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GWAS Study

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

van Rheenen W, Shatunov A, Dekker AM et al.

27455348 PubMed ID
GWAS Study Type
41398 Participants
Explore Publication View on PubMed
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Chapter I

Publication Details

Comprehensive information about this research publication

Journal Nat Genet
Publication Date 2016-07-25
Disease/Trait Amyotrophic lateral sclerosis
DOI 10.1038/ng.3622
ISSN 1546-1718

Authors

VR
van Rheenen W
SA
Shatunov A
DA
Dekker AM
MR
McLaughlin RL
DF
Diekstra FP
PS
Pulit SL
VD
van der Spek RA
VU
Võsa U
DJ
de Jong S
RM
Robinson MR
YJ
Yang J
FI
Fogh I
VD
van Doormaal PT
TG
Tazelaar GH
KM
Koppers M
BA
Blokhuis AM
SW
Sproviero W
JA
Jones AR
KK
Kenna KP
VE
van Eijk KR
HO
Harschnitz O
SR
Schellevis RD
BW
Brands WJ
MJ
Medic J
MA
Menelaou A
VA
Vajda A
TN
Ticozzi N
LK
Lin K
RB
Rogelj B
VK
Vrabec K
RM
Ravnik-Glavač M
KB
Koritnik B
ZJ
Zidar J
LL
Leonardis L
GL
Grošelj LD
MS
Millecamps S
SF
Salachas F
MV
Meininger V
DC
de Carvalho M
PS
Pinto S
MJ
Mora JS
RR
Rojas-García R
PM
Polak M
CS
Chandran S
CS
Colville S
SR
Swingler R
MK
Morrison KE
SP
Shaw PJ
HJ
Hardy J
OR
Orrell RW
PA
Pittman A
SK
Sidle K
FP
Fratta P
MA
Malaspina A
TS
Topp S
PS
Petri S
AS
Abdulla S
DC
Drepper C
SM
Sendtner M
MT
Meyer T
OR
Ophoff RA
SK
Staats KA
WM
Wiedau-Pazos M
LC
Lomen-Hoerth C
VD
Van Deerlin VM
TJ
Trojanowski JQ
EL
Elman L
ML
McCluskey L
BA
Basak AN
TC
Tunca C
HH
Hamzeiy H
PY
Parman Y
MT
Meitinger T
LP
Lichtner P
RM
Radivojkov-Blagojevic M
AC
Andres CR
MC
Maurel C
BG
Bensimon G
LB
Landwehrmeyer B
BA
Brice A
PC
Payan CA
SS
Saker-Delye S
DA
Dürr A
WN
Wood NW
TL
Tittmann L
LW
Lieb W
FA
Franke A
RM
Rietschel M
CS
Cichon S
NM
Nöthen MM
AP
Amouyel P
TC
Tzourio C
DJ
Dartigues JF
UA
Uitterlinden AG
RF
Rivadeneira F
EK
Estrada K
HA
Hofman A
CC
Curtis C
BH
Blauw HM
VD
van der Kooi AJ
DV
de Visser M
GA
Goris A
WM
Weber M
SC
Shaw CE
SB
Smith BN
PO
Pansarasa O
CC
Cereda C
DB
Del Bo R
CG
Comi GP
DS
D'Alfonso S
BC
Bertolin C
SG
Sorarù G
ML
Mazzini L
PV
Pensato V
GC
Gellera C
TC
Tiloca C
RA
Ratti A
CA
Calvo A
MC
Moglia C
BM
Brunetti M
AS
Arcuti S
CR
Capozzo R
ZC
Zecca C
LC
Lunetta C
PS
Penco S
RN
Riva N
PA
Padovani A
FM
Filosto M
MB
Muller B
SR
Stuit RJ
BI
Blair I
ZK
Zhang K
ME
McCann EP
FJ
Fifita JA
NG
Nicholson GA
RD
Rowe DB
PR
Pamphlett R
KM
Kiernan MC
GJ
Grosskreutz J
WO
Witte OW
RT
Ringer T
PT
Prell T
SB
Stubendorff B
KI
Kurth I
HC
Hübner CA
LP
Leigh PN
CF
Casale F
CA
Chio A
BE
Beghi E
PE
Pupillo E
TR
Tortelli R
LG
Logroscino G
PJ
Powell J
LA
Ludolph AC
WJ
Weishaupt JH
RW
Robberecht W
VD
Van Damme P
FL
Franke L
PT
Pers TH
BR
Brown RH
GJ
Glass JD
LJ
Landers JE
HO
Hardiman O
AP
Andersen PM
CP
Corcia P
VP
Vourc'h P
SV
Silani V
WN
Wray NR
VP
Visscher PM
DB
de Bakker PI
VE
van Es MA
PR
Pasterkamp RJ
LC
Lewis CM
BG
Breen G
AA
Al-Chalabi A
VD
van den Berg LH
VJ
Veldink JH
View on PubMed View DOI More from Journal Similar Studies
Chapter II

Abstract

Summary of the research findings

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.

12,577 European ancestry cases, 23,475 European ancestry controls

Chapter III

Study Statistics

Key metrics and study information

41398
Total Participants
GWAS
Study Type
Yes
Replicated
2,579 European ancestry cases, 2,767 European ancestry controls
Replication Participants
European
Ancestry
U.S., Belgium, France, Germany, Netherlands, Switzerland, Finland, Republic of Ireland, Sweden, U.K., Italy, Portugal, Spain, Australia, Turkey
Recruitment Country
Chapter IV

Analysis

Comprehensive review of health and genetic findings

Important Disclaimer: This review has been performed semi-automatically and is provided for informational purposes only. While we strive for accuracy, this analysis may contain errors, omissions, or misinterpretations of the original research. DNA Genics disclaims all liability for any inaccuracies, errors, or consequences arising from the use of this information. Users should independently verify all information and consult original research publications before making any decisions based on this content. This analysis is not intended as a substitute for professional scientific review or medical advice.

Analysis In Progress

Our analysis of this publication is currently being prepared. Please check back soon for comprehensive insights into the health and genetic findings discussed in this research.

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