Biomarkers of systemic treatment response in people with psoriasis: a scoping review

Author:

Corbett Mark1,Ramessur Ravi2ORCID,Marshall David1,Acencio Marcio L.3ORCID,Ostaszewski Marek3,Barbosa Ines A.2,Dand Nick4ORCID,Di Meglio Paola2ORCID,Haddad Salma5,Jensen Andreas H.M.6ORCID,Koopmann Witte7,Mahil Satveer K.2,Rahmatulla Seher8ORCID,Rastrick Joe9,Saklatvala Jake4,Weidinger Stephan10ORCID,Wright Kath1,Eyerich Kilian1112,Barker Jonathan N.2,Ndlovu Matladi9,Conrad Curdin13,Skov Lone14ORCID,Smith Catherine H.2,

Affiliation:

1. Centre for Reviews and Dissemination University of York York UK

2. St John’s Institute of Dermatology, School of Basic & Medical Biosciences, Faculty of Life Sciences & Medicine King’s College London London UK

3. Luxembourg Centre for Systems Biomedicine University of Luxembourg Esch-sur-Alzette Luxembourg

4. Department of Medical & Molecular Genetics, School of Basic & Medical Biosciences, Faculty of Life Sciences & Medicine King’s College London London UK

5. University College Hospital NHS Trust London UK

6. University of Copenhagen Copenhagen Denmark

7. Department of Translational Medicine LEO Pharma A/S Ballerup Denmark

8. West Hertfordshire NHS Trust Watford UK

9. Department of Immunology Research UCB Brussels Belgium

10. Department of Dermatology and Allergy University Hospital Schleswig-Holstein Kiel Germany

11. Department of Dermatology and Allergy Technical University of Munich Munich Germany

12. Division of Dermatology, Department of Medicine Karolinska Institutet Stockholm Sweden

13. Department of Dermatology Lausanne University Hospital CHUV & University of Lausanne Lausanne Switzerland

14. Department of Dermatology and Allergy, Herlev and Gentofte Hospital, Department of Clinical Medicine University of Copenhagen Copenhagen Denmark

Abstract

Abstract Background Responses to the systemic treatments commonly used to treat psoriasis vary. Biomarkers that accurately predict effectiveness and safety would enable targeted treatment selection, improved patient outcomes and more cost-effective healthcare. Objectives To perform a scoping review to identify and catalogue candidate biomarkers of systemic treatment response in psoriasis for the translational research community. Methods A systematic search of CENTRAL, Embase, LILACS and MEDLINE was performed for relevant articles published between 1990 and December 2021. Eligibility criteria were studies involving patients with psoriasis (any age, n ≥ 50) reporting biomarkers associated with systemic treatment response. The main outcomes were any measure of systemic treatment efficacy or safety. Data were extracted by one reviewer and checked by a second; studies meeting minimal quality criteria (use of methods to control for confounding) were formally assessed for bias. Candidate biomarkers were identified by an expert multistakeholder group using a majority voting consensus exercise and mapped to relevant cellular and molecular pathways. Results Of 71 included studies (67 studying effectiveness outcomes and eight safety outcomes; four studied both), most reported genomic or proteomic biomarkers associated with response to biologics (48 studies). Methodological or reporting limitations frequently compromised the interpretation of findings, including inadequate control for key covariates, lack of adjustment for multiple testing, and selective outcome reporting. We identified candidate biomarkers of efficacy to tumour necrosis factor inhibitors [variation in CARD14, CDKAL1, IL1B, IL12B and IL17RA loci, and lipopolysaccharide-induced phosphorylation of nuclear factor (NF)-κB in type 2 dendritic cells] and ustekinumab (HLA-C*06:02 and variation in an IL1B locus). None were supported by sufficient evidence for clinical use without further validation studies. Candidate biomarkers were found to be involved in the immune cellular crosstalk implicated in psoriasis pathogenesis, most notably antigen presentation, T helper (Th)17 cell differentiation, positive regulation of NF-κB, and Th17 cell activation. Conclusions This comprehensive catalogue provides a key resource for researchers and reveals a diverse range of biomarker types and outcomes in the included studies. The candidate biomarkers identified require further evaluation in methodologically robust studies to establish potential clinical utility. Future studies should aim to address the common methodological limitations highlighted in this review to expedite discovery and validation of biomarkers for clinical use. What is already known about this topic?  Responses to the systemic treatments commonly used to treat psoriasis vary.Biomarkers that accurately predict effectiveness and safety would enable targeted treatment selection, improved patient outcomes and more cost-effective healthcare. What does this study add?  This review provides a comprehensive catalogue of investigated biomarkers of systemic treatment response in psoriasis.A diverse range of biomarker types and outcomes was found in the included studies, serving as a key resource for the translational research community.

Funder

Innovative Medicines Initiative

International Psoriasis Council

NIHR Biomedical Research Centre (BRC) at King’s College London

Publisher

Oxford University Press (OUP)

Subject

Dermatology

Reference44 articles.

1. Psoriasis

2. National, regional, and worldwide epidemiology of psoriasis: systematic analysis and modelling study;Parisi;BMJ,2020

3. Comparison of cumulative clinical benefits of biologics for the treatment of psoriasis over 16 weeks: results from a network meta-analysis;Warren;J Am Acad Dermatol,2020

4. The role of biologics in the treatment of moderate-to-severe plaque psoriasis;Puig;G Ital Dermatol Venereol,2017

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