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GWAS Study

Common variation at 1q23.3, 2p23.3, 2q33.3, and 2p21 influences risk of acute myeloid leukemia.

Ranasinghe D, Lin WY, Fordham SE et al.

41610418 PubMed ID
GWAS Study Type
17648 Participants
116 Views
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Chapter I

Publication Details

Comprehensive information about this research publication

Authors

RD
Ranasinghe D
LW
Lin WY
FS
Fordham SE
AA
Alharbi A
SN
Sunter NJ
EC
Elstob C
NM
Nahari MH
XY
Xu Y
PC
Park C
HE
Hungate E
QA
Quante A
SK
Strauch K
GC
Gieger C
SA
Skol A
RT
Rahman T
SL
Sucheston-Campbell L
HT
Hahn T
CA
Clay-Gilmour AI
JG
Jones GL
MH
Marr HJ
JG
Jackson GH
MT
Menne T
CM
Collin M
IA
Ivey A
HR
Hills RK
BA
Burnett AK
RN
Russell NH
FJ
Fitzgibbon J
LR
Larson RA
LB
Le Beau MM
SW
Stock W
HO
Heidenreich O
EA
Enshaei A
GD
Gunasinghe D
HZ
Hawking ZL
HH
Heslop H
ND
Nandana D
DB
Di B
PA
Plokhuta A
BI
Brown IT
AD
Allsup DJ
HR
Houlston RS
CA
Collins A
MP
Milne P
NJ
Norden J
DA
Dickinson AM
LC
Lendrem C
DA
Daly AK
PL
Palm L
PK
Piechocki K
JS
Jeffries S
BM
Bornhäuser M
RC
Röllig C
AH
Altmann H
RL
Ruhnke L
KD
Kunadt D
WL
Wagenführ L
CH
Cordell HJ
DR
Darlay R
AM
Andersen MK
FM
Fontana MC
MG
Martinelli G
MG
Marconi G
SM
Sanz MA
CJ
Cervera J
GI
Gómez-Seguí I
CT
Cluzeau T
MC
Moreilhon C
RS
Raynaud S
SH
Sill H
VM
Voso MT
DH
Dombret H
CM
Cheok M
PC
Preudhomme C
GR
Gale RE
LD
Linch D
WJ
Weisinger J
MA
Masszi A
ND
Nowak D
HW
Hofmann WK
GA
Gilkes A
PK
Porkka K
MF
Milosevic Feenstra JD
KR
Kralovics R
WJ
Wang J
MM
Meggendorfer M
HT
Haferlach T
KS
Krizsán S
BC
Bödör C
PB
Parkin B
MS
Malek SN
SF
Stölzel F
OK
Onel K
AJ
Allan JM
Chapter II

Abstract

Summary of the research findings

Acute myeloid leukemia (AML) is a complex hematologic malignancy with multiple disease subgroups defined by somatic mutations and heterogeneous outcomes. Although genome-wide association studies (GWAS) have identified a small number of common genetic variants influencing AML risk, the heritable component of this disease outside of familial susceptibility remains largely undefined. Here, we perform a meta-analysis of 4 published GWAS plus 2 new GWAS, totaling 4710 AML cases and 12 938 controls. We identify a new genome-wide significant risk locus for pan-AML at 2p23.3 (rs4665765; P = 1.35 × 10-8; EFR3B, POMC, DNMT3A, and DNAJC27), which also significantly associates with patient survival (P = 6.09 × 10-3). Our analysis also identifies 3 new genome-wide significant risk loci for disease subgroups, including AML with deletions of chromosome 5 and/or 7 at 1q23.3 (rs12078864; P = 7.0 × 10-10; DUSP23) and cytogenetically complex AML at 2q33.3 (rs12988876; P = 3.28 × 10-8; PARD3B) and 2p21 (rs79918355; P = 1.60 × 10-9; EPCAM). We also investigated loci previously associated with the risk of clonal hematopoiesis (CH) or CH of indeterminate potential and identified several variants associated with the risk of AML. Our results further inform on AML etiology and demonstrate the existence of disease subgroup specific risk loci.

4,710 European ancestry cases, 12,938 European ancestry controls

Chapter III

Study Statistics

Key metrics and study information

17648
Total Participants
GWAS
Study Type
No
Replicated
European
Ancestry
U.S., Hungary, Finland, U.K., Germany
Recruitment Country
Chapter IV

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