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Detailed stratified GWAS analysis for severe COVID-19 in four European populations.

Authors :
Degenhardt F
Ellinghaus D
Juzenas S
Lerga-Jaso J
Wendorff M
Maya-Miles D
Uellendahl-Werth F
ElAbd H
Rühlemann MC
Arora J
Özer O
Lenning OB
Myhre R
Vadla MS
Wacker EM
Wienbrandt L
Blandino Ortiz A
de Salazar A
Garrido Chercoles A
Palom A
Ruiz A
Garcia-Fernandez AE
Blanco-Grau A
Mantovani A
Zanella A
Holten AR
Mayer A
Bandera A
Cherubini A
Protti A
Aghemo A
Gerussi A
Ramirez A
Braun A
Nebel A
Barreira A
Lleo A
Teles A
Kildal AB
Biondi A
Caballero-Garralda A
Ganna A
Gori A
Glück A
Lind A
Tanck A
Hinney A
Carreras Nolla A
Fracanzani AL
Peschuck A
Cavallero A
Dyrhol-Riise AM
Ruello A
Julià A
Muscatello A
Pesenti A
Voza A
Rando-Segura A
Solier A
Schmidt A
Cortes B
Mateos B
Nafria-Jimenez B
Schaefer B
Jensen B
Bellinghausen C
Maj C
Ferrando C
de la Horra C
Quereda C
Skurk C
Thibeault C
Scollo C
Herr C
Spinner CD
Gassner C
Lange C
Hu C
Paccapelo C
Lehmann C
Angelini C
Cappadona C
Azuure C
Bianco C
Cea C
Sancho C
Hoff DAL
Galimberti D
Prati D
Haschka D
Jiménez D
Pestaña D
Toapanta D
Muñiz-Diaz E
Azzolini E
Sandoval E
Binatti E
Scarpini E
Helbig ET
Casalone E
Urrechaga E
Paraboschi EM
Pontali E
Reverter E
Calderón EJ
Navas E
Solligård E
Contro E
Arana-Arri E
Aziz F
Garcia F
García Sánchez F
Ceriotti F
Martinelli-Boneschi F
Peyvandi F
Kurth F
Blasi F
Malvestiti F
Medrano FJ
Mesonero F
Rodriguez-Frias F
Hanses F
Müller F
Hemmrich-Stanisak G
Bellani G
Grasselli G
Pezzoli G
Costantino G
Albano G
Cardamone G
Bellelli G
Citerio G
Foti G
Lamorte G
Matullo G
Baselli G
Kurihara H
Neb H
My I
Kurth I
Hernández I
Pink I
de Rojas I
Galván-Femenia I
Holter JC
Afset JE
Heyckendorf J
Kässens J
Damås JK
Rybniker J
Altmüller J
Ampuero J
Martín J
Erdmann J
Banales JM
Badia JR
Dopazo J
Schneider J
Bergan J
Barretina J
Walter J
Hernández Quero J
Goikoetxea J
Delgado J
Guerrero JM
Fazaal J
Kraft J
Schröder J
Risnes K
Banasik K
Müller KE
Gaede KI
Garcia-Etxebarria K
Tonby K
Heggelund L
Izquierdo-Sanchez L
Bettini LR
Sumoy L
Sander LE
Lippert LJ
Terranova L
Nkambule L
Knopp L
Gustad LT
Garbarino L
Santoro L
Téllez L
Roade L
Ostadreza M
Intxausti M
Kogevinas M
Riveiro-Barciela M
Berger MM
Schaefer M
Niemi MEK
Gutiérrez-Stampa MA
Carrabba M
Figuera Basso ME
Valsecchi MG
Hernandez-Tejero M
Vehreschild MJGT
Manunta M
Acosta-Herrera M
D'Angiò M
Baldini M
Cazzaniga M
Grimsrud MM
Cornberg M
Nöthen MM
Marquié M
Castoldi M
Cordioli M
Cecconi M
D'Amato M
Augustin M
Tomasi M
Boada M
Dreher M
Seilmaier MJ
Joannidis M
Wittig M
Mazzocco M
Ciccarelli M
Rodríguez-Gandía M
Bocciolone M
Miozzo M
Imaz Ayo N
Blay N
Chueca N
Montano N
Braun N
Ludwig N
Marx N
Martínez N
Cornely OA
Witzke O
Palmieri O
Faverio P
Preatoni P
Bonfanti P
Omodei P
Tentorio P
Castro P
Rodrigues PM
España PP
Hoffmann P
Rosenstiel P
Schommers P
Suwalski P
de Pablo R
Ferrer R
Bals R
Gualtierotti R
Gallego-Durán R
Nieto R
Carpani R
Morilla R
Badalamenti S
Haider S
Ciesek S
May S
Bombace S
Marsal S
Pigazzini S
Klein S
Pelusi S
Wilfling S
Bosari S
Volland S
Brunak S
Raychaudhuri S
Schreiber S
Heilmann-Heimbach S
Aliberti S
Ripke S
Dudman S
Wesse T
Zheng T
Bahmer T
Eggermann T
Illig T
Brenner T
Pumarola T
Feldt T
Folseraas T
Gonzalez Cejudo T
Landmesser U
Protzer U
Hehr U
Rimoldi V
Monzani V
Skogen V
Keitel V
Kopfnagel V
Friaza V
Andrade V
Moreno V
Albrecht W
Peter W
Poller W
Farre X
Yi X
Wang X
Khodamoradi Y
Karadeniz Z
Latiano A
Goerg S
Bacher P
Koehler P
Tran F
Zoller H
Schulte EC
Heidecker B
Ludwig KU
Fernández J
Romero-Gómez M
Albillos A
Invernizzi P
Buti M
Duga S
Bujanda L
Hov JR
Lenz TL
Asselta R
de Cid R
Valenti L
Karlsen TH
Cáceres M
Franke A
Source :
Human molecular genetics [Hum Mol Genet] 2022 Nov 28; Vol. 31 (23), pp. 3945-3966.
Publication Year :
2022

Abstract

Given the highly variable clinical phenotype of Coronavirus disease 2019 (COVID-19), a deeper analysis of the host genetic contribution to severe COVID-19 is important to improve our understanding of underlying disease mechanisms. Here, we describe an extended genome-wide association meta-analysis of a well-characterized cohort of 3255 COVID-19 patients with respiratory failure and 12 488 population controls from Italy, Spain, Norway and Germany/Austria, including stratified analyses based on age, sex and disease severity, as well as targeted analyses of chromosome Y haplotypes, the human leukocyte antigen region and the SARS-CoV-2 peptidome. By inversion imputation, we traced a reported association at 17q21.31 to a ~0.9-Mb inversion polymorphism that creates two highly differentiated haplotypes and characterized the potential effects of the inversion in detail. Our data, together with the 5th release of summary statistics from the COVID-19 Host Genetics Initiative including non-Caucasian individuals, also identified a new locus at 19q13.33, including NAPSA, a gene which is expressed primarily in alveolar cells responsible for gas exchange in the lung.<br /> (© The Author(s) 2022. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Details

Language :
English
ISSN :
1460-2083
Volume :
31
Issue :
23
Database :
MEDLINE
Journal :
Human molecular genetics
Publication Type :
Academic Journal
Accession number :
35848942
Full Text :
https://doi.org/10.1093/hmg/ddac158