Genome-wide Analyses Identify KIF5A as a Novel ALS Gene

全基因组分析鉴定出KIF5A是一种新的ALS基因

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作者:Nicolas,Aude,Kenna,Kevin P,Renton,Alan E,Ticozzi,Nicola,Faghri,Faraz,Chia,Ruth,Dominov,Janice A,Kenna,Brendan J,Nalls,Mike A,Keagle,Pamela,Rivera,Alberto M,van Rheenen,Wouter,Murphy,Natalie A,van Vugt,Joke J F A,Geiger,Joshua T,Van der Spek,Rick A,Pliner,Hannah A,Shankaracharya,Smith,Bradley N,Marangi,Giuseppe,Topp,Simon D,Abramzon,Yevgeniya,Gkazi,Athina Soragia,Eicher,John D,Kenna,Aoife,Mora,Gabriele,Calvo,Andrea,Mazzini,Letizia,Riva,Nilo,Mandrioli,Jessica,Caponnetto,Claudia,Battistini,Stefania,Volanti,Paolo,La Bella,Vincenzo,Conforti,Francesca L,Borghero,Giuseppe,Messina,Sonia,Simone,Isabella L,Trojsi,Francesca,Salvi,Fabrizio,Logullo,Francesco O,D'Alfonso,Sandra,Corrado,Lucia,Capasso,Margherita,Ferrucci,Luigi,Moreno,Cristiane de Araujo Martins,Kamalakaran,Sitharthan,Goldstein,David B,Gitler,Aaron D,Harris,Tim,Myers,Richard M,Phatnani,Hemali,Musunuri,Rajeeva Lochan,Evani,Uday Shankar,Abhyankar,Avinash,Zody,Michael C,Kaye,Julia,Finkbeiner,Steven,Wyman,Stacia K,LeNail,Alex,Lima,Leandro,Fraenkel,Ernest,Svendsen,Clive N,Thompson,Leslie M,Van Eyk,Jennifer E,Berry,James D,Miller,Timothy M,Kolb,Stephen J,Cudkowicz,Merit,Baxi,Emily,Benatar,Michael,Taylor,J Paul,Rampersaud,Evadnie,Wu,Gang,Wuu,Joanne,Lauria,Giuseppe,Verde,Federico,Fogh,Isabella,Tiloca,Cinzia,Comi,Giacomo P,Sorarù,Gianni,Cereda,Cristina,Corcia,Philippe,Laaksovirta,Hannu,Myllykangas,Liisa,Jansson,Lilja,Valori,Miko,Ealing,John,Hamdalla,Hisham,Rollinson,Sara,Pickering-Brown,Stuart,Orrell,Richard W,Sidle,Katie C,Malaspina,Andrea,Hardy,John,Singleton,Andrew B,Johnson,Janel O,Arepalli,Sampath,Sapp,Peter C,McKenna-Yasek,Diane,Polak,Meraida,Asress,Seneshaw,Al-Sarraj,Safa,King,Andrew,Troakes,Claire,Vance,Caroline,de Belleroche,Jacqueline,Baas,Frank,Ten Asbroek,Anneloor L M A,Muñoz-Blanco,José Luis,Hernandez,Dena G,Ding,Jinhui,Gibbs,J Raphael,Scholz,Sonja W,Floeter,Mary Kay,Campbell,Roy H,Landi,Francesco,Bowser,Robert,Pulst,Stefan M,Ravits,John M,MacGowan,Daniel J L,Kirby,Janine,Pioro,Erik P,Pamphlett,Roger,Broach,James,Gerhard,Glenn,Dunckley,Travis L,Brady,Christopher B,Kowall,Neil W,Troncoso,Juan C,Le Ber,Isabelle,Mouzat,Kevin,Lumbroso,Serge,Heiman-Patterson,Terry D,Kamel,Freya,Van Den Bosch,Ludo,Baloh,Robert H,Strom,Tim M,Meitinger,Thomas,Shatunov,Aleksey,Van Eijk,Kristel R,de Carvalho,Mamede,Kooyman,Maarten,Middelkoop,Bas,Moisse,Matthieu,McLaughlin,Russell L,Van Es,Michael A,Weber,Markus,Boylan,Kevin B,Van Blitterswijk,Marka,Rademakers,Rosa,Morrison,Karen E,Basak,A Nazli,Mora,Jesús S,Drory,Vivian E,Shaw,Pamela J,Turner,Martin R,Talbot,Kevin,Hardiman,Orla,Williams,Kelly L,Fifita,Jennifer A,Nicholson,Garth A,Blair,Ian P,Rouleau,Guy A,Esteban-Pérez,Jesús,García-Redondo,Alberto,Al-Chalabi,Ammar,Rogaeva,Ekaterina,Zinman,Lorne,Ostrow,Lyle W,Maragakis,Nicholas J,Rothstein,Jeffrey D,Simmons,Zachary,Cooper-Knock,Johnathan,Brice,Alexis,Goutman,Stephen A,Feldman,Eva L,Gibson,Summer B,Taroni,Franco,Ratti,Antonia,Gellera,Cinzia,Van Damme,Philip,Robberecht,Wim,Fratta,Pietro,Sabatelli,Mario,Lunetta,Christian,Ludolph,Albert C,Andersen,Peter M,Weishaupt,Jochen H,Camu,William,Trojanowski,John Q,Van Deerlin,Vivianna M,Brown,Robert H Jr,van den Berg,Leonard H,Veldink,Jan H,Harms,Matthew B,Glass,Jonathan D,Stone,David J,Tienari,Pentti,Silani,Vincenzo,Chiò,Adriano,Shaw,Christopher E,Traynor,Bryan J,Landers,John E
期刊:Neuron影响因子:15.000
时间:2018起止号:2018 Mar 21;97(6):1267-1288
doi:10.1016/j.neuron.2018.02.027

Abstract

To identify novel genes associated with ALS, we undertook two lines of investigation. We carried out a genome-wide association study comparing 20,806 ALS cases and 59,804 controls. Independently, we performed a rare variant burden analysis comparing 1,138 index familial ALS cases and 19,494 controls. Through both approaches, we identified kinesin family member 5A (KIF5A) as a novel gene associated with ALS. Interestingly, mutations predominantly in the N-terminal motor domain of KIF5A are causative for two neurodegenerative diseases: hereditary spastic paraplegia (SPG10) and Charcot-Marie-Tooth type 2 (CMT2). In contrast, ALS-associated mutations are primarily located at the C-terminal cargo-binding tail domain and patients harboring loss-of-function mutations displayed an extended survival relative to typical ALS cases. Taken together, these results broaden the phenotype spectrum resulting from mutations in KIF5A and strengthen the role of cytoskeletal defects in the pathogenesis of ALS.

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