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9 research outputs found

Genome assembly using quantum and quantum-inspired annealing

Author: Boev A. S.
Fedorov A. K.
Ilinsky V. V.
Kiktenko E. O.
Kobzeva A. N.
Popov I. V.
Rakitko A. S.
Usmanov S. R.
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/06/2021
Field of study

Recent advances in DNA sequencing open prospects to make whole-genome analysis rapid and reliable, which is promising for various applications including personalized medicine. However, existing techniques for {\it de novo} genome assembly, which is used for the analysis of genomic rearrangements, chromosome phasing, and reconstructing genomes without a reference, require solving tasks of high computational complexity. Here we demonstrate a method for solving genome assembly tasks with the use of quantum and quantum-inspired optimization techniques. Within this method, we present experimental results on genome assembly using quantum annealers both for simulated data and the

\phi

X 174 bacteriophage. Our results pave a way for an increase in the efficiency of solving bioinformatics problems with the use of quantum computing and, in particular, quantum annealing. We expect that the new generation of quantum annealing devices would outperform existing techniques for {\it de novo} genome assembly. To the best of our knowledge, this is the first experimental study of de novo genome assembly problems both for real and synthetic data on quantum annealing devices and quantum-inspired techniques.Comment: 9 pages, 4 figure

arXiv.org e-Print Archive

Directory of Open Access Journals

Increased risk of severe clinical course of COVID-19 in carriers of HLA-C*04:01

Author: Alice Braun
Arjun Arkal Rao
Balnis Joseph
Beer Juerg H.
Beule Dieter
Binder Ronald
Blueher Anja
Borodina Tatiana
Calfee Carolyn S.
Consortium COMET
Corman Victor M.
Danninger Kathrin
Doehn Jan-Moritz
Drosten Christian
Erle David J.
Fernandez-Fuertes Marta
Fragiadakis Gabriela K.
García Federico
Guettouche Toumy
Heidecker Bettina
Helbig Elisa T.
Hendrickson Carolyn M.
Hinzmann Bernd
Hippenstiel Stefan
Holtgrewe Manuel
Hübner Ralf-Harto
Ilinsky Valery
Jaitovich Ariel
Jones Terry C.
Jurisic Stjepan
Kangelaris Kirsten N.
Karadeniz Zehra
Krummel Matthew F.
Krüger Ulrike
Kurth Florian
Landmesser Ulf
Langelier Charles R.
Lippert Lena J.
Macías Juan
Mick Eran
Mühlemann Barbara
Müller Melina
Patriki Dimitri
Pineda Juan A.
Poller Wolfgang
Popov Iaroslav
Quedenau Claudia
Rakitko Alexander
Real Luis M.
Ripke Stephan
Rutishauser Jonas
Saccomanno Jacopo
Salvo Mauricio
Sander Leif E.
Schmid Hansruedi
Siemann Sandra
Skurk Carsten
Stubbemann Paula
Study Group Pa-COVID
Suttorp Norbert
Suwalski Phillip
Thibeault Charlotte
Venkataramani Urmila
Wang Xiaomin
Weiner January 3rd
Wiggli Benedikt
Witzenrath Martin
Woodruff Prescott G.
Zemojtel Tomasz
Zyla Joanna
Publication venue
Publication date: 01/01/2021
Field of study

Background: Since the beginning of the coronavirus disease 2019 (COVID-19) pandemic, there has been increasing urgency to identify pathophysiological characteristics leading to severe clinical course in patients infected with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Human leukocyte antigen alleles (HLA) have been suggested as potential genetic host factors that affect individual immune response to SARS-CoV-2. We sought to evaluate this hypothesis by conducting a multicenter study using HLA sequencing. Methods: We analyzed the association between COVID-19 severity and HLAs in 435 individuals from Germany (n = 135), Spain (n = 133), Switzerland (n = 20) and the United States (n = 147), who had been enrolled from March 2020 to August 2020. This study included patients older than 18 years, diagnosed with COVID19 and representing the full spectrum of the disease. Finally, we tested our results by meta-analysing data from prior genome-wide association studies (GWAS). Findings: We describe a potential association of HLA-C*04:01 with severe clinical course of COVID-19. Carriers of HLA-C*04:01 had twice the risk of intubation when infected with SARS-CoV-2 (risk ratio 1.5 [95% CI 1.1-2.1], odds ratio 3.5 [95% CI 1.9-6.6], adjusted p-value = 0.0074). These findings are based on data from four countries and corroborated by independent results from GWAS. Our findings are biologically plausible, as HLA-C*04:01 has fewer predicted bindings sites for relevant SARS-CoV-2 peptides compared to other HLA alleles. Interpretation: HLA-C*04:01 carrier state is associated with severe clinical course in SARS-CoV-2. Our findings suggest that HLA class I alleles have a relevant role in immune defense against SARS-CoV-2. Funding: Funded by Roche Sequencing Solutions, Inc

Institutional Repository of the Freie Universität Berlin

PubMed Central

eScholarship - University of California

Fondo Bibliográfico Digital Institucional

Increased risk of severe clinical course of COVID-19 in carriers of HLA-C*04:01

Author: Arjun Arkal R.
Balnis J.
Beer J.H.
Beule D.
Binder R.
Blueher A.
Borodina T.
Braun A.
Calfee C.S.
Corman V.M.
Danninger K.
Doehn J.M.
Drosten C.
Erle D.J.
Fernandez-Fuertes M.
Fragiadakis G.K.
García F.
Guettouche T.
Heidecker B.
Helbig E.T.
Hendrickson C.M.
Hinzmann B.
Hippenstiel S.
Holtgrewe M.
Hübner R.H.
Ilinsky V.
Jaitovich A.
Jones T.C.
Jurisic S.
Kangelaris K.N.
Karadeniz Z.
Krummel M.F.
Krüger U.
Kurth F.
Landmesser U.
Langelier C.R.
Lippert L.J.
Macías J.
Mick E.
Mühlemann B.
Müller M.
Patriki D.
Pineda J.A.
Popov I.
Quedenau C.
Rakitko A.
Real L.M.
Ripke S.
Rutishauser J.
Saccomanno J.
Salvo M.
Sander L.E.
Schmid H.
Siemann S.
Skurk C.
Stubbemann P.
Suttorp N.
Suwalski P.
Thibeault C.
Venkataramani U.
Wang X.
Weiner J.
Wiggli B.
Witzenrath M.
Wolfgang P.
Woodruff P.G.
Zemojtel T.
Zyla J.
Publication venue: 'Elsevier BV'
Publication date: 01/10/2021
Field of study

BACKGROUND: Since the beginning of the coronavirus disease 2019 (COVID-19) pandemic, there has been increasing urgency to identify pathophysiological characteristics leading to severe clinical course in patients infected with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Human leukocyte antigen alleles (HLA) have been suggested as potential genetic host factors that affect individual immune response to SARS-CoV-2. We sought to evaluate this hypothesis by conducting a multicenter study using HLA sequencing. METHODS: We analyzed the association between COVID-19 severity and HLAs in 435 individuals from Germany ((n) = 135), Spain ((n) = 133), Switzerland ((n) = 20) and the United States ((n) = 147), who had been enrolled from March 2020 to August 2020. This study included patients older than 18 years, diagnosed with COVID-19 and representing the full spectrum of the disease. Finally, we tested our results by meta-analysing data from prior genome-wide association studies (GWAS). FINDINGS: We describe a potential association of HLA-C*04:01 with severe clinical course of COVID-19. Carriers of HLA-C*04:01 had twice the risk of intubation when infected with SARS-CoV-2 (risk ratio 1.5 [95% CI 1.1-2.1], odds ratio 3.5 [95% CI 1.9-6.6], adjusted (p)-value = 0.0074). These findings are based on data from four countries and corroborated by independent results from GWAS. Our findings are biologically plausible, as HLA-C*04:01 has fewer predicted bindings sites for relevant SARS-CoV-2 peptides compared to other HLA alleles. INTERPRETATION: HLA-C*04:01 carrier state is associated with severe clinical course in SARS-CoV-2. Our findings suggest that HLA class I alleles have a relevant role in immune defense against SARS-CoV-2

MDC Repository

Apremilast Pharmacogenomics in Russian Patients with Moderate-to-Severe and Severe Psoriasis

Author: Alexander Rakitko
Alexandr Chernitsov
Alexey A. Kubanov
Anna Krasnenko
Arfenya E. Karamova
Artem Elmuratov
Dmitry A. Verbenko
Dmitry G. Deryabin
Olga G. Artamonova
Victoria S. Solomka
Publication venue: 'MDPI AG'
Publication date: 29/12/2020
Field of study

One of the target drugs for plaque psoriasis treatment is apremilast, which is a selective phosphodiesterase 4 (PDE4) inhibitor. In this study, 34 moderate-to-severe and severe plaque psoriasis patients from Russia were treated with apremilast for 26 weeks. This allowed us to observe the effectiveness of splitting patient cohorts based on clinical outcomes, which were assessed using the Psoriasis Area Severity Index (PASI). In total, 14 patients (41%) indicated having an advanced outcome with delta PASI 75 after treatment; 20 patients indicated having moderate or no effects. Genome variability was investigated using the Illumina Infinium Global Screening Array. Genome-wide analysis revealed apremilast therapy clinical outcome associations at three compact genome regions with undefined functions situated on chromosomes 2, 4, and 5, as well as on a single single-nucleotide polymorphism (SNP) on chromosome 23. Pre-selected SNP sets were associated with psoriasis vulgaris analysis, which was used to identify four SNP-associated targeted therapy efficiencies: IL1β (rs1143633), IL4 (IL13) (rs20541), IL23R (rs2201841), and TNFα (rs1800629) genes. Moreover, we showed that the use of the global polygenic risk score allowed for the prediction of onset psoriasis in Russians. Therefore, these results can serve as a starting point for creating a predictive model of apremilast therapy response in the targeted therapy of patients with psoriasis vulgaris

Multidisciplinary Digital Publishing Institute

Impact of non‐stationarity on hybrid ensemble filters: A study with a doubly stochastic advection‐diffusion‐decay model

Author: Alexander Rakitko
Apte A.
Arnold L.
Bai J.
Banerjee S.
Chatfield C.
Dunlop M.M.
Michael Tsyrulnikov
Olevskaya S.M.
Piterbarg L.
Seaman R.
Whittle P.
Yaglom A.M.
Publication venue: 'Wiley'
Publication date
Field of study

Crossref

Mapping the human genetic architecture of COVID-19

Author: Abdelrazik M.
Abdullah T.
Abe R.
Abe S.
Abecasis G. R.
Abel L.
Abernathy C.
Abraheem A.
Abul-Husn N. S.
Acosta-Herrera M.
Acquilini D.
Adachi T.
Adachi Y.
Adams C.
Adams K.
Adanini O.
Adeleye O.
Adeniji K.
Adra D.
Afifi N.
Afilalo J.
Afilalo M.
Afolabi D.
Afrasiabi Z.
Afset J. E.
Agasou A.
Aghemo A.
Agranoff D.
Agrawal S.
Aguirre L. A.
Agwuh K.
Ahmad H. F.
Ahmad N.
Ahmed A.
Ahmed C.
Ahmed K. A.
Ai M.
Ail D.
Akeroyd L.
Akhtar M. N.
Akhtar S.
Akinkugbe O.
Aksentijevich A.
Al Thani A.
Al-Muftah W.
Al-Sarraj Y.
Alarcon C.
Alarcon-Riquelme M. E.
Alasdair F.
Alaverdian D.
Alavere H.
Albertos R.
Albillos A.
Albrecht W.
Albrich W.
Albrich W. C.
Aldera E. L.
Aldridge J.
Alegria A.
Alex B.
Alexander P.
Alfonso J.
Algera A. G.
Ali A.
Ali I. A. M.
Ali S.
Aliberti S.
Allan A.
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Alldis Z.
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Allison K. S.
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Almaden-Boyle C.
Altabaibeh A.
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Alvaro A.
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Amin V.
Amitrano S.
Amiya S.
Ampuero J.
Anan R.
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Anastasescu E.
Anderson F.
Anderson J.
Anderson M.
Anderson P.
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Anderson T.
Ando A.
Andolfo I.
Andrade V.
Andretta F.
Andreucci E.
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Andrews S. J.
Andrikopoulos P.
Anedda F.
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Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2021
Field of study

The genetic make-up of an individual contributes to the susceptibility and response to viral infection. Although environmental, clinical and social factors have a role in the chance of exposure to SARS-CoV-2 and the severity of COVID-191,2, host genetics may also be important. Identifying host-specific genetic factors may reveal biological mechanisms of therapeutic relevance and clarify causal relationships of modifiable environmental risk factors for SARS-CoV-2 infection and outcomes. We formed a global network of researchers to investigate the role of human genetics in SARS-CoV-2 infection and COVID-19 severity. Here we describe the results of three genome-wide association meta-analyses that consist of up to 49,562 patients with COVID-19 from 46 studies across 19 countries. We report 13 genome-wide significant loci that are associated with SARS-CoV-2 infection or severe manifestations of COVID-19. Several of these loci correspond to previously documented associations to lung or autoimmune and inflammatory diseases3–7. They also represent potentially actionable mechanisms in response to infection. Mendelian randomization analyses support a causal role for smoking and body-mass index for severe COVID-19 although not for type II diabetes. The identification of novel host genetic factors associated with COVID-19 was made possible by the community of human genetics researchers coming together to prioritize the sharing of data, results, resources and analytical frameworks. This working model of international collaboration underscores what is possible for future genetic discoveries in emerging pandemics, or indeed for any complex human disease

Archivio istituzionale della ricerca - Politecnico di Milano

Archivio della ricerca - Università degli studi di Napoli Federico II

Archivio della Ricerca - Università degli Studi di Siena

Archivio istituzionale della ricerca - Alma Mater Studiorum Università di Bologna

Archivio istituzionale della ricerca - Università di Genova

UTUPub

Archivio istituzionale della ricerca - Università di Modena e Reggio Emilia

Archivio istituzionale della ricerca - Università di Padova

A second update on mapping the human genetic architecture of COVID-19

Author: Abd Elghafar MS
Abdel-Aziz M
Abdelrazik M
Abdullah MS
Abe R
Abe S
Abel L
Abel L
Abernathy C
Abraham R
Abraheem A
Abu Alragheb BO
Abulail JA
Acklery A
Acosta-Herrera M
Adachi T
Adachi Y
Adam R
Adams C
Adams K
Adams N
Adanini O
Afifi N
Afilalo J
Afilalo M
Afolabi D
Afrasiabi Z
Afset JE
Agasou A
Aghemo A
Agravante K
Agrawal A
Agrawal S
Aguado JM
Aguilar C
Aguilar SEV
Aguilar-Salinas CA
Aguilera-Albesa S
Agüero D
Ahmad HF
Ahmad N
Ahmadhaider N
Ahmed A
Ahmed C
Ahram M
Ai M
Ain Q
Aitkin E
Akeroyd L
Akhtar MN
Akinkugbe O
Al-Ani A
Al-Ja’afreh MM
Al-Kadash A
Al-Kasasbeh MM
Al-Moasseb H
Al-Muftah W
Al-Sarraj Y
Alamer LM
Alasdair F
Alawneh FM
Alawneh LM
Albaiceta GM
Albano G
Albillos A
Albrecht W
Aldridge J
Alexander P
Alfonso J
Alhousani TN
Ali A
Ali HH
Ali IAM
Ali S
Aliberti S
ALjalamdeh M
Allan A
Allan E
Allan J
Alldis Z
Allen L
Allen M
Allen S
Allen U
Allibone S
Allison KS
Allouzy SK
Ally SM
Almadana V
Almaden-Boyle C
Almoguera B
Alpuche-Aranda C
AlRawashdeh TJ
Alsafadi DB
Alshaer W
Alsoub FS
Altabaibeh A
Alvarez N
Alvaro A
Alzuraiqi MR
Amamio M
Aman NF
Amin V
Amiya S
Ampuero J
Anan R
Anastasescu E
Andersen S
Anderson J
Anderson M
Anderson P
Anderson S
Anderson S
Anderson T
Ando A
Andrade V
Andreou P
Andreu-Bernabeu Á
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Andrew G
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Angelini C
Ansari AI
Antcliffe D
Antoine P
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Dinh KM
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Überla K
Þorsteinsdóttir U
Publication venue: Nature Research
Publication date: 21/06/2023
Field of study

Spiral - Imperial College Digital Repository

Mapping the human genetic architecture of COVID-19

Author: Abdelrazik M
Abdullah T
Abe R
Abe S
Abecasis GR
Abel L
Abernathy C
Abraheem A
Abul-Husn NS
Acosta-Herrera M
Acquilini D
Acquilini D
Adachi T
Adachi Y
Adams C
Adams K
Adanini O
Adeleye O
Adeniji K
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Afilalo J
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Afolabi D
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Afset JE
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Aguirre LA
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Aksentijevich A
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Al-Muftah W
Al-Sarraj Y
Alarcon C
Alarcon-Riquelme ME
Alasdair F
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Alegria A
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Amin V
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Andolfo I
Andrade V
Andretta F
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Andrew A
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Andrews SJ
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Anedda F
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Angelini C
Angus B
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Antoni MD
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Bettini LR
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Bhatterjee R
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Bochud PY
Bochud PY
Bociek A
Boer C
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Bogaard HJ
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Borislavova B
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Bretherick AD
Brett M
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Bridgett V
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Brinkworth E
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Brouwer MC
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Burt K
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Busson A
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Butler-Laporte G
Butler-Laporte G
Butler-Laporte G
Butler-Laporte G
Butte MJ
Butterworth AS
Butterworth-Cowin N
Button H
Buxbaum JD
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Buxbaum JD
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Cabrelli L
Caceres M
Cadilla CL
Cagova L
Caldarelli GP
Calderon EJ
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Campbell A
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Campbell R
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Canaccini A
Canakoglu A
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Cantor MN
Capasso M
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Cappadona C
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Cardamone G
Carella M
Carey DJ
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Carmody M
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Carnahan M
Carnero-Montoro E
Carrabba M
Carracedo AD
Carreras Nolla A
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Carson G
Carter A
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Castelli F
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Catterall BWA
Caulfield MJ
Caulfield MJ
Cavazza A
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Cawthron K
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Cea C
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Ceri S
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Chadbourn I
Chadwick D
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Chambler D
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Chandler B
Chang D
Chang TS
Chang X
Chang Y
Chapman S
Charles B
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Charney AW
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Chen H-H
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Chouchane O
Choudhury Y
Chowdhury M
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Chukkambotla S
Chukkambotla S
Chung R
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Churchhouse C
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Cirulli ET
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Clamp S
Clapham M
Claringbould A
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Clark R
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Clark V
Clarke D
Clarke EA
Clarke N
Clarkson M
Clayton S
Clement I
Clements S
Clerc O
Cloherty A
Clohisey S
Clohisey S
Clohisey S
Clohisey S
Coates C
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Coetzee S
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Coles H
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Collignon A
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Collins A
Collins BL
Collins C
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Collins E
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Combes E
Conen A
Connolly K
Connor M
Conticini E
Convery K
Conyngham J-A
Cooke GS
Cooper J
Cooper L
Cooper L
Corcoran E
Cordero AIH
Cordioli M
Cordioli M
Cordioli M
Cordioli M
Cordioli M
Cordioli M
Cordioli M
Cornberg M
Cornell S
Cornely OA
Corral MA
Correia GDS
Corridi M
Cortes B
Cortes B
Cosgrove C
Cosgrove D
Cosier T
Cossarizza A
Costantino G
Cother N
Coton Z
Coulding M
Coutts A
Coventry T
Coviello DA
Cowley A
Cowley A
Cowley N
Cowton A
Cox A
Cox H
Cox NJ
Coyle J
Craig J
Crawley R
Creagh-Brown B
Crew A
Crickmore V
CRiPSI
Crisp N
Criste K
Cristiano D
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Croft M
Crook DW
Crooks K
Crotti L
Crowe R
Crowley M
Cruz C
Cullum L
Cunningham A
Cunningham M
Cupitt J
Cupitt J
Curgenven H
Curtis CJ
Cusack R
Cusick C
Cutino-Moguel M-T
Cutler S
D'Acremont V
D'Alessandro M
D'Amato M
D'Angio M
D'Sylva S
Da Gloria EF
Dabe S
Daga S
Daglish J
Dale K
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Dalton J
Dalton K
Daly M
Daly MJ
Daly Z
Dalziel J
Damas JK
Dance A
Danesh J
Daniel A
Daniel P
Daniels A
Darcis G
Dark P
Dark P
Darlington K
Darwish D
Dasgin J
Daubney E
Davey M
Davey M
David B
David C
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Davies C
Davies E
Davies F
Davies G
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Davies L
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Davis C
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Davis LK
Davison C
Dawson C
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Day N
Daya M
de Brabander J
de Bree G
de Bruin S
de Cid R
de Cid R
de Geus EJC
de Gordoa LO-R
de Gordoa LO-R
De Grandi A
de Jong H
de Jong MD
De la Horra C
De Neef M
de Pablo R
de Rojas I
de Salazar A
de Silva T
De Vivo O
De Vivo O
de Vries H
Deacon B
Deacon B
Dearden J
Death Y
Deboever C
Debreceni G
Deelen P
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Deery J
Degenhardt F
Dei S
Dela Rosa A
Delaneau O
Delgado CC
Delgado J
Della Monica M
Dellot P
Deloukas P
Demetriou C
Denmade C
Dennis C
Dent K
Dent M
Depante M
Dervisevic S
Desanctis E
Desgranges F
deSouza F
Di Angelantonio E
di Bartolomeo C
Di Biagio A
Di Domenico P
Di Pietro M
Di Sarno L
Di Valentin E
Digby B
Digby S
Dincarslan O
Ding L
Ding Y
Djeugam B
Do R
Dobano C
Dobson E
Docherty AB
Doddato G
Dodds S
Domingues F
Donaldson A
Donaldson D
Donati A
Dongelmans D
Donlon S
Donnachie J
Donne B
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Donner K
Donnison P
Donnison P
Donohue C
Dooks E
Doonan R
Dopazo X
Dore R
Dormand N
Douglas K
Douthwaite S
Downes C
Drake TM
Dreher M
Drummond A
Drummond A
Duberly S
Dudman S
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Duffield J
Duffin D
Duffy K
Duffy S
Duga S
Duga S
Duga S
Dumas M-E
Duncan E
Duncan T
Dunham I
Dunmore C
Dunn C
Dunning J
DuRand I
Durand M
Durga L
Durham C
Durie A
Durrans LJ
Durrant G
Dushianthan A
Duskova M
Dutta AK
Dutta AK
Dutta AK
Dyer P
Dyer T
Dykes J
Dyrhol-Riise AM
Eapen B
Earle SG
Eastgate-Jackson C
Easthope A
Easthope A
Easthope A
Easton J
Ebano P
Eckbad C
Edahiro R
Edmond I
Edwards M
Efford G
Egan J
Egger T
Eggermann T
El Kandoussi K
Elabd H
Elbers P
Elhassan M
Ellinghaus D
Elliott A
Elliott K
Ellis H
Elsaadany M
Elston K
Eltayeb A
Emiliozzi A
Emmert D
Endo A
Endo M
English K
Enomoto T
Erard V
Erard V
Erdmann J
Eriguchi Y
Esko T
Esmaeeli S
Espana PP
Esparza-Gordillo J
Evans A
Evans C
Evitts J
Ezeobu O
Eziefula C
Fabbiani M
Fadeur M
Fagan A
Fairfield CJ
Falcone M
Falcone M
Fallerini C
Farh K
Farnell-Ward S
Farquhar F
Farre X
Farre X
Farzad Z
Faucon A
Faucon AB
Faulkner B
Faulkner M
Fava F
Fave M-J
Faverio P
Fawkes A
Fazaal J
Fearby M
Febbo P
Fegan C
Feldt T
Felton T
Feng Y-CA
Ferguson S
Feri M
Fernandes K
Fernandes R
Fernandez J
Fernandez Z
Fernandez-Cadenas I
Fernandez-Cadenas I
Fernandez-Cadenas I
Fernandez-Roman J
Ferrando C
Ferreira MAR
Ferrer R
Ferrero GB
Ferri C
Ferrusquia-Acosta J
Ferwerda B
FHoGID
Fidler K
Filipe ADS
Filipe H
Filipovic M
Filippidis P
Filshtein-Sonmez T
Finch C
Finch L
Findlay L
Fine C
Finer S
Finer S
Finernan P
Finn A
Finn J
Finn S
Finney C
Finucane H
Finucane H
Fiorentino G
Fisher E
Fisher LWS
Flaherty L
Flanagan R
Fletcher T
Fleuren L
Flint N
Foco L
Fofano A
Folkersen L
Folkersen L
Folkes L
Folseraas T
Foote D
Force HCT
Ford A
Forgetta V
Forgetta V
Forsey M
Forsey M
Foster L
Foster T
Foti G
Fotiadis S
Fottrell-Gould D
Foucras S
Fourman MH
Fourman MH
Fowler S
Fowler T
Fox C
Fox H
Fox J
Fracanzani AL
Francescatto M
Francescatto M
Franchi F
Francioli L
Francisci D
Franke A
Franke G
Franke L
Franke L
Frankham J
Frediani B
Freimer N
Friaza V
Friedman P
Friolet R
Frippiat F
Frischknecht M
Frise M
Frithiof R
Frullanti E
Fuchimoto Y
Fuchsberger C
Fuchsberger C
Fujitani S
Fujiwara A
Fuke S
Fukui T
Fukunaga K
Fukuyama S
Fuller B
Fullerton D
Funatsu Y
Fundin B
Furini S
Furlong A
Furniss J
Furniss J
Gabbi C
Gabrieli A
Gaddis M
Gaede KI
Gales A
Galimberti D
Gallagher B
Gallego-Duran R
Galvan-Femenia I
Galvan-Femenia I
Gamble C
Ganesan A
Ganna A
Ganna A
Ganna A
Ganna A
Garbarino L
Garcia Sanchez F
Garcia F
Garcia SM
Garcia-Aymerich J
Garcia-Dorival I
Garcia-Etxebarria K
Garcia-Fernandez A-E
Gardner A
Garg A
Garg S
Garland Z
Garmendia A
Garner L
Garrido Chercoles A
Garrioch S
Gascoyne R
Gass MC
Gassner C
Gatti F
Gay B
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Gaylard J
Gaziano JM
Gazon H
Geary T
Geerlings S
Geerts B
Geijtenbeek T
Gellamucho M
Gemmell L
Gendall E
George A
George L
Georges M
Georges M
Gerussi A
Geschwind DH
Geschwind DH
Gettler K
Gharavi AG
Gherman A
Ghosh B
Ghoussaini M
Giannattasio F
Gibson S
Gignoux CR
Gilbert K
Gilchrist T
Giles J
Giliberti A
Gill J
Gill M
Giorgio E
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Giot J-B
Girach R
Girardis M
Girbes A
Giroule F
Girshick A
Girvan M
Gkrania-Klotsas E
Glasgow S
Glass L
Gledhill L
Glessner JR
Glueck A
Goddard W
Godden J
Goerg S
Goff E
Goffard J-C
Gofflot S
Gogele M
Goikoetxea J
Golden D
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Golder K
Golding H
Goldsmith A
Goldstein DB
Goldstein JI
Golightly A
Gomez R
Gomez-Cabrero D
Gon Y
Gondo P
Gonzalez Cejudo T
Goodchild D
Goodsell J
Goodwin E
Goorhuis B
Gopal S
Gordon A
Gordon E
Gori A
Gori M
Gorman C
Gorzynski J
Gountouna E
Graham C
Grasselli G
Grassi D
Gratrix A
Grau N
Grauslyte L
Green CA
Green J
Green RC
Greenhalf W
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Greer S
Gregory J
Greig J
Griffin D
Griffin JL
Griffiths C
Griffiths CJ
Griffiths F
Grimes G
Grimmer L
Grimsrud MM
Grobusch MP
Grp NS-CS
Grzymski JJ
Gualtierotti R
Guarnaccia A
Guarnaccia A
Gudbjartsson DF
Gude ET
Guerin J
Guerrero JM
Guerrini S
Guery B
Guidelli L
Guillet A
Guindo-Martinez M
Guiot J
Gulati A
Gumbrill B
Gummadi M
Gunning P
Guntz J
Gupta A
Gupta R
Gupta RK
Gurasashvili J
Gurr L
Gustad LT
Gutierrez-Stampa MA
Guturu H
Guyat-Jacques C
Guzman C
Hadebe B
Haefliger D
Hafezi K
Hafkamp F
Hagens L
Haider S
Hairsine B
Hakonarson H
Haldeos A
Hales D
Haley C
Halkes M
Hall K
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Halpin S
Ham SY
Hamann J
Hambrook G
Hamidi Z
Hamilton D
Hamilton DO
Hammer C
Hammerton K
Hammond N
Han C
Han Y
Hanley S
Hanratty H
Hanses F
Hanson H
Hanson K
Hansson K
Hao K
Haq R
Hara R
Harada M
Harada N
Hard K
Harden L
Harding P
Hardwick H
Hardy E
Hardy J
Harford R
Hargreaves J
Harling R
Harper R
Harrington K
Harris C
Harris J
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Harris N
Harris V
Harrison A
Harrison A
Harrison D
Harrison EM
Harrison J
Harrison L
Harrison W
Harry E
Hartley C
Hartley J
Hartridge P
Hartshorn S
Harvey A
Harvey D
Hase I
Hasegawa N
Hasegawa T
Hasegawa Y
Hashiguchi M
Hashimoto N
Hashimoto S
Hashino T
Hass I
Hatton J
Havalda P
Hawcutt D
Hawcutt DB
Hawes J
Hayashi K
Hayashi R
Hayashi S
Hayes A
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Hayman M
Hays C
Hayward C
Hazelton T
Heeney E
Heggelund L
Hehr U
Heidecker B
Heilmann-Heimbach S
Helbig ET
Helm D
Hemke R
Hemmrich-Stanisak G
Henderson S
Hendry R
Hendry R
Henket M
Henry D
Hensen K
Herdman-Grant R
Hermans SM
Hernandez Quero J
Hernandez I
Hernandez-Tejero M
Heron AE
Herr C
Herrmann S
Hershman S
Hesseldon L
Heunks L
Hewitt C
Hey S
Heyckendorf J
Hibbert M
Hicks A
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Hiester LL
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Hijazi M
Hiki M
Hill H
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Hilldrith A
Hilltout P
Hilton M
Hindale J
Hinds C
Hinney A
Hirai Y
Hirano T
Hirata H
Hiscox JA
Hizawa N
Ho AYW
Ho Y-L
Hobden G
Hobrok M
Hobrok M
Hod E
Hodgkiss T
Hodgson L
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Hoff DAL
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Niemi MEK
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Pairo-Castineira E
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Pancrazi A
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Pantet O
Papakonstantinou D
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Parker R
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Parkinson P
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Parravicini P
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Parsons P
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Partridge R
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Pasaniuc B
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Pascual-Iglesias A
Pasko D
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Patel A
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Paxton WA
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Pink I
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Pinnell J
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Piscopo C
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Polikowsky HG
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Pollard R
Poller W
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Pooni JS
Popescu M
Popov I
Porteous DJ
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Poscente M
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Post F
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Pothecary C
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Potla D
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Publication venue
Publication date: 01/01/2021
Field of study

The genetic make-up of an individual contributes to the susceptibility and response to viral infection. Although environmental, clinical and social factors have a role in the chance of exposure to SARS-CoV-2 and the severity of COVID-191,2, host genetics may also be important. Identifying host-specific genetic factors may reveal biological mechanisms of therapeutic relevance and clarify causal relationships of modifiable environmental risk factors for SARS-CoV-2 infection and outcomes. We formed a global network of researchers to investigate the role of human genetics in SARS-CoV-2 infection and COVID-19 severity. Here we describe the results of three genome-wide association meta-analyses that consist of up to 49,562 patients with COVID-19 from 46 studies across 19 countries. We report 13 genome-wide significant loci that are associated with SARS-CoV-2 infection or severe manifestations of COVID-19. Several of these loci correspond to previously documented associations to lung or autoimmune and inflammatory diseases3,4,5,6,7. They also represent potentially actionable mechanisms in response to infection. Mendelian randomization analyses support a causal role for smoking and body-mass index for severe COVID-19 although not for type II diabetes. The identification of novel host genetic factors associated with COVID-19 was made possible by the community of human genetics researchers coming together to prioritize the sharing of data, results, resources and analytical frameworks. This working model of international collaboration underscores what is possible for future genetic discoveries in emerging pandemics, or indeed for any complex human disease

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Increased risk of severe clinical course of COVID-19 in carriers of HLA-C*04:01.

Author: Alice Braun
Arjun Arkal Rao
Balnis Joseph
Beer Juerg H
Beule Dieter
Binder Ronald
Blueher Anja
Borodina Tatiana
Calfee Carolyn S
Comet Consortium
Corman Victor M
Danninger Kathrin
Doehn Jan-Moritz
Drosten Christian
Erle David J
Fernandez-Fuertes Marta
Fragiadakis Gabriela K
García Federico
Guettouche Toumy
Heidecker Bettina
Helbig Elisa T
Hendrickson Carolyn M
Hinzmann Bernd
Hippenstiel Stefan
Holtgrewe Manuel
Hübner Ralf-Harto
Ilinsky Valery
Jaitovich Ariel
Jones Terry C
Jurisic Stjepan
Kangelaris Kirsten N
Karadeniz Zehra
Krummel Matthew F
Krüger Ulrike
Kurth Florian
Landmesser Ulf
Langelier Charles R
Lippert Lena J
Macías Juan
Mick Eran
Mühlemann Barbara
Müller Melina
Pa-Covid Study Group
Patriki Dimitri
Pineda Juan A
Poller Wolfgang
Popov Iaroslav
Quedenau Claudia
Rakitko Alexander
Real Luis M
Ripke Stephan
Rutishauser Jonas
Saccomanno Jacopo
Salvo Mauricio
Sander Leif E
Schmid Hansruedi
Siemann Sandra
Skurk Carsten
Stubbemann Paula
Suttorp Norbert
Suwalski Phillip
Thibeault Charlotte
Venkataramani Urmila
Wang Xiaomin
Weiner January
Wiggli Benedikt
Witzenrath Martin
Woodruff Prescott G
Zemojtel Tomasz
Zyla Joanna
Publication venue: eScholarship, University of California
Publication date: 01/10/2021
Field of study

BackgroundSince the beginning of the coronavirus disease 2019 (COVID-19) pandemic, there has been increasing urgency to identify pathophysiological characteristics leading to severe clinical course in patients infected with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Human leukocyte antigen alleles (HLA) have been suggested as potential genetic host factors that affect individual immune response to SARS-CoV-2. We sought to evaluate this hypothesis by conducting a multicenter study using HLA sequencing.MethodsWe analyzed the association between COVID-19 severity and HLAs in 435 individuals from Germany (n = 135), Spain (n = 133), Switzerland (n = 20) and the United States (n = 147), who had been enrolled from March 2020 to August 2020. This study included patients older than 18 years, diagnosed with COVID-19 and representing the full spectrum of the disease. Finally, we tested our results by meta-analysing data from prior genome-wide association studies (GWAS).FindingsWe describe a potential association of HLA-C*04:01 with severe clinical course of COVID-19. Carriers of HLA-C*04:01 had twice the risk of intubation when infected with SARS-CoV-2 (risk ratio 1.5 [95% CI 1.1-2.1], odds ratio 3.5 [95% CI 1.9-6.6], adjusted p-value = 0.0074). These findings are based on data from four countries and corroborated by independent results from GWAS. Our findings are biologically plausible, as HLA-C*04:01 has fewer predicted bindings sites for relevant SARS-CoV-2 peptides compared to other HLA alleles.InterpretationHLA-C*04:01 carrier state is associated with severe clinical course in SARS-CoV-2. Our findings suggest that HLA class I alleles have a relevant role in immune defense against SARS-CoV-2.FundingFunded by Roche Sequencing Solutions, Inc

eScholarship - University of California