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GWAS Study

Life is pain: Fibromyalgia as a nexus of multiple liability distributions.

Moscati A, Faucon AB, Arnaiz-Yépez C et al.

37334860 PubMed ID
GWAS Study Type
16024 Participants
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Chapter I

Publication Details

Comprehensive information about this research publication

Authors

MA
Moscati A
FA
Faucon AB
AC
Arnaiz-Yépez C
LS
Lönn SL
SJ
Sundquist J
SK
Sundquist K
BG
Belbin GM
NG
Nadkarni G
CJ
Cho JH
LR
Loos RJF
DL
Davis LK
KK
Kendler KS
Chapter II

Abstract

Summary of the research findings

Fibromyalgia is a complex disease of unclear etiology that is complicated by difficulties in diagnosis, treatment, and clinical heterogeneity. To clarify this etiology, healthcare-based data are leveraged to assess the influences on fibromyalgia in several domains. Prevalence is less than 1% of females in our population register data, and about 1/10th that in males. Fibromyalgia often presents with co-occurring conditions including back pain, rheumatoid arthritis, and anxiety. More comorbidities are identified with hospital-associated biobank data, falling into three broad categories of pain-related, autoimmune, and psychiatric disorders. Selecting representative phenotypes with published genome-wide association results for polygenic scoring, we confirm genetic predispositions to psychiatric, pain sensitivity, and autoimmune conditions show associations with fibromyalgia, although these may differ by ancestry group. We conduct a genome-wide association analysis of fibromyalgia in biobank samples, which did not result in any genome-wide significant loci; further studies with increased sample size are necessary to identify specific genetic effects on fibromyalgia. Overall, fibromyalgia appears to have strong clinical and likely genetic links to several disease categories, and could usefully be understood as a composite manifestation of these etiological sources.

275 African American or African ancestry cases, 15,749 African American or African ancestry controls

Chapter III

Study Statistics

Key metrics and study information

16024
Total Participants
GWAS
Study Type
No
Replicated
African American or Afro-Caribbean, African unspecified, European
Ancestry
U.S.
Recruitment Country
Chapter IV

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