<p>Atypical frontotemporal lobar degeneration with ubiquitin-positive inclusions (aFTLD-U) is neuropathologically characterized by aggregation of the FET family of proteins and clinically manifests as sporadic young-onset frontotemporal dementia. Here we describe a major risk locus on chr15q14 identified through a genome-wide association study in 59 pathologically confirmed aFTLD-U cases and 3,153 controls (lead single nucleotide polymorphism rs549846383, <i>P</i> = 5.85 × 10<sup>−21</sup>, odds ratio 26.7). When combined with data from 28 additional aFTLD-U cases, 3,712 controls and 3,215 individuals with other neurodegenerative diseases and by leveraging in-house and public long-read genome sequencing data from 1,715 individuals, we identified a tandem repeat expansion on the associated haplotypes in an intron of <i>GOLGA8A</i>. We found variation in repeat length, motif length, and motif sequence, with long CT-dimer expansions strongly associated with aFTLD-U. Although the functional consequence of this repeat remains unknown, its presence in nearly 60% of aFTLD-U cases points to a fundamental role in disease pathogenesis.</p>

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A repeat expansion in GOLGA8A is a major risk factor for atypical frontotemporal lobar degeneration with ubiquitin-positive inclusions

  • Wouter De Coster,
  • Marleen Van den Broeck,
  • Matt Baker,
  • Nikhil B. Ghayal,
  • Sarah Wynants,
  • Anthony Batzler,
  • Cyril Pottier,
  • Sara Alidadiani,
  • Fahri Küçükali,
  • Gregory D. Jenkins,
  • Rafaela Policarpo,
  • Marka van Blitterswijk,
  • Mariely DeJesus-Hernandez,
  • Alexandra I. Soto-Beasley,
  • Júlia Faura,
  • Elise Coopman,
  • Saskia Hutten,
  • Merel O. Mol,
  • David Wallon,
  • Anne Sieben,
  • Elizabeth C. Finger,
  • Melissa E. Murray,
  • Shelley L. Forrest,
  • Maria C. Tartaglia,
  • Claire Troakes,
  • Jeroen G. J. van Rooij,
  • Aivi T. Nguyen,
  • R. Ross Reichard,
  • Natalie L. Woodman,
  • Alissa L. Nana,
  • Sandra Weintraub,
  • Tamar Gefen,
  • Bart De Vil,
  • Istvan Bodi,
  • Oscar L. Lopez,
  • Susana Boluda,
  • Serge Belliard,
  • Florence Lebert,
  • Florent Marguet,
  • Qinwen Mao,
  • Marsel M. Mesulam,
  • Adam L. Boxer,
  • Mathieu Vandenbulcke,
  • EunRan Suh,
  • Jolien Schaeverbeke,
  • Jean-Charles Lambert,
  • Sonja W. Scholz,
  • Clifton L. Dalgard,
  • Bryan J. Traynor,
  • Raphael J. Gibbs,
  • Gerard D. Schellenberg,
  • Dorothee Dormann,
  • Geert Joris,
  • Tim De Pooter,
  • Peter De Rijk,
  • Svenn D’Hert,
  • Jasper Van Dongen,
  • Julie van der Zee,
  • Mojca Strazisar,
  • Marla Gearing,
  • Thomas Kukar,
  • Margaret Flanagan,
  • Sebastiaan Engelborghs,
  • Bernardino Ghetti,
  • Kathy L. Newell,
  • Andrew King,
  • Sigrun Roeber,
  • Howard J. Rosen,
  • Salvatore Spina,
  • Patrick Cras,
  • Nilüfer Ertekin-Taner,
  • Zbigniew K. Wszolek,
  • Ryan J. Uitti,
  • William P. Cheshire,
  • Wolfgang Singer,
  • Jochen Herms,
  • Keith A. Josephs,
  • Jennifer L. Whitwell,
  • Ronald C. Petersen,
  • Florence Pasquier,
  • Gaël Nicolas,
  • Rudolph Castellani,
  • Jonathan Glass,
  • Bruce L. Miller,
  • Gabor G. Kovacs,
  • Robert A. Rissman,
  • Annie Hiniker,
  • Vincent Deramecourt,
  • Lee-Cyn Ang,
  • Jin Lee-Way,
  • Vivianna M. Van Deerlin,
  • Brittany N. Dugger,
  • Dietmar R. Thal,
  • Lea T. Grinberg,
  • Carlos Cruchaga,
  • Thomas Arzberger,
  • David G. Munoz,
  • Julia Keith,
  • Lorne Zinman,
  • Ekaterina Rogaeva,
  • Edward B. Lee,
  • Stephen J. Haggarty,
  • Olaf Ansorge,
  • Masud Husain,
  • Glenda M. Halliday,
  • Safa Al-Sarraj,
  • Owen A. Ross,
  • Kristel Sleegers,
  • Rik Vandenberghe,
  • Bradley F. Boeve,
  • Neill R. Graff-Radford,
  • Julia Kofler,
  • Charles L. White III,
  • Tammaryn Lashley,
  • Manuela Neumann,
  • Joanna M. Biernacka,
  • William W. Seeley,
  • Harro Seelaar,
  • John C. van Swieten,
  • Jonathan D. Rohrer,
  • Dennis W. Dickson,
  • Ian R. A. Mackenzie,
  • Rosa Rademakers

摘要

Atypical frontotemporal lobar degeneration with ubiquitin-positive inclusions (aFTLD-U) is neuropathologically characterized by aggregation of the FET family of proteins and clinically manifests as sporadic young-onset frontotemporal dementia. Here we describe a major risk locus on chr15q14 identified through a genome-wide association study in 59 pathologically confirmed aFTLD-U cases and 3,153 controls (lead single nucleotide polymorphism rs549846383, P = 5.85 × 10−21, odds ratio 26.7). When combined with data from 28 additional aFTLD-U cases, 3,712 controls and 3,215 individuals with other neurodegenerative diseases and by leveraging in-house and public long-read genome sequencing data from 1,715 individuals, we identified a tandem repeat expansion on the associated haplotypes in an intron of GOLGA8A. We found variation in repeat length, motif length, and motif sequence, with long CT-dimer expansions strongly associated with aFTLD-U. Although the functional consequence of this repeat remains unknown, its presence in nearly 60% of aFTLD-U cases points to a fundamental role in disease pathogenesis.