280 research outputs found
The short-time structural plasticity of dendritic spines is altered in a model of Rett syndrome
- Author
- A Bird
- A Cruz-MartĂn
- A Holtmaat
- A Holtmaat
- A Pavlowsky
- A Yoshii
- AJ D'Ercole
- AL Carvalho
- AM Baker
- AM Wegner
- B Thongsong
- BE Pulford
- CA Chapleau
- CD Harvey
- CE Stewart
- D Tropea
- D Tropea
- DP Wolfer
- E Carro
- EM Boggio
- G Feng
- G Lonetti
- H Thoenen
- H Wang
- HY Zoghbi
- JI Arellano
- JL Marks
- JL Trejo
- JR O'Kusky
- K Takano
- LM GarcÄąa-Segura
- M Auletta
- M Chahrour
- M Itoh
- M Matsuzaki
- MC Marchetto
- MM Ramsey
- MP Nieto-Bona
- N Voituron
- NA Stearns
- P ThĂŠvenaz
- PV Belichenko
- PV Belichenko
- Q Chang
- R Riikonen
- R Riikonen
- R Riikonen
- RE Humbel
- RR Reinhardt
- RZ Chen
- S Landi
- S Ricciardi
- SM Woodall
- T Nishijima
- WM Pardridge
- Publication venue
- Nature Publishing Group
- Publication date
- Field of study
Get PDFThe maturation of excitatory transmission comes about through a developmental period in which dendritic spines are highly motile and their number, form and size are rapidly changing. Surprisingly, although these processes are crucial for the formation of cortical circuitry, little is known about possible alterations of these processes in brain disease. By means of acute in vivo 2-photon imaging we show that the dynamic properties of dendritic spines of layer V cortical neurons are deeply affected in a mouse model of Rett syndrome (RTT) at a time around P25 when the neuronal phenotype of the disease is still mild. Then, we show that 24h after a subcutaneous injection of IGF-1 spine dynamics is restored. Our study demonstrates that spine dynamics in RTT mice is severely impaired early during development and suggest that treatments for RTT should be started very early in order to reestablish a normal period of spine plasticity
Biogenic amines and their metabolites are differentially affected in the Mecp2-deficient mouse brain
- Author
- A Balkowiec
- AC Bonham
- Adeline Ghata
- AM Khan
- B Hagberg
- BH Guevara
- CL Laurvick
- CW Berridge
- D Tropea
- DM Katz
- DT Lioy
- G Calfa
- G Paxinos
- J Guy
- JC Roux
- JC Roux
- JC Viemari
- Jean-Christophe Roux
- JL Neul
- JP Tassin
- JT Erickson
- K Isoda
- Laurent Villard
- M Chahrour
- M Pratte
- M Rodriguez Fermepin
- M Santos
- MB Youdim
- MM Poo
- N Panayotis
- Nicolas Panayotis
- P Taneja
- Q Chang
- Q Gu
- RC Samaco
- RE Amir
- RZ Chen
- S Ide
- S Kutlu
- SJ Sara
- SL Fyffe
- TF Oo
- VK Yadav
- VS Dani
- Publication venue
- BioMed Central
- Publication date
- 01/01/2011
- Field of study
Get PDFInternational audienceBACKGROUND: Rett syndrome (RTT, MIM #312750) is a severe neurological disorder caused by mutations in the X-linked methyl-CpG binding protein 2 (MECP2) gene. Female patients are affected with an incidence of 1/15000 live births and develop normally from birth to 6-18 months of age before the onset of deficits in autonomic, cognitive, motor functions (stereotypic hand movements, impaired locomotion) and autistic features. Studies on Mecp2 mouse models, and specifically null mice, revealed morphological and functional alterations of neurons. Several functions that are regulated by bioaminergic nuclei or peripheral ganglia are impaired in the absence of Mecp2. RESULTS: Using high performance liquid chromatography, combined with electrochemical detection (HPLC/EC) we found that Mecp2(-/y) mice exhibit an alteration of DA metabolism in the ponto-bulbar region at 5 weeks followed by a more global alteration of monoamines when the disease progresses (8 weeks). Hypothalamic measurements suggest biphasic disturbances of norepinephrine and serotonin at pathology onset (5 weeks) that were found stabilized later on (8 weeks). Interestingly, the postnatal nigrostriatal dopaminergic deficit identified previously does not parallel the reduction of the other neurotransmitters investigated. Finally, dosage in cortical samples do not suggest modification in the monoaminergic content respectively at 5 and 8 weeks of age. CONCLUSIONS: We have identified that the level of catecholamines and serotonin is differentially affected in Mecp2(-/y) brain areas in a time-dependent fashion
X-ray emission from the Sombrero galaxy: discrete sources
- Author
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- Abbiendi G
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- Acosta D
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- Adiguzel A
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- Adzic P
- Agostino L
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- Aguilar-Benitez M
- Aguilo E
- Ahmad M
- Ahmad WH
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- Yilmaz Y
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- Zatserklyaniy A
- Zeinali M
- Zeise M
- Zeuner WD
- Zeyrek M
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- Zhukov V
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- Ziebarth EB
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- Zoeller MH
- Zorbilmez C
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- Zumerle G
- Zuranski A
- Publication venue
- 'IOP Publishing'
- Publication date
- 01/01/2010
- Field of study
Get PDFWe present a study of discrete X-ray sources in and around the
bulge-dominated, massive Sa galaxy, Sombrero (M104), based on new and archival
Chandra observations with a total exposure of ~200 ks. With a detection limit
of L_X = 1E37 erg/s and a field of view covering a galactocentric radius of ~30
kpc (11.5 arcminute), 383 sources are detected. Cross-correlation with Spitler
et al.'s catalogue of Sombrero globular clusters (GCs) identified from HST/ACS
observations reveals 41 X-rays sources in GCs, presumably low-mass X-ray
binaries (LMXBs). We quantify the differential luminosity functions (LFs) for
both the detected GC and field LMXBs, whose power-low indices (~1.1 for the
GC-LF and ~1.6 for field-LF) are consistent with previous studies for
elliptical galaxies. With precise sky positions of the GCs without a detected
X-ray source, we further quantify, through a fluctuation analysis, the GC LF at
fainter luminosities down to 1E35 erg/s. The derived index rules out a
faint-end slope flatter than 1.1 at a 2 sigma significance, contrary to recent
findings in several elliptical galaxies and the bulge of M31. On the other
hand, the 2-6 keV unresolved emission places a tight constraint on the field
LF, implying a flattened index of ~1.0 below 1E37 erg/s. We also detect 101
sources in the halo of Sombrero. The presence of these sources cannot be
interpreted as galactic LMXBs whose spatial distribution empirically follows
the starlight. Their number is also higher than the expected number of cosmic
AGNs (52+/-11 [1 sigma]) whose surface density is constrained by deep X-ray
surveys. We suggest that either the cosmic X-ray background is unusually high
in the direction of Sombrero, or a distinct population of X-ray sources is
present in the halo of Sombrero.Comment: 11 figures, 5 tables, ApJ in pres
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
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- Yi K
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- Zachariadou A
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- Zatzerklyany A
- Zeidler C
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- Zeise M
- Zelepoukine S
- Zeuner WD
- Zeyrek M
- Zhang J
- Zhang L
- Zhang Y
- Zhang Z
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- Zhokin A
- Zhu B
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- Zhukov V
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- Ziebarth EB
- Zielinski M
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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
Transcriptional Responses of Cultured Rat Sympathetic Neurons during BMP-7-Induced Dendritic Growth
- Author
- A Chiaramello
- A Harada
- AB Brann
- AL Prieto
- AM Craig
- AP DeBernardo
- BM Bolstad
- BS Shankaranarayana Rao
- C Aglah
- C Chang
- C Spilker
- CA Pardo
- Christina A. Harrington
- D Higgins
- D Higgins
- D Purves
- D Purves
- DA Bruckenstein
- DB Sparrow
- DE Read
- DG Flood
- DL Benson
- DL Smith
- DP Purpura
- DW Cleveland
- E Abe
- E Gazzerro
- E Gratacos
- E Hay
- E Sharma
- EA Sivertsen
- EK Scott
- EM Schuman
- EM Smith
- F Metzger
- FB Gao
- Ferdinando Di Cunto
- G Banisadr
- G Maussion
- GS Withers
- H Appaiah
- H Kimura
- H Sikder
- HG Bernstein
- HN Beck
- HY Zoghbi
- I Lopez-Coviella
- IC Scott
- J Berger-Sweeney
- J Opatz
- JC Hocking
- JH Kim
- JI Moon
- JJ Breunig
- JP de Ruiter
- JP Miller
- K Drahushuk
- K Ibata
- K Ibata
- K Jin
- K Miyazono
- K Ohno
- KA Pavelock
- KE Smith
- L Redmond
- L Van Aelst
- LC Yeh
- LC Yeh
- LM Bianchi
- M Hartmann
- M Knofler
- M Miyashita
- M Quartu
- M Tropea
- M Urbanska
- MA Thal
- ME Williams
- Michael M. Wang
- Michelle M. Garred
- MJ Lee
- MK Lakshmana
- MM Corty
- MR Schiller
- P Lein
- P Lein
- P Lonn
- P Salama-Cohen
- Pamela J. Lein
- PJ Lein
- Q Wei
- R Gisler
- R Knutsen
- R Seijffers
- RA Irizarry
- S Esquenazi
- S Gehler
- S Vyas
- SL Connors
- T Kameda
- T Licht
- T McAvoy
- T Svitkina
- T Yabe
- TA Deuel
- TF Dijkmans
- TJ Sejnowski
- V Jagadha
- WS Choi
- WY Kim
- X Guo
- X Guo
- X Wu
- Xin Guo
- Y Iwasaki
- Y Kang
- Y Levkovitz
- Y Ou
- Y Zheng
- YQ Wang
- ZJ Tan
- Publication venue
- Public Library of Science
- Publication date
- 01/01/2011
- Field of study
Get PDFDendrites are the primary site of synapse formation in the vertebrate nervous system; however, relatively little is known about the molecular mechanisms that regulate the initial formation of primary dendrites. Embryonic rat sympathetic neurons cultured under defined conditions extend a single functional axon, but fail to form dendrites. Addition of bone morphogenetic proteins (BMPs) triggers these neurons to extend multiple dendrites without altering axonal growth or cell survival. We used this culture system to examine differential gene expression patterns in naĂŻve vs. BMP-treated sympathetic neurons in order to identify candidate genes involved in regulation of primary dendritogenesis.To determine the critical transcriptional window during BMP-induced dendritic growth, morphometric analysis of microtubule-associated protein (MAP-2)-immunopositive processes was used to quantify dendritic growth in cultures exposed to the transcription inhibitor actinomycin-D added at varying times after addition of BMP-7. BMP-7-induced dendritic growth was blocked when transcription was inhibited within the first 24 hr after adding exogenous BMP-7. Thus, total RNA was isolated from sympathetic neurons exposed to three different experimental conditions: (1) no BMP-7 treatment; (2) treatment with BMP-7 for 6 hr; and (3) treatment with BMP-7 for 24 hr. Affymetrix oligonucleotide microarrays were used to identify differential gene expression under these three culture conditions. BMP-7 significantly regulated 56 unique genes at 6 hr and 185 unique genes at 24 hr. Bioinformatic analyses implicate both established and novel genes and signaling pathways in primary dendritogenesis.This study provides a unique dataset that will be useful in generating testable hypotheses regarding transcriptional control of the initial stages of dendritic growth. Since BMPs selectively promote dendritic growth in central neurons as well, these findings may be generally applicable to dendritic growth in other neuronal cell types
Modulation of dendritic spine development and plasticity by BDNF and vesicular trafficking: fundamental roles in neurodevelopmental disorders associated with mental retardation and autism
- Author
- A Balkowiec
- A Dittie
- A Dunaevsky
- A Gartner
- A Mizrahi
- A Peters
- AC Horton
- AC Horton
- AC Horton
- AJ Holtmaat
- AK Percy
- AL Collins
- AM Connolly
- Anne Theibert
- B Lu
- B Racz
- BB Zeev
- C Austin
- C Vicario-Abejon
- C-H Kwon
- CA Chapleau
- CA Chapleau
- CA Chapleau
- Christopher A. Chapleau
- CR Bramham
- D Armstrong
- D Ehninger
- D Tropea
- DB Campbell
- DD Armstrong
- DG Jugloff
- DP Purpura
- E Ballestar
- E Korkotian
- EA Nimchinsky
- ED Nelson
- G Aicardi
- G Lynch
- G Nagappan
- GR Lewin
- GW Knott
- H Wang
- HT Chao
- I Maezawa
- IB Black
- IJ Delgado
- IM Ethell
- J Bourne
- J Grutzendler
- J Guy
- J Guy
- J Nectoux
- J Noguchi
- J Roohi
- J Sebat
- J Tanaka
- J Yang
- JC Fiala
- JC Lauterborn
- Jennifer L. Larimore
- JL Larimore
- JS Bonifacino
- JT Trachtenberg
- K Hashimoto
- K Martinowich
- K Miyazaki
- KB Nelson
- L Abuhatzira
- L Meikle
- L Pozzo-Miller
- LF Reichardt
- Lucas Pozzo-Miller
- M Alonso
- M Barbacid
- M Chahrour
- M Chahrour
- M Fischer
- M Hartmann
- M Marin-Padilla
- M Marin-Padilla
- M Matsuzaki
- M Ogier
- M Park
- M Segal
- M Shahbazian
- M Zagrebelsky
- MD Amaral
- MD Amaral
- MD Amaral
- ME Klein
- MF Egan
- MG Murer
- ML Bauman
- ML Bauman
- MM Poo
- N Ballas
- N Kishi
- N Matsuo
- NC Schanen
- NE Ziv
- NP Belichenko
- P Moretti
- PL Jones
- PR Huttenlocher
- PR Huttenlocher
- PV Belichenko
- PV Belichenko
- Q Chang
- R Katoh-Semba
- R Katoh-Semba
- R Lappalainen
- R Riikonen
- R Riikonen
- R Vanhala
- R Yuste
- RA McKinney
- RA Segal
- RD Smrt
- RE Amir
- RG Parton
- RH Edwards
- RJ Klose
- RZ Chen
- S Naidu
- S Urbe
- SA Tooze
- SE Newey
- SM Cusack
- T Bienvenu
- T Brigadski
- T Fukuda
- T Matsumoto
- T Sadakata
- T Sadakata
- T Sadakata
- TH Wassink
- UA Nuber
- V Deng
- VS Dani
- W Stoorvogel
- W Tyler
- W Tyler
- WE Kaufmann
- WE Kaufmann
- WE Kaufmann
- WE Kaufmann
- WE Kaufmann
- WG Chen
- WJ Tyler
- WJ Tyler
- WJ Tyler
- X Nan
- X Nan
- X Tao
- Y Asaka
- Y Ji
- Z Parnass
- Z Zhou
- ZY Chen
- ZY Chen
- Publication venue
- Springer US
- Publication date
- 01/01/2009
- Field of study
Get PDFThe process of axonal and dendritic development establishes the synaptic circuitry of the central nervous system (CNS) and is the result of interactions between intrinsic molecular factors and the external environment. One growth factor that has a compelling function in neuronal development is the neurotrophin brain-derived neurotrophic factor (BDNF). BDNF participates in axonal and dendritic differentiation during embryonic stages of neuronal development, as well as in the formation and maturation of dendritic spines during postnatal development. Recent studies have also implicated vesicular trafficking of BDNF via secretory vesicles, and both secretory and endosomal trafficking of vesicles containing synaptic proteins, such as neurotransmitter and neurotrophin receptors, in the regulation of axonal and dendritic differentiation, and in dendritic spine morphogenesis. Several genes that are either mutated or deregulated in neurodevelopmental disorders associated with mental retardation have now been identified, and several mouse models of these disorders have been generated and characterized. Interestingly, abnormalities in dendritic and synaptic structure are consistently observed in human neurodevelopmental disorders associated with mental retardation, and in mouse models of these disorders as well. Abnormalities in dendritic and synaptic differentiation are thought to underlie altered synaptic function and network connectivity, thus contributing to the clinical outcome. Here, we review the roles of BDNF and vesicular trafficking in axonal and dendritic differentiation in the context of dendritic and axonal morphological impairments commonly observed in neurodevelopmental disorders associated with mental retardation
CMS Data Processing Workflows during an Extended Cosmic Ray Run
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- Abadjiev K
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- Abbiendi G
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- Abdullin S
- Abelev B
- Acosta D
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- 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
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- Albajar C
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- 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
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- Auffray E
- Aurisano A
- Autermann C
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- Barashko V
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- Bechtel F
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- Bejar JC
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- Cockerill DJA
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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
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Mesenchymal stem/stromal cells as a delivery platform in cell and gene therapies
- Author
- A Augello
- A Banas
- A Banas
- A Bartholomew
- A Dulamea
- A Glavaski-Joksimovic
- A Uccelli
- A Vercelli
- A Xagorari
- AF Steinert
- AI Caplan
- AJ Friedenstein
- AR Williams
- B Bi
- B Imberti
- B Li
- B Parekkadan
- B Yamout
- BR Sousa
- C Hopkins
- C Lee
- C Limbert
- C Moriscot
- C Westenfelder
- C-C Yang
- Carlotta Spano
- CB Ripoll
- CJ Burton
- CY Tan
- D Boison
- D Chen
- D Drago
- D Karussis
- D Marolt
- D Zhang
- E Favaro
- E Gerdoni
- E GĂłmez-Barrena
- E Manning
- EA Wang
- Edwin M. Horwitz
- EM Horwitz
- F Bianchi
- F Davatchi
- F Ezquer
- F Gao
- F Mao
- F TĂśgel
- F TĂśgel
- F Zhen-Qiang
- Fabio Catani
- Filippo Rossignoli
- G Constantin
- G Ren
- G Zhen
- GA Norambuena
- Giulia Golinelli
- Giulia Grisendi
- H Ishikawa
- H Kanazawa
- H Li
- H Madry
- H Peng
- H Wu
- I Boumaza
- J Chen
- J Liu
- J Rehman
- J Xu
- JM Wozney
- JS Lee
- K Cho
- K English
- K Kurozumi
- K Schenke-Layland
- K Wakabayashi
- KA Tropea
- KM Akram
- L Sun
- L Xing
- LA Ortiz
- LV Bonzo di
- M Dominici
- M Gnecchi
- M Gnecchi
- M Gnecchi
- M Hagiwara
- M Jurewicz
- M Liu
- M Mohamadnejad
- M Mohyeddin-Bonab
- M Morigi
- M OâReilly
- M Rojas
- M Suzuki
- M-C Kastrinaki
- MA Puglisi
- Massimo Dominici
- MB Herrera
- MB Murphy
- ME Reinders
- MF Pittenger
- MF Pittenger
- MK McCoy
- MM Bonab
- N Gupta
- N Ikeda
- N Lin
- N Nagaya
- Naomi Dâsouza
- ND Dey
- NE Davis
- NK Venkataramana
- NKF Chen
- O Candini
- O Honmou
- Olivia Candini
- OY Bang
- P Chhabra
- P Connick
- P Fiorina
- P Kharaziha
- P Prasajak
- P-C Tsai
- P-O Carlsson
- PA Lysy
- Paolo Paolucci
- Q Li
- R Higashiyama
- R Jethva
- R Madonna
- R Madonna
- R Pal
- R Uemura
- RH Lee
- RH Lee
- RPH Meier
- RR Sharma
- RT Franceschi
- S Bruno
- S Bruno
- S Chen
- S Gatti
- S Greish
- S Llufriu
- S Marconi
- S Otsuru
- S Sadat
- S Wakitani
- Satoru Osturu
- SHJ Mei
- SM Phadnis
- SW OâDriscoll
- T Deuse
- T Friis
- T Kucic
- T Li
- TC Moloney
- TJ Burdon
- V Mundra
- W Gu
- W Zhang
- X Bai
- X Bai
- X Gao
- X Liu
- Y Horita
- Y Miki
- Y Miyahara
- Y Moodley
- Y Qin
- Y Shi
- Y Si
- Y Xiao
- Y Yan
- Y Zhou
- Y Zhu
- Y-T Lin
- Z Du
- Z Jiang
- Z Kokaia
- Z Zhang
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- Field of study
Full text linkSearch for dijet resonances in 7 TeV pp collisions at CMS
- Author
- Abbaneo D
- Abbiendi G
- Abbrescia M
- Abdel-Basit A
- Abdullin S
- Acosta D
- Acosta JG
- Acosta MV
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- Zanetti M
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- Zoeller MH
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- Publication venue
- 'American Physical Society (APS)'
- Publication date
- 01/01/2010
- 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 APSA search for narrow resonances in the dijet mass spectrum is performed using data corresponding to an integrated luminosity of 2.9ââpb-1 collected by the CMS experiment at the Large Hadron Collider. Upper limits at the 95% confidence level are presented on the product of the resonance cross section, branching fraction into dijets, and acceptance, separately for decays into quark-quark, quark-gluon, or gluon-gluon pairs. The data exclude new particles predicted in the following models at the 95% confidence level: string resonances, with mass less than 2.50 TeV, excited quarks, with mass less than 1.58 TeV, and axigluons, colorons, and E6 diquarks, in specific mass intervals. This extends previously published limits on these models.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 and WCU (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); MSTD (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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