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7 research outputs found

Social behaviour and collective motion in plant-animal worms

Author: Doran Carolina
Franks Nigel R.
Gamble Margaret L.
Gorman Alice R.
Grant Katherine A. G.
Grant Katherine A.J.
Plackett Harriet
Sendova-Franks Ana B.
Stumpe Martin
Stumpe Martin C.
Vizard Victoria
Worley Alan
Publication venue: 'The Royal Society'
Publication date: 24/02/2015
Field of study

© 2016 The Author(s) Published by the Royal Society. All rights reserved. Social behaviour may enable organisms to occupy ecological niches that would otherwise be unavailable to them. Here, we test this major evolutionary prin- ciple by demonstrating self-organizing social behaviour in the plant-animal, Symsagittifera roscoffensis. These marine aceol flat worms rely for all of their nutrition on the algae within their bodies: hence their common name. We show that individual worms interact with one another to coordinate their movements so that even at low densities they begin to swim in small polarized groups and at increasing densities such flotillas turn into circular mills. We use computer simulations to: (i) determine if real worms interact socially by com- paring them with virtual worms that do not interact and (ii) show that the social phase transitions of the real worms can occur based only on local inter- actions between and among them. We hypothesize that such social behaviour helps the worms to form the dense biofilms or mats observed on certain sun- exposed sandy beaches in the upper intertidal of the East Atlantic and to become in effect a super-organismic seaweed in a habitat where macro-algal seaweeds cannot anchor themselves. Symsagittifera roscoffensis, a model organ- ism in many other areas in biology (including stem cell regeneration), also seems to be an ideal model for understanding how individual behaviours can lead, through collective movement, to social assemblages

Crossref

UWE Bristol Research Repository

Association of C-reactive protein with bacterial and respiratory syncytial virus-associated pneumonia among children aged <5 years in the PERCH study

Author: Adrian P.V. (Peter)
Akarasewi P. (Pasakorn)
Anderson T.P. (Trevor P.)
Antonio M. (Martin)
Ashraf H. (Hasan)
Awori J.O. (Juliet O.)
Baggett H.C. (Henry C.)
Baillie V.L. (Vicky L.)
Brooks W.A. (W. Abdullah)
Bunthi C. (Charatdao)
Cascio S. (Stephanie)
Chipeta J. (James)
Chuananon S. (Somchai)
Crawley J. (Jane)
DeLuca A.N. (Andrea N.)
Driscoll A.J. (Amanda J.)
Ebruke B.E. (Bernard E.)
Endtz H.P. (Hubert)
Fancourt N. (Nicholas)
Feikin D.R. (Daniel R.)
Fu W. (Wei)
Goswami D. (Doli)
Groome M.J. (Michelle J.)
Hammitt L.L. (Laura L.)
Higdon M.M. (Melissa M.)
Hossain L. (Lokman)
Howie S.R.C. (Stephen R.C.)
Jahan Y. (Yasmin)
Kaewpan A. (Anek)
Kagucia E.W. (E. Wangeci)
Kahn G. (Geoff)
Kamau A. (Alice)
Karani A. (Angela)
Karron R. (Ruth)
Kazungu S. (Sidi)
Knoll M.D. (Maria Deloria)
Kotloff K.L. (Karen L.)
Kourouma N. (Nana)
Kuwanda L. (Locadiah)
Kwenda G. (Geoffrey)
Le T. (Tham)
Levine O.S. (Orin S.)
Li M. (Mengying)
Machuka E. (Eunice)
Mackenzie G. (Grant)
Madhi S.A. (Shabir A.)
Mahomed N. (Nasreen)
Maloney S.A. (Susan A.)
McLellan J. (Jessica)
Mitchell J. (Joanne)
Moore D.P. (David P.)
Morpeth S.C. (Susan C.)
Mudau A. (Azwifarwi)
Murdoch D.R. (David R.)
Mwananyanda L. (Lawrence)
Mwansa J. (James)
O'Brien K.L. (Katherine L.)
Ominde M.S. (Micah Silaba)
Onwuchekwa U. (Uma)
Park D.E. (Daniel E.)
Prosperi C. (Christine)
Rahman M.Z. (Mohammed Ziaur)
Rhodes J. (Julia)
Salaudeen R. (Rasheed)
Sawatwong P. (Pongpun)
Scott J.A.G. (J. Anthony G.)
Seidenberg P. (Phil)
Shamsul A. (Arifin)
Somwe S.W. (Somwe Wa)
Sow S.O. (Samba O.)
Sylla M. (Mamadou)
Tamboura B. (Boubou)
Tapia M.D. (Milagritos D.)
Thamthitiwat S. (Somsak)
Thea D.M. (Donald M.)
Toure A. (Aliou)
Watson N.L. (Nora L.)
Wu Z. (Zhenke)
Zaman K. (Khalequ)
Zaman S.M.A. (Syed M.A.)
Zeger S.L. (Scott L.)
Publication venue: 'Oxford University Press (OUP)'
Publication date: 01/01/2017
Field of study

Background. Lack of a gold standard for identifying bacterial and viral etiologies of pneumonia has limited evaluation of C-reactive protein (CRP) for identifying bacterial pneumonia. We evaluated the sensitivity and specificity of CRP for identifying bacterial vs respiratory syncytial virus (RSV) pneumonia in the Pneumonia Etiology Research for Child Health (PERCH) multicenter case-control study. Methods. We measured serum CRP levels in cases with World Health Organization-defined severe or very severe pneumonia and a subset of community controls. We evaluated the sensitivity and specificity of elevated CRP for "confirmed" bacterial pneumonia (positive blood culture or positive lung aspirate or pleural fluid culture or polymerase chain reaction [PCR]) compared to "RSV pneumonia" (nasopharyngeal/oropharyngeal or induced sputum PCR-positive without confirmed/suspected bacterial pneumonia). Receiver operating characteristic (ROC) curves were constructed to assess the performance of elevated CRP in distinguishing these cases. Results. Among 601 human immunodeficiency virus (HIV)-negative tested controls, 3% had CRP ≥40 mg/L. Among 119 HIVnegative cases with confirmed bacterial pneumonia, 77% had CRP ≥40 mg/L compared with 17% of 556 RSV pneumonia cases. The ROC analysis produced an area under the curve of 0.87, indicating very good discrimination; a cut-point of 37.1 mg/L best discriminated confirmed bacterial pneumonia (sensitivity 77%) from RSV pneumonia (specificity 82%). CRP ≥100 mg/L substantially improved specificity over CRP ≥40 mg/L, though at a loss to sensitivity. Conclusions. Elevated CRP was positively associated with confirmed bacterial pneumonia and negatively associated with RSV pneumonia in PERCH. CRP may be useful for distinguishing bacterial from RSV-associated pneumonia, although its role in discriminating against other respiratory viral-associated pneumonia needs further study

Erasmus University Digital Repository

Evaluating the Effects of SARS-CoV-2 Spike Mutation D614G on Transmissibility and Pathogenicity

Author: Aanensen David M.
Abudahab Khalil
Acheson Erwan
Adams Alexander
Adams Helen
Adriaenssens Evelien M.
Afifi Safiah
Aggarwal Dinesh
Ahmad Shazaad S.Y.
Alam Mohammad T.
Alcolea-Medina Adela
Alderton Alex
Alikhan Nabil-Fareed
Allan John
Allara Elias
Amato Roberto
Andersson Monique
Angyal Adrienn
Aranday-Cortes Elihu
Ariani Cristina
Asad Hibo
Asamaphan Patawee
Ashworth Jordan
Atkinson Laura
Attwood Stephen
Auckland Cressida
Awan Ali R.
Aydin Alp
Baker David J.
Baker Paul
Balcazar Carlos E.
Ball Jonathan
Barton Edward
Bashton Matthew
Batra Rahul
Baxter Laura
Beale Mathew A.
Beaver Charlotte
Beckett Angela
Beer Robert
Beggs Andrew
Bell Andrew
Bellis Katherine L.
Berger Duncan J.
Berriman Matt
Berry Lisa
Berry Louise
Betancor Gilberto
Betteridge Emma
Bewshea Claire M.
Bibby David
Bicknell Kelly
Birchley Alec
Bird Paul
Bishop Chloe
Blane Beth
Bolt Frances
Bonsall David
Boswell Tim
Bosworth Andrew
Bourgeois Yann
Boyd Olivia
Boyes John
Bradley Declan T.
Bradshaw Daniel
Breen Cassie
Bresner Catherine
Breuer Judith
Bridgewater Hannah E.
Brooks Tony T.
Broos Alice
Brown Julianne Rose
Brown Paul E.
Brown Rebecca
Brunker Kirstyn
Bucca Giselda
Buck David
Buddenborg Sarah K.
Bull Matthew
Bull Matthew
Burton-Fanning Shirelle
Butcher Ethan
Caddy Sarah L.
Caller Laura G.
Campbell Sharon
Carlile Matthew
Carmichael Stephen N.
Casey Anna
Castellano Sergi
Chalker Vicki
Chand Meera
Chapman Michael R.
Chappell Joseph G.
Charalampous Themoula
Charles Ian G.
Chaudhry Yasmin
Chauhan Anoop J.
Cheng Jeffrey K.J.
Churcher Carol M.
Clark Gemma
Coll Francesc
Collins Jennifer
Colquhoun Rachel
Colquhoun Rachel M.
Connor Thomas R.
Connor Thomas R.
Constantinidou Chrystala
Coombes Jason
Corden Sally
Cormie Claire
Cortes Nicholas
Cortes Nick
Cottrell Simon
Coupland Lindsay J.
Cowell Angela
Cox Alison
Craine Noel
Cronin Michelle
Crooke Derrick
Curran Martin D.
Curran Tanya
da Silva Filipe Ana
da Silva Filipe Ana
Dabrera Gavin
Danesh John
Darby Alistair C.
Davidson Rose K.
Davies Alisha
Davis Thomas
de Cesare Mariateresa
De Lacy Elen
de Oliveira Martins Leonardo
de Silva Thushan I.
Debebe Johnny
Dervisevic Samir
Dewar Rebecca
Dias Joana
Diaz Maria
Dibling Thomas
Dorman Matthew J.
Downing Fatima
Drury Eleanor
du Plessis Louis
Duckworth Nichola
Dyal Patricia L.
Eccles Richard
Edgeworth Jonathan
Edwards Sue
Eldirdiri Sahar
Ellaby Nicholas
Ellard Sian
Elliott Scott
Eltringham Gary
Elumogo Ngozi
Essex Sarah
Evans Cariad
Evans Johnathan M.
Eyre David
Fairley Derek J.
Fallon Karlie
Farbos Audrey
Farr Ben
Feltwell Theresa
Fina Laia
Findlay Jacqueline
Fisher Chloe L.
Fleming Vicki M.
Forrest Leysa M.
Forrest Sally
Foulser Luke
Francois Sarah
Fraser Christophe
Freeman Timothy M.
Frost Lucy R.
Fuller William
Gallagher Eileen
Gallagher Michael D.
Garcia-Casado Maria V.
Gaskin Amy
Gatica-Wilcox Bree
Gavriil Artemis
Geidelberg Lily
Geidelberg Lily
Gemmell Matthew
Georgana Iliana
George Ryan P.
Gifford Laura
Gilbert Lauren
Gill Harmeet K.
Gilroy Rachel A.J.
Girgis Sophia T.
Glaysher Sharon
Golubchik Tanya
Goncalves Sonia
Goodfellow Ian
Goodfellow Ian G.
Goodwin Scott
Graham Clive
Graham Lee
Gramatopoulos Dimitris
Green Angie
Green Luke R.
Greenaway Jane
Gregory Richard
Griffith Luke
Groves Danielle C.
Groves Natalie
Guest Martyn
Gulliver Huw
Gutierrez Ana Victoria
Hadjirin Nazreen F.
Haldenby Sam T.
Hale Antony D.
Hall Grant
Halstead Fenella
Hamilton William L.
Haque Tanzina
Harper Katherine L.
Harris Kathryn Ann
Harrison Ewan M.
Harrison Ian
Harrison James W.
Hartman Hassan
Hattersley Andrew
Heaney Judith
Helmer Thomas
Hesketh Andrew R.
Heyburn David
Higginson Ellen E.
Hill Verity
Hill Verity
Hilvers Ember
Hiscox Julian A.
Holden Matthew T.G.
Holmes Alison
Holmes Christopher
Holmes Nadine
Hoosdally Sarah
Hopes Richard
Hosmillo Myra
Houldcroft Charlotte J.
Howe Robin
Howson-Wells Hannah C.
Hubb Jonathan
Hughes Joseph
Hughes Margaret
Hunter Adam D.
Hutchings Stephanie
Impey Robert
Irish-Tavares Dianne
Iturriza-Gomara Miren
Jackson Ben
Jackson Ben
Jackson David A.
Jackson David K.
Jackson Kathryn A.
Jahun Aminu S.
James Keith
Jamrozy Dorota
Jarrett Ruth
Jeffries Aaron R.
Jesudason Natasha
Jesudason Natasha G.
John Michaela
Johnson Kate
Johnson Natasha
Johnson Rob
Johnson Robert
Johnston Ian
Jones Hannah
Jones Katie
Jones Rachel
Jones Sophie
Jorgensen David
Jorgensen David
Joseph Amelia
Justice Anita
Kane Leanne
Kay Gemma L.
Kay Sally
Keatley Jon-Paul
Keeley Alexander J.
Kenyon Anita
Kermack Leanne M.
Khakh Manjinder
Khokhar Fahad A.
Kidd Stephen
Kingsley Robert A.
Kitchen Christine
Knight Bridget A.
Kolyva Anastasia
Koshy Cherian
Kraemer Moritz
Kristiansen Mark
Kumziene-Summerhayes Sara
Kwiatkowski Dominic
Lackenby Angie
Langford Cordelia
Lawniczak Mara
Le-Viet Thanh
Lee David
Lee Jack C.D.
Letchford Laura
Levene Nick
Levett Lisa J.
Li Kathy
Li Kathy K.
Liggett Steven
Lindsey Benjamin B.
Lister Michelle M.
Livett Rich
Lloyd Allyson
Lo Stephanie
Loh Joshua
Loman Nicholas J.
Loman Nicholas J.
Loose Matthew W.
Loveson Katie F.
Lowe Hannah
Lucaci Anita O.
Ludden Catherine
Lynch Jessica
Lyons Ronan A.
Macfarlane-Smith Louissa R.
Machin Nicholas W.
MacIntyre-Cockett George
Madona Pinglawathee
Maes Mailis
Mahungu Tabitha W.
Mair Daniel
Maksimovic Joshua
Manesis Nikos
Manley Robin
Manso Carmen
Marchbank Angela
Martincorena Inigo
Martinez-Nunez Rocio T.
Masoli Jane A.H.
Mason Jenifer
Mather Alison E.
Mbisa Tamyo
McCluggage Kathryn
McClure Patrick C.
McCrone J.T.
McCrone John T.
McGuigan Samantha
McHugh Martin P.
McKenna James P.
McKerr Caoimhe
McMinn Liz
McMurray Claire
Meader Emma J.
Meadows Lizzie
Menegazzo Mirko
Meredith Luke W.
Merrick Ian
Mestek-Boukhibar Lamia
Miah Shahjahan
Michell Stephen L.
Michelsen Michelle L.
Molnar Zoltan
Monaghan Lynn
Mookerjee Siddharth
Moore Catherine
Moore Catrin
Moore Christopher
Moore Nathan
Morgan Mari
Morgan Sian
Mori Matilde
Moses Samuel
Muir Peter
Munn Robert
Myers Richard
Nascimento Fabricia F.
Nascimento Fabricia F.
Naydenova Plamena
Neaverson Alexandra S.
Nebbia Gaia
Nelson Andrew
Nelson Charlotte
Nelson Rachel
Nicholls Sam
Nicholls Samuel M.
Nichols Jenna
Niebel Marc O.
Niola Paola
Nomikou Kyriaki
O'Toole Elaine
O'Toole Áine
Orton Richard J.
Osman Husam
Ott Sascha
O’Grady Justin
O’Toole Áine
Pacchiarini Nicole
Pacchiarini Nicole
Padgett Debra
Page Andrew J.
Palmer Sophie
Palmer Steve
Panchbhaya Yasmin N.
Pandey Sarojini
Park Naomi
Parker Matthew D.
Parmar Surendra
Parr Yasmin A.
Parsons Paul J.
Partridge David G.
Pascall David J.
Patel Gaurang
Patel Minal
Patel Vineet
Paterson Steve
Payne Brendan A.I.
Peacock Sharon J.
Pearson Clare
Perry Malorie
Peto Timothy
Pinckert Malte L.
Platt Steven
Plimmer Amy
Poplawski Radoslaw
Potter Will
Prakash Reenesh
Prestwood Liam
Price Anna
Price Anna
Price James
Puethe Christoph
Pybus Oliver
Pybus Oliver G.
Pymont Hannah M.
Quail Mike
Quick Joshua
Raghwani Jayna
Ragonnet-Cronin Manon
Rainbow Lucille
Rajatileka Shavanthi
Rambaut Andrew
Rambaut Andrew
Ramsay Mary
Randell Paul A.
Raviprakash Veena
Raza Mohammad
Resende Silva Paola C.
Rey Sara
Rey Sara M.
Reynolds Nicola
Richter Alex
Robertson David L.
Robertson David L.
Robinson Esther
Robinson Trevor I.
Robson Samuel C.
Rogers Hazel A.
Rooke Stefan
Rowan Aileen
Rowe Will
Roy Sunando
Rudder Steven
Ruis Chris
Ryan Felicity
Sambles Christine M.
Sang Fei
Scarlett Garry P.
Schaefer Ulf
Scher Emily
Scott Carol
Scott Garren
Sethi Dheeraj K.
Shaaban Sharif
Shah Divya
Shah Rajiv
Shah Rajiv N.
Shankar Giri
Shaw Robert
Shepherd James
Shepherd James G.
Sheriff Nicola
Shirley Lesley
Signell Adrian W.
Sillitoe John
Simpson David A.
Singer Joshua B.
Sivaprakasam Venkat
Siveroni Igor
Siveroni Igor
Sloan Tim J.
Sluga Graciela
Smith Christen
Smith Colin P.
Smith Darren
Smith Nikki
Smith Wendy
Smollett Katherine L.
Snell Luke B.
Souster Emily
Southgate Joel
Southgate Joel
Spellman Karla
Spencer-Chapman Michael
Sridhar Sushmita
Stanley Rachael
Stanton Thomas D.
Starinskij Igor
Stark Richard
Stockton Joanne
Stuart Claire
Studholme David J.
Swindells Emma
Swingler Tracey
Taha Yusri
Tang Julian
Taylor Ben E.W.
Taylor Graham P.
Taylor Sarah
Taylor-Joyce Grace
Tedim Ana P.
Temperton Ben
Templeton Kate E.
Thompson Thomas
Thomson Emma C.
Thomson Emma C.
Thomson Nicholas M.
Thornton Alicia
Thurston Scott
Todd John A.
Tong Lily
Tonkin-Hill Gerry
Torok M. Estee
Trebes Amy
Trotter Alexander J.
Tsoleridis Theocharis
Tucker Rachel M.
Turtle Lance
Tutill Helena J.
Underwood Anthony P.
Unnikrishnan Meera
Vamos Edith E.
Vasylyeva Tetyana
Vattipally Sreenu
Vipond Ian B.
Volz Erik
Volz Erik M.
Wain John
Walsh Sarah
Wang Dennis
Wantoch Michelle
Warne Ben
Warwick-Dugdale Joanna
Wastenge Elizabeth
Watkins Joanne
Watts Joanne
Waugh Sheila
Webber Mark A.
Weeks Sam
Weldon Danni
Whitehead Mark
Williams Charlotte A.
Williams Chris
Williams David
Williams Rachel J.
Williams Rebecca
Williams Thomas
Williamson Kathleen A.
Willingham Iona
Wilson Harry D.
Wise Emma
Workman Trudy
Wright Victoria
Wyles Matthew
Wyllie Sarah
Yakovleva Anna
Yasir Muhammad
Yeats Corin A.
Yew Wen C.
Young Gregory R.
Young Jamie
Yu Xiaoyu
Zarebski Alex
Publication venue: Elsevier
Publication date: 07/01/2021
Field of study

Global dispersal and increasing frequency of the SARS-CoV-2 spike protein variant D614G are suggestive of a selective advantage but may also be due to a random founder effect. We investigate the hypothesis for positive selection of spike D614G in the United Kingdom using more than 25,000 whole genome SARS-CoV-2 sequences. Despite the availability of a large dataset, well represented by both spike 614 variants, not all approaches showed a conclusive signal of positive selection. Population genetic analysis indicates that 614G increases in frequency relative to 614D in a manner consistent with a selective advantage. We do not find any indication that patients infected with the spike 614G variant have higher COVID-19 mortality or clinical severity, but 614G is associated with higher viral load and younger age of patients. Significant differences in growth and size of 614G phylogenetic clusters indicate a need for continued study of this variant

Northumbria Research Link

Crossref

Online Research @ Cardiff

Lichaamsmetabolisme

Author: A. Clark
A. Iyer
A. Misra
A. Tsuchida
A.E. Butler
A.J. Walley
A.M. Cypess
A.M. Cypess
A.M. Shapiro
Alison M Paterson
B. Keymeulen
B. Marcheva
B.O. Roep
C.J. Willer
C.M. Larsen
Cécile Bossu
D. Delmeire
D. Lavens
D. Meyre
D.A. Stoffers
D.L. Eizirik
D.M. Stern
E. Hu
E. Hultman
E. Selvin
E. Woldt
Elizabeth Selvin
F. Chimienti
F. Schuit
F.A. Scheer
F.A. Scheer
F.C. Schuit
F.C. Schuit
F.K. Gorus
F.M. Ashcroft
George F. Cahill
Guy H. E. J. Vijgen
H. Arefanian
H. Chen
I. De Bourdeaudhuij
I. Weets
J. Krakoff
J. Rahier
J. Wu
J.A. Gebe
J.A. Todd
J.C. Erickson
J.L. Halaas
J.P. Chaput
J.R. Speakman
Janne C. de Ruyter
K. Clement
K. Lemaire
K. Moens
K. Yamagata
K. Yasuda
K.M. Narayan
K.M. Narayan
K.M. Utzschneider
Katherine M. Flegal
L. C. Antunes
L. Klein
L. Nistico
L. Thorrez
L.A. Tartaglia
L.J. Scott
L.L. Baggio
Luc F. Van Gaal
M. Brownlee
M. Cnop
M. Feuerer
M. Harrington
M. Ridderstrale
M. Solar
M. Stoffel
M. Vaxillaire
M.C. Sugden
M.R. Brodeur
M.S. Phillips
M.T. Malecki
N. Matsuoka
N.F. Bradford
P. Boström
P. Froguel
P. Samama
P. Ulrich
P. Zimmet
P.C. Buijs
P.E. Scherer
P.G. Kopelman
P.H. Moghaddam
P.O. Astrand
Per Westermark
R. Luft
R. Sladek
R.J. Loos
R.S. Jackson
S. Baekkeskov
S. Malkani
S. Seino
S.C. Collins
S.F. Grant
S.P. Weisberg
S.S. Rich
T. Brown
T. Kadowaki
T. Otonkoski
T. Otonkoski
T. Yamauchi
T.H. Lindner
V. Steinthorsdottir
V.L. Crotzer
W. Creutzfeldt
W. Gepts
W. Gepts
W. Kimber
W.D. van Marken Lichtenbelt
W.V. Brown
X. Xu
Y. Arita
Y. Oomura
Y. Zhang
Y.J. Liu
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

Genome-wide association identifies nine common variants associated with fasting proinsulin levels and provides new insights into the pathophysiology of type 2 diabetes

Author: Abecasis G. (Goncalo)
Abecasis G.R. (Gonçalo)
Abecasis G.R. (Gonçalo)
Aben K.K.H. (Katja)
Absher D. (Devin)
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Ahlqvist E. (Emma)
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Boekholdt S.M. (Matthijs)
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Cambien F. (François)
Campbell H. (Harry)
Cappuccio F.P. (Francesco P.)
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Carlquist J.F. (John)
Cauchi S. (Stephane)
Caulfield M. (Mark)
Cavalcanti-Proença C. (Christine)
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Chanock S.J. (Stephen)
Charpentier G. (Guillaume)
Chasman D.I. (Daniel)
Chatterjee N. (Nilanjan)
Chen C.-M. (Chih-Mei)
Chen H. (Han)
Chen L. (Li)
Chines P.S. (Peter)
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Clarke R.
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Coin L. (Lachlan)
Coin L. (Lachlan)
Collins F.S. (Francis S.)
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Cooper C. (Charles)
Cooper C.C. (Cyrus C.)
Cooper M.N. (Matthew N.)
Cooper M.N. (Matthew)
Cornelis M. (Marilyn)
Couper D.J. (David)
Crawford G. (Gabe)
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Danesh J. (John)
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Dedoussis G.V. (George)
Dedoussis G.V. (George)
Dedoussis G.V. (George)
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Deloukas P. (Panagiotis)
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Dupuis J. (Josée)
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Holm H. (Hilma)
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Hu F.B. (Frank)
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Illig T. (Thomas)
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Iribarren C. (Carlos)
Ishaq M. (Muhammad)
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Johnson P. (Paul)
Johnson P.R.V. (Paul R.V.)
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Kettunen J. (Johannes)
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Klopp N. (Norman)
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Kyriakou T. (Theodosios)
Kähönen M. (Mika)
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Lecoeur C. (Cécile)
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Lettre G. (Guillaume)
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Levinson D.F. (Douglas)
Li M. (Man)
Li S. (Shengxu)
Li X. (Xiaohui)
Liang L. (Liming)
Lieb W. (Wolfgang)
Lieverse A.G. (Aloysius)
Linksted P. (Pamela)
Liu J. (Jianjun)
Liu J. (Jianjun)
Lokki M.L.
Loley C. (Christina)
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Luan J.
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Marre M. (Michel)
Martin N.G. (Nicholas)
Martinez-Larrad M.T. (Maria Teresa)
McCarroll S.A. (Steven)
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Penninx B.W.J.H.
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Petersen A.K.
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Quyyumi A.A. (Arshed)
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Raitakari O. (Olli)
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Reilly M.P. (Muredach P.)
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Ripatti S. (Samuli)
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Segrè A.V. (Ayellet)
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Stančcáková A. (Alena)
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Strawbridge R.J. (Rona)
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Sun Q. (Qi)
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Syvänen A.C.
Tammesoo M.L.
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Thompson J.R. (John)
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Thorand B. (Barbara)
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Vliet-Ostaptchouk J.V. (Jana) van
Voight B.F. (Benjamin)
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Wallaschofski H. (Henri)
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Watanabe R.M. (Richard)
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Weedon M.N. (Michael)
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Welch R. (Ryan)
Welch R.P. (Ryan)
Wells G.A. (George)
Weyant R.J. (Robert)
Wheeler E. (Eleanor)
White C.C. (Charles)
Wichmann H.-E. (H-Erich)
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Wiegand S. (Susanna)
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Wiklund F. (Fredrik)
Wild P.S. (Philipp)
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Willemsen G.A.H.M. (Gonneke)
Willenborg C. (Christina)
Willer C.J. (Cristen)
Wilson J.F. (James F.)
Wingerden S. (Sophie) van
Winkler T.W. (Thomas W.)
Witte D.R. (Daniel R.)
Witte D.R. (Deniel)
Witteman J. (Jacqueline)
Witteman J.C.M. (Jacqueline)
Witteman J.C.M. (Jaqueline C.M.)
Wood A.R. (Andrew)
Workalemahu T. (Tsegaselassie)
Wright A.F. (Alan)
Wright B.J. (Benjamin)
Wu G. (Guanming)
Xie W. (Weijia)
Xu J. (Jianfeng)
Yang J. (Jian)
Yang J. (Joanna)
Yang T.-P. (Tsun-Po)
Ye S. (Shu)
Zabena C. (Carina)
Zaidi M.A. (Aghar)
Zaman K.S. (Khan Shah)
Zeggini E. (Eleftheria)
Zeller T. (Tanja)
Zethelius B. (Björn)
Zgaga L. (Lina)
Zhang Q. (Qunyuan)
Zhang W. (Weihua)
Zhao J.H. (Jing Hua)
Ziegler A. (Andreas)
Ziegler A. (Andreas)
Zillikens M.C. (Carola)
Zitting P. (Paavo)
Zondervan K.T. (Krina T.)
Zondervan K.T. (Krina)
Zwart J-A. (John-Anker)
Öhrvik J. (John)
Östenson C.-G. (Claes-Göran)
Publication venue
Publication date: 01/10/2011
Field of study

OBJECTIVE - Proinsulin is a precursor of mature insulin and C-peptide. Higher circulating proinsulin levels are associated with impaired b-cell function, raised glucose levels, insulin resistance, and type 2 diabetes (T2D). Studies of the insulin processing pathway could provide new insights about T2D pathophysiology. RESEARCH DESIGN AND METHODS - We have conducted a meta-analysis of genome-wide association tests of ;2.5 million genotyped or imputed single nucleotide polymorphisms (SNPs) and fasting proinsulin levels in 10,701 nondiabetic adults of European ancestry, with follow-up of 23 loci in up to 16,378 individuals, using additive genetic models adjusted for age, sex, fasting insulin, and study-specific covariates. RESULTS - Nine SNPs at eight loci were associated with proinsulin levels (P < 5 × 10-8). Two loci (LARP6 and SGSM2) have not been previously related to metabolic traits, one (MADD) has been associated with fasting glucose, one (PCSK1) has been implicated in obesity, and four (TCF7L2, SLC30A8, VPS13C/ C2CD4A/B, and ARAP1, formerly CENTD2) increase T2D risk. The proinsulin-raising allele of ARAP1 was associated with a lower fasting glucose (P = 1.7 3 10-4), improved b-cell function (P = 1.1 × 10-5), and lower risk of T2D (odds ratio 0.88; P = 7.8 × 10-6). Notably, PCSK1 encodes the protein prohormone convertase 1/3, the first enzyme in the insulin processing pathway. A genotype score composed of the nine proinsulin-raising alleles was not associated with coronary disease in two large case-control datasets. CONCLUSIONS - We have identified nine genetic variants associated with fasting proinsulin. Our findings illuminate the biology underlying glucose homeostasis and T2D development in humans and argue against a direct role of proinsulin in coronary artery disease pathogenesis

Erasmus University Digital Repository

Search for gravitational waves from Scorpius X-1 with a hidden Markov model in O3 LIGO data

Author: Abbott R.
Abe H.
Acernese F.
Ackley K.
Adhikari N.
Adhikari R.X.
Adkins V.K.
Adya V.B.
Affeldt C.
Agarwal D.
Agathos M.
Agatsuma K.
Aggarwal N.
Aguiar O.D.
Aiello Lorenzo
Ain A.
Ajith P.
Akutsu T.
Albanesi S.
Alfaidi R.A.
Allocca A.
Altin P.A.
Amato A.
Anand C.
Anand S.
Ananyeva A.
Anderson S.B.
Anderson W.G.
Ando M.
Andrade T.
Andres N.
Andri? T.
Andrés-Carcasona M.
Angelova S.V.
Ansoldi S.
Antelis J.M.
Antier S.
Apostolatos T.
Appavuravther E.Z.
Appert S.
Apple S.K.
Arai K.
Araya A.
Araya M.C.
Areeda J.S.
Arellano F.E.Peña
Aritomi N.
Arnaud N.
Arogeti M.
Aronson S.M.
Arène M.
Asada H.
Asali Y.
Ashton G.
Aso Y.
Assiduo M.
Aston S.M.
Astone P.
Aubin F.
AultONeal K.
Austin C.
Babak S.
Badaracco F.
Bader M.K.M.
Badger C.
Bae S.
Bae Y.
Baer A.M.
Bagnasco S.
Bai Y.
Baird J.
Bajpai R.
Baka T.
Ball M.
Ballardin G.
Ballmer S.W.
Balsamo A.
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Zhao G.
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Zhao Yue
Zhou R.
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Zhu Z.-H.
Zimmerman A.B.
Zucker M.E.
Zweizig J.
Publication venue: 'American Physical Society (APS)'
Publication date: 21/09/2022
Field of study

Results are presented for a semicoherent search for continuous gravitational waves from the low-mass x-ray binary Scorpius X-1, using a hidden Markov model (HMM) to allow for spin wandering. This search improves on previous HMM-based searches of Laser Interferometer Gravitational-Wave Observatory data by including the orbital period in the search template grid, and by analyzing data from the latest (third) observing run. In the frequency range searched, from 60 to 500 Hz, we find no evidence of gravitational radiation. This is the most sensitive search for Scorpius X-1 using a HMM to date. For the most sensitive subband, starting at 256.06 Hz, we report an upper limit on gravitational wave strain (at 95% confidence) of h 95 % 0 = 6.16 × 10 − 26 , assuming the orbital inclination angle takes its electromagnetically restricted value ι = 4 4 ° . The upper limits on gravitational wave strain reported here are on average a factor of ∼ 3 lower than in the second observing run HMM search. This is the first Scorpius X-1 HMM search with upper limits that reach below the indirect torque-balance limit for certain subbands, assuming ι = 4 4 °

Online Research @ Cardiff

Whole-genome sequencing reveals host factors underlying critical COVID-19

Author: Abd Elghafar Mohamed S.
Abdel-Aziz Mahmoud
Abdelrazik Marwa
Abdollahi Hamed
Abdullah T.
Abecasis Goncalo
Abedalthagafi M.
Abel Lynn
Abernathy C.
Abraheem Azmeralde
Abul-Husn Noura S.
Acquilini D.
Adams C.
Adams Emma L.
Adams K.
Adamsara Alireza
Adanini Olurenke
Adeleye O.
Adra D.
Afilalo J.
Afilalo M.
Afolabi D.
Afrasiabi Z.
Agasou A.
Agrawal Shruti
Agüero D.
Ahmad N.
Ahmadi Saeideh
Ahmed A.
Ahmed Cecilia
Akeroyd L.
Akhtar M.N.
Akinkugbe O.
Aksentijevich Alexandra
Al-Afghani H.
Al-Awdah L.
Alaamery M.
Alahmadey Z.Z.
Alaverdian D.
Alavere H.
Albader A.
Albaiceta G.M.
Albakri J.K.
AlBardis H.
Albeladi M.
Albesher N.
Albrich W.
AlDhawi N.
Aldridge J.
Aleagha Afshar Etemadi
Alexander Peter.
Alfonso J.
Alghamdi B.
Alghamdi J.
Ali A.
Ali Altaf
Ali I.A.M.
Ali Syamlan
Aliannejad Rasoul
Aljawini N.
AlJohani S.
Alkwai S.
Allan A.
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Alldis Zoe
Allen L.
Allen Meryem
Allen Schvearn
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Allison K.S.
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Almohammed I.
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Childs D.
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Choudhury Yasmin
Christine Almaden-Boyle None
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Churchhouse C.
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Cockrell Maeve
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Cother Naiara
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Crew A.
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Curgenven H.
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Cutler Sean
Cárcel-Márquez Jara
D'Alessandro M.
D'Mellow Kenton
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Da Gloria Edna Fernandes
Daga S.
Daglish Jacqueline
Dale K.
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Dalmau D.
Daly Mark J.
Daly Zoe
Dalziel Jack
Dance A.
Danesh J.
Daniel A.
Daniel Priya
Daniels A.
Darcis G.
Dark P.
Darlington K.
Das Mihaela
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Davey Miriam
David B.
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Day Nicky
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de Almeida Martins L.G.
de Cid R.
de Geus E.
de Gordoa Laura Ortiz-Ruiz
de la Cal-Sabater P.
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De Vivo O.
Deacon Bethan
Dearden Joy
Death Y.
Debreceni G.
DeDiego M.L.
Deelen P.
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Dennis C.
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Digby Brian
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Do Ron
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Durrant Georgia
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Elgar Greg
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Ferreira Manuel A.R.
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Glasgow Susannah.
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Joy Rosie
Jude Edward
Jung J.
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Sabrina R.
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Salehi Shahla
Salerni L.
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Samakomva Tinashe
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Schumacher N.
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Scott Zoe
Scotton P.G.
Scriven James
Sealfon Stuart
Seaman Rebecca
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Publication venue
Publication date: 01/01/2022
Field of study

Altres ajuts: Department of Health and Social Care (DHSC); Illumina; LifeArc; Medical Research Council (MRC); UKRI; Sepsis Research (the Fiona Elizabeth Agnew Trust); the Intensive Care Society, Wellcome Trust Senior Research Fellowship (223164/Z/21/Z); BBSRC Institute Program Support Grant to the Roslin Institute (BBS/E/D/20002172, BBS/E/D/10002070, BBS/E/D/30002275); UKRI grants (MC_PC_20004, MC_PC_19025, MC_PC_1905, MRNO2995X/1); UK Research and Innovation (MC_PC_20029); the Wellcome PhD training fellowship for clinicians (204979/Z/16/Z); the Edinburgh Clinical Academic Track (ECAT) programme; the National Institute for Health Research, the Wellcome Trust; the MRC; Cancer Research UK; the DHSC; NHS England; the Smilow family; the National Center for Advancing Translational Sciences of the National Institutes of Health (CTSA award number UL1TR001878); the Perelman School of Medicine at the University of Pennsylvania; National Institute on Aging (NIA U01AG009740); the National Institute on Aging (RC2 AG036495, RC4 AG039029); the Common Fund of the Office of the Director of the National Institutes of Health; NCI; NHGRI; NHLBI; NIDA; NIMH; NINDS.Critical COVID-19 is caused by immune-mediated inflammatory lung injury. Host genetic variation influences the development of illness requiring critical care or hospitalization after infection with SARS-CoV-2. The GenOMICC (Genetics of Mortality in Critical Care) study enables the comparison of genomes from individuals who are critically ill with those of population controls to find underlying disease mechanisms. Here we use whole-genome sequencing in 7,491 critically ill individuals compared with 48,400 controls to discover and replicate 23 independent variants that significantly predispose to critical COVID-19. We identify 16 new independent associations, including variants within genes that are involved in interferon signalling (IL10RB and PLSCR1), leucocyte differentiation (BCL11A) and blood-type antigen secretor status (FUT2). Using transcriptome-wide association and colocalization to infer the effect of gene expression on disease severity, we find evidence that implicates multiple genes-including reduced expression of a membrane flippase (ATP11A), and increased expression of a mucin (MUC1)-in critical disease. Mendelian randomization provides evidence in support of causal roles for myeloid cell adhesion molecules (SELE, ICAM5 and CD209) and the coagulation factor F8, all of which are potentially druggable targets. Our results are broadly consistent with a multi-component model of COVID-19 pathophysiology, in which at least two distinct mechanisms can predispose to life-threatening disease: failure to control viral replication; or an enhanced tendency towards pulmonary inflammation and intravascular coagulation. We show that comparison between cases of critical illness and population controls is highly efficient for the detection of therapeutically relevant mechanisms of disease

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