103 research outputs found
Lactate Dehydrogenase-B Is Silenced by Promoter Methylation in a High Frequency of Human Breast Cancers
- Author
- A Glen
- A Jemal
- A Le
- A Leiblich
- AC Liao
- AM Gonzalez-Angulo
- Branko Perunovic
- CA Pettaway
- CL Markert
- CV Dang
- EK Rofstad
- F Hirschhaeuser
- FR Miller
- I Rehman
- Ishtiaq Rehman
- JW Kim
- K Yoshikuni
- L Elbarghati
- M Esteller
- M Lopez-Lazaro
- M Maekawa
- M Zhou
- MH Forouzanfar
- MI Koukourakis
- MI Koukourakis
- MI Koukourakis
- MI Koukourakis
- Mohammad Arafa
- N Draoui
- Nicola J. Brown
- O Feron
- P Dell' Antone
- P Montcourrier
- P Seth
- P Vaupel
- Paul van Diest
- R Hussien
- RA Gatenby
- RE Burke
- RL Momparler
- S Dhup
- Sabapathy Balasubramanian
- SC Tsoi
- SJ Bensinger
- Sue E. Higham
- W Zhou
- WH Koppenol
- Y Kolev
- ZY Wang
- Publication venue
- 'Public Library of Science (PLoS)'
- Publication date
- 21/02/2013
- Field of study
Get PDFObjective: Under normoxia, non-malignant cells rely on oxidative phosphorylation for their ATP production, whereas cancer cells rely on Glycolysis; a phenomenon known as the Warburg effect. We aimed to elucidate the mechanisms contributing to the Warburg effect in human breast cancer.
Experimental design: Lactate Dehydrogenase (LDH) isoenzymes were profiled using zymography. LDH-B subunit expression was assessed by reverse transcription PCR in cells, and by Immunohistochemistry in breast tissues. LDH-B promoter methylation was assessed by sequencing bisulfite modified DNA.
Results: Absent or decreased expression of LDH isoenzymes 1-4, were seen in T-47D and MCF7 cells. Absence of LDH-B mRNA was seen in T-47D cells, and its expression was restored following treatment with the demethylating agent 5'Azacytadine. LDH-B promoter methylation was identified in T-47D and MCF7 cells, and in 25/ 25 cases of breast cancer tissues, but not in 5/ 5 cases of normal breast tissues. Absent immuno-expression of LDH-B protein (<10% cells stained), was seen in 23/ 26 (88%) breast cancer cases, and in 4/8 cases of adjacent ductal carcinoma in situ lesions. Exposure of breast cancer cells to hypoxia (1% O2), for 48 hours resulted in significant increases in lactate levels in both MCF7 (14.0 fold, pâ=â0.002), and T-47D cells (2.9 fold, pâ=â0.009), but not in MDA-MB-436 (-0.9 fold, pâ=â0.229), or MCF10AT (1.2 fold, pâ=â0.09) cells.
Conclusions: Loss of LDH-B expression is an early and frequent event in human breast cancer occurring due to promoter methylation, and is likely to contribute to an enhanced glycolysis of cancer cells under hypoxia
Ex Vivo Activity of Cardiac Glycosides in Acute Leukaemia
- Author
- A Perne
- AG Goldin
- Anna Eriksson
- B Stenkvist
- B Stenkvist
- B Stenkvist
- DW Harris
- E Lindhagen
- H Weidemann
- Helene HallbÜÜk
- Irina Agoulnik
- J Felth
- J Haux
- Jenny Felth
- Joachim Gullbo
- K Bielawski
- K Ihenetu
- K Winnicka
- L Naumovski
- Lars Bohlin
- M Lopez-Lazaro
- M Nesher
- MI Khan
- MI Khan
- Mürten Fryknäs
- N Kawazoe
- N Turan
- P Kometiani
- PB Raghavendra
- R Bassan
- R Graves
- R Larsson
- RA Newman
- RA Newman
- Rolf Larsson
- T Bohmer
- T Mekhail
- W Schoner
- WT Beck
- Y Jing
- Y Masuda
- Z Xie
- Publication venue
- Public Library of Science
- Publication date
- 05/01/2011
- Field of study
Get PDFBACKGROUND: Despite years of interest in the anti-cancerous effects of cardiac glycosides (CGs), and numerous studies in vitro and in animals, it has not yet been possible to utilize this potential clinically. Reports have demonstrated promising in vitro effects on different targets as well as a possible therapeutic index/selectivity in vitro and in experimental animals. Recently, however, general inhibition of protein synthesis was suggested as the main mechanism of the anti-cancerous effects of CGs. In addition, evidence of species differences of a magnitude sufficient to explain the results of many studies called for reconsideration of earlier results. PRINCIPAL FINDINGS: In this report we identified primary B-precursor and T-ALL cells as being particularly susceptible to the cytotoxic effects of CGs. Digitoxin appeared most potent and IC(50) values for several patient samples were at concentrations that may be achieved in the clinic. Significant protein synthesis inhibition at concentrations corresponding to IC(50) was demonstrated in colorectal tumour cell lines moderately resistant to the cytotoxic effects of digoxin and digitoxin, but not in highly sensitive leukaemia cell lines. CONCLUSION: It is suggested that further investigation regarding CGs may be focused on diagnoses like T- and B-precursor ALL
Performance of the CMS Cathode Strip Chambers with Cosmic Rays
- Author
- Abadjiev K
- Abbaneo D
- Abbiendi G
- Abbrescia M
- Abdullin S
- Abelev B
- Acosta D
- Acosta JG
- Acosta MV
- Actis O
- Adam N
- Adam W
- Adams MR
- Adams T
- Adiguzel A
- Adler V
- Adolphi R
- Adzic P
- Afaq MA
- Agostino L
- Agram JL
- Aguilar-Benitez M
- Ahmad M
- Ahmad WH
- Ahmed I
- Ahmed W
- Ahuja S
- Aisa D
- Aisa S
- Akchurin N
- Akgun B
- Akgun U
- Akimenko S
- Akin IV
- Alagoz E
- Alampi G
- Albajar C
- Albayrak EA
- Alberdi J
- Albergo S
- Albert E
- Albrow M
- Alexander J
- Alidra M
- Aliev T
- Allfrey P
- Almeida N
- Altenhofer G
- Altsybeev I
- Alver B
- Alverson G
- Alves GA
- Amaglobeli N
- Amapane N
- Ambroglini F
- Amsler C
- Anagnostou G
- Ananthan B
- Anastassov A
- Andelin D
- Anderson M
- Andrea J
- Andreev V
- Andreev Y
- Anghel IM
- Anguelov T
- Anh T. Vu
- Anisimov A
- Antillon E
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- Anttila E
- Antunes JR
- Antunovic Z
- Apanasevich L
- Apollinari G
- Apresyan A
- Arce P
- Arcidiacono R
- Arenton MW
- Arfaei H
- Argiro S
- Arisaka K
- Arneodo M
- Arnold B
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- Asghar MI
- Ashby S
- Askew A
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- Atramentov O
- Auffray E
- Aurisano A
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- Zeidler C
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- Zelepoukine S
- Zeuner WD
- Zeyrek M
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- Zhokin A
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- Zhukov V
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- Ziebarth EB
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- Zinonos Z
- Zito G
- Zoeller MH
- Zotto P
- Zub S
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- 'IOP Publishing'
- Publication date
- 01/01/2009
- Field of study
Get PDFThe Cathode Strip Chambers (CSCs) constitute the primary muon tracking device
in the CMS endcaps. Their performance has been evaluated using data taken
during a cosmic ray run in fall 2008. Measured noise levels are low, with the
number of noisy channels well below 1%. Coordinate resolution was measured for
all types of chambers, and fall in the range 47 microns to 243 microns. The
efficiencies for local charged track triggers, for hit and for segments
reconstruction were measured, and are above 99%. The timing resolution per
layer is approximately 5 ns
Quiescence and ÎłH2AX in neuroblastoma are regulated by ouabain/Na,K-ATPase
- Author
- A Aperia
- A Kulikov
- A Miyakawa
- A Miyakawa-Naito
- AK Tyagi
- AY Bagrov
- B Stenkvist
- B SveinbjĂśrnsson
- BS Huang
- C Vaklavas
- CJ Sherr
- DJ McConkey
- E Wassberg
- GI Evan
- GM Brodeur
- H Hiyoshi
- H van Attikum
- I Prassas
- J Bartek
- J Bartkova
- J I Johnsen
- J Li
- J Luo
- J Tian
- JA Downs
- JH Kaplan
- JH Kim
- JM Maris
- JM Maris
- JR Murrell
- JR Park
- KS Richards
- L Desfrere
- L Desfrere
- L Sang
- L SegerstrĂśm
- M Andang
- M Andäng
- M Lopez-Lazaro
- M Malumbres
- M Nuriya
- M Yasui
- MC Liu
- MD Planas-Silva
- MI Khan
- MM Tomayko
- P Kogner
- P UhlĂŠn
- PJ Hilton
- R Millikan
- RK Wetzel
- S Abdelhady
- S Bao
- S Frese
- S Lapenna
- SP Linke
- T Cheng
- T K Lundgren
- T Mijatovic
- T Waldman
- TD Halazonetis
- W Schoner
- WM Bonner
- WS el-Deiry
- Y Liu
- Publication venue
- Nature Publishing Group
- Publication date
- 01/01/2012
- Field of study
Get PDFCellular quiescence is a state of reversible proliferation arrest that is induced by anti-mitogenic signals. The endogenous cardiac glycoside ouabain is a specific ligand of the ubiquitous sodium pump, Na,K-ATPase, also known to regulate cell growth through unknown signalling pathways.
To investigate the role of ouabain/Na,K-ATPase in uncontrolled neuroblastoma growth we used xenografts, flow cytometry, immunostaining, comet assay, real-time PCR, and electrophysiology after various treatment strategies.
The ouabain/Na,K-ATPase complex induced quiescence in malignant neuroblastoma. Tumour growth was reduced by >50% when neuroblastoma cells were xenografted into immune-deficient mice that were fed with ouabain. Ouabain-induced S-G2 phase arrest, activated the DNA-damage response (DDR) pathway marker ÎłH2AX, increased the cell cycle regulator p21Waf1/Cip1 and upregulated the quiescence-specific transcription factor hairy and enhancer of split1 (HES1), causing neuroblastoma cells to ultimately enter G0. Cells re-entered the cell cycle and resumed proliferation, without showing DNA damage, when ouabain was removed.
Conclusion:
These findings demonstrate a novel action of ouabain/Na,K-ATPase as a regulator of quiescence in neuroblastoma, suggesting that ouabain can be used in chemotherapies to suppress tumour growth and/or arrest cells to increase the therapeutic index in combination therapies
Campylobacter jejuni transcriptome changes during loss of culturability in water
- Author
- A Flint
- A GarĂŠnaux
- A Hitchcock
- A Kloda
- A Kornberg
- A Smith
- A Vendeville
- A Wingstrand
- AD Pearson
- Anita Lucaci
- AW Van de Giessen
- B Langmead
- B Lazaro
- B Said
- BA Rader
- C Berrier
- C Bronowski
- C Friis
- C Murphy
- C Thomas
- CC Tam
- CC Tam
- Charlotte Nelson
- Chloe E. James
- Christina Bronowski
- CM Buswell
- Craig Winstanley
- CS Bakshi
- D Gangaiah
- D Hofreuter
- D Hofreuter
- D Hofreuter
- D Purdy
- DE Fouts
- DG Newell
- DL Wilson
- DM Rollins
- E Laskowska
- EC Pesci
- EV Taylor
- EV Taylor
- FM Colles
- G Haddock
- G Rajashekara
- HL Candon
- I Cools
- I Miettinen
- Ian Goodhead
- IG Jones
- IH Ahmed
- II Kassem
- IR Booth
- J Parkhill
- JL Tholozan
- K Jones
- K Shibayama
- KA Ridley
- Kasem Mustafa
- KB Xavier
- KF Chan
- KT Baek
- KT Young
- L Brøndsted
- M Drozd
- M Hnninen
- M Martin
- M Stahl
- ME Konkel
- MI Van Dyke
- MJ Blaser
- MJ Sellars
- MM Wosten
- MS Pittman
- N French
- Nicola J. Williams
- NJ Williams
- O Gundogdu
- P Glaus
- P Guerry
- Paul Wigley
- PJ Hepworth
- S Anders
- S Goon
- S Guillou
- S Hwang
- S Martin
- S Suerbaum
- S-R Li
- SF Park
- SJ Hall
- SL Svensson
- SM Crim
- SP de Vries
- T Alter
- T Birk
- T Carver
- T Kakuda
- T Seemann
- TJ Carver
- Tom J. Humphrey
- V Patrone
- W Chaisowwong
- WA Day
- WC Hazeleger
- XT Bui
- Yung-Fu Chang
- Publication venue
- 'Public Library of Science (PLoS)'
- Publication date
- 15/06/2017
- Field of study
Get PDFBackground:
Water serves as a potential reservoir for Campylobacter, the leading cause of bacterial gastroenteritis in humans. However, little is understood about the mechanisms underlying variations in survival characteristics between different strains of C. jejuni in natural environments, including water.
Results:
We identified three Campylobacter jejuni strains that exhibited variability in their ability to retain culturability after suspension in tap water at two different temperatures (4°C and 25°C). Of the three strains C. jejuni M1 exhibited the most rapid loss of culturability whilst retaining viability. Using RNAseq transcriptomics, we characterised C. jejuni M1 gene expression in response to suspension in water by analyzing bacterial suspensions recovered immediately after introduction into water (Time 0), and from two sampling time/temperature combinations where considerable loss of culturability was evident, namely (i) after 24 h at 25°C, and (ii) after 72 h at 4°C. Transcript data were compared with a culture-grown control. Some gene expression characteristics were shared amongst the three populations recovered from water, with more genes being up-regulated than down. Many of the up-regulated genes were identified in the Time 0 sample, whereas the majority of down-regulated genes occurred in the 25°C (24 h) sample.
Conclusions:
Variations in expression were found amongst genes associated with oxygen tolerance, starvation and osmotic stress. However, we also found upregulation of flagellar assembly genes, accompanied by down-regulation of genes involved in chemotaxis. Our data also suggested a switch from secretion via the sec system to via the tat system, and that the quorum sensing gene luxS may be implicated in the survival of strain M1 in water. Variations in gene expression also occurred in accessory genome regions. Our data suggest that despite the loss of culturability, C. jejuni M1 remains viable and adapts via specific changes in gene expression
Padrþes de aleitamento materno exclusivo e internação por diarrÊia entre 1999 e 2008 em capitais brasileiras
- Author
- Bahl R
- Benicio MHD'A
- Bittencourt SA
- Boccolini CS
- Caldeira AP
- Cristiano Siqueira Boccolini
- Cruz JR
- Davidson LA
- Escuder MML
- Gissler M
- Goldman AS
- Hengstermann S
- Klein MI
- Kramer MS
- Kramer MS
- Macedo SEC
- Maria InĂŞs Couto de Oliveira
- Matijasevich A
- Morrow AL
- MĂĄrcia Lazaro de Carvalho
- Newburg DS.
- Paramasivam K
- Patricia de Moraes Mello Boccolini
- Quigley MA
- Victora CG
- Vieira GO
- Publication venue
- 'FapUNIFESP (SciELO)'
- Publication date
- Field of study
Full text linkCMS Data Processing Workflows during an Extended Cosmic Ray Run
- Author
- Abadjiev K
- Abbaneo D
- Abbiendi G
- Abbrescia M
- Abdullin S
- Abelev B
- Acosta D
- Acosta JG
- Acosta MV
- Actis O
- Adam N
- Adam W
- Adams MR
- Adams T
- Adiguzel A
- Adler V
- Adolphi R
- Adzic P
- Afaq MA
- Agostino L
- Agram JL
- Aguilar-Benitez M
- Ahmad M
- Ahmad WH
- Ahmed I
- Ahmed W
- Ahuja S
- Aisa D
- Aisa S
- Akchurin N
- Akgun B
- Akgun U
- Akimenko S
- Akin IV
- Alagoz E
- Alampi G
- Albajar C
- Albayrak EA
- Alberdi J
- Albergo S
- Albert E
- Albrow M
- Alexander J
- Alidra M
- Aliev T
- Allfrey P
- Almeida N
- Altenhofer G
- Altsybeev I
- Alver B
- Alverson G
- Alves GA
- Amaglobeli N
- Amapane N
- Ambroglini F
- Amsler C
- Anagnostou G
- Ananthan B
- Anastassov A
- Andelin D
- Anderson M
- Andrea J
- Andreev V
- Andreev Y
- Anghel IM
- Anguelov T
- Anisimov A
- Antillon E
- Antipov P
- Antonelli L
- Anttila E
- Antunes JR
- Antunovic Z
- Apanasevich L
- Apollinari G
- Apresyan A
- Arce P
- Arcidiacono R
- Arenton MW
- Arfaei H
- Argiro S
- Arisaka K
- Arneodo M
- Arnold B
- Arora S
- Artamonov A
- Asaadi J
- Asghar MI
- Ashby S
- Askew A
- Atac M
- Atramentov O
- Auffray E
- Aurisano A
- Autermann C
- Avery P
- Avetisyan A
- Avila C
- Awan MIM
- Ayan AS
- Ayhan A
- Azhgirey I
- Aziz T
- Azzi P
- Azzurri P
- Baarmand MM
- Babb J
- Babucci E
- Baccaro S
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- Bacchi W
- Bachtis M
- Baden D
- Badgett W
- Baechler J
- Baer H
- Baesso P
- Baffioni S
- Bagby L
- Bagliesi G
- Bahk SY
- Bailleux D
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- Bakirci MN
- Bakken JA
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- Baldin B
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- Barashko V
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- Publication venue
- INSTITUTE OF PHYSICS PUBLISHING
- Publication date
- 01/01/2009
- Field of study
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Aligning the CMS Muon Chambers with the Muon Alignment System during an Extended Cosmic Ray Run
- Author
- Abadjiev K
- Abbaneo D
- Abbiendi G
- Abbrescia M
- Abdullin S
- Abelev B
- Acosta D
- Acosta JG
- Acosta MV
- Actis O
- Adam N
- Adam W
- Adams MR
- Adams T
- Adiguzel A
- Adler V
- Adolphi R
- Adzic P
- Afaq MA
- Agostino L
- Agram JL
- Aguilar Benitez M
- Ahmad M
- Ahmad WH
- Ahmed I
- Ahmed W
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- Aisa S
- Akchurin N
- Akgun B
- Akgun U
- Akimenko S
- Akin IV
- Alagoz E
- Alampi G
- Albajar C
- Albayrak EA
- Alberdi J
- Albergo S
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- Alexander J
- Alidra M
- Aliev T
- Allfrey P
- Almeida N
- Altenhofer G
- Altsybeev I
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- Alverson G
- Alves GA
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- Amsler C
- Anagnostou G
- Ananthan B
- Anastassov A
- Andelin D
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- Andreev V
- Andreev Y
- Anghel IM
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- Anh T. Vu
- Anisimov A
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- Yuste C
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- Zachariadou A
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- Zanetti M
- Zang SL
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- Zatzerklyany A
- Zeidler C
- Zeinali M
- Zeise M
- Zelepoukine S
- Zeuner WD
- Zeyrek M
- Zhang J
- Zhang L
- Zhang Y
- Zhang Z
- Zheng Y
- Zhiltsov V
- Zhokin A
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- Zhu K
- Zhu RY
- Zhukov V
- Zhukova V
- Ziebarth EB
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- 01/01/2009
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Alignment of the CMS muon system with cosmic-ray and beam-halo muons
- Author
- A. A. Gokce
- A. A. Ocampo Rios
- A. B. Meyer
- A. C. Benvenuti
- A. C. Garcia Bonilla
- A. C. Le Bihan
- A. D. Peris
- A. F. Garfinkel
- A. F. Osorio Oliveros
- A. G. Raboso
- A. H. Ball
- A. H. Heering
- A. K. Mohanty
- A. K. Sanchez
- A. K. Srivastava
- A. K. Topaksu
- A. L. Virto
- A. M. Brett
- A. M. Cordonnier
- A. M. Guler
- A. M. Magnan
- A. M. Pineda
- A. M. Rossi
- A. M. Sirunyan
- A. O. M. Iorio
- A. P. R. Gay
- A. R. Jimeno
- A. S. Ayan
- A. S. Hernandez
- A. S. Muhammad
- A. S. Von Dratzig
- A. S. Yoon
- A. T. Laasanen
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- A. Adiguzel
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- Y. Ma
- Y. Mao
- Y. Maravin
- Y. Mel'Nik
- Y. Musienko
- Y. Onel
- Y. Pakhotin
- Y. Patois
- Y. Roh
- Y. Shcheglov
- Y. Shinde
- Y. Sirois
- Y. Velikzhanin
- Y. Weng
- Y. Yang
- Y. Yilmaz
- Y. Zhang
- Y. Zheng
- Z. C. Yang
- Z. J. Guo
- Z. L. Trocsanyi
- Z. Antunovic
- Z. Chen
- Z. Gecse
- Z. Geese
- Z. Hu
- Z. Szabo
- Z. Szillasi
- Z. Toteva
- Z. Wan
- Z. Wang
- Z. Xie
- Z. Xue
- Z. Zhang
- Z. Zinonos
- Publication venue
- 'IOP Publishing'
- Publication date
- 01/01/2009
- Field of study
Get PDFThis is the Pre-print version of the Article. The official published version of the Paper can be accessed from the link below - Copyright @ 2010 IOPThe CMS muon system has been aligned using cosmic-ray muons collected in 2008 and beam-halo muons from the 2008 LHC circulating beam tests. After alignment, the resolution of the most sensitive coordinate is 80 microns for the relative positions of superlayers in the same barrel chamber and 270 microns for the relative positions of endcap chambers in the same ring structure. The resolution on the position of the central barrel chambers relative to the tracker is comprised between two extreme estimates, 200 and 700 microns, provided by two complementary studies. With minor modifications, the alignment procedures can be applied using muons from LHC collisions, leading to additional significant improvements.This work is supported by FMSR (Austria); FNRS and FWO (Belgium); CNPq, CAPES, FAPERJ,
and FAPESP (Brazil); MES (Bulgaria); CERN; CAS, MoST, and NSFC (China); COLCIENCIAS
(Colombia); MSES (Croatia); RPF (Cyprus); Academy of Sciences and NICPB (Estonia);
Academy of Finland, ME, and HIP (Finland); CEA and CNRS/IN2P3 (France); BMBF, DFG,
and HGF (Germany); GSRT (Greece); OTKA and NKTH (Hungary); DAE and DST (India); IPM (Iran); SFI (Ireland); INFN (Italy); NRF (Korea); LAS (Lithuania); CINVESTAV, CONACYT,
SEP, and UASLP-FAI (Mexico); PAEC (Pakistan); SCSR (Poland); FCT (Portugal); JINR(Armenia, Belarus, Georgia, Ukraine, Uzbekistan); MST and MAE (Russia); MSTDS (Serbia); MICINN and CPAN (Spain); Swiss Funding Agencies (Switzerland); NSC (Taipei); TUBITAK and TAEK (Turkey); STFC (United Kingdom); DOE and NSF (USA)
Commissioning of the CMS high-level trigger with cosmic rays
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- Publication venue
- 'IOP Publishing'
- Publication date
- 26/11/2009
- Field of study
Get PDFThis is the Pre-print version of the Article. The official published version of the paper can be accessed from the link below - Copyright @ 2010 IOPThe CMS High-Level Trigger (HLT) is responsible for ensuring that data samples with potentially interesting events are recorded with high efficiency and good quality. This paper gives an overview of the HLT and focuses on its commissioning using cosmic rays. The selection of triggers that were deployed is presented and the online grouping of triggered events into streams and primary datasets is discussed. Tools for online and offline data quality monitoring for the HLT are described, and the operational performance of the muon HLT algorithms is reviewed. The average time taken for the HLT selection and its dependence on detector and operating conditions are presented. The HLT performed reliably and helped provide a large dataset. This dataset has proven to be invaluable for understanding the performance of the trigger and the CMS experiment as a whole.This work is supported by FMSR (Austria); FNRS and FWO (Belgium); CNPq, CAPES, FAPERJ,
and FAPESP (Brazil); MES (Bulgaria); CERN; CAS, MoST, and NSFC (China); COLCIENCIAS
(Colombia); MSES (Croatia); RPF (Cyprus); Academy of Sciences and NICPB (Estonia);
Academy of Finland, ME, and HIP (Finland); CEA and CNRS/IN2P3 (France); BMBF, DFG, and HGF (Germany); GSRT (Greece); OTKA and NKTH (Hungary); DAE and DST (India); IPM (Iran); SFI (Ireland); INFN (Italy); NRF (Korea); LAS (Lithuania); CINVESTAV, CONACYT, SEP, and UASLP-FAI (Mexico); PAEC (Pakistan); SCSR (Poland); FCT (Portugal); JINR
(Armenia, Belarus, Georgia, Ukraine, Uzbekistan); MST and MAE (Russia); MSTDS (Serbia); MICINN and CPAN (Spain); Swiss Funding Agencies (Switzerland); NSC (Taipei); TUBITAK and TAEK (Turkey); STFC (United Kingdom); DOE and NSF (USA)
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