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Identification and Filtering of Uncharacteristic Noise in the CMS Hadron Calorimeter

Author: Abadjiev K
Abbaneo D
Abbiendi G
Abbrescia M
Abdullin S
Abelev B
Acosta D
Acosta JG
Acosta MV
Actis O
Adam N
Adam W
Adams MR
Adams T
Adiguzel A
Adler V
Adolphi R
Adzic P
Afaq MA
Agostino L
Agram JL
Aguilar-Benitez M
Ahmad M
Ahmad WH
Ahmed I
Ahmed W
Ahuja S
Aisa D
Aisa S
Akchurin N
Akgun B
Akgun U
Akimenko S
Akin IV
Alagoz E
Alampi G
Albajar C
Albayrak EA
Alberdi J
Albergo S
Albert E
Albrow M
Alexander J
Alidra M
Aliev T
Allfrey P
Almeida N
Altenhofer G
Altsybeev I
Alver B
Alverson G
Alves GA
Amaglobeli N
Amapane N
Ambroglini F
Amsler C
Anagnostou G
Ananthan B
Anastassov A
Andelin D
Anderson M
Andrea J
Andreev V
Andreev Y
Anghel IM
Anguelov T
Anisimov A
Antillon E
Antipov P
Antonelli L
Anttila E
Antunes JR
Antunovic Z
Apanasevich L
Apollinari G
Apresyan A
Arce P
Arcidiacono R
Arenton MW
Arfaei H
Argiro S
Arisaka K
Arneodo M
Arnold B
Arora S
Artamonov A
Asaadi J
Asghar MI
Ashby S
Askew A
Atac M
Atramentov O
Auffray E
Aurisano A
Autermann C
Avery P
Avetisyan A
Avila C
Awan MIM
Ayan AS
Ayhan A
Azhgirey I
Aziz T
Azzi P
Azzurri P
Baarmand MM
Babb J
Babucci E
Baccaro S
Bacchetta N
Bacchi W
Bachtis M
Baden D
Badgett W
Baechler J
Baer H
Baesso P
Baffioni S
Bagby L
Bagliesi G
Bahk SY
Bailleux D
Baillon P
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Bakhshiansohi H
Bakirci MN
Bakken JA
Balazs M
Baldin B
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Ball G
Ballin J
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Ban Y
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Banerjee S
Banerjee S
Banicz K
Bansal S
Banzuzi K
Barashko V
Barbagli G
Barberis E
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Publication venue: INSTITUTE OF PHYSICS PUBLISHING
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Oestradiol-17β plasma concentrations after intramuscular injection of oestradiol benzoate or oestradiol cypionate in llamas (Lama glama)

Author: AC Evans
AK Cancino
BG England
BH Ali
BX Chen
Carolina P Bianchi
CB Navarre
CB Navarre
CP Bianchi
CR Burke
E Rubianes
GA Bo
GA Bo
GA Bo
GP Adams
GP Adams
J Baggot
J Sirois
J Thundathil
JA Skidmore
JJ Reeves
JL Vaughan
JL Vaughan
L Vynckier
M O'Rourke
M Oukessou
M San-Martín
MA Aba
MA Aba
MA Aba
MA Aba
Marcelo A Aba
María V Cavilla
MF Martínez
MG Chaves
MG Colazo
MG Diskin
MH Ratto
MJ D'Occhio
OJ Ginther
PW Bravo
PW Bravo
RJ Mapletoft
Publication venue: BioMed Central
Publication date: 01/01/2010
Field of study

Abstract Background Llamas (<it>Lama glama</it>) are induced ovulators and the process of ovulation depends on dominant follicular size. In addition, a close relationship between behavioural estrus and ovulation is not registered in llamas. Therefore, the exogenous control of follicular development with hormones aims to predict the optimal time to mate. Oestradiol-17β (E2) and its esters are currently used in domestic species, including camelids, in synchronization treatments. But, in llamas, there is no reports regarding the appropriate dosages to be used and most protocols have been designed by extrapolation from those recommended for other ruminants. The aim of the present study was to characterize plasma E2 concentrations in intact female llamas following a single intramuscular (i.m.) injection of two oestradiol esters: oestradiol benzoate (EB) and oestradiol cypionate (ECP). Methods Twelve non pregnant and non lactating sexually mature llamas were i.m. injected on day 0 with 2.5 mg of EB (EB group, n = 6) or ECP (ECP group, n = 6). Blood samples were collected immediately before injection, at 1, 6, 12, 24 h after treatment and then daily until day 14 post injection. Changes in hormone concentrations with time were analyzed in each group by analysis of variance (ANOVA) using a repeated measures (within-SS) design. Plasma E2 concentrations and area under the concentration-time curve (AUC) values were compared between groups by ANOVA. In all cases a Least-Significant Difference test (LSD) was used to determine differences between means. Hormonal and AUC data are expressed as mean ± S.E.M. Results Peak plasma E2 concentrations were achieved earlier and were higher in EB group than in ECP group. Thereafter, E2 returned to physiological concentrations earlier in EB group (day 5) than in ECP group (day 9). Although plasma E2 profiles differed over time among groups there were no differences between them on AUC values. Conclusions The i.m. injection of a single dose of both oestradiol esters resulted in plasma E2 concentrations exceeding physiological values for a variable period. Moreover, the plasma E2 profiles observed depended on the derivative of oestradiol administered. This basic information becomes relevant at defining treatment protocols including oestrogens in llamas.</p

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Structural Basis for Certain Naturally Occurring Bioflavonoids to Function as Reducing Co-Substrates of Cyclooxygenase I and II

Author: B Bambai
Bao Ting Zhu
BT Zhu
CA Rouzer
Christophe Herman
D Amic
D Thompson
FJ van der Ouderaa
G Wu
HW Bai
HW Bai
Hyoung-Woo Bai
I Wells
J Sirois
JL Lee
JR Kiefer
JW Regan
LM Landino
M Bala
M Hamberg
M Lecomte
ME Hemler
MG Malkowski
MK O'Banion
MM Silva
OH Callan
Pan Wang
PJ Harvison
R Dietz
RG Kurumbail
RG Kurumbail
RJ Kulmacz
S Burda
T Hla
T Miyamoto
W Bors
WL Smith
Y Hsuanyu
YM Sung
Publication venue: Public Library of Science
Publication date: 01/08/2010
Field of study

Recent studies showed that some of the dietary bioflavonoids can strongly stimulate the catalytic activity of cyclooxygenase (COX) I and II in vitro and in vivo, presumably by facilitating enzyme re-activation. In this study, we sought to understand the structural basis of COX activation by these dietary compounds.A combination of molecular modeling studies, biochemical analysis and site-directed mutagenesis assay was used as research tools. Three-dimensional quantitative structure-activity relationship analysis (QSAR/CoMFA) predicted that the ability of bioflavonoids to activate COX I and II depends heavily on their B-ring structure, a moiety known to be associated with strong antioxidant ability. Using the homology modeling and docking approaches, we identified the peroxidase active site of COX I and II as the binding site for bioflavonoids. Upon binding to this site, bioflavonoid can directly interact with hematin of the COX enzyme and facilitate the electron transfer from bioflavonoid to hematin. The docking results were verified by biochemical analysis, which reveals that when the cyclooxygenase activity of COXs is inhibited by covalent modification, myricetin can still stimulate the conversion of PGG(2) to PGE(2), a reaction selectively catalyzed by the peroxidase activity. Using the site-directed mutagenesis analysis, we confirmed that Q189 at the peroxidase site of COX II is essential for bioflavonoids to bind and re-activate its catalytic activity.These findings provide the structural basis for bioflavonoids to function as high-affinity reducing co-substrates of COXs through binding to the peroxidase active site, facilitating electron transfer and enzyme re-activation

Public Library of Science (PLOS)

TRAF6 and IRF7 Control HIV Replication in Macrophages

Author: A Matsuda
AA Lambert
AJ Smith
B Beutler
BK Weaver
CE Samuel
Christopher H. Woelk
CJ Shah Mohak
DD Richman
E Izmailova
E Meylan
Fabrizio Mammano
G Dennis Jr
G Peng
GJ Nuovo
GR Stark
H Chen
H Kato
H Konno
HC Schroder
I Marie
J Ruland
Jacques Corbeil
JF Fortin
Jérôme Estaquier
K Honda
K Takeda
KA Fitzgerald
KN Bishop
L Campillo-Gimenez
L Song
LG Xu
Lynda Robitaille
M Covic
M Laforge
M Oldak
M Sato
M Sato
M Sato
M Sgarbanti
M Sgarbanti
M Shah
M Stremlau
M Yoneyama
M Yoneyama
M Yoneyama
MG Wathelet
Mohak Shah
MS Kunzi
Mélissa Sirois
N Buettner
N Jouvenet
NF Muto
P Genin
PR Meylan
R Colina
R Lin
R Medzhitov
R Yoshida
RB Seth
Robin Allary
RS Kornbluth
S Ning
S Pestka
S Sato
S Sharma
SD Barr
SJ Neil
T Kawai
T Kawai
Z Wu
Publication venue: Public Library of Science
Publication date: 28/11/2011
Field of study

The innate immune system recognizes virus infection and evokes antiviral responses which include producing type I interferons (IFNs). The induction of IFN provides a crucial mechanism of antiviral defense by upregulating interferon-stimulated genes (ISGs) that restrict viral replication. ISGs inhibit the replication of many viruses by acting at different steps of their viral cycle. Specifically, IFN treatment prior to in vitro human immunodeficiency virus (HIV) infection stops or significantly delays HIV-1 production indicating that potent inhibitory factors are generated. We report that HIV-1 infection of primary human macrophages decreases tumor necrosis factor receptor-associated factor 6 (TRAF6) and virus-induced signaling adaptor (VISA) expression, which are both components of the IFN signaling pathway controlling viral replication. Knocking down the expression of TRAF6 in macrophages increased HIV-1 replication and augmented the expression of IRF7 but not IRF3. Suppressing VISA had no impact on viral replication. Overexpression of IRF7 resulted in enhanced viral replication while knocking down IRF7 expression in macrophages significantly reduced viral output. These findings are the first demonstration that TRAF6 can regulate HIV-1 production and furthermore that expression of IRF7 promotes HIV-1 replication

Southampton (e-Prints Soton)

The Francis Crick Institute

Emerging Roles of PAR-1 and PAFR in Melanoma Metastasis

Author: A Boire
A Boucharaba
A Calignano
A Cucina
A Fallani
A Mantovani
A Ueno
B Bussolati
B Nieswandt
C Gaggioli
C Rudroff
C Tellez
C Tellez
CA Demopoulos
CE Lewis
CS Tellez
D Massi
DD Deo
DD Deo
DJ Dauer
DR Senger
E Pikarsky
EC Fabo De
EG Fischer
EG Robert
F Balkwill
F Bussolino
FP Noonan
G Camussi
G Camussi
G Mannori
G Montrucchio
G Montrucchio
G Montrucchio
G Montrucchio
Gabriel J. Villares
GC Haralabopoulos
GJ Gasic
GK Marathe
GK Marathe
H Bito
H Shindou
HM Ko
IJ Fidler
J Benveniste
J Benveniste
JB Travers
JJ Li
JP Walterscheid
JR Brown
JT Lee
KK Hansen
KS Smalley
L Biancone
LA Barber
LM Coussens
LM Coussens
LM Postovit
M Nakamura
M Palma De
ME Bromberg
Menashe Bar-Eli
MF Brizzi
MG Sirois
ML Blank
ML Blank
ML Nierodzik
ML Nierodzik
ML Nierodzik
MY Hsu
MZ Wojtukiewicz
MZ Wojtukiewicz
N Kepner
NI Affara
NK Haass
O Nyormoi
PJ O’Brien
Q Zhang
R Maliba
R Mohle
RA Gupta
RD Ye
S Even-Ram
S Ishii
S Rollin
S Sato
S Shimizu
S Zucker
SC Even-Ram
SC Robinson
SE Ullrich
SY Im
T Schwarz
TD Tlsty
TW Axelrad
V Kaushal
Vladislava O. Melnikova
VO Melnikova
W Ruf
W Ruf
Y Pei
Y Sheng
Y Uemura
YQ Huang
Publication venue: Springer Netherlands
Publication date: 01/01/2008
Field of study

Melanoma growth, angiogenesis and metastatic progression are strongly promoted by the inflammatory tumor microenvironment due to high levels of cytokine and chemokine secretion by the recruited inflammatory and stromal cells. In addition, platelets and molecular components of procoagulant pathways have been recently emerging as critical players of tumor growth and metastasis. In particular, thrombin, through the activity of its receptor protease-activated receptor-1 (PAR-1), regulates tumor cell adhesion to platelets and endothelial cells, stimulates tumor angiogenesis, and promotes tumor growth and metastasis. Notably, in many tumor types including melanoma, PAR-1 expression directly correlates with their metastatic phenotype and is directly responsible for the expression of interleukin-8, matrix metalloproteinase-2 (MMP-2), vascular endothelial growth factor, platelet-derived growth factor, and integrins. Another proinflammatory receptor–ligand pair, platelet-activating factor (PAF) and its receptor (PAFR), have been shown to act as important modulators of tumor cell adhesion to endothelial cells, angiogenesis, tumor growth and metastasis. PAF is a bioactive lipid produced by a variety of cells from membrane glycerophospholipids in the same reaction that releases arachidonic acid, and can be secreted by platelets, inflammatory cells, keratinocytes and endothelial cells. We have demonstrated that in metastatic melanoma cells, PAF stimulates the phosphorylation of cyclic adenosine monophosphate response element-binding protein (CREB) and activating transcription factor 1 (ATF-1), which results in overexpression of MMP-2 and membrane type 1-MMP (membrane type 1-MMP). Since only metastatic melanoma cells overexpress CREB/ATF-1, we propose that metastatic melanoma cells are better equipped than their non-metastatic counterparts to respond to PAF within the tumor microenvironment. The evidence supporting the hypothesis that the two G-protein coupled receptors, PAR-1 and PAFR, contribute to the acquisition of the metastatic phenotype of melanoma is presented and discussed

Springer - Publisher Connector

University of Liverpool Repository

A Deep Neural Network for Simultaneous Estimation of b Jet Energy and Resolution

Author: Aarrestad TK
Abbaneo D
Abbiendi G
Abbrescia M
Abdalla H
Abdullah WATW
Abdullin S
Abercrombie D
Acharya H
Acosta D
Acosta JG
Adam W
Adams MR
Adams T
Adzic P
Adán DP
Afanasiev S
Agapitos A
Agarwal G
Aggleton R
Agram J-L
Aguilar-Benitez M
Ahmad A
Ahmad M
Ahmad M
Ahmad WH
Ahuja S
Akbiyik M
Akchurin N
Akgun B
Albajar C
Albergo S
Albert A
Albrow M
Aleksandrov A
Alexander J
Alhusseini M
Alimena J
Allen B
Almond J
Alonso AG
Alvarez JDR
Alverson G
Alves FL
Alves GA
Aly R
Alyari M
Amapane N
Ambrogi F
Amendola C
Amin N
Amsler C
Anagnostou G
Anampa KH
Anderson D
Andrea J
Andreev V
Andreev Y
Andrews MB
Androsov K
Angioni GLP
Antchev G
Antunovic Z
Anuar AAB
Apanasevich L
Apollinari G
Apresyan A
Apyan A
Araujo M
Arbelaez NV
Arbol PMRD
Arcaro D
Arcidiacono R
Arenton MW
Argiro S
Arneodo M
Asavapibhop B
Asawatangtrakuldee C
Asenov P
Askew A
Asmuss P
Atakisi IO
Ather MW
Attikis A
Auffray E
Aushev T
Autermann C
Auzinger G
Avati V
Avery P
Avila C
Ayala E
Azarkin M
Azhgirey I
Aziz T
Azzi P
Azzurri P
Baarmand MM
Babaev A
Babounikau I
Bacchetta N
Bachiller I
Bachtis M
Backhaus M
Baden A
Baechler J
Bagliesi G
Bahinipati S
Baillon P
Bainbridge R
Bakas G
Bakhshiansohi H
Ball AH
Ban Y
Band R
Banerjee S
Banerjee S
Bansal S
Barbagli G
Barberis E
Bargassa P
Baringer P
Barker A
Barnes VE
Barney D
Barnyakov A
Baron O
Barrera CB
Barrera CO
Barria P
Bartek R
Barth C
Bartosik N
Bartók M
Baselga M
Baskakov A
Bastos D
Bat A
Battilana C
Baty A
Bauerdick LAT
Baur S
Bayshev I
Bean A
Beauceron S
Beaudette F
Becerra DAS
Bedoya C
Beernaert K
Beghin D
Behera PK
Behnke O
Behrens U
Bein S
Belforte S
Bell KW
Bellan R
Belloni A
Bellora A
Belyaev A
Belyaev A
Benaglia A
Benato L
Bencze G
Bendavid J
Benecke A
Benelli G
Beni N
Benitez JF
Benussi L
Beretvas A
Bergauer T
Berger P
Berger T
Beri SB
Bernardes CA
Bernet C
Berry D
Berryhill J
Bertacchi V
Bertsche D
Besancon M
Beschi A
Betts RR
Bhal E
Bhandari R
Bhardwaj A
Bhardwaj R
Bharti M
Bhat MA
Bhat PC
Bhatnagar V
Bhattacharya R
Bhattacharya S
Bhattacharya S
Bhattacharya S
Bhawandeep U
Bheesette S
Bhowmik D
Bhowmik S
Bhyun JH
Bi R
Bialkowska H
Bianchini L
Bianco M
Bianco S
Biasini M
Bihan A-CL
Biino C
Bilei GM
Bilin B
Bilki B
Bindhu VKMN
Bisello D
Bitioukov S
Blekman F
Blinov V
Blobel V
Bloch D
Bloch P
Bloom K
Bluj M
Blumenfeld B
Boccali T
Bocci A
Bodek A
Boimska B
Boletti A
Bologna S
Bols ES
Bonacorsi D
Bonchev M
Bondu O
Boos E
Boran F
Borchsh V
Boren S
Borg J
Borgonovi L
Bornheim A
Borras K
Bortignon P
Bose T
Bossini E
Botta C
Botta V
Boudoul G
Bouhali O
Bourgatte G
Bourilkov D
Bouza VR
Bowen J
Bozzo M
Bragagnolo A
Braghieri A
Braibant-Giacomelli S
Brainerd C
Brandt S
Branson JG
Bravo C
Breedon R
Breeze S
Brew C
Brigljevic V
Brinkerhoff A
Brivio F
Brom J-M
Brondolin E
Brooke JJ
Brown RM
Bruno G
Brzhechko D
Bucci R
Buccilli A
Buchanan J
Buchmuller O
Bueghly J
Bundock A
Bunin P
Bunkowski K
Buontempo S
Burgo RD
Burkett K
Burkle B
Burns D
Burt K
Busson P
Busza W
Butler JN
Butler PH
Butz E
Bylinkin A
Bylsma B
Byszuk A
Caballero IG
Cabrera A
Cabrillo IJ
Cadamuro L
Caillol C
Cakir A
Calabria C
Calderon A
Cali IA
Call K
Calligaris L
Camen C
Caminada L
Campagnari C
Campanini R
Campbell A
Campderros JD
Camporesi T
Candelise V
Canelli MF
Canepa A
Cankocak K
Capiluppi P
Cappati A
Caputo C
Caratelli A
Caraway B
Cardini A
Carle A
Carlin R
Carlsmith D
Cartiglia N
Carvalho W
Casarsa M
Caspart R
Cassese A
Castaldi R
Castilla-Valdez H
Castro A
Cavallari F
Cavallo FR
Cavallo N
Cavanaugh R
Ceballos GG
Ceccarelli R
Celik A
Cepeda M
Cerati GB
Cerci DS
Cerci S
Cerminara G
Cerrada M
Cerri O
Chabert EC
Chadeeva M
Chagas EBBD
Chahal G
Chang P
Chang P
Chanon N
Chao Y
Chapon E
Charlot C
Chatterjee RM
Chatterjee S
Chauhan S
Chauhan S
Chawla R
Checchia P
Chen G
Chen GM
Chen HS
Chen KF
Chen M
Chen PH
Chen X
Chen Y
Chenarani S
Cheng T
Cheng Y
Cherepanov V
Chernyavskaya N
Chertok M
Cheung HWK
Chhibra SS
Chiarito B
Chierici R
Chinellato J
Chlebana F
Cho S
Choi J
Choi S
Choi Y
Chou JP
Choudhary BC
Choudhury S
Chowdhury SR
Chtchipounov L
Chu J
Chudasama R
Chwalek T
Ciangottini D
Cifuentes JAB
Ciocca C
Ciocci MA
Cipriani M
Ciriolo V
Cirkovic P
Citron M
Cittolin S
Ciulli V
Civinini C
Claes DR
Clare R
Clement E
Clerbaux B
CMS Collaboration .
Cockerill DJA
Cocoros A
Codispoti G
Coelho E
Colaleo A
Cole JE
Colino N
Collard C
Colling D
Cometti S
Connor P
Contardo D
Conte E
Contreras-Campana C
Conway J
Conway R
Cooper SI
Cooperstein S
Cornelis T
Cortezon EP
Cossutti F
Costa M
Costa S
Coubez X
Couderc F
Coughlan JA
Cousins R
Covarelli R
Cox B
Cox PT
Creanza D
Cremonesi M
Crescenzo AD
Cristella L
Croce DD
Cruz SS
Csanad M
Csorgo T
Cucciati G
Cuevas J
Cuffiani M
Cumalat JP
Cummings G
Cussans D
Cutts D
Czellar S
D'Alessandro R
D'Alfonso M
d'Enterria D
D'Hondt J
Da Costa EM
Da Rold A
Da Silva De Araujo FT
Da Silva WLP
Da Silveira GG
Dabrowski A
Daci N
Dalchenko M
Dallavalle GM
Damarseckin S
Damgov J
Damiani DD
Danilov V
Daponte V
Darwish MR
Das P
Das S
Dasgupta A
Daskalakis G
Dasu S
Datta A
Dauncey P
David A
David P
Davies G
Davignon O
De Almeida MM
de Barbaro P
De Boer W
De Bruyn I
de Cassagnac RG
De Castro Manzano P
De Clercq J
De Cosa A
de Fatis TT
De Filippis N
De Guio F
De Iorio A
De Jesus Damiao D
De Klundert MV
De La BarcaSanchez MC
De La Cruz-Burelo E
De Lentdecker G
De Mattia M
de Monchenault GH
De Oliveira Martins C
De Oliveira ACA
De Palma M
De Roeck A
De Souza SF
de Trocóniz JF
De Wit A
De Wolf EA
Deelen N
Defranchis MM
Deile M
Deiters K
Dejardin M
DeLa Cruz B
Delaere C
Delannoy AG
Delannoy H
Delcourt M
Delgado A
Delgado MAS
Dell'Orso R
Demaria N
Demina R
Demiragli Z
Demiroglu ZS
Denegri D
Depasse P
Derdzinski M
Dermenev A
Dev N
Dewanjee RK
Dezoort G
Dharmaratna WGD
Dhingra N
Diab B
Diamantopoulou M
Diemoz M
Dierlamm A
Dildick S
Dilsiz K
Dimitrov A
Dimova T
Dinardo ME
Dini P
Dissertori G
Dittmann J
Dittmar M
Dittmer S
Doan TH
Dobson M
Dobur D
Dodd L
Dolek F
Dolen J
Dominguez A
Donato S
Donckt MV
Donegà M
Doninck WV
Dordevic M
Dorfer C
Dorigo T
Dorney B
Doroba K
Dosselli U
Dozen C
Dragicevic M
Dremin I
Dreyer T
Drugakov V
Duarte J
Dube S
Dubinin M
Dudenas V
Dudko L
Dugad S
Duh YT
Dulemba JL
Dumanoglu I
Dupont N
Durgut S
Duric S
Durkin LS
Dutta D
Dutta I
Dutta S
Dutta V
Dünser M
Ebrahimi A
Eckerlin G
Ecklund KM
Eckstein D
Eerola P
Ehataht K
Eichhorn T
Elgammal S
Elliott-Peisert A
Elmer P
Elmetenawee W
Elvira VD
Elwood A
Eminizer N
Emriskova N
Eno SC
Epshteyn V
Erbacher R
Erdmann M
Erdmann W
Eren E
Erice C
Erodotou E
Errico F
Ershov A
Erö J
Espinosa TAG
Estrada CU
Etesami SM
Eusebi R
Evangelou I
Evans A
Evdokimov O
Everaerts P
Eysermans J
Fabbri F
Fabbro B
Fabozzi F
Faccioli P
Fallavollita F
Fallon C
Falmagne G
Faltermann N
Fanfani A
Fang W
Fangmeier C
Fanò L
Fasanella D
Faure JL
Favart L
Fay J
Fedi G
Feindt F
Felcini M
Feld L
Feng Y
Ferbel T
Ferencek D
Ferguson T
Fernandez M
Fernández AÁ
Fernández JRG
Ferri F
Ferro F
Field RD
Fienga F
Figueiredo DM
Finco L
Finger M
Finger M
Fiore L
Fiorendi S
Fiori F
Fiorina D
Fischer B
Flacher H
Flechl M
Flix J
Florent A
Flores C
Florez C
Florio AD
Flügge G
Focardi E
Folgueras S
Fontaine J-C
Fontanesi E
Ford WT
Forthomme L
Foudas C
Fouz MC
Francesco AD
Francis B
Francois B
Frankenthal A
Franzoni G
Freed S
Freeman J
Freer C
Fröhlich A
Frühwirth R
Fulcher J
Funk G
Funk W
Gadrat S
Galanti M
Galati G
Galinhas B
Gallinaro M
Gallo E
Galloni C
Gandrajula RP
Gandrakota A
Ganjour S
Gao X
Garbers C
Garcia F
Garcia JMV
Garcia-Bellido A
Garg RB
Garutti E
Gary JW
Gascon S
Gasparini F
Gasparini U
Gastler D
Gavrilenko M
Gavrilov V
Gecse Z
Geiser A
Gelmi A
Gelé D
Gennai S
Geralis T
Gerber CE
Gerosa R
Gershtein Y
Geurts FJM
Ghezzi A
Ghosh S
Ghosh S
Giacomelli P
Giammanco A
Giani S
Gianneios P
Giannini L
Giassi A
Giffels M
Gigi D
Gilbert A
Gilbert D
Giljanović D
Gill K
Gilmore J
Givernaud A
Glege F
Gleyzer SV
Gninenko S
Go Y
Godinovic N
Goerlach U
Goh J
Gokbulut G
Gola M
Goldenzweig P
Goldouzian R
Goldstein J
Golf F
Golovtcov V
Golubev N
Golutvin I
Gomber B
Gomez G
Gomez JP
Goncharov M
Gonzalez BA
Gonzalez D
Gonzalez JS
González CAS
Gorbunov I
Gottmann A
Gottschalk E
Gouskos L
Gouzevitch M
Govoni P
Gozzelino A
Grab C
Grandi C
Gras P
Gray L
Grebenyuk A
Green D
Greene S
Gregores EM
Gribushin A
Grippo MT
Gritsan AV
Grohsjean A
Gruchala M
Grunewald M
Grynyov B
Grzanka L
Grünendahl S
Guativa LMH
Guchait M
Guerrero D
Guiducci L
Guilbaud M
Guisao JM
Guler E
Guler Y
Gulhan D
Gunnellini P
Gunter T
Gupta R
Gurrola A
Gutay L
Guthoff M
Guts S
Gutsche O
Guzzi L
Górski M
Gülmez E
Ha S
Haddad Y
Hadjiiska R
Hadley M
Hadley NJ
Haevermaet HV
Hagopian S
Hagopian V
Hahn KA
Hajdu C
Hakala J
Halkiadakis E
Hall A
Hall G
Haller J
Hangal DA
Hanlon J
Hansen P
Hanson G
Haranko M
Harb A
Hardenbrook J
Harder K
Harper S
Harr R
Harrendorf MA
Harrington C
Harris P
Harris RM
Hart A
Hartmann F
Hasegawa S
Hashemi B
Hassan Q
Hatakeyama K
Haubrich N
Hauser J
Havukainen J
Haytmyradov M
He H
Heath GP
Heath HF
Hebbeker T
Hegde V
Hegeman J
Heidegger C
Heikkilä JK
Heindl M
Heintz U
Heller R
Henderson C
Hensel C
Hernandez AC
Hernandez AMV
Hernandez JM
Herndon M
Hernández CFG
Herrera CM
Hervé A
Higginbotham S
Hildreth M
Hill C
Hiltbrand J
Hindrichs O
Hinzmann A
Hirosky R
Hirschauer J
Hits D
Hlushchenko O
Hobson PR
Hoepfner K
Hofman DJ
Hogan JM
Hoh SY
Hohlmann M
Hollar J
Hong B
Hoorani HR
Horisberger R
Hortiangtham A
Horvath D
Hos I
Hosseinabadi FR
Hou W-S
Hove PV
Hsu D
Hu M
Hu Z
Huang T
Hughes E
Hung WT
Husemann U
Hussain U
Hwang C
Iaselli G
Iashvili I
Iaydjiev P
Ibarguen HAS
Ibrahim ZA
Idris FM
Iemmi F
Ignatenko M
Iiyama Y
Iles G
Ille B
Incandela J
Ince M
Ingram Q
Innocente V
Ioannou A
Iorio AOM
Isidori T
Isik C
Isildak B
Iuzhakov A
Ivanchenko V
Ivanov A
Ivanov T
Ivanov Y
Jabeen S
Jafari A
Jaime MM
Jain S
Jain S
James T
Janjam R
Janot P
Jansová M
Janssen X
Jarrin EC
Jarry P
Jayatilaka B
Jeitler M
Jeng GY
Jensen F
Jeon D
Jeon S
Jeong Y
Jessop C
Jha V
Ji W
Jiang CH
Jindariani S
Johns W
Johnson KF
Johnson M
Jomhari NZ
Jones M
Josa MI
Joshi BM
Joshi U
Joshi YR
Joyce M
Jung AW
Jung H
Juodagalvis A
Kaadze K
Kachanov V
Kadastik M
Kadija K
Kaestli HC
Kalbhor P
Kalinowski A
Kalogeropoulos A
Kalsi AK
Kamalieddin R
Kamenev A
Kamon T
Kangal EE
Kansal B
Kaplan S
Kapoor A
Kar C
Kara O
Karacheban O
Karancsi J
Karapinar G
Karapostoli G
Karathanasis G
Karavdina A
Karchin PE
Kardapoltsev L
Karimäki V
Karjavine V
Karmakar S
Karmgard DJ
Karneyeu A
Kasem A
Kasemann M
Kasieczka G
Kaspar J
Katsoulis P
Kaur A
Kaur M
Kaur S
Kaveh H
Kaya M
Kaya O
Kaynak B
Kazana M
Keaveney J
Keller H
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Publication venue
Publication date: 01/01/2020
Field of study

We describe a method to obtain point and dispersion estimates for the energies of jets arising from b quarks produced in proton-proton collisions at an energy of s = 13 TeV at the CERN LHC. The algorithm is trained on a large sample of simulated b jets and validated on data recorded by the CMS detector in 2017 corresponding to an integrated luminosity of 41 fb - 1 . A multivariate regression algorithm based on a deep feed-forward neural network employs jet composition and shape information, and the properties of reconstructed secondary vertices associated with the jet. The results of the algorithm are used to improve the sensitivity of analyses that make use of b jets in the final state, such as the observation of Higgs boson decay to b b ¯

UCL Discovery

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
Abbaneo D
Abbiendi G
Abbrescia M
Abdullah WATW
Abdullin S
Abercrombie D
Acharya H
Acosta D
Acosta JG
Adam W
Adams E
Adams MR
Adams T
Adloff C
Adzic P
Adán DP
Afanasiev S
Agapitos A
Agarwal G
Aggleton R
Agram J-L
Aguilar-Benitez M
Ahmad A
Ahmad M
Ahmad WH
Ahmed A
Ahuja S
Aime' C
Akchurin N
Akgun B
Akpinar A
Albajar C
Albergo S
Albert A
Albrow M
Aleksandrov A
Alexander J
Alhusseini M
Alimena J
Alison J
Allen B
Almond J
Alonso AG
Alvarez JDR
Alverson G
Alves GA
Aly R
Alyari M
Amapane N
Amaral SMSD
Amendola C
Amin N
Amram O
Amsler C
Anagnostou G
Anampa KH
Anderson D
Andrea J
Andreev V
Andreev Y
Andrews MB
Androsov K
Angioni GLP
Antchev G
Antunovic Z
Anuar AAB
Apanasevich L
Apollinari G
Appelt E
Apresyan A
Apyan A
Araujo M
Arbelaez NV
Arbol PMRD
Arcaro D
Arcidiacono R
Arenton MW
Argiro S
Arneodo M
Aruta C
Asavapibhop B
Asawatangtrakuldee C
Asenov P
Asghar MI
Asilar E
Askew A
Asmuss P
Atakisi IO
Atanasov I
Ather MW
Attikis A
Auffray E
Aushev T
Auzinger G
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Cifuentes JAB
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Ciriolo V
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Dharmaratna WGD
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González CAS
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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

Repositorio Institucional de la Universidad de Oviedo