87 research outputs found
Effect of malaria infection on hematological profiles of people living with human immunodeficiency virus in Gambella, southwest Ethiopia
- Author
- A Berg
- AA Lamikanra
- AR Bharti
- D Kassa
- DN Tagoe
- DR Kuritzkes
- Ethiopian health and nutrition research institute (EHNRI)
- F Kirchhoff
- FE Mckenzie
- FO Akinbo
- GC Santis De
- GG Tchinda
- J Crawley
- JP Quintero
- K Grimwade
- NR Maina
- O Erhabor
- PE Etusim
- PS Sullivan
- PS Sullivan
- R Kyeyune
- S Hochman
- SS Parinitha
- TE Coyle
- W Iqbal
- World Health Organization (WHO)
- Y Wondimeneh
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- Field of study
Full text linkCarcinoma Matrix Controls Resistance to Cisplatin through Talin Regulation of NF-kB
- Author
- A Aleshin
- A Berrier
- A Schultze
- AC Bharti
- AL Berrier
- AL Berrier
- Allison L. Berrier
- C Egles
- C Van Waes
- CA Sherman-Baust
- CR Leemans
- Dong-Yan Jin
- DR Critchley
- E Cukierman
- E Peterson-Roth
- F Li
- G Benton
- HA Sansing
- HC Chen
- HE Kim
- Hope A. Sansing
- I Serebriiskii
- I Vlodavsky
- J Kruegel
- J Zhao
- JA Green
- JC Puigvert
- JH Wang
- JL Snider
- JM Lamar
- JT Parsons
- K Aoki
- Karen E. Eberle
- KR Levental
- M Benhar
- M Cardinali
- MA Chrenek
- MJ Paszek
- MT Lai
- N Masumoto
- N Tikhmyanova
- P Defilippi
- Peter Szaniszlo
- PJ Morin
- PM Specenier
- PS Hodkinson
- R Castello-Cros
- R Castello-Cros
- S Kook
- S Lee
- S Liu
- S Maubant
- S Sakamoto
- S Shamimi-Noori
- SD Funk
- SJ Franco
- T Petzold
- T Tamatani
- T Tamatani
- V Gabarra-Niecko
- Vicente A. Resto
- W Kim
- W Woessmann
- WM Abuzeid
- X Peng
- X Zhang
- Y Pengetnze
- Publication venue
- Public Library of Science
- Publication date
- 24/06/2011
- Field of study
Get PDFExtracellular matrix factors within the tumor microenvironment that control resistance to chemotherapeutics are poorly understood. This study focused on understanding matrix adhesion pathways that control the oral carcinoma response to cisplatin. Our studies revealed that adhesion of HN12 and JHU012 oral carcinomas to carcinoma matrix supported tumor cell proliferation in response to treatment with cisplatin. Proliferation in response to 30 µM cisplatin was not observed in HN12 cells adherent to other purified extracellular matrices such as Matrigel, collagen I, fibronectin or laminin I. Integrin β1 was important for adhesion to carcinoma matrix to trigger proliferation after treatment with cisplatin. Disruption of talin expression in HN12 cells adherent to carcinoma matrix increased cisplatin induced proliferation. Pharmacological inhibitors were used to determine signaling events required for talin deficiency to regulate cisplatin induced proliferation. Pharmacological inhibition of NF-kB reduced proliferation of talin-deficient HN12 cells treated with 30 µM cisplatin. Nuclear NF-kB activity was assayed in HN12 cells using a luciferase reporter of NF-kB transcriptional activity. Nuclear NF-kB activity was similar in HN12 cells adherent to carcinoma matrix and collagen I when treated with vehicle DMSO. Following treatment with 30 µM cisplatin, NF-kB activity is maintained in cells adherent to carcinoma matrix whereas NF-kB activity is reduced in collagen I adherent cells. Expression of talin was sufficient to trigger proliferation of HN12 cells adherent to collagen I following treatment with 1 and 30 µM cisplatin. Talin overexpression was sufficient to trigger NF-kB activity following treatment with cisplatin in carcinoma matrix adherent HN12 cells in a process disrupted by FAK siRNA. Thus, adhesions within the carcinoma matrix create a matrix environment in which exposure to cisplatin induces proliferation through the function of integrin β1, talin and FAK pathways that regulate NF-kB nuclear activity
EGCG Enhances the Therapeutic Potential of Gemcitabine and CP690550 by Inhibiting STAT3 Signaling Pathway in Human Pancreatic Cancer
- Author
- A Jemal
- A Tomillero
- AC Bharti
- AG Porter
- B-T Ji
- BB Aggarwal
- C Almoguera
- C Schindler
- DC Borie
- DE Levy
- DJ Dauer
- DN Syed
- E Devarajan
- E Kudlacz
- F Garcia Soriano
- F Konoeda
- G-p Yu
- GD Stoner
- H Akaishi
- H Burris
- H Fujiki
- H Kayed
- H Yu
- H-Y Ahn
- Hana Algül
- HB Park
- IE Dreosti
- J Abdulghani
- J Darnell
- J Kim
- J Rius
- JE Chrencik
- JE Cooper
- JE Darnell
- JE Darnell Jr
- JN Ihle
- Junsheng Fu
- K Nakachi
- K Takeda
- K West
- L Levy
- M Berishaj
- M Karin
- M Korc
- M Shimizu
- M Zapatka
- MB Sporn
- MD Siegelin
- MG Schlieman
- N Ahmad
- N Ahmad
- N Ahmad
- N Lee
- P Ghaneh
- PP Tak
- PS Changelian
- R Buettner
- Rakesh K. Srivastava
- RS Chapman
- S Balasubramanian
- S Gupta
- S Nam
- S Shankar
- S Shankar
- S Shankar
- S-S Liau
- Sharmila Shankar
- SI Grivennikov
- SJ Schreiner
- Su-Ni Tang
- T Welte
- VM Adhami
- WE Naugler
- Y Cao
- Y-C Liang
- Z Dong
- Z Ren
- Publication venue
- Public Library of Science
- Publication date
- 13/02/2012
- Field of study
Get PDFBackground: Signal Transducer and Activator of Transcription 3 (STAT3) is an oncogene, which promotes cell survival, proliferation, motility and progression in cancer cells. Targeting STAT3 signaling may lead to the development of novel therapeutic approaches for human cancers. Here, we examined the effects of epigallocathechin gallate (EGCG) on STAT3 signaling in pancreatic cancer cells, and assessed the therapeutic potential of EGCG with gemcitabine or JAK3 inhibitor CP690550 (Tasocitinib) for the treatment and/or prevention of pancreatic cancer. Methodology/Principal Findings: Cell viability and apoptosis were measured by XTT assay and TUNEL staining, respectively. Gene and protein expressions were measured by qRT-PCR and Western blot analysis, respectively. The results revealed that EGCG inhibited the expression of phospho and total JAK3 and STAT3, STAT3 transcription and activation, and the expression of STAT3-regulated genes, resulting in the inhibition of cell motility, migration and invasion, and the induction of caspase-3 and PARP cleavage. The inhibition of STAT3 enhanced the inhibitory effects of EGCG on cell motility and viability. Additionally, gemcitabine and CP690550 alone inhibited STAT3 target genes and synergized with EGCG to inhibit cell viability and induce apoptosis in pancreatic cancer cells. Conclusions/Significance: Overall, these results suggest that EGCG suppresses the growth, invasion and migration of pancreatic cancer cells, and induces apoptosis by interfering with the STAT3 signaling pathway. Moreover, EGCG furthe
Iron Behaving Badly: Inappropriate Iron Chelation as a Major Contributor to the Aetiology of Vascular and Other Progressive Inflammatory and Degenerative Diseases
- Author
- A Abbott
- A Abou-Raya
- A Aljandali
- A Ambesi-Impiombato
- A Aydin
- A Balcerczyk
- A Besarab
- A Brzezinski
- A Campbell
- A Carrillo-Vico
- A Cavalli
- A Chattopadhyay
- A Chattopadhyay
- A Cherubini
- A Dey
- A Doms
- A Donovan
- A Donovan
- A Dávalos
- A Gaeta
- A Garny
- A Gnjec
- A Gomes
- A Gopalakrishnan
- A Hald
- A Henney
- A Hirayama
- A Hoffmann
- A Huber
- A Hugman
- A Iannetti
- A Ide-Ektessabi
- A Jacobs
- A Jeyabalan
- A Kahvejian
- A Karrar
- A Kasztler
- A Kibel
- A Kocyigit
- A Kotha
- A Kumral
- A Lass
- A Lecube
- A Lewén
- A Lotery
- A Maggio
- A Malek
- A Malik
- A Mantovani
- A Matsuzawa
- A Mitra
- A Monge
- A Murakami
- A Murakami
- A Murakami
- A Murakami
- A Mutti
- A Nijnik
- A Nunomura
- A Nunomura
- A Patt
- A Persson
- A Pietrangelo
- A Piga
- A Pirat
- A Post
- A Pradhan
- A Protti
- A Rattner
- A Ravati
- A Rehman
- A Reynolds
- A Richmond
- A Roetto
- A Roetto
- A Rostom
- A Rumbold
- A Russo
- A Rötig
- A Saltelli
- A Saltelli
- A Sandek
- A Sassano
- A Scalbert
- A Scalbert
- A Scalbert
- A Sica
- A Smahi
- A Sola
- A Stintzi
- A Szewczyk
- A Taguchi
- A Tedgui
- A Terman
- A Terman
- A Terman
- A Undas
- A Virdis
- A Wagner
- A Wagner
- A Wagner
- A Wagner
- A Wojas-Pelc
- A Wong
- A Xu
- A Yoritaka
- A Yoshimura
- A-L Barabási
- AA Andreadis
- AA Borisy
- AA Farooqui
- AA Qutub
- AA Qutub
- AA Vlessis
- AB Nathens
- AB Parsons
- AB Parsons
- AB Thompson
- AB Thomson
- AC Bayne
- AC Bharti
- AC Cave
- AC Mello Filho
- AD d'Hardemare
- AD de Silva
- Ad hoc committee on systemic lupus erythematosus response criteria for fatigue
- ADL van der
- AE Aust
- AE Baue
- AE Finefrock
- AE Heazell
- AE Heazell
- AE Kartikasari
- AEC Ihekwaba
- AEC Ihekwaba
- AF Tramontano
- AH Berg
- AH Koeppen
- AH Koeppen
- AH Tong
- AI Bush
- AI Bush
- AI Bush
- AI Bush
- AI Faden
- AJ Ghio
- AJ Ghio
- AJ Ghio
- AJ Hulbert
- AJ Kowaltowski
- AJ Lusis
- AJ Matthews
- AJ Reyes
- AJ van Oostrom
- AJ Watson
- AJ White
- AJ Williams
- AK Junk
- AL Beal
- AL Hemdahl
- AL Hopkins
- AL Hopkins
- AL Lagan
- AL Mark
- AL Sirén
- AL Sirén
- AL Sirén
- AL Takeda
- AM Abeles
- AM Borzychowski
- AM Choi
- AM Dolga
- AM Elneihoum
- AM Elneihoum
- AM Feist
- AM Harvey
- AM Jenkinson
- AM Lin
- AM Samuni
- AM Snyder
- AN Crowson
- AN Tabah
- AP Bolger
- AP Breen
- AP Liappis
- AR Kallianpur
- AR Kallianpur
- AR Martin
- AR Ness
- AR Rechner
- AR Rumbold
- AS Baldwin Jr
- AS Binbrek
- AS Kaprelyants
- AS Wierzbicki
- AT McKie
- AV Lebedev
- AV Perkins
- AV Rao
- AW Maresso
- AY Andreyev
- AY Sun
- B Chakravarti
- B Chance
- B Cronin
- B de Valk
- B De Vries
- B Desoize
- B Drayer
- B Faller
- B Goodell
- B Halliwell
- B Halliwell
- B Halliwell
- B Halliwell
- B Halliwell
- B Halliwell
- B Halliwell
- B Halliwell
- B Huppertz
- B Jayawardhana
- B Kwak
- B Lachili
- B Lipinski
- B Mackenzie
- B Marshall
- B Mignotte
- B Oldenburg
- B Poeggeler
- B Pradines
- B Pradines
- B Regland
- B Russell
- B Schiessl
- B Shipley
- B Skibska
- B Sturm
- B Thorand
- B Wang
- B Wolff
- B Wolozin
- B Wolozin
- B Xu
- B Zhang
- B Zhou
- BA Maddux
- BA Molitoris
- BB Aggarwal
- BB Aggarwal
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- BB Aggarwal
- BB Sizoo
- BB Song
- BB Song
- BC Daniels
- BC Jones
- BD LaMarca
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- BP Leung
- BP Oberg
- BP Yu
- BR Kwak
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- BS Chen
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- BT Mossman
- BV Naidu
- BY Tung
- BØ Palsson
- C Arnaud
- C Beaumont
- C Behl
- C Biondi
- C Bolin
- C Bozzini
- C Breymann
- C Brooksbank
- C Bubici
- C Bubici
- C Burdon
- C Camaschella
- C Camaschella
- C Caris
- C Cavdar
- C Chen
- C Delaby
- C Demougeot
- C Finch
- C Fleury
- C García-Ruiz
- C Gasche
- C Gasche
- C Gerhäuser
- C Goble
- C Henry
- C Herce-Pagliai
- C Herder
- C Hershko
- C Hershko
- C Hershko
- C Hershko
- C Jacob
- C Kenyon
- C Knox
- C Kretz-Remy
- C Kunsch
- C Köhle
- C Leadbeater
- C Li
- C Lu
- C Manach
- C Manach
- C Manach
- C Mancuso
- C Moon
- C Moon
- C Mouralian
- C Muscoli
- C Peyssonnaux
- C Peyssonnaux
- C Peyssonnaux
- C Pigeon
- C Popa
- C Quintana
- C Ramassamy
- C Ramassamy
- C Ratledge
- C Rigamonti
- C Ritter
- C Ritter
- C Ritter
- C Savino
- C Savoia
- C Savoia
- C Schmeer
- C Shirky
- C Singh
- C Smith
- C Thrasivoulou
- C Trenkwalder
- C Troeger
- C Urbich
- C Vermylen
- C Vélez-Pardo
- C Vélez-Pardo
- C Wandersman
- C Xu
- CA Combs
- CA Dorrepaal
- CA Genco
- CA Hubel
- CA Hubel
- CA Hubel
- CA Hubel
- CA Lynch
- CA Papaharalambus
- CA Rice-Evans
- CA Rice-Evans
- CA Rice-Evans
- CA Rottkamp
- CC Chen
- CC Chiueh
- CC Hsieh
- CC Neto
- CC Neto
- CC Neto
- CC Winterbourn
- CD Davis
- CD Vulpe
- CE Beyer
- CE Finch
- CE Wrede
- CESDI
- CF Bolton
- CF Taylor
- CG Fraga
- CG Moles
- CG Pham
- CG Walker
- CH Wang
- CI Cook
- CJ Binder
- CJ Boos
- CJ Burrows
- CJ Chen
- CJ Hukshorn
- CJ Kaupke
- CJ Maynard
- CJ Needham
- CJ Parsa
- CJ Vaughan
- CJA Doelman
- CK Lee
- CK Roberts
- CK Roberts
- CK Sen
- CL Dent
- CM Anderson
- CM Craven
- CN Hales
- CN Lumeng
- CN Roy
- CP Doherty
- CP Martin
- CR Allerson
- CR Sunstein
- CS Shin
- CS Stevenson
- CS Yang
- CT Keith
- CT Murphy
- CT Noguchi
- CV Jongeneel
- CW Olanow
- CW Pugh
- CW Redman
- CW Redman
- CW Redman
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- CW Trenam
- CW Trenam
- CW Trenam
- CW Yang
- CWM Adams
- CY Wang
- CY Wu
- D Agnello
- D Barisani
- D Ben Shachar
- D Berg
- D Berg
- D Blum
- D Closa
- D De Roure
- D DeFaria Yeh
- D Fliser
- D Furlani
- D Galaris
- D Galter
- D Guagnozzi
- D HaMai
- D Hamerman
- D Harman
- D Howe
- D Hristovski
- D Hull
- D Hull
- D Imbert
- D Johnson
- D Kaur
- D Kaur
- D Lapenna
- D Law
- D Meyer
- D Mozaffarian
- D Noble
- D Noble
- D Ponraj
- D Prá
- D Rowley
- D Salvemini
- D Tapscott
- D Thorne
- D Trinder
- D Walz
- D Weininger
- D Yoon
- D Zozulinska
- DA Butterfield
- DA Butterfield
- DA Drechsel
- DA Fell
- DA Fell
- DA Rand
- DA Shoskes
- DA Weinstein
- DB Kell
- DB Kell
- DB Kell
- DB Kell
- DB Kell
- DB Kell
- DB Kell
- DB Kell
- DB Kell
- DB Kell
- DB Kell
- DB Kell
- DB Kell
- DB Kell
- DB Lovejoy
- DB Lovejoy
- DC Lau
- DC Souza-Costa
- DC Whitcomb
- DD Harrison-Findik
- DD Harrison-Findik
- DE Featherstone
- DE Ferrara
- DE Kelley
- DE Nelson
- DF Benyo
- DF Benyo
- DG Hackam
- DG Meyers
- DH Anderson
- DH Goetz
- DH Lee
- DH Lee
- DH Lee
- DH Lee
- DH Lee
- DH Walter
- DJ Fleming
- DJ Freeman
- DJ Grainger
- DJ Rader
- DJC Mackay
- DM Bailey
- DM Bailey
- DM Frazer
- DM Frazer
- DM Miller
- DM Niedowicz
- DM Paternoster
- DM Wojchowski
- DM Wrighting
- DN Granger
- DN Leung
- DN Seril
- DN Syed
- Douglas B Kell
- DP Bentley
- DR Bentley
- DR Flower
- DR Janero
- DR Petersen
- DR Richardson
- DR Richardson
- DR Richardson
- DR Richardson
- DR Richardson
- DR Richardson
- DR Rosen
- DR Swanson
- DR Swanson
- DR Zerbino
- DS Cassarino
- DS Grimes
- DS Kalinowski
- DS Kalinowski
- DS Kalinowski
- DS Kalinowski
- DS Warner
- DS Warner
- DS Wilson
- DT Dexter
- DW Kamp
- DW Kamp
- DW Killilea
- DW Lee
- DW Lee
- DW McCarey
- DW Reid
- DW Reif
- DW Swinkels
- DW Swinkels
- DX Bu
- E Aigner
- E Ates
- E Becker
- E Berenshtein
- E Berenshtein
- E Beutler
- E Bonilla
- E Bonilla
- E Butelli
- E Cadenas
- E Calabrese
- E Casanueva
- E Chwelatiuk
- E Corradini
- E Crimi
- E Crimi
- E Devrim
- E DiFederico
- E Donato
- E Floor
- E Gaggelli
- E Gao
- E Gazzano
- E Gitto
- E Guneli
- E Heiss
- E Kemna
- E Klipp
- E Lee
- E Lesnefsky
- E Mariani
- E Messaris
- E Middleton
- E Napoli
- E Nemeth
- E Nemeth
- E Nemeth
- E Nemeth
- E Nemeth
- E Nisbet-Brown
- E Pennisi
- E Sapey
- E Schleicher
- E Schwedhelm
- E Trushina
- EA Ostrakhovitch
- EA Platz
- EA Price
- EB Montgomery Jr
- EC Jury
- ED Rosen
- ED Weinberg
- ED Weinberg
- ED Weinberg
- ED Weinberg
- ED Weinberg
- ED Weinberg
- ED Weinberg
- ED Weinberg
- EDE Papathanassoglou
- EE Tuppo
- EE Voest
- EG McGeer
- EH Cao
- EH Kemna
- EH Sharman
- EJ Calabrese
- EJ Calabrese
- EJ Dombrecht
- EJ Dombrecht
- EJ Dombrecht
- EJ Jacobs
- EJ Kasarskis
- EJ Kunkel
- EJ Masoro
- EJ Neufeld
- EJ Sharples
- EL Que
- EM Balk
- EM Bulger
- EM Sikorski
- EM Tan
- EO Farombi
- ER Miller 3rd
- ER Norwitz
- ER Stadtman
- ER Taylor
- ES Fenjves
- ES Ford
- ES Hwang
- ES Lein
- EW Jacobsen
- EW Miller
- F Afaq
- F Aigner
- F Amersi
- F Aouad
- F Balkwill
- F Balkwill
- F Costello
- F Fiordaliso
- F Foury
- F Foury
- F Foury
- F Gao
- F Gueler
- F Gueler
- F Kim
- F L'Eplattenier
- F Lezoualc'h
- F Licastro
- F Longpré
- F Mateos
- F Molina-Holgado
- F Mulhaupt
- F Palau
- F Paul
- F Petrat
- F Sesti
- F Shahidi
- F Tiker
- F Watt
- FB Hu
- FB Johnson
- FC Lau
- FD Reynolds
- FE Parodi
- FJ Doyle 3rd
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- FK Lin
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- FW Booth
- G Barja
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- G Block
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- G Gloire
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- G Grass
- G Grasso
- G Grasso
- G Lefevre
- G Lenaz
- G Lenaz
- G Lenaz
- G Letechipia-Vallejo
- G Liu
- G Mello
- G Minotti
- G Minotti
- G Nicolas
- G Nicolas
- G Nicolas
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- G Papanikolaou
- G Pappa
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- G Ramakrishna
- G Reverter-Branchat
- G Semrin
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- G Shen
- G Sommer
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- G Weiss
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- G Weitz-Schmidt
- G Williamson
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- G Ye
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- GJ Kelloff
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- GM Rodriguez
- GN Gilbert
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- GS Hotamisligil
- GS Martin
- GS Omenn
- GV Paolini
- H Akiyama
- H Ashrafian
- H Boukhalfa
- H Chen
- H Drakesmith
- H Drechsel
- H Ehrenreich
- H Ehrenreich
- H Ehrenreich
- H El Hajji
- H Glickstein
- H Gunshin
- H Haas
- H Haas
- H Jick
- H Kacser
- H Kacser
- H Kaiserová
- H Kitano
- H Kitano
- H Kitano
- H Kolb
- H Kourlas
- H Koutnikova
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- H Kulaksiz
- H Kurata
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- H Ma
- H Ma
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- H Wang
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- H Yue
- H Zheng
- H Zheng
- H Zheng
- HA O'Neill
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- I Caniggia
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- The Long-Term Intervention with Pravastatin in Ischaemic Disease (LIPID) Study Group
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- Publication venue
- Publication date
- 09/08/2008
- Field of study
Get PDFThe production of peroxide and superoxide is an inevitable consequence of
aerobic metabolism, and while these particular "reactive oxygen species" (ROSs)
can exhibit a number of biological effects, they are not of themselves
excessively reactive and thus they are not especially damaging at physiological
concentrations. However, their reactions with poorly liganded iron species can
lead to the catalytic production of the very reactive and dangerous hydroxyl
radical, which is exceptionally damaging, and a major cause of chronic
inflammation. We review the considerable and wide-ranging evidence for the
involvement of this combination of (su)peroxide and poorly liganded iron in a
large number of physiological and indeed pathological processes and
inflammatory disorders, especially those involving the progressive degradation
of cellular and organismal performance. These diseases share a great many
similarities and thus might be considered to have a common cause (i.e.
iron-catalysed free radical and especially hydroxyl radical generation). The
studies reviewed include those focused on a series of cardiovascular, metabolic
and neurological diseases, where iron can be found at the sites of plaques and
lesions, as well as studies showing the significance of iron to aging and
longevity. The effective chelation of iron by natural or synthetic ligands is
thus of major physiological (and potentially therapeutic) importance. As
systems properties, we need to recognise that physiological observables have
multiple molecular causes, and studying them in isolation leads to inconsistent
patterns of apparent causality when it is the simultaneous combination of
multiple factors that is responsible. This explains, for instance, the
decidedly mixed effects of antioxidants that have been observed, etc...Comment: 159 pages, including 9 Figs and 2184 reference
Search for invisible decays of the Higgs boson produced via vector boson fusion in proton-proton collisions at root s=13 TeV
- Author
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Get PDFGingival fibromatosis: clinical, molecular and therapeutic issues
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Full text linkRecommended from our members
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- Álvarez Fernández A
- Özçelik Ö
- Publication venue
- Springer Nature on behalf of SISSA
- Publication date
- 01/08/2022
- Field of study
Get PDFA preprint version of the article is available at arXiv:2204.12945v2 [hep-ex], https://arxiv.org/abs/2204.12945v2 . Comments: Replaced with the published version. Added the journal reference and the DOI. All the figures and tables can be found at https://cms-results.web.cern.ch/cms-results/public-results/publications/HIG-19-014 (CMS Public Pages). Report number: CMS-HIG-19-014, CERN-EP-2022-019.Results are presented from a search for the Higgs boson decay H → Zγ, where Z → ℓ+ℓ− with ℓ = e or μ. The search is performed using a sample of proton-proton (pp) collision data at a center-of-mass energy of 13 TeV, recorded by the CMS experiment at the LHC, corresponding to an integrated luminosity of 138 fb^{−1}. Events are assigned to mutually exclusive categories, which exploit differences in both event topology and kinematics of distinct Higgs production mechanisms to enhance signal sensitivity. The signal strength μ, defined as the product of the cross section and the branching fraction [σ(pp → H)B(H → Zγ)] relative to the standard model prediction, is extracted from a simultaneous fit to the ℓ+ℓ−γ invariant mass distributions in all categories and is found to be μ = 2.4 ± 0.9 for a Higgs boson mass of 125.38 GeV. The statistical significance of the observed excess of events is 2.7 standard deviations. This measurement corresponds to σ(pp → H)B(H → Zγ) = 0.21 ± 0.08 pb. The observed (expected) upper limit at 95% confidence level on μ is 4.1 (1.8). The ratio of branching fractions B(H → Zγ)/B(H → γγ) is measured to be 1.5 +0.7−0.6, which agrees with the standard model prediction of 0.69 ± 0.04 at the 1.5 standard deviation level.SCOAP3
Observation of triple J/ψ meson production in proton-proton collisions
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- Özçelik Ö
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- 19/01/2023
- Field of study
Get PDFData availability:
Tabulated results are provided in the HEPData record for this analysis71. Release and preservation of data used by the CMS Collaboration as the basis for publications is guided by the CMS policy as stated in CMS data preservation, re-use and open access policy.Code availability:
The CMS core software is publically available at https://github.com/cms-sw/cmssw.Copyright . Protons consist of three valence quarks, two up-quarks and one down-quark, held together by gluons and a sea of quark-antiquark pairs. Collectively, quarks and gluons are referred to as partons. In a proton-proton collision, typically only one parton of each proton undergoes a hard scattering – referred to as single-parton scattering – leaving the remainder of each proton only slightly disturbed. Here, we report the study of double- and triple-parton scatterings through the simultaneous production of three J/ψ mesons, which consist of a charm quark-antiquark pair, in proton-proton collisions recorded with the CMS experiment at the Large Hadron Collider. We observed this process – reconstructed through the decays of J/ψ mesons into pairs of oppositely charged muons – with a statistical significance above five standard deviations. We measured the inclusive fiducial cross-section to be 272+141−104(stat)±17(syst)fb, and compared it to theoretical expectations for triple-J/ψ meson production in single-, double- and triple-parton scattering scenarios. Assuming factorization of multiple hard-scattering probabilities in terms of single-parton scattering cross-sections, double- and triple-parton scattering are the dominant contributions for the measured process.SCOAP3.Change history:
27 February 2023A Correction to this paper has been published: https://doi.org/10.1038/s41567-023-01992-
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- Yumiceva F
- Zabi A
- Zacharopoulou A
- Zaleski S
- Zalewski P
- Zanetti M
- Zarubin A
- Zarucki M
- Zecchinelli AG
- Zeinali M
- Zeuner WD
- Zghiche A
- Zhang F
- Zhang H
- Zhang J
- Zhang L
- Zhang W
- Zhang Y
- Zhang Y
- Zhang Y
- Zhang Z
- Zhao J
- Zhizhin I
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- Ziemons T
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- Zorbakir IS
- Zorbilmez C
- Zotto P
- Zotz A
- Zou D
- Zou R
- Zucchetta A
- Zumerle G
- Zuo X
- Zuolo D
- Zygala L
- Álvarez Fernández A
- Özçelik Ö
- Publication venue
- Elsevier
- Publication date
- 15/09/2022
- Field of study
Get PDFData availability:
Release and preservation of data used by the CMS Collaboration as the basis for publications is guided by the CMS policy as stated in “CMS data preservation, re-use and open access policy”.A preprint version of this article is archived at: arXiv:2205.09597v2 [hep-ex], https://arxiv.org/abs/2205.09597v2 . Comments: Replaced with the published version. Added the journal reference. All the figures and tables, including additional supplementary figures and tables, can be found at https://cms-results.web.cern.ch/cms-results/public-results/publications/SUS-21-002 (CMS Public Pages). Report number: CMS-SUS-21-002, CERN-EP-2022-031This Letter presents a search for direct production of charginos and neutralinos via electroweak interactions. The results are based on data from proton-proton collisions at a center-of-mass energy of 13 TeV collected with the CMS detector at the LHC, corresponding to an integrated luminosity of 137 fb^{-1}. The search considers final states with large missing transverse momentum and pairs of hadronically decaying bosons WW, WZ, and WH, where H is the Higgs boson. These bosons are identified using novel algorithms. No significant excess of events is observed relative to the expectations from the standard model. Limits at the 95% confidence level are placed on the cross section for production of mass-degenerate wino-like supersymmetric particles χ~±1 and χ~02, and mass-degenerate higgsino-like supersymmetric particles χ~±1, χ~02, and χ~03. In the limit of a nearly-massless lightest supersymmetric particle χ~01, wino-like particles with masses up to 870 and 960 GeV are excluded in the cases of χ~02 → Zχ~01 and χ~02 → Hχ~01, respectively, and higgsino-like particles are excluded between 300 and 650 GeV.SCOAP3
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Search for light Higgs bosons from supersymmetric cascade decays in pp collisions at √s=13TeV
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- Yumiceva F
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- Zacharopoulou A
- Zahid S
- Zaleski S
- Zalewski P
- Zanetti M
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- Zecchinelli AG
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- Zeuner WD
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- Zorbilmez C
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- Zygala L
- Álvarez CR
- Özçelik Ö
- Publication venue
- Springer Science and Business Media LLC
- Publication date
- 06/07/2023
- Field of study
Get PDFA search is reported for pairs of light Higgs
bosons (H1) produced in supersymmetric cascade decays in
f
inal states with small missing transverse momentum. A data
set of LHC pp collisions collected with the CMS detector
at √s = 13TeV and corresponding to an integrated lumi
nosity of 138fb−1 is used. The search targets events where
both H1 bosons decay into b¯b pairs that are reconstructed
as large-radius jets using substructure techniques. No evi
dence is found for an excess of events beyond the back
ground expectations of the standard model (SM). Results
from the search are interpreted in the next-to-minimal super
symmetric extension of the SM, where a “singlino” of small
mass leads to squark and gluino cascade decays that can pre
dominantly end in a highly Lorentz-boosted singlet-like H1
andasinglino-likeneutralinoofsmalltransversemomentum.
Upperlimitsaresetontheproductofthesquarkorgluinopair
production cross section and the square of the b¯b branching
fraction of the H1 in a benchmark model containing almost
mass-degenerategluinosandlight-flavoursquarks.Underthe
assumption of an SM-like H1 → b¯b branching fraction, H1
bosonswithmassesintherange40–120GeVarisingfromthe
decays of squarks or gluinos with a mass of 1200–2500GeV
are excluded at 95% confidence level.SCOA
- …
