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GWAS Study

Identification of novel common variants associated with chronic pain using conditional false discovery rate analysis with major depressive disorder and assessment of pleiotropic effects of LRFN5.

Johnston KJA, Adams MJ, Nicholl BI et al.

31748543 PubMed ID
GWAS Study Type
153851 Participants
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Chapter I

Publication Details

Comprehensive information about this research publication

Authors

JK
Johnston KJA
AM
Adams MJ
NB
Nicholl BI
WJ
Ward J
SR
Strawbridge RJ
MA
McIntosh AM
SD
Smith DJ
BM
Bailey MES
Chapter II

Abstract

Summary of the research findings

Chronic pain is a complex trait that is moderately heritable and genetically, as well as phenotypically, correlated with major depressive disorder (MDD). Use of the conditional false discovery rate (cFDR) approach, which leverages pleiotropy identified from existing GWAS outputs, has been successful in discovering novel associated variants in related phenotypes. Here, genome-wide association study outputs for both von Korff chronic pain grade and for MDD were used to identify variants meeting a cFDR threshold for each outcome phenotype separately, as well as a conjunctional cFDR (ccFDR) threshold for both phenotypes together. Using a moderately conservative threshold, we identified a total of 11 novel single nucleotide polymorphisms (SNPs), six of which were associated with chronic pain grade and nine of which were associated with MDD. Four SNPs on chromosome 14 were associated with both chronic pain grade and MDD. SNPs associated only with chronic pain grade were located within SLC16A7 on chromosome 12. SNPs associated only with MDD were located either in a gene-dense region on chromosome 1 harbouring LINC01360, LRRIQ3, FPGT and FPGT-TNNI3K, or within/close to LRFN5 on chromosome 14. The SNPs associated with both outcomes were also located within LRFN5. Several of the SNPs on chromosomes 1 and 14 were identified as being associated with expression levels of nearby genes in the brain and central nervous system. Overall, using the cFDR approach, we identified several novel genetic loci associated with chronic pain and we describe likely pleiotropic effects of a recently identified MDD locus on chronic pain.

10,543 European ancestry chronic pain cases, 43,028 major depressive disorder cases, 12,758 European ancestry controls, 87,522 controls

Chapter III

Study Statistics

Key metrics and study information

153851
Total Participants
GWAS
Study Type
No
Replicated
European
Ancestry
Chapter IV

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