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Genome-wide Association Study of Late-Onset Myasthenia Gravis: Confirmation of TNFRSF11A, and Identification of ZBTB10 and Three Distinct HLA Associations.

Seldin MF, Alkhairy OK, Lee AT et al.

26562150 PubMed ID
GWAS Study Type
2660 Participants
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Chapter I

Publication Details

Comprehensive information about this research publication

Authors

SM
Seldin MF
AO
Alkhairy OK
LA
Lee AT
LJ
Lamb JA
SJ
Sussman J
PR
Pirskanen-Matell R
PF
Piehl F
VJ
Verschuuren JJGM
KA
Kostera-Pruszczyk A
SP
Szczudlik P
MD
McKee D
MA
Maniaol AH
HH
Harbo HF
LB
Lie BA
MA
Melms A
GH
Garchon HJ
WN
Willcox N
GP
Gregersen PK
HL
Hammarstrom L
Chapter II

Abstract

Summary of the research findings

To investigate the genetics of late-onset myasthenia gravis (LOMG), we conducted a genome-wide association study imputation of>6 million single nucleotide polymorphisms (SNPs) in 532 LOMG cases (anti-acetylcholine receptor [AChR] antibody positive; onset age≥50 years) and 2,128 controls matched for sex and population substructure. The data confirm reported TNFRSF11A associations (rs4574025, P = 3.9 × 10-7, odds ratio [OR] 1.42) and identify a novel candidate gene, ZBTB10, achieving genome-wide significance (rs6998967, P = 8.9 × 10-10, OR 0.53). Several other SNPs showed suggestive significance including rs2476601 (P = 6.5 × 10-6, OR 1.62) encoding the PTPN22 R620W variant noted in early-onset myasthenia gravis (EOMG) and other autoimmune diseases. In contrast, EOMG-associated SNPs in TNIP1 showed no association in LOMG, nor did other loci suggested for EOMG. Many SNPs within the major histocompatibility complex (MHC) region showed strong associations in LOMG, but with smaller effect sizes than in EOMG (highest OR ~2 versus ~6 in EOMG). Moreover, the strongest associations were in opposite directions from EOMG, including an OR of 0.54 for DQA1*05:01 in LOMG (P = 5.9 × 10-12) versus 2.82 in EOMG (P = 3.86 × 10-45). Association and conditioning studies for the MHC region showed three distinct and largely independent association peaks for LOMG corresponding to (a) MHC class II (highest attenuation when conditioning on DQA1), (b) HLA-A and (c) MHC class III SNPs. Conditioning studies of human leukocyte antigen (HLA) amino acid residues also suggest potential functional correlates. Together, these findings emphasize the value of subgrouping myasthenia gravis patients for clinical and basic investigations and imply distinct predisposing mechanisms in LOMG.

532 European ancestry cases, 2,128 European ancestry controls

Chapter III

Study Statistics

Key metrics and study information

2660
Total Participants
GWAS
Study Type
No
Replicated
European
Ancestry
Sweden, U.S., Poland, Netherlands, Germany, U.K., France, Norway
Recruitment Country
Chapter IV

AI-Generated Summary

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