Multi-ancestry genome-wide meta-analysis of 56,241 individuals identifiesLRRC4C, LHX5-AS1and nominates ancestry-specific lociPTPRK,GRB14, andKIAA0825as novel risk loci for Alzheimer’s disease: the Alzheimer’s Disease Genetics Consortium

Farid Rajabli,Penelope Benchek,Giuseppe Tosto,Nicholas A. Kushch, Sha Jiang,Katrina Bazemore,Congcong Zhu,Wan‐Ping Lee, Jacob Haut,Kara L. Hamilton‐Nelson,Nicholas R. Wheeler,Yi Zhao,John Farrell,Michelle Grunin,Yuk Yee Leung,Pavel P. Kuksa,Donghe Li, Eder Lúcio da Fonseca,Jesse Mez,Ellen L. Palmer,Jagan A. Pillai,Richard Sherva,Yeunjoo E. Song,Xiaoling Zhang, Taha Iqbal,Omkar Pathak,Otto Valladares,Amanda B. Kuzma,Erin L. Abner,Perrie M. Adams,Alyssa Aguirre,Marilyn Albert,Roger L. Albin,Mariet Allen,Luis Alvarez,Liana G. Apostolova,Steven E. Arnold,Sanjay Asthana,Craig S. Atwood, Gayle Ayres,Clinton T. Baldwin,Robert C. Barber,Lisa L. Barnes,Sandra Barral,Thomas G. Beach,James T. Becker,Gary W. Beecham,Duane Beekly,Bruno A. Benitez,David A. Bennett,John Bertelson,Thomas D. Bird,Deborah Blacker,Bradley F. Boeve,James D. Bowen,Adam L. Boxer,James B. Brewer,James R. Burke,Jeffrey M. Burns,Joseph D. Buxbaum,Nigel J. Cairns,Laura B. Cantwell,Chuanhai Cao,Christopher S. Carlson,Cynthia M. Carlsson,Regina M. Carney,Minerva M. Carrasquillo, Scott A. Chasse,Marie‐Françoise Chesselet,Nathaniel A. Chin,Helena C. Chui,Jaeyoon Chung,Suzanne Craft,Paul K. Crane,David H. Cribbs,Elizabeth Crocco,Carlos Cruchaga,Michael L. Cuccaro,Munro Cullum,Eveleen Darby,Barbara Davis,Philip L. De Jager,Charles DeCarli, John C. DeToledo,Malcolm Dick,Dennis W. Dickson,Beth A. Dombroski,Rachelle S. Doody,Ranjan Duara,Nilüfer Ertekin-Taner,Denis A. Evans,Kelley Faber,Thomas J. Fairchild,Kenneth B. Fallon,David W. Fardo,Martin R. Farlow, Victoria Fernandez-Hernandez,Steven H. Ferris,Tatiana Foroud,Matthew P. Frosch,Brian Fulton‐Howard, Douglas Galasko, Adriana C. Gamboa,Marla Gearing,Daniel H. Geschwind,Bernardino Ghetti,John R. Gilbert,Alison Goate,Thomas J. Grabowski, Neill R. Graff‐Radford,Robert C. Green,John H. Growdon,Hákon Hákonarson,James Hall,Ronald L. Hamilton,Oscar Harari,John Hardy,Lindy E. Harrell,Elizabeth Head,Victor W. Henderson, Michelle Hernández,Timothy J. Hohman,Lawrence S. Honig,Ryan M. Huebinger, Matthew J. Huentelman,Christine M. Hulette, Bradley T. Hyman,Linda S. Hynan,Laura Ibáñez,Gail P. Jarvik,Suman Jayadev,Lee‐Way Jin, Kurt E. Johnson,Leigh Johnson,M. Ilyas Kamboh,Anna Karydas,Mindy J. Katz,John S. K. Kauwe,Jeffrey Kaye,C. Dirk Keene, Aisha Khaleeq,Ronald Kim,Janice Knebl,Neil W. Kowall,Joel H. Kramer,Walter A. Kukull,Frank M. LaFerla,James J. Lah,Eric B. Larson,Alan J. Lerner, James B. Leverenz,Aĺlan I. Levey,Andrew P. Lieberman,Richard B. Lipton,Mark W. Logue,Oscar L. López,Kathryn L. Lunetta,Constantine G. Lyketsos,Douglas A. Mains,Flanagan E. Margaret,Daniel C. Marson,Eden R. Martin,Frank Martiniuk,Deborah C. Mash, Eliezer Masliah, Paul J. Massman, Arjun V. Masurkar,Wayne C. McCormick,Susan M. McCurry,Andrew McDavid, Stefan I. McDonough,Ann C. McKee,Marsel Mesulam,Bruce L. Miller,Carol A. Miller,Joshua W. Miller,Thomas J. Montine,Edwin S. Monuki, John C. Morris,Shubhabrata Mukherjee,Amanda Myers, Trung Dung Nguyen,Sid O’Bryant,John Olichney, Marcia G. Ory, Raymond F. Palmer, Joseph E. Parisi,Henry L. Paulson, Valory N. Pavlik,David Paydarfar,Victoria Pérez,Elaine R. Peskind, Ronald C. Petersen,Aimee Pierce, Marsha J. Polk,Wayne W. Poon,Huntington Potter,Liming Qu,Mary Quiceno,Joseph F. Quinn,Ashok Raj,Murray A. Raskind, Eric M. Reiman,Barry Reisberg,Joan Reisch,John M. Ringman,Erik D. Roberson, Monica Rodriguear,Ekaterina Rogaeva, Howard J. Rosen, Roger N. Rosenberg,Donald R. Royall,Mark A. Sager,Mary Sano,Andrew J. Saykin,Julie A. Schneider,Lon S. Schneider,William W. Seeley,Susan H. Slifer,Scott A. Small,Amanda Smith, Janet P. Smith,Joshua A. Sonnen,Salvatore Spina,Peter St George-Hyslop,Robert A. Stern,Alan Stevens,Stephen M. Strittmatter, David L. Sultzer, Russell H. Swerdlow,Rudolph E. Tanzi,Jeffrey L. Tilson, John Q. Trojanowski,Juan C. Troncoso,Debby W. Tsuang,Vivianna M. Van Deerlin,Linda J. Van Eldik,Jeffery M. Vance,Badri N. Vardarajan,Robert Vassar, Harry V. Vinters,Jean‐Paul Vonsattel,Sandra Weıntraub,Kathleen A. Welsh‐Bohmer,Patrice L. Whitehead,Ellen M. Wijsman,Kirk C. Wilhelmsen,Benjamin Williams,Jennifer Williamson,Henrik Wilms,Thomas S. Wingo, Thomas Wısnıewskı,Randall L. Woltjer, Martin Woon,Clinton B. Wright,Chuang‐Kuo Wu,Steven G. Younkin,Chang‐En Yu,Lei Yu, Xiongwei Zhu,Brian W. Kunkle,William S. Bush,Li-San Wang,Lindsay A. Farrer,Jonathan L. Haines, Richard Mayeux,Margaret A. Pericak‐Vance,Gerard D. Schellenberg,Gyungah Jun,Christiane Reitz,Adam C. Naj

medRxiv (Cold Spring Harbor Laboratory)(2023)

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摘要
Limited ancestral diversity has impaired our ability to detect risk variants more prevalent in non-European ancestry groups in genome-wide association studies (GWAS). We constructed and analyzed a multi-ancestry GWAS dataset in the Alzheimer's Disease (AD) Genetics Consortium (ADGC) to test for novel shared and ancestry-specific AD susceptibility loci and evaluate underlying genetic architecture in 37,382 non-Hispanic White (NHW), 6,728 African American, 8,899 Hispanic (HIS), and 3,232 East Asian individuals, performing within-ancestry fixed-effects meta-analysis followed by a cross-ancestry random-effects meta-analysis. We identified 13 loci with cross-ancestry associations including known loci at/near CR1 , BIN1 , TREM2 , CD2AP , PTK2B , CLU , SHARPIN , MS4A6A , PICALM , ABCA7 , APOE and two novel loci not previously reported at 11p12 ( LRRC4C ) and 12q24.13 ( LHX5-AS1 ). Reflecting the power of diverse ancestry in GWAS, we observed the SHARPIN locus using 7.1% the sample size of the original discovering single-ancestry GWAS (n=788,989). We additionally identified three GWS ancestry-specific loci at/near ( PTPRK ( P =2.4×10 -8 ) and GRB14 ( P =1.7×10 -8 ) in HIS), and KIAA0825 ( P =2.9×10 -8 in NHW). Pathway analysis implicated multiple amyloid regulation pathways (strongest with Padjusted =1.6×10 -4 ) and the classical complement pathway ( Padjusted =1.3×10 -3 ). Genes at/near our novel loci have known roles in neuronal development ( LRRC4C, LHX5-AS1 , and PTPRK ) and insulin receptor activity regulation ( GRB14 ). These findings provide compelling support for using traditionally-underrepresented populations for gene discovery, even with smaller sample sizes.
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alzheimers,individuals identifies<i>lrrc4c,genetics,multi-ancestry,genome-wide,meta-analysis,ancestry-specific
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