Elsevier

Infection, Genetics and Evolution

Volume 66, December 2018, Pages 286-307
Infection, Genetics and Evolution

Research paper
Genetic susceptibility to infectious diseases: Current status and future perspectives from genome-wide approaches

https://doi.org/10.1016/j.meegid.2017.09.028Get rights and content

Highlights

  • Relatively few GWASs for infectious diseases were performed.

  • Phenotype heterogeneity and case/control misclassification can affect GWAS power.

  • Adaptive and innate immunity loci were identified in several infectious disease GWASs.

  • Unexpected loci (e.g., lncRNAs) were also associated with infection susceptibility.

  • GWASs should integrate host and pathogen diversity and use complex association models.

Abstract

Genome-wide association studies (GWASs) have been widely applied to identify genetic factors that affect complex diseases or traits. Presently, the GWAS Catalog includes > 2800 human studies. Of these, only a minority have investigated the susceptibility to infectious diseases or the response to therapies for the treatment or prevention of infections. Despite their limited application in the field, GWASs have provided valuable insights by pinpointing associations to both innate and adaptive immune response loci, as well as novel unexpected risk factors for infection susceptibility. Herein, we discuss some issues and caveats of GWASs for infectious diseases, we review the most recent findings ensuing from these studies, and we provide a brief summary of selected GWASs for infections in non-human mammals. We conclude that, although the general trend in the field of complex traits is to shift from GWAS to next-generation sequencing, important knowledge on infectious disease-related traits can be still gained by GWASs, especially for those conditions that have never been investigated using this approach. We suggest that future studies will benefit from the leveraging of information from the host's and pathogen's genomes, as well as from the exploration of models that incorporate heterogeneity across populations and phenotypes. Interactions within HLA genes or among HLA variants and polymorphisms located outside the major histocompatibility complex may also play an important role in shaping the susceptibility and response to invading pathogens.

Abbreviations

GWAS
Genome-wide association study
MHC
major histocompatibility complex
HLA
human leukocyte antigen
KIR
Killer-cell immunoglobulin-like receptor
lncRNA
long non-coding RNA
PCA
principal components analysis
LD
linkage disequilibrium
SNP
single nucleotide polymorphism
T2D
Type 2 diabetes
TB
tuberculosis
HCV
hepatitis C virus
HIV-1
Human Immunodeficiency virus type 1
HBV
hepatitis B virus
HCC
hepatocellular carcinoma
eQTL
expression quantitative trait locus
HPV
Human Papillomavirus
VZV
Varicella Zooster virus
IAV
Influenza A virus
PCT
periodontal complex trait
CNV
copy number variant
CJD
Creutzfeldt-Jacob disease
CC
Collaborative Cross
EBOV
Ebola virus
WNV
West Nile virus
PRRSV
porcine reproductive and respiratory syndrome virus

Keywords

GWAS
Infectious disease
Response to treatment or vaccine

Cited by (0)

1

These authors contributed equally to this work.

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