BTNL2 region: rs3135365 (NL; P = 0.015), rs3177928 (NL; P < 0.001), rs6937545 (LS; P = 0.012), and rs5007259 (disease activity; P = 0.002). These SNPs act as expression quantitative trait loci (eQTL) for HLA-DRB1 and/or HLA-DRB5. In conclusion, we found novel SNPs in BTNL2 and HLA-DRA regions associating with sarcoidosis. Our finding further establishes that polymorphisms in the HLA-DRA and BTNL2 have a role in sarcoidosis susceptibility. This multi-population study demonstrates that at least a part of these associations are HLA-DRB1 independent (e.g., not due to LD) and shared across ancestral origins. The variants that were independent of HLA-DRB1 associations acted as eQTL for HLA-DRB1 and/or -DRB5, suggesting a role in regulating gene expression.
Highlights
Sarcoidosis (MIM 609464) is a multiorgan inflammatory disorder of unknown etiology
SNPs located in the major histocompatibility complex (MHC) that are associated with sarcoidosis and shared between four European populations with distinct ancestral origins (Finnish, Swedish, Dutch, and Czech)
We identified two novel HLA-DR alpha (HLA-DRA) downstream variants that were independent of HLA-DRB1 alleles: rs3177928 associated with non-Löfgren sarcoidosis patients (NL) and rs6937545 associated with Löfgren syndrome (LS)
Summary
Sarcoidosis (MIM 609464) is a multiorgan inflammatory disorder of unknown etiology. Current understanding views sarcoidosis primarily as a multifactorial disorder with heritability estimates up to 66%, with possible environmental triggers in addition to the susceptibility gene(s) [2,3,4]. Sarcoidosis is manifested by accumulation of activated CD4positive T lymphocytes and macrophages at disease sites suggesting a functional role for antigen-presenting molecules and immune mediator genes [4]. The search for genetic components, indicated on the basis of family and multi-ancestral studies [2, 5], has shown a strong role of the major histocompatibility complex (MHC) region at chromosome 6p21.3 in susceptibility to sarcoidosis. Several genome-wide association studies have indicated other regions of interest as well [6,7,8], but none as influential as the MHC
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