Shotgun Metagenomics Reveals an Enrichment of Potentially Cross-reactive Bacterial Epitopes in Ankylosing Spondylitis Patients, As Well As the Effects of TNFi Therapy Upon Microbiome Composition

Overview

Journal Ann Rheum Dis

Specialty Rheumatology

Date 2019 Oct 31

PMID 31662318

Citations 60

Authors

Jian Yin

Peter Richard Sternes

Mingbang Wang

Jing Song

Mark Morrison

Ting Li

Ling Zhou

Xin Wu

Fusheng He

Jian Zhu

Matthew A Brown

Huji Xu

Affiliations

Soon will be listed here.

Abstract

Objectives: Diverse evidence including clinical, genetic and microbiome studies support a major role of the gut microbiome in the common immune-mediated arthropathy, ankylosing spondylitis (AS). We set out to (1) further define the key microbial characteristics driving disease, and (2) examine the effects of tumour necrosis factor-inhibitor (TNFi) therapy upon the microbiome.

Methods: The stools from a case-control cohort of 250 Han-Chinese subjects underwent shotgun metagenomic sequencing. All subjects were genotyped using the Illumina CoreExome SNP microarray.

Results: Previous reports of gut dysbiosis in AS were reconfirmed and several notable bacterial species and functional categories were differentially abundant. TNFi therapy was correlated with a restoration the perturbed microbiome observed in untreated AS cases to that of healthy controls, including several important bacterial species that have been previously associated with AS and other related diseases. Enrichment of bacterial peptides homologous to HLA-B27-presented epitopes was observed in the stools of patients with AS, suggesting that either HLA-B27 fails to clear these or that they are involved in driving HLA-B27-associated immune reactions. TNFi therapy largely restored the perturbed microbiome observed in untreated AS cases to that of healthy controls, including several important bacterial species that have been previously associated with AS and other related diseases. TNFi therapy of patients with AS was also associated with a reduction of potentially arthritogenic bacterial peptides, relative to untreated patients.

Conclusion: These findings emphasise the key role that the gut microbiome plays in driving the pathogenesis of AS and highlight potential therapeutic and/or preventative targets.

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