Large-scale exome analyses reveal new rare variant contributions in amyotrophic lateral sclerosis

大规模外显子组分析揭示了肌萎缩侧索硬化症中新的罕见变异贡献

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作者:Hop,Paul J,Kooyman,Maarten,Kenna,Brendan J,Zwamborn,Ramona A J,van Eijk,Kristel R,Wang,Yan,van Dijk,Charlotte H,Bekema,Erwin,van Rheenen,Wouter,Beele,Paul,van Vugt,Joke J F A,Khleifat,Ahmad Al,Iacoangeli,Alfredo,Cooper-Knock,Johnathan,Smith,Bradley N,Topp,Simon,van der Kooi,Anneke J,Fominykh,Vera,Drory,Vivian,Lerner,Yossef,Shovman,Yehuda,Rowe,Dominic B,Williams,Kelly L,McLaughlin,Russell L,Hurt,Jessica,Huang,Yunfeng,Chen,Chia-Yen,Tsai,Ellen,Runz,Heiko,Aronica,Eleonora,Groen,Ewout J N,van Es,Michael A,Pasterkamp,R Jeroen,Farhan,Sali M K,Garton,Fleur C,McRae,Allan F,McCombe,Pamela A,Henderson,Robert D,Fan,Dongsheng,Šlachtová,Lenka,Høyer,Helle,Nishimura,Agnes L,Cauchi,Ruben J,Brylev,Lev,Rogelj,Boris,Koritnik,Blaž,Zidar,Janez,Salas,Teresa,Mora Pardina,Jesus S,Gotkine,Marc,Povedano,Monica,Corcia,Philippe,Vourc'h,Patrick,Couratier,Philippe,Weber,Markus,Kiernan,Matthew C,Pamphlett,Roger,Blair,Ian P,de Carvalho,Mamede,Başak,Nazli A,Ingre,Caroline,Andersen,Peter M,Zinman,Lorne,Rogaeva,Ekaterina,MacKenzie,Ian R,Dupre,Nicolas,Rouleau,Guy A,Traynor,Bryan J,Ticozzi,Nicola,Chiò,Adriano,Silani,Vincenzo,Hardiman,Orla,Phatnani,Hemali,Harms,Matthew B,Dalgard,Clifton L,Glass,Jonathan D,Landers,John E,Van Damme,Philip,Morrison,Karen E,Shaw,Pamela J,Shaw,Chris E,Al-Chalabi,Ammar,van den Berg,Leonard H,Kenna,Kevin P,Veldink,Jan H
期刊:Nature Genetics影响因子:29.000
时间:2026起止号:2026 Apr;58(4):717-725
doi:10.1038/s41588-026-02535-9

Abstract

Amyotrophic lateral sclerosis (ALS) is a heritable disorder where rare variants with low-to-moderate penetrance are thought to dominate genetic risk. To identify such rare variants, we harmonized and analyzed exome data from 22 cohorts, totaling 17,919 individuals with ALS and 200,703 controls across discovery and replication phases. Rare variant analyses identified several new risk genes, with replication confirming association of YKT6 and supporting HTR3C, GBGT1 and KNTC1. We also provide strong, independent validation for genes with limited previous evidence: ARPP21, DNAJC7 and CFAP410. Notably, in ARPP21, we identified a new high-effect variant (p.P747L) and confirmed that p.P563L is an ALS-associated variant leading to an aggressive disease course. Beyond new discoveries, our analyses largely recapitulated the known genetic architecture of ALS, identifying risk variants in over 20% of cases and supporting a cumulative oligogenic risk model. These findings highlight new translational targets and show that rare variant analyses capture substantially more genetic risk than common variant genome-wide association studies.

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