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

The Acne Genetic Study Group

doi:10.1038/s41467-018-07459-5

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

The Acne Genetic Study Group

Department of Dermatology

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

39 Citations (Scopus)

Abstract

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.

Original language	English
Article number	5075
Journal	Nature communications
Volume	9
Issue number	1
DOIs	https://doi.org/10.1038/s41467-018-07459-5
Publication status	Published - 2018 Dec 1

All Science Journal Classification (ASJC) codes

General Chemistry
General Biochemistry,Genetics and Molecular Biology
General Physics and Astronomy

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10.1038/s41467-018-07459-5

Cite this

@article{59e1e3f1ad8c4de4bcdee0dd4fc28784,

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

abstract = "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.",

author = "{The Acne Genetic Study Group} and Christos Petridis and Navarini, {Alexander A.} and Nick Dand and Jake Saklatvala and David Baudry and Michael Duckworth and Allen, {Michael H.} and Curtis, {Charles J.} and Lee, {Sang Hyuck} and Burden, {A. David} and Alison Layton and Veronique Bataille and Pink, {Andrew E.} and Anton Alexandroff and Alex Anstey and Jaskiran Azad and Omar Aziz and Nigel Burrows and Aamir Butt and Peter Cartwright and Anna Chapman and Clayton, {Timothy H.} and Sandeep Cliff and Tim Cutler and Brigid Daly and Amrit Darvay and Claudia DeGiovanni and Anthony Downs and Colm Dwyer and John English and Adam Ferguson and Colin Fleming and Elizabeth Fraser-Andrews and Mark Goodfield and Grattan, {Clive E.} and Hartmut Hempel and Sue Hood and Bronwyn Hughes and Evmorfia Ladoyanni and Calum Lyon and Ali Mahmud and Moshin Malik and Eleanor Mallon and Simon Meggitt and Andrew Messenger and Yaaseen Moosa and Stephanie Munn and Anthony Ormerod and Deepak Rallan and McGrath, {John A.}",

note = "Publisher Copyright: {\textcopyright} 2018, The Author(s).",

year = "2018",

month = dec,

day = "1",

doi = "10.1038/s41467-018-07459-5",

language = "English",

volume = "9",

journal = "Nature communications",

issn = "2041-1723",

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T1 - Genome-wide meta-analysis implicates mediators of hair follicle development and morphogenesis in risk for severe acne

AU - The Acne Genetic Study Group

AU - Petridis, Christos

AU - Navarini, Alexander A.

AU - Dand, Nick

AU - Saklatvala, Jake

AU - Baudry, David

AU - Duckworth, Michael

AU - Allen, Michael H.

AU - Curtis, Charles J.

AU - Lee, Sang Hyuck

AU - Burden, A. David

AU - Layton, Alison

AU - Bataille, Veronique

AU - Pink, Andrew E.

AU - Alexandroff, Anton

AU - Anstey, Alex

AU - Azad, Jaskiran

AU - Aziz, Omar

AU - Burrows, Nigel

AU - Butt, Aamir

AU - Cartwright, Peter

AU - Chapman, Anna

AU - Clayton, Timothy H.

AU - Cliff, Sandeep

AU - Cutler, Tim

AU - Daly, Brigid

AU - Darvay, Amrit

AU - DeGiovanni, Claudia

AU - Downs, Anthony

AU - Dwyer, Colm

AU - English, John

AU - Ferguson, Adam

AU - Fleming, Colin

AU - Fraser-Andrews, Elizabeth

AU - Goodfield, Mark

AU - Grattan, Clive E.

AU - Hempel, Hartmut

AU - Hood, Sue

AU - Hughes, Bronwyn

AU - Ladoyanni, Evmorfia

AU - Lyon, Calum

AU - Mahmud, Ali

AU - Malik, Moshin

AU - Mallon, Eleanor

AU - Meggitt, Simon

AU - Messenger, Andrew

AU - Moosa, Yaaseen

AU - Munn, Stephanie

AU - Ormerod, Anthony

AU - Rallan, Deepak

AU - McGrath, John A.

PY - 2018/12/1

Y1 - 2018/12/1

N2 - 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.

AB - 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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U2 - 10.1038/s41467-018-07459-5

DO - 10.1038/s41467-018-07459-5

M3 - Article

C2 - 30542056

AN - SCOPUS:85058572472

SN - 2041-1723

VL - 9

JO - Nature communications

JF - Nature communications

IS - 1

M1 - 5075

ER -

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

Abstract

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