413 research outputs found
Increased variability in ApcMin/+ intestinal tissue can be measured with microultrasound
- Author
- AA Gibson
- AF van der Steen
- AH Reitmair
- AR Moser
- AR Moser
- AS Tunis
- AT Yeung
- BM Boman
- BM McCartney
- C Luongo
- C Niehrs
- CM Moran
- CS Potten
- D Trani
- D Wang
- EE Deschner
- FS Foster
- FT D’Astous
- G Aust
- G Lanza
- GD Ludwig
- HS Wasan
- JC Bamber
- JE Paulsen
- JH Song
- JI Daksis
- KA Wear
- KK Lee
- LK Su
- M Bjerknes
- M Lipkin
- M Plodinec
- M van de Wetering
- MC Kolios
- MD Sherar
- MM Ivancic
- NN Mahmoud
- O Tetsu
- PA Janmey
- PL Appleton
- RF Jacoby
- RK Saha
- RM Vlad
- S Chaffai
- S You
- SA Nelson
- TC He
- TP Pretlow
- X Chen
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- 01/01/2016
- Field of study
Get PDFAltered tissue structure is a feature of many disease states and is usually measured by microscopic methods, limiting analysis to small areas. Means to rapidly and quantitatively measure the structure and organisation of large tissue areas would represent a major advance not just for research but also in the clinic. Here, changes in tissue organisation that result from heterozygosity in Apc, a precancerous situation, are comprehensively measured using microultrasound and three-dimensional high-resolution microscopy. Despite its normal appearance in conventionally examined cross-sections, both approaches revealed a significant increase in the variability of tissue organisation in Apc heterozygous tissue. These changes preceded the formation of aberrant crypt foci or adenoma. Measuring these premalignant changes using microultrasound provides a potential means to detect microscopically abnormal regions in large tissue samples, independent of visual examination or biopsies. Not only does this provide a powerful tool for studying tissue structure in experimental settings, the ability to detect and monitor tissue changes by microultrasound could be developed into a powerful adjunct to screening endoscopy in the clinic
Aberrant epithelial GREM1 expression initiates colonic tumorigenesis from cells outside the stem cell niche
- Author
- A Brech
- A Lewis
- A Merlos-Suárez
- A Subramanian
- Andrew Silver
- Annabelle Lewis
- AP Feinberg
- AP Haramis
- AR Moser
- C Luongo
- CB Westphalen
- Chiara Bardella
- DH Scoville
- DJ Weisenberger
- E De Sousa
- E Gazzerro
- E Jaeger
- E Jaeger
- EE Torlakovic
- Emma Jaeger
- ER Fearon
- Florian R Greten
- Francesc C Giner
- GR Dhamdhere
- GR van den Brink
- Hannah Rafferty
- Hayley Davis
- Huw Thomas
- I Tomlinson
- Ian Tomlinson
- IM Shih
- J Muñoz
- James E East
- JB Sneddon
- JC Hardwick
- JC Hardwick
- KT Bieging
- Lai Mun Wang
- LE Batts
- Luke Freeman-Mills
- Manuel Rodriguez-Justo
- Marco Novelli
- Mukesh Bansal
- N Barker
- N Barker
- Owen J Sansom
- Pedro Rodenas-Cuadrado
- R Rudling
- Richard Poulsom
- Rosemary Jeffery
- Runjan Chetty
- S Hayashi
- S Schwitalla
- S Segditsas
- SC Whitelaw
- Shazia Irshad
- Simon J Leedham
- SL Preston
- Sreelakshmi Mallappa
- Susan Clark
- T Sato
- T Sato
- TA Potti
- Tatjana Boitsova
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- 17/10/2014
- Field of study
Get PDFHereditary mixed polyposis syndrome (HMPS) is characterized by the development of mixed-morphology colorectal tumors and is caused by a 40-kb genetic duplication that results in aberrant epithelial expression of the gene encoding mesenchymal bone morphogenetic protein antagonist, GREM1. Here we use HMPS tissue and a mouse model of the disease to show that epithelial GREM1 disrupts homeostatic intestinal morphogen gradients, altering cell fate that is normally determined by position along the vertical epithelial axis. This promotes the persistence and/or reacquisition of stem cell properties in Lgr5-negative progenitor cells that have exited the stem cell niche. These cells form ectopic crypts, proliferate, accumulate somatic mutations and can initiate intestinal neoplasia, indicating that the crypt base stem cell is not the sole cell of origin of colorectal cancer. Furthermore, we show that epithelial expression of GREM1 also occurs in traditional serrated adenomas, sporadic premalignant lesions with a hitherto unknown pathogenesis, and these lesions can be considered the sporadic equivalents of HMPS polyps
Impaired mitochondrial calcium efflux contributes to disease progression in models of Alzheimer’s disease
- Author
- A Nunomura
- A Raffaello
- AC Paula-Lima
- AF Macaskill
- BC Tong
- C Cardenas
- CV Logan
- D Del Prete
- D Gabuzda
- D Kapogiannis
- D Pratico
- D Sepulveda-Falla
- E Alberdi
- E Area-Gomez
- E Area-Gomez
- E Tamagno
- ED Roberson
- EH Chang
- F Gillardon
- G Csordas
- G Kroemer
- G Szalai
- G Thinakaran
- H Du
- H Du
- H Du
- H Tuokko
- IL Ferreira
- J Chu
- J Cummings
- J Cummings
- J Yao
- JC Liu
- JG Begley
- JZ Tsien
- K Mallilankaraman
- KS Lee
- LM Billings
- M Calvo-Rodriguez
- M Citron
- M Kostic
- M Mayford
- M Patron
- M Verma
- ME Evangelopoulos
- MP Mattson
- MP Mattson
- MP Mattson
- MV Ivannikov
- PF Giannopoulos
- PF Giannopoulos
- R Kandimalla
- R Li
- R Palty
- R Vassar
- R Yan
- R Yan
- S Oddo
- T Nakagawa
- TS Luongo
- TS Luongo
- U Dreses-Werringloer
- V Rhein
- WC Skarnes
- Y Hirabayashi
- Y Tong
- Y Xie
- Z Dong
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- Field of study
Get PDFImpairments in neuronal intracellular calcium (iCa2+) handling may contribute to Alzheimer’s disease (AD) development. Metabolic dysfunction and progressive neuronal loss are associated with AD progression, and mitochondrial calcium (mCa2+) signaling is a key regulator of both of these processes. Here, we report remodeling of the mCa2+ exchange machinery in the prefrontal cortex of individuals with AD. In the 3xTg-AD mouse model impaired mCa2+ efflux capacity precedes neuropathology. Neuronal deletion of the mitochondrial Na+/Ca2+ exchanger (NCLX, Slc8b1 gene) accelerated memory decline and increased amyloidosis and tau pathology. Further, genetic rescue of neuronal NCLX in 3xTg-AD mice is sufficient to impede AD-associated pathology and memory loss. We show that mCa2+ overload contributes to AD progression by promoting superoxide generation, metabolic dysfunction and neuronal cell death. These results provide a link between the calcium dysregulation and metabolic dysfunction hypotheses of AD and suggest mCa2+ exchange as potential therapeutic target in AD
Profiling Critical Cancer Gene Mutations in Clinical Tumor Samples
- Author
- A Lievre
- A Velasco
- Adam J. Bass
- AJ Sievert
- Alissa C. Baker
- Caroline M. Emery
- Catarina D. Campbell
- CH Yeang
- Chandrani Mondal
- Charles D. Stiles
- Charles Hatton
- Chris Jones
- CS Karapetis
- DA Eberhard
- Deborah J. Goff
- DR Bentley
- E Van Cutsem
- F Loupakis
- Franco Roviello
- GD Demetri
- Gianni Corso
- GM Brodeur
- H Prenen
- JC Venter
- JD Carpten
- Jennifer Chan
- JG Paez
- Jonathan A. Fletcher
- Juliet Philips
- K Flaherty
- Keith L. Ligon
- Keluo Yao
- Kornelia Polyak
- Laura E. MacConaill
- Lauren Luongo
- Levi A. Garraway
- Lili Niu
- M Pearce
- M Schwab
- Mark A. Rubin
- Mark W. Kieran
- Matt Davis
- Matthew L. Meyerson
- Megan Hanna
- Michelangelo Fiorentino
- Ramesh Shivdasani
- RK Thomas
- S Khambata-Ford
- S Ogino
- S Pfister
- Sandro Santagata
- Sarah M. Kehoe
- T Forshew
- TJ Lynch
- W Pao
- William C. Hahn
- Y Cheng
- Yuexiang Wang
- Publication venue
- Public Library of Science
- Publication date
- 01/01/2009
- Field of study
Get PDFBACKGROUND:
Detection of critical cancer gene mutations in clinical tumor specimens may predict patient outcomes and inform treatment options; however, high-throughput mutation profiling remains underdeveloped as a diagnostic approach. We report the implementation of a genotyping and validation algorithm that enables robust tumor mutation profiling in the clinical setting.
METHODOLOGY:
We developed and implemented an optimized mutation profiling platform ("OncoMap") to interrogate approximately 400 mutations in 33 known oncogenes and tumor suppressors, many of which are known to predict response or resistance to targeted therapies. The performance of OncoMap was analyzed using DNA derived from both frozen and FFPE clinical material in a diverse set of cancer types. A subsequent in-depth analysis was conducted on histologically and clinically annotated pediatric gliomas. The sensitivity and specificity of OncoMap were 93.8% and 100% in fresh frozen tissue; and 89.3% and 99.4% in FFPE-derived DNA. We detected known mutations at the expected frequencies in common cancers, as well as novel mutations in adult and pediatric cancers that are likely to predict heightened response or resistance to existing or developmental cancer therapies. OncoMap profiles also support a new molecular stratification of pediatric low-grade gliomas based on BRAF mutations that may have immediate clinical impact.
CONCLUSIONS:
Our results demonstrate the clinical feasibility of high-throughput mutation profiling to query a large panel of "actionable" cancer gene mutations. In the future, this type of approach may be incorporated into both cancer epidemiologic studies and clinical decision making to specify the use of many targeted anticancer agents
Molecular mechanisms of cell death: recommendations of the Nomenclature Committee on Cell Death 2018.
- Author
- A Aouacheria
- A Aouacheria
- A Aranovich
- A Ashkenazi
- A Ashkenazi
- A Ashkenazi
- A Bernet
- A Buque
- A Chiche
- A Conte
- A Costanzo
- A Crockford
- A Degterev
- A Degterev
- A Dey
- A Gast
- A Gross
- A Hakkim
- A Hamacher-Brady
- A Hunger
- A Kaczmarek
- A Kamb
- A Koenig
- A Kotschy
- A Letai
- A Linkermann
- A Linkermann
- A Linkermann
- A Linkermann
- A Mousa
- A Muir
- A Mukherjee
- A Nilsson
- A Oberst
- A Oberst
- A Pagotto
- A Pyakurel
- A Rongvaux
- A Rubartelli
- A Sahaboglu
- A Seiler
- A Serrano-Puebla
- A Shamas-Din
- A Sistigu
- A Strasser
- A Strasser
- A Strasser
- A Strasser
- A Strasser
- A Strasser
- A Sumoza-Toledo
- A Sundararaman
- A Tittarelli
- A Trautmann
- A Villunger
- A Witt
- A Zychlinsky
- AA Fatokun
- AA Mailleux
- Aaron Ciechanover
- AB Pardee
- Abhishek D. Garg
- AC Bellail
- AC Schinzel
- AD Garg
- AD Garg
- AD Garg
- AD Garg
- AD Garg
- AD Garg
- AD Garg
- Adi Kimchi
- AE Alsop
- AE Feldstein
- AJ Schile
- AL Anding
- AL Genevois
- Alexey V. Antonov
- AM Chinnaiyan
- AM Distefano
- AM Dudek
- AM Verhagen
- AN Antony
- AN Barclay
- Ana J. García-Sáez
- Andreas Linkermann
- Andreas Strasser
- Andreas Villunger
- Andrew Oberst
- Andrew Thorburn
- Antonella Sistigu
- AP West
- AR Delbridge
- AT Schneider
- AT Ting
- AT Ting
- Atan Gross
- AV Follis
- AV Jacobsen
- AV Vaseva
- AV Vaseva
- AW Roberts
- B Antonsson
- B Aslan
- B Conradt
- B Fadeel
- B Gerlach
- B Gibert
- B Gooptu
- B McDonald
- B Schellenberg
- B Van Do
- B Xia
- BA Carlson
- BA Hilton
- BA Napier
- BB Aggarwal
- BC Barnhart
- Bertrand Joseph
- Beth Levine
- BG Childs
- BG Childs
- BG Childs
- BG Lambrus
- BG Yipp
- Boris Turk
- Boris Zhivotovsky
- BP Eckelman
- BP Eckelman
- BR Stockwell
- Brent R. Stockwell
- Brian D. Dynlacht
- BT Cookson
- C Bergmann
- C Dominguez-Brauer
- C Du
- C Frezza
- C Gerle
- C Guenebeaud
- C Gunther
- C Gunther
- C Helmke
- C Hernandez
- C Hockings
- C Lood
- C Lopez-Garcia
- C Lopez-Otin
- C Lopez-Otin
- C Louandre
- C Louandre
- C Nelson
- C Oberle
- C Piot
- C Rogers
- C Scaffidi
- C Vanpouille-Box
- C White
- C Xie
- Carlos López-Otín
- Carmen Garrido
- Catherine Brenner
- CC Wu
- CD Simpson
- CD Wiley
- Cecilia M.P. Rodrigues
- CF Wenceslau
- Christoph Borner
- CJ Kearney
- CK Ea
- CK Lam
- CK McPhee
- CL Buchheit
- CL Buchheit
- CL Buchheit
- CL Case
- Claudio Hetz
- CM Henry
- CN Casson
- Colin S. Duckett
- CP Baines
- CP Baines
- CP Dillon
- CP Dillon
- CP Dillon
- Cristina Muñoz-Pinedo
- CT Tan
- D Brenner
- D Brough
- D Chen
- D Crighton
- D Denton
- D Denton
- D Denton
- D Denton
- D Denton
- D Denton
- D Gatica
- D Goldschneider
- D Kranz
- D Li
- D Malin
- D Martin-Sanchez
- D Merino
- D Munoz-Espin
- D Piani
- D Ren
- D Stojkov
- D Tang
- D Tang
- D Vercammen
- D Vercammen
- D Wallach
- D Weaver
- D Yang
- DA Flusberg
- DA Rodriguez
- Daniel J. Klionsky
- Daolin Tang
- David C. Rubinsztein
- David M. Pereira
- David W. Andrews
- David Wallach
- DC Gray
- DH Cho
- Didac Carmona-Gutierrez
- Dieter Adam
- DJ Baker
- DJ Baker
- DJ Klionsky
- DJ McIlroy
- DL Berry
- DL Vaux
- DM Moquin
- DM Moujalled
- DM Pilla
- DM Rothwarf
- Domagoj Vucic
- Douglas R. Green
- DR Green
- DR Green
- DR Green
- DR Green
- DR Green
- DR Green
- DR Green
- DS Kempe
- DV Krysko
- E Arama
- E Basso
- E Buytaert
- E Candi
- E Fouquerel
- E Gavathiotis
- E Gavathiotis
- E Giampazolias
- E Kip
- E Lachaier
- E Lafont
- E Meunier
- E Perez
- E Vacchelli
- E Varfolomeev
- E Venereau
- E Zandi
- E Zandi
- EA Miao
- Edward A. Miao
- EF Lee
- EH Cheng
- EH Cheng
- EH Hinchcliffe
- EJ Park
- Eleonora Candi
- Eli Arama
- Emad S. Alnemri
- Emily H. Cheng
- Emre Sayan
- Enrico Lugli
- Eric H. Baehrecke
- Erwin F. Wagner
- Evripidis Gavathiotis
- EY Bassoy
- Eyal Gottlieb
- F Basit
- F Chalmin
- F Chen
- F Edlich
- F Ghiringhelli
- F Ke
- F Ke
- F Ke
- F Llambi
- F Llambi
- F Llambi
- F Loison
- F Madeo
- F Martin-Sanchez
- F McNab
- F Meitinger
- F Mille
- F Pietrocola
- F Todt
- F Wartha
- FB Chekeni
- FC Kischkel
- Feng Shao
- FK Chan
- FK Chan
- FL Scott
- FM Menzies
- FM Menzies
- FR Greten
- Francesca Bernassola
- Francesco Cecconi
- Francesco Di Virgilio
- Francis K.-M. Chan
- Frank Madeo
- G Brumatti
- G Casinelli
- G Denecker
- G Dewson
- G Droga-Mazovec
- G Ichim
- G Ichim
- G Kroemer
- G Kroemer
- G Kroemer
- G Monaco
- G Nunez
- G Quarato
- G Sun
- Gabriel A. Rabinovich
- Gabriel Nuñez
- Gerald M. Cohen
- Gerry Melino
- Gian Maria Fimia
- GO Latunde-Dada
- GP Sims
- GS Salvesen
- Guido Kroemer
- GW Dorn 2nd
- Gwenola Manic
- Gyorgy Hajnoczky
- Gyorgy Szabadkai
- H Appelqvist
- H Dai
- H Dai
- H Du
- H Hsu
- H Imai
- H Inoue
- H Inuzuka
- H Kazama
- H Kim
- H Kim
- H Li
- H Li
- H Otera
- H Parker
- H Puthalakath
- H Puthalakath
- H Sakahira
- H Wajant
- H Wang
- H Wang
- H Wang
- H Wang
- H Wang
- H Wang
- H Yang
- H Yang
- H Yuan
- H Yuan
- H Yuan
- H Zhang
- H Zhang
- HA Park
- Hamsa Puthalakath
- Hans-Uwe Simon
- HC Chen
- HE Kamber Kaya
- Henning Walczak
- Herbert W. Virgin
- Hidenori Ichijo
- Hinrich Gronemeyer
- HL Tang
- I Adkins
- I Amelio
- I Jaco
- I Jorgensen
- I Jorgensen
- I Jorgensen
- I Maejima
- I Martins
- I Marzo
- I Poursaitidis
- I Sturmlechner
- I Vitale
- I Vitale
- I Vitale
- I Vitale
- I Vitale
- I Vitale
- I Zanoni
- IC Low
- IE Dumitriu
- IE Gentle
- IE Wertz
- Ilio Vitale
- IP Nezis
- IP Nezis
- IR Powley
- Isaac S. Harris
- Ivano Amelio
- J Alanko
- J Bove
- J Brojatsch
- J Campisi
- J Cedervall
- J Chai
- J Chai
- J Chang
- J Desai
- J Desai
- J Ding
- J Ding
- J Fitamant
- J Fombonne
- J Fucikova
- J Fullgrabe
- J Fullgrabe
- J Geng
- J Gilloteaux
- J He
- J He
- J Hitomi
- J Huai
- J Huun
- J Karch
- J Kaur
- J Kers
- J Kim
- J Li
- J Lin
- J Liu
- J Maelfait
- J Majkut
- J Michels
- J Nunnari
- J Nylandsted
- J Parrish
- J Pecot
- J Puccini
- J Seo
- J Shi
- J Shi
- J Shi
- J Silke
- J Sosna
- J Suzuki
- J Suzuki
- J Suzuki
- J Warne
- J Wu
- J Xu
- J Yang
- J Yu
- J Zhang
- J Zhao
- J Zou
- J. Marie Hardwick
- JA DiDonato
- JA Ewald
- JA Hagar
- JA Mason
- JA Rickard
- James A. Wells
- Jan Paul Medema
- JC Acosta
- JC Hamann
- JD Bernet
- JE Chipuk
- JE Chipuk
- JE Kokoszka
- JE Vince
- JE Vince
- Jean-Christophe Marine
- Jean-Claude Martinou
- Jeffery D. Molkentin
- Jerry E. Chipuk
- JH Woo
- JI Jun
- JJ Guan
- JJ Schulman
- JL Lin
- JM Bravo-San Pedro
- JM Brouwer
- JM Deursen van
- JM Gump
- JM Hildebrand
- JM Jamison
- JM Mulcahy Levy
- JM Murphy
- JMM Levy
- Jochen H.M. Prehn
- John A. Cidlowski
- John J. Lemasters
- John M. Abrams
- John Silke
- John W. Elrod
- Josef M. Penninger
- JP Coppe
- JP Friedmann Angeli
- JPF Angeli
- JQ Kwong
- JQ Kwong
- JT Sockolosky
- JU Schweichel
- Juan R. Cubillos-Ruiz
- Junying Yuan
- JV Brower
- JV Lu
- JW Harper
- JW Upton
- JW Upton
- K Csomos
- K Eichholz
- K Huang
- K Kawane
- K Li
- K Martinod
- K Mills
- K Moriwaki
- K Moriwaki
- K Newton
- K Newton
- K Newton
- K Ruckdeschel
- K Schleich
- K Schleich
- K Segawa
- K Segawa
- K Sharma
- K Shimada
- K Tada
- K Tracy
- K Vlantis
- K Wang
- K Yacobi-Sharon
- K Zhang
- Karen H. Vousden
- Katiuscia Bianchi
- KD Metzler
- KD Metzler
- KE Gascoigne
- KE Lawlor
- Kevin M. Ryan
- KF Hsu
- KG Fleten
- KH Jang
- KH Szymczyk
- KJ Mackenzie
- KJ Neelsen
- KJ Oh
- KJ Weigel
- KK David
- KK David
- KL Lu
- KL O’Neill
- Klas Blomgren
- Klaus-Michael Debatin
- KM Backus
- KN Alavian
- KN Alavian
- KS Lang
- L Antonioli
- L Apetoh
- L Aram
- L Bezu
- L Broutier
- L Burri
- L Chen
- L Chen
- L Corrales
- L Dara
- L Deng
- L Dorstyn
- L Duprez
- L Fazal
- L Franchi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Galluzzi
- L Garcia-Prat
- L Grosse
- L Groth-Pedersen
- L Jiang
- L Jiang
- L Kaestner
- L Lin
- L Luo
- L Mosteiro
- L Sborgi
- L Scorrano
- L Scorrano
- L Sun
- L Tortola
- L Virag
- L Zitvogel
- L Zitvogel
- LA Barclay
- LA Gillies
- LA O’ Reilly
- LA Timmerman
- Laurence Zitvogel
- LG Yu
- LH Ho
- LJ Siskind
- LJ Yant
- LL Fava
- Lloyd A. Greene
- LM Kutscher
- Lorenzo Galluzzi
- LS Dickens
- LS Dickens
- LS Hinojosa
- Luca Scorrano
- Lucia Altucci
- LY Li
- M Aziz
- M Bonora
- M Bonora
- M Bonora
- M Castedo
- M Castedo
- M Castedo
- M Castedo
- M Castets
- M Colombini
- M Conrad
- M Dannappel
- M Demaria
- M Demaria
- M Demers
- M Ditzel
- M Enari
- M Fricker
- M Gao
- M Gao
- M Grandin
- M Grandin
- M Gyrd-Hansen
- M Haemmerle
- M Hayano
- M Hoare
- M Jamal-Hanjani
- M Jennis
- M Krajcovic
- M Krajcovic
- M Krajcovic
- M Laforge
- M Lazarou
- M Li
- M Lork
- M Mashimo
- M Matsushita
- M Michaud
- M Mihara
- M Morshed
- M Moulin
- M Muzio
- M Naito
- M Nguyen-Chi
- M Obeid
- M Onizawa
- M Overholtzer
- M Pasparakis
- M Sebbagh
- M Serrano
- M Storer
- M Taniguchi
- M Vivo
- M Wang
- M Yabal
- M Yabas
- M Zhou
- MA Carpio
- MA Hughes
- MA Kelliher
- MA Mellen
- MA O’Donnell
- MA O’Donnell
- MA Sanjuan
- MA Toscano
- Manolis Pasparakis
- Marcus Conrad
- Marcus E. Peter
- Margherita Annicchiarico-Petruzzelli
- Marion MacFarlane
- Marja Jäättelä
- Markus Rehm
- Mathieu J. M. Bertrand
- Matthew G. Vander Heiden
- Mauro Piacentini
- MB Fuertes
- MC Bonnet
- MC Tanzer
- MC Wei
- MF Luciani
- MG Heiden Vander
- MG Heiden Vander
- Michael Karin
- Michael O. Hengartner
- Michael Overholtzer
- Michal Malewicz
- Michelangelo Campanella
- Michele Pagano
- Mikhail V. Blagosklonny
- MJ Barsoum
- MJ Bertrand
- MJ Eliasson
- MJ Phillips
- MJ White
- MK Ruhland
- ML Coleman
- ML Goodall
- ML Sassano
- MM Aranha
- MM Coissieux
- Mohanish Deshmukh
- Moshe Oren
- MP Baar
- MP Boldin
- MP Boldin
- MP Chao
- MP Luna-Vargas
- MP Soares
- MR Elliott
- MR Sprick
- MT Gyparaki
- MT Lotze
- MV Clement
- MX Li
- N Ahmed
- N Bidere
- N Branzk
- N Echeverry
- N Fricker
- N Furth
- N Kayagaki
- N Kayagaki
- N Kayagaki
- N Lalaoui
- N Peltzer
- N Peltzer
- N Plotegher
- N Robinson
- N Rodic
- N Takahashi
- N Vanlangenakker
- N Vanlangenakker
- N Yagoda
- N Yatim
- N Yatim
- N Zamzami
- N Zamzami
- N Zamzami
- Navdeep S. Chandel
- NE Sharpless
- NE Sharpless
- Nektarios Tavernarakis
- NF Trincheri
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- Ying Wang
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- Yoshihide Tsujimoto
- YS Cho
- Yufang Shi
- Z Cai
- Z Cai
- Z Wang
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- Z Zhang
- Z Zhong
- Zahra Zakeri
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- ZT Schafer
- ZX Chen
- ZX Chen
- Publication venue
- Cell Death Differ
- Publication date
- 01/01/2018
- Field of study
Get PDFOver the past decade, the Nomenclature Committee on Cell Death (NCCD) has formulated guidelines for the definition and interpretation of cell death from morphological, biochemical, and functional perspectives. Since the field continues to expand and novel mechanisms that orchestrate multiple cell death pathways are unveiled, we propose an updated classification of cell death subroutines focusing on mechanistic and essential (as opposed to correlative and dispensable) aspects of the process. As we provide molecularly oriented definitions of terms including intrinsic apoptosis, extrinsic apoptosis, mitochondrial permeability transition (MPT)-driven necrosis, necroptosis, ferroptosis, pyroptosis, parthanatos, entotic cell death, NETotic cell death, lysosome-dependent cell death, autophagy-dependent cell death, immunogenic cell death, cellular senescence, and mitotic catastrophe, we discuss the utility of neologisms that refer to highly specialized instances of these processes. The mission of the NCCD is to provide a widely accepted nomenclature on cell death in support of the continued development of the field
Measurement of the tt¯tt¯ production cross section in pp collisions at √s=13 TeV with the ATLAS detector
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- Zhemchugov A
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- Zhulanov V
- Zieminska D
- Zimine NI
- Zimmermann S
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- Zoccoli A
- Zoch K
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- Åkesson TPA
- Öncel ÖO
- Ženiš T
- Živković L
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- 16/11/2021
- Field of study
Get PDFA measurement of four-top-quark production using proton-proton collision data at a centre-of-mass energy of 13 TeV collected by the ATLAS detector at the Large Hadron Collider corresponding to an integrated luminosity of 139 fb−1 is presented. Events are selected if they contain a single lepton (electron or muon) or an opposite-sign lepton pair, in association with multiple jets. The events are categorised according to the number of jets and how likely these are to contain b-hadrons. A multivariate technique is then used to discriminate between signal and background events. The measured four-top-quark production cross section is found to be 26+17−15 fb, with a corresponding observed (expected) significance of 1.9 (1.0) standard deviations over the background-only hypothesis. The result is combined with the previous measurement performed by the ATLAS Collaboration in the multilepton final state. The combined four-top-quark production cross section is measured to be 24+7−6 fb, with a corresponding observed (expected) signal significance of 4.7 (2.6) standard deviations over the background-only predictions. It is consistent within 2.0 standard deviations with the Standard Model expectation of 12.0 ± 2.4 fb
Measurements of Higgs bosons decaying to bottom quarks from vector boson fusion production with the ATLAS experiment at √=13TeV
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- Abbott B
- Abbott DC
- Abeling K
- Abhayasinghe DK
- Abidi SH
- AbouZeid OS
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- Buttinger W
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- Chiu I
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- Zhemchugov A
- Zheng Z
- Zhong D
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- Zhu Y
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- Zhukov K
- Zhulanov V
- Zieminska D
- Zimine NI
- Zimmermann S
- Zinonos Z
- Ziolkowski M
- Zoccoli A
- Zoch K
- Zorbas TG
- Zou R
- Zwalinski L
- Åkesson TPA
- Öncel ÖO
- Ženiš T
- Živković L
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- 23/06/2021
- Field of study
Get PDFThe paper presents a measurement of the Standard Model Higgs Boson decaying to b-quark pairs in the vector boson fusion (VBF) production mode. A sample corresponding to 126 fb−1 of s√=13TeV proton–proton collision data, collected with the ATLAS experiment at the Large Hadron Collider, is analyzed utilizing an adversarial neural network for event classification. The signal strength, defined as the ratio of the measured signal yield to that predicted by the Standard Model for VBF Higgs production, is measured to be 0.95+0.38−0.36 , corresponding to an observed (expected) significance of 2.6 (2.8) standard deviations from the background only hypothesis. The results are additionally combined with an analysis of Higgs bosons decaying to b-quarks, produced via VBF in association with a photon
Muon reconstruction and identification efficiency in ATLAS using the full Run 2 pp collision data set at \sqrt{s}=13 TeV
- Author
- Aad G
- Abbott B
- Abbott DC
- Abeling K
- Abhayasinghe DK
- Abidi SH
- AbouZeid OS
- Abraham NL
- Abramowicz H
- Abreu H
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- Zhemchugov A
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- Zorbas TG
- Zou R
- Zwalinski L
- Publication venue
- 'Springer Fachmedien Wiesbaden GmbH'
- Publication date
- 01/01/2021
- Field of study
Get PDFThis article documents the muon reconstruction and identification efficiency obtained by the ATLAS experiment for 139 \hbox {fb}^{-1} of pp collision data at \sqrt{s}=13 TeV collected between 2015 and 2018 during Run 2 of the LHC. The increased instantaneous luminosity delivered by the LHC over this period required a reoptimisation of the criteria for the identification of prompt muons. Improved and newly developed algorithms were deployed to preserve high muon identification efficiency with a low misidentification rate and good momentum resolution. The availability of large samples of Z\rightarrow \mu \mu and J/\psi \rightarrow \mu \mu decays, and the minimisation of systematic uncertainties, allows the efficiencies of criteria for muon identification, primary vertex association, and isolation to be measured with an accuracy at the per-mille level in the bulk of the phase space, and up to the percent level in complex kinematic configurations. Excellent performance is achieved over a range of transverse momenta from 3 GeV to several hundred GeV, and across the full muon detector acceptance of |\eta |<2.7
Search for dark matter in events with missing transverse momentum and a Higgs boson decaying into two photons in pp collisions at root s=13 TeV with the ATLAS detector
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- Yexley MR
- Yildiz HD
- Yin P
- Yorita K
- Yoshihara K
- Young C
- Young CJS
- Yuan R
- Yue X
- Zaazoua M
- Zabinski B
- Zacharis G
- Zaffaroni E
- Zagazeta LFG
- Zahreddine J
- Zaitsev AM
- Zakareishvili T
- Zakharchuk N
- Zambito S
- Zanzi D
- Zeissner S
- Zeitnitz C
- Zemaityte G
- Zeng JC
- Zenin O
- Zenis T
- Zenz S
- Zerradi S
- Zerwas D
- Zgubic M
- Zhang B
- Zhang DF
- Zhang G
- Zhang J
- Zhang K
- Zhang L
- Zhang L
- Zhang M
- Zhang R
- Zhang S
- Zhang X
- Zhang X
- Zhang Y
- Zhang Z
- Zhao P
- Zhao Y
- Zhao Z
- Zhemchugov A
- Zheng Z
- Zhong D
- Zhou B
- Zhou C
- Zhou H
- Zhou M
- Zhou N
- Zhou Y
- Zhu C
- Zhu CG
- Zhu H
- Zhu HL
- Zhu J
- Zhu Y
- Zhuang X
- Zhukov K
- Zhulanov V
- Zieminska D
- Zimine N
- Zimmermann S
- Zinonos Z
- Ziolkowski M
- Zivkovic L
- Zoccoli A
- Zoch K
- Zorbas TG
- Zou R
- Zwalinski L
- Publication venue
- 'Springer Fachmedien Wiesbaden GmbH'
- Publication date
- 01/10/2021
- Field of study
Get PDFA search for dark-matter particles in events with large missing transverse momentum and a Higgs boson candidate decaying into two photons is reported. The search uses 139 fb−1 of proton-proton collision data collected at s√ = 13 TeV with the ATLAS detector at the CERN LHC between 2015 and 2018. No significant excess of events over the Standard Model predictions is observed. The results are interpreted by extracting limits on three simplified models that include either vector or pseudoscalar mediators and predict a final state with a pair of dark-matter candidates and a Higgs boson decaying into two photons
Configuration and performance of the ATLAS b-jet triggers in Run 2
- Author
- Aad G
- Abbott B
- Abbott DC
- Abed Abud A
- Abeling K
- Abhayasinghe DK
- Abidi SH
- AbouZeid OS
- Abraham NL
- Abramowicz H
- Abreu H
- Abulaiti Y
- Acharya BS
- Achkar B
- Adam Bourdarios C
- Adam L
- Adamczyk L
- Adamek L
- Adelman J
- Adiguzel A
- Adorni S
- Adye T
- Affolder AA
- Afik Y
- Agapopoulou C
- Agaras MN
- Aggarwal A
- Agheorghiesei C
- Aguilar-Saavedra JA
- Ahmad A
- Ahmadov F
- Ahmed WS
- Ai X
- Aielli G
- Akatsuka S
- Akbiyik M
- Akesson TPA
- Akilli E
- Akimov AV
- Al Khoury K
- Alberghi GL
- Albert J
- Alconada Verzini MJ
- Alderweireldt S
- Aleksa M
- Aleksandrov IN
- Alexa C
- Alexopoulos T
- Alfonsi A
- Alfonsi F
- Alhroob M
- Ali B
- Ali S
- Aliev M
- Alimonti G
- Alison J
- Allaire C
- Allbrooke BMM
- Allport PP
- Aloisio A
- Alonso F
- Alpigiani C
- Alunno Camelia E
- Alvarez Estevez M
- Alviggi MG
- Amaral Coutinho Y
- Ambler A
- Ambroz L
- Amelung C
- Amidei D
- Amor Dos Santos SP
- Amoroso S
- Amrouche CS
- Anastopoulos C
- Andari N
- Andeen T
- Anders JK
- Andrean SY
- Andreazza A
- Andrei V
- Anelli CR
- Angelidakis S
- Angerami A
- Anisenkov AV
- Annovi A
- Antel C
- Anthony MT
- Antipov E
- Antonelli M
- Antrim DJA
- Anulli F
- Aoki M
- Aparisi Pozo JA
- Aparo MA
- Aperio Bella L
- Aranzabal N
- Araujo Ferraz V
- Arcangeletti C
- Arce ATH
- Arguin J-F
- Argyropoulos S
- Arling J-H
- Armbruster AJ
- Armstrong A
- Arnaez O
- Arnold H
- Arrubarrena Tame ZP
- Artoni G
- Asada H
- Asai K
- Asai S
- Asawatavonvanich T
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- Publication venue
- 'Springer Fachmedien Wiesbaden GmbH'
- Publication date
- 01/12/2021
- Field of study
Get PDFSeveral improvements to the ATLAS triggers used to identify jets containing b-hadrons (b-jets) were implemented for data-taking during Run 2 of the Large Hadron Collider from 2016 to 2018. These changes include reconfiguring the b-jet trigger software to improve primary-vertex finding and allow more stable running in conditions with high pile-up, and the implementation of the functionality needed to run sophisticated taggers used by the offline reconstruction in an online environment. These improvements yielded an order of magnitude better light-flavour jet rejection for the same b-jet identification efficiency compared to the performance in Run 1 (2011–2012). The efficiency to identify b-jets in the trigger, and the conditional efficiency for b-jets that satisfy offline b-tagging requirements to pass the trigger are also measured. Correction factors are derived to calibrate the b-tagging efficiency in simulation to match that observed in data. The associated systematic uncertainties are substantially smaller than in previous measurements. In addition, b-jet triggers were operated for the first time during heavy-ion data-taking, using dedicated triggers that were developed to identify semileptonic b-hadron decays by selecting events with geometrically overlapping muons and jets
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