Phenotype‐specific signatures of systems‐level gut microbiome associated with childhood airway allergies

Author:

Chiu Chih‐Yung12ORCID,Chang Ko‐Chun3,Chang Lun‐Ching4,Wang Chia‐Jung12,Chung Wen‐Hung5,Hsieh Wen‐Ping3,Su Shih‐Chi5ORCID

Affiliation:

1. Division of Pediatric Pulmonology, Chang Gung Memorial Hospital at Linkou, College of Medicine Chang Gung University Taoyuan Taiwan

2. Clinical Metabolomics Core Laboratory Chang Gung Memorial Hospital at Linkou Taoyuan Taiwan

3. Institute of Statistics National Tsing‐Hua University Hsinchu Taiwan

4. Department of Mathematical Sciences Florida Atlantic University Boca Raton USA

5. Whole‐Genome Research Core Laboratory of Human Diseases Chang Gung Memorial Hospital Keelung Taiwan

Abstract

AbstractBackgroundPerturbation of gut symbiosis has been linked to childhood allergic diseases. However, the underlying host–microbe interaction connected with specific phenotypes is poorly understood.MethodsTo address this, integrative analyses of stool metagenomic and metabolomic profiles associated with IgE reactions in 56 children with mite‐sensitized airway allergies (25 with rhinitis and 31 with asthma) and 28 nonallergic healthy controls were conducted.ResultsWe noted a decrease in the number and abundance of gut microbiome‐encoded carbohydrate‐active enzyme (CAZyme) genes, accompanied with a reduction in species richness, in the asthmatic gut microflora but not in that from allergic rhinitis. Such loss of CAZymes was consistent with the observation that a CAZyme‐linked decrease in fecal butyrate was found in asthmatics and negatively correlated with mite‐specific IgE responses. Different from the CAZymes, we demonstrated an increase in α diversity at the virulome levels in asthmatic gut microbiota and identified phenotype‐specific variations of gut virulome. Moreover, use of fecal metagenomic and metabolomic signatures resulted in distinct effects on differentiating rhinitis and asthma from nonallergic healthy controls.ConclusionOverall, our integrative analyses reveal several signatures of systems‐level gut microbiome in robust associations with fecal metabolites and disease phenotypes, which may be of etiological and diagnostic implications in childhood airway allergies.

Funder

Chang Gung Medical Foundation

Ministry of Science and Technology, Taiwan

Publisher

Wiley

Subject

Immunology,Immunology and Allergy,Pediatrics, Perinatology and Child Health

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