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111 research outputs found

B7-H4 Treatment of T Cells Inhibits ERK, JNK, p38, and AKT Activation

Author: A Honstettre
A Veillette
A Weiss
AE Krambeck
Alice Mui
B Su
B Su
B Tringler
BA Irving
C Meagher
C. Bruce Verchere
CE Whitehurst
CE Whitehurst
CL Yuan
CR Calvo
D Ou
DA Cross
Daniel L. Metzger
Dawei Ou
DB Straus
DV Prasad
E Kelly
G Kong
Garth L. Warnock
GG Chiang
GL Sica
H Owaki
I Kryczek
I Kryczek
IH Choi
Jianqiang Hao
K Toyooka
L Karnitz
L Van Parijs
LH Boise
Lieping Chen
LP Kane
NN Ahmed
NS Awadallah
RG Jones
RH Schwartz
RV Parry
Ryan M. Teague
S Salceda
SF Ziegler
W Kolanus
X Wang
X Zang
Xiaojie Wang
Ziliang Ao
Publication venue: Public Library of Science
Publication date: 04/01/2012
Field of study

B7-H4 is a newly identified B7 homolog that plays an important role in maintaining T-cell homeostasis by inhibiting T-cell proliferation and lymphokine-secretion. In this study, we investigated the signal transduction pathways inhibited by B7-H4 engagement in mouse T cells. We found that treatment of CD3+ T cells with a B7-H4.Ig fusion protein inhibits anti-CD3 elicited T-cell receptor (TCR)/CD28 signaling events, including phosphorylation of the MAP kinases, ERK, p38, and JNK. B7-H4.Ig treatment also inhibited the phosphorylation of AKT kinase and impaired its kinase activity as assessed by the phosphorylation of its endogenous substrate GSK-3. Expression of IL-2 is also reduced by B7-H4. In contrast, the phosphorylation state of the TCR proximal tyrosine kinases ZAP70 and lymphocyte-specific protein tyrosine kinase (LCK) are not affected by B7-H4 ligation. These results indicate that B7-H4 inhibits T-cell proliferation and IL-2 production through interfering with activation of ERK, JNK, and AKT, but not of ZAP70 or LCK

Public Library of Science (PLOS)

Crossref

Directory of Open Access Journals

PubMed Central

Percutaneous treatment of patients with heart diseases: selection, guidance and follow-up. A review

Author: A Carpentier
A Dowson
A Giardini
A Pearson
A Vahanian
A Vahanian
AJ Camm
AK Aslam
Alessandra Giamundo
Antonio Rapacciuolo
B Iung
B Schneider
B Vaidyanathan
BJL Van den Branden
BS Rana
C Jayasuriya
C Tamburino
Carla Contaldi
Carlo Di Nardo
CR Asher
CR Smith
DR Holmes
E Branwald
E Donal
E Grube
EA Bermudez
ES Brilakis
European Stroke Organisation (ESO) Executive Committee
F Maisano
F Roques
FE Silvestry
FE Silvestry
Federico Piscione
FH Edwards
G Webb
GE Pate
GE Pate
Giovanni Esposito
GP Ussia
H Hara
I Meissner
IM Singh
J Kefer
JF Piechaud
JL Mass
JL Zamorano
JM Jones
JW Park
K Yared
Lucia S Parrella
M Brainin
M De Bonis
Maria Prastaro
Maria-Angela Losi
MB Leon
MC Post
MR Di Tullio
MS Kim
NE Moat
NM Van Mieghem
NS Peters
O Onalan
O Zhong-Dong
P Davison
P Garg
R Al-Lamee
R Pisters
RA Krasushi
Raffaella Lombardi
RL Sacco
RO Bonow
Roberto Puglia
RR Moss
S Betocchi
S Homma
Sandro Betocchi
SK Thambidorai
SL Goldberg
SM Teague
SS Goels
T Feldman
T Feldman
TD Woods
U Krumsdorf
V Fernandes
Valentina Parisi
WA Zoghbi
WA Zoghbi
WB Kannel
YH Li
YLB Bayard
Z Amin
Publication venue: BioMed Central
Publication date: 01/01/2012
Field of study

Aortic stenosis and mitral regurgitation, patent foramen ovale, interatrial septal defect, atrial fibrillation and perivalvular leak, are now amenable to percutaneous treatment. These percutaneous procedures require the use of Transthoracic (TTE), Transesophageal (TEE) and/or Intracardiac echocardiography (ICE). This paper provides an overview of the different percutaneous interventions, trying to provide a systematic and comprehensive approach for selection, guidance and follow-up of patients undergoing these procedures, illustrating the key role of 2D echocardiography

Archivio della ricerca - Università degli studi di Napoli Federico II

Crossref

Springer

Springer - Publisher Connector

PubMed Central

Archivio della Ricerca - Università di Salerno

Enhancing assertive community treatment with cognitive behavioral social skills training for schizophrenia: study protocol for a randomized controlled trial

Author: AF Lehman
AR Weissman
AS Bellack
AS Bellack
AT Beck
AT Beck
BC Ho
Christine Rufener
CJ Wallace
CJL Murray
CR Bowie
D Hedeker
D Hedeker
D Lukoff
D Wiersma
David Sommerfeld
DB Cane
DG Kingdon
DG Robinson
Dimitri Perivoliotis
E Granholm
E Granholm
E Granholm
E Granholm
E Granholm
Eric Granholm
EW Twamley
G Haddock
GA Aarons
GB Teague
GL Haas
GM Curran
Gregory A. Aarons
H Häfner
HC Kraemer
J Usall
Jason L. Holden
JR McQuaid
JS Beck
Kim Mueser
KT Mueser
KT Mueser
KT Mueser
LJ Damschroder
MC Angermeyer
MD Sayers
ME Thase
MF Green
MF Green
MF Green
MK Benton
ML Davison
MM Kurtz
NC Andreasen
NM Laird
P Diggle
PM Grant
PS Jensen
RE Drake
RS Keefe
S Rosenberg
SL Sayers
T Greenhalgh
T Wykes
WM Trochim
WM Trochim
WMK Trochim
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 30/09/2015
Field of study

BACKGROUND: Schizophrenia leads to profound disability in everyday functioning (e.g., difficulty finding and maintaining employment, housing, and personal relationships). Medications can effectively reduce positive symptoms (e.g., hallucinations and delusions), but they do not meaningfully improve daily life functioning. Psychosocial evidence-based practices (EBPs) improve functioning, but these EBPs are not available to most people with schizophrenia. The field must close the research and service delivery gap by adapting EBPs for schizophrenia to facilitate widespread implementation in community settings. Our hybrid effectiveness and implementation study represents an initiative to bridge this divide. In this study we will test whether an existing EBP (i.e., Cognitive Behavioral Social Skills Training (CBSST)) modified to work in practice settings (i.e., Assertive Community Treatment (ACT) teams) commonly available to persons with schizophrenia results in better consumer outcomes. We will also identify key factors relevant to developing future CBSST implementation strategies. METHODS/DESIGN: For the effectiveness study component, persons with schizophrenia will be recruited from existing publicly funded ACT teams operating in community settings. Participants will be randomized to one of the 2 treatments (ACT alone or ACT + Adapted CBSST) and followed longitudinally for 18 months with assessments every 18 weeks after baseline (5 in total). The primary outcome domain is psychosocial functioning (e.g., everyday living skills and activities related to employment, education, and housing) as measured by self-report, testing, and observation. Additional outcome domains of interest include mediators of change in functioning, symptoms, and quality of services. Primary analyses will be conducted using linear mixed-effects models for continuous data. The implementation study component consists of a structured, mixed qualitative-quantitative methodology (i.e., Concept Mapping) to characterize and assess the implementation experience from multiple stakeholder perspectives in order to inform future implementation initiatives. DISCUSSION: Adapting CBSST to fit into the ACT service delivery context found throughout the United States creates an opportunity to substantially increase the number of persons with schizophrenia who could have access to and benefit from EBPs. As part of the implementation learning process training materials and treatment workbooks have been revised to promote easier use of CBSST in the context of brief community-based ACT visits. TRIAL REGISTRATION: ClinicalTrials.gov NCT02254733. Date of registration: 25 April 2014

Crossref

PubMed Central

eScholarship - University of California

Analysis of the genetic phylogeny of multifocal prostate cancer identifies multiple independent clonal expansions in neoplastic and morphologically normal prostate tissue.

Author: Adam Butler
Alan Thompson
AM Dworkin
Andrew Futreal
Andrew G Lynch
Andrew Menzies
Anne Y Warren
AY Warren
B Reva
B Tareen
Barbara Kremeyer
Ben Robinson
Cathy Corbishley
CE Barbieri
Charlie E Massie
Christopher Greenman
Christopher Ogden
Christopher S Foster
Christopher Woodhouse
Claire Hardy
Colin S Cooper
CR Leemans
CS Grasso
Cyril Fisher
Dan Berney
Daniel Leongamornlert
Daniel S Brewer
David C Wedge
David E Neal
David Jones
David Nicol
Douglas Easton
DP Slaughter
DR Zerbino
Elizabeth Anderson
Erik Mayer
G Attard
G Nilsen
Gunes Gundem
H Holstege
H Li
Hayley C Whitaker
Hayley J Luxton
J Clark
J Lindberg
J Weischenfeldt
Jeremy Clark
Jon Hinton
Jon Teague
Jonathan Kay
Jorge Zamora
K Ye
Keiran Raine
L Cheng
Laura Mudie
LB Alexandrov
LB Alexandrov
LK Boyd
Lucy Matthews
Lucy Stebbings
Ludmil B Alexandrov
M Andreoiu
M Gerlinger
M Karavitakis
M Kobayashi
M-F Tsai
MA Svensson
Manasa Ramakrishna
Mark Maddison
MF Berger
Michael Fraser
Michael R Stratton
MS Lawrence
Naomi Livni
Nening Dennis
Niedzica Camacho
Nimish C Shah
NR Mucci
NT Gaisa
Olivia Joseph
P Van Loo
Pardeep Kumar
Paul C Boutros
Peter Campbell
Peter Van Loo
PJ Campbell
PJ Campbell
PJ Stephens
Rachel Hurst
Richard Mithen
Robert G Bristow
Rosalind Eeles
S Nik-Zainal
S Nik-Zainal
Sandra Edwards
Sarah O'Meara
Sarah Thomas
SC Baca
Serena Nik-Zainal
Stephen Gamble
Steven Hazell
Stuart McLaren
Sue Merson
Susanna Cooke
Thierry Voet
Tim Dudderidge
Ultan McDermott
Victoria Goody
Vincent Gnanapragasam
X Chang
Zsofia Kote-Jarai
Publication venue: Nat Genet
Publication date: 01/01/2015
Field of study

Genome-wide DNA sequencing was used to decrypt the phylogeny of multiple samples from distinct areas of cancer and morphologically normal tissue taken from the prostates of three men. Mutations were present at high levels in morphologically normal tissue distant from the cancer, reflecting clonal expansions, and the underlying mutational processes at work in morphologically normal tissue were also at work in cancer. Our observations demonstrate the existence of ongoing abnormal mutational processes, consistent with field effects, underlying carcinogenesis. This mechanism gives rise to extensive branching evolution and cancer clone mixing, as exemplified by the coexistence of multiple cancer lineages harboring distinct ERG fusions within a single cancer nodule. Subsets of mutations were shared either by morphologically normal and malignant tissues or between different ERG lineages, indicating earlier or separate clonal cell expansions. Our observations inform on the origin of multifocal disease and have implications for prostate cancer therapy in individual cases

Lirias

Crossref

PubMed Central

eScholarship - University of California

Spiral - Imperial College Digital Repository

The University of Manchester - Institutional Repository

Enlighten

Apollo (Cambridge)

University of East Anglia digital repository

University of St. Andrews - Pure

Effects of pre-operative isolation on postoperative pulmonary complications after elective surgery: an international prospective cohort study

Author: Ababneh H
Abad-Motos A
Abbo O
Abbott T
Abd Elwahab S
Abdelkabir M
Abdelkhalek M
Abdur-Rahman L
Abdur-Rahman L
Abebe M
Aboazamazem H
Abou Chaar MK
Abou Chaar MK
Abouelnagah G
Abozied H
Abu Salhiyeh A
Abu-Ismail L
Abu-Mehsen M
Abukhalaf SA
Abuleil A
Ackermann T
Acquah DK
Adam MEAE
Adamina M
Adamina M
Ademuyiwa A
Ademuyiwa A
Adesanya O
Adisa A
Adisa A
Adolfo Renzi
Afolabi A
Agarwal A
Agarwal G
Agastra E
Agbadebo M
Agbonrofo P
Aguiar S Jr
Aguilera-Arevalo ML
Aguilera-Arevalo ML
Ahmad A
Ahmad S
Ahmed WUR
Aigner F
Akhavizadegan H
Akhbari M
Akililu YB
Akinmade A
Al Ameer A
Al Amri A
Al Balushi Z
Al Maadany F
Al-Manaseer BM
Al-Naggar H
Aladawi O
Alajalen A
Alalawi Y
Alameer E
Alansari AHA
Alawami M
Alawneh Y
Alayan M
Albertsmeier M
Albertsmeier M
Alderazi A
Aldressi W
Alessandra Novi
Alessandro Fiorini
Alexander P
AlFakhri A
Alharthi M
Alhefdhi A
Alkadeeki G
Alkaseek A
Alkhatib A
Almabayev Y
Almeida-Reis R
Almiqlash B
Almoguera J
Almugaddami A
Almulhim AS
Alonso JAM
Alonso MD
Alonso NFP
Alqudah MA
Alrayes B
Alsaadi H
Alser O
Alshaar M
Alshahrani M
Alshareef K
Alshehri A
Alshryda S
Alsibai S
Alsunna Z
Altaf HN
Althumairi A
Althumairi A
Althumairi A
Alvarado CEO
Alyami M
Alzahrani A
Alzaidi TM
Alzate JP
Alzerwi N
Amisi N
Amnaina M
Andrea Tufo
André B
Angeles MA
Antonella Chessa
Antonio Cappiello
Anwer M
Anyanwu LJ
Aqeelah A
Aqil S
Arancibia JAC
Arango MCM
Argus L
Arias C
Arnalsteen L
Arnaud AP
Arnaud AP
Asif M
Assefa M
Atnafu B
Awad S
Ayasra F
Ayasra F
Ayoub A
Ayub B
Azevedo J
Azevedo J
Azevedo P
Aziz A
Aziz DAA
Azmi MAFM
Azmi MAFM
Azzam AY
Bacalbasa N
Badareesh L
Badenes R
Badiani S
Baia C
Bains L
Baiocchi G
Baiocchi G
Bajaj A
Bal P
Balanta-Melo J
Balercia P
Baliarsing L
Ball A
Ballouhey Q
Bankhead-Kendall B
Barillas S
Barker J
Barros AV
Bastion ML
Basu S
Batista S
Bauset JCC
Bayo HL
Behzadi A
Bekele K
Bele U
Bele U
Bellver PP
Ben Amer A
Ben Jouira RA
Benson R
Bergeat D
Bergkvist DJ
Bernal-Sprekelsen JC
Bertrand M
Bescós C
Bezabih YS
Bhanderi S
Bhangu A
Bhangu A
Bhat D
Bhatti AH
Bhende V
Biccard B
Blanco-Colino R
Blanco-Colino R
Boccalatte L
Boccalatte L
Boira MA
Boisson M
Bolatbekova R
Bolger J
Bonci EA
Bonci EA
Borda-Luque G
Borges FC
Bork U
Borowski DW
Botero MV
Bouche PA
Boucher S
Bouhuwaish A
Branquinho R
Brar A
Brar A
Bravo AMM
Bravo AMM
Breen K
Bright T
Brown W
Brunaud L
Brunner SM
Buarque I
Buarque IL
Bucyibaruta G
Bukhari SI
Burgan D
Butyrskii A
Bwala K
Bywater EP
Caiado A
Caicedo L
Cal FB
Calvache AJN
Calvache JA
Campos HGD
Cappeliez S
Cardoso P
Carrera J
Carreras-Castañer A
Caruana E
Catarzi L
Cerovac A
Cerovac A
Chadi S
Chakrabortee S
Chan KH
Chan KH
Chapatwala R
Charbonneau H
Charles S
Chaudhary MH
Chaudhry D
Chaudhry NK
Chebaro A
Cheng JQ
Chew MH
Chiuyari JR
Choong P
Chowdappa RG
Chowdhury S
Christensen P
Chuan A
Chwat C
Clancy C
Claudio Iovino
Coimbra FJF
Colás-Ruiz E
Colmenares YTC
Connelly T
Connor CO
Consorti G
Corella F
Corripio-Sanchez R
Costa LC
Costas-Chavarri A
Costea R
Cox D
Cox D
Creavin B
Crétolle C
Cristina Cerri
Croghan SM
Cukier M
Cukier M
Cullinane C
Cunha MF
Cunha MF
D'Aulerio G
Dajti I
Daniela Rega
Daoud H
Das A
Davis N
Dawson AC
Dawson AC
Dawson BE
De Andrés-Asenjo B
De Cortazar UG
de Dieu HJ
de León LRG
De Simone B
Degefa E
Delibegovic S
Delisau-Puig O
Dell A
Demetrashvili Z
Demetrashvili Z
Demetriades AK
Derilo H
des Déserts MD
Desai A
Deus AC
Dharap S
Dhondt B
Dhufera H
Di Bartolomeo
Di Martino M
Di Saverio S
Dimofte MG
Din NM
Díaz-Feijoo B
Doerner J
Domenech J
Donlon N
Drake T
Draman MR
Drasovean R
Duarte AB
Duarte CL
Dube SK
Duchalais E
Dudi-Venkata N
Duran I
Duro A
Dwaga SE
Dziakova J
Earley H
Eberbach H
Edwards J
Efetov S
Efetov S
Egoroff N
Eiras MAF
Ekenze S
Ekiti I
El-Boghdadly K
El-Hussuna A
Elhadi M
Elhadi M
Elhajdawe F
Elisa Francone
Elliott B
Ellojli I
Emile S
Emile S
Enjuto D
Escudero DG
Escudero MI
Eskander A
Espin-Basany E
Espino PC
Espinosa-Bravo M
Ester Marra
Evans J
Evelyn N
Ezanno AC
Fadzli AN
Fahadullah M
Fahmy M
Fakhradiyev I
Fakhradiyev I
Farfus A
Farik S
Farooq U
Faustin N
Fernandez JD
Fernandez LG
Fernández FS
Fernández-López AJ
Ferrer AP
Figueroa-Casanova R
Filipce V
Filipescu D
Fiore M
Fisseha T
Flamey N
Fleming C
Flexman A
Fluegen G
Flumignan R
Ford S
Forero-Torres A
Fotopoulou C
Fowler A
Francesca Ascari
Francesca Simonelli
Francesco Bianco
Francesco Maria Romano
Francesco Menegon Tasselli
Francesco Selvaggi
Franco Chioffi
Fredon F
Fuentes MA
Fuentes T
Fujimoto Y
Futaba K
Gahwagi M
Gallo G
Ganapathy T
Ganapathy T
Ganly I
Garcia-Adamez J
García LD
García-Montoya OJ
Gaujoux S
Gebreyohanes M
Gempt J
Ghauth S
Ghazwani S
Ghodke R
Ghosh D
Ghosh I
Ghozy S
Ghunaim M
Giacomo Ruffo
Gialamas E
Gianpaolo Marte
Gil-Sala D
Ginghina O
Giordana D'Aloisio
Girard E
Girard N
Giulia Bagaglini
Giuliano Barugola
Gjata A
Glasbey JC
Glasbey JC
Glowka TR
Gohar M
Golet MR
Gomes GMA
Gomez JTC
Gomez-Fernandez H
Gomez-Rosado JC
Gonzalez DS
Gonzalez SV
González JS
González-Gimeno MJ
González-Suárez S
Gourlay R
Gousias K
Gouvas N
Gouvas N
Gómez ME
Grama F
Griffiths E
Gronchi A
Groot G
Gross J
Guido Coretti
Guido Sciaudone
Guillen JRO
Gujjuri RR
Gulla A
Gunarasa Y
Gunarasa Y
Gupta A
Gupta R
Gurumeta AA
Gut AE
Ha J
Habumuremyi S
Hadzibegovic AD
Haidar H
Haider F
Hailu S
Hailu S
Hakami I
Hamad FRB
Hamdan KH
Hamdun IHS
Hameed BMZ
Haran C
Harper L
Harrison EM
Harun MHN
Hashimoto D
Hassan RA
Hayati F
Hayati F
Hecker A
Herald Nikaj
Heredia F
Heriot A
Hervieux E
Herzberg J
Hilmi A
Hirschburger M
Hodgson R
Hollington P
Horch RE
Horisberger K
Hossain K
Höhn P
Huang A
Hung WP
Husain S
Hutchinson P
Hyman GY
Ibrahim MR
Ikele H
Imanishimwe A
Imran FH
Incorvia J
Infante AR
Ingabire JA
Ionescu S
Isik A
Iskander O
Jain K
Jain R
Jamal M
Jamaris S
James HG
Javadpour M
Javed S
Jaworska N
Jayarajah U
Jeandel C
Jenkinson M
Jimaale EAM
Jimenez PMA
Jimenez R
Jimenez V
Jiménez PMA
Jin-Young J
Jira M
Jlassi H
Johan S
Johan S
Jones CS
Jonker P
Jouffret L
Kaafarani H
Kabir SMU
Kache S
Kacimi SEO
Kaidarova D
Kaiser JC
Kaman L
Kamarajah SK
Kamphues C
Kandevani NY
Kannaiyan L
Kannan R
Karout L
Karthigeyan M
Kassir R
Kauppila JH
Kauppila JH
Kavalaka A
Keatley JM
Kembuan G
Keppler AM
Keppler L
Kerawala AA
Khalifa H
Khamees A
Khan T
Khokhar MI
Khosravi MH
Kieser D
King J
Kirov M
Klat J
Knight SR
Kochetkov V
Koh C
Koh F
Koh F
Koh PS
Kolias A
Komen N
Konate I
Konrads C
Kopetskyi S
Kopjar T
Kosir JA
Kosir JA
Kowalski LP
Königsrainer A
Kpangon C
Krishnasamy S
Kronberger E
Kronberger IE
Kroon HM
Kruijff S
Kruijff S
Kudsk-Iversen S
Kulimbet M
Kulkarni A
Kumar A
Kumar A
Kuroda N
Kwan TY
Laban S
Lakkis Z
Landaluce-Olavarria A
Latif H
Lau LFR
Laudani V
Laura Enrica Benedetti
Laura SG
Lawal TA
Lawani I
Lawday S
Le Bian AZ
Lederhuber H
Lee YS
Lekuya HM
Leung E
Leventoglu S
Li E
Li E
Lidder S
Liew YT
Lim HC
Lim JZ
Lim RCS
Lincango-Naranjo E
Lincango-Naranjo E
Lindert J
Linz VC
Litvin A
Litvin A
Loaloa MR
Lohsiriwat V
Losada M
Lott N
Lou W
Lowey M
López AS
López CB
Löffler M
Löffler MW
Luca Campagnaro
Lucchini SM
Lucio Selvaggi
Lule H
Luna J
Mabood W
Macchiavello R
MacKenzie S
Madabhavi I
Madkhali T
Mah JJ
Mah JJ
Mahakalkar C
Maimbo M
Maji S
Majid HJ
Major P
Major P
Makdissi F
Makkai-Popa ST
Maldonado-Marcos E
Maleki ER
Malik MU
Manceau G
Mann H
Marçal A
Maria Paola Menna
Mariapan K
Mariapan K
Mariño LP
Mario Pannullo
Marquez L
Marson EJ
Martiínez MJ
Martin J
Martin J
Martinez ED
Martinez L
Martín MTF
Martín-Láez R
Martínez DF
Martínez MR
Mashbari H
Mashbari H
Massoud JG
Matai A
Mateo-Sierra O
Maurizio Ferrari
Mayol J
Mazingi D
McDonnell B
McGuinness MJ
McIntosh N
McKay S
Mclean KA
McNestry C
Meara JG
Meelad A
Mege D
Megersa A
Mehraj A
Mejía D
Melendez RM
Melero AV
Melo MR
Mendes F
Mendiola G
Mendoza VA
Mengesha MG
Mengesha MG
Mersich T
Metallidis S
Migliorelli F
Mihanovic J
Mihanovic J
Milan PB
Mills E
Mimica X
Mironescu A
Mishra T
Misra S
Misrai V
Mittal R
Mitul AR
Modabber A
Modolo MM
Modolo MM
Mohammed AAK
Mohan H
Mohsen MA
Mohyieldin O
Molitvin Y
Montenegro E
Montferrer N
Morales-Puebla JM
Morsy A
Moss JL
Mostafa B
Motas N
Moug S
Moya-Angeler J
Mozafari M
Mozel M
Mozo AS
Msherghi A
Muheilan M
Muniandy M
Muniandy M
Munyaneza E
Munyika A
Muralidharan V
Mustapha M
Muthkumaran G
Muthu S
Nabil S
Naffi AA
Nagar M
Nah SA
Nair AK
Nakagawa S
Nappi F
Naseem MY
Nashidengo PR
Nashidengo PR
Nayen A
Nazimi AJ
Ncogoza I
Ndayishyigikiye MD
Ndong A
Ndong A
Negoi I
Negoi I
Negussie A
Nepogodiev D
Nepogodiev D
Nessim C
Neto JPD
Ng DSW
Ng-Kamstra J
Ngu J
Niazi SU
Nidaw M
Nikolaieva K
Niquen-Jimenez M
Nitschke C
Nkembi AS
Nogueiro J
Noltes M
Noltes M
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Publication venue: Wiley
Publication date: 01/01/2021
Field of study

We aimed to determine the impact of pre-operative isolation on postoperative pulmonary complications after elective surgery during the global SARS-CoV-2 pandemic. We performed an international prospective cohort study including patients undergoing elective surgery in October 2020. Isolation was defined as the period before surgery during which patients did not leave their house or receive visitors from outside their household. The primary outcome was postoperative pulmonary complications, adjusted in multivariable models for measured confounders. Pre-defined sub-group analyses were performed for the primary outcome. A total of 96,454 patients from 114 countries were included and overall, 26,948 (27.9%) patients isolated before surgery. Postoperative pulmonary complications were recorded in 1947 (2.0%) patients of which 227 (11.7%) were associated with SARS-CoV-2 infection. Patients who isolated pre-operatively were older, had more respiratory comorbidities and were more commonly from areas of high SARS-CoV-2 incidence and high-income countries. Although the overall rates of postoperative pulmonary complications were similar in those that isolated and those that did not (2.1% vs 2.0%, respectively), isolation was associated with higher rates of postoperative pulmonary complications after adjustment (adjusted OR 1.20, 95%CI 1.05-1.36, p = 0.005). Sensitivity analyses revealed no further differences when patients were categorised by: pre-operative testing; use of COVID-19-free pathways; or community SARS-CoV-2 prevalence. The rate of postoperative pulmonary complications increased with periods of isolation longer than 3 days, with an OR (95%CI) at 4-7 days or ≥ 8 days of 1.25 (1.04-1.48), p = 0.015 and 1.31 (1.11-1.55), p = 0.001, respectively. Isolation before elective surgery might be associated with a small but clinically important increased risk of postoperative pulmonary complications. Longer periods of isolation showed no reduction in the risk of postoperative pulmonary complications. These findings have significant implications for global provision of elective surgical care

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Intellectum (Universidad de La Sabana)

Search for dark matter produced in association with a Higgs boson decaying to a pair of bottom quarks in proton-proton collisions at root s=13TeV

Author: Aarrestad TK
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Wu Z
Wuchterl S
Wulz C-E
Wuyckens S
Wyslouch B
Würthwein F
Xia F
Xiao J
Xiao M
Xiao R
Xie S
Xie W
Yagil A
Yalvac M
Yan F
Yang UK
Yang YC
Yao Y
Yarar H
Yates BR
Yazgan E
Yetkin EA
Yi K
Yohay R
Yoo HD
Yoo J
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You Z
Yu D
Yu GB
Yu I
Yu SS
Yuan L
Yuan S
Yumiceva F
Yusli MN
Yzquierdo AP-C
Zabi A
Zacharopoulou A
Zahid S
Zaleski S
Zalewski P
Zanetti M
Zarubin A
Zarucki M
Zecchinelli AG
Zenaiev O
Zeuner WD
Zghiche A
Zhang F
Zhang H
Zhang J
Zhang S
Zhang W
Zhang Y
Zhang Z
Zhao J
Zhizhin I
Zhokin A
Zhu DH
Zhu RY
Ziemons T
Zientek M
Zlebcik R
Zobec J
Zoi I
Zolkapli Z
Zorbakir IS
Zorbilmez C
Zotto P
Zou D
Zucchetta A
Zumerle G
Zuo X
Zuolo D
Zygala L
Álvarez CR
Özçelik Ö
Publication venue
Publication date: 01/01/2018
Field of study

A search for dark matter produced in association with a Higgs boson decaying to a pair of bottom quarks is performed in proton-proton collisions at a center-of-mass energy of 13 TeV collected with the CMS detector at the LHC. The analyzed data sample corresponds to an integrated luminosity of 35.9 fb(-1). The signal is characterized by a large missing transverse momentum recoiling against a bottom quark-antiquark system that has a large Lorentz boost. The number of events observed in the data is consistent with the standard model background prediction. Results are interpreted in terms of limits both on parameters of the type-2 two-Higgs doublet model extended by an additional light pseudoscalar boson a (2HDM+a) and on parameters of a baryonic Z simplified model. The 2HDM+a model is tested experimentally for the first time. For the baryonic Z model, the presented results constitute the most stringent constraints to date.Peer reviewe

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Search for Higgs Boson Pair Production in the Four b Quark Final State in Proton-Proton Collisions at root s=13 TeV

Author: Aarrestad T
Abbaneo D
Abbiendi G
Abbrescia M
Abdullah WW
Abdullin S
Abercrombie D
Abreu A
Acharya H
Acosta D
Adam W
Adamidis K
Adams E
Adams M
Adams T
Addesa F
Adloff C
Adzic P
Adán DP
Afanasiev S
Agapitos A
Agarwal G
Aggleton R
Agram J
Aguilar-Benitez M
Ahmad A
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Ahmad WH
Ahmed A
Ahuja S
Aime` C
Akchurin N
Akgun B
Akpinar A
Albergo S
Albert A
Albrecht S
Albrow M
Aleksandrov A
Alexander J
Alhusseini M
Alimena J
Alison J
Almond J
Alonso AG
Alpana K
Alvarez JR
Alverson G
Alves G
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Amaral SSD
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Ambrozas M
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Amin N
Amram O
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Álvarez CR
Özçelik Ö
Publication venue
Publication date: 01/01/2022
Field of study

ePubs: the open archive for STFC research publications

Pan-cancer analysis of whole genomes

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The ICGC/TCGA Pan-Cancer Analysis of Whole Genomes Consortium View Correspondence (jump link)
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Publication venue
Publication date: 11/12/2019
Field of study

Cancer is driven by genetic change, and the advent of massively parallel sequencing has enabled systematic documentation of this variation at the whole-genome scale(1-3). Here we report the integrative analysis of 2,658 whole-cancer genomes and their matching normal tissues across 38 tumour types from the Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium of the International Cancer Genome Consortium (ICGC) and The Cancer Genome Atlas (TCGA). We describe the generation of the PCAWG resource, facilitated by international data sharing using compute clouds. On average, cancer genomes contained 4-5 driver mutations when combining coding and non-coding genomic elements; however, in around 5% of cases no drivers were identified, suggesting that cancer driver discovery is not yet complete. Chromothripsis, in which many clustered structural variants arise in a single catastrophic event, is frequently an early event in tumour evolution; in acral melanoma, for example, these events precede most somatic point mutations and affect several cancer-associated genes simultaneously. Cancers with abnormal telomere maintenance often originate from tissues with low replicative activity and show several mechanisms of preventing telomere attrition to critical levels. Common and rare germline variants affect patterns of somatic mutation, including point mutations, structural variants and somatic retrotransposition. A collection of papers from the PCAWG Consortium describes non-coding mutations that drive cancer beyond those in the TERT promoter(4); identifies new signatures of mutational processes that cause base substitutions, small insertions and deletions and structural variation(5,6); analyses timings and patterns of tumour evolution(7); describes the diverse transcriptional consequences of somatic mutation on splicing, expression levels, fusion genes and promoter activity(8,9); and evaluates a range of more-specialized features of cancer genomes(8,10-18).Peer reviewe

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