Microbiome Modulation in Acne Patients and Clinical Correlations

Marius-Anton Ionescu; Alin Laurentiu Tatu; Camelia Busila; Elena Roxana Axente; Nelly Badalato; Marc G. J. Feuilloley; Estelle Asquier; José Dario Martínez; Luc Lefeuvre

doi:10.3390/life14060688

Life (May 2024)

Microbiome Modulation in Acne Patients and Clinical Correlations

Marius-Anton Ionescu,
Alin Laurentiu Tatu,
Camelia Busila,
Elena Roxana Axente,
Nelly Badalato,
Marc G. J. Feuilloley,
Estelle Asquier,
José Dario Martínez,
Luc Lefeuvre

Affiliations

Marius-Anton Ionescu: Dermatology Department, University Hospital “Saint Louis”, University of Paris, 75010 Paris, France
Alin Laurentiu Tatu: Clinical Medical Department, Faculty of Medicine and Pharmacy, “Dunarea de Jos” University, 800008 Galati, Romania
Camelia Busila: Clinical Medical Department, Faculty of Medicine and Pharmacy, “Dunarea de Jos” University, 800008 Galati, Romania
Elena Roxana Axente: Faculty of Medicine and Pharmacy, “Dunarea de Jos” University, 35 AI I Cuza St., 800010 Galati, Romania
Nelly Badalato: GenoScreen, 59000 Lille, France
Marc G. J. Feuilloley: Research Unit UR4312 CBSA, University Rouen, 27000 Evreux, France
Estelle Asquier: Laboratoires Dermatologiques d’Uriage, 92200 Neuilly sur-Seine, France
José Dario Martínez: Department of Internal Medicine, Faculty of Medicine, Hospital Universitario José Eleuterio González, Universidad Autónoma de Nuevo León, Monterrey 64460, Mexico
Luc Lefeuvre: Laboratoires Dermatologiques d’Uriage, 92200 Neuilly sur-Seine, France

DOI: https://doi.org/10.3390/life14060688
Journal volume & issue: Vol. 14, no. 6
p. 688

Abstract

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Background: The imbalance of skin microbiota in acne can induce changes leading to induction or to aggravation of chronic inflammatory lesions; complex mechanisms are involved. Cutibacterium acnes (C. acnes) ribotypes RT4 and RT5 express more biofilm and are associated with inflammatory acne lesions. C. acnes RT6 is a non-acne ribotype, beneficial for the skin. Objectives: In an open clinical trial, acne adults were included and assessed clinically at baseline and at month 2 using the Investigator Global Assessment of Acne (IGA) score. A topical emulsion was applied twice daily for 2 months (M2) in each included patient. In the same series of acne patients, skin swab samples were collected from acne patients at baseline and M2 from lesional and non-lesional skin; skin swabs were collected for the metagenomic long-read analysis of microbiota. Materials and Methods: Acne patients with a gravity score IGA of >1Umbelliferae associated with a polysaccharide at 1% was applied twice daily for 2 months. At baseline and M2 clinical assessments were made; skin swab samples were also taken for microbiota analysis from lesional and non-lesional skin in each included patient. Extractions of genomic DNA (gDNA) from swab samples from baseline and from M2 were made, followed by full-length (V1–V9) amplification of the 16S rDNA and sequencing of amplicon libraries for strain-level bacterial community profiling. Results: In a series of 32 adult acne patients, the mean initial IGA scale was 3.1; at M2 the IGA scale was 1.5 (p C. acnes followed by Staphylococcus epidermidis (S. epidermidis). The density of C. acnes ribotypes RT6 (non-acne strain) was increased at M2 compared to baseline and the density of ribotypes C. acnes RT1 to RT5 was decreased at M2, compared to baseline (p S. epidermidis ribotypes (1 to 36) were non significantly increased at M2, compared to baseline (p Umbelliferae and a polysaccharide at 1% twice daily, a significant clinical improvement in IGA scale for acne lesions was seen at M2, compared to baseline (p C. acnes ribotype 6 and of the decrease in the relative abundance of acne strains ribotypes C. acnes RT1 to RT5.

Published in Life

ISSN: 2075-1729 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Science
Website: http://www.mdpi.com/journal/life

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