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694 research outputs found

The small-nucleolar RNAs commonly used for microRNA normalisation correlate with tumour pathology and prognosis

Author: A Git
A Killian
A L Harris
A Markou
A Ramachandran
AB Hui
AB Hui
B Weigelt
C Camps
C Camps
C Desmedt
C West
CA Hudis
CN Hansen
DM Stults
F M Buffa
FM Buffa
G Betts
G Finak
GB van den Broek
H E Gee
H Sheldon
HE Gee
HE Gee
HJ Peltier
J Homer
J Lee
J Ragoussis
J van Riggelen
J Vandesompele
JB Welsh
JR Kerr
JS Mattick
JW Catto
KH Chang
LX Yan
M Mourtada-Maarabouni
M Patil
M Taylor
NJ Beasley
P Wirapati
PT Simpson
R Hummel
R Leek
S Loi
S Winter
T Kino
T Kiss
T Sorlie
V Kaklamani
W Roa
XY Dong
Publication venue: Nature Publishing Group
Publication date: 01/01/2011
Field of study

Background:To investigate small-nucleolar RNAs (snoRNAs) as reference genes when measuring miRNA expression in tumour samples, given emerging evidence for their role in cancer.Methods:Four snoRNAs, commonly used for normalisation, RNU44, RNU48, RNU43 and RNU6B, and miRNA known to be associated with pathological factors, were measured by real-time polymerase chain reaction in two patient series: 219 breast cancer and 46 head and neck squamous cell carcinoma (HNSCC). SnoRNA and miRNA were then correlated with clinicopathological features and prognosis.Results:Small-nucleolar RNA expression was as variable as miRNA expression (miR-21, miR-210, miR-10b). Normalising miRNA PCR expression data to these recommended snoRNAs introduced bias in associations between miRNA and pathology or outcome. Low snoRNA expression correlated with markers of aggressive pathology. Low levels of RNU44 were associated with a poor prognosis. RNU44 is an intronic gene in a cluster of highly conserved snoRNAs in the growth arrest specific 5 (GAS5) transcript, which is normally upregulated to arrest cell growth under stress. Low-tumour GAS5 expression was associated with a poor prognosis. RNU48 and RNU43 were also identified as intronic snoRNAs within genes that are dysregulated in cancer.Conclusion:Small-nucleolar RNAs are important in cancer prognosis, and their use as reference genes can introduce bias when determining miRNA expression. © 2011 Cancer Research UK All rights reserved

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PubMed Central

Oxford University Research Archive

The University of Manchester - Institutional Repository

Down-Regulation of Glucose-Regulated Protein (GRP) 78 Potentiates Cytotoxic Effect of Celecoxib in Human Urothelial Carcinoma Cells

Author: A Cusimano
A Jemal
A Kardosh
Aamir Ahmad
AH Schonthal
AJ Dannenberg
AS Lee
BJ Christian
Chih-Kang Chiang
CN Sternberg
CS Williams
D Dhawan
D Dhawan
DG Menter
DM Latini
DT Rutkowski
G Ferrandina
H von der Maase
HJ Yu
J Gee
J Li
J Qin
J Wu
JJ Virrey
JR Gee
Kuan-Lin Kuo
Kuo-How Huang
L Egger
NM Davies
P Kulkarni
P Pyrko
PT Leese
S Huang
S Tsutsumi
S Tsutsumi
Shing-Hwa Liu
Shyh-Chyan Chen
SI Mohammed
SI Mohammed
SJ Dovedi
SK Kulp
SP Ermakova
ST Chen
TC Hour
Te-I Weng
V Jendrossek
WG Harker
X Liu
Yeong-Shiau Pu
Yu-Chieh Tsai
Yuan-Ting Chuang
Z Adhim
Publication venue: Public Library of Science
Publication date: 16/03/2012
Field of study

Celecoxib is a selective cyclooxygenase-2 (COX-2) inhibitor that has been reported to elicit anti-proliferative response in various tumors. In this study, we aim to investigate the antitumor effect of celecoxib on urothelial carcinoma (UC) cells and the role endoplasmic reticulum (ER) stress plays in celecoxib-induced cytotoxicity. The cytotoxic effects were measured by MTT assay and flow cytometry. The cell cycle progression and ER stress-associated molecules were examined by Western blot and flow cytometry. Moreover, the cytotoxic effects of celecoxib combined with glucose-regulated protein (GRP) 78 knockdown (siRNA), (−)-epigallocatechin gallate (EGCG) or MG132 were assessed. We demonstrated that celecoxib markedly reduces the cell viability and causes apoptosis in human UC cells through cell cycle G1 arrest. Celecoxib possessed the ability to activate ER stress-related chaperones (IRE-1α and GRP78), caspase-4, and CCAAT/enhancer binding protein homologous protein (CHOP), which were involved in UC cell apoptosis. Down-regulation of GRP78 by siRNA, co-treatment with EGCG (a GRP78 inhibitor) or with MG132 (a proteasome inhibitor) could enhance celecoxib-induced apoptosis. We concluded that celecoxib induces cell cycle G1 arrest, ER stress, and eventually apoptosis in human UC cells. The down-regulation of ER chaperone GRP78 by siRNA, EGCG, or proteosome inhibitor potentiated the cytotoxicity of celecoxib in UC cells. These findings provide a new treatment strategy against UC

Public Library of Science (PLOS)

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PubMed Central

National Taiwan University Repository

FigShare

Search for new phenomena in final states with an energetic jet and large missing transverse momentum in pp collisions at √ s = 8 TeV with the ATLAS detector

Author: Aad G
Abbott B
Abbott DC
Abeling K
Abhayasinghe DK
Abidi SH
AbouZeid OS
Abraham NL
Abramowicz H
Abreu H
Abud AA
Abulaiti Y
Acharya BS
Achkar B
Adachi S
Adam L
Adamczyk L
Adamek L
Adelman J
Adersberger M
Adiguzel A
Adorni S
Adye T
Affolder AA
Afik Y
Agapopoulou C
Agaras MN
Aggarwal A
Agheorghiesei C
Aguilar-Saavedra JA
Ahmadov F
Ahmed WS
Ai X
Aielli G
Akatsuka S
Akesson TPA
Akilli E
Akimov A
Al Khoury K
Alberghi GL
Albert J
Alderweireldt S
Aleksa M
Aleksandrov IN
Alexa C
Alexopoulos T
Alfonsi A
Alfonsi F
Alhroob M
Ali B
Aliev M
Alimonti G
Allaire C
Allbrooke BMM
Allen BW
Allport PP
Aloisio A
Alonso F
Alpigiani C
Alshehri AA
Alvarez Estevez M
Alviggi MG
Amaral Coutinho Y
Ambler A
Ambroz L
Amelung C
Amidei D
Amor Dos Santos SP
Amoroso S
Amrouche CS
An F
Anastopoulos C
Andari N
Andeen T
Anders CF
Anders JK
Andreazza A
Andrei V
Anelli CR
Angelidakis S
Angerami A
Anisenkov A
Annovi A
Antel C
Anthony MT
Antipov E
Antonelli M
Antrim DJA
Anulli F
Aoki M
Aparisi Pozo JA
Araque JP
Araujo Ferraz V
Araujo Pereira R
Araya ST
Arcangeletti C
Arce ATH
Arduh FA
Arguin J-F
Argyropoulos S
Arling J-H
Armbruster AJ
Armstrong A
Arnaez O
Arnold H
Artoni G
Artz S
Asai S
Asawatavonvanich T
Asbah N
Asimakopoulou EM
Asquith L
Assahsah J
Assamagan K
Astalos R
Astigarraga MEP
Atkin RJ
Atkinson M
Atlay NB
Atmani H
Augsten K
Avolio G
Ayoub MK
Azuelos G
Bachacou H
Bachas K
Backes M
Backman F
Bagnaia P
Bahmani M
Bahrasemani H
Bailey AJ
Bailey VR
Baines JT
Bakalis C
Baker OK
Bakker PJ
Balaji S
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
Barbour G
Barillari T
Barisits M-S
Barkeloo J
Barklow T
Barnea R
Barnett BM
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Barnovska-Blenessy Z
Baroncelli A
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Basalaev A
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Basso MJ
Bates RL
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Batley JR
Batool B
Battaglia M
Bauce M
Bauer F
Bauer KT
Bawa HS
Beacham JB
Beau T
Beauchemin PH
Becherer F
Bechtle P
Beck HC
Beck HP
Becker K
Becot C
Beddall A
Beddall AJ
Bednyakov VA
Bedognetti M
Beermann TA
Begalli M
Begel M
Behera A
Behr JK
Beisiegel F
Bell AS
Bella G
Bella LA
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Bellerive A
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Beloborodov K
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Benchekroun D
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Benjamin DP
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Bensinger JR
Bentvelsen S
Beresford L
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Berge D
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Bergmann B
Bergsten LJ
Beringer J
Berlendis S
Berlingen JM
Bernardi G
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Bernlochner FU
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Bevan AJ
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Bhattacharya DS
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Bi R
Bianchi RM
Biebel O
Biedermann D
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Billoud TR
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Bitadze A
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Blocker C
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Blumenschein U
Bobbink GJ
Bobrovnikov VS
Bocchetta SS
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Boeriu OEV
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Bogdanchikov AG
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Bonilla JS
Boonekamp M
Booth CD
Borecka-Bielska HM
Borgna LS
Borisov A
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Bortfeldt J
Bortoletto D
Boscherini D
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Bouaouda K
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Bourdarios CA
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Burzynski JC
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Cerqueira AS
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Chapman JD
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Charlton DG
Charman TP
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Chekanov S
Chekulaev S
Chelkov GA
Chen B
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Chen X
Chen Y-H
Cheng HC
Cheng HJ
Cheplakov A
Cheremushkina E
Cheu E
Cheung K
Chevalerias TJA
Chevalier L
Chiarella V
Chiarelli G
Chiodini G
Chisholm AS
Chitan A
Chiu I
Chiu YH
Chizhov M
Choi K
Chomont AR
Chouridou S
Chow YS
Chu MC
Chu X
Chudoba J
Chwastowski JJ
Chytka L
Cieri D
Ciesla KM
Cinca D
Cindro V
Cioara IA
Ciocio A
Cirotto F
Citron ZH
Citterio M
Ciubotaru DA
Ciungu BM
Clark A
Clark MR
Clark PJ
Clement C
Coadou Y
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Coccaro A
Cochran J
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Coimbra AEC
Cole B
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Cooper-Sarkar AM
Corga KDV
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de Renstrom PAB
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Ducourthial A
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Ibragimov I
Iconomidou-Fayard L
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Knue A
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Kodama T
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Kolb M
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Komarek T
Kondo T
Kong AXY
Konig AC
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Konstantinides V
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Konya B
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Kourkoumelis C
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Kowalewska AB
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Kulinich YP
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Kurochkin YA
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Kuutmann EB
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Lai S
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Lawlor SD
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Lee ACA
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Leight WA
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Lellouch D
Leney KJC
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Li B
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Liberti B
Liblong A
Lie K
Lim S
Lin CY
Lin K
Lin TH
Linck RA
Lindon JH
Lionti AL
Lipeles E
Lipniacka A
Liss TM
Lister A
Little JD
Liu B
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Liu H
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Liu JB
Liu JKK
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Liu Y
Liu YL
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Lloyd SL
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Macchiolo A
Macdonald CM
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Madden WDB
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Manhaes de Andrade Filho L
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Milov A
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Sullivan MJ
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Suster CJE
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Zwalinski L
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2015
Field of study

Results of a search for new phenomena in final states with an energetic jet and large missing transverse momentum are reported. The search uses 20.3 fb−1 of √ s = 8 TeV data collected in 2012 with the ATLAS detector at the LHC. Events are required to have at least one jet with pT > 120 GeV and no leptons. Nine signal regions are considered with increasing missing transverse momentum requirements between Emiss T > 150 GeV and Emiss T > 700 GeV. Good agreement is observed between the number of events in data and Standard Model expectations. The results are translated into exclusion limits on models with either large extra spatial dimensions, pair production of weakly interacting dark matter candidates, or production of very light gravitinos in a gauge-mediated supersymmetric model. In addition, limits on the production of an invisibly decaying Higgs-like boson leading to similar topologies in the final state are presente

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Observation of associated near-side and away-side long-range correlations in √sNN=5.02 TeV proton-lead collisions with the ATLAS detector

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Abajyan T
Abbott B
Abdallah J
Abdel Khalek S
Abdelalim AA
Abdinov O
Aben R
Abi B
Abolins M
Abouzeid OS
Abramowicz H
Abreu H
Acharya BS
Adamczyk L
Adams DL
Addy TN
Adelman J
Adomeit S
Adragna P
Adye T
Aefsky S
Aguilar-Saavedra JA
Agustoni M
Ahlen SP
Ahles F
Ahmad A
Ahsan M
Aielli G
Akesson TP
Akimoto G
Akimov AV
Alam MA
Albert J
Albrand S
Aleksa M
Aleksandrov IN
Alessandria F
Alexa C
Alexander G
Alexandre G
Alexopoulos T
Alhroob M
Aliev M
Alimonti G
Alison J
Allbrooke BM
Allison LJ
Allport PP
Allwood-Spiers SE
Almond J
Aloisio A
Alon R
Alonso A
Alonso F
Altheimer A
Alvarez Gonzalez B
Alviggi MG
Amako K
Amelung C
Ammosov VV
Amor Dos Santos SP
Amorim A
Amoroso S
Amram N
Anastopoulos C
Ancu LS
Andari N
Andeen T
Anders CF
Anders G
Anderson KJ
Andreazza A
Andrei V
Anduaga XS
Angelidakis S
Anger P
Angerami A
Anghinolfi F
Anisenkov A
Anjos N
Annovi A
Antonaki A
Antonelli M
Antonov A
Antos J
Anulli F
Aoki M
Aperio Bella L
Apolle R
Arabidze G
Aracena I
Arai Y
Arce AT
Arfaoui S
Arguin JF
Argyropoulos S
Arik E
Arik M
Armbruster AJ
Arnaez O
Arnal V
Artamonov A
Artoni G
Arutinov D
Asai S
Ask S
Asman B
Asquith L
Assamagan K
Astalos R
Astbury A
Atkinson M
ATLAS Collaboration The
Auerbach B
Auge E
Augsten K
Aurousseau M
Avolio G
Axen D
Azuelos G
Azuma Y
Baak MA
Baccaglioni G
Bacci C
Bach AM
Bachacou H
Bachas K
Backes M
Backhaus M
Backus Mayes J
Badescu E
Bagnaia P
Bai Y
Bailey DC
Bain T
Baines JT
Baker OK
Baker S
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Banerjee P
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Banfi D
Bangert A
Bansal V
Bansil HS
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Baranov SP
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Barberio EL
Barberis D
Barbero M
Bardin DY
Barillari T
Barisonzi M
Barklow T
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Barreiro Guimarães da Costa J
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Publication venue: American Physical Society
Publication date: 01/01/2012
Field of study

Two-particle correlations in relative azimuthal angle (Δϕ) and pseudorapidity (Δη) are measured in √sNN=5.02 TeV p+Pb collisions using the ATLAS detector at the LHC. The measurements are performed using approximately 1 μb-1 of data as a function of transverse momentum (pT) and the transverse energy (ΣETPb) summed over 3.1<η<4.9 in the direction of the Pb beam. The correlation function, constructed from charged particles, exhibits a long-range (2<|Δη|<5) “near-side” (Δϕ∼0) correlation that grows rapidly with increasing ΣETPb. A long-range “away-side” (Δϕ∼π) correlation, obtained by subtracting the expected contributions from recoiling dijets and other sources estimated using events with small ΣETPb, is found to match the near-side correlation in magnitude, shape (in Δη and Δϕ) and ΣETPb dependence. The resultant Δϕ correlation is approximately symmetric about π/2, and is consistent with a dominant cos⁡2Δϕ modulation for all ΣETPb ranges and particle pT

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Search for the neutral Higgs bosons of the minimal supersymmetric standard model in pp collisions at root s=7 TeV with the ATLAS detector

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Abajyan T
Abbott B
Abdallah J
Abdelalim AA
Abdinov O
Abi B
Abolins M
AbouZeid OS
Abramowicz H
Abreu H
Acharya BS
Adam ER
Adamczyk L
Adams DL
Addy TN
Adelman J
Adomeit S
Adragna P
Adye T
Aesky S
Agar-Savedra JA
Agustoni M
Ahlen SP
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Ahmad A
Ahsan M
Aielli G
Akesson TPA
Akimoto G
Akimov AV
Alam MA
Albert J
Albrand S
Aleksa M
Aleksandrov IN
Alessandria F
Alexa C
Alexander G
Alexandre G
Alexopoulos T
Alhroob M
Aliev M
Alimonti G
Alison J
Allbrooke BMM
Allison LJ
Allport PP
Allwood-Spiers SE
Almenar CC
Almond J
Aloisio A
Alon R
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Altheimer A
Alviggi MG
Amako K
Amelung C
Ammosov VV
Amor Dos Santos SP
Amorim A
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Anastopoulos C
Ancu LS
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Anderson KJ
Andreazza A
Andrei V
Andrieux M-L
Anduaga XS
Angelidakis S
Anger P
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Anghinolfi F
Anh TV
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Antonaki A
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Antonov A
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Apolle R
Arabidze G
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Aranda CP
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Arik E
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Armbruster AJ
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Artamonov A
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Baak MA
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de Lima DEF
de Lima JGR
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De Regie JBDV
de Renstrom PAB
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Degenhardt J
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della Porta GZ
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Deviveiros PO
Dewhurst A
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Doan TKO
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Espinal Curull X
Esposito B
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Etienvre AI
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Fabre C
Fajardo LSG
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Favareto A
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Fedorko W
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Feligioni L
Feng C
Feng EJ
Fenyuk AB
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Ferrando BMS
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Fiedler F
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Filthaut F
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Fiolhais MCN
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Fischer MJ
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Flowerdew MJ
Formica A
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Garcia BRM
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Garcia-Estan MTP
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Garrido MDMC
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Gavrilenko IL
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Gazis EN
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Publication venue
Publication date: 01/02/2013
Field of study

A search for neutral Higgs bosons of the Minimal Supersymmetric Standard Model (MSSM) is reported. The analysis is based on a sample of proton-proton collisions at a centre-of-mass energy of 7TeV recorded with the ATLAS detector at the Large Hadron Collider. The data were recorded in 2011 and correspond to an integrated luminosity of 4.7 fb-1 to 4.8 fb-1. Higgs boson decays into oppositely-charged muon or τ lepton pairs are considered for final states requiring either the presence or absence of b-jets. No statistically significant excess over the expected background is observed and exclusion limits at the 95% confidence level are derived. The exclusion limits are for the production cross-section of a generic neutral Higgs boson, φ, as a function of the Higgs boson mass and for h/A/H production in the MSSM as a function of the parameters mA and tan β in the mhmax scenario for mA in the range of 90GeV to 500 GeV. Copyright CERN

Oxford University Research Archive

Queen Mary Research Online

Search for R-parity-violating supersymmetry in events with four or more leptons in sqrt(s) =7 TeV pp collisions with the ATLAS detector

Author: Aad G
Abajyan T
Abbott B
Abdallah J
Khalek SA
Abdelalim AA
Abdinov O
Aben R
Abi B
Abolins M
AbouZeid OS
Abramowicz H
Abreu H
Acharya BS
Adamczyk L
Adams DL
Addy TN
Adelman J
Adomeit S
Adragna P
Adye T
Aefsky S
Aguilar-Saavedra JA
Agustoni M
Aharrouche M
Ahlen SP
Ahles F
Ahmad A
Ahsan M
Aielli G
Akesson TPA
Akimoto G
Akimov AV
Alam MS
Alam MA
Albert J
Albrand S
Aleksa M
Aleksandrov IN
Alessandria F
Alexa C
Alexander G
Alexandre G
Alexopoulos T
Alhroob M
Aliev M
Alimonti G
Alison J
Allbrooke BMM
Allport PP
Allwood-Spiers SE
Almond J
Aloisio A
Alon R
Alonso A
Alonso F
Altheimer A
Gonzalez BA
Alviggi MG
Amako K
Amelung C
Ammosov VV
Amor Dos Santos SP
Amorim A
Amram N
Anastopoulos C
Ancu LS
Andari N
Andeen T
Anders CF
Anders G
Anderson KJ
Andreazza A
Andrei V
Andrieux M-L
Anduaga XS
Angelidakis S
Anger P
Angerami A
Anghinolfi F
Anisenkov A
Anjos N
Annovi A
Antonaki A
Antonelli M
Antonov A
Antos J
Anulli F
Aoki M
Aoun S
Bella LA
Apolle R
Arabidze G
Aracena I
Arai Y
Arce ATH
Arfaoui S
Arguin J-F
Argyropoulos S
Arik E
Arik M
Armbruster AJ
Arnaez O
Arnal V
Arnault C
Artamonov A
Artoni G
Arutinov D
Asai S
Ask S
Asman B
Asquith L
Assamagan K
Astbury A
Atkinson M
Aubert B
Auge E
Augsten K
Aurousseau M
Avolio G
Avramidou R
Axen D
Azuelos G
Azuma Y
Baak MA
Baccaglioni G
Bacci C
Bach AM
Bachacou H
Bachas K
Backes M
Backhaus M
Mayes JB
Badescu E
Bagnaia P
Bahinipati S
Bai Y
Bailey DC
Bain T
Baines JT
Baker OK
Baker MD
Baker S
Balek P
Banas E
Banerjee P
Banerjee S
Banfi D
Bangert A
Bansal V
Bansil HS
Barak L
Baranov SP
Galtieri AB
Barber T
Barberio EL
Barberis D
Barbero M
Bardin DY
Barillari T
Barisonzi M
Barklow T
Barlow N
Barnett BM
Barnett RM
Baroncelli A
Barone G
Barr AJ
Barreiro F
da Costa JBG
Barrillon P
Bartoldus R
Barton AE
Bartsch V
Basye A
Bates RL
Batkova L
Batley JR
Battaglia A
Battistin M
Bauer F
Bawa HS
Beale S
Beau T
Beauchemin PH
Beccherle R
Bechtle P
Beck HP
Becker K
Becker S
Beckingham M
Becks KH
Beddall AJ
Beddall A
Bedikian S
Bednyakov VA
Bee CP
Beemster LJ
Begel M
Harpaz SB
Behera PK
Beimforde M
Belanger-Champagne C
Bell PJ
Bell WH
Bella G
Bellagamba L
Bellomo M
Belloni A
Beloborodova O
Belotskiy K
Beltramello O
Benary O
Benchekroun D
Bendtz K
Benekos N
Benhammou Y
Noccioli EB
Garcia JAB
Benjamin DP
Benoit M
Bensinger JR
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Kuutmann EB
Berger N
Berghaus F
Berglund E
Beringer J
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Bernius C
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Bertella C
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Bertolucci F
Besana MI
Besjes GJ
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Bianchi RM
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Bieniek SP
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Biglietti M
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Biscarat C
Bittner B
Black CW
Black KM
Blair RE
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Blanchot G
Blazek T
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Blum W
Blumenschein U
Bobbink GJ
Bobrovnikov VS
Bocchetta SS
Bocci A
Boddy CR
Boehler M
Boek J
Boek TT
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Bogdanchikov A
Bogouch A
Bohm C
Bohm J
Boisvert V
Bold T
Boldea V
Bolnet NM
Bomben M
Bona M
Boonekamp M
Bordoni S
Borer C
Borisov A
Borissov G
Borjanovic I
Borri M
Borroni S
Bortfeldt J
Bortolotto V
Bos K
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Bozovic-Jelisavcic I
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Budagov IA
Budick B
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Campana S
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Caprini I
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Castillo Gimenez V
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Chalupkova I
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Chapleau B
Chapman JD
Chapman JW
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Chavda V
Barajas CAC
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Chelkov GA
Chelstowska MA
Chen C
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Chen Y
Cheng Y
Cheplakov A
El Moursli RC
Chernyatin V
Cheu E
Cheung SL
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Childers JT
Chilingarov A
Chiodini G
Chisholm AS
Chislett RT
Chitan A
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Christidi IA
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Chromek-Burckhart D
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Ciftci AK
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Cinca D
Cindro V
Ciocca C
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Citron ZH
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Ciubancan M
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Clarke RN
Cleland W
Clemens JC
Clement B
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Coniavitis E
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Cortiana G
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Czyczula Z
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D'Onofrio M
D'Orazio A
Da Cunha Sargedas De Sousa MJ
Da Via C
Dabrowski W
Dafinca A
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Dam M
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Danielsson HO
Dao V
Darbo G
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Dassoulas JA
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De Pedis D
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Dearnaley WJ
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Degenhardt J
Del Peso J
Del Prete T
Delemontex T
Deliyergiyev M
Dell'Acqua A
Dell'Asta L
Della Pietra M
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Delmastro M
Delsart PA
Deluca C
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Demichev M
Demirkoz B
Denisov SP
Derendarz D
Derkaoui JE
Derue F
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Devetak E
Deviveiros PO
Dewhurst A
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Dhaliwal S
Dhullipudi R
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Di Donato C
Di Girolamo A
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Di Luise S
Di Mattia A
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Di Sipio R
Diaz MA
Diehl EB
Dietrich J
Dietzsch TA
Diglio S
Yagci KD
Dingfelder J
Dinut F
Dionisi C
Dita P
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Djobava T
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Do Valle Wemans A
Doan TKO
Dobbs M
Dobos D
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Doglioni C
Doherty T
Doi Y
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Dolenc I
Dolezal Z
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Dohmae T
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Donini J
Dopke J
Doria A
Dos Anjos A
Dotti A
Dova MT
Doxiadis AD
Doyle AT
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Dris M
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Dube S
Duchovni E
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Duda D
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Duerdoth IP
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Duxfield R
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Ereditato A
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Escobar C
Espinal Curull X
Esposito B
Etienne F
Etienvre AI
Etzion E
Evangelakou D
Evans H
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Fabre C
Fakhrutdinov RM
Falciano S
Fang Y
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Fassouliotis D
Fatholahzadeh B
Favareto A
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Fedorko W
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Feligioni L
Feng C
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Flowerdew MJ
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Gavrilenko IL
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Gazis EN
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Gershon A
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Giangiobbe V
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Koi T
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Kolanoski H
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Komar AA
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Kondo T
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Kononov AI
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Koperny S
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Korolkova EV
Korotkov VA
Kortner O
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Kostyukhin VV
Kotov S
Kotov VM
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Kowalski TZ
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Collaboration ATLAS
Publication venue: Springer Verlag
Publication date: 01/01/2008
Field of study

A search for new phenomena in final states with four or more leptons (electrons or muons) is presented. The analysis is based on 4.7 fb−1 of

\sqrt{s}=7\;\mathrm{TeV}

proton-proton collisions delivered by the Large Hadron Collider and recorded with the ATLAS detector. Observations are consistent with Standard Model expectations in two signal regions: one that requires moderate values of missing transverse momentum and another that requires large effective mass. The results are interpreted in a simplified model of R-parity-violating supersymmetry in which a 95% CL exclusion region is set for charged wino masses up to 540 GeV. In an R-parity-violating MSUGRA/CMSSM model, values of m 1/2 up to 820 GeV are excluded for 10 < tan β < 40

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Search for high-mass resonances decaying to dilepton final states in pp collisions at s√=7 TeV with the ATLAS detector

Author: Aad G
Abajyan T
Abbott B
Abdallah J
Abdelalim AA
Abdinov O
Aben R
Abi B
Abolins M
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Bozovic-Jelisavcic I
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Bruckman de Renstrom PA
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Buckley AG
Buda SI
Budagov IA
Budick B
Buescher V
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Bugge L
Bulekov O
Bundock AC
Bunse M
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Burdin S
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Caforio D
Cakir IT
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Calafiura P
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Caloba LP
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Caminada LM
Caminal Armadans R
Campana S
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Carrillo-Montoya GD
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Castaneda-Miranda E
Castanheira MTD
Castillo IS
Castillo LRF
Castro NF
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Catmore JR
Cattai A
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Cavalcanti TP
Cavaliere V
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Cavasinni V
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Cerri A
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Chafaq A
Chakraborty D
Chalupkova I
Chan K
Chang P
Chapleau B
Chapman JD
Chapman JW
Chareyre E
Charlton DG
Chavda V
Cheatham S
Chekanov S
Chekulaev SV
Chelkov GA
Chelstowska MA
Chen C
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Chen X
Chen Y
Cheng Y
Cheplakov A
Chernyatin V
Cheu E
Cheung SL
Chevalier L
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Childers JT
Chilingarov A
Chiodini G
Chisholm AS
Chislett RT
Chitan A
Chizhov MV
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Christidi IA
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Chromek-Burckhart D
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Chudoba J
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Ciftci AK
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Cinca D
Cindro V
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Citron ZH
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Clemens JC
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Codina EP
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Collaboration A
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Coniavitis E
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Constantinescu S
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Cooper BD
Cooper-Sarkar AM
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Cornelissen T
Corradi M
Correia AMH
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Cortiana G
Costa G
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Da Cunha Sargedas De Sousa MJ
Da Via C
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Dafinca A
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Degenhardt J
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Deliyergiyev M
Dell'Acqua A
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Deviveiros PO
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Dietzsch TA
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Fakhrutdinov RM
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Koi T
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Kolesnikov V
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Komar AA
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Kondo T
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Kononov AI
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Koperny S
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Kostyukhin VV
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Kowalski TZ
Kozanecki W
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Leney KJC
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Livermore SSA
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Macina D
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Milov A
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Minashvili IA
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Wasicki C
Watanabe I
Watkins PM
Watson AT
Watson IJ
Watson MF
Watts G
Watts S
Waugh AT
Waugh BM
Weber MS
Webster JS
Weidberg AR
Weigell P
Weingarten J
Weiser C
Wells PS
Wemans ADV
Wenaus T
Wendland D
Wengler T
Wengu Z
Wenig S
Wermes N
Werner M
Werner P
Werth M
Wessels M
Wetter J
Weydert C
Whalen K
White A
White MJ
White S
Whitehead SR
Whiteson D
Whittington D
Wicek F
Wicke D
Wickens FJ
Wiedenmann W
Wielers M
Wienemann P
Wiglesworth C
Wiik-Fuchs LAM
Wijeratne PA
Wildauer A
Wildt MA
Wilhelm I
Wilkens HG
Will JZ
Williams E
Williams HH
Willis W
Willocoq S
Wilson A
Wilson JA
Wilson MG
Wingerter-Seez I
Winkelmann S
Winklmeier F
Wittgen M
Wollstadt SJ
Wolter MW
Wolters H
Wong WC
Wooden G
Wosiek BK
Wotschack J
Woudstra MJ
Wozniak KW
Wraight K
Wright M
Wrona B
Wu SL
Wu X
Wu Y
Wulf E
Wynne BM
Xella S
Xiao M
Xie S
Xu C
Xu D
Xu L
Yabsley B
Yacoob S
Yagci KD
Yamada M
Yamaguchi H
Yamamoto A
Yamamoto K
Yamamoto S
Yamamura T
Yamanaka T
Yamazaki T
Yamazaki Y
Yan Z
Yang H
Yang UK
Yang Y
Yang Z
Yanush S
Yao L
Yao Y
Yasu Y
Ye J
Ye S
Yildiz HD
Yilmaz M
Yoosoofmiya R
Yorita K
Yoshida R
Yoshihara K
Young C
Young CJ
Youssef S
Yu D
Yu DR
Yu J
Yu J
Yuan L
Yurkewicz A
Zabinski B
Zaidan R
Zaitsev AM
Zajacova Z
Zanello L
Zanzi D
Zaytsev A
Zeitnitz C
Zeman M
Zemla A
Zendler C
Zenin O
Zenis T
Zerwas D
Zhang D
Zhang H
Zhang J
Zhang X
Zhang Z
Zhao L
Zhao Z
Zhemchugov A
Zhong J
Zhou B
Zhou N
Zhou Y
Zhu CG
Zhu H
Zhu J
Zhu Y
Zhuang X
Zhuravlov V
Zibell A
Zieminska D
Zimin NI
Zimmermann R
Zimmermann S
Zimmermann S
Zinonos Z
Ziolkowski M
Zitoun R
Zivkovic L
Zmouchko VV
Zobernig G
Zoccoli A
zur Nedden M
Zutshi V
Zwalinski L
Publication venue: Springer
Publication date: 23/11/2012
Field of study

The ATLAS detector at the Large Hadron Collider is used to search for high-mass resonances decaying to an electron-positron pair or a muon-antimuon pair. The search is sensitive to heavy neutral Z′ gauge bosons, Randall-Sundrum gravitons, Z * bosons, techni-mesons, Kaluza-Klein Z/γ bosons, and bosons predicted by Torsion models. Results are presented based on an analysis of pp collisions at a center-of-mass energy of 7 TeV corresponding to an integrated luminosity of 4.9 fb−1 in the e + e − channel and 5.0 fb−1 in the μ + μ −channel. A Z ′ boson with Standard Model-like couplings is excluded at 95 % confidence level for masses below 2.22 TeV. A Randall-Sundrum graviton with coupling k/MPl=0.1 is excluded at 95 % confidence level for masses below 2.16 TeV. Limits on the other models are also presented, including Technicolor and Minimal Z′ Models

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Following a foraging fish-finder : diel habitat use of Blainville's beaked whales revealed by echolocation

Author: A De Robertis
AGV Salvanes
Alberto Brito
B Hölldobler
B Jones
B McConnell
BA Cartwright
BA Seibel
D Malakoff
D Thompson
DE Claridge
DJ McSweeney
DN Maclennan
DP Costa
DP Costa
DW Sims
E Barham
ED Barton
EL Hazen
Fernando Bordes
GH Pyke
GL Kooyman
GT Waring
J Cohen
J Mauchline
JC Drazen
JJ Childress
JJ Childress
KJ Benoit-Bird
KJ Benoit-Bird
LA Levin
M Biuw
MA Hindell
Mark P. Johnson
MJR Gee
MP Johnson
MP Johnson
MP Johnson
MP Johnson
MV Angel
MW Johnson
N Aguilar de Soto
Natacha Aguilar de Soto
NB Marshall
Patricia Arranz
PD Jepson
Peter T. Madsen
PJ Butler
PJO Miller
PL Tyack
PL Tyack
PT Madsen
R Arditi
R Baird
RP Wilson
RP Wilson
RW Davis
RW Davis
SL Watwood
TC Kane
Y Watanabe
Yan Ropert-Coudert
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 07/12/2011
Field of study

© The Author(s), 2011. This article is distributed under the terms of the Creative Commons Attribution License. The definitive version was published in PLoS One 6 (2011): e28353, doi:10.1371/journal.pone.0028353.Simultaneous high resolution sampling of predator behavior and habitat characteristics is often difficult to achieve despite its importance in understanding the foraging decisions and habitat use of predators. Here we tap into the biosonar system of Blainville's beaked whales, Mesoplodon densirostris, using sound and orientation recording tags to uncover prey-finding cues available to echolocating predators in the deep-sea. Echolocation sounds indicate where whales search and encounter prey, as well as the altitude of whales above the sea-floor and the density of organisms around them, providing a link between foraging activity and the bio-physical environment. Tagged whales (n = 9) hunted exclusively at depth, investing most of their search time either in the lower part of the deep scattering layer (DSL) or near the sea-floor with little diel change. At least 43% (420/974) of recorded prey-capture attempts were performed within the benthic boundary layer despite a wide range of dive depths, and many dives included both meso- and bentho-pelagic foraging. Blainville's beaked whales only initiate searching when already deep in the descent and encounter prey suitable for capture within 2 min of the start of echolocation, suggesting that these whales are accessing prey in reliable vertical strata. Moreover, these prey resources are sufficiently dense to feed the animals in what is effectively four hours of hunting per day enabling a strategy in which long dives to exploit numerous deep-prey with low nutritional value require protracted recovery periods (average 1.5 h) between dives. This apparent searching efficiency maybe aided by inhabiting steep undersea slopes with access to both the DSL and the sea-floor over small spatial scales. Aggregations of prey in these biotopes are located using biosonar-derived landmarks and represent stable and abundant resources for Blainville's beaked whales in the otherwise food-limited deep-ocean.The work was funded by the Office of Naval Research and the National Ocean Partnership Program (US), by a consortium consisting of the Canary Islands Government, the Spanish Ministry of Environment and the Spanish Ministry of Defense, and by the European environmental funding LIFE-INDEMARES program for the inventory and designation of the Natura 2000 network in marine areas of the Spanish territory, headed by Fundacion Biodiversidad, with additional support from the Cabildo Insular of El Hierro. PA is currently supported by the National Research Project: Cetacean, Oceanography and Biodiversity from La Palma and El Hierro (CGL2009-13112) of the Spanish Ministry of Science and NAS by a Marie Curie fellowship from the 7th European Frame Program. MJ was supported by grants from the Strategic Environmental Research Development Program and from the National Ocean Partnership Program. PTM was supported by frame grants from the National Danish Science Foundation

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Hepatitis C Virus (HCV) Evades NKG2D-Dependent NK Cell Responses through NS5A-Mediated Imbalance of Inflammatory Cytokines

Author: A Datta
A De Maria
A Dolganiuc
A Krmpotic
A Rolle
Arielle R. Rosenberg
B Hoechst
B Hoechst
B Meresse
B Oliviero
BD Lindenbach
C Cerboni
C Morishima
Christopher M. Walker
Céline Hernandez
D Vermijlen
Damien Sène
DH Raulet
E Mortier
Evelyne Jouvin-Marche
Franck Levasseur
G Ahlenstiel
G Maloney
G Par
H Li
I Kinjyo
J Corado
J Nattermann
J Stockl
J Yu
J Zhong
J Zhong
JC Lee
K Bieback
K Gee
KA Walters
KA Walters
L Golden-Mason
L Golden-Mason
L Golden-Mason
L Golden-Mason
LL Lanier
M Abel
M Benahmed
M Gale Jr
M Jinushi
M Lodoen
M Thomas
MA Friese
Marion Lambert
Michal Abel
MM Sandau
MT Brady
N Stern-Ginossar
P Bonorino
P Bonorino
Patrice Cacoub
Patrice N. Marche
PJ Lucas
PT Kennedy
R Castriconi
S Akira
S Bauer
S Chang
S Crotta
S Hue
S Hue
S Kottilil
S Norris
S Yamagiwa
SI Khakoo
SJ Conry
SL Lambert
SM Dann
Sophie Caillat-Zucman
T Deignan
T Ebihara
T Fukao
T Horng
T Wakita
UC Meier
V Groh
V Groh
V Tieng
Véronique Pène
W Ma
Xavier Camous
YT Bryceson
Publication venue: Public Library of Science
Publication date: 01/01/2010
Field of study

Understanding how hepatitis C virus (HCV) induces and circumvents the host's natural killer (NK) cell-mediated immunity is of critical importance in efforts to design effective therapeutics. We report here the decreased expression of the NKG2D activating receptor as a novel strategy adopted by HCV to evade NK-cell mediated responses. We show that chronic HCV infection is associated with expression of ligands for NKG2D, the MHC class I-related Chain (MIC) molecules, on hepatocytes. However, NKG2D expression is downmodulated on circulating NK cells, and consequently NK cell-mediated cytotoxic capacity and interferon-γ production are impaired. Using an endotoxin-free recombinant NS5A protein, we show that NS5A stimulation of monocytes through Toll-like Receptor 4 (TLR4) promotes p38- and PI3 kinase-dependent IL-10 production, while inhibiting IL-12 production. In turn, IL-10 triggers secretion of TGFβ which downmodulates NKG2D expression on NK cells, leading to their impaired effector functions. Moreover, culture supernatants of HCV JFH1 replicating Huh-7.5.1 cells reproduce the effect of recombinant NS5A on NKG2D downmodulation. Exogenous IL-15 can antagonize the TGFβ effect and restore normal NKG2D expression on NK cells. We conclude that NKG2D-dependent NK cell functions are modulated during chronic HCV infection, and demonstrate that this alteration can be prevented by exogenous IL-15, which could represent a meaningful adjuvant for therapeutic intervention

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C. elegans Agrin Is Expressed in Pharynx, IL1 Neurons and Distal Tip Cells and Does Not Genetically Interact with Genes Involved in Synaptogenesis or Muscle Function

Author: AA Khan
AC Hart
AC Millet
AJ Denzer
AJ Denzer
AJ Groffen
Ana Hrus
BD Ackley
BD Ackley
BD Williams
C Bessou
C Gally
C Magill-Solc
C Magill-Solc
C Magill-Solc
CA Pearson
CC Mello
CL Batchelor
D Fischer
DC Merz
DE Michele
DE Michele
DG Albertson
DJ Glass
DK Chow
DL Riddle
E Gasteiger
EL Tsalik
EM Hedgecock
EM Jorgensen
EW Godfrey
F Rupp
FR Neumann
G Bezakova
G Bezakova
G Tsen
Gordon Lau
GP Mullen
H Hutter
Harald Hutter
Hernan Lopez-Schier
I Letunic
J Sambrook
J Zhang
JA Lewis
Jacqueline Ferralli
JD Bendtsen
JE Sulston
JG White
JH Thomas
JL Bessereau
JM Kaplan
JM Kramer
JT Fleming
K Gieseler
K Okada
KW Tsim
L Avery
L Chen
M Clamp
M Durbeej
M Finney
M Gautam
M Gesemann
M Gesemann
M Gesemann
M Koga
M Krause
M Lee
M Nguyen
M Pagni
MA Ruegg
MA Ruegg
MA Smith
Marianne Brown-Luedi
MJ Ferns
MM Francis
NH Brown
O Hobert
O Hobert
P Rice
P Scotton
PJ Campagnola
PK Grewal
PT Martin
R Francis
RA Kammerer
RM Nitkin
RP Johnson
RR Zwaal
Ruth Chiquet-Ehrismann
RW Burgess
RW Burgess
RY Lee
S Brenner
S Strome
SH Gee
SH Kang
SP Koushika
Stefano Canevascini
Susanne Schenk
SW L'Hernault
T Cheusova
T Schedl
TM DeChiara
TM Rogalski
TM Rogalski
U Winzen
UJ McMahan
UK Laemmli
W Hoch
WC Forrester
ZG Luo
Publication venue: Public Library of Science
Publication date: 01/08/2007
Field of study

Agrin is a basement membrane protein crucial for development and maintenance of the neuromuscular junction in vertebrates. The C. elegans genome harbors a putative agrin gene agr-1. We have cloned the corresponding cDNA to determine the primary structure of the protein and expressed its recombinant fragments to raise specific antibodies. The domain organization of AGR-1 is very similar to the vertebrate orthologues. C. elegans agrin contains a signal sequence for secretion, seven follistatin domains, three EGF-like repeats and two laminin G domains. AGR-1 loss of function mutants did not exhibit any overt phenotypes and did not acquire resistance to the acetylcholine receptor agonist levamisole. Furthermore, crossing them with various mutants for components of the dystrophin-glycoprotein complex with impaired muscle function did not lead to an aggravation of the phenotypes. Promoter-GFP translational fusion as well as immunostaining of worms revealed expression of agrin in buccal epithelium and the protein deposition in the basal lamina of the pharynx. Furthermore, dorsal and ventral IL1 head neurons and distal tip cells of the gonad arms are sources of agrin production, but no expression was detectable in body muscles or in the motoneurons innervating them. Recombinant worm AGR-1 fragment is able to cluster vertebrate dystroglycan in cultured cells, implying a conservation of this interaction, but since neither of these proteins is expressed in muscle of C. elegans, this interaction may be required in different tissues. The connections between muscle cells and the basement membrane, as well as neuromuscular junctions, are structurally distinct between vertebrates and nematodes

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