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375 research outputs found

New approaches to measuring anthelminthic drug efficacy: parasitological responses of childhood schistosome infections to treatment with praziquantel

Author: A Danso-Appiah
A Fenwick
A Montresor
A Vidyashankar
AC Gelman
AE Butterworth
AL Bustinduy
Alexandra U. Scherrer
AU Scherrer
B Levecke
BM Bolker
CH King
Charles H. King
CJL Murray
CL Black
D Alonso
D Bates
F Thiongo
G Raso
Giovanna Raso
GR Olds
IM Silva
J Cabaret
J Modha
J Smith
J Utzinger
J Utzinger
J Utzinger
J. Russell Stothard
JA Hanley
JC Sousa-Figueiredo
JD Hadfield
Jean T. Coulibaly
José Carlos Sousa-Figueiredo
JP Webster
JT Coulibaly
Jürg Utzinger
K Stete
Katarina Stete
M Albonico
M Booth
M Ismail
M Nielsen
M Reddy
M Walker
Maria-Gloria Basáñez
Martin Walker
ME Mejía
MEJ Woolhouse
MG Basáñez
MJ Bockarie
MJ Doenhoff
MJ Doenhoff
P Andrews
P Fallon
PH Lamberton
Piero L. Olliaro
PJ Brindley
PJ Diggle
PJ Hotez
PL Olliaro
PNM Mwinzi
R Core Team
S Anayi
SD Melman
SJ Vlas de
SN Lahiri
SV Subramanian
Tarub S. Mabud
TW Jia
U Halekoh
W Harnett
W Wang
World Health Organization
World Health Organization
World Health Organization
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 19/11/2015
Field of study

By 2020, the global health community aims to control and eliminate human helminthiases, including schistosomiasis in selected African countries, principally by preventive chemotherapy (PCT) through mass drug administration (MDA) of anthelminthics. Quantitative monitoring of anthelminthic responses is crucial for promptly detecting changes in efficacy, potentially indicative of emerging drug resistance. Statistical models offer a powerful means to delineate and compare efficacy among individuals, among groups of individuals and among populations.; We illustrate a variety of statistical frameworks that offer different levels of inference by analysing data from nine previous studies on egg counts collected from African children before and after administration of praziquantel.; We quantify responses to praziquantel as egg reduction rates (ERRs), using different frameworks to estimate ERRs among population strata, as average responses, and within strata, as individual responses. We compare our model-based average ERRs to corresponding model-free estimates, using as reference the World Health Organization (WHO) 90 % threshold of optimal efficacy. We estimate distributions of individual responses and summarize the variation among these responses as the fraction of ERRs falling below the WHO threshold.; Generic models for evaluating responses to anthelminthics deepen our understanding of variation among populations, sub-populations and individuals. We discuss the future application of statistical modelling approaches for monitoring and evaluation of PCT programmes targeting human helminthiases in the context of the WHO 2020 control and elimination goals

LSTM Research Portal

Crossref

Springer - Publisher Connector

edoc

PubMed Central

Spiral - Imperial College Digital Repository

A Novel G Protein-Coupled Receptor of Schistosoma mansoni (SmGPR-3) Is Activated by Dopamine and Is Widely Expressed in the Nervous System

Author: A Maule
A Taman
A Taman
AB Kohn
AC Fontana
AK Pani
Amira Taman
AS Taft
B Roth
BI Joffe
D Gold
D Massotte
EY Chien
F El-Shehabi
F El-Shehabi
F Hamdan
F Lewis
FF Hamdan
FF Hamdan
FF Hamdan
Fouad El-Shehabi
G Gianutsos
G Liapakis
GR Mair
GR Mair
JA Ballesteros
JM Beaulieu
K Nishimura
K Tamura
KS Eriksson
L Holden-Dye
L Shi
Lorena S. Moali
M Berriman
M-H Abdulla
MB Larsen
MJ Doenhoff
MJ Kimber
MKS Gustafsson
MKS Gustafsson
MYS Kalani
N Patocka
N Takeda
Nelly El-Sakkary
P Laduron
P Ribeiro
P Ribeiro
Paula Ribeiro
PG Fallon
R Del Carmine
RA Pax
S Suo
S William
Serap Aksoy
SMC Robb
TK Tomosky
TN Mellin
V Cherezov
Y Orido
Z Wang
Publication venue: Public Library of Science
Publication date: 28/02/2012
Field of study

Schistosomes have a well developed nervous system that coordinates virtually every activity of the parasite and therefore is considered to be a promising target for chemotherapeutic intervention. Neurotransmitter receptors, in particular those involved in neuromuscular control, are proven drug targets in other helminths but very few of these receptors have been identified in schistosomes and little is known about their roles in the biology of the worm. Here we describe a novel Schistosoma mansoni G protein-coupled receptor (named SmGPR-3) that was cloned, expressed heterologously and shown to be activated by dopamine, a well established neurotransmitter of the schistosome nervous system. SmGPR-3 belongs to a new clade of “orphan” amine-like receptors that exist in schistosomes but not the mammalian host. Further analysis of the recombinant protein showed that SmGPR-3 can also be activated by other catecholamines, including the dopamine metabolite, epinine, and it has an unusual antagonist profile when compared to mammalian receptors. Confocal immunofluorescence experiments using a specific peptide antibody showed that SmGPR-3 is abundantly expressed in the nervous system of schistosomes, particularly in the main nerve cords and the peripheral innervation of the body wall muscles. In addition, we show that dopamine, epinine and other dopaminergic agents have strong effects on the motility of larval schistosomes in culture. Together, the results suggest that SmGPR-3 is an important neuronal receptor and is probably involved in the control of motor activity in schistosomes. We have conducted a first analysis of the structure of SmGPR-3 by means of homology modeling and virtual ligand-docking simulations. This investigation has identified potentially important differences between SmGPR-3 and host dopamine receptors that could be exploited to develop new, parasite-selective anti-schistosomal drugs

CiteSeerX

Public Library of Science (PLOS)

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PubMed Central

The Francis Crick Institute

Effects of Hormone Agonists on Sf9 Cells, Proliferation and Cell Cycle Arrest

Methoxyfenozide and methoprene are two insecticides that mimic the action of the main hormones involved in the control of insect growth and development, 20-hydroxyecdysone and juvenile hormone. We investigated their effect on the Spodoptera frugiperda Sf9 cell line. Methoxyfenozide was more toxic than methoprene in cell viability tests and more potent in the inhibition of cellular proliferation. Cell growth arrest occurred in the G2/M phase after a methoprene treatment and more modestly in G1 after methoxyfenozide treatment. Microarray experiments and real-time quantitative PCR to follow the expression of nuclear receptors ultraspiracle and ecdysone receptor were performed to understand the molecular action of these hormone agonists. Twenty-six genes were differentially expressed after methoxyfenozide treatment and 55 genes after methoprene treatment with no gene in common between the two treatments. Our results suggest two different signalling pathways in Sf9 cells

Public Library of Science (PLOS)

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PubMed Central

ProdInra

Is increased time to diagnosis and treatment in symptomatic cancer associated with poorer outcomes?:Systematic review

Author: A Akdas
A Annakkaya
A Brazda
A Currie
A Eastman
A Ferrari
A Hendry
A Maguire
A Mohan
A Saithna
A Van Hout
A Yilmaz
A Zafar
AE Obermair
AF Balasa
AG Goddard
AG Singal
AHP Loh
AJ Ziliotto
AR Jensen
AWM Lee
B Cassileth
B France
B Valentin-Lopez
B Williams
BA Grotenhuis
BK Hollenbeck
BS Lim
BT Rougraff
C Arvanitakis
C Cerdan-Santacruz
C Chilvers
C Renzi
C Tomlinson
C Wilkinson
CC Kariyawasan
CD Lethaby
CL Roland
CM Erwenne
CM Nagle
CR Friese
CR Friese
D Bell
D Moher
D O’Brien
D Sharpe
D Sidler
D Sundi
D Weller
DA Raptis
DF Fossa
DG Altman
DM Tromp
DM Wallace
E Christensen
E D Mitchell
E Ermiah
E Fernandez
E Huyghe
E Launay
E Radzikowska
E Salomaa
EC Halperin
EC Pirog
EC Smith
EM Smith
ET Warner
F Liedberg
FJ Gonzalez-Barcala
G Bacci
G Bacci
G Lurie
G Maconi
G Myrdal
G Ramsay
G Rubin
GA Vernham
GJ Bosl
GP Wright
GR Prout
GR Sue
H Scher
H Singh
H Teppo
H Teppo
H Teppo
H Teppo
ID Miziara
IG Martin
J Caudell
J Crawford
J Emery
J Emery
J Fallon-Ferguson
J Goy
J Menczer
J Menczer
J Menczer
J Norum
J Seoane
J Seoane
J Wang
J Wildt
JA Hayden
JA Hayden
JE Krige
JF Brasme
JF Brasme
JF Brasme
JK Olsson
JL Wagner
JM McLaughlin
JS Terhaar sive Droste
JW Moul
JYK Yang
K Dieckmann
K Kukal
K Shaw
K Skaug
KI Wishnow
KM Robinson
KP Guzman-Laura
L Butros
L Elit
L Sheng
L Temoshok
LC Loh
LD Wurtz
LJ Esserman
M Alam
M Egger
M Gort
M Harding
M Hendry
M L Tørring
M Montella
M Mujar
M Pickett
M Pitchers
M Prabhu
M Ramos
M Ramos
M Sun
M Waldert
MA Richards
MA Richards
MA Richards
MA Richards
MA Wallach
MC Gulliford
MC McGurk
Medical Research Council Work Party Testicular Tumours
MH Schmid-Wendtner
MK Gould
ML Tørring
ML Tørring
ML Tørring
MM Kameda-Smith
MM Lins
MP Napier
MR Thompson
MR Thompson
MT Redaniel
N Al-Rajhi
N Jacobi
N Stuart
N U Din
N Williams
NM Fahmy
O Alho
O Hansen
P Allison
P Baade
P Brocken
P Carli
P Foulc
P Helsing
P Koivunen
P Murchie
P Tharmanathan
PG Gobbi
PJ Meffan
PM Simpson
PR Hanson
R D Neal
R Diaconescu
R Korets
R Lewis
RD Neal
RD Neal
RG Fruchter
RK Marwaha
RK Marwaha
RV Sethi
S Bertoli
S Cotton
S Crawford
S Deng
S Franceschi
S Holmang
S Kumar
S Metzger
S Mommsen
S Pita-Fernandez
S Toth-Fejel
SE Scott
SK Wahl
SL Pruitt
SM Ware
SR McLean
T Ho
T Murai
T Nakamura
T Rai
T Umezu
TC Windham
TK Haugstvedt
U Macleod
W Hamilton
W Ruka
X Brouha
X Brouha
X Brouha
Y Tokuda
YH Kim
YH Yun
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 03/03/2015
Field of study

background: It is unclear whether more timely cancer diagnosis brings favourable outcomes, with much of the previous evidence, in some cancers, being equivocal. We set out to determine whether there is an association between time to diagnosis, treatment and clinical outcomes, across all cancers for symptomatic presentations. methods: Systematic review of the literature and narrative synthesis. results: We included 177 articles reporting 209 studies. These studies varied in study design, the time intervals assessed and the outcomes reported. Study quality was variable, with a small number of higher-quality studies. Heterogeneity precluded definitive findings. The cancers with more reports of an association between shorter times to diagnosis and more favourable outcomes were breast, colorectal, head and neck, testicular and melanoma. conclusions: This is the first review encompassing many cancer types, and we have demonstrated those cancers in which more evidence of an association between shorter times to diagnosis and more favourable outcomes exists, and where it is lacking. We believe that it is reasonable to assume that efforts to expedite the diagnosis of symptomatic cancer are likely to have benefits for patients in terms of improved survival, earlier-stage diagnosis and improved quality of life, although these benefits vary between cancers

University of Liverpool Repository

Repository@Hull - Worktribe

Crossref

PubMed Central

Open Research Exeter

Bangor University Research Portal

University of Melbourne Institutional Repository

Effect of garlic on cardiovascular disorders: a review

Author: A Bordia
A Bordia
A Bordia
A Bordia
A Elkayam
A Fugh-Berman
A Keys
A Rabinkov
A Rashid
A Sendl
AA Qureshi
AD Kaye
AE Falleroni
AG Chanderkar
AG Ciplea
AK Banerjee
AK Bordia
AK Bordia
AK Bordia
AK Bordia
AK Jain
AN Makheja
AN Orekhov
AY Sial
B Rietz
B Rodger
BC Mathew
BE Burnham
BS Kendler
BW McCrindle
C Borek
C Egen-Schwind
C Legnani
C Luley
C Silagy
C Stevinson
CA Silagy
CD Gardner
CG Sheela
CG Sheela
CJ Schwartz
CR Rajasree
CV Pantoja
D Abramovitz
D Farva
D Papageogiou
DB Foushee
DJ Boullin
DJ Byrne
DK Granner
E Beck
E Betz
E Block
EM Jung
F Damru
F el-Sabban
F el-Sabban
FG McMahon
FK Konig
G Lewin
G Li
G Vorberg
GL Piotrowski'ail en
GR Kumar
GS Sainani
GS Sainani
H Gallwitz
H Isensee
H Kiesewetter
H Kiesewetter
H Kiesewetter
H Wagner
HA Neil
HK Berthold
HP Koch
HR Superko
HS Lau Benjamin
J Harenberg
J Imai
J Lutomski
J Morris
J Ruffin
JH Campbell
JJ Petry
JK Mand
JL Efendy
JL Isaacsohn
JS Munday
JY Vanderhock
K Breithaupt-Grogler
K Breithaupt-Grogler
K Rahman
K Ryu
KC Srivastava
KC Srivastava
KC Srivsatava
KD Rose
KK Al-Qattan
KT Augusti
KT Augusti
KT Augusti
L Chen
LA Simons
LD Lawson
LY Sheen
LY Sheen
M Ali
M Ali
M Ali
M Ali
M Ali
M Brandle
M Leoper
M Steiner
M Steiner
M Steiner
M Thomson
MB Aqel
MB Fallon
MLW Chang
MP Jamaluddin
MS Chi
MS Chi
N Martin
N Martin
OC Ohaeri
PK Joseph
PT Mathew
PW Woodward
R Apitz-Castro
R Apitz-Castro
R Apitz-Castro
R Apitz-Castro
R Apitz-Castro
R Gebhardt
R Kojima
RC Arora
RC Arora
RC Jain
RC Jain
RC Jain
RC Jain
RR Samson
RS Rivlin
S Kasuga
S Kim-Park
S Moyers
S Mukherjee
S Nakagawa
S Patumraj
S Warshafsky
S Ziaei
SA Eming
SA Mirhadi
Sanjay K Banerjee
SK Banerjee
SK Banerjee
SK Banerjee
SK Chutani
SK Swanston-Flatt
SK Tongia
Subir K Maulik
T Ariga
T Das
T Yamasaki
V Petkov
V Schulz
VP Dixit
VS Kamanna
VS Kamanna
W Auer
W Auer
W Qidwai
W Zimmermann
WH Sunter
WJ Harfenist
WVD Laurence
XH Zhang
Yeh Yu-Yan
Z Geng
Z Wei
ZA Malik
Zheziang Institute of Traditional Chinese Medicine
Publication venue: BioMed Central
Publication date: 01/01/2002
Field of study

Garlic and its preparations have been widely recognized as agents for prevention and treatment of cardiovascular and other metabolic diseases, atherosclerosis, hyperlipidemia, thrombosis, hypertension and diabetes. Effectiveness of garlic in cardiovascular diseases was more encouraging in experimental studies, which prompted several clinical trials. Though many clinical trials showed a positive effect of garlic on almost all cardiovascular conditions mentioned above, however a number of negative studies have recently cast doubt on the efficary of garlic specially its cholesterol lowering effect of garlic. It is a great challenge for scientists all over the world to make a proper use of garlic and enjoy its maximum beneficial effect as it is the cheapest way to prevent cardiovascular disease. This review has attempted to make a bridge the gap between experimental and clinical study and to discuss the possible mechanisms of such therapeutic actions of garlic

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The insect pathogenic bacterium Xenorhabdus innexi has attenuated virulence in multiple insect model hosts yet encodes a potent mosquitocidal toxin

Author: A Bhasin
A Castagnola
A Hachani
A Jamet
Adler R. Dillman
AP Jackson
AR Dillman
AR Dillman
BT Ho
C Carrillo
C Condon
CJ Song
D Blackburn
D Lu
D Toubarro
D Vallenet
Dariush T. Aghai
DD Bondage
DJ Fallon
DK Mitani
DR Sugar
E Bonifassi
E Boszormenyi
E Hussa
EE Herbert
EI Vivas
Erin J. Mans
F Bashey
F Jacob-Dubuisson
F Vigneux
FR Cianfanelli
G Bisch
GB Dunphy
GFA White
GR Richards
H Zhang
HB Bode
HE Gavin
Heidi Goodrich-Blair
I Antic
IH Kim
Il-Hwan Kim
J Alcoforado Diniz
J Brillard
J Castresana
J Masschelein
J Masschelein
J Sambrook
J Xu
JC Ensign
JC Ogier
JC Ogier
JC Whitney
JD Mougous
JE Hellberg
Jean-Claude Ogier
Jerald C. Ensign
JL Veesenmeyer
JM Chaston
JM Crawford
JM Hawdon
JS Rosa
K Blin
K Das
K Krebs
K Lengyel
K Nikolakakis
K Nikolouli
Kai Hillman
KB Nguyen
KB Nguyen
KB Nguyen
KE Murfin
KE Murfin
KJ Satchell
KN Cowles
L Cerenius
L Du
LK Assie
LN Pham
LT Svensson
M Biancucci
M Röttig
M Sicard
M Sicard
M Wilcke
MA Beresky
MC Hunt
Michael P. Kozuch
MM Benning
MM Lee
N Balasubramanian
N Galtier
N Waterfield
N Waterfield
N Waterfield
NE Boemare
OS da Silva
P Kumari
P Singh
P Tailliez
PS Grewal
S Seo
SA Nadler
SE Spiridonov
SF Altschul
SJ Pidot
SK Aoki
SK Aoki
SK Aoki
SK Straus
Sophie Gaudriault
SS Orchard
Sudarshan K. Aryal
SW Fuchs
SW Fuchs
T Asai
Terra J. Mauer
TG Andreadis
TK Teal
TP Bonner
V Converse
VL Challinor
Walter G. Goodman
Y Bao
Y Wang
Y Zhang
Z Gyorfy
ZC Ruhe
Ángel M. Casanova-Torres
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

The impact of viral mutations on recognition by SARS-CoV-2 specific T cells.

Author: Aanensen DM
Abudahab K
Adams A
Adams H
Adeniji K
Afifi S
Aggarwal D
Agranoff D
Agwuh K
Ahmad SSY
Ahmed KA
Aigrain L
Ail D
Alcolea-Medina A
Aldera EL
Alegria A
Alex B
Alikhan N-F
Allara E
Allen S
Amato R
Andrikopoulos P
Angus B
Angyal A
Annett T
Aplin S
Ariani CV
Armstrong JA
Asad H
Ash A
Ashfield P
Ashford F
Ashish A
Ashworth M
Asiimwe IG
Atkinson D
Atkinson L
Attwood SW
Auckland C
Aydin A
Bach B
Baillie JK
Baker DJ
Baker P
Bakshi S
Balcazar CE
Ball J
Barclay WS
Bari S
Barlow G
Barlow SL
Barnass S
Barrett JC
Barrett N
Barrow M
Barton E
Bashton M
Bassett AR
Bassford C
Basude S
Batra R
Baxter C
Baxter D
Bayzid N
Beadsworth M
Beaver C
Beckett AH
Beckwith SM
Bedford L
Beer R
Beggs A
Bellis KL
Bernatoniene J
Berridge J
Berry C
Berry L
Bertolusso B
Best A
Best N
Betteridge E
Bibby D
Bicknell K
Binns D
Birchley A
Bird PW
Bishop C
Blacow R
Blakey V
Blane B
Bogaert D
Bolt F
Bonfield J
Bonner S
Bonsall D
Booth L
Boswell T
Bosworth A
Bothma P
Bourgeois Y
Boyd O
Bradley DT
Breen C
Brennan B
Bresner C
Breuer J
Bridgett S
Brittain-Long R
Bronner IF
Brooks E
Broos A
Brown JR
Brown R
Bucca G
Buchan SL
Buck D
Bull M
Bullock K
Bulteel N
Burden T
Burns PJ
Burtenshaw A
Burton-Fanning S
Byaruhanga T
Byott M
Campbell S
Carabelli AM
Cargill JS
Carlile M
Carlucci N
Carracedo AD
Carson G
Caruth V
Carvalho SF
Casey A
Cass E
Castigador A
Catalan J
Catterall BWA
Chadwick D
Chadwick D
Chalker V
Chaloner NJ
Chambler D
Chand M
Chand M
Chappell JG
Charalampous T
Chatterton W
Chaudhry Y
Chechi K
Chee N
Child J
Chukkambotla S
Churcher CM
Clark G
Clark JJ
Clark T
Clarke EA
Clarke P
Clohisey S
Cogger BJ
Cole K
Cole S
Cole S
Collini P
Collins J
Colquhoun R
Connor M
Connor TR
Cook KF
Cooke GS
Coombes J
Cooper L
Corden S
Cormie C
Correia GDS
Cortes N
Cosgrove C
Cotic M
Cotton S
Cottrell S
Coupland L
Cox A
Cox H
Cox M
Craine N
Crawford L
Cross A
Crown MR
Crudgington D
Cumley N
Cupitt J
Curran MD
Curran T
Cutino-Moguel M-T
da Silva Filipe A
da Silva Filipe A
Dabrera G
Dalton J
Darby AC
Dark P
Davidson RK
Davies A
Davies RM
Davis C
Davis T
Dawson C
de Angelis D
De Lacy E
de Oliveira Martins L
de Silva TI
Debebe J
Denton-Smith R
Dervisevic S
Dervisevic S
Dewar R
Dey J
Dias J
Dincarslan O
Dobie D
Docherty AB
Donegan C
Dong D
Dong T
Donnison P
Donohue C
Dorman MJ
Douthwaite S
Downing F
Driscoll M
Drummond A
du Plessis L
Duckworth N
Dumas M-E
Dunachie S
Dunn C
Dunning J
DuRand I
Durham J
Dushianthan A
Dyer P
Dyer T
Eastick K
Easton LJ
Eccles R
Edgeworth J
Edwards S
El Bouzidi K
Eldirdiri S
Ellaby N
Elliott A
Elliott S
Eltringham G
Ensell L
Erkiert MJ
Essex S
Evans A
Evans C
Evans C
Evans JM
Everson W
Eziefula C
Fairley DJ
Fallon K
Fanaie A
Farr BW
Fearn C
Fegan C
Feltwell T
Ferguson L
Fina L
Finch L
Finn A
Fisher LWS
Flaherty L
Flaviani F
Fleming VM
Fletcher T
Forrest S
Foster T
Foster-Nyarko E
Foulkes BH
Foulser L
Fragakis M
Frampton D
Francois S
Fraser C
Freeman TM
Fryer H
Fuchs M
Fuller W
Fullerton D
Gajee K
Galai K
Gallagher A
Gallagher E
Gallagher MD
Gallis M
Gamble C
Garcia-Dorival I
Garg A
Garg S
Garg S
Gaskin A
Gatica-Wilcox B
Geidelberg L
Gemmell M
Georgana I
George RP
Gifford L
Gilbert L
Girgis ST
Girvan M
Gkrania-Klotsas E
Glaysher S
Godden J
Goldsmith A
Goldstein EJ
Golubchik T
Gomes AN
Gonçalves S
Goodfellow IG
Goodwin S
Goudarzi S
Gourtovaia M
Graham C
Graham C
Graham L
Grant PR
Green A
Green CA
Green LR
Greenaway J
Greenhalf W
Gregory R
Griffin JL
Griffiths F
Guest M
Gunning P
Gunson RN
Gupta RK
Gupta RK
Gutierrez B
Haldenby ST
Halpin S
Hamilton WL
Hansford SE
Haque T
Hardwick H
Hardy E
Harris KA
Harrison EM
Harrison EM
Harrison I
Harrison J
Hart J
Hartley C
Hartley JA
Hartshorn S
Harvey D
Harvey M
Harvey WT
Hassan-Ibrahim MO
Havalda P
Hawcutt DB
Heaney J
Helmer T
Henderson JH
Hendry R
Hesketh AR
Hey J
Heyburn D
Higginson EE
Hill JD
Hill V
Hilson RA
Hilvers E
Hiscox JA
Hobrok M
Hodgson L
Holden MTG
Hollis A
Holmes A
Holmes AH
Holmes CW
Holmes N
Hopes R
Horby PW
Hormis A
Hornsby HR
Hosmillo M
Houlihan C
Howson-Wells HC
Hsu NS
Hubb J
Huckson H
Hughes J
Hughes M
Hughes W
Hutchings S
Idle G
Ijaz S
Illingworth CJ
Impey R
Irish-Tavares D
Iturriza-Gomara M
Izuagbe R
Jackson B
Jackson C
Jackson C
Jackson DK
Jackson KA
Jackson LM
Jacobs M
Jahun AS
Jain S
James K
James V
Jeanes C
Jeffries AR
Jennings P
Jensen RL
Jeremiah S
Jermy A
John M
Johnson K
Johnson R
Johnston I
Jones CB
Jones CR
Jones H
Jones N
Jones O
Jones S
Jones TR
Joseph A
Judges S
Kaliappan A
Kasipandian V
Kay GL
Kay S
Keating S
Keatley J-P
Keeley AJ
Kegg S
Kelsey M
Kendall J
Kenyon A
Kermack LM
Kerrison C
Kerslake I
Khakh M
Khandaker S
Khoo S
Kidd SP
Kimuli M
King K
Kirk S
Kitchen C
Kitchman K
Kiy RT
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Publication venue: iScience
Publication date: 01/01/2021
Field of study

We identify amino acid variants within dominant SARS-CoV-2 T cell epitopes by interrogating global sequence data. Several variants within nucleocapsid and ORF3a epitopes have arisen independently in multiple lineages and result in loss of recognition by epitope-specific T cells assessed by IFN-γ and cytotoxic killing assays. Complete loss of T cell responsiveness was seen due to Q213K in the A∗01:01-restricted CD8+ ORF3a epitope FTSDYYQLY207-215; due to P13L, P13S, and P13T in the B∗27:05-restricted CD8+ nucleocapsid epitope QRNAPRITF9-17; and due to T362I and P365S in the A∗03:01/A∗11:01-restricted CD8+ nucleocapsid epitope KTFPPTEPK361-369. CD8+ T cell lines unable to recognize variant epitopes have diverse T cell receptor repertoires. These data demonstrate the potential for T cell evasion and highlight the need for ongoing surveillance for variants capable of escaping T cell as well as humoral immunity.This work is supported by the UK Medical Research Council (MRC); Chinese Academy of Medical Sciences(CAMS) Innovation Fund for Medical Sciences (CIFMS), China; National Institute for Health Research (NIHR)Oxford Biomedical Research Centre, and UK Researchand Innovation (UKRI)/NIHR through the UK Coro-navirus Immunology Consortium (UK-CIC). Sequencing of SARS-CoV-2 samples and collation of data wasundertaken by the COG-UK CONSORTIUM. COG-UK is supported by funding from the Medical ResearchCouncil (MRC) part of UK Research & Innovation (UKRI),the National Institute of Health Research (NIHR),and Genome Research Limited, operating as the Wellcome Sanger Institute. T.I.d.S. is supported by a Well-come Trust Intermediate Clinical Fellowship (110058/Z/15/Z). L.T. is supported by the Wellcome Trust(grant number 205228/Z/16/Z) and by theUniversity of Liverpool Centre for Excellence in Infectious DiseaseResearch (CEIDR). S.D. is funded by an NIHR GlobalResearch Professorship (NIHR300791). L.T. and S.C.M.are also supported by the U.S. Food and Drug Administration Medical Countermeasures Initiative contract75F40120C00085 and the National Institute for Health Research Health Protection Research Unit (HPRU) inEmerging and Zoonotic Infections (NIHR200907) at University of Liverpool inpartnership with Public HealthEngland (PHE), in collaboration with Liverpool School of Tropical Medicine and the University of Oxford.L.T. is based at the University of Liverpool. M.D.P. is funded by the NIHR Sheffield Biomedical ResearchCentre (BRC – IS-BRC-1215-20017). ISARIC4C is supported by the MRC (grant no MC_PC_19059). J.C.K.is a Wellcome Investigator (WT204969/Z/16/Z) and supported by NIHR Oxford Biomedical Research Centreand CIFMS. The views expressed are those of the authors and not necessarily those of the NIHR or MRC

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Measurement of inclusive very forward jet cross sections in proton-lead collisions at \sqrt{sNN} = 5:02 TeV

Author: Aarrestad TK
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Wuerthwein F
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Yagil A
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Yetkin EA
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Zarubin A
Zarucki M
Zeinali M
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Zeuner WD
Zevi Della Porta G
Zeyrek M
Zghiche A
Zhang A
Zhang F
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Zhao J
Zhaozhong S
Zhiltsov V
Zhokin A
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Zhu RY
Zhukov V
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Zumerle G
Publication venue: 'Springer Fachmedien Wiesbaden GmbH'
Publication date: 01/01/2019
Field of study

Measurements of differential cross sections for inclusive very forward jet production in proton-lead collisions as a function of jet energy are presented. The data were collected with the CMS experiment at the LHC in the laboratory pseudorapidity range −6.6 < η < −5.2. Asymmetric beam energies of 4 TeV for protons and 1.58 TeV per nucleon for Pb nuclei were used, corresponding to a center-of-mass energy per nucleon pair of \sqrt{sNN} = 5:02 TeV. Collisions with either the proton (p+Pb) or the ion (Pb+p) traveling towards the negative η hemisphere are studied. The jet cross sections are unfolded to stable-particle level cross sections with p_{T} ≳ 3 GeV, and compared to predictions from various Monte Carlo event generators. In addition, the cross section ratio of p+Pb and Pb+p data is presented. The results are discussed in terms of the saturation of gluon densities at low fractional parton momenta. None of the models under consideration describes all the data over the full jet-energy range and for all beam configurations. Discrepancies between the differential cross sections in data and model predictions of more than two orders of magnitude are observed

UCL Discovery

Search for Wγ resonances in proton-proton collisions at s=13 TeV using hadronic decays of Lorentz-boosted W bosons

Author: M. M.
a M. K.
Aarrestad T. K.
Aarup Petersen H.
Abbaneo D.
Abbiendi G.
Abbrescia M.
Abdullin S.
Abercrombie D.
Abu Zeid S.
Acharya H.
Acosta D.
Acosta J. G.
Adam W.
Adams E.
Adams M. R.
Adams T.
Addesa F. M.
Adloff C.
Adzic P.
Afanasiev S.
Agapitos A.
Agarwal G.
Aggleton R.
Agram J. -L.
Aguilar-Benitez M.
Ahmad A.
Ahmad M.
Ahmed A.
Ahuja S.
Aimè C.
Akchurin N.
Akgun B.
Akpinar A.
al K.
Albergo S.
Albert A.
Albrow M.
Alcaraz Maestre J.
Aldaya Martin M.
Aldá Júnior W. L.
Aleks
Alex
Alhusseini M.
Alimena J.
Alison J.
Almond J.
Alvarez Gonzalez B.
Alverson G.
Alves G. A.
Aly R.
Alyari M.
Amapane N.
Ambrozas M.
Amendola C.
Amin N.
Amram O.
Amsler C.
an S.
Anagnostou G.
Andrea J.
Andreassi G.
Andreev V.
Andreev Yu.
Andrejkovic J. W.
Andrews M. B.
Androsov K.
Antchev G.
Antunovic Z.
ao Malbouisson H.
Apanasevich L.
Apollinari G.
Apparu D.
Appelt E.
Apresyan A.
Apyan A.
Araujo M.
Arcaro D.
Arcidiacono R.
Arenton M. W.
Argiro S.
Arneodo M.
aro J.
Aruta C.
Asavapibhop B.
Asawatangtrakuldee C.
Asenov P.
Asghar M. I.
Asilar E.
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Atakisi I. O.
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Attikis A.
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Publication venue
Publication date: 01/01/2022
Field of study

A search for Wγ resonances in the mass range between 0.7 and 6.0 TeV is presented. The W boson is reconstructed via its hadronic decays, with the final-state products forming a single large-radius jet, owing to a high Lorentz boost of the W boson. The search is based on proton-proton collision data at s=13 TeV, corresponding to an integrated luminosity of 137 fb−1, collected with the CMS detector at the LHC in 2016–2018. The Wγ mass spectrum is parameterized with a smoothly falling background function and examined for the presence of resonance-like signals. No significant excess above the predicted background is observed. Model-specific upper limits at 95% confidence level on the product of the cross section and branching fraction to the Wγ channel are set. Limits for narrow resonances and for resonances with an intrinsic width equal to 5% of their mass, for spin-0 and spin-1 hypotheses, range between 0.17 fb at 6.0 TeV and 55 fb at 0.7 TeV. These are the most restrictive limits to date on the existence of such resonances over a large range of probed masses. In specific heavy scalar (vector) triplet benchmark models, narrow resonances with masses between 0.75 (1.15) and 1.40 (1.36) TeV are excluded for a range of model parameters. Model-independent limits on the product of the cross section, signal acceptance, and branching fraction to the Wγ channel are set for minimum Wγ mass thresholds between 1.5 and 8.0 TeV

Archivio istituzionale della ricerca - Università di Cagliari

Evidence for electroweak production of four charged leptons and two jets in proton-proton collisions at √<i>s</i>=13 TeV

Author: Aarrestad TK
Abbaneo D
Abbiendi G
Abbrescia M
Abdullah WATW
Abdullin S
Abdulsalam A
Abercrombie D
Abu Zeid S
Ackert A
Acosta D
Acosta G
Adam W
Adams MR
Adams T
Adzic P
Afanasiev S
Agapitos A
Agaras MN
Aggleton R
Agram J-L
Ahmad A
Ahmad M
Ahmad M
Ahmed I
Ahuja S
Akbiyik M
Akchurin N
Akgun B
Al-Bataineh A
Albajar C
Albergo S
Albert A
Albrow M
Alcaraz Maestre J
Aleksandrov A
Alexakhin V
Alexander J
Alhusseini M
Ali MABM
Alimena J
Allen B
Almond J
Alvarez Fernandez A
Alvarez JDR
Alverson G
Alves FL
Alves GA
Alyari M
Amapane N
Ambrogi F
Amendola C
Amin N
Amsler C
Anagnostou G
Anampa KH
Anderson D
Andrea J
Andreev V
Andreev Y
Andrews MB
Androsov K
Angioni GLP
Antonelli L
Antropov I
Antunovic Z
Apanasevich L
Apollinari G
Apresyan A
Apyan A
Araujo M
Arcaro D
Arcidiacono R
Arenton MW
Argiro S
Arndt T
Arneodo M
Asavapibhop B
Asawatangtrakuldee C
Asghar MI
Asilar E
Askew A
Assran Y
Atakisi IO
Atay S
Ather MW
Attikis A
Auffray E
Aushev T
Autermann C
Auzinger G
Avdeeva E
Avery P
Avila C
Ayala E
Azarkin M
Azhgirey I
Aziz T
Azzi P
Azzolini V
Azzurri P
Baarmand MM
Babaev A
Babounikau I
Bacchetta N
Bachiller I
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Backhaus M
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Bahinipati S
Baidali S
Baillon P
Bainbridge R
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Ball AH
Ball F
Ban Y
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Bani L
Bansal S
Barbagli G
Barberis E
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Baringer P
Barker A
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Barrera CO
Barria P
Barrio Luna M
Bartek R
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Bartok M
Bartosik N
Baselga M
Baskakov A
Bat A
Battilana C
Baty A
Bauer G
Bauerdick LAT
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Bayshev I
Bean A
Beauceron S
Beaudette F
Becerra DAS
Beck L
Beernaert K
Beghin D
Behera PK
Behnke O
Behrens U
Bein S
Beirao Da Cruz E Silva C
Belchior Batista Das Chagas E
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Bell KW
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Cumalat JP
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Da Costa EM
Da Silveira GG
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de Barbaro P
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de Monchenault GH
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de Troconiz JF
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Delannoy AG
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Potenza R
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Poyraz D
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Prado Da Silva WL
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Publication venue: Elsevier
Publication date: 03/12/2020
Field of study

Queen Mary Research Online