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Table 3 Genome-wide significant variants from treatment-specific GWAS for IFNβ-1a s.c

From: Treatment- and population-specific genetic risk factors for anti-drug antibodies against interferon-beta: a GWAS

ADA

Variant

Chr.

Pos. (bp)

MA

MAF (KI)

MAF (TUM)

OR/β (Disc.)

p (Disc.)

OR/β (Repl.)

p(one-sided) (Repl.)

OR/β (Pool.)

p (Pool.)

nADA pres.

rs77278603

6

32,469,421

A

0.43

0.40

3.33OR

5.3 × 10−19

4.43OR

1.9 × 10−09

3.55OR

2.1 × 10−26

nADA pres.

rs9271700

6

32,593,198

G

0.42

0.39

3.16OR

8.6 × 10−19

5.08OR

1.2 × 10−10

3.48OR

5.4 × 10−27

nADA titer

rs77278603

6

32,469,421

A

0.43

0.40

0.38β

2.2 × 10−19

0.36β

8.1 × 10−10

0.37β

2.4 × 10−27

nADA titer

rs9271673

6

32,592,833

C

0.41

0.39

0.37β

3.0 × 10−19

0.38β

5.2 × 10−11

0.37β

2.1 × 10−28

bADA level

rs9281962

6

32,594,597

T

0.44

0.43

0.51β

6.0 × 10−22

0.51β

5.5 × 10− 12

0.51β

4.6 × 10−32

  1. The top GWAS association signals that showed genome-wide significance in the discovery-stage analysis (α = 5 × 10−8) and replicated (α = 3 × 10−3) in the analysis of IFNβ-1a s.c.-treated patients. For nADA presence, odds ratios are provided (marked by OR), and for quantitative ADA measures effect sizes (marked by β). For detailed association statistics, including conditional analyses, correlated HLA alleles, nearby genes, eQTL results, permutation p values, and preparation-specific association results, see Additional file 12. For locus-specific Manhattan plots of each locus, see Additional file 18. For forest plots of each association, including treatment preparation-specific effects, see Additional file 19. Abbreviations: Chr. chromosome; Pos. position in base pairs (build hg19); MA minor and effect allele; MAF minor allele frequency; KI Karolinska Institutet, Sweden; TUM Technical University of Munich, Germany; OR odds ratio; β effect size; Disc discovery; Repl. replication; Pool. pooled; pres. presence