Elucidating the relationship between migraine risk and brain structure using genetic data

偏头痛 孟德尔随机化 大脑大小 全基因组关联研究 遗传关联 脑形态计量学 神经科学 心理学 生物 医学 遗传学 基因 遗传变异 精神科 单核苷酸多态性 磁共振成像 基因型 放射科
作者
Brittany L. Mitchell,Santiago Díaz-Torres,Svetlana Bivol,Gabriel Cuéllar-Partida,Padhraig Gormley,Verneri Anttila,Bendik S. Winsvold,Priit Palta,Tõnu Esko,Tune H. Pers,Kai-How Farh,Ester Cuenca-León,Mikko Muona,Nicholas A. Furlotte,Tobias Kurth,Andrés Ingason,George Davey Smith,Lannie Ligthart,Gisela M. Terwindt,Mikko Kallela,Tobias Freilinger,Caroline Ran,Scott D. Gordon,Anine H Stam,Stacy Steinberg,Guntram Borck,Markku Koiranen,George Davey Smith,Hieab H.H. Adams,Terho Lehtimäki,Roy Thurik,Juho Wedenoja,David A. Hinds,Julie E. Buring,Markus Schürks,Paul M Ridker,Maria Gudlaug Hrafnsdottir,Hreinn Stefánsson,Susan M. Ring,Jouke‐Jan Hottenga,Brenda W.J.H. Penninx,Martti Färkkilâ,Ville Artto,Mari Kaunisto,Salli Vepsäläinen,Rainer Malik,Andrew C. Heath,Elina Hyppönen,Nicholas G. Martin,Grant W. Montgomery,Mitja Kurki,Mart Kals,Reedik Mägi,Kalle Pärn,Eija‐Riitta Hämäläinen,Hailiang Huang,Andrea Byrnes,Lude Franke,Jie Huang,Evie Stergiakouli,Phil H. Lee,Cynthia Sandor,Caleb Webber,M. Zameel Cader,Bertram Müller‐Myhsok,Stefan Schreiber,Thomas Meitinger,Johan G. Eriksson,Veikko Salomaa,Kauko Heikkilä,Elizabeth Loehrer,André G. Uitterlinden,Albert Hofman,Cornelia M. van Duijn,Lynn Cherkas,Linda M. Pedersen,Audun Stubhaug,Christopher Sivert Nielsen,Minna Männikkö,Reedik Mägi,Lili Milani,Hartmut Göbel,Ann-Louise Esserlind,Anne Francke Christensen,Thomas Hansen,Thomas Werge,Sigrid Børte,Bru Cormand,Else Eising,Lyn R. Griffiths,Eija Hämäläinen,Marjo Hiekkala,Risto Kajanne,Lenore J. Launer,Terho Lehtimäki,Davor Leslsel,Alfons Macaya,Massimo Mangino,Nancy L. Pedersen,Daniëlle Posthuma,Patricia Pozo‐Rosich,Alice Pressman,Cèlia Sintas,Marta Vila‐Pueyo,Huiying Zhao Jaakko Kaprio,Arpo Aromaa,Olli Raitakari,M. Arfan Ikram,Tim D. Spector,Marjo‐Riitta Järvelin,Andres Metspalu,Christian Kubisch,David P. Strachan,Michel D. Ferrari,Andrea Carmine Belin,Martin Dichgans,Maija Wessman,Arn M. J. M. van den Maagdenberg,John Hardy,Dorret I. Boomsma,George Davey Smith,Kāri Stefánsson,Nicholas Eriksson,Mark J. Daly,Benjamin M. Neale,Jes Olesen,Daniel I. Chasman,Dale R. Nyholt,Aarno Palotie,Zachary F. Gerring,Nicholas G. Martin,Sarah E. Medland,Katrina L. Grasby,Dale R. Nyholt,Miguel E. Rentería
出处
期刊:Brain [Oxford University Press]
卷期号:145 (9): 3214-3224 被引量:11
标识
DOI:10.1093/brain/awac105
摘要

Migraine is a highly common and debilitating disorder that often affects individuals in their most productive years of life. Previous studies have identified both genetic variants and brain morphometry differences associated with migraine risk. However, the relationship between migraine and brain morphometry has not been examined on a genetic level, and the causal nature of the association between brain structure and migraine risk has not been determined. Using the largest available genome-wide association studies to date, we examined the genome-wide genetic overlap between migraine and intracranial volume, as well as the regional volumes of nine subcortical brain structures. We further focused the identification and biological annotation of genetic overlap between migraine and each brain structure on specific regions of the genome shared between migraine and brain structure. Finally, we examined whether the size of any of the examined brain regions causally increased migraine risk using a Mendelian randomization approach. We observed a significant genome-wide negative genetic correlation between migraine risk and intracranial volume (rG = -0.11, P = 1 × 10-3) but not with any subcortical region. However, we identified jointly associated regional genomic overlap between migraine and every brain structure. Gene enrichment in these shared genomic regions pointed to possible links with neuronal signalling and vascular regulation. Finally, we provide evidence of a possible causal relationship between smaller total brain, hippocampal and ventral diencephalon volume and increased migraine risk, as well as a causal relationship between increased risk of migraine and a larger volume of the amygdala. We leveraged the power of large genome-wide association studies to show evidence of shared genetic pathways that jointly influence migraine risk and several brain structures, suggesting that altered brain morphometry in individuals with high migraine risk may be genetically mediated. Further interrogation of these results showed support for the neurovascular hypothesis of migraine aetiology and shed light on potentially viable therapeutic targets.

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