| Literature DB >> 33001460 |
Noora Ottman1, Mauricio Barrientos-Somarribas2, Nanna Fyhrquist1,3, Helen Alexander4, Lukas Wisgrill5, Peter Olah6,7, Sophia Tsoka8, Dario Greco9,10,11, Francesca Levi-Schaffer12, Vassili Soumelis13,14, Jens M Schröder15, Juha Kere16,17, Frank O Nestle18, Jonathan Barker19, Annamari Ranki20, Antti Lauerma20, Bernhard Homey6, Björn Andersson2, Harri Alenius1,3.
Abstract
It is well established that different sites in healthy human skin are colonized by distinct microbial communities due to different physiological conditions. However, few studies have explored microbial heterogeneity between skin sites in diseased skin, such as atopic dermatitis (AD) lesions. To address this issue, we carried out deep analysis of the microbiome and transcriptome in the skin of a large cohort of AD patients and healthy volunteers, comparing two physiologically different sites: upper back and posterior thigh. Microbiome samples and biopsies were obtained from both lesional and nonlesional skin to identify changes related to the disease process. Transcriptome analysis revealed distinct disease-related gene expression profiles depending on anatomical location, with keratinization dominating the transcriptomic signatures in posterior thigh, and lipid metabolism in the upper back. Moreover, we show that relative abundance of Staphylococcus aureus is associated with disease severity in the posterior thigh, but not in the upper back. Our results suggest that AD may select for similar microbes in different anatomical locations-an "AD-like microbiome," but distinct microbial dynamics can still be observed when comparing posterior thigh to upper back. This study highlights the importance of considering the variability across skin sites when studying the development of skin inflammation.Entities:
Keywords: atopic dermatitis; inflammation; microbiome
Mesh:
Year: 2020 PMID: 33001460 DOI: 10.1111/all.14606
Source DB: PubMed Journal: Allergy ISSN: 0105-4538 Impact factor: 13.146