Shotgun metagenomic sequencing on skin microbiome indicates dysbiosis exists prior to the onset of atopic dermatitis

Author:

Chaudhary Prem Prashant1,Myles Ian A.1ORCID,Zeldin Jordan1,Dabdoub Shareef2,Deopujari Varsha3,Baveja Rajiv4,Baker Robin4,Bengtson Sarah56,Sutton Ashleigh6,Levy Shira6,Hourigan Suchitra K.6

Affiliation:

1. Epithelial Therapeutics Unit National Institute of Allergy and Infectious Diseases, National Institutes of Health Bethesda Maryland USA

2. Division of Biostatistics and Computational Biology College of Dentistry, University of Iowa Iowa City Iowa USA

3. Inova Children's Hospital Falls Church Virginia USA

4. Fairfax Neonatal Associates Fairfax Virginia USA

5. College of William and Mary Williamsburg Virginia USA

6. Clinical Microbiome Unit National Institute of Allergy and Infectious Diseases, National Institutes of Health Bethesda Maryland USA

Abstract

AbstractBackgroundWhile the microbiome is increasingly seen as a targetable contributor to atopic dermatitis (AD), questions remain as to whether the dysbiosis is secondary to diseased skin or if it predates symptom onset. Previous work has evaluated how the skin microbiome changes with age and established the influence of factors like delivery mode and breastfeeding on global microbiome diversity. However, these studies were unable to identify taxa which predict subsequent AD.MethodsSkin swab samples were collected from the first week of life for 72 children in the neonatal intensive care unit (NICU) at a single site hospital. Participants were followed for 3 years to determine their health status. We applied shotgun metagenomic sequencing to assess the microbiome differences between 31 children who went on to develop AD and 41 controls.ResultsWe identified that subsequent development of AD was associated with differential abundance of several bacterial and fungal taxa as well as several metabolic pathways, each of which have been previously associated with active AD.ConclusionsOur work provides evidence of reproducibility for the previously reported dysbiotic signatures predating AD onset while also expanding prior findings through the first use of metagenomic assessment prior to AD onset. While extrapolation of our findings beyond the pre‐term, NICU cohort is limited, our findings add to the evidence that the dysbiosis associated with AD pre‐dates disease onset rather than reflect a secondary consequence of skin inflammation.

Funder

National Institutes of Health

Publisher

Wiley

Subject

Immunology,Immunology and Allergy

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