Longitudinal Study of the Psoriasis-Associated Skin Microbiome During Therapy with Ustekinumab in A Randomized Phase 3b Clinical Trial

Overview

Journal J Invest Dermatol

Publisher Elsevier

Specialty Dermatology

Date 2018 Mar 22

PMID 29559344

Citations 29

Authors

Michael A Loesche

Kamyar Farahi

Kimberly Capone

Steven Fakharzadeh

Andrew Blauvelt

Kristina Callis Duffin

Samuel E DePrimo

Ernesto J Munoz-Elias

Carrie Brodmerkel

Bidisha Dasgupta

Marc Chevrier

Kevin Smith

Joseph Horwinski

Amanda Tyldsley

Elizabeth A Grice

Affiliations

Soon will be listed here.

Abstract

Plaque psoriasis, a chronic inflammatory disease primarily affecting the skin, is thought to have a multifactorial etiology, including innate immune system dysregulation, environmental triggers, and genetic susceptibility. We sought to further understand the role of skin microbiota in psoriasis pathogenesis, as well as their response to therapy. We systematically analyzed dynamic microbiota colonizing psoriasis lesions and adjacent nonlesional skin in 114 patients prior to and during ustekinumab treatment in a phase 3b clinical trial. By sequencing the bacterial 16S ribosomal RNA gene from skin swab samples obtained at six anatomical sites, we identified minor, site-specific differences in microbial diversity and composition between pretreatment lesional and nonlesional skin. During therapy, microbial communities within lesional and nonlesional skin diverged, and body-site dispersion increased, reflecting microbial skin site-specificity. Microbiota demonstrated greater pretreatment heterogeneity in psoriatic lesions than in nonlesional skin, and variance increased as treatment progressed. Microbiota colonizing recurrent lesions did not overlap with pretreatment lesional microbiota, suggesting colonization patterns varied between initial and recurrent psoriatic lesions. While plaque psoriasis does not appear to be associated with specific microbes and/or microbial diversity, this large dataset provides insight into microbial variation associated with (i) disease in different body locations, (ii) initial versus recurrent lesions, and (iii) anti-IL12/23 therapy.

Citing Articles

IL-12 family cytokines and autoimmune diseases: A potential therapeutic target?.

Cui X, Liu W, Jiang H, Zhao Q, Hu Y, Tang X J Transl Autoimmun. 2025; 10:100263.

PMID: 39759268 PMC: 11697604. DOI: 10.1016/j.jtauto.2024.100263.

The healing process of diabetic ulcers correlates with changes in the cutaneous microbiota.

Bruni E, Scaglione G, Tampone D, Primerano A, Bartolini B, Tenoglio C Sci Rep. 2024; 14(1):27628.

PMID: 39528566 PMC: 11554885. DOI: 10.1038/s41598-024-77987-2.

The Contribution of the Skin Microbiome to Psoriasis Pathogenesis and Its Implications for Therapeutic Strategies.

Radaschin D, Tatu A, Iancu A, Beiu C, Popa L Medicina (Kaunas). 2024; 60(10).

PMID: 39459406 PMC: 11509136. DOI: 10.3390/medicina60101619.

Decrypting Skin Microbiome in Psoriasis: Current Status.

Arya P, Kaur M, Chosyang S, Kushwaha N, Singh B J Psoriasis Psoriatic Arthritis. 2024; 8(4):166-178.

PMID: 39301472 PMC: 11361554. DOI: 10.1177/24755303231194293.

Alterations in the Skin Microbiome in Dermatologic Diseases and with External Exposures: CME Part 2.

MacGibeny M, Adjei S, Pyle H, Bunick C, Ghannoum M, Grada A J Am Acad Dermatol. 2024; .

PMID: 39173885 PMC: 11839956. DOI: 10.1016/j.jaad.2024.07.1499.