Comparative Genetic Analysis of Psoriatic Arthritis and Psoriasis for the Discovery of Genetic Risk Factors and Risk Prediction Modeling

the BADBIR Study Group; the BSTOP study group

doi:10.1002/art.42154

Comparative Genetic Analysis of Psoriatic Arthritis and Psoriasis for the Discovery of Genetic Risk Factors and Risk Prediction Modeling

the BADBIR Study Group, the BSTOP study group

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19 Citations (Scopus)

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Abstract

Objectives: Psoriatic arthritis (PsA) has a strong genetic component, and the identification of genetic risk factors could help identify the ~30% of psoriasis patients at high risk of developing PsA. Our objectives were to identify genetic risk factors and pathways that differentiate PsA from cutaneous-only psoriasis (PsC) and to evaluate the performance of PsA risk prediction models. Methods: Genome-wide meta-analyses were conducted separately for 5,065 patients with PsA and 21,286 healthy controls and separately for 4,340 patients with PsA and 6,431 patients with PsC. The heritability of PsA was calculated as a single-nucleotide polymorphism (SNP)–based heritability estimate (h²_SNP) and biologic pathways that differentiate PsA from PsC were identified using Priority Index software. The generalizability of previously published PsA risk prediction pipelines was explored, and a risk prediction model was developed with external validation. Results: We identified a novel genome-wide significant susceptibility locus for the development of PsA on chromosome 22q11 (rs5754467; P = 1.61 × 10⁻⁹), and key pathways that differentiate PsA from PsC, including NF-κB signaling (adjusted P = 1.4 × 10⁻⁴⁵) and Wnt signaling (adjusted P = 9.5 × 10⁻⁵⁸). The heritability of PsA in this cohort was found to be moderate (h²_SNP = 0.63), which was similar to the heritability of PsC (h²_SNP = 0.61). We observed modest performance of published classification pipelines (maximum area under the curve 0.61), with similar performance of a risk model derived using the current data. Conclusion: Key biologic pathways associated with the development of PsA were identified, but the investigation of risk classification revealed modest utility in the available data sets, possibly because many of the PsC patients included in the present study were receiving treatments that are also effective in PsA. Future predictive models of PsA should be tested in PsC patients recruited from primary care.

Original language	English
Pages (from-to)	1535-1543
Number of pages	9
Journal	Arthritis and Rheumatology
Volume	74
Issue number	9
Early online date	4 Aug 2022
DOIs	https://doi.org/10.1002/art.42154
Publication status	Published - Sept 2022

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Comparative Genetic Analysis_SOOMRO_Publishedonline4August2022_GOLD VoR CC BYFinal published version, 594 KBLicence: CC BY

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@article{af8022af22704a9c83167af521356c33,

title = "Comparative Genetic Analysis of Psoriatic Arthritis and Psoriasis for the Discovery of Genetic Risk Factors and Risk Prediction Modeling",

abstract = "Objectives: Psoriatic arthritis (PsA) has a strong genetic component, and the identification of genetic risk factors could help identify the ~30% of psoriasis patients at high risk of developing PsA. Our objectives were to identify genetic risk factors and pathways that differentiate PsA from cutaneous-only psoriasis (PsC) and to evaluate the performance of PsA risk prediction models. Methods: Genome-wide meta-analyses were conducted separately for 5,065 patients with PsA and 21,286 healthy controls and separately for 4,340 patients with PsA and 6,431 patients with PsC. The heritability of PsA was calculated as a single-nucleotide polymorphism (SNP)–based heritability estimate (h2SNP) and biologic pathways that differentiate PsA from PsC were identified using Priority Index software. The generalizability of previously published PsA risk prediction pipelines was explored, and a risk prediction model was developed with external validation. Results: We identified a novel genome-wide significant susceptibility locus for the development of PsA on chromosome 22q11 (rs5754467; P = 1.61 × 10−9), and key pathways that differentiate PsA from PsC, including NF-κB signaling (adjusted P = 1.4 × 10−45) and Wnt signaling (adjusted P = 9.5 × 10−58). The heritability of PsA in this cohort was found to be moderate (h2SNP = 0.63), which was similar to the heritability of PsC (h2SNP = 0.61). We observed modest performance of published classification pipelines (maximum area under the curve 0.61), with similar performance of a risk model derived using the current data. Conclusion: Key biologic pathways associated with the development of PsA were identified, but the investigation of risk classification revealed modest utility in the available data sets, possibly because many of the PsC patients included in the present study were receiving treatments that are also effective in PsA. Future predictive models of PsA should be tested in PsC patients recruited from primary care.",

author = "{the BADBIR Study Group} and {the BSTOP study group} and Mehreen Soomro and Michael Stadler and Nick Dand and James Bluett and Deepak Jadon and Farideh Jalali-najafabadi and Michael Duckworth and Pauline Ho and Helena Marzo-Ortega and Helliwell, {Philip S.} and Ryan, {Anthony W.} and David Kane and Eleanor Korendowych and Simpson, {Michael A.} and Jonathan Packham and Ross McManus and Cem Gabay and C{\'e}line Lamacchia and Nissen, {Michael J.} and Brown, {Matthew A.} and Verstappen, {Suzanne M.M.} and {Van Staa}, Tjeerd and Barker, {Jonathan N.} and Catherine Smith and Robert Chalmers and Carsten Flohr and Karen Watson and David Prieto-Merino and Oras Alabas and Jonathan Barker and Gabrielle Becher and Anthony Bewley and David Burden and Simon Morrison and Phil Laws and Ian Evans and Christopher Griffiths and Shehnaz Ahmed and Brian Kirby and Elise Kleyn and Linda Lawson and Teena Mackenzie and Tess McPherson and Kathleen McElhone and Ruth Murphy and Anthony Ormerod and Catherine Smith and Catherine Smith and Sara Brown and Nick Dand",

note = "Funding Information: Supported by Versus Arthritis (grants 21173, 21754, and 21755), the NIHR Cambridge Biomedical Research Centre (grant BRC‐1215‐20014), and Cambridge Arthritis Research Endeavour (CARE). Mr. Stadler's work was supported by an MRC Doctoral Training Partnership (DTP) Studentship (grant MR/N013751/1). Dr. Jalali‐najafabadi's work was supported by a Medical Research Council (MRC)/University of Manchester Skills Development Fellowship (grant MR/R016615). Dr. Marzo‐Ortega's work was supported by the Leeds NIHR Biomedical Research Centre (LBRC). Dr. Warren's work was supported by the Manchester NIHR Biomedical Research Centre. Dr. Barton's work was supported by the NIHR. Funding Information: We are grateful for the assistance given by The University of Manchester IT Services and for the use of the Computational Shared Facility. We thank all of the patient participants and acknowledge the enthusiastic collaboration of all clinicians and research teams in the UK and the Republic of Ireland who recruited for this study. We gratefully acknowledge the substantial contribution to administration of this project by the following members of the Data Monitoring Committee (DMC) of the BADBIR Study Group: Dr. Robert Chalmers, Dr. Carsten Flohr (Chair), Dr. Karen Watson, and David Prieto-Merino. We also thank the following members of the BADBIR Steering Committee: Oras Alabas, Professor Jonathan Barker, Gabrielle Becher, Anthony Bewley, David Burden, Simon Morrison, Professor Phil Laws (Chair), Mr. Ian Evans, Professor Christopher Griffiths, Shehnaz Ahmed, Dr. Brian Kirby, Elise Kleyn, Ms. Linda Lawson, Teena Mackenzie, Tess McPherson, Dr. Kathleen McElhone, Dr. Ruth Murphy, Professor Anthony Ormerod, Dr. Caroline Owen, Professor Nick Reynolds, Amir Rashid, Professor Catherine Smith, and Dr. Richard Warren. We are grateful to the following members of the BSTOP Steering Committee for their valuable role in the oversight of the study delivery: Professor David Burden (Chair), Professor Catherine Smith, Professor Stefan Siebert, Professor Sara Brown, Helen McAteer, Dr. Julia Schofield, and Dr. Nick Dand. Finally, we acknowledge the enthusiastic collaboration of all the dermatologists and specialist nurses in the UK and the Republic of Ireland who provided the BADBIR and BSTOP data. The principal investigators at the participating sites can be found at the following website: http://www.badbir.org/Clinicians/. Open access funding was enabled and organized by Projekt DEAL. Publisher Copyright: {\textcopyright} 2022 The Authors. Arthritis & Rheumatology published by Wiley Periodicals LLC on behalf of American College of Rheumatology.",

year = "2022",

month = sep,

doi = "10.1002/art.42154",

language = "English",

volume = "74",

pages = "1535--1543",

journal = "Arthritis and Rheumatology",

issn = "2326-5191",

publisher = "Wiley",

number = "9",

}

TY - JOUR

T1 - Comparative Genetic Analysis of Psoriatic Arthritis and Psoriasis for the Discovery of Genetic Risk Factors and Risk Prediction Modeling

AU - the BADBIR Study Group

AU - the BSTOP study group

AU - Soomro, Mehreen

AU - Stadler, Michael

AU - Dand, Nick

AU - Bluett, James

AU - Jadon, Deepak

AU - Jalali-najafabadi, Farideh

AU - Duckworth, Michael

AU - Ho, Pauline

AU - Marzo-Ortega, Helena

AU - Helliwell, Philip S.

AU - Ryan, Anthony W.

AU - Kane, David

AU - Korendowych, Eleanor

AU - Simpson, Michael A.

AU - Packham, Jonathan

AU - McManus, Ross

AU - Gabay, Cem

AU - Lamacchia, Céline

AU - Nissen, Michael J.

AU - Brown, Matthew A.

AU - Verstappen, Suzanne M.M.

AU - Van Staa, Tjeerd

AU - Barker, Jonathan N.

AU - Smith, Catherine

AU - Chalmers, Robert

AU - Flohr, Carsten

AU - Watson, Karen

AU - Prieto-Merino, David

AU - Alabas, Oras

AU - Barker, Jonathan

AU - Becher, Gabrielle

AU - Bewley, Anthony

AU - Burden, David

AU - Morrison, Simon

AU - Laws, Phil

AU - Evans, Ian

AU - Griffiths, Christopher

AU - Ahmed, Shehnaz

AU - Kirby, Brian

AU - Kleyn, Elise

AU - Lawson, Linda

AU - Mackenzie, Teena

AU - McPherson, Tess

AU - McElhone, Kathleen

AU - Murphy, Ruth

AU - Ormerod, Anthony

AU - Smith, Catherine

AU - Brown, Sara

AU - Dand, Nick

N1 - Funding Information: Supported by Versus Arthritis (grants 21173, 21754, and 21755), the NIHR Cambridge Biomedical Research Centre (grant BRC‐1215‐20014), and Cambridge Arthritis Research Endeavour (CARE). Mr. Stadler's work was supported by an MRC Doctoral Training Partnership (DTP) Studentship (grant MR/N013751/1). Dr. Jalali‐najafabadi's work was supported by a Medical Research Council (MRC)/University of Manchester Skills Development Fellowship (grant MR/R016615). Dr. Marzo‐Ortega's work was supported by the Leeds NIHR Biomedical Research Centre (LBRC). Dr. Warren's work was supported by the Manchester NIHR Biomedical Research Centre. Dr. Barton's work was supported by the NIHR. Funding Information: We are grateful for the assistance given by The University of Manchester IT Services and for the use of the Computational Shared Facility. We thank all of the patient participants and acknowledge the enthusiastic collaboration of all clinicians and research teams in the UK and the Republic of Ireland who recruited for this study. We gratefully acknowledge the substantial contribution to administration of this project by the following members of the Data Monitoring Committee (DMC) of the BADBIR Study Group: Dr. Robert Chalmers, Dr. Carsten Flohr (Chair), Dr. Karen Watson, and David Prieto-Merino. We also thank the following members of the BADBIR Steering Committee: Oras Alabas, Professor Jonathan Barker, Gabrielle Becher, Anthony Bewley, David Burden, Simon Morrison, Professor Phil Laws (Chair), Mr. Ian Evans, Professor Christopher Griffiths, Shehnaz Ahmed, Dr. Brian Kirby, Elise Kleyn, Ms. Linda Lawson, Teena Mackenzie, Tess McPherson, Dr. Kathleen McElhone, Dr. Ruth Murphy, Professor Anthony Ormerod, Dr. Caroline Owen, Professor Nick Reynolds, Amir Rashid, Professor Catherine Smith, and Dr. Richard Warren. We are grateful to the following members of the BSTOP Steering Committee for their valuable role in the oversight of the study delivery: Professor David Burden (Chair), Professor Catherine Smith, Professor Stefan Siebert, Professor Sara Brown, Helen McAteer, Dr. Julia Schofield, and Dr. Nick Dand. Finally, we acknowledge the enthusiastic collaboration of all the dermatologists and specialist nurses in the UK and the Republic of Ireland who provided the BADBIR and BSTOP data. The principal investigators at the participating sites can be found at the following website: http://www.badbir.org/Clinicians/. Open access funding was enabled and organized by Projekt DEAL. Publisher Copyright: © 2022 The Authors. Arthritis & Rheumatology published by Wiley Periodicals LLC on behalf of American College of Rheumatology.

PY - 2022/9

Y1 - 2022/9

N2 - Objectives: Psoriatic arthritis (PsA) has a strong genetic component, and the identification of genetic risk factors could help identify the ~30% of psoriasis patients at high risk of developing PsA. Our objectives were to identify genetic risk factors and pathways that differentiate PsA from cutaneous-only psoriasis (PsC) and to evaluate the performance of PsA risk prediction models. Methods: Genome-wide meta-analyses were conducted separately for 5,065 patients with PsA and 21,286 healthy controls and separately for 4,340 patients with PsA and 6,431 patients with PsC. The heritability of PsA was calculated as a single-nucleotide polymorphism (SNP)–based heritability estimate (h2SNP) and biologic pathways that differentiate PsA from PsC were identified using Priority Index software. The generalizability of previously published PsA risk prediction pipelines was explored, and a risk prediction model was developed with external validation. Results: We identified a novel genome-wide significant susceptibility locus for the development of PsA on chromosome 22q11 (rs5754467; P = 1.61 × 10−9), and key pathways that differentiate PsA from PsC, including NF-κB signaling (adjusted P = 1.4 × 10−45) and Wnt signaling (adjusted P = 9.5 × 10−58). The heritability of PsA in this cohort was found to be moderate (h2SNP = 0.63), which was similar to the heritability of PsC (h2SNP = 0.61). We observed modest performance of published classification pipelines (maximum area under the curve 0.61), with similar performance of a risk model derived using the current data. Conclusion: Key biologic pathways associated with the development of PsA were identified, but the investigation of risk classification revealed modest utility in the available data sets, possibly because many of the PsC patients included in the present study were receiving treatments that are also effective in PsA. Future predictive models of PsA should be tested in PsC patients recruited from primary care.

AB - Objectives: Psoriatic arthritis (PsA) has a strong genetic component, and the identification of genetic risk factors could help identify the ~30% of psoriasis patients at high risk of developing PsA. Our objectives were to identify genetic risk factors and pathways that differentiate PsA from cutaneous-only psoriasis (PsC) and to evaluate the performance of PsA risk prediction models. Methods: Genome-wide meta-analyses were conducted separately for 5,065 patients with PsA and 21,286 healthy controls and separately for 4,340 patients with PsA and 6,431 patients with PsC. The heritability of PsA was calculated as a single-nucleotide polymorphism (SNP)–based heritability estimate (h2SNP) and biologic pathways that differentiate PsA from PsC were identified using Priority Index software. The generalizability of previously published PsA risk prediction pipelines was explored, and a risk prediction model was developed with external validation. Results: We identified a novel genome-wide significant susceptibility locus for the development of PsA on chromosome 22q11 (rs5754467; P = 1.61 × 10−9), and key pathways that differentiate PsA from PsC, including NF-κB signaling (adjusted P = 1.4 × 10−45) and Wnt signaling (adjusted P = 9.5 × 10−58). The heritability of PsA in this cohort was found to be moderate (h2SNP = 0.63), which was similar to the heritability of PsC (h2SNP = 0.61). We observed modest performance of published classification pipelines (maximum area under the curve 0.61), with similar performance of a risk model derived using the current data. Conclusion: Key biologic pathways associated with the development of PsA were identified, but the investigation of risk classification revealed modest utility in the available data sets, possibly because many of the PsC patients included in the present study were receiving treatments that are also effective in PsA. Future predictive models of PsA should be tested in PsC patients recruited from primary care.

UR - http://www.scopus.com/inward/record.url?scp=85135518463&partnerID=8YFLogxK

U2 - 10.1002/art.42154

DO - 10.1002/art.42154

M3 - Article

C2 - 35507331

AN - SCOPUS:85135518463

SN - 2326-5191

VL - 74

SP - 1535

EP - 1543

JO - Arthritis and Rheumatology

JF - Arthritis and Rheumatology

IS - 9

ER -

Comparative Genetic Analysis of Psoriatic Arthritis and Psoriasis for the Discovery of Genetic Risk Factors and Risk Prediction Modeling

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