Skin microbiome before development of atopic dermatitis: Early colonization with commensal staphylococci at 2 months is associated with a lower risk of atopic dermatitis at 1 year DOI Creative Commons
Elizabeth A. Kennedy,

Jennifer Connolly,

Jonathan O’B Hourihane

et al.

Journal of Allergy and Clinical Immunology, Journal Year: 2016, Volume and Issue: 139(1), P. 166 - 172

Published: Sept. 9, 2016

Disease flares of established atopic dermatitis (AD) are generally associated with a low-diversity skin microbiota and Staphylococcus aureus dominance. The temporal transition the microbiome between early infancy dysbiosis AD is unknown.We randomly selected 50 children from Cork Babies After SCOPE: Evaluating Longitudinal Impact Using Neurological Nutritional Endpoints (BASELINE) longitudinal birth cohort for sampling at 3 points in first 6 months life 4 sites relevant to AD: antecubital popliteal fossae, nasal tip, cheek. We identified 10 infants compared them control no AD. performed bacterial 16S ribosomal RNA sequencing analysis directly clinical samples.Bacterial community structures diversity shifted over time, suggesting that age strongly affects infants. Unlike AD, these patients infantile did not have noticeably dysbiotic communities before or disease were colonized by S aureus. In comparing subjects, who had affected month 12 statistically significant differences on fossa 2 unaffected 12. particular, commensal staphylococci significantly less abundant 12, this genus might protect against later development AD.This study suggests 12-month-old having Additional studies needed confirm whether colonization modulates immunity attenuates

Language: Английский

Treg cell-based therapies: challenges and perspectives DOI
Caroline Raffin, Linda T. Vo, Jeffrey A. Bluestone

et al.

Nature reviews. Immunology, Journal Year: 2019, Volume and Issue: 20(3), P. 158 - 172

Published: Dec. 6, 2019

Language: Английский

Citations

544
The Dynamics of the Skin’s Immune System DOI Open Access
Alan V. Nguyen, Athena M. Soulika

International Journal of Molecular Sciences, Journal Year: 2019, Volume and Issue: 20(8), P. 1811 - 1811

Published: April 12, 2019

The skin is a complex organ that has devised numerous strategies, such as physical, chemical, and microbiological barriers, to protect the host from external insults. In addition, contains an intricate network of immune cells resident tissue, crucial for defense well tissue homeostasis. event insult, skin-resident are not only prevention infection but also reconstruction. Deregulation responses often leads impaired healing poor restoration function. this review, we will discuss defensive components focus on function in homeostasis their role wound healing.

Language: Английский

Citations

515
A Weaning Reaction to Microbiota Is Required for Resistance to Immunopathologies in the Adult DOI Creative Commons
Ziad Al Nabhani,

Sophie Dulauroy,

Rute Marques

et al.

Immunity, Journal Year: 2019, Volume and Issue: 50(5), P. 1276 - 1288.e5

Published: March 19, 2019

Language: Английский

Citations

492
Staphylococcus aureus and Staphylococcus epidermidis strain diversity underlying pediatric atopic dermatitis DOI Open Access
Allyson L. Byrd, Clay Deming,

Sara K. B. Cassidy

et al.

Science Translational Medicine, Journal Year: 2017, Volume and Issue: 9(397)

Published: July 5, 2017

Genomic and functional analyses of staphylococcal strain specificity reveal roles for microbes in human atopic dermatitis pathogenesis.

Language: Английский

Citations

475
Foxp3 and Toll-like receptor signaling balance Treg cell anabolic metabolism for suppression DOI
Valerie A. Gerriets, Rigel J. Kishton,

Marc O. Johnson

et al.

Nature Immunology, Journal Year: 2016, Volume and Issue: 17(12), P. 1459 - 1466

Published: Oct. 3, 2016

Language: Английский

Citations

462
MAIT cells are imprinted by the microbiota in early life and promote tissue repair DOI Open Access
Michael G. Constantinides, Verena M. Link,

Samira Tamoutounour

et al.

Science, Journal Year: 2019, Volume and Issue: 366(6464)

Published: Oct. 24, 2019

Commensals rule the MAITrix Mucosal-associated invariant T (MAIT) cells play an important role in mucosal homeostasis. MAIT recognize microbial small molecules presented by major histocompatibility complex class Ib molecule MR1. are absent germ-free mice, and mechanisms which microbiota control cell development unknown (see Perspective Oh Unutmaz). Legoux et al. show that, of within thymus is governed bacterial product 5-(2-oxopropylideneamino)-6- d -ribitylaminouracil, rapidly traffics from mucosa to thymus, where it captured MR1 developing cells. Constantinides report that induction only occurs during a limited, early-life window requires exposure defined microbes produce riboflavin derivatives. Continual interactions between commensals skin modulates tissue repair functions. Together, these papers highlight how can direct immune subsequent function at sites secreting compounds act like self-antigens. Science , this issue p. 494 eaax6624 ; see also 419

Language: Английский

Citations

439
Staphylococcus aureus and Atopic Dermatitis: A Complex and Evolving Relationship DOI
Joan A. Geoghegan, Alan D. Irvine, Timothy J. Foster

et al.

Trends in Microbiology, Journal Year: 2017, Volume and Issue: 26(6), P. 484 - 497

Published: Dec. 9, 2017

Language: Английский

Citations

415
The microbiome in patients with atopic dermatitis DOI Creative Commons
Amy S. Paller, Heidi H. Kong, Patrick C. Seed

et al.

Journal of Allergy and Clinical Immunology, Journal Year: 2018, Volume and Issue: 143(1), P. 26 - 35

Published: Nov. 23, 2018

As an interface with the environment, skin is a complex ecosystem colonized by many microorganisms that coexist in established balance. The cutaneous microbiome inhibits colonization pathogens, such as Staphylococcus aureus, and crucial component for function of epidermal barrier. Moreover, crosstalk between commensals immune system now recognized because can modulate both innate adaptive responses. Host-commensal interactions also have effect on developing infants and, subsequently, occurrence diseases, asthma atopic dermatitis (AD). Later life, contributes to development course disease. Accordingly, patients AD, decrease diversity correlates disease severity increased pathogenic bacteria, S aureus. Early clinical studies suggest topical application commensal organisms (eg, hominis or Roseomonas mucosa) reduces AD severity, which supports important role decreasing aureus AD. Advancing knowledge its modulating disorders, might result novel therapeutic strategies. A multitude microbiota inhabit our human epithelial surfaces. Although there increasing evidence these microbiota, live bodies, are health disease, functions consequences resident remain poorly understood. Given challenges being able adequately culture all microbes present given sample, technological advances genome sequencing ability interrogate microbiomes (the full collection microbiota). Several technical study composition collectively enlightened understanding pathogenesis (AD) modification (Fig 1).1Byrd A.L. Belkaid Y. Segre J.A. microbiome.Nat Rev Microbiol. 2018; 16: 143-155Crossref PubMed Scopus (917) Google Scholar animal models cannot fully recapitulate states, use model deeply investigate host-microbial relationships has elucidated intriguing biological mechanisms. continued integration gleaned from patient-derived models, will be critical approaches. 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Davis Young A.C. al.Topographical temporal microbiome.Science. 2009; 324: 1190-1192Crossref (1840) 4Oh Byrd NISC program al.Biogeography individuality shape metagenome.Nature. 2014; 514: 59-64Crossref (624) 5Costello E.K. Lauber C.L. Hamady M. Fierer N. Gordon J.I. Knight R. Bacterial community variation habitats across space time.Science. 326: 1694-1697Crossref (2181) hosts most diverse body, more than 1000 species 19 phyla.3Grice 6Kong molecular revolution biology: investigating microbiome.J Invest Dermatol. 2017; 137: e119-e122Abstract Full Text PDF (31) unique features specific some shared reflect physiology: sebaceous sites often Cutibacterium acnes (formerly known Propionibacterium acnes). Small adult volunteers shown relatively stable months years each person possess personalized microbiome.7Oh Park Comparative Sequencing Program Temporal stability microbiome.Cell. 2016; 165: 854-866Abstract (495) Studies demonstrated subjects at life stages. 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Language: Английский

Citations

411
Helper T cell differentiation DOI Open Access
Jordy Saravia, Nicole M. Chapman, Hongbo Chi

et al.

Cellular and Molecular Immunology, Journal Year: 2019, Volume and Issue: 16(7), P. 634 - 643

Published: March 12, 2019

Citations

395
Non-classical Immunity Controls Microbiota Impact on Skin Immunity and Tissue Repair DOI Creative Commons
Jonathan L. Linehan, Oliver J. Harrison,

Seong-Ji Han

et al.

Cell, Journal Year: 2018, Volume and Issue: 172(4), P. 784 - 796.e18

Published: Jan. 18, 2018

Language: Английский

Citations

394