Jessye Maxwell, Brittany L Mitchell, Xinyi Du-Harpur, Luba M Pardo, Willemijn C A M Witkam, Nick Dand, Meike Bartels, Michael J Betti, Dorret I Boomsma, Xianjun Dong, Zachary Gerring, Sarah Finer, Fiona A Hagenbeek, Jouke Jan Hottenga, George Hripcsak, Laura Huilaja, Kristian Hveem, Benjamin M Jacobs, Mart Kals, James Kaufman-Cook, Johannes Kettunen, Atlas Khan, Külli Kingo, Krzysztof Kiryluk, Mari Løset, Gerton Lunter, Michelle K Lupton, Josine L Min, Nicholas G Martin, Sarah E Medland, Andres Metspalu, Dorien Neijzen, Tamar E C Nijsten, Tiit Nikopensius, Catherine M Olsen, Lynn Petukhova, Anu Reigo, Miguel E Rentería, Rossella Rispoli, Jake Saklatvala, Eeva Sliz, Kaisa Tasanen-Määttä, Maris Teder-Laving, Laurent Thomas, Richard C Trembath, Mariliis Vaht, David A van Heel, Chunhua Weng, David C Whiteman, Jonathan N Barker, Catherine Smith, Michael A Simpson
{"title":"Genome-wide association meta-regression identifies stem cell lineage orchestration as a key driver of acne risk.","authors":"Jessye Maxwell, Brittany L Mitchell, Xinyi Du-Harpur, Luba M Pardo, Willemijn C A M Witkam, Nick Dand, Meike Bartels, Michael J Betti, Dorret I Boomsma, Xianjun Dong, Zachary Gerring, Sarah Finer, Fiona A Hagenbeek, Jouke Jan Hottenga, George Hripcsak, Laura Huilaja, Kristian Hveem, Benjamin M Jacobs, Mart Kals, James Kaufman-Cook, Johannes Kettunen, Atlas Khan, Külli Kingo, Krzysztof Kiryluk, Mari Løset, Gerton Lunter, Michelle K Lupton, Josine L Min, Nicholas G Martin, Sarah E Medland, Andres Metspalu, Dorien Neijzen, Tamar E C Nijsten, Tiit Nikopensius, Catherine M Olsen, Lynn Petukhova, Anu Reigo, Miguel E Rentería, Rossella Rispoli, Jake Saklatvala, Eeva Sliz, Kaisa Tasanen-Määttä, Maris Teder-Laving, Laurent Thomas, Richard C Trembath, Mariliis Vaht, David A van Heel, Chunhua Weng, David C Whiteman, Jonathan N Barker, Catherine Smith, Michael A Simpson","doi":"10.1101/2025.06.27.25330406","DOIUrl":null,"url":null,"abstract":"<p><p>Over 85% of the population experience acne at some point in their lives, with its severity spanning a quantitative spectrum, from mild, transient outbreaks to more persistent, severe forms of the condition. Moderate to severe disease poses a substantial global burden arising from both the physical and psychological impacts of this highly visible condition. The analytical approach taken in this study aimed to address the impact of variation in the dichotomisation of acne case control status, driven by ascertainment and study design, on effect size estimates across independent genetic association studies of acne. Through a fixed intercept meta-regression framework, we combined evidence genome-wide for association with acne across studies in which case-control status had been ascertained in different settings, allowing for different severity threshold definitions. Across a combined sample of 73,997 cases and 1,103,940 controls of European, South Asian and African American ancestry we identify genetic variation at 165 genomic loci that influence acne risk. There is evidence for both shared and ancestry specific components to the genetic susceptibility to acne and for sex differences in the magnitude of effect of risk alleles at three loci. We observe that common genetic variation explains 13.4% of acne heritability on the liability scale. Consistent with the hypothesis that genetic risk primarily operates at the level of individual pilosebaceous units, a polygenic score derived from this case-control study of acne susceptibility is associated with both self-reported and clinically assessed acne severity in adolescence, further strengthening the link between genetic risk and disease severity. Prioritisation of causal genes at the identified acne risk loci, provides genetic validation of the targets of established and emerging acne therapies, including retinoid treatments. The identified acne risk loci are enriched for genes encoding downstream effectors of <i>RXRA</i> signalling, including <i>SOX9</i> and components of the <i>WNT</i> and p53 pathways. Illustrating that the control of stem cell lineage plasticity and cellular fate are important mechanisms through which genetic variation influences acne susceptibility within the pilosebaceous unit.</p>","PeriodicalId":94281,"journal":{"name":"medRxiv : the preprint server for health sciences","volume":" ","pages":""},"PeriodicalIF":0.0000,"publicationDate":"2025-09-26","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC12262744/pdf/","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"medRxiv : the preprint server for health sciences","FirstCategoryId":"1085","ListUrlMain":"https://doi.org/10.1101/2025.06.27.25330406","RegionNum":0,"RegionCategory":null,"ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"","JCRName":"","Score":null,"Total":0}
引用次数: 0
Abstract
Over 85% of the population experience acne at some point in their lives, with its severity spanning a quantitative spectrum, from mild, transient outbreaks to more persistent, severe forms of the condition. Moderate to severe disease poses a substantial global burden arising from both the physical and psychological impacts of this highly visible condition. The analytical approach taken in this study aimed to address the impact of variation in the dichotomisation of acne case control status, driven by ascertainment and study design, on effect size estimates across independent genetic association studies of acne. Through a fixed intercept meta-regression framework, we combined evidence genome-wide for association with acne across studies in which case-control status had been ascertained in different settings, allowing for different severity threshold definitions. Across a combined sample of 73,997 cases and 1,103,940 controls of European, South Asian and African American ancestry we identify genetic variation at 165 genomic loci that influence acne risk. There is evidence for both shared and ancestry specific components to the genetic susceptibility to acne and for sex differences in the magnitude of effect of risk alleles at three loci. We observe that common genetic variation explains 13.4% of acne heritability on the liability scale. Consistent with the hypothesis that genetic risk primarily operates at the level of individual pilosebaceous units, a polygenic score derived from this case-control study of acne susceptibility is associated with both self-reported and clinically assessed acne severity in adolescence, further strengthening the link between genetic risk and disease severity. Prioritisation of causal genes at the identified acne risk loci, provides genetic validation of the targets of established and emerging acne therapies, including retinoid treatments. The identified acne risk loci are enriched for genes encoding downstream effectors of RXRA signalling, including SOX9 and components of the WNT and p53 pathways. Illustrating that the control of stem cell lineage plasticity and cellular fate are important mechanisms through which genetic variation influences acne susceptibility within the pilosebaceous unit.
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