Integrated proteomics and genomics analysis of paradoxical eczema in psoriasis patients treated with biologics

Ali Al-Janabi; Paul Martin; Adnan R. Khan; Amy C. Foulkes; Catherine H. Smith; Christopher E.M. Griffiths; Andrew P. Morris; Steve Eyre; Richard B. Warren; BSTOP Study Group and the BADBIR Study Group

doi:10.1016/j.jaci.2023.07.011

Integrated proteomics and genomics analysis of paradoxical eczema in psoriasis patients treated with biologics

Ali Al-Janabi^*, Paul Martin, Adnan R. Khan, Amy C. Foulkes, Catherine H. Smith, Christopher E.M. Griffiths, Andrew P. Morris, Steve Eyre, Richard B. Warren, BSTOP Study Group and the BADBIR Study Group

^*Corresponding author for this work

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

Abstract

Background: Few studies have explored the immunology and genetic risk of paradoxical eczema occurring as an adverse event of biologic therapy in patients with psoriasis. Objectives: We sought to describe the systemic inflammatory signature of paradoxical eczema using proteomics and explore whether this is genetically mediated. Methods: This study used the Olink Target 96 Inflammation panel on 256 serum samples from 71 patients with psoriasis and paradoxical eczema, and 75 controls with psoriasis to identify differentially expressed proteins and enriched gene sets. Case samples from 1 or more time points (T1 prebiologic, T2 postbiologic, and T3 postparadoxical eczema) were matched 1:1 with control samples. Genes contributing to enriched gene sets were selected, and functional single nucleotide polymorphisms used to create polygenic risk scores in a genotyped cohort of 88 paradoxical eczema cases and 3124 psoriasis controls. Results: STAMBP expression was lower in cases at T1 than in controls (log-fold change: −0.44; adjusted P = .022); no other proteins reached statistical significance at equivalent time points. Eleven gene sets including cytokine and chemokine pathways were enriched in cases at T2 and 10 at T3. Of the 39 proteins contributing to enriched gene sets, the majority are associated with the atopic dermatitis serum proteome. A polygenic risk score including 38 functional single nucleotide polymorphisms linked to enriched gene sets was associated with paradoxical eczema (adjusted P = .046). Conclusions: The paradoxical eczema systemic inflammatory proteome trends toward atopic dermatitis at a gene-set level and is detectable before onset of the phenotype. This signature could be genetically determined.

Original language	English
Pages (from-to)	1237-1246
Number of pages	10
Journal	Journal of Allergy and Clinical Immunology
Volume	152
Issue number	5
Early online date	1 Aug 2023
DOIs	https://doi.org/10.1016/j.jaci.2023.07.011
Publication status	Published - Nov 2023

Keywords / Materials (for Non-textual outputs)

atopic dermatitis
genomics
paradoxical eczema
polygenic risk score
proteomics
Psoriasis

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Al-Janabi, A., Martin, P., Khan, A. R., Foulkes, A. C., Smith, C. H., Griffiths, C. E. M., Morris, A. P., Eyre, S., Warren, R. B., & BSTOP Study Group and the BADBIR Study Group (2023). Integrated proteomics and genomics analysis of paradoxical eczema in psoriasis patients treated with biologics. Journal of Allergy and Clinical Immunology, 152(5), 1237-1246. https://doi.org/10.1016/j.jaci.2023.07.011

@article{01d43fcc9aa84dba80eb10609c1700ce,

title = "Integrated proteomics and genomics analysis of paradoxical eczema in psoriasis patients treated with biologics",

abstract = "Background: Few studies have explored the immunology and genetic risk of paradoxical eczema occurring as an adverse event of biologic therapy in patients with psoriasis. Objectives: We sought to describe the systemic inflammatory signature of paradoxical eczema using proteomics and explore whether this is genetically mediated. Methods: This study used the Olink Target 96 Inflammation panel on 256 serum samples from 71 patients with psoriasis and paradoxical eczema, and 75 controls with psoriasis to identify differentially expressed proteins and enriched gene sets. Case samples from 1 or more time points (T1 prebiologic, T2 postbiologic, and T3 postparadoxical eczema) were matched 1:1 with control samples. Genes contributing to enriched gene sets were selected, and functional single nucleotide polymorphisms used to create polygenic risk scores in a genotyped cohort of 88 paradoxical eczema cases and 3124 psoriasis controls. Results: STAMBP expression was lower in cases at T1 than in controls (log-fold change: −0.44; adjusted P = .022); no other proteins reached statistical significance at equivalent time points. Eleven gene sets including cytokine and chemokine pathways were enriched in cases at T2 and 10 at T3. Of the 39 proteins contributing to enriched gene sets, the majority are associated with the atopic dermatitis serum proteome. A polygenic risk score including 38 functional single nucleotide polymorphisms linked to enriched gene sets was associated with paradoxical eczema (adjusted P = .046). Conclusions: The paradoxical eczema systemic inflammatory proteome trends toward atopic dermatitis at a gene-set level and is detectable before onset of the phenotype. This signature could be genetically determined.",

keywords = "atopic dermatitis, genomics, paradoxical eczema, polygenic risk score, proteomics, Psoriasis",

author = "Ali Al-Janabi and Paul Martin and Khan, \{Adnan R.\} and Foulkes, \{Amy C.\} and Smith, \{Catherine H.\} and Griffiths, \{Christopher E.M.\} and Morris, \{Andrew P.\} and Steve Eyre and Warren, \{Richard B.\} and \{BSTOP Study Group and the BADBIR Study Group\} and Shehnaz Ahmed and Oras Alabas and Jonathan Barker and Gabrielle Becher and Anthony Bewley and Ian Evans and Philip Hampton and Brian Kirby and Elise Kleyn and Philip Laws and Linda Lawson and Teena Mackenzie and Kathleen McElhone and Tess McPherson and Simon Morrison and Caroline Owen and Eleanor Pearson and Amir Rashid and Nick Reynolds and Anja Strangfeld and Shernaz Walton and Zenas Yiu and Girish Gupta and Anja Strangfeld and Richard Weller and Vera Zietemann and Nadia Aldoori and Mahmud Ali and Ahmed Al-Rusan and Caroline Angit and Alex Anstey and Fiona Antony and Charles Archer and Suzanna August and Periasamy Balasubramaniam and David Baudry and Kay Baxter and Alexandra Bonsall and Sara Brown and Victoria Brown and David Burden and Ekaterina Burova and Aamir Butt and Mel Caswell and Anna Chapman and Sandeep Cliff and Mihaela Costache and Sharmela Darne and Claudia DeGiovanni and Trupti Desai and Victoria Diba and Eva Domanne and Michael Duckworth and Harvey Dymond and Caoimhe Fahy and Susanne Farwer and Leila Ferguson and Gkini, \{Maria Angeliki\} and Alison Godwin and Jon Goulding and Fiona Hammonds and Shaheen Haque and Caroline Higgins and Sue Hood and Teresa Joseph and Sarah Johnson and Manju Kalavala and Mohsen Khorshid and Liberta Labinoti and Ruth Lamb and Nicole Lawson and Alison Layton and Tara Lees and Nick Levell and Helen Lewis and Chris Lovell and Calum Lyon and Helen McAteer and Sandy McBride and Sally McCormack and Kevin McKenna and Serap Mellor and Fiona Meredith and Ruth Murphy and Paul Norris and Richard Parslew and Gay Perera and Nabil Ponnambath and Urvi Popli and James Powell and Raakhee Ramesh and Helen Ramsay and Aruni Ranasinghe and Saskia Reeken and Rebecca Rose and Rada Rotarescu and Ingrid Salvary and Kathy Sands and Tapati Sinha and Julia Schofield and Alexa Shipman and Stefan Siebert and Simina Stefanescu and Kavitha Sundararaj and Kathy Taghipour and Michelle Taylor and Michelle Thomson and Joanne Topliffe and Roberto Verdolini and Rachel Wachsmuth and Martin Wade and Shymal Wahie and Sarah Walsh and Louise Wilcox and Diane Williamson and Andrew Wright",

year = "2023",

month = nov,

doi = "10.1016/j.jaci.2023.07.011",

language = "English",

volume = "152",

pages = "1237--1246",

journal = "Journal of Allergy and Clinical Immunology",

issn = "0091-6749",

publisher = "Elsevier",

number = "5",

}

Al-Janabi, A, Martin, P, Khan, AR, Foulkes, AC, Smith, CH, Griffiths, CEM, Morris, AP, Eyre, S, Warren, RB & BSTOP Study Group and the BADBIR Study Group 2023, 'Integrated proteomics and genomics analysis of paradoxical eczema in psoriasis patients treated with biologics', Journal of Allergy and Clinical Immunology, vol. 152, no. 5, pp. 1237-1246. https://doi.org/10.1016/j.jaci.2023.07.011

TY - JOUR

T1 - Integrated proteomics and genomics analysis of paradoxical eczema in psoriasis patients treated with biologics

AU - Al-Janabi, Ali

AU - Martin, Paul

AU - Khan, Adnan R.

AU - Foulkes, Amy C.

AU - Smith, Catherine H.

AU - Griffiths, Christopher E.M.

AU - Morris, Andrew P.

AU - Eyre, Steve

AU - Warren, Richard B.

AU - BSTOP Study Group and the BADBIR Study Group

AU - Ahmed, Shehnaz

AU - Alabas, Oras

AU - Barker, Jonathan

AU - Becher, Gabrielle

AU - Bewley, Anthony

AU - Evans, Ian

AU - Hampton, Philip

AU - Kirby, Brian

AU - Kleyn, Elise

AU - Laws, Philip

AU - Lawson, Linda

AU - Mackenzie, Teena

AU - McElhone, Kathleen

AU - McPherson, Tess

AU - Morrison, Simon

AU - Owen, Caroline

AU - Pearson, Eleanor

AU - Rashid, Amir

AU - Reynolds, Nick

AU - Strangfeld, Anja

AU - Walton, Shernaz

AU - Yiu, Zenas

AU - Gupta, Girish

AU - Strangfeld, Anja

AU - Weller, Richard

AU - Zietemann, Vera

AU - Aldoori, Nadia

AU - Ali, Mahmud

AU - Al-Rusan, Ahmed

AU - Angit, Caroline

AU - Anstey, Alex

AU - Antony, Fiona

AU - Archer, Charles

AU - August, Suzanna

AU - Balasubramaniam, Periasamy

AU - Baudry, David

AU - Baxter, Kay

AU - Bonsall, Alexandra

AU - Brown, Sara

AU - Brown, Victoria

AU - Burden, David

AU - Burova, Ekaterina

AU - Butt, Aamir

AU - Caswell, Mel

AU - Chapman, Anna

AU - Cliff, Sandeep

AU - Costache, Mihaela

AU - Darne, Sharmela

AU - DeGiovanni, Claudia

AU - Desai, Trupti

AU - Diba, Victoria

AU - Domanne, Eva

AU - Duckworth, Michael

AU - Dymond, Harvey

AU - Fahy, Caoimhe

AU - Farwer, Susanne

AU - Ferguson, Leila

AU - Gkini, Maria Angeliki

AU - Godwin, Alison

AU - Goulding, Jon

AU - Hammonds, Fiona

AU - Haque, Shaheen

AU - Higgins, Caroline

AU - Hood, Sue

AU - Joseph, Teresa

AU - Johnson, Sarah

AU - Kalavala, Manju

AU - Khorshid, Mohsen

AU - Labinoti, Liberta

AU - Lamb, Ruth

AU - Lawson, Nicole

AU - Layton, Alison

AU - Lees, Tara

AU - Levell, Nick

AU - Lewis, Helen

AU - Lovell, Chris

AU - Lyon, Calum

AU - McAteer, Helen

AU - McBride, Sandy

AU - McCormack, Sally

AU - McKenna, Kevin

AU - Mellor, Serap

AU - Meredith, Fiona

AU - Murphy, Ruth

AU - Norris, Paul

AU - Parslew, Richard

AU - Perera, Gay

AU - Ponnambath, Nabil

AU - Popli, Urvi

AU - Powell, James

AU - Ramesh, Raakhee

AU - Ramsay, Helen

AU - Ranasinghe, Aruni

AU - Reeken, Saskia

AU - Rose, Rebecca

AU - Rotarescu, Rada

AU - Salvary, Ingrid

AU - Sands, Kathy

AU - Sinha, Tapati

AU - Schofield, Julia

AU - Shipman, Alexa

AU - Siebert, Stefan

AU - Stefanescu, Simina

AU - Sundararaj, Kavitha

AU - Taghipour, Kathy

AU - Taylor, Michelle

AU - Thomson, Michelle

AU - Topliffe, Joanne

AU - Verdolini, Roberto

AU - Wachsmuth, Rachel

AU - Wade, Martin

AU - Wahie, Shymal

AU - Walsh, Sarah

AU - Wilcox, Louise

AU - Williamson, Diane

AU - Wright, Andrew

PY - 2023/11

Y1 - 2023/11

N2 - Background: Few studies have explored the immunology and genetic risk of paradoxical eczema occurring as an adverse event of biologic therapy in patients with psoriasis. Objectives: We sought to describe the systemic inflammatory signature of paradoxical eczema using proteomics and explore whether this is genetically mediated. Methods: This study used the Olink Target 96 Inflammation panel on 256 serum samples from 71 patients with psoriasis and paradoxical eczema, and 75 controls with psoriasis to identify differentially expressed proteins and enriched gene sets. Case samples from 1 or more time points (T1 prebiologic, T2 postbiologic, and T3 postparadoxical eczema) were matched 1:1 with control samples. Genes contributing to enriched gene sets were selected, and functional single nucleotide polymorphisms used to create polygenic risk scores in a genotyped cohort of 88 paradoxical eczema cases and 3124 psoriasis controls. Results: STAMBP expression was lower in cases at T1 than in controls (log-fold change: −0.44; adjusted P = .022); no other proteins reached statistical significance at equivalent time points. Eleven gene sets including cytokine and chemokine pathways were enriched in cases at T2 and 10 at T3. Of the 39 proteins contributing to enriched gene sets, the majority are associated with the atopic dermatitis serum proteome. A polygenic risk score including 38 functional single nucleotide polymorphisms linked to enriched gene sets was associated with paradoxical eczema (adjusted P = .046). Conclusions: The paradoxical eczema systemic inflammatory proteome trends toward atopic dermatitis at a gene-set level and is detectable before onset of the phenotype. This signature could be genetically determined.

AB - Background: Few studies have explored the immunology and genetic risk of paradoxical eczema occurring as an adverse event of biologic therapy in patients with psoriasis. Objectives: We sought to describe the systemic inflammatory signature of paradoxical eczema using proteomics and explore whether this is genetically mediated. Methods: This study used the Olink Target 96 Inflammation panel on 256 serum samples from 71 patients with psoriasis and paradoxical eczema, and 75 controls with psoriasis to identify differentially expressed proteins and enriched gene sets. Case samples from 1 or more time points (T1 prebiologic, T2 postbiologic, and T3 postparadoxical eczema) were matched 1:1 with control samples. Genes contributing to enriched gene sets were selected, and functional single nucleotide polymorphisms used to create polygenic risk scores in a genotyped cohort of 88 paradoxical eczema cases and 3124 psoriasis controls. Results: STAMBP expression was lower in cases at T1 than in controls (log-fold change: −0.44; adjusted P = .022); no other proteins reached statistical significance at equivalent time points. Eleven gene sets including cytokine and chemokine pathways were enriched in cases at T2 and 10 at T3. Of the 39 proteins contributing to enriched gene sets, the majority are associated with the atopic dermatitis serum proteome. A polygenic risk score including 38 functional single nucleotide polymorphisms linked to enriched gene sets was associated with paradoxical eczema (adjusted P = .046). Conclusions: The paradoxical eczema systemic inflammatory proteome trends toward atopic dermatitis at a gene-set level and is detectable before onset of the phenotype. This signature could be genetically determined.

KW - atopic dermatitis

KW - genomics

KW - paradoxical eczema

KW - polygenic risk score

KW - proteomics

KW - Psoriasis

UR - https://www.scopus.com/pages/publications/85169840584

U2 - 10.1016/j.jaci.2023.07.011

DO - 10.1016/j.jaci.2023.07.011

M3 - Article

C2 - 37536512

AN - SCOPUS:85169840584

SN - 0091-6749

VL - 152

SP - 1237

EP - 1246

JO - Journal of Allergy and Clinical Immunology

JF - Journal of Allergy and Clinical Immunology

IS - 5

ER -

Integrated proteomics and genomics analysis of paradoxical eczema in psoriasis patients treated with biologics

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