Blood Single-Cell Transcriptomic and Proteomic Signatures of Paradoxical Eczema in Patients with Psoriasis Treated with Biologics

Ali Al-Janabi; Paul Martin; Catherine Simpson; Hefin Rhys; Adnan R. Khan; Steve Eyre; Maria Christofi; Amy C. Foulkes; Andrew Skelton; Sebastien Viatte; Anne Barton; Andrew P. Morris; Catherine H. Smith; Christopher E.M. Griffiths; Richard B. Warren

doi:10.1016/j.jid.2025.02.153

Blood Single-Cell Transcriptomic and Proteomic Signatures of Paradoxical Eczema in Patients with Psoriasis Treated with Biologics

Ali Al-Janabi, Paul Martin, Catherine Simpson, Hefin Rhys, Adnan R. Khan, Steve Eyre, Maria Christofi, Amy C. Foulkes, Andrew Skelton, Sebastien Viatte, Anne Barton, Andrew P. Morris, Catherine H. Smith, Christopher E.M. Griffiths, Richard B. Warren

Division of Musculoskeletal & Dermatological Sciences (L5)

Research output: Contribution to journal › Article › peer-review

Abstract

Biologics targeting the TNF and IL-17/23 axis are highly effective treatments for psoriasis but can result in cutaneous adverse events. The pathogenesis of paradoxical eczema, the occurrence of an atopic dermatitis phenotype after biologic initiation in people with psoriasis, is unknown. Using single-cell RNA sequencing and mass cytometry, we found increased expression of TNF, IFN-γ, and IFN-α and their signaling pathways in paradoxical eczema case cell clusters compared with that in matched psoriasis controls. Genetic variants influencing the expression of chemokine signaling and TNF pathway genes were associated with paradoxical eczema in a separate genotyped cohort, and this association was independent of known atopic risk loci. This suggests that paradoxical eczema has a predominantly type 1 systemic inflammatory signature and that genetic susceptibility to aberrant chemokine and TNF pathway signaling could contribute to development of this phenotype during biologic treatment.

Original language	English
Journal	Journal of Investigative Dermatology
Early online date	27 Mar 2025
DOIs	https://doi.org/10.1016/j.jid.2025.02.153
Publication status	E-pub ahead of print - 27 Mar 2025

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10.1016/j.jid.2025.02.153Licence: CC BY

NIHR Manchester Biomedical Research Centre
Bruce, I. (PI), Lord, G. (CoI), Lennon, R. (CoI), Black, G. (CoI), Wedge, D. (CoI), Morris, A. (CoI), Hussell, T. (CoI), Sharrocks, A. (CoI), Stivaros, S. (CoI), Buch, M. (CoI), Gough, J. (CoI), Kostarelos, K. (CoI), Thistlethwaite, F. (CoI), Kadler, K. (CoI), Barton, A. (CoI), Hyrich, K. (CoI), Mcbeth, J. (CoI), O'Neill, T. (CoI), Vestbo, J. (CoI), Simpson, A. (CoI), Singh, S. (CoI), Smith, J. (CoI), Felton, T. (CoI), Murray, C. (CoI), Griffiths, C. (CoI), Cullum, N. (CoI), Rhodes, L. (CoI), Warren, R. (CoI), Paus, R. (CoI), Dumville, J. (CoI), Viros Usandizaga, A. (CoI), Keavney, B. (CoI), Tomaszewski, M. (CoI), Allan, S. (CoI), Body, R. (CoI), Cartwright, E. (CoI), Heagerty, A. (CoI), Kalra, P. (CoI), Miller, C. (CoI), Rutter, M. (CoI), Smith, C. (CoI), Trafford, A. (CoI), Evans, D. (CoI), Crosbie, E. (CoI), Crosbie, P. (CoI), Harvie, M. (CoI), Howell, S. (CoI), Renehan, A. (CoI), Dive, C. (CoI), Blackhall, F. (CoI), Landers, D. (CoI), Krebs, M. (CoI), Cook, N. (CoI), Clarke, R. (CoI), Taylor, S. (CoI), Jorgensen, C. (CoI), Lorigan, P. (CoI), Jayson, G. (CoI), Valle, J. (CoI), Mccabe, M. (CoI), Armstrong, A. (CoI), Freitas, A. (CoI), Illidge, T. (CoI), Choudhury, A. (CoI), Hoskin, P. (CoI), West, C. (CoI), Van Herk, M. (CoI), Faivre-Finn, C. (CoI), Bristow, R. (CoI), Kirkby, K. (CoI), Birtle, A. (CoI), Mackay, R. (CoI), Radford, J. (CoI), Linton, K. (CoI), Higham, C. (CoI), Munro, K. (CoI), Plack, C. (CoI), Arden Armitage, C. (CoI), Bruce, I. (CoI), Moore, D. (CoI), Saunders, G. (CoI), Stone, M. (CoI), Haddock, G. (CoI), Lewis, S. (CoI), Elliott, R. (CoI), Green, J. (CoI), Lovell, K. (CoI), Morrison, A. (CoI), Shaw, J. (CoI), Bucci, S. (CoI), Ainsworth, J. (CoI), Webb, R. (CoI), Newman, W. (CoI), Banka, S. (CoI), Clayton-Smith, J. (CoI), Payne, K. (CoI), Moldovan, R. (CoI), Wynn, R. (CoI) & Jones, S. (CoI)
1/12/22 → 30/11/27
Project: Research

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Al-Janabi, A., Martin, P., Simpson, C., Rhys, H., Khan, A. R., Eyre, S., Christofi, M., Foulkes, A. C., Skelton, A., Viatte, S., Barton, A., Morris, A. P., Smith, C. H., Griffiths, C. E. M., & Warren, R. B. (2025). Blood Single-Cell Transcriptomic and Proteomic Signatures of Paradoxical Eczema in Patients with Psoriasis Treated with Biologics. Journal of Investigative Dermatology. Advance online publication. https://doi.org/10.1016/j.jid.2025.02.153

@article{c63e393e3f5e41dcbd92ea20cb48e9dd,

title = "Blood Single-Cell Transcriptomic and Proteomic Signatures of Paradoxical Eczema in Patients with Psoriasis Treated with Biologics",

abstract = "Biologics targeting the TNF and IL-17/23 axis are highly effective treatments for psoriasis but can result in cutaneous adverse events. The pathogenesis of paradoxical eczema, the occurrence of an atopic dermatitis phenotype after biologic initiation in people with psoriasis, is unknown. Using single-cell RNA sequencing and mass cytometry, we found increased expression of TNF, IFN-γ, and IFN-α and their signaling pathways in paradoxical eczema case cell clusters compared with that in matched psoriasis controls. Genetic variants influencing the expression of chemokine signaling and TNF pathway genes were associated with paradoxical eczema in a separate genotyped cohort, and this association was independent of known atopic risk loci. This suggests that paradoxical eczema has a predominantly type 1 systemic inflammatory signature and that genetic susceptibility to aberrant chemokine and TNF pathway signaling could contribute to development of this phenotype during biologic treatment.",

author = "Ali Al-Janabi and Paul Martin and Catherine Simpson and Hefin Rhys and Khan, \{Adnan R.\} and Steve Eyre and Maria Christofi and Foulkes, \{Amy C.\} and Andrew Skelton and Sebastien Viatte and Anne Barton and Morris, \{Andrew P.\} and Smith, \{Catherine H.\} and Griffiths, \{Christopher E.M.\} and Warren, \{Richard B.\}",

year = "2025",

month = mar,

day = "27",

doi = "10.1016/j.jid.2025.02.153",

language = "English",

journal = "Journal of Investigative Dermatology",

issn = "0022-202X",

publisher = "Elsevier BV",

}

Al-Janabi, A, Martin, P, Simpson, C, Rhys, H, Khan, AR, Eyre, S, Christofi, M, Foulkes, AC, Skelton, A, Viatte, S , Barton, A, Morris, AP, Smith, CH, Griffiths, CEM & Warren, RB 2025, 'Blood Single-Cell Transcriptomic and Proteomic Signatures of Paradoxical Eczema in Patients with Psoriasis Treated with Biologics', Journal of Investigative Dermatology. https://doi.org/10.1016/j.jid.2025.02.153

TY - JOUR

T1 - Blood Single-Cell Transcriptomic and Proteomic Signatures of Paradoxical Eczema in Patients with Psoriasis Treated with Biologics

AU - Al-Janabi, Ali

AU - Martin, Paul

AU - Simpson, Catherine

AU - Rhys, Hefin

AU - Khan, Adnan R.

AU - Eyre, Steve

AU - Christofi, Maria

AU - Foulkes, Amy C.

AU - Skelton, Andrew

AU - Viatte, Sebastien

AU - Barton, Anne

AU - Morris, Andrew P.

AU - Smith, Catherine H.

AU - Griffiths, Christopher E.M.

AU - Warren, Richard B.

PY - 2025/3/27

Y1 - 2025/3/27

N2 - Biologics targeting the TNF and IL-17/23 axis are highly effective treatments for psoriasis but can result in cutaneous adverse events. The pathogenesis of paradoxical eczema, the occurrence of an atopic dermatitis phenotype after biologic initiation in people with psoriasis, is unknown. Using single-cell RNA sequencing and mass cytometry, we found increased expression of TNF, IFN-γ, and IFN-α and their signaling pathways in paradoxical eczema case cell clusters compared with that in matched psoriasis controls. Genetic variants influencing the expression of chemokine signaling and TNF pathway genes were associated with paradoxical eczema in a separate genotyped cohort, and this association was independent of known atopic risk loci. This suggests that paradoxical eczema has a predominantly type 1 systemic inflammatory signature and that genetic susceptibility to aberrant chemokine and TNF pathway signaling could contribute to development of this phenotype during biologic treatment.

AB - Biologics targeting the TNF and IL-17/23 axis are highly effective treatments for psoriasis but can result in cutaneous adverse events. The pathogenesis of paradoxical eczema, the occurrence of an atopic dermatitis phenotype after biologic initiation in people with psoriasis, is unknown. Using single-cell RNA sequencing and mass cytometry, we found increased expression of TNF, IFN-γ, and IFN-α and their signaling pathways in paradoxical eczema case cell clusters compared with that in matched psoriasis controls. Genetic variants influencing the expression of chemokine signaling and TNF pathway genes were associated with paradoxical eczema in a separate genotyped cohort, and this association was independent of known atopic risk loci. This suggests that paradoxical eczema has a predominantly type 1 systemic inflammatory signature and that genetic susceptibility to aberrant chemokine and TNF pathway signaling could contribute to development of this phenotype during biologic treatment.

U2 - 10.1016/j.jid.2025.02.153

DO - 10.1016/j.jid.2025.02.153

M3 - Article

SN - 0022-202X

JO - Journal of Investigative Dermatology

JF - Journal of Investigative Dermatology

ER -

Blood Single-Cell Transcriptomic and Proteomic Signatures of Paradoxical Eczema in Patients with Psoriasis Treated with Biologics

Abstract

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NIHR Manchester Biomedical Research Centre

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