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Exome-wide association study to identify rare variants influencing COVID-19 outcomes : Results from the Host Genetics Initiative

Author: Adam Butterworth
Akinori Kimura
Albandari Binowayn
Alberto Gómez-Carballa
Alessandra Renieri
Alex Stuckey
Alexander W. Charney
Alexandre Bolze
Alexis Stephens
Alfredo Gonzalez
Amal Almutairi
Amy D. Stockwell
Andrea Ganna
Antonio Salas
Anurag Verma
Axel Schmidt
Bartlomiej Przychodzen
Bogdan Pasaniuc
Brian Yaspan
Carlo Rivolta
Chadi Saad
Chureerat Phokaew
COVID-19 Host Genetics Initiative
Daniel H. Geschwind
Daniel M. Jordan
David B. Goldstein
David Langlais
David Morrison
DeCOI Host Genetics Group
Diane Del Valle
Ebtehal A. Alsolm
Efren Sandoval
Elifnaz Çelik
Elizabeth T. Cirulli
Elżbieta Kaja
Eric E. Schadt
Esther Cheng
Eva C. Schulte
Fabian Brand
Fang Cai
Fatima Alqubaishi
Fawz S. Al Harthi
Federico Martinón-Torres
Francesca Fava
Francesca Mari
Francisco Tanudjaja
GEN-COVID consortium (Spain)
GEN-COVID Multicenter Study (Italy)
GenOMICC Consortium
Guillaume Bourque
Guillaume Butler-Laporte
Gundula Povysil
Hadeel El Bardisy
Hamdi Mbarek
Ho Namkoong
Hugo Zeberg
Ilaria Meloni
Irene Rivero-Calle
Iva Neveux
J Brent Richards
J Kenneth Baillie
Jack A. Kosmicki
Jacobo Pardo-Seco
Japan COVID-19 Task Force
Jessica Nordlund
Joseph D. Buxbaum
Joseph J. Grzymski
Junghyun Jung
Karolina Chwialkowska
Katsushi Tokunaga
Kelly M. Schiabor Barrett
Kerstin U. Ludwig
Klaudia Walter
Koichi Fukunaga
Konrad J. Karczewski
Kousik Kundu
Krzysztof Kiryluk
Kumar Veerapen
Laura G. Sloofman
Maciej Dabrowski
Magdalena Niemira
Malak S. Abedalthagafi
Manal Alaamery
Manish J. Butte
Mansour S. Almutairi
Manuel A. R. Ferreira
Marcin Moniuszko
Mark Lathrop
Masaya Sugiyama
Mateusz Sypniewski
Mathieu Bourgey
Mathieu Quinodoz
Michael E. Broudy
Michael Hultström
Miklos Lipcsey
Miriam Merad
Miroslaw Kwasniewski
Mohammad Fawzy
Monnat Pongpanich
Mount Sinai Clinical Intelligence Center
Nattiya Hirankarn
Nicolas Casadei
Nicole L. Washington
Nicole Simons
Nicole Soranzo
Nikhil Chavan
Ning Shang
Noam D. Beckmann
Nora Aljawini
Olaf Riess
Pajaree Chariyavilaskul
Paul C. Boutros
Paul J. Tung
Pawel Olszewski
Pawel Zawadzki
Pierre-Yves Bochud
Regeneron Genetics Center
Robert Frithiof
Robert JM Eveleigh
Robert Sebra
Ruth Johnson
Ryan C. Thompson
Ryuya Edahiro
Sacha Gnjatic
Said I. Ismail
Salam Massadeh
Saleh A. Alqahtani
Sandra Smieszek
Sarah Alotaibi
Satoru Miyano
Seishi Ogawa
Seiya Imoto
Serghei Mangul
Sergio Daga
Seunghee Kim-Schulze
Shaun Dabe
Shu Tao
Simon White
Simone Furini
Stefan Eng
Stephan Ossowski
Stephanie Arteaga
Stephanie Bibert
Stephen Riffle
Susanne Motameny
Szymon Pula
Takafumi N. Yamaguchi
Takanori Hasegawa
Takanori Kanai
Tatsuhiko Naito
Tess D. Pottinger
Theodore Drivas
Timothy Chang
Timothy Sanders
Tomoko Nakanishi
Urszula Korotko
Vincent Mooser
Vincenzo Forgetta
Voraphoj Nilaratanakul
Vorasuk Shotelersuk
Wanna Chetruengchai
William Lee
Xabier Bello
Yanara Marincevic-Zuniga
Yaseen M. Arabi
Yosuke Kawai
Yu Pan
Yukinori Okada
Publication venue
Publication date: 01/01/2022
Field of study

Publisher Copyright: Copyright: © 2022 Butler-Laporte et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.Host genetics is a key determinant of COVID-19 outcomes. Previously, the COVID-19 Host Genetics Initiative genome-wide association study used common variants to identify multiple loci associated with COVID-19 outcomes. However, variants with the largest impact on COVID-19 outcomes are expected to be rare in the population. Hence, studying rare variants may provide additional insights into disease susceptibility and pathogenesis, thereby informing therapeutics development. Here, we combined whole-exome and whole-genome sequencing from 21 cohorts across 12 countries and performed rare variant exome-wide burden analyses for COVID-19 outcomes. In an analysis of 5,085 severe disease cases and 571,737 controls, we observed that carrying a rare deleterious variant in the SARS-CoV-2 sensor toll-like receptor TLR7 (on chromosome X) was associated with a 5.3-fold increase in severe disease (95% CI: 2.75–10.05, p = 5.41x10-7). This association was consistent across sexes. These results further support TLR7 as a genetic determinant of severe disease and suggest that larger studies on rare variants influencing COVID-19 outcomes could provide additional insights.Peer reviewe

Archivio della Ricerca - Università degli Studi di Siena

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Archivio istituzionale della ricerca - Alma Mater Studiorum Università di Bologna

Digitala Vetenskapliga Arkivet - Academic Archive On-line

Helsingin yliopiston digitaalinen arkisto

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Leicester Research Archive

Exome-wide association study to identify rare variants influencing COVID-19 outcomes: Results from the Host Genetics Initiative

Author: Adam Butterworth
Akinori Kimura
Albandari Binowayn
Alberto Gómez-Carballa
Alessandra Renieri
Alex Stuckey
Alexander W. Charney
Alexandre Bolze
Alexis Stephens
Alfredo Gonzalez
Amal Almutairi
Amy D. Stockwell
Andrea Ganna
Antonio Salas
Anurag Verma
Axel Schmidt
Bartlomiej Przychodzen
Bogdan Pasaniuc
Brian Yaspan
Carlo Rivolta
Chadi Saad
Chureerat Phokaew
COVID-19 Host Genetics Initiative
Daniel H. Geschwind
Daniel M. Jordan
David B. Goldstein
David Langlais
David Morrison
DeCOI Host Genetics Group
Diane Del Valle
Ebtehal A. Alsolm
Efren Sandoval
Elifnaz Çelik
Elizabeth T. Cirulli
Elżbieta Kaja
Eric E. Schadt
Esther Cheng
Eva C. Schulte
Fabian Brand
Fang Cai
Fatima Alqubaishi
Fawz S. Al Harthi
Federico Martinón-Torres
Francesca Fava
Francesca Mari
Francisco Tanudjaja
GEN-COVID consortium (Spain)
GEN-COVID Multicenter Study (Italy)
GenOMICC Consortium
Guillaume Bourque
Guillaume Butler-Laporte
Gundula Povysil
Hadeel El Bardisy
Hamdi Mbarek
Ho Namkoong
Hugo Zeberg
Ilaria Meloni
Irene Rivero-Calle
Iva Neveux
J Brent Richards
J Kenneth Baillie
Jack A. Kosmicki
Jacobo Pardo-Seco
Japan COVID-19 Task Force
Jessica Nordlund
Joseph D. Buxbaum
Joseph J. Grzymski
Junghyun Jung
Karolina Chwialkowska
Katsushi Tokunaga
Kelly M. Schiabor Barrett
Kerstin U. Ludwig
Klaudia Walter
Koichi Fukunaga
Konrad J. Karczewski
Kousik Kundu
Krzysztof Kiryluk
Kumar Veerapen
Laura G. Sloofman
Maciej Dabrowski
Magdalena Niemira
Malak S. Abedalthagafi
Manal Alaamery
Manish J. Butte
Mansour S. Almutairi
Manuel A. R. Ferreira
Marcin Moniuszko
Mark Lathrop
Masaya Sugiyama
Mateusz Sypniewski
Mathieu Bourgey
Mathieu Quinodoz
Michael E. Broudy
Michael Hultström
Miklos Lipcsey
Miriam Merad
Miroslaw Kwasniewski
Mohammad Fawzy
Monnat Pongpanich
Mount Sinai Clinical Intelligence Center
Nattiya Hirankarn
Nicolas Casadei
Nicole L. Washington
Nicole Simons
Nicole Soranzo
Nikhil Chavan
Ning Shang
Noam D. Beckmann
Nora Aljawini
Olaf Riess
Pajaree Chariyavilaskul
Paul C. Boutros
Paul J. Tung
Pawel Olszewski
Pawel Zawadzki
Pierre-Yves Bochud
Regeneron Genetics Center
Robert Frithiof
Robert JM Eveleigh
Robert Sebra
Ruth Johnson
Ryan C. Thompson
Ryuya Edahiro
Sacha Gnjatic
Said I. Ismail
Salam Massadeh
Saleh A. Alqahtani
Sandra Smieszek
Sarah Alotaibi
Satoru Miyano
Seishi Ogawa
Seiya Imoto
Serghei Mangul
Sergio Daga
Seunghee Kim-Schulze
Shaun Dabe
Shu Tao
Simon White
Simone Furini
Stefan Eng
Stephan Ossowski
Stephanie Arteaga
Stephanie Bibert
Stephen Riffle
Susanne Motameny
Szymon Pula
Takafumi N. Yamaguchi
Takanori Hasegawa
Takanori Kanai
Tatsuhiko Naito
Tess D. Pottinger
Theodore Drivas
Timothy Chang
Timothy Sanders
Tomoko Nakanishi
Urszula Korotko
Vincent Mooser
Vincenzo Forgetta
Voraphoj Nilaratanakul
Vorasuk Shotelersuk
Wanna Chetruengchai
William Lee
Xabier Bello
Yanara Marincevic-Zuniga
Yaseen M. Arabi
Yosuke Kawai
Yu Pan
Yukinori Okada
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 01/01/2022
Field of study

Archivio della Ricerca - Università degli Studi di Siena

Combining rare and common genetic variants improves population risk stratification for breast cancer

Author: Alexa Anderson
Alexandre Bolze
Catherine Hajek
Daniel Kiser
Ekaterina Orlova
Elizabeth T. Cirulli
Gai Elhanan
Harry Reed
Ildiko Thibodeau
Iva Neveux
Jamie M. Schnell Blitstein
Joseph J. Grzymski
Kelly M. Schiabor Barrett
Matthew J. Ferber
Natalie Telis
Nicole L. Washington
Ruomu Jiang
Shaun Dabe
William J. Metcalf
Publication venue: Elsevier
Publication date: 01/01/2024
Field of study

Purpose: This study aimed to evaluate the performance of different genetic screening approaches to identify women at high risk of breast cancer in the general population. Methods: We retrospectively studied 25,591 women with available electronic health records and genetic data, participants in the Healthy Nevada Project. Results: Family history of breast cancer was ascertained on or after the record of breast cancer for 78% of women with both, indicating that this risk assessment method is not being properly utilized for early screening. Genetics offered an alternative method for risk assessment. 11.4% of women were identified as high risk based on possessing a predicted loss-of-function (pLOF) variant in BRCA1, BRCA2, or PALB2 (hazard ratio = 10.4, 95% confidence interval: 8.1-13.5) or a pLOF variant in ATM or CHEK2 (hazard ratio = 3.4, CI: 2.4-4.8) or being in the top 10% of the polygenic risk score (PRS) distribution (hazard ratio = 2.4, CI: 2.0-2.8). Moreover, women with a pLOF in ATM or CHEK2 and ranking in the top 50% of the PRS displayed a high risk (39.2% probability of breast cancer at age 70), whereas their counterparts in the bottom 50% of the PRS were not at high risk (14.4% probability at age 70). Conclusion: Our findings suggest that a combined monogenic and polygenic approach allowed a better identification of participants with high risk while minimizing false positives

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Emergence and rapid transmission of SARS-CoV-2 B.1.1.7 in the United States.

Author: Andersen Kristian G
Anderson Catelyn
Antico Jay
Austin Brett
Bakhtar Omid
Basler Tracy
Becker David
Bolze Alexandre
Cassens Tyler
Chiu Charles Y
Cirulli Elizabeth T
de Feo Eileen
De Hoff Peter
Deng Xianding
Febbo Phillip G
Gangavarapu Karthik
Gietzen Kimberly
Harding Aaron
Hoon Kelly
Hughes Laura D
Isaksson Magnus
Jacobs Sharoni
Knight Rob
Kurzban Ezra
Larsen Brendan B
Laurent Louise C
Laurent Marc
Lee William
Levan Geraint
Liu Jingtao
Lu James T
MacCannell Duncan
McDonald Eric
Nguyen Jason
Ramirez Jimmy M
Rivera-Garcia Charlotte
Robles-Sikisaka Refugio
Sandoval Efren
Sathe Shashank
Schiabor Barrett Kelly M
Seaver Phoebe
Servellita Venice
Sickler Brad
Spencer Emily
Suchard Marc A
Valentine Holly
Wang Candace
Wang Xueqing
Washington Nicole L
White Simon
Wong David
Worobey Michael
Yeo Gene W
Zeller Mark
Publication venue: eScholarship, University of California
Publication date: 01/05/2021
Field of study

The highly transmissible B.1.1.7 variant of SARS-CoV-2, first identified in the United Kingdom, has gained a foothold across the world. Using S gene target failure (SGTF) and SARS-CoV-2 genomic sequencing, we investigated the prevalence and dynamics of this variant in the United States (US), tracking it back to its early emergence. We found that, while the fraction of B.1.1.7 varied by state, the variant increased at a logistic rate with a roughly weekly doubling rate and an increased transmission of 40%-50%. We revealed several independent introductions of B.1.1.7 into the US as early as late November 2020, with community transmission spreading it to most states within months. We show that the US is on a similar trajectory as other countries where B.1.1.7 became dominant, requiring immediate and decisive action to minimize COVID-19 morbidity and mortality

eScholarship - University of California

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Genomic epidemiology identifies emergence and rapid transmission of SARS-CoV-2 B.1.1.7 in the United States.

Author: Andersen Kristian G
Anderson Catelyn
Antico Jay
Austin Brett
Bakhtar Omid
Barrett Kelly M Schiabor
Basler Tracy
Becker David
Bolze Alexandre
Cassens Tyler
Chiu Charles
Cirulli Elizabeth T
de Feo Eileen
De Hoff Peter
Deng Xianding
Febbo Phillip G
Gangavarapu Karthik
Gietzen Kimberly
Harding Aaron
Hoon Kelly
Hughes Laura D
Isaksson Magnus
Jacobs Sharoni
Knight Rob
Kurzban Ezra
Larsen Brendan B
Laurent Louise C
Laurent Marc
Lee William
Levan Geraint
Liu Jingtao
Lu James T
McDonald Eric
Nguyen Jason
Ramirez Jimmy M
Rivera-Garcia Charlotte
Robles-Sikisaka Refugio
Sandoval Efren
Sathe Shashank
Seaver Phoebe
Servellita Venice
Sickler Brad
Spencer Emily
Suchard Marc A
Valentine Holly
Wang Candace
Wang Xueqing
Washington Nicole L
White Simon
Wong David
Worobey Michael
Yeo Gene W
Zeller Mark
Publication venue: eScholarship, University of California
Publication date: 07/02/2021
Field of study

As of January of 2021, the highly transmissible B.1.1.7 variant of SARS-CoV-2, which was first identified in the United Kingdom (U.K.), has gained a strong foothold across the world. Because of the sudden and rapid rise of B.1.1.7, we investigated the prevalence and growth dynamics of this variant in the United States (U.S.), tracking it back to its early emergence and onward local transmission. We found that the RT-qPCR testing anomaly of S gene target failure (SGTF), first observed in the U.K., was a reliable proxy for B.1.1.7 detection. We sequenced 212 B.1.1.7 SARS-CoV-2 genomes collected from testing facilities in the U.S. from December 2020 to January 2021. We found that while the fraction of B.1.1.7 among SGTF samples varied by state, detection of the variant increased at a logistic rate similar to those observed elsewhere, with a doubling rate of a little over a week and an increased transmission rate of 35-45%. By performing time-aware Bayesian phylodynamic analyses, we revealed several independent introductions of B.1.1.7 into the U.S. as early as late November 2020, with onward community transmission enabling the variant to spread to at least 30 states as of January 2021. Our study shows that the U.S. is on a similar trajectory as other countries where B.1.1.7 rapidly became the dominant SARS-CoV-2 variant, requiring immediate and decisive action to minimize COVID-19 morbidity and mortality

eScholarship - University of California

Recommended from our members

Genomic epidemiology identifies emergence and rapid transmission of SARS-CoV-2 B.1.1.7 in the United States.

Author: Andersen Kristian G
Anderson Catelyn
Antico Jay
Austin Brett
Bakhtar Omid
Basler Tracy
Becker David
Bolze Alexandre
Cassens Tyler
Chiu Charles
Cirulli Elizabeth T
de Feo Eileen
De Hoff Peter
Deng Xianding
Febbo Phil
Gangavarapu Karthik
Gietzen Kimberly
Harding Aaron
Hoon Kelly
Hughes Laura D
Isaksson Magnus
Jacobs Sharoni
Knight Rob
Kurzban Ezra
Larsen Brendan B
Laurent Louise C
Laurent Marc
Lee William
Levan Geraint
Liu Jingtao
Lu James T
McDonald Eric
Nguyen Jason
Ramirez Jimmy M
Rivera-Garcia Charlotte
Robles-Sikisaka Refugio
Sandoval Efren
Sathe Shashank
Schiabor Barrett Kelly M
Seaver Phoebe
Servellita Venice
Sickler Brad
Spencer Emily
Suchard Marc A
Valentine Holly
Wang Candace
Wang Xueqing
Washington Nicole L
White Simon
Wong David
Worobey Michael
Yeo Gene W
Zeller Mark
Publication venue: eScholarship, University of California
Publication date: 07/02/2021
Field of study

eScholarship - University of California

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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Altabaibeh A.
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Alvaro A.
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Anan R.
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Worner R.
Worsley L.
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Wozniak H.
Wray G.
Wren L.
Wright D.
Wright J.
Wright M.
Wrobel N.
Wu Y.
Wulandari R.
Wyllie D. H.
Wynter I.
Xavier K.
Xue X.
Yadav A.
Yagi K.
Yamada M.
Yamada Y.
Yamagata K.
Yamasaki M.
Yang G.
Yang J.
Yang Z.
Yaspan B.
Yasui Y.
Yates B.
Yatomi M.
Ye C.
Yengo L.
Yermakovich D.
Yi X.
Yonekawa A.
Yoon H.
Yoon K. J.
Yoshida K.
Yoshida S.
Yoshida S.
Yoshida T.
Yoshihara T.
Yoshiya K.
Yoshiyama T.
Youlton N.
Young P.
Yun N.
Zak A.
Zaki A.
Zambon M.
Zamikula J.
Zanella A.
Zanella I.
Zanelli G.
Zara F.
Zarate R.
Zborowski A. C.
Zeberg H.
Zechner M.
Zguro K.
Zhai R.
Zhang M.
Zhao J. H.
Zhen J.
Zheng C.
Zheng T.
Zhou W.
Zhu W.
Zitter L.
Zlatopolsky M.
Zoller H.
Zollner S.
Zongo O.
Zucchi P.
Zyndorf M.
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

Wastewater sequencing reveals early cryptic SARS-CoV-2 variant transmission.

Author: Abelman Dismas B.
Aceves Christine M.
Aigner Stefan
Andersen Kristian G.
Anderson Catelyn
Anderson Cheryl
Austin Brett
Baer Nathan A.
Bakhtar Omid
Barber Tom
Becker David
Belda-Ferre Pedro
Birmingham Amanda
Bolze Alexandre
Brenner David
Bruner Judith C.
Buckley Anne
Chacón Marisol
Cheung Willi
Cirulli Elizabeth T.
Cresini Evelyn S.
De Hoff Peter
Dimmock David P.
Eisner Emily R.
Ellison Michael
Farmer Sawyer
Fielding-Miller Rebecca
Fisch Kathleen M.
Gaines Tommi
Gangavarapu Karthik
Garfein Richard S.
Gattas Jeffrey
Gonias Steven L.
Gurfield Nikos
Hakim Abbas
Hale Matt
Harding Aaron
Hawkins Faith
Henson Benjamin
Hobbs Charlotte A.
Hufbauer Emory
Humphrey Greg
Ikeda Lydia
Isaksson Magnus
Jepsen Kristen
Jhaveri Hemlata
Johnson Ted
Karthikeyan Smruthi
Kellen Vince
Khosla Pradeep K.
Kingsmore Stephen F.
Knight Rob
Kremer Brendan
Kurzban Ezra
Lastrella Alma L.
Laurent Louise C.
Lawrence Elijah S.
Lee Justin
Lee William
Levy Joshua I.
Longhurst Christopher
MacCannell Duncan R.
Malone John D.
Mark Adam M.
Marotz Clarisse A.
Martin Natasha K.
Matteson Nathaniel L.
Matthews Gary
Maysent Patty
McDonald Daniel
McDonald Eric
McHardy Ian H.
McLawhon Ronald W.
Mendoza Art
Moshiri Niema
Neuhard Robert M.
Ngo Toan T.
Nicholson Laura
Ostrander Tyler
Ouillet Pierre
Park Daniel
Parker Edyth
Perkins Sarah A.
Plascencia Ashley
Pradenas Allorah
Pride David
Ramesh Karthik S.
Reed Sharon
Riggs Lindsay
Robles-Sikisaka Refugio
Salido Rodolfo A.
Sanders Alison
Sathe Shashank
Satterlund Alysson M.
Schafer Ashleigh Murphy
Schiabor Barrett Kelly M.
Schooley Robert
Schwab Madison A.
Scioscia Angela L.
Seaver Phoebe
Shah Seema
Simmons Elizabeth H.
Smoot Elizabeth W.
Sollenberger Bradley
Song Angela
Spencer Emily
Stous Sarah
Tribelhorn Caitlin E.
Tsai Rebecca
Tubb Helena M.
Valles Tommy
Washington Nicole L.
White Benjamin
Winbush Terri
Wohl Shirlee
Yeo Gene W.
Yu Alexander T.
Zeller Mark
Publication venue: eScholarship, University of California
Publication date: 01/01/2022
Field of study

As SARS-CoV-2 continues to spread and evolve, detecting emerging variants early is critical for public health interventions. Inferring lineage prevalence by clinical testing is infeasible at scale, especially in areas with limited resources, participation, or testing and/or sequencing capacity, which can also introduce biases1-3. SARS-CoV-2 RNA concentration in wastewater successfully tracks regional infection dynamics and provides less biased abundance estimates than clinical testing4,5. Tracking virus genomic sequences in wastewater would improve community prevalence estimates and detect emerging variants. However, two factors limit wastewater-based genomic surveillance: low-quality sequence data and inability to estimate relative lineage abundance in mixed samples. Here we resolve these critical issues to perform a high-resolution, 295-day wastewater and clinical sequencing effort, in the controlled environment of a large university campus and the broader context of the surrounding county. We developed and deployed improved virus concentration protocols and deconvolution software that fully resolve multiple virus strains from wastewater. We detected emerging variants of concern up to 14 days earlier in wastewater samples, and identified multiple instances of virus spread not captured by clinical genomic surveillance. Our study provides a scalable solution for wastewater genomic surveillance that allows early detection of SARS-CoV-2 variants and identification of cryptic transmission

PubMed Central

eScholarship - University of California

Exome-wide association study to identify rare variants influencing COVID-19 outcomes : Results from the Host Genetics Initiative

Author: Abedalthagafi Malak S.
Al Harthi Fawz S.
Alaamery Manal
Aljawini Nora
Almutairi Amal
Almutairi Mansour S.
Alotaibi Sarah
Alqahtani Saleh A.
Alqubaishi Fatima
Alsolm Ebtehal A.
Arabi Yaseen M.
Arteaga Stephanie
Bardisy Hadeel El
Beckmann Noam D.
Bello Xabier
Bibert Stephanie
Binowayn Albandari
Bochud Pierre Yves
Bolze Alexandre
Bourgey Mathieu
Bourque Guillaume
Boutros Paul C.
Brand Fabian
Brent Richards J.
Broudy Michael E.
Butler-Laporte Guillaume
Butte Manish J.
Butterworth Adam
Buxbaum Joseph D.
Cai Fang
Casadei Nicolas
Center Regeneron Genetics
Chang Timothy
Chariyavilaskul Pajaree
Charney Alexander W.
Chavan Nikhil
Cheng Esther
Chetruengchai Wanna
Chwialkowska Karolina
Cirulli Elizabeth T.
Dabe Shaun
Dabrowski Maciej
Del Valle Diane
Drivas Theodore
Edahiro Ryuya
Eng Stefan
Eveleigh Robert J.M.
Fava Francesca
Fawzy Mohammad
Ferreira Manuel A.R.
Forgetta Vincenzo
Frithiof Robert
Fukunaga Koichi
Furini Simone
Ganna Andrea
Geschwind Daniel H.
Gnjatic Sacha
Goldstein David B.
Gonzalez Alfredo
Grzymski Joseph J.
Gómez-Carballa Alberto
Hasegawa Takanori
Hirankarn Nattiya
Hultström Michael
Imoto Seiya
Ismail Said I.
Johnson Ruth
Jordan Daniel M.
Jung Junghyun
Kaja Elżbieta
Kanai Takanori
Karczewski Konrad J.
Kawai Yosuke
Kenneth Baillie J.
Kim-Schulze Seunghee
Kimura Akinori
Kiryluk Krzysztof
Korotko Urszula
Kosmicki Jack A.
Kundu Kousik
Kwasniewski Miroslaw
Langlais David
Lathrop Mark
Lee William
Lipcsey Miklos
Ludwig Kerstin U.
Mangul Serghei
Mari Francesca
Marincevic-Zuniga Yanara
Martinón-Torres Federico
Massadeh Salam
Mbarek Hamdi
Merad Miriam
Miyano Satoru
Moniuszko Marcin
Mooser Vincent
Morrison David
Motameny Susanne
Naito Tatsuhiko
Nakanishi Tomoko
Namkoong Ho
Neveux Iva
Niemira Magdalena
Nilaratanakul Voraphoj
Nordlund Jessica
Ogawa Seishi
Okada Yukinori
Olszewski Pawel
Ossowski Stephan
Pan Yu
Pardo-Seco Jacobo
Pasaniuc Bogdan
Phokaew Chureerat
Pongpanich Monnat
Pottinger Tess D.
Povysil Gundula
Przychodzen Bartlomiej
Pula Szymon
Quinodoz Mathieu
Renieri Alessandra
Riess Olaf
Riffle Stephen
Rivero-Calle Irene
Rivolta Carlo
Saad Chadi
Salas Antonio
Sanders Timothy
Sandoval Efren
Schadt Eric E.
Schiabor Barrett Kelly M.
Schmidt Axel
Schulte Eva C.
Sebra Robert
Shang Ning
Shotelersuk Vorasuk
Simons Nicole
Sloofman Laura G.
Smieszek Sandra
Soranzo Nicole
Stephens Alexis
Stockwell Amy D.
Stuckey Alex
Sugiyama Masaya
Sypniewski Mateusz
Tanudjaja Francisco
Tao Shu
Thompson Ryan C.
Tokunaga Katsushi
Tung Paul J.
Veerapen Kumar
Verma Anurag
Walter Klaudia
Washington Nicole L.
White Simon
Yamaguchi Takafumi N.
Yaspan Brian
Zawadzki Pawel
Zeberg Hugo
Çelik Elifnaz
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 03/11/2022
Field of study

Helsingin yliopiston digitaalinen arkisto

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
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Aguado JM
Aguilar C
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Aguilar-Salinas CA
Aguilera-Albesa S
Agüero D
Ahmad HF
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Al-Ja’afreh MM
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Al-Moasseb H
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Alamer LM
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Alawneh FM
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Albaiceta GM
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Alhousani TN
Ali A
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Ali IAM
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Almoguera B
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AlRawashdeh TJ
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Baddeley A
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Baikady RR
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Baldini M
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Bamford A
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Banach D
Banales JM
Banasik K
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Bancroft H
Band G
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Bandla N
Bani younis FM
Bano S
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Baptista-Rosas RC
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Basikolo C
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Bercades G
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Bevan E
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Bezerra JF
Bezerra MAC
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Bhatterjee R
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Biros D
Birt M
Bishop L
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Blackledge B
Blackman H
Blakemore H
Blanco-Grau A
Bland Y
Blasi F
Blay N
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Bliddal S
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Blunt M
Boada M
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Bocchieri P
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Bociek A
Boer C
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Boix-Palop L
Bokhari M
Boland A
Bolger A
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Boltwood K
Bolze A
Bombace S
Bombard Y
Bonfanti P
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Bonnici J
Booker L
Borgundvaag B
Borislavova B
Borja AL
Borra C
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Bossé Y
Botello A
Botfield D
Botfield L
Boua PR
Bouab M
Bough L
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Bowes A
Bowey A
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Bradley-Potts J
Bradshaw Z
Brady A
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Braun A
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Brayne A
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Bretherick AD
Brett M
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Brickell K
Bridgett V
Brimfield L
Brinkworth E
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Budylowski P
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Bull R
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Bunni L
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Burda D
Burgos C
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Burn I
Burnett C
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Burns K
Burrow A
Burt K
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Burton M
Busson A
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Butler A
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Butler S
Butler-Laporte G
Butler-Laporte G
Butt F
Butte MJ
Butte MJ
Butterworth-Cowin N
Button H
Buttriss C
Caballero-Garralda A
Cabral-Ortega L
Cabrelli L
Cabrero DG
Cadenas IF
Cadilla CL
Cagova L
Cal-Sabater P
Calderón EJ
Calderón EJ
Cale E
Callaghan M
Callam S
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Camarena A
Campbell A
Campbell B
Campbell H
Campbell R
Campbell S
Campigotto A
Campos A
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Camsooksai J
Cantú-Brito C
Capozzi L
Cappadona C
Cappelli C
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Carbonell C
Cardamone G
Cardwell A
Carmody M
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Carnahan M
Carpani R
Carrabba M
Carracedo Á
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Carter A
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Castelao JE
Castillejos-López M
Castoldi M
Castro P
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Catalán MA
Caterson J
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Catlow L
Caulfield MJ
Cavallero A
Cavazza A
Cave A
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Cazzaniga M
Cea C
Ceballos FC
Cecconi M
Cejudo TG
Ceriotti F
Cerpa LC
Cha M
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Chadwick R
Chaliasos K
Chan G
Chan R
Chandler B
Chandna H
Chang D
Chang TS
Chao G
Chapman S
Charles B
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Cheatley PL
Cheema Y
Chen H-H
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Chercoles AG
Cherian S
Chernitsov A
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Cherubini A
Chesters K
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Cheyne C
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Chihara Y
Chikowore P
Childs D
Chiquete E
Chirino-Pérez A
Chirouze C
Chisholm C
Chiu A
Choe K-W
Choudhr O
Choudhury Y
Chowdhary S
Christaki E
Christian MA
Chubachi S
Chueca N
Chuhan NT
Chukkambotla S
Chung M
Churchhouse C
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Chávez-Manzanera E
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Cirulli ET
Citerio G
Claire D-R
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Clark A
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Clark M
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Clark V
Clarke N
Clarkson M
Clausen M
Clayton S
Clement I
Clements S
Coates C
Cobat A
Cochrane P
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Corcoran E
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Cordero-Lorenzana ML
Cordioli M
Cordioli M
Corin C
Cornberg M
Cornell S
Cornell T
Cornely OA
Corner A
Corral MA
Cortes B
Cortes-Sanchez JL
Corton M
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Cother N
Coto E
Coton Z
Cottam L-J
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Coventry T
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Cowan J
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Crew A
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Cruz-Bautista I
Cruz-Cruz AD
Csabi P
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Damås JK
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Darlington K
Darnaude MT
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Das M
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Daubney E
Davey M
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De Jesús Suárez López J
De la Horra C
De León-Garduño AP
De los Ángeles Vargas-Martínez M
De Martino-Rodríguez A
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De Pablo R
De Quirós FGB
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De Salazar A
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Degenhardt F
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Del Consuelo Rodríguez Mancilla M
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Diaba C
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Dinh KM
Dixit RD
Diz-de Almeida S
Djeugam B
Dobaño C
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Domingo C
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Domínguez-Mayoral A
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Ducharme FM
Dudman S
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Dutta AK
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Décary S
Díaz-Olavarrieta C
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El-Shanshory MR
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Elliott LT
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Elzeiny A
Elías-López D
Emblem J
Endo A
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España PP
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Ezeobu O
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Falcone EL
Fan CC
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Farquhar F
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Faulkner B
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Faverio P
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Fazaal J
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Feldt-Rasmussen U
Felton T
Feng Y-CA
Ferguson S
Fernandes F
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Fernandes MR
Fernandez R
Fernandez Z
Fernandez-Cadenas I
Fernandez-Roman J
Fernandez-Ruiz J
Fernández J
Fernández-Robelo U
Fernández-Rodríguez A
Fernández-Villa T
Ferrando C
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Figuera Basso ME
Filipe H
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Finch C
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Fine C
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Flanagan R
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Fowler S
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Francescatto M
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Francis S
Frangione E
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Franke G
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Frankham J
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Friar Z
Frias E
Friaza V
Friedman SM
Frise M
Frithiof R
Fritzler M
Frost V
Fuchimoto Y
Fuentes M
Fuentes-Guajardo M
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Fujiwara A
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Fukuyama S
Funatsu Y
Fung CYJ
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Gago-Domínguez M
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Gallego-Durán R
Galván-Femenia I
Galván-Femenía I
Ganesan A
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Garant J-M
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Garcia F
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Garcia-Aymerich J
Garcia-Etxebarria K
Garcia-Fernandez A-E
García K
García-Clemente M
García-García L
García-Grimshaw M
García-Madrona S
Gardner A
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Garmendia A
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Gascoyne R
Gassner C
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Genetu R
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Georgiou I
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Gill J
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Gingras A-C
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Glasgow S
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Gloria EFD
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González-Lara MF
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González-Neira A
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Grimsrud MM
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Guadarrama-Pérez C
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Guerra-García MT
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Guillen-Pineda LE
Guillén-Quintero DM
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Helbig ET
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Herbrick J-A
Herdman-Grant R
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Hernández Cordero AI
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Silbiger VN
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Zainulabid UA
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Zamudio IPM
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Zarate R
Zarei N
Zavaleta DAF
Zawadzki P
Zawati MH
Zborowski AC
Zeberg H
Zechner M
Zhang Q
Zhao X
Zheng C
Zheng T
Zhlawi HJ
Zhlawi MWJ
Zholdybayeva E
Zhou W
Zhu W
Zitter L
Zoller H
Zongo O
Zorloni C
Zuñiga-Pacheco P
Zárate RN
Zúñiga-Ramos J
Álvarez BG
Ávila-Arcos MA
Ávila-Arcos MC
Özer O
Überla K
Þorsteinsdóttir U
Publication venue: Nature Research
Publication date: 21/06/2023
Field of study

Spiral - Imperial College Digital Repository