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191 research outputs found

Profiles of Human Serum Antibody Responses Elicited by Three Leading HIV Vaccines Focusing on the Induction of Env-Specific Antibodies

Author: AJ Conley
AJ Hessell
BF Haynes
C Karnasuta
Cheryl A. Stoddart
D Casimiro
David Montefiori
DC Montefiori
DH Barouch
EA Emini
ET Crooks
IK Srivastava
James Arthos
JF Conway
JF Scheid
JM Binley
JM Decker
JR Mascola
JR Mascola
LM Walker
M Li
M. Juliana McElrath
Michael Vaine
MJJ Fleury
ML Clements-Mann
MN Forsell
ND Christensen
ND Russell
NM Flynn
NR Derby
PA Goepfert
Paul Goepfert
Qin Liu
R Hofmann-Lehmann
R Hofmann-Lehmann
S Rerks-Ngarm
S Wang
Shan Lu
Shixia Wang
SP Buchbinder
T Zhou
VR Gomez-Roman
X Wu
Y Li
Y Li
Publication venue: Public Library of Science
Publication date: 09/11/2010
Field of study

In the current report, we compared the specificities of antibody responses in sera from volunteers enrolled in three US NIH-supported HIV vaccine trials using different immunization regimens. HIV-1 Env-specific binding antibody, neutralizing antibody, antibody-dependent cell-mediated cytotoxicity (ADCC), and profiles of antibody specificity were analyzed for human immune sera collected from vaccinees enrolled in the NIH HIV Vaccine Trial Network (HVTN) Study #041 (recombinant protein alone), HVTN Study #203 (poxviral vector prime-protein boost), and the DP6-001 study (DNA prime-protein boost). Vaccinees from HVTN Study #041 had the highest neutralizing antibody activities against the sensitive virus along with the highest binding antibody responses, particularly those directed toward the V3 loop. DP6-001 sera showed a higher frequency of positive neutralizing antibody activities against more resistant viral isolate with a significantly higher CD4 binding site (CD4bs) antibody response compared to both HVTN studies #041 and #203. No differences were found in CD4-induced (CD4i) antibody responses, ADCC activity, or complement activation by Env-specific antibody among these sera. Given recent renewed interest in realizing the importance of antibody responses for next generation HIV vaccine development, different antibody profiles shown in the current report, based on the analysis of a wide range of antibody parameters, provide critical biomarker information for the selection of HIV vaccines for more advanced human studies and, in particular, those that can elicit antibodies targeting conformational-sensitive and functionally conserved epitopes

Public Library of Science (PLOS)

Knockout and transgenic mice of Trp53: what have we learned about p53 in breast cancer?

The human p53 tumor suppressor gene TP53 is mutated at a high frequency in sporadic breast cancer, and Li-Fraumeni syndrome patients who carry germline mutations in one TP53 allele have a high incidence of breast cancer. In the 10 years since the first knockout of the mouse p53 tumor suppressor gene (designated Trp53) was published, much has been learned about the contribution of p53 to biology and tumor suppression in the breast through the use of p53 transgenic and knockout mice. The original mice deficient in p53 showed no mammary gland phenotype. However, studies using BALB/c-Trp53-deficient mice have demonstrated a delayed involution phenotype and a mammary tumor phenotype. Together with other studies of mutant p53 transgenes and p53 bitransgenics, a greater understanding has been gained of the role of p53 in involution, of the regulation of p53 activity by hormones, of the effect of mouse strain and modifier genes on tumor phenotype, and of the cooperation between p53 and other oncogenic pathways, chemical carcinogens and hormonal stimulation in mammary tumorigenesis. Both p53 transgenic and knockout mice are important in vivo tools for understanding breast cancer, and are yet to be exploited for developing therapeutic strategies in breast cancer

Crossref

ScholarWorks@UMass Amherst

PubMed Central

Jet energy measurement with the ATLAS detector in proton-proton collisions at root s=7 TeV

Author: Aad G
Abbott B
Abdallah J
Abdelalim AA
Abdesselam A
Abdinov O
Abi B
Abolins M
Abramowicz H
Abreu H
Acerbi E
Acharya BS
Adams DL
Addy TN
Adelman J
Aderholz M
Adomeit S
Adragna P
Adye T
Aefsky S
Aguilar-Saavedra JA
Aharrouche M
Ahlen SP
Ahles F
Ahmad A
Ahsan M
Aielli G
Akdogana T
Akesson TPA
Akimoto G
Akimov AV
Akiyama A
Aktas A
Alam MA
Alam MS
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
Aliyev M
Allport PP
Allwood-Spiers SE
Almenar CC
Almond J
Aloisio A
Alon R
Alonso A
Alviggi MG
Amako K
Amaral P
Amelung C
Ammosov VV
Amorim A
Amoros G
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
Angerami A
Anghinolfi F
Anh TV
Anjos N
Annovi A
Antonaki A
Antonelli M
Antonov A
Antos J
Anulli F
Aoun S
Apolle R
Arabidze G
Aracena I
Arai Y
Aranda CP
Arce ATH
Archambault JP
Arfaoui S
Arguin J-F
Arik E
Arik M
Armbruster AJ
Arnaez O
Arnault C
Artamonov A
Artoni G
Arutinov D
Asai S
Asfandiyarov R
Ask S
Asman B
Asner D
Asquith L
Assamagan K
Astbury A
Astvatsatourov A
Atoian G
Aubert B
Auge E
Augsten K
Aurousseau M
Austin N
Avolio G
Avramidou R
Axen D
Ay C
Azuelos G
Azuma Y
Baak MA
Baccaglioni G
Bacci C
Bach AM
Bachacou H
Bachas K
Bachy G
Backes M
Backhaus M
Badescu E
Bagnaia P
Bahinipati S
Bai Y
Bailey DC
Bain T
Baines JT
Baker MD
Baker OK
Baker S
Banas E
Banerjee P
Banerjee S
Banfi D
Bangert A
Bansal V
Bansil HS
Barajas CAC
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Baranov SP
Barashkou A
Barber T
Barberio EL
Barberis D
Barbero M
Bardin DY
Barillari T
Barisonzi M
Barklow T
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Barnett BM
Barnett RM
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Batley JR
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Battistoni G
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Beauchemin PH
Beccherle R
Bechtle P
Beck GA
Beck HP
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Becks KH
Beddall A
Beddall AJ
Bedikian S
Bednyakov VA
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Behera PK
Beimforde M
Belanger-Champagne C
Belenguer MJ
Bell PJ
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Bella LA
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Bellina F
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Botterill D
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Boyko IR
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Bozovic-Jelisavcic I
Bracinik J
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Brodbeck TJ
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Castanheira MTD
Castillo LRF
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Chekanov S
Chekulaev SV
Chelkov GA
Chelstowska MA
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Chen H
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Chen X
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Cheong ALF
Cheplakov A
Chepurnov VF
Chernyatin V
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Collaboration ATLAS
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Curtis CJ
Curull XE
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Czyczula Z
D'Auria S
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D'Orazio A
Da Costa JBG
Da Costa JGPF
Da Silva PVM
Da Via C
Dabrowski W
Dai T
Dallapiccola C
Daly CH
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Danielsson HO
Dannheim D
Dao V
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Favareto A
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Fazio S
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Ferrere D
Ferretti C
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Fiedler F
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Filippas A
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Fiolhais MCN
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Fisher MJ
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Flechl M
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Kotamaki MJ
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Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/03/2013
Field of study

The jet energy scale and its systematic uncertainty are determined for jets measured with the ATLAS detector at the LHC in proton-proton collision data at a centre-of-mass energy of √s = 7TeV corresponding to an integrated luminosity of 38 pb-1. Jets are reconstructed with the anti-kt algorithm with distance parameters R=0. 4 or R=0. 6. Jet energy and angle corrections are determined from Monte Carlo simulations to calibrate jets with transverse momenta pT≥20 GeV and pseudorapidities {pipe}η{pipe}<4. 5. The jet energy systematic uncertainty is estimated using the single isolated hadron response measured in situ and in test-beams, exploiting the transverse momentum balance between central and forward jets in events with dijet topologies and studying systematic variations in Monte Carlo simulations. The jet energy uncertainty is less than 2. 5 % in the central calorimeter region ({pipe}η{pipe}<0. 8) for jets with 60≤pT<800 GeV, and is maximally 14 % for pT<30 GeV in the most forward region 3. 2≤{pipe}η{pipe}<4. 5. The jet energy is validated for jet transverse momenta up to 1 TeV to the level of a few percent using several in situ techniques by comparing a well-known reference such as the recoiling photon pT, the sum of the transverse momenta of tracks associated to the jet, or a system of low-pT jets recoiling against a high-pT jet. More sophisticated jet calibration schemes are presented based on calorimeter cell energy density weighting or hadronic properties of jets, aiming for an improved jet energy resolution and a reduced flavour dependence of the jet response. The systematic uncertainty of the jet energy determined from a combination of in situ techniques is consistent with the one derived from single hadron response measurements over a wide kinematic range. The nominal corrections and uncertainties are derived for isolated jets in an inclusive sample of high-pT jets. Special cases such as event topologies with close-by jets, or selections of samples with an enhanced content of jets originating from light quarks, heavy quarks or gluons are also discussed and the corresponding uncertainties are determined. © 2013 CERN for the benefit of the ATLAS collaboration

Oxford University Research Archive

Queen Mary Research Online

Measurement of the inclusive and dijet cross-sections of b-jets in pp collisions at sqrt(s) = 7 TeV with the ATLAS detector

Author: Aad G
Abbott B
Abdallah J
Abdelalim AA
Abdesselam A
Abdinov O
Abi B
Abolins M
Abramowicz H
Abreu H
Acerbi E
Acharya BS
Ackers M
Adams DL
Addy TN
Adelman J
Aderholz M
Adomeit S
Adragna P
Adye T
Aefsky S
Aguilar-Saavedra JA
Aharrouche M
Ahlen SP
Ahles F
Ahmad A
Ahsan M
Aielli G
Akdogan T
Akesson TPA
Akimoto G
Akimov AV
Alam MA
Alam MS
Albrand S
Aleksa M
Aleksandrov IN
Aleppo M
Alessandria F
Alexa C
Alexander G
Alexandre G
Alexopoulos T
Alhroob M
Aliev M
Alimonti G
Alison J
Aliyev M
Allport PP
Allwood-Spiers SE
Almenar CC
Almond J
Aloisio A
Alon R
Alonso A
Alonso J
Alviggi MG
Amako K
Amaral P
Amelung C
Ammosov VV
Amorim A
Amoros G
Amram N
Anastopoulos C
Andari N
Andeen T
Anders CF
Anderson KJ
Andreazza A
Andrei V
Andrieux M-L
Anduaga XS
Angerami A
Anghinolfi F
Anh TV
Anjos N
Annovi A
Antonaki A
Antonelli M
Antonelli S
Antos J
Anulli F
Aoun S
Apolle R
Arabidze G
Aracena I
Arai Y
Arce ATH
Archambault JP
Arfaoui S
Arguin J-F
Arik E
Arik M
Armbruster AJ
Arms KE
Armstrong SR
Arnaez O
Arnault C
Artamonov A
Artoni G
Arutinov D
Asai S
Asfandiyarov R
Ask S
Asman B
Asquith L
Assamagan K
Astbury A
Astvatsatourov A
Atoian G
Aubert B
Auerbach B
Auge E
Augsten K
Aurousseau M
Austin N
Avramidou R
Axen D
Ay C
Azuelos G
Azuma Y
Baak MA
Baccaglioni G
Bacci C
Bach AM
Bachacou H
Bachas K
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Badescu E
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Bai Y
Bailey DC
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Bangert A
Bansal V
Bansil HS
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Baranov SP
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Barberio EL
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Bardin DY
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Barisonzi M
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Barnett BM
Barnett RM
Baroncelli A
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Barrera CO
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Cheong ALF
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Chepurnov VF
Cherkaoui El Moursli R
Chernyatin V
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Childers JT
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Chizhov MV
Choudalakis G
Chouridou S
Christidi IA
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Chromek-Burckhart D
Chu ML
Chudoba J
Ciapetti G
Ciftci AK
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Cinca D
Cindro V
Ciobotaru MD
Ciocca C
Ciocio A
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Ciubancan M
Clark A
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Cleland W
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Collaboration A
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do Vale MAB
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Federic P
Fedin OL
Fedorko I
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Gordon HA
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Hernandez Jimenez Y
Hernandez AMC
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zur Nedden M
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Zwalinski L
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 31/12/2010
Field of study

The inclusive and dijet production cross-sections have been measured for jets containing b-hadrons (b-jets) in proton-proton collisions at a centre-of-mass energy of sqrt(s) = 7 TeV, using the ATLAS detector at the LHC. The measurements use data corresponding to an integrated luminosity of 34 pb^-1. The b-jets are identified using either a lifetime-based method, where secondary decay vertices of b-hadrons in jets are reconstructed using information from the tracking detectors, or a muon-based method where the presence of a muon is used to identify semileptonic decays of b-hadrons inside jets. The inclusive b-jet cross-section is measured as a function of transverse momentum in the range 20 < pT < 400 GeV and rapidity in the range |y| < 2.1. The bbbar-dijet cross-section is measured as a function of the dijet invariant mass in the range 110 < m_jj < 760 GeV, the azimuthal angle difference between the two jets and the angular variable chi in two dijet mass regions. The results are compared with next-to-leading-order QCD predictions. Good agreement is observed between the measured cross-sections and the predictions obtained using POWHEG + Pythia. MC@NLO + Herwig shows good agreement with the measured bbbar-dijet cross-section. However, it does not reproduce the measured inclusive cross-section well, particularly for central b-jets with large transverse momenta.Comment: 10 pages plus author list (21 pages total), 8 figures, 1 table, final version published in European Physical Journal

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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

Author: Aad G
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
Ahles F
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
Alonso A
Alonso F
Altheimer A
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
Andrieux M-L
Anduaga XS
Angelidakis S
Anger P
Angerami A
Anghinolfi F
Anh TV
Anisenkov A
Anjos N
Annovi A
Antonaki A
Antonelli M
Antonov A
Antos J
Anulli F
Aoki M
Aoun S
Apolle R
Arabidze G
Aracena I
Arai Y
Aranda CP
Arce ATH
Arfaoui S
Arguin J-F
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
Astbury A
Atkinson M
Aubert B
Auge E
Augsten K
Aurousseau M
Avolio G
Axen A
Azuelos G
Azuma Y
Baak MA
Baccaglioni G
Bacci C
Bach AM
Bachacou H
Bachas K
Backes M
Backhaus M
Badescu E
Bagnaia P
Bai Y
Bailey DC
Bain T
Baines JT
Baker OK
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Banerjee P
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Banfi D
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Bansil HS
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Baranov SP
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Bell PJ
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Bozovic-Jelisavcic I
Bracinik J
Branchini P
Brandt A
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Brandt O
Bratzler U
Brau B
Brau JE
Braun HM
Brazzale SF
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Budagov IA
Budick B
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Bundock AC
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Castanheira MTD
Castillo Gimenez V
Castillo IS
Castillo LRF
Castro NF
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Cavalcanti TP
Cavaliere V
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Chalupkova I
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Chang P
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Chapman JW
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Chekulaev SV
Chelkov GA
Chelstowska MA
Chen C
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Chen X
Chen Y
Cheng Y
Cheplakov A
Chernyatin V
Cheu E
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Chilingarov A
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Collaboration ATLAS
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Cooper BD
Cooper-Sarkar AM
Copic K
Cornelissen F
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Correia AMH
Corriveau F
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Cortiana G
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Da Costa JGPF
Da Cunha Sargedas De Sousa MJ
Da Via C
Dabrowski V
Dafinca A
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Damazio DO
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Dao V
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De Regie JBDV
de Renstrom PAB
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Degenhardt J
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Delemontex T
Deliyergiyev M
Dell'Acqua A
Dell'Asta L
Della Pietra M
della Porta GZ
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Demirkoz B
Denisov SP
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Deviveiros PO
Dewhurst A
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Di Girolamo A
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Dietzsch TA
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Dinut F
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Do Valle Wemans A
Doan TKO
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Dos Santos DR
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Duerdoth IP
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El Moursli RC
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Espinal Curull X
Esposito B
Etienne F
Etienvre AI
Etzion E
Evangelakou D
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Fabre C
Fajardo LSG
Fakhrutdinov RM
Fakhrutdinov RM
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Fassouliotis D
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Favareto A
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Feng C
Feng EJ
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Ferrando BMS
Ferrando J
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Fiolhais MCN
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Fischer MJ
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Flowerdew MJ
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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
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Bozovic-Jelisavcic I
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Buckley AG
Buda SI
Budagov IA
Budick B
Buescher V
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Caforio D
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Caminal Armadans R
Campana S
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Caprini I
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Castillo Gimenez V
Castro NF
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Cerri A
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Chalupkova I
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Chang P
Chapleau B
Chapman JD
Chapman JW
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Chavda V
Barajas CAC
Cheatham S
Chekanov S
Chekulaev SV
Chelkov GA
Chelstowska MA
Chen C
Chen H
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Chen X
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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Citron ZH
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Ciubancan M
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Clemens JC
Clement B
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Coniavitis E
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Cortiana G
Costa 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
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Dafinca A
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Danielsson HO
Dao V
Darbo G
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Delemontex T
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Dell'Acqua A
Dell'Asta L
Della Pietra M
della Volpe D
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Delsart PA
Deluca C
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Demirkoz B
Denisov SP
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Deviveiros PO
Dewhurst A
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Di Girolamo A
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Dietzsch TA
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Doan TKO
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Dos Anjos A
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Espinal Curull X
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Etienvre AI
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Jez P
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Koi T
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Komar AA
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Kondo T
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Koperny S
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Korolkov I
Korolkova EV
Korotkov VA
Kortner O
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Kostyukhin VV
Kotov S
Kotov VM
Kotwal A
Kourkoumelis C
Kouskoura V
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Kowalewski R
Kowalski TZ
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Olivares Pino SA
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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
Zinonos Z
Zerwas D
della Porta GZ
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
Ziolkowski M
Zitoun R
Zivkovic L
Zmouchko VV
Zobernig G
Zoccoli A
zur Nedden M
Zutshi V
Zwalinski L
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
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 R
Ahmad A
Ahsan M
Aielli G
Akesson TPA
Akimoto G
Akimov AV
Alam MA
Alam MS
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
Almenar CC
Almond J
Aloisio A
Alon R
Alonso A
Alonso F
Altheimer A
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
Anh TV
Anisenkov A
Anjos N
Annovi A
Antonaki A
Antonelli M
Antonov A
Antos J
Anulli F
Aoki M
Aoun S
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
Badescu E
Bagnaia P
Bahinipati S
Bai Y
Bailey DC
Bain T
Baines JT
Baker MD
Baker OK
Baker S
Balek P
Banas E
Banerjee P
Banerjee S
Banfi D
Bangert A
Bansal V
Bansil HS
Barajas CAC
Barak L
Baranov SP
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
Barrera CO
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Bartsch V
Basye A
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Batley JR
Battaglia A
Battistin M
Bauer F
Bawa HS
Beale S
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Beauchemin PH
Beccherle R
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Beck HP
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Becks KH
Beddall A
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Bedikian S
Bednyakov VA
Bee CP
Beemster LJ
Begel M
Behera PK
Beimforde M
Belanger-Champagne C
Belenguer MJ
Bell PJ
Bell WH
Bella G
Bella LA
Bellagamba L
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Beloborodova O
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Benoit M
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Black CW
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Bruckman de Renstrom PA
Bruncko D
Bruneliere R
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Bruni A
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Buanes T
Buat Q
Bucci F
Buchanan J
Buchholz P
Buckingham RM
Buckley AG
Buda SI
Budagov IA
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Bugge L
Bulekov O
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Buran T
Burckhart H
Burdin S
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Busato E
Bussey P
Bustos ACF
Buszello CP
Butler B
Butler JM
Buttar CM
Butterworth JM
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Cabrera Urban S
Caforio D
Cakir IT
Cakir O
Calafiura P
Calderini G
Calfayan P
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Caloba LP
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Calvet D
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Camarri P
Cameron D
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Caminada LM
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Canale V
Canelli F
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Cantero J
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Caprini I
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Catastini R
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Cavalcanti TP
Cavaliere V
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Cavalli D
Cavalli-Sforza M
Cavasinni V
Ceradini F
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Cerri A
Cerrito L
Cerutti F
Cetin SA
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
Chen H
Chen S
Chen X
Chen Y
Cheng Y
Cheplakov A
Chernyatin V
Cheu E
Cheung SL
Chevalier L
Chiefari G
Chikovani L
Childers JT
Chilingarov A
Chiodini G
Chisholm AS
Chislett RT
Chitan A
Chizhov MV
Choudalakis G
Chouridou S
Christidi IA
Christov A
Chromek-Burckhart D
Chu ML
Chudoba J
Ciapetti G
Ciftci AK
Ciftci R
Cinca D
Cindro V
Ciocca C
Ciocio A
Cirilli M
Cirkovic R
Citron ZH
Citterio M
Ciubancan M
Clark A
Clark PJ
Clarke RN
Cleland W
Clemens JC
Clement B
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Cobal M
Coccaro A
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Codina EP
Coffey L
Cogan JG
Coggeshall J
Cogneras E
Colas J
Cole S
Colijn AP
Collaboration A
Collins NJ
Collins-Tooth C
Collot J
Colombo T
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Conde Muino P
Coniavitis E
Conidi MC
Consonni SM
Consorti V
Constantinescu S
Conta C
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Cooke M
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Cooper-Sarkar AM
Copic K
Cornelissen T
Corradi M
Correia AMH
Corriveau F
Cortes-Gonzalez A
Cortiana G
Costa G
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Cote D
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Cowan G
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Cox BE
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Crepe-Renaudin S
Crescioli F
Cristinziani M
Crosetti G
Cuciuc C-M
Cummings J
Curatolo M
Curtis CJ
Cuthbert C
Cwetanski P
Czirr H
Czodrowski P
Czyczula Z
D'Auria S
D'Onofrio M
D'Orazio A
da Costa JBG
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Da Cunha Sargedas De Sousa MJ
Da Via C
Dabrowski W
Dafinca A
Dai T
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Dam M
Damazio DO
Dameri M
Damiani DS
Danielsson HO
Dao V
Darbo G
Darlea GL
Dassoulas JA
Davey W
Davidek T
Davidson N
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de Asmundis R
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de Graat J
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de Jong P
De la Taille C
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de Lima DEF
de Lima JGR
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de Mora L
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De Regie JBDV
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Dearnaley WJ
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Debenedetti C
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Dedovich DV
Degenhardt J
Del Peso J
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Dell'Acqua A
Dell'Asta L
Della Pietra M
della Porta GZ
della Volpe D
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Delsart PA
Deluca C
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Toro RC
Torregrosa EF
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zur Nedden M
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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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Constitutive Phosphorylation of Aurora-A on Ser51 Induces Its Stabilization and Consequent Overexpression in Cancer

Author: A Castro
A Castro
A Hershko
AC Carrano
AW Murray
C Lindon
C Sakakura
CM Pfleger
CW Carroll
D Guardavaccaro
D Li
D Zhang
E Eytan
H Yamano
H Zhou
HG Nguyen
Hidehiko Kawai
Ikuko Ogawa
JM Peters
JR Bischoff
K Honda
LE Littlepage
LE Littlepage
M Carmena
M Glotzer
M Tatsuka
Masaaki Tatsuka
Michele Pagano
MM Tanner
N Mailand
Nils Cordes
P Meraldi
R Crane
R Reiter
S Anand
S Kitajima
S Rojanala
S Stewart
S Taguchi
Shojiro Kitajima
SS Wang
T Fukuda
T Marumoto
T Ota
T Takahashi
T Tanaka
T Watanabe
T Yagi
Takashi Takata
TM Goepfert
TM Gritsko
V Horn
V Janssens
Y Arlot-Bonnemains
Y Miyoshi
Yasusei Kudo
YM Jeng
Publication venue: Public Library of Science
Publication date: 01/09/2007
Field of study

The serine/threonine kinase Aurora-A (Aur-A) is a proto-oncoprotein overexpressed in a wide range of human cancers. Overexpression of Aur-A is thought to be caused by gene amplification or mRNA overexpression. However, recent evidence revealed that the discrepancies between amplification of Aur-A and overexpression rates of Aur-A mRNA were observed in breast cancer, gastric cancer, hepatocellular carcinoma, and ovarian cancer. We found that aggressive head and neck cancers exhibited overexpression and stabilization of Aur-A protein without gene amplification or mRNA overexpression. Here we tested the hypothesis that aberration of the protein destruction system induces accumulation and consequently overexpression of Aur-A in cancer.Aur-A protein was ubiquitinylated by APC(Cdh1) and consequently degraded when cells exited mitosis, and phosphorylation of Aur-A on Ser51 was observed during mitosis. Phosphorylation of Aur-A on Ser51 inhibited its APC(Cdh1)-mediated ubiquitylation and consequent degradation. Interestingly, constitutive phosphorylation on Ser51 was observed in head and neck cancer cells with protein overexpression and stabilization. Indeed, phosphorylation on Ser51 was observed in head and neck cancer tissues with Aur-A protein overexpression. Moreover, an Aur-A Ser51 phospho-mimetic mutant displayed stabilization of protein during cell cycle progression and enhanced ability to cell transformation.Broadly, this study identifies a new mode of Aur-A overexpression in cancer through phosphorylation-dependent inhibition of its proteolysis in addition to gene amplification and mRNA overexpression. We suggest that the inhibition of Aur-A phosphorylation can represent a novel way to decrease Aur-A levels in cancer therapy

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Progression to AIDS in South Africa Is Associated with both Reverting and Compensatory Viral Mutations

We lack the understanding of why HIV-infected individuals in South Africa progress to AIDS. We hypothesised that in end-stage disease there is a shifting dynamic between T cell imposed immunity and viral immune escape, which, through both compensatory and reverting viral mutations, results in increased viral fitness, elevated plasma viral loads and disease progression. We explored how T cell responses, viral adaptation and viral fitness inter-relate in South African cohorts recruited from Bloemfontein, the Free State (n = 278) and Durban, KwaZulu-Natal (n = 775). Immune responses were measured by γ-interferon ELISPOT assays. HLA-associated viral polymorphisms were determined using phylogenetically corrected techniques, and viral replication capacity (VRC) was measured by comparing the growth rate of gag-protease recombinant viruses against recombinant NL4-3 viruses. We report that in advanced disease (CD4 counts <100 cells/µl), T cell responses narrow, with a relative decline in Gag-directed responses (p<0.0001). This is associated with preserved selection pressure at specific viral amino acids (e.g., the T242N polymorphism within the HLA-B*57/5801 restricted TW10 epitope), but with reversion at other sites (e.g., the T186S polymorphism within the HLA-B*8101 restricted TL9 epitope), most notably in Gag and suggestive of “immune relaxation”. The median VRC from patients with CD4 counts <100 cells/µl was higher than from patients with CD4 counts ≥500 cells/µl (91.15% versus 85.19%, p = 0.0004), potentially explaining the rise in viral load associated with disease progression. Mutations at HIV Gag T186S and T242N reduced VRC, however, in advanced disease only the T242N mutants demonstrated increasing VRC, and were associated with compensatory mutations (p = 0.013). These data provide novel insights into the mechanisms of HIV disease progression in South Africa. Restoration of fitness correlates with loss of viral control in late disease, with evidence for both preserved and relaxed selection pressure across the HIV genome. Interventions that maintain viral fitness costs could potentially slow progression

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Chronic Apocynin Treatment Attenuates Beta Amyloid Plaque Size and Microglial Number in hAPP(751)SL Mice

Author: A Cagnin
A Cordle
A Sasaki
AM Floden
AS Tan
AV Peskin
B Hutter-Paier
B Liu
BA Yankner
BA Yankner
BL Wilkinson
BL Wilkinson
BL Wilkinson
BM Babior
BP Imbimbo
BP Rutten
CK Combs
D Valtier
DC Wu
E Albrecht-Goepfert
E Rockenstein
E Van den Worm
E Werner
EG McGeer
EG Reed-Geaghan
G Li
GF Paxinos
HM Gao
HM Gao
HM Gao
HM Wu
J Rogers
JM Deshusses
L Hui-guo
L Meda
L Qian
L Qin
L Qin
L Qin
LM Sayre
M Wedenig
M Willis
MA Bradley
Melinda E. Lull
Michael J. Surace
Michelle L. Block
ML Block
ML Block
ML Block
ML Block
ML Block
ML Block
MSM Li
N Jantaratnotai
P Cheepsunthorn
PL McGeer
PL McGeer
R Sultana
S Levesque
S Rosi
S Shimohama
SE Hickman
Shannon Levesque
SL Liu
ST Dheen
Stephen D. Ginsberg
W Zhang
WS Griffin
Y Liu
Z Pei
Publication venue: Public Library of Science
Publication date: 01/01/2011
Field of study

Background: NADPH oxidase is implicated in neurotoxic microglial activation and the progressive nature of Alzheimer’s Disease (AD). Here, we test the ability of two NADPH oxidase inhibitors, apocynin and dextromethorphan (DM), to reduce learning deficits and neuropathology in transgenic mice overexpressing human amyloid precursor protein with the Swedish and London mutations (hAPP(751)SL). Methods: Four month old hAPP(751)SL mice were treated daily with saline, 15 mg/kg DM, 7.5 mg/kg DM, or 10 mg/kg apocynin by gavage for four months. Results: Only hAPP(751)SL mice treated with apocynin showed reduced plaque size and a reduction in the number of cortical microglia, when compared to the saline treated group. Analysis of whole brain homogenates from all treatments tested (saline, DM, and apocynin) demonstrated low levels of TNFa, protein nitration, lipid peroxidation, and NADPH oxidase activation, indicating a low level of neuroinflammation and oxidative stress in hAPP(751)SL mice at 8 months of age that was not significantly affected by any drug treatment. Despite in vitro analyses demonstrating that apocynin and DM ameliorate Ab-induced extracellular superoxide production and neurotoxicity, both DM and apocynin failed to significantly affect learning and memory tasks or synaptic density in hAPP(751)SL mice. To discern how apocynin was affecting plaque levels (plaque load) and microglial number in vivo, in vitro analysis of microglia was performed, revealing no apocynin effects on beta-amyloid (Ab) phagocytosis, microglial proliferation, or microglial survival. Conclusions: Together, this study suggests that while hAPP(751)SL mice show increases in microglial number and plaque load, they fail to exhibit elevated markers of neuroinflammation consistent with AD at 8 months of age, which may be a limitation of this animal model. Despite absence of clear neuroinflammation, apocynin was still able to reduce both plaque size and microglial number, suggesting that apocynin may have additional therapeutic effects independent of anti-inflammatory characteristics

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