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GWAS Study

Genome-wide association analyses define pathogenic signaling pathways and prioritize drug targets for IgA nephropathy.

Kiryluk K, Sanchez-Rodriguez E, Zhou XJ et al.

37337107 PubMed ID
GWAS Study Type
25852 Participants
76 Views
Explore Publication View on PubMed
Scroll to explore
Chapter I

Publication Details

Comprehensive information about this research publication

Journal Nat Genet
Publication Date 2023-06-19
Disease/Trait IgA nephropathy
DOI 10.1038/s41588-023-01422-x
ISSN 1546-1718

Authors

KK
Kiryluk K
SE
Sanchez-Rodriguez E
ZX
Zhou XJ
ZF
Zanoni F
LL
Liu L
MN
Mladkova N
KA
Khan A
MM
Marasa M
ZJ
Zhang JY
BO
Balderes O
SS
Sanna-Cherchi S
BA
Bomback AS
CP
Canetta PA
AG
Appel GB
RJ
Radhakrishnan J
TH
Trimarchi H
SB
Sprangers B
CD
Cattran DC
RH
Reich H
PY
Pei Y
RP
Ravani P
GK
Galesic K
MD
Maixnerova D
TV
Tesar V
SB
Stengel B
MM
Metzger M
CG
Canaud G
MN
Maillard N
BF
Berthoux F
BL
Berthelot L
PE
Pillebout E
MR
Monteiro R
NR
Nelson R
WR
Wyatt RJ
SW
Smoyer W
MJ
Mahan J
SA
Samhar AA
HG
Hidalgo G
QA
Quiroga A
WP
Weng P
SR
Sreedharan R
SD
Selewski D
DK
Davis K
KM
Kallash M
VT
Vasylyeva TL
RM
Rheault M
CA
Chishti A
RD
Ranch D
WS
Wenderfer SE
SD
Samsonov D
CD
Claes DJ
AO
Akchurin O
GD
Goumenos D
SM
Stangou M
NJ
Nagy J
KT
Kovacs T
FE
Fiaccadori E
AA
Amoroso A
BC
Barlassina C
CD
Cusi D
DV
Del Vecchio L
BG
Battaglia GG
BM
Bodria M
BE
Boer E
BL
Bono L
BG
Boscutti G
CG
Caridi G
LF
Lugani F
GG
Ghiggeri G
CR
Coppo R
PL
Peruzzi L
EV
Esposito V
EC
Esposito C
FS
Feriozzi S
PR
Polci R
FG
Frasca G
GM
Galliani M
GM
Garozzo M
MA
Mitrotti A
GL
Gesualdo L
GS
Granata S
ZG
Zaza G
LF
Londrino F
MR
Magistroni R
PI
Pisani I
MA
Magnano A
MC
Marcantoni C
MP
Messa P
MR
Mignani R
PA
Pani A
PC
Ponticelli C
RD
Roccatello D
SM
Salvadori M
SE
Salvi E
SD
Santoro D
GG
Gembillo G
SS
Savoldi S
SD
Spotti D
ZP
Zamboli P
IC
Izzi C
AF
Alberici F
DE
Delbarba E
FM
Florczak M
KN
Krata N
MK
Mucha K
PL
Pączek L
NS
Niemczyk S
MB
Moszczuk B
PM
Pańczyk-Tomaszewska M
MM
Mizerska-Wasiak M
PA
Perkowska-Ptasińska A
BT
Bączkowska T
DM
Durlik M
PK
Pawlaczyk K
SP
Sikora P
ZM
Zaniew M
KD
Kaminska D
KM
Krajewska M
KI
Kuzmiuk-Glembin I
HZ
Heleniak Z
BB
Bullo-Piontecka B
LT
Liberek T
DA
Dębska-Slizien A
HT
Hryszko T
MA
Materna-Kiryluk A
MM
Miklaszewska M
SM
Szczepańska M
DK
Dyga K
ME
Machura E
SK
Siniewicz-Luzeńczyk K
PM
Pawlak-Bratkowska M
TM
Tkaczyk M
RD
Runowski D
KN
Kwella N
DD
Drożdż D
HI
Habura I
KF
Kronenberg F
PL
Prikhodina L
VH
van Heel D
FB
Fontaine B
CC
Cotsapas C
WC
Wijmenga C
FA
Franke A
AV
Annese V
GP
Gregersen PK
PS
Parameswaran S
WM
Weirauch M
KL
Kottyan L
HJ
Harley JB
SH
Suzuki H
NI
Narita I
GS
Goto S
LH
Lee H
KD
Kim DK
KY
Kim YS
PJ
Park JH
CB
Cho B
CM
Choi M
VW
Van Wijk A
HA
Huerta A
AE
Ars E
BJ
Ballarin J
LS
Lundberg S
VB
Vogt B
ML
Mani LY
CY
Caliskan Y
BJ
Barratt J
AT
Abeygunaratne T
KP
Kalra PA
GD
Gale DP
PU
Panzer U
RT
Rauen T
FJ
Floege J
SP
Schlosser P
EA
Ekici AB
EK
Eckardt KU
CN
Chen N
XJ
Xie J
LR
Lifton RP
LR
Loos RJF
KE
Kenny EE
II
Ionita-Laza I
KA
Köttgen A
JB
Julian BA
NJ
Novak J
SF
Scolari F
ZH
Zhang H
GA
Gharavi AG
View on PubMed View DOI More from Journal Similar Studies Europe PMC
Chapter II

Abstract

Summary of the research findings

IgA nephropathy (IgAN) is a progressive form of kidney disease defined by glomerular deposition of IgA. Here we performed a genome-wide association study of 10,146 kidney-biopsy-diagnosed IgAN cases and 28,751 controls across 17 international cohorts. We defined 30 genome-wide significant risk loci explaining 11% of disease risk. A total of 16 loci were new, including TNFSF4/TNFSF18, REL, CD28, PF4V1, LY86, LYN, ANXA3, TNFSF8/TNFSF15, REEP3, ZMIZ1, OVOL1/RELA, ETS1, IGH, IRF8, TNFRSF13B and FCAR. The risk loci were enriched in gene orthologs causing abnormal IgA levels when genetically manipulated in mice. We also observed a positive genetic correlation between IgAN and serum IgA levels. High polygenic score for IgAN was associated with earlier onset of kidney failure. In a comprehensive functional annotation analysis of candidate causal genes, we observed convergence of biological candidates on a common set of inflammatory signaling pathways and cytokine ligand-receptor pairs, prioritizing potential new drug targets.

3,549 European ancestry cases, 10,140 European ancestry controls, 4,590 East Asian ancestry cases, 7,573 East Asian ancestry controls

Chapter III

Study Statistics

Key metrics and study information

25852
Total Participants
GWAS
Study Type
No
Replicated
European, East Asian
Ancestry
Argentina, Hungary, Spain, Canada, Czech Republic, Sweden, Turkey, U.S., Belgium, Poland, Italy, U.K., France, Germany, Croatia, China, Japan, Republic of Korea
Recruitment Country
Chapter IV

AI-Generated Summary

AI-generated by DNAGENICS

Independent AI summary of health and genetic findings from the published study

Important: This summary is AI-generated by DNAGENICS for informational purposes only. It was not created by, affiliated with, or endorsed by the researchers behind the original publication, and is based solely on that published research. It may contain errors or omissions. DNAGENICS disclaims all liability for any inaccuracies or consequences arising from use of this information. Verify all information against the original publication. This is not professional scientific review or medical advice.

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