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Sm/Lsm Genes Provide a Glimpse into the Early Evolution of the Spliceosome

Author: A Drummond
A Roesner
A Stoltzfus
Andrey Rzhetsky
AR Robart
AV Sverdlov
AV Sverdlov
C Gille
C Kambach
Christopher Wills
CJ Wilusz
D Schümperli
I Törö
I Törö
IB Rogozin
IB Rogozin
J Yong
JD Beggs
JM Archibald
JS Nielsen
K Nagai
KS Makarova
L Aravind
L Carmel
L Collins
L Lo Conte
M Hetzer
M Hochstrasser
M Seetharaman
MA Schumacher
MP Spiller
MR Lerner
MT Franze de Fernandez
N Toor
P Khusial
PA Sharp
Philip E. Bourne
Philippe Youkharibache
R Edgar
R Tarrío
Ruben E. Valas
S Guindon
S Lin-Chao
S Thore
S Valadkhan
Stella Veretnik
TR Cech
U Narayanan
V Agrawal
W Martin
W Qiu
Y Sato
Publication venue: Public Library of Science
Publication date: 01/01/2009
Field of study

The spliceosome, a sophisticated molecular machine involved in the removal of intervening sequences from the coding sections of eukaryotic genes, appeared and subsequently evolved rapidly during the early stages of eukaryotic evolution. The last eukaryotic common ancestor (LECA) had both complex spliceosomal machinery and some spliceosomal introns, yet little is known about the early stages of evolution of the spliceosomal apparatus. The Sm/Lsm family of proteins has been suggested as one of the earliest components of the emerging spliceosome and hence provides a first in-depth glimpse into the evolving spliceosomal apparatus. An analysis of 335 Sm and Sm-like genes from 80 species across all three kingdoms of life reveals two significant observations. First, the eukaryotic Sm/Lsm family underwent two rapid waves of duplication with subsequent divergence resulting in 14 distinct genes. Each wave resulted in a more sophisticated spliceosome, reflecting a possible jump in the complexity of the evolving eukaryotic cell. Second, an unusually high degree of conservation in intron positions is observed within individual orthologous Sm/Lsm genes and between some of the Sm/Lsm paralogs. This suggests that functional spliceosomal introns existed before the emergence of the complete Sm/Lsm family of proteins; hence, spliceosomal machinery with considerably fewer components than today's spliceosome was already functional

CiteSeerX

Public Library of Science (PLOS)

Ulcerative colitis and irritable bowel patients exhibit distinct abnormalities of the gut microbiota

Abstract Background Previous studies suggest a link between gut microbiota and the development of ulcerative colitis (UC) and irritable bowel syndrome (IBS). Our aim was to investigate any quantitative differences in faecal bacterial compositions in UC and IBS patients compared to healthy controls, and to identify individual bacterial species that contribute to these differences. Methods Faecal microbiota of 13 UC patients, 11 IBS patients and 22 healthy volunteers were analysed by PCR-Denaturing Gradient Gel Electrophoresis (DGGE) using universal and Bacteroides specific primers. The data obtained were normalized using in-house developed statistical method and interrogated by multivariate approaches. The differentiated bands were excised and identified by sequencing the V3 region of the 16S rRNA genes. Results Band profiles revealed that number of predominant faecal bacteria were significantly different between UC, IBS and control group (p < 10-4). By assessing the mean band numbers in UC (37 ± 5) and IBS (39 ± 6), compared to the controls (45 ± 3), a significant decrease in bacterial species is suggested (p = 0.01). There were no significant differences between IBS and UC. Biodiversity of the bacterial species was significantly lower in UC (μ = 2.94, σ = 0.29) and IBS patients (μ = 2.90, σ = 0.38) than controls (μ = 3.25, σ = 0.16; p = 0.01). Moreover, similarity indices revealed greater biological variability of predominant bacteria in UC and IBS compared to the controls (median Dice coefficients 76.1% (IQR 70.9 - 83.1), 73.8% (IQR 67.0 - 77.5) and 82.9% (IQR 79.1 - 86.7) respectively). DNA sequencing of discriminating bands suggest that the presence of <it>Bacteroides vulgatus, B. ovatus, B. uniformis</it>, and <it>Parabacteroides sp</it>. in healthy volunteers distinguishes them from IBS and UC patients. DGGE profiles of Bacteroides species revealed a decrease of Bacteroides community in UC relative to IBS and controls. Conclusion Molecular profiling of faecal bacteria revealed abnormalities of intestinal microbiota in UC and IBS patients, while different patterns of Bacteroides species loss in particular, were associated with UC and IBS.</p

University of East Anglia digital repository

Inhibition of nuclear factor kappa-B signaling reduces growth in medulloblastoma in vivo

Abstract Background Medulloblastoma is a highly malignant pediatric brain tumor that requires surgery, whole brain and spine irradiation, and intense chemotherapy for treatment. A more sophisticated understanding of the pathophysiology of medulloblastoma is needed to successfully reduce the intensity of treatment and improve outcomes. Nuclear factor kappa-B (NFκB) is a signaling pathway that controls transcriptional activation of genes important for tight regulation of many cellular processes and is aberrantly expressed in many types of cancer. Methods To test the importance of NFκB to medulloblastoma cell growth, the effects of multiple drugs that inhibit NFκB, pyrrolidine dithiocarbamate, diethyldithiocarbamate, sulfasalazine, curcumin and bortezomib, were studied in medulloblastoma cell lines compared to a malignant glioma cell line and normal neurons. Expression of endogenous NFκB was investigated in cultured cells, xenograft flank tumors, and primary human tumor samples. A dominant negative construct for the endogenous inhibitor of NFκB, IκB, was prepared from medulloblastoma cell lines and flank tumors were established to allow specific pathway inhibition. Results We report high constitutive activity of the canonical NFκB pathway, as seen by Western analysis of the NFκB subunit p65, in medulloblastoma tumors compared to normal brain. The p65 subunit of NFκB is extremely highly expressed in xenograft tumors from human medulloblastoma cell lines; though, conversely, the same cells in culture have minimal expression without specific stimulation. We demonstrate that pharmacological inhibition of NFκB in cell lines halts proliferation and leads to apoptosis. We show by immunohistochemical stain that phosphorylated p65 is found in the majority of primary tumor cells examined. Finally, expression of a dominant negative form of the endogenous inhibitor of NFκB, dnIκB, resulted in poor xenograft tumor growth, with average tumor volumes 40% smaller than controls. Conclusions These data collectively demonstrate that NFκB signaling is important for medulloblastoma tumor growth, and that inhibition can reduce tumor size and viability in vivo. We discuss the implications of NFκB signaling on the approach to managing patients with medulloblastoma in order to improve clinical outcomes.</p

TBK1: a new player in ALS linking autophagy and neuroinflammation.

Author: A Chio
A Freischmidt
A Goncalves
A Larabi
AC Bowling
B Boland
B Richter
C Pottier
C Zhang
CH Jung
D Tu
D Xu
DR Rosen
E Helgason
ET Cirulli
F Fecto
F Ikeda
F Li
G Borghero
G Matsumoto
GM Morotz
H Maruyama
H Nakashima
I Ber Le
J Cui
J Kong
J Li
J Liu
J Magrane
J Yu
James A. Oakes
JG O'Rourke
JH Son
JK Lee
JM Heo
JY Kim
JY Lee
KJ Spiller
KL Williams
M DeJesus-Hernandez
M Herman
M Komatsu
M Lazarou
M Pilli
M Uhlen
Maria C. Davies
Mark O. Collins
MJ Lindberg
MP Mattson
MS Awadalla
N Mizushima
N Morimoto
N Suzuki
NA Sutedja
O Kann
O Komine
OM Peters
PA Carpentier
PM Sullivan
R Ritch
R Roubenoff
RG Miller
S Kimura
S Pillai
S Sasaki
S Sasaki
S Zarei
T Hara
T Kawai
TL Thurston
X Ma
Y Ichimura
Y Kiriyama
YB Lee
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2017
Field of study

Amyotrophic lateral sclerosis (ALS) is an adult-onset neurodegenerative disorder affecting motor neurons, resulting in progressive muscle weakness and death by respiratory failure. Protein and RNA aggregates are a hallmark of ALS pathology and are thought to contribute to ALS by impairing axonal transport. Mutations in several genes known to contribute to ALS result in deposition of their protein products as aggregates; these include TARDBP, C9ORF72, and SOD1. In motor neurons, this can disrupt transport of mitochondria to areas of metabolic need, resulting in damage to cells and can elicit a neuroinflammatory response leading to further neuronal damage. Recently, eight independent human genetics studies have uncovered a link between TANK-binding kinase 1 (TBK1) mutations and ALS. TBK1 belongs to the IKK-kinase family of kinases that are involved in innate immunity signaling pathways; specifically, TBK1 is an inducer of type-1 interferons. TBK1 also has a major role in autophagy and mitophagy, chiefly the phosphorylation of autophagy adaptors. Several other ALS genes are also involved in autophagy, including p62 and OPTN. TBK1 is required for efficient cargo recruitment in autophagy; mutations in TBK1 may result in impaired autophagy and contribute to the accumulation of protein aggregates and ALS pathology. In this review, we focus on the role of TBK1 in autophagy and the contributions of this process to the pathophysiology of ALS

White Rose Research Online

Tissue engineering of functional articular cartilage: the current status

Author: A Asanbaeva
A Barbero
A Petit
A Yasuda
AA Worster
AH Huang
AJ Salgado
AN Buxton
AT Mehlhorn
BA Byers
BD Elder
BD Elder
BG Sengers
BG Sengers
BG Sengers
BO Diekman
BP Flynn
BT Estes
C Bari De
C Chung
C Chung
C Chung
C Hidaka
C Huang
C Kaps
C Seifarth
CA Arevalo-Silva
CB Foldager
CC Donkelaar van
CG Jeong
CG Williams
CM Revell
Corrinus C. van Donkelaar
CT Buckley
D Eyrich
DJ Kelly
DJ Responte
DL Cohen
DL Hicks
DM Yoon
DM Yoon
DR Wagner
E Grimaud
E Steck
E Volkmer
EB Hunziker
EB Hunziker
EG Lima
EG Lima
EJ Caterson
EM Darling
EM Darling
EM Darling
EM Darling
F Barry
F Guilak
FT Moutos
G Bentley
G Candiani
G Chen
G Chen
GH Welsch
GI Im
GM Williams
H Koga
HJ Kim
I Sekiya
IE Erickson
J Bujia
J Fischer
J Heyland
J Malda
J Malda
J Malda
J Xu
JA Buckwalter
JA Burdick
JC Hu
JC Hu
JD Kisiday
JD Kisiday
JL Puetzer
JM Pestka
JR Owen
JS Temenoff
K Miyanishi
K Miyanishi
K Sakao
K Wiegandt
Keita Ito
KH Chua
KJ Gooch
KL Spiller
KW Ng
KW Ng
KW Ng
KW Ng
L Bian
L Bian
L Bian
L Meinel
L Song
LA Solchaga
LE Freed
LH Nguyen
LH Nguyen
Linda Kock
LM Kock
LM Kock
M Kawanishi
M Khoshgoftar
M Pei
M Sun
M Takagi
MA Rice
MA Wimmer
MC Ronziere
MC Turnhout van
ML Alves da Silva
MP Lutolf
N Indrawattana
N Saeidi
N Veilleux
NG Genes
P Angele
P Giannoni
P Kraan van der
PC Kreuz
Q Li
R Ogawa
R Shirazi
R Shirazi
R Wenger
RK Korhonen
RL Mauck
RL Mauck
RL Mauck
RL Mauck
RL Mauck
RM Coleman
RM Natoli
RM Schulz
RM Schulz
S Boeuf
S Marlovits
S Miot
S Munirah
S Nuernberger
S Strobel
S Terada
SC Chang
SD Thorpe
SD Waldman
SD Waldman
SH Elder
SH Park
SJ Bryant
SJ Bryant
SL Bevill
SM Klisch
SM Lien
SN Redman
T Blunk
T Dehne
T Fukumoto
T Hennig
T Kurth
TA Kelly
TAE Ahmed
TBF Woodfield
TI Morales
TJ Klein
TJ Klein
TJ Klein
TJ Klein
TK Kim
TP Appelman
TT Chowdhury
UR Goessler
UR Goessler
V Prabhakar
W Schuurman
W Wilson
W Wilson
W-JW-J Li
WC Puelacher
Y Ikada
Y Park
Y Park
Y Wang
Y Xiang
YM Bastiaansen-Jenniskens
YM Jenniskens
ZJ Luo
Publication venue: Springer-Verlag
Publication date: 01/01/2011
Field of study

Osteoarthritis is a degenerative joint disease characterized by pain and disability. It involves all ages and 70% of people aged >65 have some degree of osteoarthritis. Natural cartilage repair is limited because chondrocyte density and metabolism are low and cartilage has no blood supply. The results of joint-preserving treatment protocols such as debridement, mosaicplasty, perichondrium transplantation and autologous chondrocyte implantation vary largely and the average long-term result is unsatisfactory. One reason for limited clinical success is that most treatments require new cartilage to be formed at the site of a defect. However, the mechanical conditions at such sites are unfavorable for repair of the original damaged cartilage. Therefore, it is unlikely that healthy cartilage would form at these locations. The most promising method to circumvent this problem is to engineer mechanically stable cartilage ex vivo and to implant that into the damaged tissue area. This review outlines the issues related to the composition and functionality of tissue-engineered cartilage. In particular, the focus will be on the parameters cell source, signaling molecules, scaffolds and mechanical stimulation. In addition, the current status of tissue engineering of cartilage will be discussed, with the focus on extracellular matrix content, structure and its functionality

Repository TU/e

Pure OAI Repository

Search for High-Mass Resonances Decaying to τν in pp Collisions at √s=13 TeV with the ATLAS Detector

Author: Aaboud M
Aad G
Abbott B
Abdinov O
Abeloos B
Abidi SH
AbouZeid OS
Abraham NL
Abramowicz H
Abreu H
Abulaiti Y
Acharya BS
Adachi S
Adamczyk L
Adelman J
Adersberger M
Adye T
Affolder AA
Afik Y
Agheorghiesei C
Aguilar-Saavedra JA
Ahlen SP
Ahmadov F
Aielli G
Akatsuka S
Akesson TPA
Akilli E
Akimov AV
Alberghi GL
Albert J
Albicocco P
Alconada Verzini MJ
Alderweireldt S
Aleksa M
Aleksandrov IN
Alexa C
Alexander G
Alexopoulos T
Alhroob M
Ali B
Aliev M
Alimonti G
Alison J
Alkire SP
Allaire C
Allbrooke BMM
Allen BW
Allport PP
Aloisio A
Alonso A
Alonso F
Alpigiani C
Alshehri AA
Alstaty MI
Alvarez Gonzalez B
Alvarez Piqueras D
Alviggi MG
Amadio BT
Amaral Coutinho Y
Ambroz L
Amelung C
Amidei D
Amor Dos Santos SP
Amoroso S
Amrouche CS
Anastopoulos C
Ancu LS
Andari N
Andeen T
Anders CF
Anders JK
Anderson KJ
Andreazza A
Andrei V
Angelidakis S
Angelozzi I
Angerami A
Anisenkov AV
Annovi A
Antel C
Anthony MT
Antonelli M
Antrim DJ
Anulli F
Aoki M
Arabidze G
Arai Y
Araque JP
Araujo Ferraz V
Araujo Pereira R
Araya S Tapia
Arce ATH
Ardell RE
Arduh FA
Arguin J-F
Argyropoulos S
Armadans R Caminal
Armbruster AJ
Armitage LJ
Arnaez O
Arnold H
Arratia M
Arslan O
Artamonov A
Artoni G
Artz S
Asai S
Asbah N
Ashkenazi A
Asimakopoulou EM
Asquith L
Assamagan K
Astalos R
Astigarraga ME Pozo
Atkin RJ
Atkinson M
Atlay NB
Augsten K
Avolio G
Avramidou R
Axen B
Ayoub MK
Azuelos G
Baas AE
Baca MJ
Bachacou H
Bachas K
Backes M
Bagnaia P
Bahmani M
Bahrasemani H
Baines JT
Bajic M
Baker OK
Bakker PJ
Baldin EM
Balek P
Balli F
Balunas WK
Banas E
Bandyopadhyay A
Banerjee Sw
Bannoura AAE
Barak L
Barbe WM
Barberio EL
Barberis D
Barbero M
Barillari T
Barisits M-S
Barkeloo JT
Barklow T
Barlow N
Barnea R
Barnes SL
Barnett BM
Barnett RM
Barnovska-Blenessy Z
Baroncelli A
Barone G
Barr AJ
Barranco Navarro L
Barreiro Guimaraes da Costa J
Barreiro F
Bartoldus R
Barton AE
Bartos P
Basalaev A
Bassalat A
Bates RL
Batista SJ
Batley JR
Battaglia M
Bauce M
Bauer F
Bauer KT
Bawa HS
Beacham JB
Beattie MD
Beau T
Beauchemin PH
Bechtle P
Beck HC
Beck HP
Becker K
Becker M
Becot C
Beddall A
Beddall AJ
Bednyakov VA
Bedognetti M
Bee CP
Beermann TA
Begalli M
Begel M
Behera A
Behr JK
Bell AS
Bella G
Bella L Aperio
Bellagamba L
Bellerive A
Bellomo M
Belotskiy K
Belyaev NL
Benary O
Benchekroun D
Bender M
Benekos N
Benhammou Y
Benitez J
Benjamin DP
Benoit M
Bensinger JR
Bentvelsen S
Beresford L
Beretta M
Berge D
Berger N
Bergsten LJ
Beringer J
Berlendis S
Berlingen J Montejo
Bernard NR
Bernardi G
Bernius C
Bernlochner FU
Berry T
Berta P
Bertella C
Bertoli G
Bertram IA
Bertsche C
Besjes GJ
Bessner M
Besson N
Bethani A
Bethke S
Betti A
Bevan AJ
Beyer J
Bianchi RM
Biebel O
Biedermann D
Bielski R
Bierwagen K
Biesuz NV
Biglietti M
Billoud TRV
Bindi M
Bingul A
Bini C
Biondi S
Bisanz T
Bittrich C
Bjergaard DM
Black JE
Black KM
Blair RE
Blazek T
Bloch I
Blocker C
Blue A
Blumenschein U
Blunier Dr
Bobbink GJ
Bobrovnikov VS
Bocchetta SS
Bocci A
Bock C
Boeriu OE Vickey
Boerner D
Bogavac D
Bogdanchikov AG
Bohm C
Boisvert V
Bokan P
Bold T
Boldyrev AS
Bolz AE
Bomben M
Bona M
Bonilla JS
Boonekamp M
Borisov A
Borissov G
Bortfeldt J
Bortoletto D
Bortolotto V
Boscherini D
Bosman M
Boudreau J
Bouhova-Thacker EV
Boumediene D
Bourdarios C
Boutle SK
Boveia A
Boyd J
Boyko IR
Bozson AJ
Bracinik J
Brahimi N
Brandt A
Brandt G
Brandt O
Braren F
Bratzler U
Brau B
Brau JE
Brendlinger K
Brennan AJ
Brenner L
Brenner R
Bressler S
Bret M Cano
Briglin DL
Bristow TM
Britton D
Britzger D
Brock I
Brock R
Brooijmans G
Brooks T
Brooks WK
Brost E
Broughton JH
Bruncko D
Bruni A
Bruni G
Bruni LS
Bruno S
Brunt BH
Bruschi M
Bruscino N
Bryant P
Bryngemark L
Buanes T
Buat Q
Buchholz P
Buckley AG
Budagov IA
Buehrer F
Buescher D
Buescher V
Bugge MK
Bulekov O
Bullock D
Burch TJ
Burdin S
Burgard CD
Burger AM
Burghgrave B
Burka K
Burke S
Burmeister I
Burr JTP
Buschmann E
Bussey P
Butler JM
Buttar CM
Butterworth JM
Butti P
Buttinger W
Buzatu A
Buzykaev AR
Bylund O Bessidskaia
Cabras G
Cabrera Urban S
Caforio D
Cai H
Cairo VMM
Cakir I Turk
Cakir O
Calace N
Calafiura P
Calandri A
Calderini G
Calfayan P
Callea G
Caloba LP
Calvente Lopez S
Calvet D
Calvet S
Calvet TP
Calvetti M
Camarda S
Camarri P
Cameron D
Camincher C
Campana S
Campanelli M
Camplani A
Campoverde A
Canale V
Cantero J
Cao T
Cao Y
Caprini I
Caprini M
Capua M
Carbone RM
Cardarelli R
Cardillo F
Carli I
Carli T
Carlino G
Carlson BT
Carminati L
Carney RMD
Caron S
Carquin E
Carra S
Carrillo-Montoya GD
Casadei D
Casado MP
Casha AF
Casolino M
Casper DW
Castelijn R
Castillo Gimenez V
Castillo LR Flores
Castro NF
Catinaccio A
Catmore JR
Cattai A
Caudron J
Cavaliere V
Cavallaro E
Cavalli D
Cavalli-Sforza M
Cavasinni V
Celebi E
Ceradini F
Cerda Alberich L
Cerqueira AS
Cerri A
Cerrito L
Cerutti F
Cervelli A
Cetin SA
Chafaq A
Chakraborty D
Chan SK
Chan WS
Chan YL
Chang P
Chapman JD
Charlton DG
Chau CC
Chavez Barajas CA
Che S
Chegwidden A
Chekanov S
Chekulaev SV
Chelkov GA
Chelstowska MA
Chen C
Chen C
Chen H
Chen J
Chen J
Chen S
Chen S
Chen X
Chen Y
Chen Y-H
Cheng HC
Cheng HJ
Cheplakov A
Cheremushkina E
Cheu E
Cheung K
Chevalier L
Chiarella V
Chiarelli G
Chiodini G
Chisholm AS
Chitan A
Chiu I
Chiu YH
Chizhov MV
Choi K
Chomont AR
Chouridou S
Chow YS
Christodoulou V
Chu MC
Chudoba J
Chuinard AJ
Chwastowski JJ
Chytka L
Cinca D
Cindro V
Cioara IA
Ciocio A
Cirotto F
Citron ZH
Citterio M
Clark A
Clark MR
Clark PJ
Clarke RN
Clement C
Coadou Y
Cobal M
Coccaro A
Cochran J
Colasurdo L
Cole B
Colijn AP
Collaboration ATLAS
Collot J
Conde Muino P
Coniavitis E
Connell SH
Connelly IA
Constantinescu S
Conventi F
Cooper-Sarkar AM
Corga K De Vasconcelos
Cormier F
Cormier KJR
Cornell S Diez
Corradi M
Correia AM Henriques
Corrigan EE
Corriveau F
Cortes-Gonzalez A
Costa MJ
Costanzo D
Cottin G
Cowan G
Cox BE
Crane J
Cranmer K
Crawley SJ
Creager RA
Cree G
Crepe-Renaudin S
Crescioli F
Cristinziani M
Croft V
Crosetti G
Cueto A
Cukierman AR
Curatolo M
Cuth J
Czekierda S
Czodrowski P
D'amen G
D'Auria S
D'eramo L
D'Onofrio M
Da Cunha Sargedas De Sousa MJ
Da Via C
Dabrowski W
Dado T
Dahbi S
Dai T
Dale O
Dallaire F
Dallapiccola C
Dam M
Damazio D Oliveira
Dandoy JR
Daneri MF
Dang NP
Dann NS
Danninger M
Dao V
Darbo G
Darmora S
Dartsi O
Dattagupta A
Daubney T
Davey W
David C
Davidek T
Davis DR
Dawe E
Dawson I
de Asmundis R
De Benedetti A
De Bruin PH Sales
De Castro S
De Cecco S
De Groot N
de Jong P
De la Torre H
de Lima DE Ferreira
De Lorenzi F
De Maria A
De Pedis D
De Regie JB De Vivie
de Renstrom PA Bruckman
De Salvo A
De Sanctis U
De Santo A
De K
Debenedetti C
Dedovich DV
Dehghanian N
Del Gaudio M
Del Peso J
Delgove D
Deliot F
Delitzsch CM
Dell'Acqua A
Dell'Asta L
Della Pietra M
della Volpe D
Delmastro M
Delporte C
Delsart PA
DeMarco DA
Demers S
Demichev M
Denisov SP
Denysiuk D
Derendarz D
Derkaoui JE
Derue F
Dervan P
Desch K
Deterre C
Dette K
Devesa MR
Deviveiros PO
Dewhurst A
Dhaliwal S
Di Bello FA
Di Ciaccio A
Di Ciaccio L
Di Clemente WK
Di Donato C
Di Girolamo A
Di Micco B
Di Nardo R
Di Petrillo KF
Di Simone A
Di Sipio R
Di Valentino D
Diaconu C
Diamond M
Dias do Vale T
Dias FA
Diaz MA
Dickinson J
Diehl EB
Dietrich J
Dimitrievska A
Dingfelder J
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Gorbounov PA
Gordon HA
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Goshaw AT
Gostkin MI
Gottardo CA
Goudet CR
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Goussiou AG
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Graham EC
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Gutschow C
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Hallewell GD
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Hansen E
Hansen JB
Hansen JD
Hansen MC
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Hard AS
Harenberg T
Harkusha S
Harrison PF
Hartmann NM
Hasegawa Y
Hasib A
Hassani S
Haug S
Hauser R
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Havener LB
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Hawkes CM
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Hejbal J
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Herbert GH
Herde H
Herget V
Hernandez D Paredes
Herr H
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Hervas L
Herwig TC
Hesketh GG
Hessey NP
Hetherly JW
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Hirschbuehl D
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Hladik O
Hlaluku DR
Hoad X
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Hoeferkamp MR
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Holmes TR
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Hooberman BH
Hopkins WH
Horii Y
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Hubacek Z
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Hughes EW
Huhtinen M
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Ibragimov I
Iconomidou-Fayard L
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Igonkina O
Iguchi R
Iizawa T
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Ippolito V
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Kano Y
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Karentzos E
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Karyukhin AN
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Kladiva E
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Kondo T
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Kono T
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Konya B
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Korolkova EV
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Kourlitis E
Kouskoura V
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Kowalski TZ
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Lipniacka A
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Madden WD Breaden
Mader WF
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Milov A
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Noccioli E Benhar
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Nooney T
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Norjoharuddeen N
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Novgorodova O
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Zobernig G
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Zoch K
Zorbas TG
Zou R
Zu Theenhausen H Meyer
zur Nedden M
Zwalinski L
Publication venue: 'American Physical Society (APS)'
Publication date: 01/01/2018
Field of study

A search for high-mass resonances decaying to τν using proton-proton collisions at √s=13 TeV produced by the Large Hadron Collider is presented. Only τ-lepton decays with hadrons in the final state are considered. The data were recorded with the ATLAS detector and correspond to an integrated luminosity of 36.1 fb−1. No statistically significant excess above the standard model expectation is observed; model-independent upper limits are set on the visible τν production cross section. Heavy W′ bosons with masses less than 3.7 TeV in the sequential standard model and masses less than 2.2–3.8 TeV depending on the coupling in the nonuniversal G(221) model are excluded at the 95% credibility level

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Combined measurement of differential and total cross sections in the H → γγ and the H → ZZ* → 4ℓ decay channels at s=13 TeV with the ATLAS detector

Author: Aaboud M
Aad G
Abbott B
Abdinov O
Abeloos B
Abhayasinghe DK
Abidi SH
Abouzeid OS
Abraham NL
Abramowicz H
Abreu H
Abulaiti Y
Acharya BS
Adachi S
Adamczyk L
Adelman J
Adersberger M
Adiguzel A
Adye T
Affolder AA
Afik Y
Agheorghiesei C
Aguilar-Saavedra JA
Ahmadov F
Aielli G
Akatsuka S
Akilli E
Akimov AV
Alberghi GL
Albert J
Albicocco P
Alconada Verzini MJ
Alderweireldt S
Aleksa M
Aleksandrov IN
Alexa C
Alexopoulos T
Alhroob M
Ali B
Alimonti G
Alison J
Alkire SP
Allaire C
Allbrooke BMM
Allen BW
Allport PP
Aloisio A
Alonso A
Alonso F
Alpigiani C
Alshehri AA
Alstaty MI
Alvarez Gonzalez B
Alviggi MG
Amadio BT
Amaral Coutinho Y
Ambroz L
Amelung C
Amidei D
Amor Dos Santos SP
Amoroso S
Amrouche CS
Anastopoulos C
Ancu LS
Andari N
Andeen T
Anders CF
Anders JK
Anderson KJ
Andreazza A
Andrei V
Anelli CR
Angelidakis S
Angelozzi I
Angerami A
Anisenkov AV
Annovi A
Antel C
Anthony MT
Antonelli M
Antrim DJA
Anulli F
Aoki M
Aperio Bella L
Arabidze G
Arai Y
Araque JP
Araujo Ferraz V
Araujo Pereira R
Arce ATH
Ardell RE
Arduh FA
Arguin J-F
Argyropoulos S
Armbruster AJ
Armitage LJ
Armstrong A
Arnaez O
Arnold H
Arratia M
Arslan O
Artamonov A
Artoni G
Artz S
Asai S
Asbah N
Ashkenazi A
Asimakopoulou EM
Asquith L
Assamagan K
Astalos R
Atkin RJ
Atkinson M
Atlas Collaboration
Atlay NB
Augsten K
Avolio G
Avramidou R
Axen B
Ayoub MK
Azuelos G
Baas AE
Baca MJ
Bachacou H
Bachas K
Backes M
Bagnaia P
Bahmani M
Bahrasemani H
Bailey AJ
Baines JT
Bajic M
Bakalis C
Baker OK
Bakker PJ
Bakshi Gupta D
Baldin EM
Balek P
Balli F
Balunas WK
Balz J
Banas E
Bandyopadhyay A
Banerjee S
Bannoura AAE
Barak L
Barbe WM
Barberio EL
Barberis D
Barbero M
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Butler JM
Buttar CM
Butterworth JM
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Buzykaev AR
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Cabras G
Cabrera Urbán S
Caforio D
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Calace N
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Calandri A
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Caloba LP
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Calvet D
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Camincher C
Campana S
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Campoverde A
Canale V
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Cantero J
Cao T
Cao Y
Capeans Garrido MDM
Caprini I
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Capua M
Carbone RM
Cardarelli R
Cardillo FC
Carli I
Carli T
Carlino G
Carlson BT
Carminati L
Carney RMD
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Carquin E
Carrillo-Montoya GD
Carrá S
Casadei D
Casado MP
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Castillo Gimenez V
Castillo FL
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Cavaliere V
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Celebi E
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Cervelli A
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Chafaq A
Chakraborty D
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Chapman JD
Charlton DG
Chau CC
Chavez Barajas CA
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Chegwidden A
Chekanov S
Chekulaev SV
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Chen C
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Chen X
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Cheng HC
Cheng HJ
Cheplakov A
Cheremushkina E
Cherkaoui El Moursli R
Cheu E
Cheung K
Chevalier L
Chiarella V
Chiarelli G
Chiodini G
Chisholm AS
Chitan A
Chiu I
Chiu YH
Chizhov MV
Choi K
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Chow YS
Christodoulou V
Chu MC
Chudoba J
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Chytka L
Cinca D
Cindro V
Cioară IA
Ciocio A
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Citron ZH
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Clark A
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Clement C
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Coimbra AEC
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Cooper-Sarkar AM
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Costa MJ
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Czekierda S
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D'Onofrio A
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Da Cunha Sargedas De Sousa MJ
Da Via C
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Dado T
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Dallapiccola C
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Daneri MF
Dang NP
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Dao V
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Darmora S
Dartsi O
Dattagupta A
Daubney T
Davey W
David C
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Davis DR
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De Benedetti A
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De Cecco S
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De Jong P
De La Torre H
De Lorenzi F
De Maria A
De Pedis D
De Salvo A
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De Vivie De Regie JB
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Del Peso J
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Delitzsch CM
Dell'Acqua A
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Della Pietra M
Della Volpe D
Delmastro M
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Denysiuk D
Derendarz D
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Deviveiros PO
Dewhurst A
Dhaliwal S
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Di Ciaccio A
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Di Clemente WK
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Di Girolamo A
Di Micco B
Di Nardo R
Di Petrillo KF
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Diehl EB
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Dimitrievska A
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Djuvsland JI
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Duarte-Campderros J
Dubinin F
Dubovsky M
Dubreuil A
Duchovni E
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Ducourthial A
Ducu OA
Duda D
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Dudder AC
Duffield EM
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Dumitriu AE
Duncan AK
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Duperrin A
Duran Yildiz H
Durglishvili A
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Dutta B
Duvnjak D
Dyndal M
Dysch S
Dziedzic BS
Díez Cornell S
Dührssen M
Dülsen C
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Ecker KM
Edgar RC
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El Kosseifi R
Ellajosyula V
Ellert M
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Ennis JS
Epland MB
Erdmann J
Ereditato A
Errede S
Escalier M
Escobar C
Esposito B
Estrada Pastor O
Etienvre AI
Etzion E
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Fabiani V
Facini G
Faisca Rodrigues Pereira RM
Fakhrutdinov RM
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Falke PJ
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Faucci Giannelli M
Favareto A
Fawcett WJ
Fayard L
Fedin OL
Fedorko W
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Feng C
Feng EJ
Feng M
Fenton MJ
Fenyuk AB
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Ferrari R
Ferreira De Lima DE
Ferrer A
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Ferretti C
Fiedler F
Filipčič A
Filthaut F
Finelli KD
Fiolhais MCN
Fiorini L
Fischer C
Fisher WC
Flaschel N
Fleck I
Fleischmann P
Fletcher RRM
Flick T
Flierl BM
Flores Castillo LR
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Fomin N
Forcolin GT
Formica A
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Foster AG
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Gavrilenko IL
Gavrilyuk A
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Gazis EN
Gee CNP
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Gkialas I
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González De La Hoz S
Gonçalo R
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Gordon HA
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Gostkin MI
Gottardo CA
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Graham EC
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Konya B
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Mellenthin JD
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Zur Nedden M
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Álvarez Piqueras D
Åkesson TPA
Šfiligoj T
Ženiš T
Živković L
Publication venue: Elsevier
Publication date: 01/01/2018
Field of study

A combined measurement of differential and inclusive total cross sections of Higgs boson production is performed using 36.1 fb−1 of 13 TeV proton–proton collision data produced by the LHC and recorded by the ATLAS detector in 2015 and 2016. Cross sections are obtained from measured H→γγ and H→ZZ*(→4ℓ event yields, which are combined taking into account detector efficiencies, resolution, acceptances and branching fractions. The total Higgs boson production cross section is measured to be 57.0−5.9 +6.0 (stat.) −3.3 +4.0 (syst.) pb, in agreement with the Standard Model prediction. Differential cross-section measurements are presented for the Higgs boson transverse momentum distribution, Higgs boson rapidity, number of jets produced together with the Higgs boson, and the transverse momentum of the leading jet. The results from the two decay channels are found to be compatible, and their combination agrees with the Standard Model predictions

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Anatomy of the sign-problem in heavy-dense QCD

Author: Adam E Romero
Aranda C Padilla
Arjanovic MM
Armadans R Caminal
Astigarraga ME Pozo
Barajas CA Chavez
Bechtle P
Beck HP
Becker K
Becker M
Beckingham M
Becot C
Beddall A
Beddall AJ
Bednyakov VA
Bedognetti M
Bee CP
Beemster LJ
Beermann TA
Begel M
Behr JK
Belanger-Champagne C
Bell AS
Bella G
Bellagamba L
Bellerive A
Bellomo M
Belotskiy K
Beltramello O
Belyaev NL
Benary O
Benchekroun D
Bender M
Bendtz K
Benekos N
Benhammou Y
Benitez J
Benjamin DP
Bensinger JR
Bentvelsen S
Beresford L
Beretta M
Berge D
Berger N
Berghaus F
Beringer J
Berlendis S
Berlingen J Montejo
Bernard NR
Bernius C
Bernlochner FU
Berry T
Berta P
Bertella C
Bertoli G
Bertolucci F
Bertram IA
Bertsche C
Bertsche D
Besjes GJ
Bessner M
Besson N
Betancourt C
Bethke S
Bevan AJ
Bhimji W
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Caforio D
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Canepa A
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Castillo I Santoyo
Castilloa LR Flores
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Chafaq A
Chakraborty D
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Charlton DG
Chatterjee A
Chau CC
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Chegwidden A
Chekanov S
Chekulaev SV
Chelkov GA
Chelstowska MA
Chen C
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Chen X
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Cheng HC
Cheng HJ
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Cheplakov A
Cheremushkina E
Cherkaoui El Moursli R
Chernyatin V
Cheu E
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Chiarella V
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Christodoulou V
Chromek-Burckhart D
Chudoba J
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Cinca D
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Clement C
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Cortes-Gonzalez A
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Da Costa J Goncalves Pinto Firmino
Da Cunha Sargedas De Sousa MJ
Da Via C
Dabrowski W
Dai T
Dale O
Dallaire F
Dallapiccola C
Dam M
Damazio D Oliveira
Dandoy JR
Dang NP
Daniells AC
Dann NS
Danninger M
Dao V
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Darmora S
Dassoulas J
Dattagupta A
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David C
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Davygora Y
Dawe E
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Daya-Ishmukhametova RK
de Andrade Filho L Manhaes
De Asmundisa R
De Benedetti A
De Bruin PH Sales
De Castro S
De Cecco S
De Groot N
de Jong P
De la Torre H
de Lima DE Ferreira
De Lorenzi F
De Mendizabal J Bilbao
De Pedis D
De Regie JB De Vivie
de Renstrom PA Bruckman
De Salvo A
De Sanctis U
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Debbe R
Debenedetti C
Dedovich DV
Deigaard I
Del Peso J
Del Prete T
Delgove D
Deliot F
Delitzsch CM
Deliyergiyev M
Dell'Acqua A
Dell'Asta L
Dell'Orso M
Della Pietra M
della Volpe D
Delmastro M
Delsart PA
Deluca C
DeMarco DA
Demers S
Demichev M
Demilly A
Denisov SP
Denysiuk D
Derendarz D
Derkaoui JE
Derue F
Dervan P
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Deterre C
Dette K
Deviveiros PO
Dewhurst A
Dhaliwal S
Di Ciaccio A
Di Ciaccio L
Di Clemente WK
Di Donato C
Di Girolamo A
Di Girolamo B
Di Micco B
Di Nardo R
Di Simone A
Di Sipio R
Di Valentino D
Diaconu C
Diamond M
Dias FA
Diaz MA
Diehl EB
Dietrich J
Diglio S
Dimitrievska A
Dingfelder J
Dita P
Dita S
Dittus F
Djama F
Djobava T
Djuvsland JI
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Dobos D
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Doglioni C
Dohmae T
Dolejsi J
Dolezal Z
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Donadelli M
Donati S
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Donini J
Donszelmann T Cuhadar
Dopke J
Doria A
Dova MT
Doyle AT
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Du Y
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Duchovni E
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Ducu OA
Duda D
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Duflot L
Duguid L
Duhrssen M
Dunford M
Duren M
Durglishvili A
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Dutta B
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Edwards NC
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Einsweiler K
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El Kacimi M
Ellajosyula V
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Emeliyanov D
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Endner OC
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Erdmann J
Ereditato A
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Ertel E
Escalier M
Esch H
Escobar C
Esposito B
Etienvre AI
Etzion E
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Fabbri F
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Facini G
Fakhrutdinov RM
Falciano S
Falla RJ
Faltova J
Fang Y
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Farrell S
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Farthouat P
Fassi F
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Favareto A
Fawcett WJ
Fayard L
Fedin OL
Fedorko W
Feigl S
Feligioni L
Feng C
Feng EJ
Feng H
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Feremenga L
Fernandez Martinez P
Ferrando J
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Fincke-Keeler M
Finelli KD
Fiolhaisa MCN
Fiorini L
Firan A
Fischer A
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Fisher WC
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Fleck I
Fleischmann P
Fletcher G
Fletcher GT
Fletcher RRM
Flick T
Floderus A
Flowerdew MJ
Forcolin GT
Formica A
Forti A
Foster AG
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Francavilla P
Franchini M
Francis D
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Gallop BJ
Gallus P
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Garcia BR Mellado
Garcia C
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Garcia RF Naranjo
Garcia-Sciveres M
Gardner RW
Garelli N
Garonne V
Garrido MDM Capeans
Garron Nicolas
Gatti C
Gaudiello A
Gaudio G
Gaur B
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Gavrilenko IL
Gay C
Gaycken G
Gazis EN
Gecse Z
Gee CNP
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Gemme C
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Geng C
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Gerbaudo D
Gershon A
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Giannetti P
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Gibson SM
Gignac M
Gilchriese M
Gillam TPS
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Giordani MP
Giorgi FM
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Gjelsten BK
Gkaitatzis S
Gkialas I
Gkougkousis EL
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Gongadze A
Gonzalez de la Hoz S
Gonzalez-Sevilla S
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Gorbounov PA
Gordon HA
Gorelov I
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Goshaw AT
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Gostkin MI
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Hernandez D Paredes
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Ibragimov I
Iconomidou-Fayard L
Ideal E
Idrissi Z
Iengo P
Igonkina O
Iizawa T
Ikegami Y
Ikeno M
Ilchenko Y
Iliadis D
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Ioannou P
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Ippolito V
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Kantserov VA
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Kapliy A
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Karamaoun A
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Kareem MJ
Karentzos E
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Karpov SN
Karpova ZM
Karthik K
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Karyukhin AN
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Khalil-zada F
Khandanyan H
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Kharlamov AG
Khoo TJ
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Kisielewska D
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Kladiva E
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Koi T
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Komar AA
Komori Y
Kondo T
Kondrashova N
Kono T
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Kotov VM
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Kourkoumelis C
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Yildiz H Duran
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Yuen SPY
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Zhu Y
Zhuang X
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Zimine NI
Zimmermann C
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Zoccoli A
zur Nedden M
Zurzolo G
Zwalinski L
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2016
Field of study

QCD at finite densities of heavy quarks is investigated using the density-of-states method. The phase factor expectation value of the quark determinant is calculated to unprecedented precision as a function of the chemical potential. Results are validated using those from a reweighting approach where the latter can produce a significant signalto-noise ratio. We confirm the particle–hole symmetry at low temperatures, find a strong sign problem at intermediate values of the chemical potential, and an inverse Silver Blaze feature for chemical potentials close to the onset value: here, the phase-quenched theory underestimates the density of the full theory

EDP Sciences OAI-PMH repository (1.2.0)

eScholarship - University of California

UCL Discovery

White Rose Research Online

Performance of missing transverse momentum reconstruction with the ATLAS detector using proton–proton collisions at √s = 13 TeV

Author: Aaboud M
Aad G
Abbott B
Abdinov O
Abeloos B
Abhayasinghe DK
Abidi SH
AbouZeid OS
Abraham NL
Abramowicz H
Abreu H
Abulaiti Y
Acharya BS
Adachi S
Adamczyk L
Adelman J
Adersberger M
Adiguzel A
Adye T
Affolder AA
Afik Y
Agheorghiesei C
Aguilar-Saavedra JA
Ahmadov F
Aielli G
Akatsuka S
Akesson TPA
Akilli E
Akimov AV
Alberghi GL
Albert J
Albicocco P
Alconada Verzini MJ
Alderweireldt S
Aleksa M
Aleksandrov IN
Alexa C
Alexopoulos T
Alhroob M
Ali B
Alimonti G
Alison J
Alkire SP
Allaire C
Allbrooke BMM
Allen BW
Allport PP
Aloisio A
Alonso A
Alonso F
Alpigiani C
Alshehri AA
Alstaty MI
Alvarez Gonzalez B
Alvarez Piqueras D
Alviggi MG
Amadio BT
Amaral Coutinho Y
Ambroz L
Amelung C
Amidei D
Amor Dos Santos SP
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Blumenschein U
Blunier Dr
Bobbink GJ
Bobrovnikov VS
Bocchetta SS
Bocci A
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Bruckman de Renstrom PA
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Buzatu A
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Bylund O Bessidskaia
Cabras G
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Caforio D
Cai H
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Caloba LP
Calvente Lopez S
Calvet D
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Camarda S
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Camincher C
Campana S
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Camplani A
Campoverde A
Canale V
Cantero J
Cao T
Cao Y
Capeans Garrido MDM
Caprini I
Caprini M
Capua M
Carbone RM
Cardarelli R
Cardillo FC
Carli I
Carli T
Carlino G
Carlson BT
Carminati L
Carney RMD
Caron S
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Carra S
Carrillo-Montoya GD
Casadei D
Casado MP
Casha AF
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Casper DW
Castelijn R
Castillo Gimenez V
Castillo FL
Castro NF
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Catmore JR
Cattai A
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Cavaliere V
Cavallaro E
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Cavalli-Sforza M
Cavasinni V
Celebi E
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Cerqueira AS
Cerri A
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Cerutti F
Cervelli A
Cetin SA
Chafaq A
Chakraborty D
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Chapman JD
Charlton DG
Chau CC
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Chekanov S
Chekulaev SV
Chelkov GA
Chelstowska MA
Chen C
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Chen X
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Cheng HC
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Cheplakov A
Cheremushkina E
Cheu E
Cheung K
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Chiarella V
Chiarelli G
Chiodini G
Chisholm AS
Chitan A
Chiu I
Chiu YH
Chizhov MV
Choi K
Chomont AR
Chouridou S
Chow YS
Christodoulou V
Chu MC
Chudoba J
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Chytka L
Cinca D
Cindro V
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Ciocio A
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Citron ZH
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Clark A
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Clark PJ
Clement C
Coadou Y
Cobal M
Coccaro A
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Coimbra AEC
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Collaboration ATLAS
Collot J
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Coniavitis E
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Cooper-Sarkar AM
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Cukierman AR
Cuth J
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Czodrowski P
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D'onofrio A
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Da Cunha Sargedas De Sousa MJ
Da Via C
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Dado T
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Dai T
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Dallapiccola C
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Daneri MF
Dang NP
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Danninger M
Dao V
Darbo G
Darmora S
Dartsi O
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Davis DR
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De Benedetti A
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De Vivie De Regie JB
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Delabat Diaz Y
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Dell'Acqua A
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Della Pietra M
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Denysiuk D
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Deviveiros PO
Dewhurst A
Dhaliwal S
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Di Ciaccio A
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Di Clemente WK
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Di Girolamo A
Di Micco B
Di Nardo R
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Di Valentino D
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Diehl EB
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Dimitrievska A
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Dittus F
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Djuvsland JI
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Dolezal Z
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Dubreuil A
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Ducourthial A
Ducu OA
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Duncan AK
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Etienvre AI
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Faisca Rodrigues Pereira RM
Fakhrutdinov RM
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Fiolhais MCN
Fiorini L
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Flaschel N
Fleck I
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Fletcher RRM
Flick T
Flierl BM
Flores Castillo LR
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Foerster FA
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Gavrilenko IL
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Hernandez Jimenez Y
Herr H
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Hlaluku DR
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Hopkins WH
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Ippolito V
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Ishitsuka M
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Kano Y
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Karentzos E
Karpov SN
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Karyukhin AN
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Kastanas A
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Kisielewska D
Kitali V
Kivernyk O
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Knue A
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Koehler NM
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Kondo T
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Kono T
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Konstantinides V
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Konya B
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Korolkova EV
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Kourkoumelis C
Kourlitis E
Kouskoura V
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Kowalski TZ
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Kulinich YP
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Lin CY
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Lindquist BE
Lionti AL
Lipeles E
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Liss TM
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Little JD
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Lloyd SL
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Loch P
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Lopez Solis A
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Lyu F
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Mamuzic J
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Mankinen KH
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Marley DE
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McLean KD
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McNicol CJ
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Meadows ZA
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Mellenthin JD
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Milosavljevic M Vranjes
Milov A
Milstead DA
Minaenko AA
Minano Moya M
Minashvili IA
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Minegishi Y
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Mistry KP
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Mjoernmark JU
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Monticelli F
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Myagkov AG
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Nakahama Y
Nakamura K
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Nakano I
Nanjo H
Napolitano F
Naranjo Garcia RF
Narayan R
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Naryshkin I
Naumann T
Navarro G
Nayyar R
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Nechaeva PY
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Newman PR
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Noccioli E Benhar
Noguchi Y
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Nomura MA
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Norjoharuddeen N
Novak T
Novgorodova O
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Oliveira Damazio D
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Wyatt TR
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Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2018
Field of study

The performance of the missing transverse momentum (EmissT) reconstruction with the ATLAS detector is evaluated using data collected in proton–proton collisions at the LHC at a centre-of-mass energy of 13 TeV in 2015. To reconstruct EmissT, fully calibrated electrons, muons, photons, hadronically decaying τ -leptons, and jets reconstructed from calorimeter energy deposits and charged-particle tracks are used. These are combined with the soft hadronic activity measured by reconstructed charged-particle tracks not associated with the hard objects. Possible double counting of contributions from reconstructed charged-particle tracks from the inner detector, energy deposits in the calorimeter, and reconstructed muons from the muon spectrometer is avoided by applying a signal ambiguity resolution procedure which rejects already used signals when combining the various EmissT contributions. The individual terms as well as the overall reconstructed EmissT are evaluated with various performance metrics for scale (linearity), resolution, and sensitivity to the data-taking conditions. The method developed to determine the systematic uncertainties of the EmissT scale and resolution is discussed. Results are shown based on the full 2015 data sample corresponding to an integrated luminosity of 3.2 fb−1

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