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GWAS Study

Genomic and Transcriptomic Association Studies Identify 16 Novel Susceptibility Loci for Venous Thromboembolism.

Lindström S, Wang L, Smith EN et al.

31420334 PubMed ID
GWAS Study Type
187204 Participants
136 Views
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Chapter I

Publication Details

Comprehensive information about this research publication

Authors

LS
Lindström S
WL
Wang L
SE
Smith EN
GW
Gordon W
VH
van Hylckama Vlieg A
DA
de Andrade M
BJ
Brody JA
PJ
Pattee JW
HJ
Haessler J
BB
Brumpton BM
CD
Chasman DI
SP
Suchon P
CM
Chen MH
TC
Turman C
GM
Germain M
WK
Wiggins KL
MJ
MacDonald J
BS
Braekkan SK
AS
Armasu SM
PN
Pankratz N
JR
Jackson RD
NJ
Nielsen JB
GF
Giulianini F
PM
Puurunen MK
IM
Ibrahim M
HS
Heckbert SR
DS
Damrauer SM
NP
Natarajan P
KD
Klarin D
DV
de Vries PS
SM
Sabater-Lleal M
HJ
Huffman JE
BT
Bammler TK
FK
Frazer KA
MB
McCauley BM
TK
Taylor K
PJ
Pankow JS
RA
Reiner AP
GM
Gabrielsen ME
DJ
Deleuze JF
OC
O'Donnell CJ
KJ
Kim J
MB
McKnight B
KP
Kraft P
HJ
Hansen JB
RF
Rosendaal FR
HJ
Heit JA
PB
Psaty BM
TW
Tang W
KC
Kooperberg C
HK
Hveem K
RP
Ridker PM
MP
Morange PE
JA
Johnson AD
KC
Kabrhel C
TD
Trégouët DA
SN
Smith NL
Chapter II

Abstract

Summary of the research findings

Venous thromboembolism (VTE) is a significant contributor to morbidity and mortality. To advance our understanding of the biology contributing to VTE, we conducted a genome-wide association study (GWAS) of VTE and a transcriptome-wide association study (TWAS) based on imputed gene expression from whole blood and liver. We meta-analyzed GWAS data from 18 studies for 30 234 VTE cases and 172 122 controls and assessed the association between 12 923 718 genetic variants and VTE. We generated variant prediction scores of gene expression from whole blood and liver tissue and assessed them for association with VTE. Mendelian randomization analyses were conducted for traits genetically associated with novel VTE loci. We identified 34 independent genetic signals for VTE risk from GWAS meta-analysis, of which 14 are newly reported associations. This included 11 newly associated genetic loci (C1orf198, PLEK, OSMR-AS1, NUGGC/SCARA5, GRK5, MPHOSPH9, ARID4A, PLCG2, SMG6, EIF5A, and STX10) of which 6 replicated, and 3 new independent signals in 3 known genes. Further, TWAS identified 5 additional genetic loci with imputed gene expression levels differing between cases and controls in whole blood (SH2B3, SPSB1, RP11-747H7.3, RP4-737E23.2) and in liver (ERAP1). At some GWAS loci, we found suggestive evidence that the VTE association signal for novel and previously known regions colocalized with expression quantitative trait locus signals. Mendelian randomization analyses suggested that blood traits may contribute to the underlying risk of VTE. To conclude, we identified 16 novel susceptibility loci for VTE; for some loci, the association signals are likely mediated through gene expression of nearby genes.

29,435 European ancestry cases, 157,769 European ancestry controls

Chapter III

Study Statistics

Key metrics and study information

187204
Total Participants
GWAS
Study Type
No
Replicated
European, African American or Afro-Caribbean
Ancestry
U.S., France, Netherlands, Norway, U.K.
Recruitment Country
Chapter IV

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