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229 research outputs found

Absence of N-terminal acetyltransferase diversification during evolution of eukaryotic organisms

Author: A Ametzazurra
A Ben-Bassat
A Hershko
A Marintchev
A Murthi
A Pimenta-Marques
A Shemorry
A Staes
A Yoshikawa
AF Rope
AI Saeed
AL Pang
AO Helbig
B Polevoda
B Polevoda
B Polevoda
B Polevoda
B Polevoda
B Zybailov
BC Williams
CS Hwang
D Lang
D Zattas
DC Scott
EC Park
EV Koonin
G Liszczak
G Liszczak
G Liszczak
G Talavera
G Zhang
GM Forte
H Aksnes
HS Yoon
HY Zhu
I Dikiy
I Hofmann
J Sanchez
JD Jones
JL Brown
JM Singer
JP Casey
JR Mullen
K Hole
KK Starheim
KK Starheim
KK Starheim
LG Guilgur
LM Myklebust
M Gautschi
MA Larkin
MD Katinka
ML Angus-Hill
N Arnaudo
OK Song
P Van Damme
P Van Damme
P Van Damme
P Van Damme
P Van Damme
P Van Damme
R Behnia
R Evjenth
R Shemesh
RD Finn
RD Silva
RP Moerschell
S Capella-Gutierrez
S Goetze
S Hoshiyasu
S Tanaka
SF Altschul
SR Setty
T Arnesen
T Arnesen
T Arnesen
T Arnesen
T Arnesen
T Arnesen
T Esmailpour
T van Welsem
TB Chou
TV Dinh
TV Kalvik
TY James
WV Bienvenut
WV Bienvenut
Y Wang
YY Chang
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2016
Field of study

Protein N-terminal acetylation is an ancient and ubiquitous co-translational modification catalyzed by a highly conserved family of N-terminal acetyltransferases (NATs). Prokaryotes have at least 3 NATs, whereas humans have six distinct but highly conserved NATs, suggesting an increase in regulatory complexity of this modification during eukaryotic evolution. Despite this, and against our initial expectations, we determined that NAT diversification did not occur in the eukaryotes, as all six major human NATs were most likely present in the Last Eukaryotic Common Ancestor (LECA). Furthermore, we also observed that some NATs were actually secondarily lost during evolution of major eukaryotic lineages; therefore, the increased complexity of the higher eukaryotic proteome occurred without a concomitant diversification of NAT complexes

Crossref

Ghent University Academic Bibliography

PubMed Central

Sapientia

Comprehensively Surveying Structure and Function of RING Domains from Drosophila melanogaster

Author: A Carbone
A Espinosa
A Paiardini
A Reymond
A Suzuki
AK Jain
AM Abdul-Nabi
AS Konagurthu
C Dominguez
C Sun
CG Vinuesa
Chunhong Huang
CN Pang
CS Hwang
CW Vander Kooi
D Chen
D Hasegawa
D Wei
DT Huang
E Duprez
E Pringa
E Santonico
EE Hill
F Armougom
F Ding
Fusheng Wan
G Apic
G Kleiger
G Markson
GS Winkler
H Wang
Haijun Zhao
J Dreyer
J Dundas
J Lagirand-Cantaloube
J Omwancha
J Pei
J Qu
J Salonen
JA Marteijn
JM Matthews
JP Bocock
K Assemat
K Sughra
Kemin Jie
KL Lorick
L Aravind
L Carthagena
L Holm
L Xia
LC Seeberger
LY Geer
M Minakawa
M Shatsky
M Ying
M Zhang
Muying Ying
N Guex
N Nikoh
N Saitou
N Shembade
N Zheng
O Lespinet
P Horton
P Mercier
PD Mace
Q Yin
R Rajendra
RB Dodd
RJ Deshaies
S Engelen
S Kumar
S Natarajan
S Weger
SF Altschul
SJ van Wijk
SL Stone
SM Srinivasula
SR Comeau
T Castrignanò
TS Chang
V Soundararajan
W Li
W Liao
W Wang
Wanjin Hong
Xiaotian Huang
Y Huang
Y Li
Y Ofran
Y Sun
Y Yang
Y Zhou
Yuehao Wu
Z Su
Z Xu
ZX Shen
Publication venue: Public Library of Science
Publication date: 02/09/2011
Field of study

Using a complete set of RING domains from Drosophila melanogaster, all the solved RING domains and cocrystal structures of RING-containing ubiquitin-ligases (RING-E3) and ubiquitin-conjugating enzyme (E2) pairs, we analyzed RING domains structures from their primary to quarternary structures. The results showed that: i) putative orthologs of RING domains between Drosophila melanogaster and the human largely occur (118/139, 84.9%); ii) of the 118 orthologous pairs from Drosophila melanogaster and the human, 117 pairs (117/118, 99.2%) were found to retain entirely uniform domain architectures, only Iap2/Diap2 experienced evolutionary expansion of domain architecture; iii) 4 evolutionary structurally conserved regions (SCRs) are responsible for homologous folding of RING domains at the superfamily level; iv) besides the conserved Cys/His chelating zinc ions, 6 equivalent residues (4 hydrophobic and 2 polar residues) in the SCRs possess good-consensus and conservation- these 4 SCRs function in the structural positioning of 6 equivalent residues as determinants for RING-E3 catalysis; v) members of these RING proteins located nucleus, multiple subcellular compartments, membrane protein and mitochondrion are respectively 42 (42/139, 30.2%), 71 (71/139, 51.1%), 22 (22/139, 15.8%) and 4 (4/139, 2.9%); vi) CG15104 (Topors) and CG1134 (Mul1) in C3HC4, and CG3929 (Deltex) in C3H2C3 seem to display broader E2s binding profiles than other RING-E3s; vii) analyzing intermolecular interfaces of E2/RING-E3 complexes indicate that residues directly interacting with E2s are all from the SCRs in RING domains. Of the 6 residues, 2 hydrophobic ones contribute to constructing the conserved hydrophobic core, while the 2 hydrophobic and 2 polar residues directly participate in E2/RING-E3 interactions. Based on sequence and structural data, SCRs, conserved equivalent residues and features of intermolecular interfaces were extracted, highlighting the presence of a nucleus for RING domain fold and formation of catalytic core in which related residues and regions exhibit preferential evolutionary conservation

Public Library of Science (PLOS)

Crossref

PubMed Central

How patients understand depression associated with chronic physical disease - A systematic review

Author: A Antonovsky
A Karasz
A Karasz
A Karasz
A Karasz
A Liberati
A Rogers
A Yeung
Allan House
B Lindstrom
B Lowe
B Rudisch
B Williams
BW Van Voorhees
BW Van Voorhees
C Brown
C Brown
C Brown
C Dowrick
C Heifner
CA Sarkisian
CM Bann
CS Cornford
D Martin
D Martin
DA Karp
Department of Health
DN Subramanian
DN Ugarriza
E Barley
ES Okello
F Badger
F Lobban
G Fortune
G Green
H Burroughs
HR Bogner
I Kangas
J Cape
J Grime
J Lynch
J Popay
J Srinivasan
JK Shin
JL Givens
JL Givens
K Chakraborty
K Wittkampf
Kate McLintock
KJ Petrie
KYC Pang
L Cooper-Patrick
L Gask
LA Cooper
LA Cooper
LA Cooper
LB Kirk
LD Cameron
Liz Glidewell
LJ Cabassa
M Backenstrass
M Dejman
M Maxwell
MA Kelly
MA Prins
MA Whooley
ME Addis
ME Addis
MJ Edlund
MN Wittink
MP Pignone
N Al-Saffar
National Institute of Clinical Excellence
National Institute of Clinical Excellence
NHS Centre for Reviews and Dissemination
O Johnston
P Nolan
PJ Wagner
R Manber
R Waite
RD Goldney
RL Allen
RM Carney
Robbie Foy
S Kurtz
Sarah L Alderson
SE Hampson
SE Lewis
SF Garfield
SM Gilbody
T Stecker
U Danielsson
W Kuyken
Y Leykin
Y Scattolon
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2012
Field of study

Background: Clinicians are encouraged to screen people with chronic physical illness for depression. Screening alone may not improve outcomes, especially if the process is incompatible with patient beliefs. The aim of this research is to understand peoples beliefs about depression, particularly in the presence of chronic physical disease. Methods: A mixed method systematic review involving a thematic analysis of qualitative studies and quantitative studies of beliefs held by people with current depressive symptoms. MEDLINE, EMBASE, PSYCHINFO, CINAHL, BIOSIS, Web of Science, The Cochrane Library, UKCRN portfolio, National Research Register Archive, Clinicaltrials.gov and OpenSIGLE were searched from database inception to 31st December 2010. A narrative synthesis of qualitative and quantitative data, based initially upon illness representations and extended to include other themes not compatible with that framework. Results: A range of clinically relevant beliefs was identified from 65 studies including the difficulty in labeling depression, complex causal factors instead of the biological model, the roles of different treatments and negative views about the consequences of depression. We found other important themes less related to ideas about illness: the existence of a self-sustaining depression spiral; depression as an existential state; the ambiguous status of suicidal thinking; and the role of stigma and blame in depression. Conclusions: Approaches to detection of depression in physical illness need to be receptive to the range of beliefs held by patients. Patient beliefs have implications for engagement with depression screening

Crossref

Springer - Publisher Connector

Directory of Open Access Journals

PubMed Central

White Rose Research Online

Single nucleus genome sequencing reveals high similarity among nuclei of an endomycorrhizal fungus

Author: A Bairoch
A Conesa
A Gandolfi
A Gollotte
A Stamatakis
A Stamatakis
AJ Enright
AL Price
BJ Haas
BJ Haas
BJ Haas
C Angelard
C Sbrana
CJA Sigrist
CL Schoch
CS Campbell
D Croll
D Croll
D Redecker
D Redecker
Desheng Mu
DGO Saunders
Diane G. O. Saunders
Duur K. Aanen
E Boon
E Quevillon
E Tisserant
Erik Limpens
Erli Pang
ES Dolgin
F Martin
F Martin
F Martin
G Kuhn
G Parra
G Parra
G Sun
Geraldine Butler
H Shimodaira
H Stockinger
HC den Bakker
Huifen Cao
HW Mewes
Hwangho Cha
I Korf
I Stergiopoulos
IR Arkhipova
IR Sanders
J Jorda
J Jurka
J Kämper
J Lee
J Marleau
J Win
JE Galagan
Joe Win
K Katoh
KA Sędzielewska
KO Wrzeszczynski
Kui Lin
L Li
L-J Ma
M Cokol
M Hijri
M Magrane
M Parniske
M Stanke
MW Dimmic
N Corradi
N King
N Navin
Norbert de Ruijter
O Emanuelsson
O Gotoh
O Gotoh
P Horton
P Vandenkoornhuyse
Qian Zhou
R Apweiler
R Luo
R Riley
RA Dean
RC Edgar
René Geurts
RH Nilsson
Robin van Velzen
S Altschul
S Capella-Gutiérrez
S Halary
S Joneson
S Kloppholz
Sanwen Huang
Sergey Ivanov
SF Altschul
Sophien Kamoun
TA Torto
Tao Lin
TE Pawlowska
TH Eickbush
Ton Bisseling
Trupti Sharma
TY James
TY James
V Ter-Hovhannisyan
VCG Tagua
W Li
WH Majoros
Yi Shang
Ying Li
YJ Liu
Z Iqbal
Z Iqbal
Z Xu
Zhonghua Zhang
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 01/01/2014
Field of study

Nuclei of arbuscular endomycorrhizal fungi have been described as highly diverse due to their asexual nature and absence of a single cell stage with only one nucleus. This has raised fundamental questions concerning speciation, selection and transmission of the genetic make-up to next generations. Although this concept has become textbook knowledge, it is only based on studying a few loci, including 45S rDNA. To provide a more comprehensive insight into the genetic makeup of arbuscular endomycorrhizal fungi, we applied de novo genome sequencing of individual nuclei of Rhizophagus irregularis. This revealed a surprisingly low level of polymorphism between nuclei. In contrast, within a nucleus, the 45S rDNA repeat unit turned out to be highly diverged. This finding demystifies a long-lasting hypothesis on the complex genetic makeup of arbuscular endomycorrhizal fungi. Subsequent genome assembly resulted in the first draft reference genome sequence of an arbuscular endomycorrhizal fungus. Its length is 141 Mbps, representing over 27,000 protein-coding gene models. We used the genomic sequence to reinvestigate the phylogenetic relationships of Rhizophagus irregularis with other fungal phyla. This unambiguously demonstrated that Glomeromycota are more closely related to Mucoromycotina than to its postulated sister Dikarya

Crossref

Directory of Open Access Journals

PubMed Central

Wageningen University & Research Publications

University of East Anglia digital repository

FigShare

Identification of ejaculated proteins in the house mouse (Mus domesticus) via isotopic labeling

Author: A Civetta
A Nagy
A Wong
A Wong
AC Fiumera
AC Fiumera
AC Paoletti
AF Dixson
AG Clark
AS Alghamdi
AY Olsson
AY Olsson
B Peitz
B Peitz
B Peitz
B Pilch
BM Balgley
C Voolstra
CC Wu
CD Meiklejohn
Christine C Wu
CJ Thaler
CS Carter
CSC Price
DA Dewsbury
DA Goldfoot
DB McClatchy
DG Torgerson
DJ Anderson
DJ Baumgardner
DM Good
DW Rogers
ES Kelleher
ES Kelleher
ES Kelleher
F Helfenstein
F Wartha
GA Cunningham
GA Silverman
GD Findlay
Geoffrey D Findlay
GG Ignotz
H-J Lin
J Martan
J Walters
JD Thompson
JE Aagaard
JK Eng
JL Marshall
JM Good
K Queen
K Ravi Ram
KK Stein
L Florens
L Kall
LA Herndon
LG Harshman
M Ashburner
M Diamond
M Spivak
MA Baker
MA Henault
Matthew D Dean
MB Coulthart
MC Devine
MC Devine
MD Dean
MD Dean
MD Dean
MF Palopoli
Michael J MacCoss
Michael R Hoopmann
Michael W Nachman
MKN Lawniczak
MR Hoopmann
MR Hoopmann
N Goldman
N Kawano
ND Rawlings
NL Clark
NL Clark
NL Clark
O Emanuelsson
P Khaitovich
PL Moreira
PN Robinson
R Carballada
R Porta
R Voss
R Wernersson
RA Gibbs
RB Land
RC Firman
RC Firman
RC Karn
RH Waterston
RJ Aitken
RK Sharma
RL Snyder
RL Snyder
RT Tecirlioglu
S Dorus
S Dorus
SA Asdell
SA Ramm
SA Ramm
SA Ramm
SA Robertson
SE Fawell
SF Pang
SJ O'Brien
SL Kosakovsky Pond
SL Kosakovsky Pond
SV Nuzhdin
T Chapman
TG Hartung
W Cao
W-s O
Willie J Swanson
WJ Swanson
WS O
Y Agrawal
Y Heifetz
Y Heifetz
YH Huang
Z Yang
Z Yang
Å Lundwall
Publication venue: BioMed Central
Publication date: 01/01/2011
Field of study

Abstract Background Seminal fluid plays an important role in successful fertilization, but knowledge of the full suite of proteins transferred from males to females during copulation is incomplete. The list of ejaculated proteins remains particularly scant in one of the best-studied mammalian systems, the house mouse (<it>Mus domesticus</it>), where artificial ejaculation techniques have proven inadequate. Here we investigate an alternative method for identifying ejaculated proteins, by isotopically labeling females with 15N and then mating them to unlabeled, vasectomized males. Proteins were then isolated from mated females and identified using mass spectrometry. In addition to gaining insights into possible functions and fates of ejaculated proteins, our study serves as proof of concept that isotopic labeling is a powerful means to study reproductive proteins. Results We identified 69 male-derived proteins from the female reproductive tract following copulation. More than a third of all spectra detected mapped to just seven genes known to be structurally important in the formation of the copulatory plug, a hard coagulum that forms shortly after mating. Seminal fluid is significantly enriched for proteins that function in protection from oxidative stress and endopeptidase inhibition. Females, on the other hand, produce endopeptidases in response to mating. The 69 ejaculated proteins evolve significantly more rapidly than other proteins that we previously identified directly from dissection of the male reproductive tract. Conclusion Our study attempts to comprehensively identify the proteins transferred from males to females during mating, expanding the application of isotopic labeling to mammalian reproductive genomics. This technique opens the way to the targeted monitoring of the fate of ejaculated proteins as they incubate in the female reproductive tract.</p

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Springer - Publisher Connector

Directory of Open Access Journals

PubMed Central

The University of Arizona

Epigenetic regulation of prostate cancer

Author: A Aitchison
A Altimari
A Bird
A Chase
A Cihak
A Eden
A Feinberg
A Perl
A Thibault
A Villers
AF Cashen
AM Marzo De
AR Brothman
AR Florl
AT Hark
B Halliwell
B Karanikolas
B Lee
BH Lee
BK Dunn
BR Konety
BV Kallakury
C Goessl
C Jeronimo
C Jeronimo
C Liu
C Trejo-Becerril
C Walker
CA Hamm
CK Chuang
CS Zorn
D Allen
D Krill
D Lavelle
D Rathkopf
D Seligson
D Waltregny
DC Chu
DF Jarrard
DF Jarrard
DL Marrocco
DS Schrump
DV Santi
DZ Qian
DZ Qian
DZ Qian
E Kaminskas
E Macri
E Metzger
E Papadopoulou
E Rosenbaum
F Crea
G Gravina
G Jenster
G Schwartz
G Sozzi
G Wang
G Xu
GA Calin
GH Kang
GJ Miller
GM Vidanes
GN Batty
GP Pfeifer
H Huang
H Suzuki
HM Kantarjian
HS Basu
I Thompson
I Vlodavsky
J Ellinger
J Ellinger
J Ellinger
J Ellinger
J Lee
J Reibenwein
J Tan
J Tsihlias
J Yu
JC Chuang
JC Chuang
JD Brooks
JE Visvader
JR Graff
K Appleton
K Halkidou
K Jung
K Nishioka
K Yamane
KE Gardner
KP Porkka
L Bubendorf
L Gaughan
L He
L He
L Jackson-Grusby
L Li
L Liu
L Patrawala
L Patrawala
L Richiardi
LB Hesson
LC Li
LK Gediya
LM Butler
LR Molife
M Esteller
M Gardiner-Garden
M Nakayama
M Opel
M Roupret
M Schmudde
M Schnekenburger
M Suenaga
M Wissmann
MD Hulett
ME Perry
MT Bedford
MT Lai
N Mercatelli
N Shukeir
NS Verkaik
NS Verkaik
P Cairns
P Cairns
P Cao
P Chinnaiyan
P Jones
P Jones
P Kahl
P Ostling
P Pakneshan
PA Jones
PJ Bastian
PJ Bastian
PJ Bastian
PN Munster
PS Mitchell
Q Wang
R Dammann
R Henrique
R Illingworth
R Singal
RD Kornberg
RM Yang
S Ambs
S Berger
S Dissanayake
S Galardi
S Jahr
S Santourlidis
S Shabbeer
S Sharma
S Takahashi
S Tekur
S Varambally
S Varambally
S Volinia
S Yegnasubramanian
SB Hake
SF Rashid
SG Chi
SK Kulp
SV Harden
T Bianco-Miotto
T Kouzarides
T Ogishima
T Tokizane
TB Miranda
V Lakshmikanthan
V Phé
W Lou
WA Schulz
WH Lee
X Lin
X Lin
X Nan
X Tang
Y Fujita
Y Hao
Y Hayashita
Y Pang
Y Saunthararajah
Y Shi
YE Whang
Z Zhang
ZH Huang
Publication venue: Springer-Verlag
Publication date: 01/01/2011
Field of study

Prostate cancer is a commonly diagnosed cancer in men and a leading cause of cancer deaths. Whilst the underlying mechanisms leading to prostate cancer are still to be determined, it is evident that both genetic and epigenetic changes contribute to the development and progression of this disease. Epigenetic changes involving DNA hypo- and hypermethylation, altered histone modifications and more recently changes in microRNA expression have been detected at a range of genes associated with prostate cancer. Furthermore, there is evidence that particular epigenetic changes are associated with different stages of the disease. Whilst early detection can lead to effective treatment, and androgen deprivation therapy has a high response rate, many tumours develop towards hormone-refractory prostate cancer, for which there is no successful treatment. Reliable markers for early detection and more effective treatment strategies are, therefore, needed. Consequently, there is a considerable interest in the potential of epigenetic changes as markers or targets for therapy in prostate cancer. Epigenetic modifiers that demethylate DNA and inhibit histone deacetylases have recently been explored to reactivate silenced gene expression in cancer. However, further understanding of the mechanisms and the effects of chromatin modulation in prostate cancer are required. In this review, we examine the current literature on epigenetic changes associated with prostate cancer and discuss the potential use of epigenetic modifiers for treatment of this disease

Crossref

Springer - Publisher Connector

PubMed Central

Prognostic model to predict postoperative acute kidney injury in patients undergoing major gastrointestinal surgery based on a national prospective observational cohort study.

Author: Aamir A
Abbas J
Abbas N
Abbott TEF
Abdalla M
Abdikadir H
Abuhussein N
Acquaah F
Adamson R
Adeleye O
Adeogun A
Adlan A
Aftab R
Afzal Z
Agarwal M
Aglan H
Agnew CJF
Agrawal R
Ahern D
Ahluwalia J
Ahluwalia V
Ahmad A
Ahmad K
Ahmed H
Ahmed I
Ahmed L
Ahmed N
Ahmed P
Ainger E
Ainsworth P
Aishwarya G
Ajibola-Taylor O
Akhbari M
Akhtar A
Akhtar R
Akpenyi O
Al-Ausi M
Al-Huneidi R
Al-Khudairi R
Al-Masri S
Al-Mousawi A
Al-Saadi N
Alagappan A
Alberts J
Alfa-Wali M
Ali A
Ali B
Ali I
Ali M
Ali Q
Ali S
Alturki N
Alwandi A
Amani L
Amarnath T
Amer M
Amin H
Amin MN
Amoah R
Amoah-Arko A
Anandarajah C
Ananthavarathan P
Andah EJE
Andrew K
Andrews H
Ang A
Ang HL
Ang JJ
Ani C
Anilkumar A
Anto N
Anwar S
Apperley H
Appleton S
Aquilina T
Archer M
Arif T
Arneill M
Arnell S
Arnold TJ
Arshad A
Arthur J
Arulkumaran N
Arya J
Asad M
Asemota N
Ashaye T
Ashdown T
Ashour R
Ashraf MR
Ashwood J
Asif U
Atkin G
Atkins B
Attalla M
Aubrey-Jones D
Auckburally S
Auld F
Auluck I
Azam S
Aziz R
Azizi A
Azmi F
Babatunde F
Babu VS
Bachi A
Bagga R
Bains H
Bajwa DS
Baker A
Baker C
Balai E
Balian V
Ball M
Bamford M
Bana R
Banfield DA
Bannard-Smith J
Barai I
Barclay J
Barfi L
Barker C
Barker M
Barmayehvar B
Barnfield J
Barnor-Ahiaku E
Baron C
Barr CJ
Barraclough J
Baryan HK
Basra M
Bassam N
Bath MF
Battle J
Beasley W
Beattie G
Beattie S
Beatty M
Beghal G
Begum F
Behranwala K
Belchos J
Belgaid DR
Belgaumkar A
Bell S
Ben-Gal O
Benchetrit S
Bennett M
Benons N
Bernal TL
Bertelli M
Berthaume-Hawkins SD
Best R
Betts A
Bevan K
Bews-Hair M
Bhambra R
Bhamra N
Bhangu A
Bhatte S
Bhatti A
Bhide I
Bhome R
Bhudia R
Bhullar S
Bienias A
Billyard C
Bird C
Birkinshaw F
Black J
Blake E
Blazeby JM
Bleakley A
Bloom I
Bogle R
Bolton W
Borakati A
Boraluwe-Rallage H
Borg CM
Botha A
Boualbanat Y
Boulton APR
Bountra K
Bowley D
Boyd G
Boyles L
Bradley P
Brannick S
Brayley J
Brecher J
Breen H
Bristow S
Britton N
Broad J
Brobbey P
Brock E
Brooke M
Brown A
Brown B
Brown F
Brown FS
Brown H
Brown K
Brown LR
Brown M
Brown N
Brown R
Brown S
Brown T
Bruce C
Bruce P
Budd E
Bull K
Burgin A
Burke D
Burke J
Burnage S
Burns N
Burrows A
Busti S
Butler A
Cabdi NMO
Cadden F
Cairns C
Calabria C
Calciu A
Campbell A
Campbell B
Campbell G
Campbell HS
Cannon SP
Cant M
Capella S
Cardus C
Cardwell A
Cargill Z
Caroll P
Carr G
Carr R
Carr W
Carse S
Carter N
Carter R
Castle A
Cato L
Cave D
Cecil E
Chadwick H
Chadwick M
Chan F
Chan L
Chan M
Chan SSN
Chan-lam N
Chandler E
Chandler S
Chandramoorthy L
Chandramoorthy S
Chang A
Chang LH
Chang M
Chappelow I
Chapple K
Charnley R
Chaudhry A
Chaudhry S
Chauhan P
Chavan A
Chean CS
Chen L
Chen Y
Chenciner L
Cheng J
Chesner R
Cheung W
Chin YR
China Z
Chitsabesan P
Chohan K
Choi JE
Chong A
Chong P
Choo S
Chopada A
Chouari T
Choudhary Y
Choudhry M
Choy CH
Christie S
Christopher E
Chudek D
Chui J
Church M
Church R
Cipparrone M
Claireaux HA
Clark K
Clarke B
Clement KD
Clements B
Clements SE
Cobley H
Coe P
Cohen J
Coldicutt O
Cole A
Coleman M
Collaborative S
Collins J
Collishaw A
Common M
Concannon K
Conchie H
Connelly A
Connor M
Cookson P
Cope EA
Cope T
Copeland M
Copley HC
Coppel J
Corbridge O
Cotter M
Courquin GR
Court J
Cox L
Craig ARJ
Craig N
Crane E
Cremen S
Cresswell B
Crewe A
Crilly C
Crilly L
Croghan N
Croitoru C
Cromwell D
Cronbach P
Crook H
Crozier L
Cruddas L
Cullum R
Cumber E
Cumming S
Cummings D
Cunliffe L
Cunningham L
Curtis A
Curtis J
D'Auria M
D'Souza F
Dada J
Dalal F
Dalrymple J
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STARSurg Collaborative Writing Committee, Data analysis, Steering committee, Advisory group, Regional leads, Collaborators and validators
STARSurg Collaborative Writing Committee, Data analysis, Steering committee, Advisory group, Regional leads, Collaborators and validators, Nepogodiev, D
Stechman M
Stewart D
Stewart E
Stewart H
Stewart R
Stickler E
Stoddart MT
Stokes E
Stott G
Strang S
Stringer H
Stringfellow TD
Stubbing-Moore A
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Sukirthan N
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Taribagil P
Tariq A
Tate S
Tayeh S
Taylor K
Taylor O
Taylor R
Taylor Z
Telfer R
Teng T
Tenters F
Teo R
Thachettu A
Thakrar D
Thatcher A
Theodoropoulou K
Thomas A
Thomas D
Thomas M
Thomas O
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Thompson G
Thompson J
Thoms BL
Thomson F
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Thorpe O
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Xu Y
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Yang DD
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Yasin IH
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Ye W
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Yeung J
Yin ZD
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Yogeswara T
York J
Yousaf A
Youssef H
Yu T
Yule A
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Zanichelli D
Zaver V
Zeng R
Zhang Y
Zheleniakova T
Zhu Y
Zornoza A
Zubikarai G
Zulkifli A
Zuzarte L
Publication venue: 'Wiley'
Publication date: 18/05/2018
Field of study

Background: Acute illness, existing co-morbidities and surgical stress response can all contribute to postoperative acute kidney injury (AKI) in patients undergoing major gastrointestinal surgery. The aim of this study was prospectively to develop a pragmatic prognostic model to stratify patients according to risk of developing AKI after major gastrointestinal surgery. Methods: This prospective multicentre cohort study included consecutive adults undergoing elective or emergency gastrointestinal resection, liver resection or stoma reversal in 2-week blocks over a continuous 3-month period. The primary outcome was the rate of AKI within 7 days of surgery. Bootstrap stability was used to select clinically plausible risk factors into the model. Internal model validation was carried out by bootstrap validation. Results: A total of 4544 patients were included across 173 centres in the UK and Ireland. The overall rate of AKI was 14·2 per cent (646 of 4544) and the 30-day mortality rate was 1·8 per cent (84 of 4544). Stage 1 AKI was significantly associated with 30-day mortality (unadjusted odds ratio 7·61, 95 per cent c.i. 4·49 to 12·90; P < 0·001), with increasing odds of death with each AKI stage. Six variables were selected for inclusion in the prognostic model: age, sex, ASA grade, preoperative estimated glomerular filtration rate, planned open surgery and preoperative use of either an angiotensin-converting enzyme inhibitor or an angiotensin receptor blocker. Internal validation demonstrated good model discrimination (c-statistic 0·65). Discussion: Following major gastrointestinal surgery, AKI occurred in one in seven patients. This preoperative prognostic model identified patients at high risk of postoperative AKI. Validation in an independent data set is required to ensure generalizability

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Combination of searches for heavy spin-1 resonances using 139 fb−1 of proton-proton collision data at s = 13 TeV with the ATLAS detector

Author: Aad G
Aakvaag E
Abbott B
Abeling K
Abicht NJ
Abidi SH
Aboelela M
Aboulhorma A
Abramowicz H
Abreu H
Abulaiti Y
Acharya BS
Ackermann A
Adam Bourdarios C
Adamczyk L
Addepalli SV
Addison MJ
Adelman J
Adiguzel A
Adye T
Affolder AA
Afik Y
Agaras MN
Agarwala J
Aggarwal A
Agheorghiesei C
Ahmad A
Ahmadov F
Ahmed WS
Ahuja S
Ai X
Aielli G
Aikot A
Ait Tamlihat M
Aitbenchikh B
Aizenberg I
Akbiyik M
Akimov AV
Akiyama D
Akolkar NN
Aktas S
Al Khoury K
Alberghi GL
Albert J
Albicocco P
Albouy GL
Alderweireldt S
Alegria ZL
Aleksa M
Aleksandrov IN
Alexa C
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Alfonsi F
Algren M
Alhroob M
Ali B
Ali HMJ
Ali S
Alibocus SW
Aliev M
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Alkakhi W
Allaire C
Allbrooke BMM
Allen JF
Allendes Flores CA
Allport PP
Aloisio A
Alonso F
Alpigiani C
Alvarez Estevez M
Alvarez Fernandez A
Alves Cardoso M
Alviggi MG
Aly M
Amaral Coutinho Y
Ambler A
Amelung C
Amerl M
Ames CG
Amidei D
Amirie KJ
Amor Dos Santos SP
Amos KR
An S
Ananiev V
Anastopoulos C
Andeen T
Anders JK
Andrean SY
Andreazza A
Angelidakis S
Angerami A
Anisenkov AV
Annovi A
Antel C
Anthony MT
Antipov E
Antonelli M
Anulli F
Aoki M
Aoki T
Aparisi Pozo JA
Aparo MA
Aperio Bella L
Appelt C
Apyan A
Arbiol Val SJ
Arcangeletti C
Arce ATH
Arena E
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Argyropoulos S
Arling J-H
Arnaez O
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Astalos R
Astrand KSV
Atashi S
Atkin RJ
Atkinson M
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Atmasiddha PA
Augsten K
Auricchio S
Auriol AD
Austrup VA
Avolio G
Axiotis K
Azuelos G
Babal D
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Backman F
Badea A
Baer TM
Bagnaia P
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Bahner D
Bai K
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Baines JT
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Baker OK
Bakos E
Bakshi Gupta D
Balakrishnan V
Balasubramanian R
Baldin EM
Balek P
Ballabene E
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Balunas WK
Balz J
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Bandyopadhyay A
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Barak L
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Barberio EL
Barberis D
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Barel MZ
Barends KN
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Barisits M-S
Barklow T
Baron Moreno DA
Baron P
Baroncelli A
Barone G
Barr AJ
Barr JD
Barreiro Guimarães da Costa J
Barreiro F
Barron U
Barros Teixeira MG
Barsov S
Bartels F
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Barton AE
Bartos P
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Baselga M
Bassalat A
Basso MJ
Bates RL
Batlamous S
Batool B
Battaglia M
Battulga D
Bauce M
Bauer M
Bauer P
Bazzano Hurrell LT
Beacham JB
Beau T
Beaucamp JY
Beauchemin PH
Bechtle P
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Beddall AJ
Bednyakov VA
Bee CP
Beemster LJ
Beermann TA
Begalli M
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Behera A
Behr JK
Beirer JF
Beisiegel F
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Bella G
Bellagamba L
Bellerive A
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Benchekroun D
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Benhammou Y
Benkendorfer KC
Beresford L
Beretta M
Bergeaas Kuutmann E
Berger N
Bergmann B
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Bernardi G
Bernius C
Bernlochner FU
Bernon F
Berrocal Guardia A
Berry T
Berta P
Berthold A
Bethke S
Betti A
Bevan AJ
Bhalla NK
Bhamjee M
Bhatta S
Bhattacharya DS
Bhattarai P
Bhide KD
Bhopatkar VS
Bianchi RM
Bianco G
Biebel O
Bielski R
Biglietti M
Billingsley CS
Bindi M
Bingul A
Bini C
Biondini A
Birch-sykes CJ
Bird GA
Birman M
Biros M
Biryukov S
Bisanz T
Bisceglie E
Biswal JP
Biswas D
Bjørke K
Bloch I
Blue A
Blumenschein U
Blumenthal J
Bobrovnikov VS
Boehler M
Boehm B
Bogavac D
Bogdanchikov AG
Bohm C
Boisvert V
Bokan P
Bold T
Bomben M
Bona M
Boonekamp M
Booth CD
Borbély AG
Bordulev IS
Borecka-Bielska HM
Borissov G
Bortoletto D
Boscherini D
Bosman M
Bossio Sola JD
Bouaouda K
Bouchhar N
Boudreau J
Bouhova-Thacker EV
Boumediene D
Bouquet R
Boveia A
Boyd J
Boye D
Boyko IR
Bracinik J
Brahimi N
Brandt G
Brandt O
Braren F
Brau B
Brau JE
Brener R
Brenner L
Brenner R
Bressler S
Britton D
Britzger D
Brock I
Brooijmans G
Brost E
Brown LM
Bruce LE
Bruckler TL
Bruckman de Renstrom PA
Bruni A
Bruni G
Bruschi M
Bruscino N
Brüers B
Buanes T
Buat Q
Buchin D
Buckley AG
Bulekov O
Bullard BA
Burdin S
Burgard CD
Burger AM
Burghgrave B
Burlayenko O
Burr JTP
Burton CD
Burzynski JC
Busch EL
Bussey PJ
Butler JM
Buttar CM
Butterworth JM
Buttinger W
Buxo Vazquez CJ
Buzykaev AR
Büscher V
Cabrera Urbán S
Cadamuro L
Caforio D
Cai H
Cai Y
Cai Y
Cairo VMM
Cakir O
Calace N
Calafiura P
Calderini G
Calfayan P
Callea G
Caloba LP
Calvet D
Calvet S
Calvetti M
Camacho Toro R
Camarda S
Camarero Munoz D
Camarri P
Camerlingo MT
Cameron D
Camincher C
Campanelli M
Camplani A
Canale V
Canbay AC
Canonero E
Cantero J
Cao Y
Capocasa F
Capua M
Carbone A
Cardarelli R
Cardenas JCJ
Cardillo F
Carducci G
Carli T
Carlino G
Carlotto JI
Carlson BT
Carlson EM
Carminati L
Carnelli A
Carnesale M
Caron S
Carquin E
Carratta G
Carroll AM
Carrá S
Carter TM
Casado MP
Caspar M
Castillo Garcia L
Castillo Gimenez V
Castillo FL
Castro NF
Catinaccio A
Catmore JR
Cavaliere T
Cavaliere V
Cavalli N
Cekmecelioglu YC
Celebi E
Cella S
Celli F
Centonze MS
Cepaitis V
Cerny K
Cerqueira AS
Cerri A
Cerrito L
Cerutti F
Cervato B
Cervelli A
Cesarini G
Cetin SA
Chakraborty D
Chan J
Chan WY
Chapman JD
Chapon E
Chargeishvili B
Charlton DG
Chatterjee M
Chauhan C
Che Y
Chekanov S
Chekulaev SV
Chelkov GA
Chen A
Chen B
Chen B
Chen H
Chen H
Chen J
Chen J
Chen M
Chen S
Chen SJ
Chen X
Chen X
Chen Y
Cheng CL
Cheng HC
Cheong S
Cheplakov A
Cheremushkina E
Cherepanova E
Cherkaoui El Moursli R
Cheu E
Cheung K
Chevalier L
Chiarella V
Chiarelli G
Chiedde N
Chiodini G
Chisholm AS
Chitan A
Chitishvili M
Chizhov MV
Choi K
Chou Y
Chow EYS
Chu KL
Chu MC
Chu X
Chudoba J
Chwastowski JJ
Cieri D
Ciesla KM
Cindro V
Ciocio A
Cirotto F
Citron ZH
Citterio M
Ciubotaru DA
Clark A
Clark PJ
Clarry C
Clavijo Columbie JM
Clawson SE
Clement C
Clercx J
Coadou Y
Cobal M
Coccaro A
Coelho Barrue RF
Coelho Lopes De Sa R
Coelli S
Cole B
Collot J
Conde Muiño P
Connell MP
Connell SH
Conroy EI
Conventi F
Cooke HG
Cooper-Sarkar AM
Cordeiro Oudot Choi A
Corpe LD
Corradi M
Corriveau F
Cortes-Gonzalez A
Costa MJ
Costanza F
Costanzo D
Cote BM
Cowan G
Cranmer K
Cremonini D
Crescioli F
Cristinziani M
Cristoforetti M
Croft V
Crosby JE
Crosetti G
Crépé-Renaudin S
Cueto A
Cui H
Cui Z
Cunningham WR
Curcio F
Curran JR
Czodrowski P
Czurylo MM
Da Cunha Sargedas De Sousa MJ
Da Fonseca Pinto JV
Da Via C
Dabrowski W
Dado T
Dahbi S
Dai T
Dal Santo D
Dallapiccola C
Dam M
Damp J
Dandoy JR
Danninger M
Dao V
Darbo G
Das SJ
Dattola F
David C
Davidek T
Davis-Purcell B
Dawson I
Day-hall HA
De Asmundis R
De Biase N
De Castro S
De Groot N
de Jong P
De la Torre H
De Maria A
De Salvo A
De Sanctis U
De Santis F
De Santo A
De Vivie De Regie JB
De K
Dedovich DV
Degens J
Deiana AM
Del Corso F
Del Peso J
Del Rio F
Delagrange L
Deliot F
Delitzsch CM
Della Pietra M
Della Volpe D
Dell’Acqua A
Dell’Asta L
Delmastro M
Delsart PA
Demers S
Demichev M
Denisov SP
Derendarz D
Derue F
Dervan P
Desch K
Deutsch C
Di Bello FA
Di Ciaccio A
Di Ciaccio L
Di Domenico A
Di Donato C
Di Girolamo A
Di Gregorio G
Di Luca A
Di Micco B
Di Nardo R
Diamantopoulou M
Dias Do Vale T
Dias FA
Diaz Capriles FG
Diaz MA
Didenko M
Diehl EB
Diez Pardos C
Dimitriadi C
Dimitrievska A
Dingfelder J
Dinu I-M
Dittmeier SJ
Dittus F
Divisek M
Djama F
Djobava T
Doglioni C
Dohnalova A
Dolejsi J
Dolezal Z
Dona KM
Donadelli M
Dong B
Donini J
Dopke J
Doria A
Dos Santos Fernandes N
Dougan P
Dova MT
Doyle AT
Draguet MA
Dreyer E
Drivas-koulouris I
Drnevich M
Drozdova M
du Pree TA
Du D
Dubinin F
Dubovsky M
Duchovni E
Duckeck G
Ducu OA
Duda D
Dudarev A
Duden ER
Duflot L
Duminica I
Dumitriu AE
Dunford M
Dungs S
Dunne K
Duperrin A
Duran Yildiz H
Durglishvili A
Dwyer BL
Dyckes GI
Dyndal M
Dziedzic BS
Díez Cornell S
Dührssen M
Düren M
D’amen G
D’Amico V
D’Auria S
D’avanzo A
D’Eramo L
D’Onofrio A
D’Onofrio M
D’uffizi M
Earnshaw ZO
Eberwein GH
Eckerova B
Eggebrecht S
Egidio Purcino De Souza E
Ehrke LF
Eigen G
Einsweiler K
Ekelof T
Ekman PA
El Farkh S
El Ghazali Y
El Jarrari H
El Moussaouy A
Ellajosyula V
Ellert M
Ellinghaus F
Ellis N
Elmsheuser J
Elsawy M
Elsing M
Emeliyanov D
Enari Y
Ene I
Epari S
Erland PA
Errenst M
Escalier M
Escobar C
Etzion E
Evans G
Evans H
Evans LS
Ezhilov A
Ezzarqtouni S
Fabbri F
Fabbri L
Facini G
Fadeyev V
Fakhrutdinov RM
Fakoudis D
Falciano S
Falda Ulhoa Coelho LF
Falke PJ
Fallavollita F
Faltova J
Fan C
Fan Y
Fang Y
Fanti M
Faraj M
Farazpay Z
Farbin A
Farilla A
Farooque T
Farrington SM
Fassi F
Fassouliotis D
Faucci Giannelli M
Fawcett WJ
Fayard L
Federic P
Federicova P
Fedin OL
Feickert M
Feligioni L
Fellers DE
Feng C
Feng M
Feng Z
Fenton MJ
Ferencz L
Ferguson RAM
Fernandez Luengo SI
Fernandez Martinez P
Fernoux MJV
Ferrando J
Ferrari A
Ferrari P
Ferrari R
Ferrere D
Ferretti C
Fiedler F
Fiedler P
Filipčič A
Filmer EK
Filthaut F
Fiolhais MCN
Fiorini L
Fisher WC
Fitschen T
Fitzhugh PM
Fleck I
Fleischmann P
Flick T
Flores Castillo LR
Flores Sanz De Acedo L
Flores M
Follega FM
Fomin N
Foo JH
Formica A
Forti AC
Fortin E
Fortman AW
Foti MG
Fountas L
Fournier D
Fox H
Francavilla P
Francescato S
Franchellucci S
Franchini M
Franchino S
Francis D
Franco Lima V
Franco L
Franconi L
Franklin M
Frattari G
Freund WS
Frid YY
Friend J
Fritzsche N
Froch A
Froidevaux D
Frost JA
Fu Y
Fuenzalida Garrido S
Fujimoto M
Fung KY
Furtado De Simas Filho E
Furukawa M
Fuster J
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Gabrielli A
Gadow P
Gagliardi G
Gagnon LG
Galantzan S
Gallas EJ
Gallop BJ
Gan KK
Ganguly S
Gao Y
Garay Walls FM
Garcia Alonso A
Garcia Caffaro AG
Garcia B
Garcia-Sciveres M
García Navarro JE
García C
Gardner GL
Gardner RW
Garelli N
Garg D
Garg RB
Gargan JM
Garner CA
Garvey CM
Gaspar P
Gassmann VK
Gaudio G
Gautam V
Gauzzi P
Gavrilenko IL
Gavrilyuk A
Gay C
Gaycken G
Gazis EN
Geanta AA
Gee CM
Gekow A
Gemme C
Genest MH
Gentry AD
George S
George WF
Geralis T
Gessinger-Befurt P
Geyik ME
Ghani M
Ghorbanian K
Ghosal A
Ghosh A
Ghosh A
Giacobbe B
Giagu S
Giani T
Giannetti P
Giannini A
Gibson SM
Gignac M
Gil DT
Gilbert AK
Gilbert BJ
Gillberg D
Gilles G
Ginabat L
Gingrich DM
Giordani MP
Giraud PF
Giugliarelli G
Giugni D
Giuli F
Gkialas I
Gladilin LK
Glasman C
Gledhill GR
Glemža G
Glisic M
Gnesi I
Go Y
Goblirsch-Kolb M
Gocke B
Godin D
Gokturk B
Goldfarb S
Golling T
Gololo MGD
Golubkov D
Gombas JP
Gomes Da Silva G
Gomes A
Gomez Delegido AJ
Gonella L
Gongadze A
Gonnella F
Gonski JL
Gonzalez Lopez R
Gonzalez Renteria C
Gonzalez Rodrigues MV
Gonzalez Suarez R
Gonzalez-Sevilla S
González Andana RY
González de la Hoz S
Gonçalo R
Goossens L
Gorini B
Gorini E
Gorišek A
Gosart TC
Goshaw AT
Gostkin MI
Goswami S
Gottardo CA
Gotz SA
Gouighri M
Goumarre V
Goussiou AG
Govender N
Grabowska-Bold I
Graham K
Gramstad E
Grancagnolo S
Grant CM
Gravila PM
Gravili FG
Gray HM
Greco M
Grefe C
Gregor IM
Greif KT
Grenier P
Grewe SG
Grillo AA
Grimm K
Grinstein S
Grivaz J-F
Gross E
Grosse-Knetter J
Grundy JC
Guan L
Gubbels C
Guerrero Rojas JGR
Guerrieri G
Guescini F
Gugel R
Guhit JAM
Guida A
Guilloton E
Guindon S
Guo F
Guo J
Guo L
Guo Y
Gupta R
Gupta R
Gurbuz S
Gurdasani SS
Gustavino G
Guth M
Gutierrez Zagazeta LF
Gutierrez P
Gutsche M
Gutschow C
Gwenlan C
Gwilliam CB
Haaland ES
Haas A
Habedank M
Haber C
Hadavand HK
Hadef A
Hadzic S
Hagan AI
Hahn JJ
Haines EH
Haleem M
Haley J
Hall JJ
Hallewell GD
Halser L
Hamano K
Hamer M
Hamity GN
Hampshire EJ
Han J
Han K
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Han S
Han YF
Hanagaki K
Hance M
Hangal DA
Hanif H
Hank MD
Hansen JB
Hansen PH
Hara K
Harada D
Harenberg T
Harkusha S
Harris ML
Harris YT
Harrison J
Harrison NM
Harrison PF
Hartman NM
Hartmann NM
Hasegawa Y
Hassan S
Hauser R
Hawkes CM
Hawkings RJ
Hayashi Y
Hayashida S
Hayden D
Hayes C
Hayes RL
Hays CP
Hays JM
Hayward HS
He F
He M
He Y
He Y
He Y
Heatley NB
Hedberg V
Heggelund AL
Hehir ND
Heidegger C
Heidegger KK
Heidorn WD
Heilman J
Heim S
Heim T
Heinlein JG
Heinrich JJ
Heinrich L
Hejbal J
Held A
Hellesund S
Helling CM
Hellman S
Henderson RCW
Henkelmann L
Henriques Correia AM
Herde H
Hernández Jiménez Y
Herrmann LM
Herrmann T
Herten G
Hertenberger R
Hervas L
Hesping ME
Hessey NP
Hill E
Hillier SJ
Hinds JR
Hinterkeuser F
Hirose M
Hirose S
Hirschbuehl D
Hitchings TG
Hiti B
Hobbs J
Hobincu R
Hod N
Hodgkinson MC
Hodkinson BH
Hoecker A
Hofer DD
Hofer J
Holm T
Holzbock M
Hommels LBAH
Honan BP
Hong J
Hong TM
Hooberman BH
Hopkins WH
Horii Y
Hou S
Howard AS
Howarth J
Hoya J
Hrabovsky M
Hrynevich A
Hryn’ova T
Hsu PJ
Hsu S-C
Hu M
Hu Q
Huang S
Huang X
Huang Y
Huang Y
Huang Z
Hubacek Z
Huebner M
Huegging F
Huffman TB
Hugli CA
Huhtinen M
Huiberts SK
Hulsken R
Huseynov N
Huston J
Huth J
Hyneman R
Iacobucci G
Iakovidis G
Ibragimov I
Iconomidou-Fayard L
Iddon JP
Iengo P
Iguchi R
Iizawa T
Ikegami Y
Ilic N
Imam H
Ince Lezki M
Ingebretsen Carlson T
Introzzi G
Iodice M
Ippolito V
Irwin RK
Ishino M
Islam W
Issever C
Istin S
Ito H
Iuppa R
Ivina A
Izen JM
Izzo V
Jacka P
Jackson P
Jaeger BP
Jagfeld CS
Jain G
Jain P
Jakobs K
Jakoubek T
Jamieson J
Janas KW
Javurkova M
Jeanty L
Jejelava J
Jenni P
Jessiman CE
Jia C
Jia J
Jia X
Jia X
Jia Z
Jiang C
Jiggins S
Jimenez Pena J
Jin S
Jinaru A
Jinnouchi O
Johansson P
Johns KA
Johnson JW
Jones DM
Jones E
Jones P
Jones RWL
Jones TJ
Joos HL
Joshi R
Jovicevic J
Ju X
Junggeburth JJ
Junkermann T
Juste Rozas A
Juzek MK
Kabana S
Kaczmarska A
Kado M
Kagan H
Kagan M
Kahn A
Kahn A
Kahra C
Kaji T
Kajomovitz E
Kakati N
Kalaitzidou I
Kalderon CW
Kang NJ
Kar D
Karava K
Kareem MJ
Karentzos E
Karkanias I
Karkout O
Karpov SN
Karpova ZM
Kartvelishvili V
Karyukhin AN
Kasimi E
Katzy J
Kaur S
Kawade K
Kawale MP
Kawamoto C
Kawamoto T
Kay EF
Kaya FI
Kazakos S
Kazanin VF
Ke Y
Keaveney JM
Keeler R
Kehris GV
Keller JS
Kelly AS
Kempster JJ
Kennedy PD
Kepka O
Kerridge BP
Kersten S
Kerševan BP
Keszeghova L
Ketabchi Haghighat S
Khan RA
Khanov A
Kharlamov AG
Kharlamova T
Khoda EE
Kholodenko M
Khoo TJ
Khoriauli G
Khubua J
Khwaira YAR
Kibirige B
Kilgallon A
Kim DW
Kim YK
Kimura N
Kingston MK
Kirchhoff A
Kirfel C
Kirfel F
Kirk J
Kiryunin AE
Kitsaki C
Kivernyk O
Klassen M
Klein C
Klein L
Klein MH
Klein SB
Klein U
Klimek P
Klimentov A
Klioutchnikova T
Kluit P
Kluth S
Kneringer E
Knight TM
Knue A
Kobayashi R
Kobylianskii D
Koch SF
Kocian M
Kodyš P
Koeck DM
Koenig PT
Koffas T
Kolay O
Koletsou I
Komarek T
Kong AXY
Kono T
Konstantinidis N
Kontaxakis P
Konya B
Kopeliansky R
Koperny S
Korcyl K
Kordas K
Korn A
Korn S
Korolkov I
Korotkova N
Kortman B
Kortner O
Kortner S
Kostecka WH
Kostyukhin VV
Kotsokechagia A
Kotwal A
Koulouris A
Kourkoumeli-Charalampidi A
Kourkoumelis C
Kourlitis E
Kovanda O
Kowalewski R
Kozanecki W
Kozhin AS
Kramarenko VA
Kramberger G
Kramer P
Krasny MW
Krasznahorkay A
Kraus JW
Kremer JA
Kresse T
Kretzschmar J
Kreul K
Krieger P
Krishnamurthy S
Krivos M
Krizka K
Kroeninger K
Kroha H
Kroll J
Kroll J
Krowpman KS
Kruchonak U
Krumnack N
Kruse MC
Krüger H
Kuchinskaia O
Kuday S
Kuehn S
Kuesters R
Kuhl T
Kukhtin V
Kulchitsky Y
Kuleshov S
Kumar M
Kumari N
Kumari P
Kupco A
Kupfer T
Kupich A
Kuprash O
Kurashige H
Kurchaninov LL
Kurdysh O
Kurochkin YA
Kurova A
Kuze M
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Laatu LAO
Lacasta C
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Lafarge A
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Lambert JE
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Lancaster AN
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Landon MPJ
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Laporte JF
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Laudrain A
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Lawrence Z
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Lazzaroni M
Le Boulicaut EM
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Liberti B
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Lipniacka A
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Little JD
Liu B
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Lloyd SL
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Longarini I
Longo L
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Lopez Paz I
Lopez Solis A
Lorenzo Martinez N
Lory AM
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Lou X
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Lounis A
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Lu G
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Lubatti HJ
Luci C
Lucio Alves FL
Luehring F
Luise I
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Lund-Jensen B
Lundberg O
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Lyukova MM
Löschcke Centeno G
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Maccarrone G
MacDonald JC
Machado De Abreu Farias PC
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Minashvili IA
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Yeo BK
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Yue L
Zaazoua M
Zabinski B
Zaid E
Zak ZK
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Zakharchuk N
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Zamora Saa JA
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Zanzi D
Zaplatilek O
Zeitnitz C
Zeng H
Zeng JC
Zenger DT
Zenin O
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Zerradi S
Zerwas D
Zhai M
Zhang DF
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Zhang K
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Zhang Y
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Zhang Y
Zhang Z
Zhang Z
Zhao H
Zhao T
Zhao Y
Zhao Z
Zhao Z
Zhemchugov A
Zheng J
Zheng K
Zheng X
Zheng Z
Zhong D
Zhou B
Zhou H
Zhou N
Zhou Y
Zhou Y
Zhu CG
Zhu J
Zhu Y
Zhu Y
Zhuang X
Zhukov K
Zimine NI
Zinsser J
Ziolkowski M
Zoccoli A
Zoch K
Zorbas TG
Zormpa O
Zou W
Zwalinski L
Åkesson TPA
Öncel ÖO
Ženiš T
Živković L
Publication venue: Springer Nature
Publication date: 19/04/2024
Field of study

A combination of searches for new heavy spin-1 resonances decaying into different pairings of W, Z, or Higgs bosons, as well as directly into leptons or quarks, is presented. The data sample used corresponds to 139 fb−1 of proton-proton collisions at = 13 TeV collected during 2015–2018 with the ATLAS detector at the CERN Large Hadron Collider. Analyses selecting quark pairs (qq, bb, , and tb) or third-generation leptons (τν and ττ) are included in this kind of combination for the first time. A simplified model predicting a spin-1 heavy vector-boson triplet is used. Cross-section limits are set at the 95% confidence level and are compared with predictions for the benchmark model. These limits are also expressed in terms of constraints on couplings of the heavy vector-boson triplet to quarks, leptons, and the Higgs boson. The complementarity of the various analyses increases the sensitivity to new physics, and the resulting constraints are stronger than those from any individual analysis considered. The data exclude a heavy vector-boson triplet with mass below 5.8 TeV in a weakly coupled scenario, below 4.4 TeV in a strongly coupled scenario, and up to 1.5 TeV in the case of production via vector-boson fusion

University of Liverpool Repository

Queen Mary Research Online

Measurement and interpretation of same-sign W boson pair production in association with two jets in pp collisions at s = 13 TeV with the ATLAS detector

Author: Aad G
Abbott B
Abeling K
Abicht NJ
Abidi SH
Aboulhorma A
Abramowicz H
Abreu H
Abulaiti Y
Abusleme Hoffman AC
Acharya BS
Adam Bourdarios C
Adamczyk L
Adamek L
Addepalli SV
Addison MJ
Adelman J
Adiguzel A
Adye T
Affolder AA
Afik Y
Agaras MN
Agarwala J
Aggarwal A
Agheorghiesei C
Ahmad A
Ahmadov F
Ahmed WS
Ahuja S
Ai X
Aielli G
Aikot A
Ait Tamlihat M
Aitbenchikh B
Aizenberg I
Akbiyik M
Akimov AV
Akiyama D
Akolkar NN
Al Khoury K
Alberghi GL
Albert J
Albicocco P
Albouy GL
Alderweireldt S
Aleksa M
Aleksandrov IN
Alexa C
Alexopoulos T
Alfonsi F
Algren M
Alhroob M
Ali B
Ali HMJ
Ali S
Alibocus SW
Aliev M
Alimonti G
Alkakhi W
Allaire C
Allbrooke BMM
Allen JF
Allendes Flores CA
Allport PP
Aloisio A
Alonso F
Alpigiani C
Alvarez Estevez M
Alvarez Fernandez A
Alves Cardoso M
Alviggi MG
Aly M
Amaral Coutinho Y
Ambler A
Amelung C
Amerl M
Ames CG
Amidei D
Amor Dos Santos SP
Amos KR
Ananiev V
Anastopoulos C
Andeen T
Anders JK
Andrean SY
Andreazza A
Angelidakis S
Angerami A
Anisenkov AV
Annovi A
Antel C
Anthony MT
Antipov E
Antonelli M
Anulli F
Aoki M
Aoki T
Aparisi Pozo JA
Aparo MA
Aperio Bella L
Appelt C
Apyan A
Aranzabal N
Arcangeletti C
Arce ATH
Arena E
Arguin J-F
Argyropoulos S
Arling J-H
Arnaez O
Arnold H
Artoni G
Asada H
Asai K
Asai S
Asbah NA
Assamagan K
Astalos R
Atashi S
Atkin RJ
Atkinson M
Atmani H
Atmasiddha PA
Augsten K
Auricchio S
Auriol AD
Austrup VA
Avolio G
Axiotis K
Azuelos G
Babal D
Bachacou H
Bachas K
Bachiu A
Backman F
Badea A
Bagnaia P
Bahmani M
Bailey AJ
Bailey VR
Baines JT
Baines L
Bakalis C
Baker OK
Bakos E
Bakshi Gupta D
Balakrishnan V
Balasubramanian R
Baldin EM
Balek P
Ballabene E
Balli F
Baltes LM
Balunas WK
Balz J
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Bansal S
Barak L
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Barberio EL
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Barel MZ
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Celli F
Centonze MS
Cepaitis V
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Cerri A
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Cetin SA
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Charlton DG
Charman TP
Chatterjee M
Chauhan C
Chekanov S
Chekulaev SV
Chelkov GA
Chen A
Chen B
Chen B
Chen H
Chen H
Chen J
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Chen M
Chen S
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Chen X
Chen X
Chen Y
Cheng CL
Cheng HC
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Cheremushkina E
Cherepanova E
Cherkaoui El Moursli R
Cheu E
Cheung K
Chevalier L
Chiarella V
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Chiedde N
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Chisholm AS
Chitan A
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Chizhov MV
Choi K
Chomont AR
Chou Y
Chow EYS
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Chu KL
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Cieri D
Ciesla KM
Cindro V
Ciocio A
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Ciungu BM
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Clavijo Columbie JM
Clawson SE
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Da Cunha Sargedas De Sousa MJ
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Kostyukhin VV
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Little JD
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Lopez Solis A
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Lyukova MM
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Åkesson TPA
Öncel ÖO
Ženiš T
Živković L
Publication venue: Springer Nature
Publication date: 01/04/2024
Field of study

This paper presents the measurement of fducial and diferential cross sections for both the inclusive and electroweak production of a same-sign W-boson pair in association with two jets (W±W±jj) using 139 fb−1 of proton-proton collision data recorded at a centre-of-mass energy of √s = 13 TeV by the ATLAS detector at the Large Hadron Collider. The analysis is performed by selecting two same-charge leptons, electron or muon, and at least two jets with large invariant mass and a large rapidity diference. The measured fducial cross sections for electroweak and inclusive W±W±jj production are 2.92 ± 0.22 (stat.) ± 0.19 (syst.)fb and 3.38±0.22 (stat.)±0.19 (syst.)fb, respectively, in agreement with Standard Model predictions. The measurements are used to constrain anomalous quartic gauge couplings by extracting 95% confdence level intervals on dimension-8 operators. A search for doubly charged Higgs bosons H±± that are produced in vector-boson fusion processes and decay into a same-sign W boson pair is performed. The largest deviation from the Standard Model occurs for an H±± mass near 450 GeV, with a global signifcance of 2.5 standard deviations

University of Liverpool Repository

Queen Mary Research Online

White Rose Research Online

Guidelines for the use and interpretation of assays for monitoring autophagy (4th edition)1.

Author: Abdel-Aziz AK
Abdelfatah S
Abdellatif M
Abdoli A
Abel S
Abeliovich H
Abildgaard MH
Abudu YP
Acevedo-Arozena A
Adamopoulos IE
Adeli K
Adolph TE
Adornetto A
Aflaki E
Agam G
Agarwal A
Aggarwal BB
Agnello M
Agostinis P
Agrewala JN
Agrotis A
Aguilar PV
Ahmad ST
Ahmed ZM
Ahumada-Castro U
Aits S
Aizawa S
Akkoc Y
Akoumianaki T
Akpinar HA
Al-Abd AM
Al-Akra L
Al-Gharaibeh A
Alaoui-Jamali MA
Alberti S
Alcocer-Gómez E
Alessandri C
Ali M
Alim Al-Bari MA
Aliwaini S
Alizadeh J
Almacellas E
Almasan A
Alonso A
Alonso GD
Altan-Bonnet N
Altieri DC
Alves da Costa C
Alves S
Alzaharna MM
Amadio M
Amantini C
Amaral C
Ambrosio S
Amer AO
Ammanathan V
An Z
Andersen SU
Andrabi SA
Andrade-Silva M
Andres AM
Angelini S
Ann D
Anozie UC
Ansari MY
Antas P
Antebi A
Antón Z
Anwar T
Apetoh L
Apostolova N
Araki T
Araki Y
Arasaki K
Araya J
Araújo WL
Arden C
Arguelles S
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Arikkath J
Arimoto H
Ariosa AR
Armstrong-James D
Arnauné-Pelloquin L
Aroca A
Arroyo DS
Arsov I
Artero R
Arévalo M-A
Asaro DML
Aschner M
Ashrafizadeh M
Ashur-Fabian O
Atanasov AG
Au AK
Auberger P
Auner HW
Aurelian L
Autelli R
Avagliano L
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Aveleira CA
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Hooper LV
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Huber TB
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Johnson GVW
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Karamouzis MV
Karim MR
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Kenchappa CS
Kenific CM
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Keulers TG
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Khandelwal VKM
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Khobrekar NV
Khuansuwan S
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Killackey SA
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Kinsey CG
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Kirshenbaum LA
Kiselev SL
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Kocaturk NM
Koch I
Koch JC
Koenig U
Koh YH
Kohlwein SD
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Kopp BT
Korcsmaros T
Korkmaz G
Korolchuk VI
Korsnes MS
Koskela A
Kota J
Kotake Y
Kotler ML
Kou Y
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Koustas E
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Kovács T
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Krasnodembskaya AD
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Kunnumakkara AB
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Kutlu O
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Leduc-Gaudet J-P
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Ortega-Villaizan MDM
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Papademetrio DL
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Schulze RJ
Schwamborn JC
Schwarten M
Schüller C
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Scialo F
Sciarretta S
Scott MJ
Scotto KW
Scovassi AI
Scrima A
Scrivo A
Sebastian D
Sebti S
Sedej S
Segatori L
Segev N
Seglen PO
Seiliez I
Seki E
Selleck SB
Sellke FW
Selsby JT
Sendtner M
Senturk S
Seranova E
Sergi C
Serra-Moreno R
Sesaki H
Settembre C
Setty SRG
Sgarbi G
Sha O
Shacka JJ
Shah JA
Shang D
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Sharbati S
Sharkey LM
Sharma D
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Shen H
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Shieh J-J
Shimada Y
Shimizu S
Shimozawa M
Shintani T
Shoemaker CJ
Shojaei S
Shoji I
Shravage BV
Shridhar V
Shu C-W
Shu H-B
Shui K
Shukla AK
Shutt TE
Sica V
Siddiqui A
Sierra A
Sierra-Torre V
Signorelli S
Sil P
Silva BJDA
Silva JD
Silva-Pavez E
Silvente-Poirot S
Simmonds RE
Simon AK
Simon H-U
Simons M
Singh A
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Sok SPM
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Soria LR
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Soukas AA
Soukup S-F
Sousa D
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Spagnuolo PA
Spector SA
Srinivas Bharath MM
St Clair D
Stagni V
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Sze SCW
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Tabęcka-Łonczynska A
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Tai H
Tait SWG
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Tam C
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Tang D
Tang J
Tang T-S
Tanida I
Tao Z
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Tatenhorst L
Tavernarakis N
Taylor A
Taylor GA
Taylor JM
Tchetina E
Tee AR
Tegeder I
Teis D
Teixeira N
Teixeira-Clerc F
Tekirdag KA
Tencomnao T
Tenreiro S
Tepikin AV
Testillano PS
Tettamanti G
Tharaux P-L
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Thekkinghat AA
Thellung S
Thinwa JW
Thirumalaikumar VP
Thomas SM
Thomes PG
Thorburn A
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Titorenko VI
Todi SV
Todorova K
Toivonen JM
Tomaipitinca L
Tomar D
Tomas-Zapico C
Tomić S
Tong BC-K
Tong C
Tong C-K
Tong X
Tooze SA
Torgersen ML
Torii S
Torres-López L
Torriglia A
Towers CG
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Toyokuni S
Trajkovic V
Tramontano D
Tran Q-G
Travassos LH
Trelford CB
Tremel S
Trougakos IP
Tsao BP
Tschan MP
Tse H-F
Tse TF
Tsugawa H
Tsvetkov AS
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Tumtas Y
Turcotte S
Turk B
Turk V
Turner BJ
Tuxworth RI
Tuñón MJ
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Tyutereva EV
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Ulasov IV
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Vega-Naredo I
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Velasco G
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Velotti F
Velázquez AP
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Vergne I
Verkade P
Verma M
Verstreken P
Vervliet T
Vervoorts J
Vessoni AT
Victor VM
Vidal M
Vidoni C
Vieira OV
Vierstra RD
Viganó S
Vihinen H
Vijayan V
Vila M
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Villalba JM
Villalobo A
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Villarroya F
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Vincent O
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Viscomi MT
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Vitale I
Vocadlo DJ
Voitsekhovskaja OV
Volonté C
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Von Haefen C
Vooijs MA
Voos W
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Wade-Martins R
Waguri S
Waite KA
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Walker DW
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Walter J
Wandosell FG
Wang B
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Wang D
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Wang G
Wang H
Wang H
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Wang H-G
Wang J
Wang J
Wang J
Wang J
Wang K
Wang L
Wang L
Wang M
Wang MH
Wang N
Wang P
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Wang Q
Wang QA
Wang QJ
Wang QK
Wang W
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Wang X
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Wang Z
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Warnsmann V
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Wegrzyn G
Wehman AM
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Wei Y
Weiergräber OH
Weihl CC
Weindl G
Weiskirchen R
Wells A
Wen RH
Wen X
Werner A
Weykopf B
Wheatley SP
Whitton JL
Whitworth AJ
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Wildenberg ME
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Wu A-G
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Xavier RJ
Xia H
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Xiang G
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Xiang M
Xiang W
Xiao B
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Xiao H-T
Xiao J
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Xiao Y
Xie B
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Xilouri M
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Zhang M
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Zhang W
Zhang X
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Zhang X-W
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Zhang Y
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Zhang Y
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Zhang Y-D
Zhang Y-Y
Zhang Z
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Zhao H
Zhao L
Zhao S
Zhao T
Zhao X-F
Zhao Y
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Zheng G
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Zhivotovsky B
Zhong Q
Zhou A
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Zhou K
Zhou R
Zhou X-J
Zhou Y
Zhou Y
Zhou Y
Zhou Z
Zhou Z-Y
Zhu B
Zhu C
Zhu G-Q
Zhu H
Zhu H
Zhu H
Zhu W-G
Zhu Y
Zhu Y
Zhuang H
Zhuang X
Zientara-Rytter K
Zimmermann CM
Ziviani E
Zoladek T
Zong W-X
Zorov DB
Zorzano A
Zou W
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Zuryn S
Zwerschke W
Álvarez ÉMC
Ávalos Y
Önal G
Üstün S
Čolić M
Đokić J
Žerovnik E
Publication venue: 'Informa UK Limited'
Publication date: 01/01/2021
Field of study

In 2008, we published the first set of guidelines for standardizing research in autophagy. Since then, this topic has received increasing attention, and many scientists have entered the field. Our knowledge base and relevant new technologies have also been expanding. Thus, it is important to formulate on a regular basis updated guidelines for monitoring autophagy in different organisms. Despite numerous reviews, there continues to be confusion regarding acceptable methods to evaluate autophagy, especially in multicellular eukaryotes. Here, we present a set of guidelines for investigators to select and interpret methods to examine autophagy and related processes, and for reviewers to provide realistic and reasonable critiques of reports that are focused on these processes. These guidelines are not meant to be a dogmatic set of rules, because the appropriateness of any assay largely depends on the question being asked and the system being used. Moreover, no individual assay is perfect for every situation, calling for the use of multiple techniques to properly monitor autophagy in each experimental setting. Finally, several core components of the autophagy machinery have been implicated in distinct autophagic processes (canonical and noncanonical autophagy), implying that genetic approaches to block autophagy should rely on targeting two or more autophagy-related genes that ideally participate in distinct steps of the pathway. Along similar lines, because multiple proteins involved in autophagy also regulate other cellular pathways including apoptosis, not all of them can be used as a specific marker for bona fide autophagic responses. Here, we critically discuss current methods of assessing autophagy and the information they can, or cannot, provide. Our ultimate goal is to encourage intellectual and technical innovation in the field

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