Genome-wide meta-analysis implicates mediators of hair follicle development and morphogenesis in risk for severe acne

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作者
Christos Petridis
Alexander A. Navarini
Nick Dand
Jake Saklatvala
David Baudry
Michael Duckworth
Michael H. Allen
Charles J. Curtis
Sang Hyuck Lee
A. David Burden
Alison Layton
Veronique Bataille
Andrew E. Pink
Isabelle Carlavan
Johannes J. Voegel
Timothy D. Spector
Richard C. Trembath
John A. McGrath
Catherine H. Smith
Jonathan N. Barker
Michael A. Simpson
机构
[1] King’s College London,Department of Medical and Molecular Genetics, School of Basic & Medical Biosciences
[2] University Hospital of Zurich and University of Zurich,Departement of Dermatology
[3] King’s College London,St John’s Institute of Dermatology, School of Basic & Medical Biosciences
[4] King’s College London,NIHR Maudsley Biomedical Research Centre (BRC) at South London and Maudsley NHS Foundation Trust (SLaM) & Institute of Psychiatry, Psychology and Neuroscience (IoPPN)
[5] King’s College London,Social Genetic & Developmental Psychiatry Centre, Institute of Psychiatry, Psychology and Neuroscience (IoPPN)
[6] University of Glasgow,Institute of Infection, Immunity and Inflammation
[7] Harrogate and District Foundation Trust,Department of Dermatology
[8] King’s College London,Twin Research and Genetic Epidemiology Unit, School of Basic & Medical Biosciences
[9] Galderma R&D,Research Department
[10] University Hospitals of Leicester NHS Trust,Leicester Royal Infirmary
[11] Aneurin Bevan Health Board,St Woolos Hospital
[12] South Tees Hospitals NHS Foundation,James Cook University Hospital
[13] Ipswich Hospital NHS Trust,Addenbrooke’s Hospital
[14] Cambridge University Hospitals NHS Foundation Trust,Scunthorpe General Hospital
[15] Northern Lincolnshire and Goole Hospitals NHS Foundation Trust,Queen’s Hospital
[16] Burton Hospitals NHS Foundation Trust,Queen Elizabeth Hospital Woolwich
[17] Lewisham and Greenwich NHS Trust,East Surrey Hospital
[18] Salford Royal NHS Foundation Trust and Royal Manchester Children’s Hospital,Royal Blackburn Hospital
[19] Surrey and Sussex Healthcare NHS Trust,Southmead Hospital
[20] East Lancashire NHS Trust,Brighton General Hospital
[21] North Bristol NHS Trust,Royal Devon & Exeter Hospital
[22] Brighton and Sussex University Hospitals NHS Trust,Crosshouse Hospital
[23] Royal Devon & Exeter NHS Foundation Trust,Department of Dermatology, Queen’s Medical Centre
[24] NHS Ayrshire and Arran,Royal Derby Hospitals
[25] Nottingham University Hospitals NHS Trust,Ninewells Hospital and Medical School
[26] Derby Hospitals NHS Foundation Trust,Chapel Allerton Hospital
[27] NHS Tayside,St Mary’s Hospital
[28] Dundee,Corbett Hospital
[29] Essex County Hospital,Eastbourne District General Hospital
[30] The Leeds Teaching Hospitals NHS Trust,Broomfield Hospital
[31] Norfolk and Norwich University Hospitals NHS Foundation Trust,Mayday Hospital
[32] Great Western Hospitals NHS Foundation Trust,Royal Victoria Infirmary
[33] Portsmouth Hospitals NHS Trust,Royal Hallamshire Hospital
[34] The Dudley Group of Hospitals NHS Foundation Trust,Department of Dermatology, Orpington Hospital
[35] York Teaching hospitals NHS Foundation Trust,Department of Applied Medicine, Aberdeen
[36] East Sussex Healthcare NHS Trust,University Hospital Lewisham
[37] Mid Essex Hospital Services NHS Trust,Yeovil District Hospital and Musgrove Park Hospital
[38] Chelmsford,University Hospital of North Durham
[39] Croydon Health Services NHS Trust,Hull and East Yorkshire Hospitals
[40] The Newcastle upon Tyne Hospitals NHS Foundation Trust,Department of Dermatology
[41] Sheffield Teaching Hospitals NHS Foundation Trust,Glan Clwyd Hospital
[42] St George’s Healthcare NHS Trust,Department of Dermatology, Amersham Hospital
[43] St George’s,undefined
[44] King’s College Hospital NHS Foundation Trust,undefined
[45] University of Aberdeen,undefined
[46] Lewisham and Greenwich NHS Trust,undefined
[47] James Paget University Hospital NHS Foundation Trust,undefined
[48] Taunton and Somerset NHS Trust,undefined
[49] County Durham and Darlington NHS Foundation Trust,undefined
[50] NHS Trust and Hull York Medical School,undefined
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摘要
Acne vulgaris is a highly heritable common, chronic inflammatory disease of the skin for which five genetic risk loci have so far been identified. Here, we perform a genome-wide association study of 3823 cases and 16,144 controls followed by meta-analysis with summary statistics from a previous study, with a total sample size of 26,722. We identify 20 independent association signals at 15 risk loci, 12 of which have not been previously implicated in the disease. Likely causal variants disrupt the coding region of WNT10A and a P63 transcription factor binding site in SEMA4B. Risk alleles at the 1q25 locus are associated with increased expression of LAMC2, in which biallelic loss-of-function mutations cause the blistering skin disease epidermolysis bullosa. These findings indicate that variation affecting the structure and maintenance of the skin, in particular the pilosebaceous unit, is a critical aspect of the genetic predisposition to severe acne.
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