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GWAS Study

Genome-wide host-pathogen analyses reveal genetic interaction points in tuberculosis disease.

Phelan J, Gomez-Gonzalez PJ, Andreu N et al.

36725857 PubMed ID
GWAS Study Type
714 Participants
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Chapter I

Publication Details

Comprehensive information about this research publication

Authors

PJ
Phelan J
GP
Gomez-Gonzalez PJ
AN
Andreu N
OY
Omae Y
TL
Toyo-Oka L
YH
Yanai H
MR
Miyahara R
NS
Nedsuwan S
DS
de Sessions PF
CS
Campino S
SN
Sallah N
PJ
Parkhill J
SN
Smittipat N
PP
Palittapongarnpim P
MT
Mushiroda T
KM
Kubo M
TK
Tokunaga K
MS
Mahasirimongkol S
HM
Hibberd ML
CT
Clark TG
Chapter II

Abstract

Summary of the research findings

The genetics underlying tuberculosis (TB) pathophysiology are poorly understood. Human genome-wide association studies have failed so far to reveal reproducible susceptibility loci, attributed in part to the influence of the underlying Mycobacterium tuberculosis (Mtb) bacterial genotype on the outcome of the infection. Several studies have found associations of human genetic polymorphisms with Mtb phylo-lineages, but studies analysing genome-genome interactions are needed. By implementing a phylogenetic tree-based Mtb-to-human analysis for 714 TB patients from Thailand, we identify eight putative genetic interaction points (P < 5 × 10-8) including human loci DAP and RIMS3, both linked to the IFNγ cytokine and host immune system, as well as FSTL5, previously associated with susceptibility to TB. Many of the corresponding Mtb markers are lineage specific. The genome-to-genome analysis reveals a complex interactome picture, supports host-pathogen adaptation and co-evolution in TB, and has potential applications to large-scale studies across many TB endemic populations matched for host-pathogen genomic diversity.

714 East Asian ancestry cases

Chapter III

Study Statistics

Key metrics and study information

714
Total Participants
GWAS
Study Type
No
Replicated
East Asian
Ancestry
Thailand
Recruitment Country
Chapter IV

Analysis

Comprehensive review of health and genetic findings

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