Genome-wide association analyses identify new risk variants and the genetic architecture of amyotrophic lateral sclerosis.

van Rheenen, W.; Shatunov, A.; Dekker, A.M.; McLaughlin, R.L.; Diekstra, F.P.; Pulit, S.L.; van der Spek, R.A.; Võsa, U.; de Jong, S.; Robinson, M.R.; Yang, J.; Fogh, I.; van Doormaal, P.T.; Tazelaar, G.H.; Koppers, M.; Blokhuis, A.M.; Sproviero, W.; Jones, A.R.; Kenna, K.P.; van Eijk, K.R.; Harschnitz, O.; Schellevis, R.D.; Brands, W.J.; Medic, J.; Menelaou, A.; Vajda, A.; Ticozzi, N.; Lin, K.; Rogelj, B.; Vrabec, K.; Ravnik-Glavač, M.; Koritnik, B.; Zidar, J.; Leonardis, L.; Grošelj, L.D.; Millecamps, S.; Salachas, F.; Meininger, V.; de Carvalho, M.; Pinto, S.; Mora, J.S.; Rojas-García, R.; Polak, M.; Chandran, S.; Colville, S.; Swingler, R.; Morrison, K.E.; Shaw, P.J.; Hardy, J.; Orrell, R.W.; Pittman, A.; Sidle, K.; Fratta, P.; Malaspina, A.; Topp, S.; Petri, S.; Abdulla, S.; Drepper, C.; Sendtner, M.; Meyer, T.; Ophoff, R.A.; Staats, K.A.; Wiedau-Pazos, M.; Lomen-Hoerth, C.; Van Deerlin, V.M.; Trojanowski, J.Q.; Elman, L.; McCluskey, L.; Basak, A.N.; Tunca, C.; Hamzeiy, H.; Parman, Y.; Meitinger, T.; Lichtner, P.; Radivojkov-Blagojevic, M.; Andres, C.R.; Maurel, C.; Bensimon, G.; Landwehrmeyer, B.; Brice, A.; Payan, C.A.; Saker-Delye, S.; Dürr, A.; Wood, N.W.; Tittmann, L.; Lieb, W.; Franke, A.; Rietschel, M.; Cichon, S.; Nöthen, M.M.; Amouyel, P.; Tzourio, C.; Dartigues, J.F.; Uitterlinden, A.G.; Rivadeneira, F.; Estrada, K.; Hofman, A.; Curtis, C.; Blauw, H.M.; van der Kooi, A.J.; de Visser, M.; Goris, A.; Weber, M.; Shaw, C.E.; Smith, B.N.; Pansarasa, O.; Cereda, C.; Del Bo, R.; Comi, G.P.; D'Alfonso, S.; Bertolin, C.; Sorarù, G.; Mazzini, L.; Pensato, V.; Gellera, C.; Tiloca, C.; Ratti, A.; Calvo, A.; Moglia, C.; Brunetti, M.; Arcuti, S.; Capozzo, R.; Zecca, C.; Lunetta, C.; Penco, S.; Riva, N.; Padovani, A.; Filosto, M.; Muller, B.; Stuit, R.J.; Blair, I.; Zhang, K.; McCann, E.P.; Fifita, J.A.; Nicholson, G.A.; Rowe, D.B.; Pamphlett, R.; Kiernan, M.C.; Grosskreutz, J.; Witte, O.W.; Ringer, T.; Prell, T.; Stubendorff, B.; Kurth, I.; Hübner, C.A.; Leigh, P.N.; Casale, F.; Chio, A.; Beghi, E.; Pupillo, E.; Tortelli, R.; Logroscino, G.; Powell, J.; Ludolph, A.C.; Weishaupt, J.H.; Robberecht, W.; Van Damme, P.; Franke, L.; Pers, T.H.; Brown, R.H.; Glass, J.D.; Landers, J.E.; Hardiman, O.; Andersen, P.M.; Corcia, P.; Vourc'h, P.; Silani, V.; Wray, N.R.; Visscher, P.M.; de Bakker, P.I.; van Es, M.A.; Pasterkamp, R.J.; Lewis, C.M.; Breen, G.; Al-Chalabi, A.; van den Berg, L.H.; Veldink, J.H.

doi:10.1038/ng.3622

Genome-wide association analyses identify new risk variants and the genetic architecture of amyotrophic lateral sclerosis.

Détails

Demande d'une copie

ID Serval

serval:BIB_3F1A02E2DA61

Type

Article: article d'un périodique ou d'un magazine.

Collection

Publications

Institution

Production externe

Titre

Genome-wide association analyses identify new risk variants and the genetic architecture of amyotrophic lateral sclerosis.

Périodique

Nature Genetics

Auteur⸱e⸱s

van Rheenen W., Shatunov A., Dekker A.M., McLaughlin R.L., Diekstra F.P., Pulit S.L., van der Spek R.A., Võsa U., de Jong S., Robinson M.R., Yang J., Fogh I., van Doormaal P.T., Tazelaar G.H., Koppers M., Blokhuis A.M., Sproviero W., Jones A.R., Kenna K.P., van Eijk K.R., Harschnitz O., Schellevis R.D., Brands W.J., Medic J., Menelaou A., Vajda A., Ticozzi N., Lin K., Rogelj B., Vrabec K., Ravnik-Glavač M., Koritnik B., Zidar J., Leonardis L., Grošelj L.D., Millecamps S., Salachas F., Meininger V., de Carvalho M., Pinto S., Mora J.S., Rojas-García R., Polak M., Chandran S., Colville S., Swingler R., Morrison K.E., Shaw P.J., Hardy J., Orrell R.W., Pittman A., Sidle K., Fratta P., Malaspina A., Topp S., Petri S., Abdulla S., Drepper C., Sendtner M., Meyer T., Ophoff R.A., Staats K.A., Wiedau-Pazos M., Lomen-Hoerth C., Van Deerlin V.M., Trojanowski J.Q., Elman L., McCluskey L., Basak A.N., Tunca C., Hamzeiy H., Parman Y., Meitinger T., Lichtner P., Radivojkov-Blagojevic M., Andres C.R., Maurel C., Bensimon G., Landwehrmeyer B., Brice A., Payan C.A., Saker-Delye S., Dürr A., Wood N.W., Tittmann L., Lieb W., Franke A., Rietschel M., Cichon S., Nöthen M.M., Amouyel P., Tzourio C., Dartigues J.F., Uitterlinden A.G., Rivadeneira F., Estrada K., Hofman A., Curtis C., Blauw H.M., van der Kooi A.J., de Visser M., Goris A., Weber M., Shaw C.E., Smith B.N., Pansarasa O., Cereda C., Del Bo R., Comi G.P., D'Alfonso S., Bertolin C., Sorarù G., Mazzini L., Pensato V., Gellera C., Tiloca C., Ratti A., Calvo A., Moglia C., Brunetti M., Arcuti S., Capozzo R., Zecca C., Lunetta C., Penco S., Riva N., Padovani A., Filosto M., Muller B., Stuit R.J., Blair I., Zhang K., McCann E.P., Fifita J.A., Nicholson G.A., Rowe D.B., Pamphlett R., Kiernan M.C., Grosskreutz J., Witte O.W., Ringer T., Prell T., Stubendorff B., Kurth I., Hübner C.A., Leigh P.N., Casale F., Chio A., Beghi E., Pupillo E., Tortelli R., Logroscino G., Powell J., Ludolph A.C., Weishaupt J.H., Robberecht W., Van Damme P., Franke L., Pers T.H., Brown R.H., Glass J.D., Landers J.E., Hardiman O., Andersen P.M., Corcia P., Vourc'h P., Silani V., Wray N.R., Visscher P.M., de Bakker P.I., van Es M.A., Pasterkamp R.J., Lewis C.M., Breen G., Al-Chalabi A., van den Berg L.H., Veldink J.H.

Collaborateur⸱rice⸱s

PARALS Registry, SLALOM Group, SLAP Registry, FALS Sequencing Consortium, SLAGEN Consortium, NNIPPS Study Group

ISSN

1546-1718 (Electronic)

ISSN-L

1061-4036

Statut éditorial

Publié

Date de publication

2016

Peer-reviewed

Oui

Volume

Numéro

Pages

1043-1048

Langue

anglais

Résumé

To elucidate the genetic architecture of amyotrophic lateral sclerosis (ALS) and find associated loci, we assembled a custom imputation reference panel from whole-genome-sequenced patients with ALS and matched controls (n = 1,861). Through imputation and mixed-model association analysis in 12,577 cases and 23,475 controls, combined with 2,579 cases and 2,767 controls in an independent replication cohort, we fine-mapped a new risk locus on chromosome 21 and identified C21orf2 as a gene associated with ALS risk. In addition, we identified MOBP and SCFD1 as new associated risk loci. We established evidence of ALS being a complex genetic trait with a polygenic architecture. Furthermore, we estimated the SNP-based heritability at 8.5%, with a distinct and important role for low-frequency variants (frequency 1-10%). This study motivates the interrogation of larger samples with full genome coverage to identify rare causal variants that underpin ALS risk.

Mots-clé

Amyotrophic Lateral Sclerosis/epidemiology, Amyotrophic Lateral Sclerosis/genetics, Case-Control Studies, Cohort Studies, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Munc18 Proteins/genetics, Mutation/genetics, Myelin Proteins/genetics, Netherlands/epidemiology, Proteins/genetics

DOI

10.1038/ng.3622

Pubmed

27455348

Web of science

000382398800015

Création de la notice

06/12/2017 13:42

Dernière modification de la notice

20/08/2019 14:36

Données d'usage

SERVAL

serveur académique lausannois

Genome-wide association analyses identify new risk variants and the genetic architecture of amyotrophic lateral sclerosis.

Détails