NEK1 genetic variability in a Belgian cohort of ALS and ALS-FTD patients.

We evaluated the genetic impact of the amyotrophic lateral sclerosis (ALS) risk gene never in mitosis gene a-related kinase 1 (NEK1) in a Belgian cohort of 278 patients with ALS (n = 245) or ALS with frontotemporal dementia (ALS-FTD, n = 33) and 609 control individuals. We identified 2 ALS patients carrying a loss-of-function (LOF) mutation, p.Leu854Tyrfs*2 and p.Tyr871Valfs*17, that was absent in the control group. A third LOF variant p.Ser1036* was present in 2 sibs with familial ALS but also in an unrelated control person. Missense variants were common in both patients (3.6%) and controls... Mehr ...

Verfasser: Nguyen, Hung Phuoc
Van Mossevelde, Sara
Dillen, Lubina
De Bleecker, Jan L
Moisse, Matthieu
Van Damme, Philip
Van Broeckhoven, Christine
van der Zee, Julie
BELNEU Consortium
Ivanoiu, Adrian
Dokumenttyp: Artikel
Erscheinungsdatum: 2018
Verlag/Hrsg.: Elsevier
Schlagwörter: Aged / Amyotrophic Lateral Sclerosis / Belgium / Cohort Studies / Female / Frontotemporal Dementia / Gene Frequency / Genetic Association Studies / Genetic Variation / Humans / Loss of Function Mutation / Male / Middle Aged / NIMA-Related Kinase 1 / Risk / Amyotrophic lateral sclerosis (ALS) / Frontotemporal dementia (FTD) / NEK1
Sprache: Englisch
Permalink: https://search.fid-benelux.de/Record/base-29295190
Datenquelle: BASE; Originalkatalog
Powered By: BASE
Link(s) : http://hdl.handle.net/2078.1/221796

We evaluated the genetic impact of the amyotrophic lateral sclerosis (ALS) risk gene never in mitosis gene a-related kinase 1 (NEK1) in a Belgian cohort of 278 patients with ALS (n = 245) or ALS with frontotemporal dementia (ALS-FTD, n = 33) and 609 control individuals. We identified 2 ALS patients carrying a loss-of-function (LOF) mutation, p.Leu854Tyrfs*2 and p.Tyr871Valfs*17, that was absent in the control group. A third LOF variant p.Ser1036* was present in 2 sibs with familial ALS but also in an unrelated control person. Missense variants were common in both patients (3.6%) and controls (3.0%). The missense variant, p.Arg261His, which was previously associated with ALS risk, was detected with a minor allele frequency of 0.90% in patients compared to 0.33% in controls. Taken together, NEK1 LOF variants accounted for 1.1% of patients, although interpretation of pathogenicity and penetrance is complicated by the observation of occasional LOF variants in unaffected individuals (0.16%). Furthermore, enrichment of additional ALS gene mutations was observed in NEK1 carriers, suggestive of a "second hit" model were NEK1 variants may modify disease presentation of driving mutations.