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Singlet exciton fission in solution.

Author: A Dreuw
A Rao
AM Müller
AM Müller
Andrew J. Musser
B Ehrler
B Ehrler
Brian J. Walker
C Jundt
C Ramanan
C Wang
CC Gradinaru
CD Sheraw
CE Swenberg
D Beljonne
David Beljonne
DJ Gundlach
EC Greyson
G Giri
I Paci
JC Johnson
JJ Burdett
JJ Burdett
K Schulten
MB Smith
MB Smith
MC Hanna
MR Vilar
MWB Wilson
N Geacintov
N Renaud
NA Azarova
OG Berg
PA Van Hal
PJ Jadhav
PM Zimmerman
PM Zimmerman
PM Zimmerman
RE Merrifield
RE Merrifield
Richard H. Friend
S Ito
S Singh
SCB Mannsfeld
ST Roberts
TC Berkelbach
W Barford
W Chan
W Shockley
W-L Chan
W-L Chan
Publication venue: Nat Chem
Publication date: 17/11/2013
Field of study

Singlet exciton fission, the spin-conserving process that produces two triplet excited states from one photoexcited singlet state, is a means to circumvent the Shockley-Queisser limit in single-junction solar cells. Although the process through which singlet fission occurs is not well characterized, some local order is thought to be necessary for intermolecular coupling. Here, we report a triplet yield of 200% and triplet formation rates approaching the diffusion limit in solutions of bis(triisopropylsilylethynyl (TIPS)) pentacene. We observe a transient bound excimer intermediate, formed by the collision of one photoexcited and one ground-state TIPS-pentacene molecule. The intermediate breaks up when the two triplets separate to each TIPS-pentacene molecule. This efficient system is a model for future singlet-fission materials and for disordered device components that produce cascades of excited states from sunlight.B.J.W. was supported by a Herchel Smith Research Fellowship. A.J.M. received funding from a Marie Curie Scholarship. D.B. is a FNRS Research Director. Both A.J.M and D.B. acknowledge support from the European Community’s Initial Training Network SUPERIOR (PITN-GA-2009-238177). Further funding for this project came from the Engineering and Physical Sciences Research Council (EPSRC) and a pump-prime grant from the Winton Programme for the Physics of Sustainability.This is the accepted version of an article originally published in Nature Chemistry 5, 1019–1024 and available online at http://www.nature.com/nchem/journal/v5/n12/full/nchem.1801.html. Nature Publishing Group's conditions for reuse are detailed at http://www.nature.com/authors/policies/license.html

HAL - Université de Franche-Comté

Apollo (Cambridge)

N-glycosylation of mouse TRAIL-R and human TRAIL-R1 enhances TRAIL-induced death.

APO2L/TRAIL (TNF-related apoptosis-inducing ligand) induces death of tumor cells through two agonist receptors, TRAIL-R1 and TRAIL-R2. We demonstrate here that N-linked glycosylation (N-glyc) plays also an important regulatory role for TRAIL-R1-mediated and mouse TRAIL receptor (mTRAIL-R)-mediated apoptosis, but not for TRAIL-R2, which is devoid of N-glycans. Cells expressing N-glyc-defective mutants of TRAIL-R1 and mouse TRAIL-R were less sensitive to TRAIL than their wild-type counterparts. Defective apoptotic signaling by N-glyc-deficient TRAIL receptors was associated with lower TRAIL receptor aggregation and reduced DISC formation, but not with reduced TRAIL-binding affinity. Our results also indicate that TRAIL receptor N-glyc impacts immune evasion strategies. The cytomegalovirus (CMV) UL141 protein, which restricts cell-surface expression of human TRAIL death receptors, binds with significant higher affinity TRAIL-R1 lacking N-glyc, suggesting that this sugar modification may have evolved as a counterstrategy to prevent receptor inhibition by UL141. Altogether our findings demonstrate that N-glyc of TRAIL-R1 promotes TRAIL signaling and restricts virus-mediated inhibition

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Oskar Bordeaux

An apicobasal gradient of Rac activity determines protrusion form and position

Author: A Hutterer
A Rolo
A Wodarz
AJ Ridley
AJ Ridley
AJ Ridley
AM Rajnicek
B Baum
C De Joussineau
CD Nobes
D Bilder
D Bilder
E Assemat
E Kardash
E Marinari
E Walck-Shannon
F Demontis
F Hsiung
G Venugopala Reddy
H Gon
H Zhang
J Betschinger
J Betschinger
JS King
KG Campellone
M Bischoff
M Cohen
M Georgiou
M Georgiou
MA Chesarone
NA Grzeschik
NA Mack
NA Mack
O Renaud
P Lo
RE Itoh
S Yagi
S Zaessinger
Sagar
SL Gupton
T Gomez del Pulgar
T Lee
T Nishimura
T Xu
U Tepass
W Yu
X Chen
X Wang
YC Wang
YI Wu
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 19/05/2017
Field of study

Each cell within a polarised epithelial sheet must align and correctly position a wide range of subcellular structures, including actin-based dynamic protrusions. Using in vivo inducible transgenes that can sense or modify Rac activity, we demonstrate an apicobasal gradient of Rac activity that is required to correctly form and position distinct classes of dynamic protrusion along the apicobasal axis of the cell. We show that we can modify the Rac activity gradient in genetic mutants for specific polarity proteins, with consequent changes in protrusion form and position and additionally show, using photoactivatable Rac transgenes, that it is the level of Rac activity that determines protrusion form. Thus, we demonstrate a mechanism by which polarity proteins can spatially regulate Rac activity and the actin cytoskeleton to ensure correct epithelial cell shape and prevent epithelial-to-mesenchymal transitions

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Is the meiofauna a good indicator for climate change and anthropogenic impacts?

Author: A Ahnert
A Borja
A Carpentier
A Forchino
A Guerrini
A Mazzola
A McIntyre-Wressnig
A Piot
A Pusceddu
A Pusceddu
A Pusceddu
A Pusceddu
A Rose
AA Cook
AD Kennedy
AH Parulekar
AJ Gooday
AJ Gooday
AJ Gooday
AJ Gooday
AJ Gooday
AJ Radwell
Alexandre Arvigo
Andrew J. Gooday
Ann Vanreusel
Antoine Rio-Cabello
AP Covich
AR Thurber
AW Decho
AWG Wurff van der
B Buchardt
B Freedman
B Górska
B Lebreton
BC Coull
BC Coull
BD Wigham
BE Hopper
BK Sen Gupta
BR Kuipers
BS Ingole
BS Ingole
BT Hentschel
C Alsterberg
C Bussau
C Bussau
C Colen Van
C Fontanier
C Heip
C Lizhe
C Mora
C Neira
C Neira
C Schmidt
C Vinagre
C Woulds
CD Levings
CE Richmond
Christophe Fontanier
CM Duarte
CM Jessup
CR Smith
CT Schafer
D Danovaro
D Gwyther
D Leduc
D Leduc
D Thistle
D Thistle
D Thistle
D Thistle
D Zeppilli
D Zeppilli
Daniel Leduc
Daniela Zeppilli
David Fernandes
Dendy Mahabror
DG Raffaelli
Diego Fontaneto
DK Alexeev
DL Angel
DM Miljutin
DOB Jones
DP Edwards
DT Rudnick
DU Hooper
E Alve
E Alve
E Armynot du Châtelet
E Baldrighi
E Buffan-Dubau
E Gontikaki
E Mahmoudi
E Olafsson
E Piña-Ochoa
E Piña-Ochoa
EJ Barron
EJ O’Gorman
ER Ricketts
Etienne Pouplard
F Pranovi
F Riemann
F Ruiz
F Ruiz
FB Phleger
Fenchel
FJ Jorissen
FJA Nascimento
FJA Nascimento
G Pergent
G Tita
G Veit-Köhler
G Vranken
G Vranken
G Woodward
GAP Santos Dos
GI Shapiro
GM Sheills
Gwendoline Traisnel
H Beyrem
H Ek
H Hinz
H Kurihara
H Modig
H Nomaki
H Nomaki
H Nomaki
H Nomaki
H Nomaki
H Nomaki
H Thiel
H Thiel
H Tomimatsu
H Torres-Pratts
HK Talge
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HM Bik
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IPCC
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J Gutt
J Gwyther
J Ingels
J Ingels
J Ingels
J Mallon
J Pawlowski
J Renaud-Mornant
J Schönfeld
J Turner
J Vanaverbeke
J Veillette
J Veillette
J Vidović
JBC Jackson
JG Baguley
JJ Helly
JJ Lee
JM Bernhard
JM Bernhard
JM Bernhard
JM Bernhard
JM Gee
JM Guinotte
JM Wȩsławski
Jozée Sarrazin
JP Barry
JP Barry
JS Bradshaw
Julien Thébault
Justine Castrec
JW Fleeger
JW Fleeger
JW Murray
K Grzelak
K Vopel
K Vopel
K Worsaae
KA Koho
Kevin Urvoy
KR Carman
L Ferraro
L Stramma
L Stramma
L Teuber
L Würzberg
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LA Levin
LA Levin
Laura Raimondeau
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Ludovic Hermabessiere
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M Balsamo
M Bampton
M Collins
M Curini-Galletti
M Edwards
M Gallitelli
M Grego
M Grego
M Jochum
M Kramer
M Loreau
M Mojtahid
M Raes
M Schratzberger
M Schratzberger
M Schratzberger
M Schratzberger
M Schratzberger
M Schratzberger
M Troch De
M Woombs
M Woombs
M Yasuhara
M Yasuhara
M Yasuhara
MA Green
MA Mateo
MA Miljutina
MA Miljutina
MA Rex
MA Rudd
MA Wetzel
MA Wetzel
Marc Long
Mariam Weyand
Marianna Mea
Martin V. Sørensen
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MC Murrell
Michael Pantalos
MJ Kaiser
ML Mahaut
Morgan Danielo
MV Sørensen
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O Giere
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P Jensen
P Riera
P Vassallo
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PE Renaud
Pedro Martinez Arbizu
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PJ Somerfield
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PJD Lambshead
Quentin Morel
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R Danovaro
R Danovaro
R Danovaro
R Engler
R Garcia
R Gingold
R Hale
R Harvey
R Howell
R Huys
R Riera
R Riera
R Sandulli
R Singh
Raphaelle Fumeron
RC Aller
Reinhardt Møbjerg Kristensen
RIE Newell
RJ Matear
RL Diaz
RM Warwick
RM Warwick
RM Warwick
RM Warwick
RM Warwick
RM Warwick
RN Arieli
Roxanne Langonne-Augen
RR Hessler
S Amjad
S Bonaglia
S Gollasch
S Gollasch
S Jennings
S Laakmann
S Mirto
S Mirto
S Oron
S Somot
S Wang
S Widdicombe
SA Gerlach
SA Gerlach
SA Gerlach
SA Netto
Sarah Seite
SC Doney
SC Doney
SG Bolam
SI Rogers
SJ Forster
SL Dashfield
SM Burton
SR Ernst
T Bongers
T Irizuki
T Kang
T Mascart
T Mascart
T Moens
T Radziejewska
T Radziejewska
T Wernberg
T Yamanaka
TA Scambos
Tangi Le Bot
TF Sutherland
Thomas Andro
Thomas Van Der Stegen
TK Gyedu-Ababio
TK Gyedu-Ababio
TK Pinto
Tristan James
U Braeckman
V Bouchet
V Cadre Le
Valentin Foulon
VB Pogrebov
VG Fonseca
Viatcheslav N. Ivanenko
Vivien Hulot
VMP Bouchet
VV Galtsova
WP Sijp
WS Liu
WS Liu
X Sun
XQ Ngo
ZA Ansari
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2015
Field of study

Our planet is changing, and one of the most pressing challenges facing the scientific community revolves around understanding how ecological communities respond to global changes. From coastal to deep-sea ecosystems, ecologists are exploring new areas of research to find model organisms that help predict the future of life on our planet. Among the different categories of organisms, meiofauna offer several advantages for the study of marine benthic ecosystems. This paper reviews the advances in the study of meiofauna with regard to climate change and anthropogenic impacts. Four taxonomic groups are valuable for predicting global changes: foraminifers (especially calcareous forms), nematodes, copepods and ostracods. Environmental variables are fundamental in the interpretation of meiofaunal patterns and multistressor experiments are more informative than single stressor ones, revealing complex ecological and biological interactions. Global change has a general negative effect on meiofauna, with important consequences on benthic food webs. However, some meiofaunal species can be favoured by the extreme conditions induced by global change, as they can exhibit remarkable physiological adaptations. This review highlights the need to incorporate studies on taxonomy, genetics and function of meiofaunal taxa into global change impact research

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Multi-messenger observations of a binary neutron star merger

Author: Aab A
Aartsen MG
Abbott BP
Abbott R
Abbott TD
Abbott TMC
Abdalla H
Abe F
Abeysekara AU
Abramo LR
Abramowski A
Abreu P
Acernese F
Acero F
Ackermann M
Ackley K
Ackley K
Adams C
Adams J
Adams SM
Adams T
Addesso P
Adhikari RX
Adya VB
Affeldt C
Afrough M
Agarwal B
Agathos M
Agatsuma K
Aggarwal N
Aglietta M
Agliozzo C
Agudo I
Aguiar OD
Aguilar JA
Aharonian F
Ahlers M
Ahrens M
Aiello L
Ain A
Ajith P
Akras S
Al Samarai I
Albert A
Albert A
Albuquerque IFM
Albury JM
Alcaniz JS
Alexander KD
Alfaro R
Alighieri S Di Serego
Allam S
Allekotte I
Allen B
Allen G
Allison J
Allison JR
Allocca A
Almela A
Altin PA
Altmann D
Alvarez C
Alvarez JD
Alvarez M Dovale
Alvarez-Muiz J
Amati L
Amato A
An T
Ananyeva A
Anastasi GA
Anchordoqui L
Andeen K
Anderson JP
Anderson SB
Anderson T
Anderson WG
Andrada B
Andre M
Andreoni I
Andreoni I
Andringa S
Angelova SV
Anghinolfi M
Angner EO
Angus CR
Annis J
Ansseau I
Antier S
Anton G
Antonelli LA
Antonelli LA
Anupama GC
Aoki K
Aoki W
Appert S
Aptekar RL
Arai K
Arakawa M
Aramo C
Araya MC
Arcavi I
Arceo R
Ardid M
Areeda JS
Aresu G
Argan A
Argelles C
Arnaud N
Array LWA Long Wavelength
Array MWA Murchison Widefield
Arrieta M
Arsene N
Arteaga-Velzquez JC
Artola R
Arun KG
Asakura Y
Asaoka Y
Ascenzi S
Ashall C
Ashley MCB
Ashton G
Asorey H
Assis P
Ast M
Aston SM
Astone P
Atallah DV
ATLAS
Atwood WB
Aubert J-J
Aubert P
Aublin J
Auffenberg J
Aufmuth P
Aulbert C
AultONeal K
Austin C
Avgitas T
Avila G
Avila-Alvarez A
Awad A Kuotb
Axani S
Baar S
Babak S
Bachetti M
Backes M
Bacon P
Bader MKM
Badescu AM
Bae S
Bagherpour H
Bai X
Bailes M
Baker PT
Balaceanu A
Balanutsa PV
Balasubramanian A
Balbinot E
Baldaccini F
Baldini L
Ballardin G
Ballmer SW
Bally J
Balzer A
Banagiri S
Banerji M
Bannister KW
Barayoga JC
Barbarino C
Barbato F
Barber AS
Barbiellini G
Barbiellini G
Barclay SE
Baret B
Barish BC
Barker D
Barkett K
Barnard M
Barnes J
Barone F
Barr B
Barrios-Marti J
Barron JP
Barsotti L
Barsuglia M
Barta D
Barthelmy SD
Bartlett J
Bartos I
Barway S
Barway S
Barwick SW
Basa S
Bassiri R
Basti A
Bastieri D
Batch JC
Bauer FE
Bauer FE
Baum V
Bawaj M
Bay R
Bayley JC
Bazzan M
Bazzano A
Bchele M
Beardmore AP
Beardsley A
Beatty JJ
Becerril A
Becherini Y
Bechtol K
Becker KH
Becsy B
Beer C
Bejger M
Belahcene I
Belhorma B
Bell AS
Bellazzini R
Bellido JA
Bellm E
Belmont-Moreno E
Benetti S
Benkhali F Ait
Benoit-Levy A
BenZvi SY
Berat C
Berenji B
Berge D
Berger BK
Berger E
Bergmann G
Berisso M Gomez
Berley D
Bernal A
Bernardini E
Bernardini MG
Bernhard S
Bernrhr K
Bero JJ
Beroiz M
Berry CPL
Bersanetti D
Bertaina ME
Bertin E
Bertin V
Bertolini A
Berton M
Bertou X
Bessell MS
Besson DZ
Beswick R
Betzwieser J
Bhagwat S
Bhalerao V
Bhandare R
Bhattacharya D
Biagi S
Biermann PL
Bilenko IA
Billingsley G
Billman CR
Binder G
Bindig D
Birch J
Birney R
Birnholtz O
Biscans S
Biscoveanu S
Bisht A
Bissaldi E
Bissaldi E
Biteau J
Bitossi M
Biwer C
Bizouard MA
Blackburn JK
Blackburn L
Blackman J
Blackwell R
Blaess SG
Blagorodnova N
Blair CD
Blair DG
Blair RM
Blanchard P
Blanco A
Bland PA
Blandford RD
Blaufuss E
Blazek J
Bleve C
Bloemen S
Bloom ED
Blot S
Bock O
Bode N
Boer M
Bogaert G
Bohacova M
Bohe A
Bohm C
Boisson C
Bolmont J
Bond IA
Bondu F
Bonifazi C
Bonilla E
Bonino R
Bonnand R
Bonnefoy S
Bonoli S
Booler T
Boom BA
Bordas P
Bork R
Bormuth R
Borner M
Borodai N
Bos F
Boschi V
Bose D
Bose S
Boser S
Bossie K
Botner O
Bottacini E
Bottcher M
Botti AM
Botticella MT
Bouffanais Y
Bourbeau E
Bourbeau J
Bourret S
Bouwhuis MC
Bozzi A
Bozzo E
Brack J
Bradaschia C
Bradascio F
Brady PR
Branchesi M
Brancus I
Brandt S
Brau JE
Braun J
Braun J
Bravo O Martinez
Brayeur L
Breeveld AA
Bregeon J
Bregeon J
Brenzke M
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Briant T
Bridgeman A
Briechle FL
Briggs MS
Brillet A
Brinkmann M
Brisbois C
Brisson V
Brnzas H
Brocato E
Brockill P
Broderick JW
Broida JE
Bron S
Brooks AF
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Brostean-Kaiser J
Brout D
Brown DA
Brown DD
Brown IS
Bruijn R
Brun F
Brun P
Brunett S
Brunner J
Bruun SH
Bryan M
Buchanan CC
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Buckley DAH
Buckley-Geer E
Budnev NM
Buehler R
Bueno A
Bufano F
Buffa F
Buikema A
Buitink S
Bulgarelli A
Bulger J
Bulik T
Bulik T
Bulla M
Bulten HJ
Buonanno A
Burgay M
Burgess JM
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Burhonov O
Burke DL
Burns E
Burrows DN
Buscemi M
Buskulic D
Buson S
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Buy C
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Caballero-Garcia MD
Caballero-Mora KS
Caballero-Mora KS
Cabero M
Cabral J
Caccianiga L
Cadonati L
Cagnoli G
Cahillane C
Callister TA
Calloni E
CALTECH GROWTH JAGWAR
Cameron RA
Camilo F
Camp JB
Campana S
Camuccio R
Cancio A
Canepa M
Canfora F
Canizares P
Cannella C
Cannizzaro G
Cannon KC
Cano Z
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Cao J
Cao XL
Capaccioli M
Capano CD
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Capozzi D
Cappellaro E
Caputo R
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Caraveo P
Caraveo PA
Carbognani F
Carboni G
Cardenas B Vargas
Cardillo M
Caria T
Caride S
Carlin JL
Carney MF
Caroff S
Carosi A
Carr J
Carramiana A
Carretti E
Cartier R
Caruso R
Carver T
Casadio C
Casado A Lopez
Casanova S
Casanova S
Casasola V
Casella P
Casentini C
Casey J
Casier M
Castander FJ
Castangia P
Castellina A
Castellon A
Castellon JL Nilo
Castillo J Alvarez
Castillo M
Castro JM Gonzalez
Castro ML Diaz
Castro-Tirado AJ
Casu S
Catalani F
Cataldi G
Cattaneo PW
Caudill S
Cavagli M
Cavalier F
Cavalieri R
Cavazzuti E
Cazon L
Cella G
Celli S
Cenko SB
Cepeda CB
Cerd-Durn P
Ceron JM Castro
Cerretani G
Cerruti M
Cerutti AC Cobos
Cesarini E
Chakraborty N
Chamberlin SJ
Chambers KC
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Chandra P
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Chang Z
Chao S
Charlton P
Chase E
Chassande-Mottin E
Chatterjee D
Chatterjee D
Chatziioannou K
Chaves RCG
Chavez AG
Chavushyan V
Cheeseboro BD
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Chiarusi T
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Chiummo A
Chmiel T
Cho HS
Cho M
Choi C
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Chornock R
Chow JH
Christensen N
Christov A
Chu Q
Chua AJK
Chua S
Chudoba J
Chung AKW
Chung S
Ciani G
Cikota A
Ciolfi R
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Circella M
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Clark JA
Clark K
Clark P
Clarke TE
Classen L
Clay RW
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Cleva F
Cleveland WH
Cline T
Cobb BE
Cocchieri C
Coccia E
Coelho JAB
Coelho P
Coenders S
Cohadon P-F
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Colalillo R
Colazo C
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Collette CG
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Collin GH
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Cook DO
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Maoz D
Mapelli M
Marandon V
Marcelin M
March M
Marchesoni F
Marcote B
Marcowith A
Margiotta A
Margutti R
Mariaud C
Mariazzi AG
Marinelli A
Marinelli SS
Marion F
Maris IC
Marisaldi M
Markakis C
Markosyan AS
Markowitz A
Marongiu L
Maros E
Marquina A
Marriner J
Marrocchesi PS
Marsella G
Marsh P
Marshall FE
Marshall JL
Martelli F
Martellini L
Martello D
Martin IW
Martin RM
Martin S
Martin-Carrillo A
Martinez H
Martinez O
Martinez-Castellanos I
Martinez-Castro J
Martinez-Huerta H
Martinez-Mora JA
Martini P
Martynov DV
Maruyama R
Marx R
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Masetti N
Mason K
Massera E
Masserot A
Massinger TJ
Masso-Reid M
Mastrogiovanni S
Matas A
Mate S
Mathes HJ
Matheson T
Mathys S
Matichard F
Matone L
Matsubayashi K
Matsuoka M
Matthews J
Matthews JA
Matthiae G
Mattila S
Maunu R
Maurin G
Mavalvala N
Maxted N
Mayer M
Mayotte E
Mazaeva ED
Mazumder N
Mazur PO
Mazzali PA
Mazzali PA
Mazziotta MN
McBreen S
McBrien O
McCarthy R
McClelland DE
McCormick S
McCuller L
McCully C
McEnery JE
McGuire SC
McIntyre G
McIver J
McMahon RG
McManus DJ
McNally F
McNeill L
Mcrae T
McWilliams ST
Meacher D
Meadors GD
Meagher K
Medici M
Medina C
Medina GE
Medina-Tanco G
Meegan CA
MeerKAT SKA South Africa
Mehmet M
Mehner A
Meidam J
Meier M
Meintjes PJ
Mejuto-Villa E
Melandri A
Melatos A
Mele R
Melia R
Melis A
Melis G
Melis K
Melo D
Menanteau F
Mendell G
Meng B
Menne T
Menshikov A
Mercer RA
Mereghetti S
Merenda K-D
Merilh EL
Merino G
Merzougui M
Meshkov S
Messenger C
Messick C
Metzdorff R
Metzger BD
Meures T
Meyer M
Meyer M
Meyers PM
Meza JJ Masias
Mezek G Kukec
Miao H
Miarecki S
Micallef J
Michael T
Michal S
Michalowski MJ
Michel C
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Michelson PF
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Milano L
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Ming J
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Mirabal N
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Miranda-Romagnoli P
Mishra C
Misra K
Mitchell AMW
Mitra S
Mitrica B
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Mitselmakher G
Mittleman R
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Miyazaki S
Mller A
Mockler D
Moderski R
Moffa D
Moggi A
Mogushi K
Mohamed M
Mohan M
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Mohr JJ
Mohrmann L
Moldon J
Molino A
Moller A
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Mollerach S
Moment G
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Montani M
Montaruli T
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Mooley K
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Mor K
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Moraru D
Morello C
Moreno E
Moreno G
Morihana K
Morita K
Morita T
Morlino G
Morokuma T
Morris D
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Morselli A
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Moskalenko IV
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Mostaf M
Motohara K
Moulai M
Moulin E
Mours B
Moussa A
Mow-Lowry CM
Mrka S
Mrka Z
Mueller AL
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Mueller BB
Mueller G
Mueller G
Mueller MA
Mueller S
Muir AW
Muir J
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Mukherjee D
Mukherjee S
Mukund N
Mullavey A
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Munch J
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Murach T
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Muratore M
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Murphy T
Murray PG
Mussa R
Myers ST
Nagai H
Nagashima H
Nagayama T
Nahnhauer R
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Nakajima M
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Nakaoka T
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Nakata F
Nang Y
Napier K
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Natalucci L
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Naumann U
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Navas S
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Neer G
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Negro M
Neilsen E
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Network DFN Desert Fireball
Neunzert A
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Newbold M
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Newton G
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Ng KKY
Ngeow C-C
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Nicholl M
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Nie JY
Niechciol M
Niederhausen H
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Observat Toros Transient Robotic
Oda S
Odaka H
Ofek EO
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Ogin GH
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Ohm S
Ohme F
Ohsawa R
Ohshima T
Ohta K
Oikonomou F
Ojha R
Okada MA
Okita H
Oleynik Ph P
Olinto A
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Oliver M
Omodei N
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Onori F
Oozeer N
Opiela R
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Organokov M
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Orlati A
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Ortu P
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Ou G
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Plum M
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Poe M
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Poh J
Poireau V
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Prouza M
Prrer M
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Punch M
Puncken O
Punturo M
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Qi H
Qi H
Qu JL
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Quel EJ
Querchfeld S
Querel R
Quetschke V
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Quinn L
Quinn S
Quinones C
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Raab FJ
Raab S
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Rabus M
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Rain S
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Rana J
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Reimer O
Reimer O
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Ren Z
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Reposeur T
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Resmi L
Rest A
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Ribeiro T
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Richman M
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Righini S
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Risse M
Ristori P
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Rizi V
Rizzo M
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Rol E
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Rosa-Gonzlez D
Rosell A Carnero
Rosenberg M
Rosetti S
Rosinska D
Ross MP
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Roth M
Rott C
Roulet E
Rovero AC
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Rowell G
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Roy R
Ruan JJ
Rudak B
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Ruhe T
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Ruiz-Velasco E
Rulten CB
Rumyantsev VV
Rusu F
Rutins G
Ryan K
Rybicki KA
Ryckbosch D
Rykoff ES
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Saba A
Sachdev S
Sadecki T
Sadeghian L
Sadler EM
Sadler EM
Saffe C
Saffi SJ
Saftoiu A
Sahakian V
Sai N
Saito S
Saito T
Saito Y
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Sakamoto T
Sakellariadou M
Sako M
Sako S
Salafia OS
Salamida F
Salazar H
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Sanchez E
Sanchez EJ
Sanchez F
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Sand DJ
Sandberg V
Sanders JR
Sandoval A
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Sapienza P
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Sasaki M
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Schmidt T
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Schneider M
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Scholten O
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Publication venue: 'American Astronomical Society'
Publication date: 01/01/2017
Field of study

On 2017 August 17 a binary neutron star coalescence candidate (later designated GW170817) with merger time 12:41:04 UTC was observed through gravitational waves by the Advanced LIGO and Advanced Virgo detectors. The Fermi Gamma-ray Burst Monitor independently detected a gamma-ray burst (GRB 170817A) with a time delay of ~1.7 s with respect to the merger time. From the gravitational-wave signal, the source was initially localized to a sky region of 31 deg2 at a luminosity distance of 40+8-8 Mpc and with component masses consistent with neutron stars. The component masses were later measured to be in the range 0.86 to 2.26 Mo. An extensive observing campaign was launched across the electromagnetic spectrum leading to the discovery of a bright optical transient (SSS17a, now with the IAU identification of AT 2017gfo) in NGC 4993 (at ~40 Mpc) less than 11 hours after the merger by the One- Meter, Two Hemisphere (1M2H) team using the 1 m Swope Telescope. The optical transient was independently detected by multiple teams within an hour. Subsequent observations targeted the object and its environment. Early ultraviolet observations revealed a blue transient that faded within 48 hours. Optical and infrared observations showed a redward evolution over ~10 days. Following early non-detections, X-ray and radio emission were discovered at the transient’s position ~9 and ~16 days, respectively, after the merger. Both the X-ray and radio emission likely arise from a physical process that is distinct from the one that generates the UV/optical/near-infrared emission. No ultra-high-energy gamma-rays and no neutrino candidates consistent with the source were found in follow-up searches. These observations support the hypothesis that GW170817 was produced by the merger of two neutron stars in NGC4993 followed by a short gamma-ray burst (GRB 170817A) and a kilonova/macronova powered by the radioactive decay of r-process nuclei synthesized in the ejecta

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Searches for Higgs boson pair production in the hh→bbττ, γγWW∗, γγbb, bbbb channels with the ATLAS detector

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Abbott B
Abdallah J
Abdinov O
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Zobernig G
Zoccoli A
Zurzolo G
Zwalinski L
Publication venue: 'American Physical Society (APS)'
Publication date: 01/01/2015
Field of study

Searches for both resonant and nonresonant Higgs boson pair production are performed in the hh→bbττ, γγWW∗ final states using 20.3 fb−1 of pp collision data at a center-of-mass energy of 8 TeV recorded with the ATLAS detector at the Large Hadron Collider. No evidence of their production is observed and 95% confidence-level upper limits on the production cross sections are set. These results are then combined with the published results of the hh→γγbb, bbbb analyses. An upper limit of 0.69 (0.47) pb on the nonresonant hh production is observed (expected), corresponding to 70 (48) times the SM gg→hh cross section. For production via narrow resonances, cross-section limits of hh production from a heavy Higgs boson decay are set as a function of the heavy Higgs boson mass. The observed (expected) limits range from 2.1 (1.1) pb at 260 GeV to 0.011 (0.018) pb at 1000 GeV. These results are interpreted in the context of two simplified scenarios of the Minimal Supersymmetric Standard Model

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Mechanisms of human telomerase reverse transcriptase (hTERT) regulation: clinical impacts in cancer

Author: A Azouz
A Kilian
A Kulic
A Portela
A Zhang
AA Avilion
AF Vallarelli
AG Bodnar
AH Shain
AJ Bannister
AJ Cesare
AK Chan
AM Deaton
Arnaldo Figueiredo
AS Venteicher
B McClintock
B Seynnaeve
B van Steensel
B Vogelstein
C Cifuentes-Rojas
C Harle-Bachor
CB Harley
CB Umbricht
CB Umbricht
CD Hurst
CM Counter
CM Croce
CP Morales
CW Greider
D Broccoli
D Hanahan
DG Albertson
DL Aisner
DM Cittelly
Donghyun Lee
DS Huang
E Naderlinger
E Nagore
EH Blackburn
F Ishikawa
F Peng
FW Huang
G Cimino-Reale
G Cristofari
G Di Leva
G Furtjes
GB Morin
GC Prendergast
H Populo
H Suzuki
H Tahara
H Xie
H Zhang
HH Ng
I Guilleret
I Hatada
I Kinde
J Deng
J Feng
J Li
J Vinagre
J Vinagre
J Winter
J Zhou
JA Weber
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JD Griffith
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JG Herman
JH Choi
JL Stern
Joana Dias Apolónio
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K Chiba
K Gao
K Hiyama
K Huppi
K Liu
K Vincent
K Yoshida
K Yoshida
KA Hoadley
KA Lewis
KH Shin
KJ Wu
L Bai
L Chen
L Cheng
L Harrington
L Liu
LA Carey
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LJ Valentijn
M Esteller
M Kawashima
M Kochling
M Peifer
M Wick
M Xing
M Xing
M Zimmermann
MA Jafri
MA Shammas
MJ Ahn
MK Graham
N Wang
N Wang
NG Lopatina
NJ Fredriksson
NW Kim
P Castelo-Branco
P Castelo-Branco
P Martinez
P Ostling
P Yuan
Pedro Castelo-Branco
PJ Killela
PJ Killela
PS Rachakonda
PV Glybochko
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R Meier
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Ricardo Leão
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SB Cohen
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SC Mack
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SL Weinrich
T de Lange
T de Lange
T Fernandez-Marcelo
T Saito
T Saito
T Tsujioka
T Vulliamy
TE Bartlett
TL Beattie
TM Bryan
TM Nakamura
TP Brien
TR Devereux
Uri Tabori
WC Cho
WE Wright
WE Wright
X Liu
X Liu
X Xu
X Zhao
XJ Yi
Y Allory
Y Doksani
Y Lin
Y Wu
YS Cong
YS Cong
Z Li
ZY Zhang
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/03/2018
Field of study

Background Limitless self-renewal is one of the hallmarks of cancer and is attained by telomere maintenance, essentially through telomerase (hTERT) activation. Transcriptional regulation of hTERT is believed to play a major role in telomerase activation in human cancers. Main body The dominant interest in telomerase results from its role in cancer. The role of telomeres and telomere maintenance mechanisms is well established as a major driving force in generating chromosomal and genomic instability. Cancer cells have acquired the ability to overcome their fate of senescence via telomere length maintenance mechanisms, mainly by telomerase activation. hTERT expression is up-regulated in tumors via multiple genetic and epigenetic mechanisms including hTERT amplifications, hTERT structural variants, hTERT promoter mutations and epigenetic modifications through hTERT promoter methylation. Genetic (hTERT promoter mutations) and epigenetic (hTERT promoter methylation and miRNAs) events were shown to have clinical implications in cancers that depend on hTERT activation. Knowing that telomeres are crucial for cellular self-renewal, the mechanisms responsible for telomere maintenance have a crucial role in cancer diseases and might be important oncological biomarkers. Thus, rather than quantifying TERT expression and its correlation with telomerase activation, the discovery and the assessment of the mechanisms responsible for TERT upregulation offers important information that may be used for diagnosis, prognosis, and treatment monitoring in oncology. Furthermore, a better understanding of these mechanisms may promote their translation into effective targeted cancer therapies. Conclusion Herein, we reviewed the underlying mechanisms of hTERT regulation, their role in oncogenesis, and the potential clinical applications in telomerase-dependent cancers.info:eu-repo/semantics/publishedVersio

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Antiinflammatory Therapy with Canakinumab for Atherosclerotic Disease

Author: A Abbate
A Abhyankar
A Adams
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A Akyea-Djamson
A Alan
A Alfieri
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A Alvarisqueta
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Dedkova S
Defosse C
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Dela Llana A
Delfonso F
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Delgadillo T
Dellasa M
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Dellorso M
Demidova M
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Dengler T
Dermitzakis A
Deslongchamps F
Dessalvi Cc
Destro M
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Devasia T
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Dhanak R
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Dognini Gp
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Donaubauer T
Dong X
Dormidontova G
Dorogova I
Dos Santos A
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Dragutksy B
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Dzupina A
Dékány Jn
E Eleuteri
E Englmann
Earl J
East C
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Ebeling K
Ebrahim I
Eccleston D
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Edillo C
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Einhorn D
Eki Y
El Hachem M
El Hafi S
Ellenbroek D
Ellis M
Emil B
Endo T
Engelen W
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Ervin W
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Espinosa V
Everett Bm
F Fedele
F Fonseca
F Fucci
Facello A
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Faghih M
Fail P
Falcon D
Fang C
Fang Cy
Farias E
Fattal P
Fawson A
Feitosa G
Felario Junior Ga
Felix L
Feng Y
Feng Z
Ferdinand K
Ferkl R
Fernandez Aa
Ferrari V
Ferrario M
Ferraz R
Ferreira Dos Santos T
Ferreira-Jardim A
Fien E
Filardi Pp
Filho P
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Fisher J
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Fitz-Patrick D
Fitzpatrick L
Flaksa I
Flather M
Flezar M
Fliesser-Goerzer E
Flores E
Flores E
Flores Gs
Flores H
Floro T
Foerster A
Folkeringa Rj
Fonseca A
Fontaine S
Forgon T
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Forker A
Forster T
Foster M
Foucauld J
Fowler V
Fox B
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Francoeur L
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Frankenstein L
Fratczak M
Freitas E
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Fu G
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G Gosselin
Gabito A
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Genova D
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Godoy Sanchez M
Goette A
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Goldberg N
Gomez Sanchez J
Gonsorcik J
Gonzales D
Gonzales V
Gonzalez E
Gordeev I
Gorges R
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Grigaraviciene I
Grigorova V
Gros C
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Gudipati Rvc
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Gutmann J
Guzman I
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Gyorgyova E
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Hagiwara Y
Haidar A
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Halliwell Tc
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Hamer Bjb
Hamud-Socoro A
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Hangyal T
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Hanustiakova A
Hao Y
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Hoogslag Pam
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Hsieh Ic
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Humbert J
Hurtig U
Hutchens E
Huynh T
Hwang Jj
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Høivik Ho
I Ilic
I Ivanov
Iachini K
Iannopollo G
Ibarra J
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Ibañez J
Iby M
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Igbokidi O
Iijima T
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Imbrognio M
Imre Bs
Inada T
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Indolfi C
Infusino F
Invitti C
Ipp E
Isaza D
Istratoaie O
Istvan Kp
Iteld B
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Jacques G
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Jensen Ed
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Jia Z
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Jiang X
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Jirvankar P
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Julien Ve
Julião K
Jure D
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K Kaigawa
K Katahira
K Kiroglu
K Kordic
K Kostov
Kabakchieva Vm
Kaczmarek N
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Kala P
Kaldara E
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Kamiya H
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Kara Yd
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Karsai Xz
Kastelein Jjp
Kataoka M
Katona A
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Kawka-Urbanek T
Kazanskay E
Ke Y
Keba E
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Kellnerova I
Kelly R
Kelt T
Kendall T
Kereiakes D
Khan A
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Khirmanov V
Khromtsova O
Kick J
Kiefer R
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Kitchens D
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Klemsdal To
Kleve R
Klugherz B
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Kobalava Z
Kodem Dr
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Komura Y
Kondagunta V
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Kostakou P
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Kumar Ks
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Kuzin A
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Libov I
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M Mallagray
M Mandati
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M Mcdonald
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M Mikus
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Macfadyen Jg
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Radhakrishnan V
Radin M
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Seroqui M
Servaes V
Sesto I
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Shapovalova Y
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Zirlik A
Zucchetti C
Publication venue: 'Massachusetts Medical Society'
Publication date: 01/01/2017
Field of study

Background: Experimental and clinical data suggest that reducing inflammation without affecting lipid levels may reduce the risk of cardiovascular disease. Yet, the inflammatory hypothesis of atherothrombosis has remained unproved. Methods: We conducted a randomized, double-blind trial of canakinumab, a therapeutic monoclonal antibody targeting interleukin-1β, involving 10,061 patients with previous myocardial infarction and a high-sensitivity C-reactive protein level of 2 mg or more per liter. The trial compared three doses of canakinumab (50 mg, 150 mg, and 300 mg, administered subcutaneously every 3 months) with placebo. The primary efficacy end point was nonfatal myocardial infarction, nonfatal stroke, or cardiovascular death. RESULTS: At 48 months, the median reduction from baseline in the high-sensitivity C-reactive protein level was 26 percentage points greater in the group that received the 50-mg dose of canakinumab, 37 percentage points greater in the 150-mg group, and 41 percentage points greater in the 300-mg group than in the placebo group. Canakinumab did not reduce lipid levels from baseline. At a median follow-up of 3.7 years, the incidence rate for the primary end point was 4.50 events per 100 person-years in the placebo group, 4.11 events per 100 person-years in the 50-mg group, 3.86 events per 100 person-years in the 150-mg group, and 3.90 events per 100 person-years in the 300-mg group. The hazard ratios as compared with placebo were as follows: in the 50-mg group, 0.93 (95% confidence interval [CI], 0.80 to 1.07; P = 0.30); in the 150-mg group, 0.85 (95% CI, 0.74 to 0.98; P = 0.021); and in the 300-mg group, 0.86 (95% CI, 0.75 to 0.99; P = 0.031). The 150-mg dose, but not the other doses, met the prespecified multiplicity-adjusted threshold for statistical significance for the primary end point and the secondary end point that additionally included hospitalization for unstable angina that led to urgent revascularization (hazard ratio vs. placebo, 0.83; 95% CI, 0.73 to 0.95; P = 0.005). Canakinumab was associated with a higher incidence of fatal infection than was placebo. There was no significant difference in all-cause mortality (hazard ratio for all canakinumab doses vs. placebo, 0.94; 95% CI, 0.83 to 1.06; P = 0.31). Conclusions: Antiinflammatory therapy targeting the interleukin-1β innate immunity pathway with canakinumab at a dose of 150 mg every 3 months led to a significantly lower rate of recurrent cardiovascular events than placebo, independent of lipid-level lowering. (Funded by Novartis; CANTOS ClinicalTrials.gov number, NCT01327846.

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Archivio istituzionale della ricerca - Università di Cagliari

George Washington University: Health Sciences Research Commons (HSRC)

Archivio istituzionale della ricerca - Università di Palermo

Archivio della ricerca - Università degli studi di Napoli Federico II

Archivio Istituzionale della Ricerca - Università degli Studi di Pavia

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Archivio della ricerca- Università di Roma La Sapienza

Dokuz Eylul University Research Information System

Measurement of the tt̄W and tt̄Z production cross sections in pp collisions at √s = 8 TeV with the ATLAS detector

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Abbott B
Abdallah J
Abdinov O
Aben R
Abolins M
AbouZeid OS
Abramowicz H
Abreu H
Abreu R
Abulaiti Y
Acharya BS
Adamczyk L
Adams DL
Adelman J
Adomeit S
Adye T
Affolder AA
Agatonovic-Jovin T
Agricola J
Aguilar-Saavedra JA
Ahlen SP
Ahmadov F
Aielli G
Akerstedt H
Akesson TPA
Akimov AV
Alberghi GL
Albert J
Albrand S
Alconada Verzini MJ
Aleksa M
Aleksandrov IN
Alexa C
Alexander G
Alexopoulos T
Alhroob M
Alimonti G
Alio L
Alison J
Alkire SP
Allbrooke BMM
Allport PP
Aloisio A
Alonso A
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Alpigiani C
Altheimer A
Alvarez Piqueras D
Alviggi MG
Amadio BT
Amako K
Amelung C
Amidei D
Amorim A
Amoroso S
Amram N
Amundsen G
Anastopoulos C
Ancu LS
Andari N
Andeen T
Anders CF
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Anders JK
Anderson KJ
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Angelidakis S
Angelozzi I
Anger P
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Anisenkov AV
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Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2015
Field of study

The production cross sections of top-quark pairs in association with massive vector bosons have been measured using data from pp collisions at s√ = 8 TeV. The dataset corresponds to an integrated luminosity of 20.3 fb−¹ collected by the ATLAS detector in 2012 at the LHC. Final states with two, three or four leptons are considered. A fit to the data considering the tt̄W and tt̄Z processes simultaneously yields a significance of 5.0σ (4.2σ) over the background-only hypothesis for tt¯Wtt¯W (tt̄Z) production. The measured cross sections are σtt̄W = 369 + 100−91 fb and σtt̄Z = 176 + 58−52 fb. The background-only hypothesis with neither tt̄W nor tt̄Z production is excluded at 7.1σ. All measurements are consistent with next-to-leading-order calculations for the tt̄W and tt̄Z processes

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