Author
Listed:
- Sofia Sirvent
(University of Southampton)
- Andres F. Vallejo
(University of Southampton)
- Emma Corden
(University Hospital Southampton NHS Foundation Trust)
- Ying Teo
(University of Southampton
University Hospital Southampton NHS Foundation Trust)
- James Davies
(University of Southampton
University College London (UCL) Cancer Institute)
- Kalum Clayton
(University of Southampton)
- Eleanor G. Seaby
(University of Southampton)
- Chester Lai
(University of Southampton
University Hospital Southampton NHS Foundation Trust)
- Sarah Ennis
(University of Southampton)
- Rfeef Alyami
(University of Southampton)
- Gemma Douilhet
(University of Southampton)
- Lareb S. N. Dean
(University of Southampton)
- Matthew Loxham
(University of Southampton)
- Sarah Horswill
(University Hospital Southampton NHS Foundation Trust)
- Eugene Healy
(University of Southampton
University Hospital Southampton NHS Foundation Trust)
- Graham Roberts
(University Hospital Southampton NHS Foundation Trust
University of Southampton)
- Nigel J. Hall
(University Hospital Southampton NHS Foundation Trust
University of Southampton)
- Peter S. Friedmann
(University of Southampton)
- Harinder Singh
(The University of Pittsburgh)
- Clare L. Bennett
(University College London (UCL) Cancer Institute)
- Michael R Ardern-Jones
(University of Southampton
University Hospital Southampton NHS Foundation Trust
University of Southampton)
- Marta E. Polak
(University of Southampton
University of Southampton
Janssen R&D)
Abstract
Regulation of cutaneous immunity is severely compromised in inflammatory skin disease. To investigate the molecular crosstalk underpinning tolerance versus inflammation in atopic dermatitis, we utilise a human in vivo allergen challenge study, exposing atopic dermatitis patients to house dust mite. Here we analyse transcriptional programmes at the population and single cell levels in parallel with immunophenotyping of cutaneous immunocytes revealed a distinct dichotomy in atopic dermatitis patient responsiveness to house dust mite challenge. Our study shows that reactivity to house dust mite was associated with high basal levels of TNF-expressing cutaneous Th17 T cells, and documents the presence of hub structures where Langerhans cells and T cells co-localised. Mechanistically, we identify expression of metallothioneins and transcriptional programmes encoding antioxidant defences across all skin cell types, that appear to protect against allergen-induced inflammation. Furthermore, single nucleotide polymorphisms in the MTIX gene are associated with patients who did not react to house dust mite, opening up possibilities for therapeutic interventions modulating metallothionein expression in atopic dermatitis.
Suggested Citation
Sofia Sirvent & Andres F. Vallejo & Emma Corden & Ying Teo & James Davies & Kalum Clayton & Eleanor G. Seaby & Chester Lai & Sarah Ennis & Rfeef Alyami & Gemma Douilhet & Lareb S. N. Dean & Matthew Lo, 2023.
"Impaired expression of metallothioneins contributes to allergen-induced inflammation in patients with atopic dermatitis,"
Nature Communications, Nature, vol. 14(1), pages 1-14, December.
Handle:
RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-38588-1
DOI: 10.1038/s41467-023-38588-1
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