148 research outputs found
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
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- Barberio EL
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- Bensinger JR
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- Bergsten LJ
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- Black JE
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- Bloch I
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- Blunier Dr
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- Bobrovnikov VS
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- Boeriu OE Vickey
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- Bonilla JS
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- Britton D
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- Buckley AG
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- Bulekov O
- Bullock D
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- Burgard CD
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- Burmeister I
- Burr JTP
- Buschmann E
- Bussey P
- Butler JM
- Buttar CM
- Butterworth JM
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- Buttinger W
- Buzatu A
- Buzykaev AR
- Bylund O Bessidskaia
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- Cabrera Urban S
- Caforio D
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- Cairo VMM
- Cakir I Turk
- Cakir O
- Calace N
- Calafiura P
- Calandri A
- Calderini G
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- Callea G
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- Canale V
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- Capua M
- Carbone RM
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- Carlson BT
- Carminati L
- Carney RMD
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- Carquin E
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- Carrillo-Montoya GD
- Casadei D
- Casado MP
- Casha AF
- Casolino M
- Casper DW
- Castelijn R
- Castillo Gimenez V
- Castillo LR Flores
- Castro NF
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- Catmore JR
- Cattai A
- Caudron J
- Cavaliere V
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- Cavalli-Sforza M
- Cavasinni V
- Celebi E
- Ceradini F
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- 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
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- 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
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- Clement C
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- 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
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- Costa MJ
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- Cottin G
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- Cranmer K
- Crawley SJ
- Creager RA
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- Cristinziani M
- Croft V
- Crosetti G
- Cueto A
- Cukierman AR
- Curatolo M
- Cuth J
- Czekierda S
- Czodrowski P
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- 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
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- 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
- Dittus F
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- Djuvsland JI
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- Dobre M
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- Doglioni C
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- Donadelli M
- Donini J
- Donszelmann T Cuhadar
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- Doria A
- Dova MT
- Doyle AT
- Drechsler E
- Dreyer E
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- Dris M
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- Dubinin F
- Dubreuil A
- Duchovni E
- Duckeck G
- Ducourthial A
- Ducu OA
- Duda D
- Dudarev A
- Dudder A Chr
- Duehrssen M
- Dueren M
- Duffield EM
- Duflot L
- Dulsen C
- Dumancic M
- Dumitriu AE
- Duncan AK
- Dunford M
- Duperrin A
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- Duschinger D
- Dutta B
- Duvnjak D
- Dyndal M
- Dziedzic BS
- Eckardt C
- Ecker KM
- Edgar RC
- Eifert T
- Eigen G
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- Ekelof T
- El Kacimi M
- El Kosseifi R
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- Ellert M
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- Enari Y
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- Favareto A
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- Fedin OL
- Fedorko W
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- Fenyuk AB
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- Ferrando J
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- Fiolhais MCN
- Fiorini L
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- Fleischmann P
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- Flierl BM
- Flores LM
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- Formica A
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- Zu Theenhausen H Meyer
- zur Nedden M
- Zwalinski L
- Publication venue
- 'American Physical Society (APS)'
- Publication date
- 01/01/2018
- Field of study
Get PDFA 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
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
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- Zhemchugov A
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- Zibell A
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- Zorbas TG
- Zou R
- Zur Nedden M
- Zwalinski L
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- 01/01/2018
- Field of study
Get PDFThe 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
Operation and performance of the ATLAS Tile Calorimeter in Run 1
- Author
- Aaboud M
- Aad G
- Abbott B
- Abdallah J
- Abdinov O
- Abeloos B
- Abhayasinghe DK
- Abidi SH
- Abouelfadl 
- 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
- Akerstedt H
- 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
- 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 
- Alviggi MG
- Amadio BT
- Amaral Coutinho Y
- Ambroz L
- Amelung C
- Amidei D
- Amor 
- 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
- Arce ATH
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- Arduh FA
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- Armbruster AJ
- Armitage LJ
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- Black JE
- Black KM
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- Fiolhais MCN
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- Fleck I
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- Kotwal A
- Koulouris A
- Kourkoumeli-Charalampidi A
- Kourkoumelis C
- Kourlitis E
- Kouskoura V
- Kowalewska AB
- Kowalewski R
- Kowalski TZ
- Kozakai C
- Kozanecki W
- Kozhin AS
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- Kramberger G
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- Landon MPJ
- Lanfermann MC
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- Laplace S
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- LeCompte T
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- Lee CA
- Lee GR
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- Leight WA
- Leisos A
- Leite MAL
- Leitner R
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- Lindquist BE
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- Lopez 
- Lopez JA
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- McNamara PC
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- Zwalinski L
- Ženiš T
- Živković L
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- 01/01/2018
- Field of study
Get PDFThe Tile Calorimeter is the hadron calorimeter covering the central region of the ATLAS experiment at the Large Hadron Collider. Approximately 10,000 photomultipliers collect light from scintillating tiles acting as the active material sandwiched between slabs of steel absorber. This paper gives an overview of the calorimeter’s performance during the years 2008–2012 using cosmic-ray muon events and proton–proton collision data at centre-of-mass energies of 7 and 8TeV with a total integrated luminosity of nearly 30 fb−1. The signal reconstruction methods, calibration systems as well as the detector operation status are presented. The energy and time calibration methods performed excellently, resulting in good stability of the calorimeter response under varying conditions during the LHC Run 1. Finally, the Tile Calorimeter response to isolated muons and hadrons as well as to jets from proton–proton collisions is presented. The results demonstrate excellent performance in accord with specifications mentioned in the Technical Design Report
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
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- Zhemchugov A
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- Zhu CG
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- Zhukov K
- Zhulanov V
- Zibell A
- Zieminska D
- Zimine NI
- Zimmermann S
- Zinonos Z
- Zinser M
- Ziolkowski M
- Zobernig G
- Zoccoli A
- Zoch K
- Zorbas TG
- Zou R
- Zur Nedden M
- Zwalinski L
- Álvarez Piqueras D
- Åkesson TPA
- Šfiligoj T
- Ženiš T
- Živković L
- Publication venue
- Elsevier
- Publication date
- 01/01/2018
- Field of study
Get PDFA 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
Search for pairs of highly collimated photon-jets in pp collisions 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
- Akesson TPA
- Akilli E
- Akimov AV
- Alberghi GL
- Alberich L Cerda
- Albert J
- Albicocco P
- Alderweireldt S
- Aleksa M
- Aleksandrov IN
- Alexa C
- Alexander G
- Alexopoulos T
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- Ali B
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- Allbrooke BMM
- Allen BW
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- Alvarez Piqueras D
- Alviggi MG
- Amadio BT
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- Amelung C
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- Anders CF
- Anders JK
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- Andreazza A
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- Anelli CR
- Angelidakis S
- Angelozzi I
- Angerami A
- Anisenkov AV
- Annovi A
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- Anthony MT
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- Antrim DJA
- Anulli F
- Aoki M
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- Araya S Tapia
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- Ardell RE
- Arduh FA
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- Armadans R Caminal
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- Viazlo O
- Vichou I
- Vickey OE
- Vickey T
- Viehhauser GHA
- Viel S
- Vigani L
- Villa M
- Villar DI Narrias
- Vilucchi E
- Vincter MG
- Vinogradov VB
- Vishwakarma A
- Vittori C
- Vivarelli I
- Vlachos S
- Vogel M
- Vokac P
- Volpi G
- von Buddenbrock SE
- Von Toerne E
- Vorobel V
- Vorobev K
- Vos M
- Vossebeld JH
- Vranjes N
- Vrba V
- Vreeswijk M
- Vuillermet R
- Vukotic I
- Wagner P
- Wagner W
- Wagner-Kuhr J
- Wahlberg H
- Wahrmund S
- Wakamiya K
- Walbrecht VM
- Walder J
- Walker R
- Walkowiak W
- Wallangen V
- Wang AM
- Wang C
- Wang F
- Wang H
- Wang H
- Wang J
- Wang J
- Wang P
- Wang Q
- Wang R
- Wang R
- Wang R-J
- Wang SM
- Wang W
- Wang WT
- Wang WX
- Wang Y
- Wang Z
- Wanotayaroj C
- Warburton A
- Ward CP
- Wardrope DR
- Washbrook A
- Watkins PM
- Watson AT
- Watson MF
- Watts G
- Watts S
- Waugh BM
- Webb AF
- Webb S
- Weber C
- Weber MS
- Weber SA
- Weber SM
- Webster JS
- Weidberg AR
- Weinert B
- Weingarten J
- Weirich M
- Weiser C
- Wells PS
- Wenaus T
- Wengler T
- Wenig S
- Wermes N
- Werner MD
- Werner P
- Wessels M
- Weston TD
- Whalen K
- Whallon NL
- Wharton AM
- White A
- White AS
- White MJ
- White R
- Whiteson D
- Whitmore BW
- Wickens FJ
- Wiedenmann W
- Wielers M
- Wiglesworth C
- Wiik-Fuchs LAM
- Wildauer A
- Wilk F
- Wilkens HG
- Wilkins LJ
- Williams HH
- Williams S
- Willis C
- Willocq S
- Wilson JA
- Wingerter-Seez I
- Winkels E
- Winklmeier F
- Winston OJ
- Winter BT
- Wittgen M
- Wobisch M
- Wolf A
- Wolf TMH
- Wolff R
- Wolter MW
- Wolters H
- Wong VWS
- Woods NL
- Worm SD
- Wosiek BK
- Wozniak KW
- Wraight K
- Wu M
- Wu SL
- Wu X
- Wu Y
- Wyatt TR
- Wynne BM
- Xella S
- Xi Z
- Xia L
- Xu D
- Xu H
- Xu L
- Xu T
- Xu W
- Yabsley B
- Yacoob S
- Yajima K
- Yallup DP
- Yamaguchi D
- Yamaguchi Y
- Yamamoto A
- Yamanaka T
- Yamane F
- Yamatani M
- Yamazaki T
- Yamazaki Y
- Yan Z
- Yang HJ
- Yang HT
- Yang S
- Yang Y
- Yang Z
- Yao W-M
- Yap YC
- Yasu Y
- Yatsenko E
- Ye J
- Ye S
- Yeletskikh I
- Yigitbasi E
- Yildirim E
- Yildiz H Duran
- Yorita K
- Yoshihara K
- Young C
- Young CJS
- Yu J
- Yu J
- Yue X
- Yuen SPY
- Yusuff I
- Zabinski B
- Zacharis G
- Zaffaroni E
- Zaidan R
- Zaitsev AM
- Zakharchuk N
- Zalieckas J
- Zambito S
- Zanzi D
- Zaripovas DR
- Zeissner SV
- Zeitnitz C
- Zemaityte G
- Zeng JC
- Zeng Q
- Zenin O
- Zenis T
- Zerwas D
- Zgubic M
- Zhang D
- Zhang DF
- Zhang F
- Zhang G
- Zhang H
- Zhang J
- Zhang L
- Zhang L
- Zhang M
- Zhang P
- Zhang R
- Zhang R
- Zhang X
- Zhang Y
- Zhang Z
- Zhao P
- Zhao X
- Zhao Y
- Zhao Z
- Zhemchugov A
- Zhou B
- Zhou C
- Zhou L
- Zhou M
- Zhou MS
- Zhou N
- Zhou Y
- Zhu CG
- Zhu H
- Zhu HL
- Zhu J
- Zhu Y
- Zhuang X
- Zhukov K
- Zhulanov V
- Zibell A
- Zieminska D
- Zimine NI
- Zimmermann S
- Zinonos Z
- Zinser M
- Ziolkowski M
- Zivkovic L
- Zobernig G
- Zoccoli A
- Zoch K
- Zorbas TG
- Zou R
- Zu Theenhausen H Meyer
- Zur Nedden M
- Zwalinski L
- Publication venue
- 'American Physical Society (APS)'
- Publication date
- 01/08/2018
- Field of study
Get PDFResults of a search for the pair production of photon-jets—collimated groupings of photons—in the ATLAS detector at the Large Hadron Collider are reported. Highly collimated photon-jets can arise from the decay of new, highly boosted particles that can decay to multiple photons collimated enough to be identified in the electromagnetic calorimeter as a single, photonlike energy cluster. Data from proton-proton collisions at a center-of-mass energy of 13 TeV, corresponding to an integrated luminosity of 36.7 fb−1, were collected in 2015 and 2016. Candidate photon-jet pair production events are selected from those containing two reconstructed photons using a set of identification criteria much less stringent than that typically used for the selection of photons, with additional criteria applied to provide improved sensitivity to photon-jets. Narrow excesses in the reconstructed diphoton mass spectra are searched for. The observed mass spectra are consistent with the Standard Model background expectation. The results are interpreted in the context of a model containing a new, high-mass scalar particle with narrow width, X, that decays into pairs of photon-jets via new, light particles, a. Upper limits are placed on the cross section times the product of branching ratios σ×B(X→aa)×B(a→γγ)2 for 200 GeV<mX<2 TeV and for ranges of ma from a lower mass of 100 MeV up to between 2 and 10 GeV, depending upon mX. Upper limits are also placed on σ×B(X→aa)×B(a→3π0)2 for the same range of mX and for ranges of ma from a lower mass of 500 MeV up to between 2 and 10 GeV
Immunohistochemical Detection of MYC-driven Diffuse Large B-Cell Lymphomas
- Author
- A Subramanian
- A Subramanian
- Alyssa Roy
- Bjoern Chapuy
- Donna S. Neuberg
- EC Obermann
- G Salles
- Geraldine S. Pinkus
- HW Zhang
- IT Magrath
- JL Hecht
- JR Cook
- KJ Savage
- LH Sehn
- Luwen Zhang
- M Bonnet
- M Hummel
- M Mino-Kenudson
- Margaret A. Shipp
- MB Ruzinova
- Michael J. Kluk
- N Meyer
- Paola Dal Cin
- Papiya Sinha
- S Barrans
- S Monti
- Scott J. Rodig
- SH Swerdlow
- SS Dave
- Stefano Monti
- TM Habermann
- Publication venue
- Public Library of Science
- Publication date
- 12/04/2012
- Field of study
Get PDFDiffuse large B cell lymphoma (DLBCL) is a clinically and genetically heterogeneous disease. A small subset of DLBCLs has translocations involving the MYC locus and an additional group has a molecular signature resembling Burkitt lymphoma (mBL). Presently, identification of such cases by morphology is unreliable and relies on cytogenetic or complex molecular methods such as gene transcriptional profiling. Herein, we describe an immunohistochemical (IHC) method for identifying DLBCLs with increased MYC protein expression. We tested 77 cases of DLBCL and identified 15 cases with high MYC protein expression (nuclear staining in >50% of tumor cells). All MYC translocation positive cases had increased MYC protein expression by this IHC assay. In addition, gene set enrichment analysis (GSEA) of the DLBCL transcriptional profiles revealed that tumors with increased MYC protein expression (regardless of underlying MYC translocation status) had coordinate upregulation of MYC target genes, providing molecular confirmation of the IHC results. We then generated a molecular classifier derived from the MYC IHC results in our cases and employed it to successfully classify mBLs from two previously reported independent case series, providing additional confirmation that the MYC IHC results identify clinically important subsets of DLBCLs. Lastly, we found that DLBCLs with high MYC protein expression had inferior overall survival when treated with R-CHOP. In conclusion, the IHC method described herein can be used to readily identify the biologically and clinically distinct cases of MYC-driven DLBCL, which represent a clinically significant subset of DLBCL cases due to their inferior overall survival
Expression of minichromosome maintenance protein 2 as a marker for proliferation and prognosis in diffuse large B-cell lymphoma: a tissue microarray and clinico-pathological analysis
- Author
- A Freeman
- A Tzankov
- A Tzankov
- AA Alizadeh
- Alexandar Tzankov
- AN Cheung
- Annette Zimpfer
- AR Martin
- BK Tye
- C Musahl
- CM Quinn
- DC Brown
- DE MacCallum
- DP Hunt
- E Bjorck
- E Endl
- EC Obermann
- Ellen C Obermann
- ES Jaffe
- GH Williams
- H Kato
- I Kodani
- IT Todorov
- JJ Going
- JN Winter
- K Gronbaek
- K Hashimoto
- K Rodins
- K Stoeber
- K Stoeber
- L Toschi
- M Czader
- M Llanos
- M Ritzi
- MA Gonzalez
- MA Shipp
- MB Moller
- MB Moller
- MV Meng
- P Chatrath
- P Romanowski
- P Schraml
- P Went
- PA Hall
- PC Burger
- Peter J Wild
- Philip Went
- R Verheijen
- RI Fisher
- RJ Davies
- Robert Stoehr
- S Kruger
- SB Wharton
- SS Li
- Stefano A Pileri
- Stephan Dirnhofer
- T Scholzen
- TP Miller
- WC Xue
- Publication venue
- BioMed Central
- Publication date
- 01/01/2005
- Field of study
Get PDFBACKGROUND: Minichromosome maintenance (MCM) proteins are essential for the initiation of DNA replication and have been found to be relevant markers for prognosis in a variety of tumours. The aim of this study was to assess the proliferative activity of diffuse large B-cell lymphoma (DLBCL) in tissue microarray (TMA) using one of the minichromosome maintenance proteins (Mcm2) and to explore its potential value to predict prognosis. METHODS: Immunohistochemistry for Mcm2 was performed on TMAs constructed from 302 cases of DLBCL. A monoclonal mouse antibody was used after heat induced antigen retrieval. Mcm2 expression was scored quantitatively. Positivity for Mcm2 was defined as presence of nuclear expression of Mcm2 in greater than or equal to 40 % of tumour cells. A statistical analysis was carried out of the association of Mcm2 and the clinico-pathological characteristics. RESULTS: Mcm2 expression was clearly evident in the nuclei of proliferating non-neoplastic cells and tumour cells. Positivity for Mcm2 was found in 46% (98/211) of analysable cases. A significant correlation existed between Mcm2 expression and presence of bulky disease (p = 0.003). Poor disease specific survival was observed in patients with DLBCL positive for Mcm2 expression in the univariate analysis (p = 0.0424). CONCLUSION: Mcm2 expression can be used to assess tumour proliferation and may be useful as an additional prognostic marker to refine the prediction of outcome in DLBCL
New developments in the pathology of malignant lymphoma: a review of the literature published from August to November 2009
- Author
- A Bric
- A Gloghini
- A Mannini
- A Mottok
- A Navarro
- AM Bogusz
- BG Richendollar
- C Youssif
- CE Balatoni
- CE Meacham
- D Wu
- D Zhang
- E Kan
- EC Obermann
- FR Loberiza Jr
- H Adams
- J. Han van Krieken
- JX Zhou
- K Mangseth
- K Raparia
- M Higashi
- MA Lorenzetti
- N Wada
- Q Zhang
- RL King
- RN Miranda
- RP Hasserjian
- RR Miles
- S Eckerle
- S Gujral
- S Kalungi
- S Muenst
- SE Monaco
- W Klapper
- WW Choi
- Y Natkunam
- YY Kong
- Publication venue
- Springer-Verlag
- Publication date
- 01/01/2009
- Field of study
Get PDFFLT3 mutations in canine acute lymphocytic leukemia
- Author
- AJ Dunbar
- B Etschmann
- C Choudhary
- C Choudhary
- C Khanna
- CE Carow
- D Small
- DG Gilliland
- DL Stirewalt
- DM Vail
- EC Obermann
- Eric L Seiser
- F Birg
- FM Abu-Duhier
- G Meierhoff
- George W Small
- H Kiyoi
- H Quentmeier
- HG Drexler
- K Lindblad-Toh
- K Spiekermann
- Kristy L Richards
- L Li
- LY Shih
- M Breen
- M Levis
- M Nakaichi
- M Nakao
- Matthew Breen
- MW Pfaffl
- P Brown
- PD Kottaridis
- PS Wunderli
- R Grundler
- Rachael Thomas
- S Meshinchi
- S Meshinchi
- SE Suter
- SG Usher
- Steven E Suter
- Y Yamamoto
- Z Steplewski
- Publication venue
- BioMed Central
- Publication date
- 01/01/2011
- Field of study
Get PDF<p>Abstract</p> <p>Background</p> <p>FMS-like tyrosine kinase 3 (FLT3) is a commonly mutated protein in a variety of human acute leukemias. Mutations leading to constitutively active FLT3, including internal tandem duplications of the juxtamembrane domain (ITD), result in continuous cellular proliferation, resistance to apoptotic cell death, and a poorer prognosis. A better understanding of the molecular consequences of FLT3 activation would allow improved therapeutic strategies in these patients. Canine lymphoproliferative diseases, including lymphoma and acute leukemias, share evolutionarily conserved chromosomal aberrations and exhibit conserved mutations within key oncogenes when compared to their human counterparts. A small percentage of canine acute lymphocytic leukemias (ALL) also exhibit <it>FLT3 </it>ITD mutations.</p> <p>Methods</p> <p>We molecularly characterized <it>FLT3 </it>mutations in two dogs and one cell line, by DNA sequencing, gene expression analysis via quantitative real-time PCR, and sensitivity to the FLT3 inhibitor lestaurtinib via <it>in vitro </it>proliferation assays. FLT 3 and downstream mediators of FLT3 activation were assessed by Western blotting.</p> <p>Results</p> <p>The canine B-cell leukemia cell line, GL-1, and neoplastic cells from 2/7 dogs diagnosed cytologically with ALL were found to have <it>FLT3 </it>ITD mutations and <it>FLT3 </it>mRNA up-regulation. Lestaurtinib, a small molecule FLT3 inhibitor, significantly inhibited the growth of GL-1 cells, while not affecting the growth of two other canine lymphoid cell lines without the <it>FLT3 </it>mutation. Finally, western blots were used to confirm the conserved downstream mediators of <it>FLT3 </it>activating mutations.</p> <p>Conclusions</p> <p>These results show that ALL and FLT3 biology is conserved between canine and human patients, supporting the notion that canine ALL, in conjunction with the GL-1 cell line, will be useful in the development of a relevant large animal model to aid in the study of human FLT3 mutant leukemias.</p
Functional Characterization of FLT3 Receptor Signaling Deregulation in Acute Myeloid Leukemia by Single Cell Network Profiling (SCNP)
- Author
- A Pradhan
- AI Svirnovski
- Aileen Cohen
- AJ Shah
- Alessandra Cesano
- BD Cheson
- BJ Wouters
- C Choudhary
- C Choudhary
- C Lavagna-Sevenier
- C Scholl
- C Seedhouse
- C Thiede
- CD Baldus
- CL Green
- David B. Rosen
- DL Stirewalt
- DS Krause
- EC Obermann
- Erik Evensen
- F Hayakawa
- G Marcucci
- GT Stelzer
- H Dohner
- H Kiyoi
- I Moreno
- IP Touw
- J Seita
- JA Hanley
- JA Hanley
- JL Tang
- JM Irish
- JM Irish
- John Woronicz
- K Dohner
- K Sachs
- LS Rusten
- M Beran
- M Brown
- M Dosil
- M Kondo
- M Mizuki
- Mark D. Minden
- MH Sheikhha
- N Chalhoub
- O Bruserud
- O Rosnet
- P Gorello
- PD Kottaridis
- PO Krutzik
- R Grundler
- RE Gale
- RE Gale
- RF Schlenk
- RG Verhaak
- S Frohling
- S Kayser
- S Meshinchi
- S Meshinchi
- S Meshinchi
- S Schnittger
- S Zhang
- S Zhang
- Santosh Putta
- SD de Jonge-Peeters
- SD Lyman
- SJ Baker
- SM Kornblau
- SP Srinivasa
- SP Whitman
- Steven M. Kornblau
- T Iwai
- Terence Lee
- TM Covey
- Urte Gayko
- V Bewick
- Wendy J. Fantl
- Y Kikushige
- Y Yamamoto
- Publication venue
- Public Library of Science
- Publication date
- 27/10/2010
- Field of study
Get PDFMolecular characterization of the FMS-like tyrosine kinase 3 receptor (FLT3) in cytogenetically normal acute myeloid leukemia (AML) has recently been incorporated into clinical guidelines based on correlations between FLT3 internal tandem duplications (FLT3-ITD) and decreased disease-free and overall survival. These mutations result in constitutive activation of FLT3, and FLT3 inhibitors are currently undergoing trials in AML patients selected on FLT3 molecular status. However, the transient and partial responses observed suggest that FLT3 mutational status alone does not provide complete information on FLT3 biological activity at the individual patient level. Examination of variation in cellular responsiveness to signaling modulation may be more informative.Using single cell network profiling (SCNP), cells were treated with extracellular modulators and their functional responses were quantified by multiparametric flow cytometry. Intracellular signaling responses were compared between healthy bone marrow myeloblasts (BMMb) and AML leukemic blasts characterized as FLT3 wild type (FLT3-WT) or FLT3-ITD. Compared to healthy BMMb, FLT3-WT leukemic blasts demonstrated a wide range of signaling responses to FLT3 ligand (FLT3L), including elevated and sustained PI3K and Ras/Raf/Erk signaling. Distinct signaling and apoptosis profiles were observed in FLT3-WT and FLT3-ITD AML samples, with more uniform signaling observed in FLT3-ITD AML samples. Specifically, increased basal p-Stat5 levels, decreased FLT3L induced activation of the PI3K and Ras/Raf/Erk pathways, decreased IL-27 induced activation of the Jak/Stat pathway, and heightened apoptotic responses to agents inducing DNA damage were observed in FLT3-ITD AML samples. Preliminary analysis correlating these findings with clinical outcomes suggests that classification of patient samples based on signaling profiles may more accurately reflect FLT3 signaling deregulation and provide additional information for disease characterization and management.These studies show the feasibility of SCNP to assess modulated intracellular signaling pathways and characterize the biology of individual AML samples in the context of genetic alterations
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