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143 research outputs found

A school-based program implemented by community providers previously trained for the prevention of eating and weight-related problems in secondary-school adolescents : the MABIC study protocol

Author: A Bandura
AE Field
AJ Hill
AJ Tomiyama
All Party Parliamentary Group on Body Image
American Psychiatric Association
American Psychological Association
B Sandin
BM Pratt
BR Flay
BR Flay
C Becker
C Chamay-Weber
C Sancho
CB Becker
CB Becker
Center for Media Literacy (CML)
Center for Media Literacy (CML)
CG Fairburn
D Le Grange
D Neumark-Sztainer
D Neumark-Sztainer
D Neumark-Sztainer
D Neumark-Sztainer
D Neumark-Sztainer
D Neumark-Sztainer
D Neumark-Sztainer
D Neumark-Sztainer
D Neumark-Sztainer
D Neumark-Sztainer
D Neumark-Sztainer
D Sánchez-Carracedo
D Sánchez-Carracedo
D Sánchez-Carracedo
D Watson
David Sánchez-Carracedo
DD Dunlop
DL Newman
DM Garner
DR Neumark-Sztainer
E Marchand
E Stice
E Stice
E Stice
E Stice
E Stice
E Stice
E Stice
E Stice
E Stice
E Stice
E Stice
E Stice
E Stice
EC Norton
Esther Trepat
FA Carter
G López-Guimerà
G López-Guimerà
G López-Guimerà
G López-Guimerà
G Morande
GC Patton
Gemma López-Guimerà
Government of Catalonia: Programa Salut i Escola
Grupo de Trabajo de la Guía de Práctica Clínica sobre Trastornos de la Conducta Alimentaria
H Holder
HL Littleton
J Arcelus
J Day
J Guest
J Haines
J Martin-Albo
J Mond
J Solomon
J Treasure
JA Hanley
JA O’Dea
JA O’Dea
JA O’Dea
JA O’Dea
JA O’Dea
JA Price
JF Morgan
JH Price
JI Hudson
JK Thompson
JK Thompson
JM Turner
Joaquim Puntí
Jordi Fauquet
JPA Ioannidis
JS Rawana
Juan Ramón Barrada
K Hoagwood
KA Halmi
KBC Wick
KD Reynolds
KE Holt
KL Graves
KY Liang
L Festinger
L Rojo
L Rojo-Moreno
L Smolak
M Calado
M Levine
M Perez
M Rosenberg
M Santos
MA Pelaez Fernandez
MC Fingeret
Mireia Querol
MJ Maloney
Montserrat Pàmias
N Klar
NI Larson
P Elosua
P Muro-Sans
P Warschburger
R Raich
RE Glasgow
RH Striegel-Moore
S Crow
S Stock
SA Swanson
SB Austin
SB Austin
SB Austin
SJ Crow
SL Zeger
SR Zubrick
T Baranowski
T Rodriguez-Cano
TD Wade
TJ Cole
TJ Cole
U Berger
U Berger
U Berger
WB Hansen
WR Shadish
Z Cooper
Z Yager
Z Yager
Z Yager
Z Yager
Z Yager
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2013
Field of study

Background: The prevention of eating disorders and disordered eating are increasingly recognized as public health priorities. Challenges in this field included moving from efficacy to effectiveness and developing an integrated approach to the prevention of a broad spectrum of eating and weight-related problems. A previous efficacy trial indicated that a universal disordered eating prevention program, based on the social cognitive model, media literacy educational approach and cognitive dissonance theory, reduced risk factors for disordered eating, but it is unclear whether this program has effects under more real-world conditions. The main aim of this effectiveness trial protocol is to test whether this program has effects when incorporating an integrated approach to prevention and when previously-trained community providers implement the intervention. Methods/design: The research design involved a multi-center non-randomized controlled trial with baseline, post and 1-year follow-up measures. Six schools from the city of Sabadell (close to Barcelona) participated in the intervention group, and eleven schools from four towns neighboring Sabadell participated in the control group. A total of 174 girls and 180 boys in the intervention group, and 484 girls and 490 boys in the control group were registered in class lists prior to baseline. A total of 18 community providers, secondary-school class tutors, nurses from the Catalan Government's Health and School Program, and health promotion technicians from Sabadell City Council were trained and delivered the program. Shared risk factors of eating and weight-related problems were assessed as main measures. Discussion: It will be vital for progress in disordered eating prevention to conduct effectiveness trials, which test whether interventions are effective when delivered by community providers under ecologically valid conditions, as opposed to tightly controlled research trials. The MABIC project will provide new contributions in this transition from efficacy to effectiveness and new data about progress in the integrated approach to prevention. Pending the results, the effectiveness trial meets the effectiveness standards set down by the Society for Prevention Research. This study will provide new evidence to improve and enhance disordered eating prevention programs

Crossref

LAReferencia - Red Federada de Repositorios Institucionales de Publicaciones Científicas Latinoamericanas

Springer - Publisher Connector

Repositorio Universidad de Zaragoza

PubMed Central

Diposit Digital de Documents de la UAB

AD51B in Familial Breast Cancer

Author: Achan A.
Aghmesheh M.
Aittom鋕i K.
Allan P.
Allen D.
Amor D.
Anderson L.
Andrews L.
Andrulis I.L.
Antill Y.
Anton-Culver H.
Armitage S.
Arndt V.
Arnold L.
Balleine R.
Bankier A.
Baron-Hay S.
Bastick P.
Beale P.
Beckmann M.W.
Beeghly-Fadiel A.
Beesley J.
Begbie S.
Beilby J.
Beith J.
Bell D.
Benitez J.
Bennett B.
Bennett I.
Berry G.
Billson V.
Blackburn A.
Blomfield P.
Blomqvist C.
Bogdanova N.V.
Bogwitz M.
Bojesen S.E.
Bolla M.K.
Bonaventura T.
Borresen-Dale A.-L.
Brand A.
Brauch H.
Braye S.
Brennan M.
Brenner H.
Brown B.
Brown M.
Br黱ing T.
Buckley M.
Burgess M.
Burke J.
Burwinkel B.
Butow P.
Byron K.
Byth K.
Callen D.
Camaris C.
Campbell I.
Carter J.
Challis D.
Chang-Claude J.
Chauhan D.
Chenevix-Trench G.
Christian A.
Clarke C.
Clingan P.
Colley A.
Coll閑 M.
Cotton D.
Couch F.J.
Cox A.
Crandon A.
Crook A.
Cross S.S.
Crouch R.
Cui J.
Culling B.
Cummings M.
Czene K.
Dalrymple C.
Darabi H.
Davy S.A.-M.
Dawson S.-J.
DeFazio A.
Delatycki M.
Dennis J.
Devilee P.
Dickson R.
Dixon J.
Dobrovic A.
Dodd T.
Dos-Santos-silva I.
Dudding T.
Dumont M.
Dunning A.M.
D鰎k T.
Easton D.F.
Edkins T.
Edwards L.
Edwards S.
Eisenbruch M.
Farshid G.
Fasching P.A.
Fawcett S.
Fellows A.
Fenton G.
Ferrier A.
Field M.
Figueroa J.
Firgaira F.
Flanagan J.
Fleming J.
Fong P.
Forbes J.
Fox S.
French J.
Friedlander M.
Gaff C.
Garc韆-Closas M.
Gard G.
Gardner M.
Gattas M.
George P.
Giles G.G.
Gill G.
Glasgow A.
Glendon G.
Goldblatt J.
Gonz醠ez-Neira A.
Grant P.
Greening S.
Grip M.
Grist S.
Grygiel J.
Gu閚el P.
Haan E.
Hacker N.
Haiman C.A.
Hall C.
Hall P.
Hallberg E.
Hamann U.
Hamilton A.
Hardie K.
Harnett P.
Harris M.
Hart S.
Hartikainen J.M.
Haviv I.
Hayward N.
Healey S.
Healy D.
Healy T.
Heiniger L.
Henderson D.
Hill J.
Hooning M.J.
Hopper J.L.
Horwood K.
Houghton R.
Humphrey E.
Hunt C.
Hyde S.
Jakubowska A.
James P.
Janssen H.
Jaworski R.
Jenkins M.
Jobling T.
Johnson D.
Jones A.
Kallioniemi A.
Kefford R.
Khan S.
Kidd A.
Kiely B.
Kiiski J.I.
Kirk J.
Kirsten F.
Koehler J.
Kollias J.
Kovalenko S.
Kristensen V.
Lade S.
Lakhani S.
Laurie R.
Leaming A.
Leary J.
Li J.
Lim J.
Lindblom A.
Lindeman G.
Links M.
Lipton L.
Lobb L.
Loughrey M.
Luben R.N.
Lubinski J.
Mann G.
Mannermaa A.
Manolitsas T.
Margolin S.
Marsden D.
Marsh D.
Mattson J.
McIntosh R.
McLachlan S.A.
McNally O.
McNealage J.
Meindl A.
Meiser B.
Meldrum C.
Michailidou K.
Mileshkin L.
Miller J.
Milne R.L.
Mitchell G.
Murray B.
Neesham D.
Neuhausen S.L.
Nevanlinna H.
Nevanlinna V.
Nevell D.
Newman B.
Nicklin J.
Nightingale S.
Nordestgaard B.G.
O'Callaghan N.
O'Connell S.
O'Loughlin I.
Obermair A.
Oehler M.K.
Olson J.E.
Orr N.
Osborne R.
Otton G.
Pachter N.
Papadimos D.
Parker A.
Patterson B.
Pavlakis N.
Pelttari L.M.
Perrin L.
Peterlongo P.
Peters L.
Peto J.
Pharoah P.D.P.
Phillips K.
Pierdes J.
Pittman K.
Price M.
Proietto A.
Purdie D.
Purser L.
Pyman J.
Quinn M.
Radice P.
Ranta S.
Reeve J.
Reeve T.
Richards R.
Rickard E.
Rischin D.
Robbie M.
Robertson G.
Robinson B.
Rogers P.
Rome R.
Rosenberg E.H.
Rudolph A.
Rudzki B.
Russell P.
Rutovitz J.
Saleh M.
Salisbury E.
Sambrook J.
Saunders C.
Saunus J.
Sawyer E.J.
Sayer R.
Schleutker J.
Schmidt M.K.
Schmutzler R.K.
Schumacher F.
Scott C.
Scott E.
Scott R.
Seshadri R.
Sexton A.
Seynaeve C.
Shah M.
Shannon J.
Sharma R.
Shelling A.
Simard J.
Simpson I.
Simpson P.
Southey M.C.
Spurdle A.
Stewart J.
Stuart-Harris R.
Sumithran E.
Surowy H.
Susil B.
Suthers G.
Swerdlow A.
Sykes P.
Taylor D.
Taylor J.
Thierry B.
Thompson E.
Thorne H.
Tomlinson I.
Torres D.
Townshend S.
Trainer A.
Tran L.
Truong T.
Tucker K.
Tyler J.
Valmadre S.
Van Dyck L.
Vilske S.
Visvader J.
Vuorela M.
Wain G.
Walker L.
Walpole I.
Wang Q.
Ward B.
Ward R.
Waring P.
Warner B.
Warren G.
Whiteman D.
Williams R.
Wilson J.
Winqvist R.
Winship I.
Wu K.
Wyld D.
Yannoukakos D.
Young B.
Young M.A.
Zheng W.
Publication venue
Publication date: 01/01/2016
Field of study

Common variation on 14q24.1, close to RAD51B, has been associated with breast cancer: rs999737 and rs2588809 with the risk of female breast cancer and rs1314913 with the risk of male breast cancer. The aim of this study was to investigate the role of RAD51B variants in breast cancer predisposition, particularly in the context of familial breast cancer in Finland. We sequenced the coding region of RAD51B in 168 Finnish breast cancer patients from the Helsinki region for identification of possible recurrent founder mutations. In addition, we studied the known rs999737, rs2588809, and rs1314913 SNPs and RAD51B haplotypes in 44,791 breast cancer cases and 43,583 controls from 40 studies participating in the Breast Cancer Association Consortium (BCAC) that were genotyped on a custom chip (iCOGS). We identified one putatively pathogenic missense mutation c.541C>T among the Finnish cancer patients and subsequently genotyped the mutation in additional breast cancer cases (n = 5259) and population controls (n = 3586) from Finland and Belarus. No significant association with breast cancer risk was seen in the meta-analysis of the Finnish datasets or in the large BCAC dataset. The association with previously identified risk variants rs999737, rs2588809, and rs1314913 was replicated among all breast cancer cases and also among familial cases in the BCAC dataset. The most significant association was observed for the haplotype carrying the risk-alleles of all the three SNPs both among all cases (odds ratio (OR): 1.15, 95% confidence interval (CI): 1.11–1.19, P = 8.88 x 10−16) and among familial cases (OR: 1.24, 95% CI: 1.16–1.32, P = 6.19 x 10−11), compared to the haplotype with the respective protective alleles. Our results suggest that loss-of-function mutations in RAD51B are rare, but common variation at the RAD51B region is significantly associated with familial breast cancer risk

Measurement of ϒ production in pp collisions at √s = 2.76 TeV

Author: Aaij R.
Adeva B.
Adinolfi M.
Affolder A.
Aix-Marseille Univ. CNRS, MADIREL (UMR 7246)
Ajaltouni Z.
Albor V. Fernandez
Albrecht J.
Alessio F.
Alexander M.
Ali S.
Alkhazov G.
Altarelli M. Pepe
Alvarez A. Pazos
Alves A.A.
Amato S.
Amerio S.
Amhis Y.
Anderlini L.
Anderson J.
Andreassen R.
Andreotti M.
Andrews J.E.
Appleby R.B.
Archilli F.
Artamonov A.
Artuso M.
Aslanides E.
Astrophysics Group Cavendish Laboratory
Auriemma G.
Baalouch M.
Bachmann S.
Back J.J.
Badalov A.
Balagura V.
Baldini W.
Barlow R.J.
Barschel C.
Barsuk S.
Barter W.
Batozskaya V.
Bauer Th
Bay A.
Beddow J.
Bedeschi F.
Bediaga I.
Belogurov S.
Belous K.
Belyaev I.
Ben-Haim E.
Bencivenni G.
Benson S.
Benton J.
Berezhnoy A.
Bernet R.
Bettler M.-O.
Bien A.
Bifani S.
Bird T.
Bizzeti A.
Bjørnstad P.M.
Blake T.
Blanc F.
Blouw J.
Blusk S.
Bocci V.
Bondar A.
Bondar N.
Bonivento W.
Borghi S.
Borgia A.
Borsato M.
Bowcock T. J. V.
Bowen E.
Bozzi C.
Brambach T.
Bressieux J.
Brett D.
Britsch M.
Britton T.
Brook N.H.
Brown H.
Budker Institute of Nuclear Physics of the Siberian Branch of the RAS
Bursche A.
Busetto G.
Buytaert J.
Cadeddu S.
Calabrese R.
Callot O.
Calvi M.
Camboni A.
Campana P.
Canto A. Di
Carbone A.
Carboni G.
Cardinale R.
Cardini A.
Cardoso L. A. Granado
Carranza-Mejia H.
Carson L.
Cartelle P. Alvarez
Carvalhoakiba K.
Casasus M. Plo
Casse G.
Cattaneo M.
Cauet Ch
Cenci R.
Centre National de la Recherche Scientifique
Centro Brasileiro de Pesquisas Físicas (CBPF)
Charles M.
Charpentier Ph
Cheung S.-F.
Chiapolini N.
Chrzaszcz M.
Ciba K.
Cidvidal X.
Ciezarek G.
Cittadella Universitaria
Clarendon Laboratory
Clarke P. E. L.
Clemencic M.
Cliff H.V.
Closier J.
CNRS/IN2P3
Coca C.
Coco V.
Cogan J.
Cogneras E.
collaboration The LHCb
Collins P.
Comerma-Montells A.
Contu A.
Cook A.
Coombes M.
Coquereau S.
Corti G.
Counts I.
Coutinho R. Silva
Couturier B.
Cowan G.A.
Craik D.C.
Cunliffe S.
Currie R.
Dalseno J.
David P.
David P. N. Y.
Davis A.
De Bonis Bonis I.
De Bruyn Bruyn K.
De Capua Capua S.
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De Miranda Miranda J.M.
De Paula B. Souza
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De Silva Silva W.
De Simone Simone P.
De Vries Vries J.A.
Decamp D.
Deckenhoff M.
Del Buono Buono L.
Derkach D.
Deschamps O.
Dettori F.
Diaz R. Graciani
Dijkstra H.
Dipartimento di Fisica dell'Università
Donleavy S.
Dordei F.
Dorigo M.
Dorosz P.
Dos Reis Reis A.C.
Dossett D.
Dovbnya A.
Dupertuis F.
Durante P.
Dzhelyadin R.
Dziurda A.
Dzyuba A.
Déléage N.
D’Ambrosio C.
Easo S.
Egede U.
Egorychev V.
Eidelman S.
Eisenhardt S.
Eitschberger U.
Ekelhof R.
Eklund L.
El Rifai Rifai I.
Elsasser Ch
EPFL
Esen S.
European Organization for Nuclear Research
Faculty of Physics and Applied Computer Science
Falabella A.
Farinelli C.
Farry S.
Federal University of Rio de Janeiro
Ferguson D.
Ferro-Luzzi M.
Filippov S.
Fiore M.
Fiorini M.
Fitzpatrick C.
Fontana M.
Fontanelli F.
Forty R.
Francisco O.
Frank M.
Frei C.
Frosini M.
Fu J.
Furfaro E.
Färber C.
Galli D.
Gandelman M.
Gandini P.
Gao Y.
Garcia L. Castillo
Garcia M. Ubeda
Garofoli J.
Garrido L.
Gaspar C.
Gauld R.
Gersabeck E.
Gersabeck M.
Gershon T.
Ghez Ph
Gianelle A.
Giani’ S.
Gibson V.
Giubega L.
Gligorov V.V.
Goicochea J. M. Otalora
Golubkov D.
Golutvin A.
Gomes A.
Gomez M. Calvo
Gomez R. Vazquez
Gordon H.
Graugés E.
Graziani G.
Grecu A.
Greening E.
Gregson S.
Griffith P.
Grillo L.
Grünberg O.
Gui B.
Guimaraes V. Salustino
Gushchin E.
Gutierrez O. Aquines
Guz Yu
Gys T.
Gándara M. Grabalosa
Göbel C.
Hadjivasiliou C.
Haefeli G.
Haen C.
Hafkenscheid T.W.
Haines S.C.
Hall S.
Hamilton B.
Hampson T.
Hansmann-Menzemer S.
Harnew N.
Harnew S.T.
Harrison J.
Hartmann T.
He J.
Head T.
Heijne V.
Hennessy K.
Henrard P.
Henry L.
Henryk Niewodniczanski Institute of Nuclear Physics Polish Academy of Sciences
Heß M.
Hicheur A.
High-Energy Frontier
Hill D.
Hoballah M.
Hombach C.
Horia Hulubei National Institute of Physics and Nuclear Engineering
Hulsbergen W.
Hunt P.
Hussain N.
Hutchcroft D.
Hynds D.
Iakovenko V.
Idzik M.
Ilten P.
Imperial College
IN2P3 Institut National de Physique Nucleaire et de Physique des Particules
INFN - Sezione di Bologna
Infn Sezione di Ferrara
INFN Sezione di Firenze
INFN Sezione di Milano-Bicocca
INFN Sezione di Padova
INFN-Sezione di Bari
INFN-Sezione di Pisa
INS CNRS
Institute for High Energy Physics (IHEP)
Institute for Nuclear Research of the National Academy of Sciences (KINR)
Institute for Nuclear Research of the Russian Academy of Sciences (INR RAN)
Institute of Theoretical and Experimental Physics (ITEP)
Jacobsson R.
Jaeger A.
Jans E.
Jaton P.
Jawahery A.
Jing F.
John M.
Johnson D.
Jones C.R.
Joram C.
Jost B.
Jurik N.
Kaballo M.
Kandybei S.
Kanso W.
Karacson M.
Karbach T.M.
Kelsey M.
Kenyon I.R.
Ketel T.
Khanji B.
Khurewathanakul C.
Klaver S.
Kochebina O.
Komarov I.
Koopman R.F.
Koppenburg P.
Korolev M.
Kozlinskiy A.
Kravchuk L.
Kreplin K.
Kreps M.
Krocker G.
Krokovny P.
Kruse F.
Kucharczyk M.
Kudryavtsev V.
Kurek K.
Kvaratskheliya T.
La Thi Thi V.N.
Laboratoire d'Annecy de Physique des Particules (LAPP) Univ. Grenoble Alpes, Université Savoie Mont Blanc
Laboratori Nazionali di Frascati dell'INFN
Lacarrere D.
Lafferty G.
Lai A.
Lambert D.
Lambert R.W.
Lanciotti E.
Lanfranchi G.
Langenbruch C.
Latham T.
Lazzeroni C.
Le Gac Gac R.
Lebedev Physical Institute and NRNU MEPhl
Lees J.-P.
Leflat A.
Lefrançois J.
Lefèvre R.
Leo S.
Leroy O.
Lesiak T.
Leverington B.
Li Y.
Liles M.
Lindner R.
Linn C.
Lionetto F.
Liu B.
Liu G.
Lohn S.
Longstaff I.
Lopes J.H.
Lopez-March N.
Lowdon P.
Lu H.
Lucchesi D.
Luisier J.
Luo H.
Luppi E.
Lupton O.
Machefert F.
Machikhiliyan I.V.
Maciuc F.
Maev O.
Malde S.
Manca G.
Mancinelli G.
Manisa Celal Bayar University
Manzali M.
Maratas J.
Marconi U.
Marino P.
Marks J.
Martellotti G.
Martens A.
Martinelli M.
Massachusetts Institute of Technology
Massafferri A.
Matev R.
Mathe Z.
Matteuzzi C.
Max-Planck-Institut für Kernphysik (MPIK)
Mazurov A.
Mccann M.
Mccarthy J.
Mcnab A.
Mcnulty R.
Mcskelly B.
Meadows B.
Meier F.
Meissner M.
Merk M.
Milanes D.A.
Minard M.-N.
Molina V. Rives
Monteil S.
Moran D.
Morandin M.
Morata J. A. Hernando
Morawski P.
Mordà A.
Morello M.J.
Moscow State University
Mountain R.
Muheim F.
Muresan R.
Muryn B.
Muster B.
Märki R.
Müller K.
Naik P.
Nakada T.
Nandakumar R.
Nasteva I.
National Centre for Nuclear Research (NCBJ)
National Research Centre Kurchatov Institute
Navarro A. Puig
Needham M.
Neri N.
Neubert S.
Neufeld N.
Nguyen A.D.
Nguyen T.D.
Nguyen-Mau C.
Nicol M.
Niess V.
Niet R.
Nikhef
Nikitin N.
Nikodem T.
Novoselov A.
Novosibirsk State University
NSC Kharkiv Institute of Physics and Technology (NSC KIPT)
Oblakowska-Mucha A.
Obraztsov V.
Oggero S.
Ogilvy S.
Okhrimenko O.
Oldeman R.
Olloqui E. Picatoste
Onderwater G.
Orlandea M.
Owen P.
Oyanguren A.
Pal B.K.
Palano A.
Palombo F.
Palutan M.
Panman J.
Papanestis A.
Pappagallo M.
Pappalardo L.
Paris Diderot University - Paris VII
Parkes C.
Parkinson C.J.
Passaleva G.
Patel G.D.
Patel M.
Patrignani C.
Pavel-Nicorescu C.
Pearce A.
Pellegrino A.
Penso G.
Perazzini S.
Perez D. Campora
Perez P. Rodriguez
Perret P.
Perrin-Terrin M.
Pescatore L.
Pesen E.
Pessina G.
Petersburg Nuclear Physics Institute (PNPI)
Petridis K.
Petrolini A.
Pietrzyk B.
Pilař T.
Pinci D.
Pistone A.
Playfer S.
Polci F.
Polok G.
Poluektov A.
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Precision Frontier
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Vrije Universiteit Amsterdam de Boelelaan
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Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2014
Field of study

The production of ϒ(1S), ϒ(2S) and ϒ(3S) mesons decaying into the dimuon final state is studied with the LHCb detector using a data sample corresponding to an integrated luminosity of 3.3 pb−1 collected in proton–proton collisions at a centre-of-mass energy of √s = 2.76 TeV. The differential production cross-sections times dimuon branching fractions are measured as functions of the ϒ transverse momentum and rapidity, over the ranges pT < 15 GeV/c and 2.0 < y < 4.5. The total cross-sections in this kinematic region, assuming unpolarised production, are measured to be σ (pp → ϒ(1S)X) × B ϒ(1S)→μ+μ− = 1.111 ± 0.043 ± 0.044 nb, σ (pp → ϒ(2S)X) × B ϒ(2S)→μ+μ− = 0.264 ± 0.023 ± 0.011 nb, σ (pp → ϒ(3S)X) × B ϒ(3S)→μ+μ− = 0.159 ± 0.020 ± 0.007 nb, where the first uncertainty is statistical and the second systematic

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Global patient outcomes after elective surgery: prospective cohort study in 27 low-, middle- and high-income countries.

Author: Ab Majid MA
Ab Rahman AS
Ab Rahman R
Abayasinghe C
Abbott T
Abdullah NH
Abdur-Rahman L
Abeloos J
Abernethy C
Abidin UN
Abrunhosa A
Absar M
Adam S
Adams D
Adams G
Adamson M
Adekola O
Adelaja Y
Ademola A
Adenekan A
Adenike O
Adeolu AA
Adetoye A
Adewale B
Adigun T
Adolfsson A
Aflori L
Africander C
Afshari A
Agarwal V
Agodirin O
Aguero Vera M
Aguzzoli C
Ahmad A
Ahmad N
Ahmad T
Ahmad T
Ahmad Y
Ahmed A
Ahmed J
Ai Y
Aignatoaie M
Aimoniotou-Georgiou E
Akanmu O
Akerman N
Akinwale M
Akring I
Al 'Amri K
Al Anizi M
Al hussaini S
Al-Soudaine Y
Aladin H
Alagbe-Briggs O
Alaman Laguarda G
Albaj S
Alcock D
Alcock L
Aldecoa C
Aldecoa C
Aleixo FB
Alexander H
Alexander M
Alexander-Sefre F
Alherz F
Ali H
Ali M
Ali S
Alias A
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Alias RLR
Alit MA
Allen S
Allen SJ
Allison J
Alloj C
Allorto NL
Allsop J
Almeida W
Alonso E
Alphonsus C
Alvares D
Alves MJ
Amador JCB
Ameer Y
Amendola CP
Ami N
Amstrup-Hansen L
Anagnou A
Andersen C
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Andreadaki E
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Andrew A
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Lopez AG
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Ververidou O
Vesely M
Vetsiou E
Vilela dos Santos AM
Virdi P
Visser L
Visvalingam S
Vivian M
Vlachogianni G
Vohra A
Vohra R
Voldaeva O
Voloudakis N
Volta CA
Von Heymann C
von Rhaden R
Voruz F
Wadams B
Waggett H
Walder B
Walkden G
Walker A
Walker E
Walker R
Walker R
Walker T
Wallace A
Wallace K
Wallet F
Walsgrove J
Walsh D
Wan X
Wang D
Wang D
Wang F
Wang G
Wang H
Wang H
Wang J
Wang J
Wang J
Wang J
Wang J
Wang K
Wang L
Wang L
Wang L
Wang S
Wang S
Wang S
Wang T
Wang W
Wang X-L
Wang Y
Wang Y
Wang Z
Wang Z
Wang Z
Wang Z
Ward J
Wasmund C
Wassall R
Watanabe Oliveira HR
Watson A
Watson N
Watt P
Waugh D
Waweru P
Waworuntu N
Waymouth E
Weatherall L
Weatherill J
Webb S
Weber E
Wei J
Weimann J
Weller D
Welsh S
Wen XH
Wen Y
Wen Z
Wendling PR
Wessels JD
Wetzel P
Weyland A
White S
White S
whitehouse A
Whitman Z
Whittle N
Whitworth H
Whysall K
Wibrandt I
Wickboldt N
Wickenhauser R
Wid WM
Widmark C
Wiegand-Loehnert C
Wighton E
Wigmore G
Wijeysundera D
Wikner M
Wild J
Wildes T
Wildi S
Williams A
Williams M
Williams S
Wilscott-Davids C
Wilson A
Wilson D
Wilson L
Wilson N
Wima S
Winch D
Winstone U
Winterton D
Wir WM
Wise R
Wittmann M
Wolfer A
Wollaston J
Wong C
Wong CW
Wong JY
Wong K
Wong KWK
Wong SM
Wong T
Wong WL
Woodgate A
Woolsey A
Woon YL
Worreth M
Wouters P
Wrench I
Wright S
Wu C
Wu C
Wu J
Wu J
Wu Q
Wu S
Wyffels P
Wylie K
Xia J
Xia Y
Xia Z-Y
Xiao W
Xiao W
Xie G
Xie J
Xie J
Xie K
Xifara A
Xiong X
Xiong Y
Xouplidis K
Xu G-J
Xu L
Xu L
Xu Q
Xu S
Xue R
Yagnik A
Yan Y
Yang J
Yang L
Yang Q
Yang S
Yang T
Yang Y
Yao S
Yao Y
Yap HL
Yarwood J
Yassaee A
Ye H
Ye H
Yegnaram S
Yeh E
Yin N
Yip CP
Yong J
Yu HC
Yu S
Yu T
Yu Y
Yuan D
Yuan F
Yuan J
Yuan J
Yuan Y
Yuliana A
Zaimi D
Zakynthinos S
Zamudio D
Zangrillo A
Zapata DDM
Zbitnew G
Zeidan L
Zeng Q
Zerman L
Zettergren J
Zhang B
Zhang E
Zhang H
Zhang H
Zhang H
Zhang J
Zhang K
Zhang L
Zhang M
Zhang M
Zhang Q
Zhang R
Zhang S
Zhang W
Zhang X
Zhang X
Zhang X
Zhang X
Zhang Y
Zhang Y
Zhang Y
Zhang Y
Zhao B
Zhao B
Zhao C
Zhao J
Zhao J
Zhao L
Zhao L
Zhao S
Zhao T
Zhao W
Zhao W
Zhao X
Zhen J
Zheng K
Zheng L
Zheng T
Zhong Y
Zhou C
Zhou D
Zhou H
Zhou H
Zhou J
Zhou J
Zhou J
Zhou X-J
Zhu X
Zhu X
Zhu Y
Zhu Z
Zhuang X
Zilis G
Zin NHM
Zingerle N
Zingg U
Zoerner F
Zonneveldt H
Zou X
Zoulamoglou M
Zsisku L
Publication venue: 'Oxford University Press (OUP)'
Publication date: 01/01/2016
Field of study

BACKGROUND: As global initiatives increase patient access to surgical treatments, there remains a need to understand the adverse effects of surgery and define appropriate levels of perioperative care. METHODS: We designed a prospective international 7-day cohort study of outcomes following elective adult inpatient surgery in 27 countries. The primary outcome was in-hospital complications. Secondary outcomes were death following a complication (failure to rescue) and death in hospital. Process measures were admission to critical care immediately after surgery or to treat a complication and duration of hospital stay. A single definition of critical care was used for all countries. RESULTS: A total of 474 hospitals in 19 high-, 7 middle- and 1 low-income country were included in the primary analysis. Data included 44 814 patients with a median hospital stay of 4 (range 2-7) days. A total of 7508 patients (16.8%) developed one or more postoperative complication and 207 died (0.5%). The overall mortality among patients who developed complications was 2.8%. Mortality following complications ranged from 2.4% for pulmonary embolism to 43.9% for cardiac arrest. A total of 4360 (9.7%) patients were admitted to a critical care unit as routine immediately after surgery, of whom 2198 (50.4%) developed a complication, with 105 (2.4%) deaths. A total of 1233 patients (16.4%) were admitted to a critical care unit to treat complications, with 119 (9.7%) deaths. Despite lower baseline risk, outcomes were similar in low- and middle-income compared with high-income countries. CONCLUSIONS: Poor patient outcomes are common after inpatient surgery. Global initiatives to increase access to surgical treatments should also address the need for safe perioperative care. STUDY REGISTRATION: ISRCTN5181700

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Evidence-based Kernels: Fundamental Units of Behavioral Influence

Author: A Ankjaer-Jensen
A Appels
A Biglan
A Biglan
A Biglan
A Biglan
A Carlsson
A Hudson
A Ridgway
A Robin
A Rolider
A Spirito
A Tanskanen
A Theodore
AA Berlin
AC Wagenaar
AD Pellegrini
AD Pellegrini
AE Kazdin
AG White
AH Crisp
AJ Abramowitz
AJ Abramowitz
AJ Richardson
AK Bay-Hinitz
AK Dellatan
AL Dunn
AL Dunn
AL Stoll
AL Stoll
AL Stoll
AM Cevasco
AM Greca la
AM Hall
Anthony Biglan
AP McCain
AR Cavalier
AS Matheson
AS Olafsdottir
AT Vazsonyi
AU Rickel
AW Todd
AY Mikami
B Beersma
B Cabello
B Egeland
B Krevor
B Larsson
B Law
B Nemets
BC Barmann
BC Barmann
BC Etzel
BC McCarty
BD Winn
BF Walsh
BK Martens
BL Burke
BR Flay
BS Cox
C Choenarom
C Conyers
C Conyers
C Harding
C Heap
C Hughes
C Lonnecker
C Ostrower
C Pechmann
C Pechmann
C Pechmann
C Pechmann
C Schwartz
C Webster-Stratton
CA Christle
CA Ferguson
CB Ferster
CB Gesch
CC Piazza
CD Adams
CD Furr-Holden
CH Hitchcock
CH Hitchcock
CH Lawshe
CH Skinner
CJ Walker
CL Harris
CL Melville
CL Ringwalt
CL Storr
CM Robinson
CM Saunders
CN Jacklin
CR Collier
CR Greenwood
CR Greenwood
CS Green
CS Lieber
CV Wilson
D Barnes
D Ben Shalom
D Borfitz
D Brown
D Burgess
D DeMartini-Scully
D Fletcher
D Hallfors
D Hallfors
D Houlihan
D McDougall
D Mischoulon
D Newbern
D Newbern
D Paquette
D Premack
D Waard de
DA Wolfe
DB Lennox
DB Shabani
DB Shabani
DC Grossman
DD Embry
DD Embry
DD Embry
DD Embry
DD Embry
DD Embry
DD Hallfors
DE Wolfe
Dennis D. Embry
DF Bjorklund
DF Dansereau
DF Dansereau
DH Allsopp
DH Schunk
DH Welsh
DJ Crews
DJ Flannery
DJ Howard
DK Smith
DL Schilling
DL Trammel
DM Browder
DM Kamps
DM Koffman
DO Rudin
DP Fry
DS Pine
DS Wilson
DW Blick
E Atlantis
E Clark
E Clark
E Rodrigues
E Scott
EG Krug
EJ Doyne
EJ Thomas
EM Rogers
ES Geller
ES Petscher
ET Hartley
ET Hartley
F Jorgensen
F Juarez
F Lősel
F Merrett
F Scafidi
FE Hoath
FJ Silva
FR Blue
G Diamond
G Gaskell
G Perna
G Zivin
GA Fabiano
GD Sideridis
GJ Anderson
GJ DuPaul
GL Cohen
GL Schilmoeller
GM Egeland
GR Mayer
GR Mayer
GS Sorock
GT Taylor
GW Joe
GW Joe
H Aase
H Blumenfeld
H Deutsch
H Farber
H Jorgenson
H Lalramnghinglova
H Marin
HA Filcheck
HA Murphy
HAC Ninness
HB Andrews
HC Ninness
HH Barrish
HKM Antunes
HL Peck
HM Parsons
HM Parsons
HS Henderson
HS Terrace
HW Thorpe
HW Thorpe
IB Helland
J Backon
J Bernstein
J Derzon
J Gordon
J Hevel Van
J Hill
J Liu
J McCambridge
J Merrett
J Owusu-Bempah
J Owusu-Bempah
J Panksepp
J Szapocznik
JA Blumenthal
JB Barker
JB Hutton
JC Delquadri
JD Shannon
JE Fishbein
JE Mazur
JH Derzon
JH Sumner
JJ McCarl
JJ Priya
JK Fillingham
JK Luiselli
JK Porterfield
JL Lambert
JM Campbell
JM DiFilippo
JM Ducharme
JM Ducharme
JM Ducharme
JM Ducharme
JM Ducharme
JM Ducharme
JM Leibowitz
JM Richards
JM Smyth
JM Standley
JM Standley
JR Boyle
JR Hibbeln
JR Hibbeln
JR Hibbeln
JR Hibbeln
JR Hibbeln
JR Hibbeln
JR Hibbeln
JR Hibbeln
JS Downs
JS Kahn
JV Roca
JW Libb
JW Maag
JW Wedel
K Larson
K Mishima
K Nakano
K Resnicow
K Spindler
K Steiner
K Vaddadi
K-P Sund
KA Edwards
KA Maglieri
KA Rickards-Schlichting
KD Lakes
KE McGoey
KE Robinson
KK Kellum
KL Bledsoe
KM Greenwood
KM Hume
KR Harris
KT Kivlighan
KV Naveen
KW Reagles
L Chassin
L Kern
L Maheady
L Maheady
L McDonnell
L Selznick
LA Jason
LA Jason
LA Jason
LA Jason
LA Moore
LA Pawlow
LA Sisson
LAR Stein
LB Zaichkowsky
LC Sobell
LD Allen
LE Arnold
LE Arnold
LE Homme
LE Melchiori
LE Possell
LJ Pfiffner
LM Saari
LS Robertson
LS Robertson
LV Majovski
M Agathon
M Agran
M Bilici
M Cook
M Czuchry
M Czuchry
M Czuchry
M Czuchry
M Dekovic
M Fava
M Gonzalez
M Haag
M Heffner
M Hines
M Lowndes
M Marchant
M Marchant
M Marion
M O’Reilly
M Sherif
M Sherif
M Sherif
M Sherif
M Sidman
M Taubman
M Wolery
M Wolf
M-P Leblanc
MA Bray
MA Clarke
MA Diego
MA Woltersdorf
MB Medland
MB Stein
MC Keel
MC Luciano
MC Luciano-Soriano
MC Roberts
MC Zanarini
MJ Boulton
MJ Ford
MJ Koepp
MJ McMorrow
ML Kelley
ML McGrath
ML Rock
MM Acker
MM Wolf
MMR Madaus
MP Freeman
MP Freeman
MR Burch
MR Dadds
MR Sanders
MR Sanders
MR Sanders
MS Forgatch
MS Forgatch
MS Holloway
MT Hegel
MT Palermo
MW Arthur
MY Mathes
N Neave
N Nicol
N Ram
N Rusch
NA Jones
NC Jackson
NK McGrath-Hanna
NM Hunkin
NM Petry
NM Petry
NM Petry
NM Petry
NM Petry
NM Petry
NM Petry
NM Petry
NN Singh
NN Singh
NR Sharma
NS Gordon
NS Tobler
OS Elegbeleye
OS Jarrett
P Khatri
P Palmgreen
PG Mathes
PJ Krantz
PJ Schloss
PL Ellickson
PM Fischer
PM Monti
PM Stecker
PN Williamson
PT Norris
PW Clement
PW Dowrick
PW Dowrick
R Beyth-Marom
R Feldman
R Gardner
R Gupta
R Hoigaard
R Houten Van
R Houten Van
R Houten Van
R Houten Van
R Jarvinen
R Leclerc
R McGee
R Meadow
R Nordstrom
R Nordstrom
R Sandyk
R Snell
RA Block
RA Davis
RA Hirasing
RA Rawson
RB Reamer
RC Martella
RD Abbott
RE Dustman
RE Glasgow
RE Glasgow
RE Glasgow
RE Hosford
RF Putnam
RG Carey
RG Harrison
RJ Cowen
RJ Sampson
RM Bell
RM Foxx
RM Foxx
RP Liberman
RP West
RS Drabman
RS Morrison
RS Ragnarsson
RV Briscoe
RW Collins
S Akhondzadeh
S Akhtar
S Erkal
S Ghosh
S Gudbjarnason
S Houghton
S Kubesch
S Moore
S Plummer
S Rajan
S Roos
S Scott
S Sykes
S Telles
SA Godfrey
SA Stage
SC Bratton
SC Carr
SC Duncan
SC Hayes
SC Hayes
SE Rosenkoetter
SG Ferber
SG Kellam
SG Kellam
SG Stella
SI Gray
SJ Haas-Warner de
SJ Scholer
SJ Wood
SJ Wood
SK Clare
SK Wurtele
SM Burn
SM Colby
SM Dees
SM Ludington-Hoe
SM Shimabukuro
SM Siviy
SP Spera
SR Eisenstein
SS Leff
SS Meharg
SS Meharg
ST Ennett
SW Marshall
SW Twemlow
T Bellamy
T Buggey
T Buggey
T Buggey
T Dalton
T Field
T Field
T Field
T Field
T Norlander
T Ogden
T Reed
T Suzuki
TA Manger
TD Mickleborough
TF McLaughlin
TF McLaughlin
TH Wang
TH Wasserman
TJ Kehle
TJ Knapp
TK Taylor
TL St. Pierre
TL Stawar
TM Field
TM Field
TN Robinson
TO Lowe
TS Ball
TS Watson
TW Bean
TW Hosie
U Pitre
U Pitre
U Pitre
V Anderson
V Hertz
V Sanchez
VG Spencer
VL Taylor
VW Cotter
W Bennett
WB Davis
WR Miller
WS Agras
WT Phillips
XP Chen
Z Wencai
Publication venue: Springer US
Publication date: 01/01/2008
Field of study

This paper describes evidence-based kernels, fundamental units of behavioral influence that appear to underlie effective prevention and treatment for children, adults, and families. A kernel is a behavior–influence procedure shown through experimental analysis to affect a specific behavior and that is indivisible in the sense that removing any of its components would render it inert. Existing evidence shows that a variety of kernels can influence behavior in context, and some evidence suggests that frequent use or sufficient use of some kernels may produce longer lasting behavioral shifts. The analysis of kernels could contribute to an empirically based theory of behavioral influence, augment existing prevention or treatment efforts, facilitate the dissemination of effective prevention and treatment practices, clarify the active ingredients in existing interventions, and contribute to efficiently developing interventions that are more effective. Kernels involve one or more of the following mechanisms of behavior influence: reinforcement, altering antecedents, changing verbal relational responding, or changing physiological states directly. The paper describes 52 of these kernels, and details practical, theoretical, and research implications, including calling for a national database of kernels that influence human behavior

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PubMed Central

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

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Abdel-Aziz M.
Abdelrazik M.
Abdollahi H.
Abdullah T.
Abecasis G. R.
Abedalthagafi M.
Abel L.
Abernathy C.
Abraheem A.
Abul-Husn N. S.
Acquilini D.
Adams C.
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Adamsara A.
Adanini O.
Adeleye O.
Adra D.
Afilalo J.
Afilalo M.
Afolabi D.
Afrasiabi Z.
Agasou A.
Agrawal S.
Aguero D.
Ahmad N.
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Akeroyd L.
Akhtar M. N.
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Aksentijevich A.
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 A. E.
Alexander P.
Alfonso J.
Alghamdi B.
Alghamdi J.
Ali A.
Ali A.
Ali I. A. M.
Ali S.
Aliannejad R.
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AlJohani S.
Alkwai S.
Allan A.
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Almalki F.
Almohammed I.
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Zhao J. H.
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Zlatopolsky M.
Zollner S.
Zongo O.
Zucchi P.
Zyndorf M.
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2022
Field of study

Critical COVID-19 is caused by immune-mediated inflammatory lung injury. Host genetic variation influences the development of illness requiring critical care1 or hospitalization2–4 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

PubliCatt

Archivio istituzionale della ricerca - Università di Modena e Reggio Emilia

Study of the doubly charmed tetraquark T+cc

Author: Aaij R.
Abdelmotteleb A.S.W.
Abrantes F. Goncalves
Ackernley T.
Adeva B.
Adinolfi M.
Afsharnia H.
Agapopoulou C.
Aidala C.A.
Aiola S.
Aix-Marseille Univ. CNRS, MADIREL (UMR 7246)
Ajaltouni Z.
Akar S.
Akiba K. Carvalho
Albero A. Alfonso
Albrecht J.
Alepuz C. Remon
Alessio F.
Alexander M.
Aliouche Z.
Alkhazov G.
Altarelli M. Pepe
Amato S.
Amey J.L.
Amhis Y.
An L.
Anderlini L.
Andreianov A.
Andreotti M.
Archilli F.
Arctic Centre Univ. of Groningen
Artamonov A.
Artuso M.
Arzymatov K.
Aslanides E.
Astrophysics Group Cavendish Laboratory
Atzeni M.
Audurier B.
Bachmann S.
Bachmayer M.
Back J.J.
Balagura V.
Baldini W.
Barajas C. A. Chavez
Barbetti M.
Barlow R.J.
Barsuk S.
Barter W.
Bartolini M.
Baryshnikov F.
Basels J.M.
Bashir S.
Bassi G.
Batsukh B.
Battig A.
Bay A.
Beck A.
Becker M.
Bedeschi F.
Bediaga I.
Beiter A.
Belavin V.
Belin S.
Bellee V.
Belous K.
Belov I.
Belyaev I.
Ben-Haim E.
Bencivenni G.
Benito C. Marin
Berezhnoy A.
Bernet R.
Berninghoff D.
Bernstein H.C.
Bertella C.
Bertolin A.
Betancourt C.
Beteta C. Abellán
Betti F.
Bezshyiko Ia
Bhasin S.
Bhom J.
Bian L.
Bieker M.S.
Bifani S.
Billoir P.
Birch M.
Bishop F.C.R.
Bitadze A.
Bizzeti A.
Bjørn M.
Blago M.P.
Blake T.
Blanc F.
Blusk S.
Bobulska D.
Boelhauve J.A.
Boettcher T.
Boldyrev A.
Bondar A.
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Borghi S.
Borisyak M.
Borsato M.
Borsuk J.T.
Bouchiba S.A.
Bowcock T.J.V.
Boyer A.
Bozzi C.
Bradley M.J.
Braun S.
Brodzicka J.
Bruch D. Vom
Brundu D.
Budker Institute of Nuclear Physics of the Siberian Branch of the RAS
Buonaura A.
Buonincontri L.
Buono L. Del
Burke A.T.
Burr C.
Bursche A.
Butkevich A.
Butter J.S.
Buytaert J.
Byczynski W.
Cadeddu S.
Cai H.
Calabrese R.
Calefice L.
Cali S.
Calladine R.
Calvi M.
Campana P.
Canudas N. Valls
Capelli S.
Capriotti L.
Carbone A.
Carboni G.
Cardinale R.
Cardini A.
Cardoso L. A. Granado
Carli I.
Carniti P.
Cartelle P. Alvarez
Carus L.
Casasus M. Plo
Casse G.
Castro A. Pereiro
Castro J. Lomba
Cattaneo M.
Cavallero G.
Cazon B. R. Gruberg
Celani S.
Central China Normal University
Centre National de la Recherche Scientifique
Centro Brasileiro de Pesquisas Físicas (CBPF)
Cerasoli J.
Cervenkov D.
Chadwick A.J.
Chapman M.G.
Charles M.
Charpentier Ph
Chatzikonstantinidis G.
Chefdeville M.
Chen C.
Chen S.
Chernov A.
Chobanova V.
Cholak S.
Chrzaszcz M.
Chubykin A.
Chulikov V.
Ciambrone P.
Cicala M.F.
Cicco A. Di
Ciezarek G.
Cittadella Universitaria
Clarendon Laboratory
Clarke P.E.L.
Clemencic M.
Cliff H.V.
Closier J.
CNRS/IN2P3
Cobbledick J.L.
Coco V.
Coelho J.A.B.
Cogan J.
Cogneras E.
Cojocariu L.
collaboration LHCb
Collins P.
Colombo T.
Congedo L.
Contu A.
Cooke N.
Coombs G.
Corredoira I.
Corti G.
Coutinho R. Silva
Couturier B.
Craik D.C.
Crkovská J.
Currie R.
Dadabaev S.
Dai L.
Dall’Occo E.
Dalseno J.
Danilina A.
Davies J.E.
Davis A.
De Aguiar Francisco Aguiar Francisco O.
De Almeida F. L. Souza
De Bruyn Bruyn K.
De Capua Capua S.
De Cian Cian M.
De Miranda Miranda J.M.
De Paula B. Souza
De Paula Paula L.
De Serio Serio M.
De Simone Simone D.
De Simone Simone P.
De Vellis Vellis F.
de Vries Vries J.A.
Dean C.T.
Debernardis F.
Decamp D.
Dedu V.
Delaney B.
Dembinski H.-P.
Dendek A.
Denysenko V.
Derkach D.
Deschamps O.
Desse F.
Dettori F.
Dey B.
Diaz L. Calero
Diaz M. Vieites
Didenko S.
Dijk M. Van
Dijkstra H.
Dipartimento di Fisica dell'Università
Dobishuk V.
Dong C.
Donohoe A.M.
Dordei F.
dos Reis Reis A.C.
Douglas L.
Dovbnya A.
Downes A.G.
Dudek M.W.
Dufour L.
Duk V.
Durante P.
Durham J.M.
Dutta D.
Dziurda A.
Dzyuba A.
D’Ambrosio C.
d’Argent P.
Easo S.
Ecole Polytechnique
Egede U.
Egorychev V.
Eidelman S.
Eisenhardt S.
Ek-In S.
Eklund L.
Ely S.
Ene A.
Eotvos Lorand University
EPFL
Epple E.
Escher S.
Eschle J.
Esen S.
European Organization for Nuclear Research
Evans T.
Evolutionary and Behavioural Ecology Unit Museu de Ciències Naturals de Barcelona
Faculty of Physics and Applied Computer Science
Falabella A.
Fan J.
Fan Y.
Fang B.
Farry S.
Fazzini D.
Federal University of Rio de Janeiro
Fernandez R. A. Ruiz
Fernandez S. Gomez
Fernez A.D.
Ferrari F.
Ferrillo M.
Ferro-Luzzi M.
Figueras E. Vilella
Filippov S.
Fini R.A.
Fiorini M.
Firlej M.
Fischer K.M.
Fitzgerald D.S.
Fitzpatrick C.
Fiutowski T.
Fkiaras A.
Fleuret F.
Fontana M.
Fontanelli F.
Forty R.
Foulds-Holt D.
Frank M.
Franzoso E.
Frau G.
Frei C.
Friday D.A.
Fu J.
Fuehring Q.
Féo M.
Gabriel E.
Gac R. Le
Galati G.
Gallego F. J. Abudinen
Galli D.
Gambetta S.
Gan Y.
Gandelman M.
Gandini P.
Gao Y.
Garau M.
Garcia L. Meyer
Garcia O. Boente
Garrido L.
Gaspar C.
Geertsema R.E.
Gerick D.
Gerken L.L.
Gersabeck E.
Gersabeck M.
Gershon T.
Gerstel D.
Giambastiani L.
Gibson V.
Giemza H.K.
Gilman A.L.
Giovannetti M.
Gioventù A.
Gironell P. Gironella
Giubega L.
Giugliano C.
Gizdov K.
Gkougkousis E.L.
Gligorov V.V.
Goicochea J. M. Otalora
Golobardes E.
Golubkov D.
Golutvin A.
Gomes A.
Gomez M. Calvo
Gomez R. Vazquez
Goncerz M.
Gong G.
Gonzalo A. Brossa
Gorbounov P.
Gorelov I.V.
Gotti C.
Govorkova E.
Grabowski J.P.
Grammatico T.
Gras C. Sanchez
Graugés E.
Graverini E.
Graziani G.
Grecu A.
Greeven L.M.
Grieser N.A.
Grillo L.
Gromov S.
Gu C.
Guarise M.
Guittiere M.
Gushchin E.
Guth A.
Guz Y.
Gys T.
Göbel C.
Günther P.A.
Hadavizadeh T.
Haefeli G.
Haen C.
Haimberger J.
Halewood-leagas T.
Hamilton P.M.
Hammerich J.P.
Han Q.
Han X.
Hancock T.H.
Hansen E.B.
Hansmann-Menzemer S.
Harnew N.
Harrison T.
Hasse C.
Hatch M.
He J.
Hecker M.
Heijhoff K.
Heinicke K.
Hennequin A.M.
Hennessy K.
Henry L.
Henryk Niewodniczanski Institute of Nuclear Physics Polish Academy of Sciences
Heuel J.
Hicheur A.
Hill D.
Hilton M.
Hollitt S.E.
Horia Hulubei National Institute of Physics and Nuclear Engineering
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Yandex School of Data Analysis
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Zunica G.
Publication venue: Nature Research
Publication date: 01/01/2021
Field of study

Quantum chromodynamics, the theory of the strong force, describes interactions of coloured quarks and gluons and the formation of hadronic matter. Conventional hadronic matter consists of baryons and mesons made of three quarks and quark-antiquark pairs, respectively. Particles with an alternative quark content are known as exotic states. Here a study is reported of an exotic narrow state in the D0D0π+ mass spectrum just below the D*+D0 mass threshold produced in proton-proton collisions collected with the LHCb detector at the Large Hadron Collider. The state is consistent with the ground isoscalar T+cc tetraquark with a quark content of ccu⎯⎯⎯d⎯⎯⎯ and spin-parity quantum numbers JP = 1+. Study of the DD mass spectra disfavours interpretation of the resonance as the isovector state. The decay structure via intermediate off-shell D*+ mesons is consistent with the observed D0π+ mass distribution. To analyse the mass of the resonance and its coupling to the D*D system, a dedicated model is developed under the assumption of an isoscalar axial-vector T+cc state decaying to the D*D channel. Using this model, resonance parameters including the pole position, scattering length, effective range and compositeness are determined to reveal important information about the nature of the T+cc state. In addition, an unexpected dependence of the production rate on track multiplicity is observed

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Abdul Rasheed A.
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Publication venue: Springer Science and Business Media LLC
Publication date: 31/01/2024
Field of study

Dimethyl fumarate (DMF) inhibits inflammasome-mediated inflammation and has been proposed as a treatment for patients hospitalised with COVID-19. This randomised, controlled, open-label platform trial (Randomised Evaluation of COVID-19 Therapy [RECOVERY]), is assessing multiple treatments in patients hospitalised for COVID-19 (NCT04381936, ISRCTN50189673). In this assessment of DMF performed at 27 UK hospitals, adults were randomly allocated (1:1) to either usual standard of care alone or usual standard of care plus DMF. The primary outcome was clinical status on day 5 measured on a seven-point ordinal scale. Secondary outcomes were time to sustained improvement in clinical status, time to discharge, day 5 peripheral blood oxygenation, day 5 C-reactive protein, and improvement in day 10 clinical status. Between 2 March 2021 and 18 November 2021, 713 patients were enroled in the DMF evaluation, of whom 356 were randomly allocated to receive usual care plus DMF, and 357 to usual care alone. 95% of patients received corticosteroids as part of routine care. There was no evidence of a beneficial effect of DMF on clinical status at day 5 (common odds ratio of unfavourable outcome 1.12; 95% CI 0.86-1.47; p = 0.40). There was no significant effect of DMF on any secondary outcome

White Rose Research Online

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

Author: Abd Elghafar M.S.
Abdel-Aziz M.
Abdelrazik M.
Abdollahi H.
Abdullah T.
Abecasis G.R.
Abecasis G.R.
Abedalthagafi M.
Abel L.
Abernathy C.
Abraheem A.
Abul-Husn N.S.
Acquilini D.
Adams C.
Adams E.L.
Adams K.
Adamsara A.
Adanini O.
Adeleye O.
Adra D.
Afilalo J.
Afilalo M.
Afolabi D.
Afrasiabi Z.
Agasou A.
Agrawal S.
Agüero D.
Ahmad N.
Ahmadi S.
Ahmed A.
Ahmed C.
Akeroyd L.
Akhtar M.N.
Akinkugbe O.
Aksentijevich A.
Al Harthi F.
Al Mutairi A.
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 A.E.
Alexander P.
Alfonso J.
Alghamdi B.
Alghamdi J.
Ali A.
Ali A.
Ali I.A.M.
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Aliannejad R.
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Allan A.
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Almohammed I.
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Zöllner S.
Åsvold B.O.
Publication venue: Springer Science and Business Media LLC
Publication date: 07/07/2022
Field of study

Critical COVID-19 is caused by immune-mediated inflammatory lung injury. Host genetic variation influences the development of illness requiring critical care1 or hospitalization2,3,4 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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