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447 research outputs found

A New Vaccine for Tuberculosis: The Challenges of Development and Deployment

Author: A Williams
AT Kamath
Centers for Disease Control Prevention (CDC)
D Connelly
D Minnies
DE Snider Jr
EL Corbett
EZ Soliman
GA Colditz
HB Ibanga
Helen A. Fletcher
Helen McShane
IM Orme
J Morrison
K Huygen
K Samson
MJ Brennan
MJ McElrath
MJ Selgelid
MJ Selgelid
MJ Selgelid
NR Gandhi
O Shisana
RE Tascon
S Garattini
SL Baldwin
SP Buchbinder
Tony Hawkridge
WA Hanekom
World Health Organization
Publication venue: Springer Netherlands
Publication date: 01/01/2009
Field of study

Tuberculosis (TB) is one of the world’s leading causes of death due to infection and efforts to control TB would be substantially aided by the availability of an improved TB vaccine. There are currently nine new TB vaccines in clinical development, and the first efficacy trials are due to commence in 2009. There are many complex ethical issues which arise at all stages of TB vaccine development, from the need to conduct trials in developing countries to informed consent and the process of ethical review. While it is important that these issues are discussed, it may also be timely to consider the challenges which may arise if a vaccine in clinical development proves to be highly effective. We examine a number of scenarios where decisions on the deployment of a new TB vaccine may impact on the rights and liberty of the individual

Crossref

LSHTM Research Online

Springer - Publisher Connector

PubMed Central

Oxford University Research Archive

Receptor Complementation and Mutagenesis Reveal SR-BI as an Essential HCV Entry Factor and Functionally Imply Its Intra- and Extra-Cellular Domains

Author: A Garcia
A Owsianka
AM Owsianka
B Bartosch
B Bartosch
B Bartosch
B Bartosch
Birke Bartosch
C Bertaux
C Voisset
C Voisset
CD Rodrigues
CJ Harder
CW Shepard
D Calvo
D Delgrange
D Lavillette
D Lavillette
D Lavillette
D Nègre
D Rhainds
D Wustner
David Durantel
Dimitri Lavillette
DL Silver
DM Tscherne
E Blanchard
E Reaven
E Scarselli
ER Eckhardt
ER Eckhardt
Fabien Zoulim
François-Loïc Cosset
G Catalano
G Kellner-Weibel
G Randall
GJ de Grooth
Géraldine Verney
H Komori
H Nakabayashi
J Babitt
J Dubuisson
J Grove
J Zhang
JC Meunier
Judith Fresquet
JV Mulcahy
K Stiasny
L Meertens
M de la Llera Moya
M de la Llera-Moya
M Dreux
M Dreux
M Flint
M Hsu
M Ikemoto
M Kielian
M Krieger
M Marsh
M Umashankar
M Vinals
MA Connelly
MA Connelly
MA Connelly
Marlène Dreux
Maryse Guérin
Matthew J. Evans
MB Zeisel
MJ Evans
MT Catanese
NR Webb
O Silvie
P Maillard
P Oquendo
P Pileri
PV Subbaiah
R Thomssen
S Parathath
S Parathath
S Yalaoui
SB Kapadia
SS Rawat
T von Hahn
T vonHahn
TH Heo
TJ Nieland
V Agnello
V Sandrin
Viet Loan Dao Thi
W Le Goff
X Gu
X Gu
X Gu
XF Qin
Y Zhang
Zélie Julia
Publication venue: Public Library of Science
Publication date: 01/02/2009
Field of study

HCV entry into cells is a multi-step and slow process. It is believed that the initial capture of HCV particles by glycosaminoglycans and/or lipoprotein receptors is followed by coordinated interactions with the scavenger receptor class B type I (SR-BI), a major receptor of high-density lipoprotein (HDL), the CD81 tetraspanin, and the tight junction protein Claudin-1, ultimately leading to uptake and cellular penetration of HCV via low-pH endosomes. Several reports have indicated that HDL promotes HCV entry through interaction with SR-BI. This pathway remains largely elusive, although it was shown that HDL neither associates with HCV particles nor modulates HCV binding to SR-BI. In contrast to CD81 and Claudin-1, the importance of SR-BI has only been addressed indirectly because of lack of cells in which functional complementation assays with mutant receptors could be performed. Here we identified for the first time two cell types that supported HCVpp and HCVcc entry upon ectopic SR-BI expression. Remarkably, the undetectable expression of SR-BI in rat hepatoma cells allowed unambiguous investigation of human SR-BI functions during HCV entry. By expressing different SR-BI mutants in either cell line, our results revealed features of SR-BI intracellular domains that influence HCV infectivity without affecting receptor binding and stimulation of HCV entry induced by HDL/SR-BI interaction. Conversely, we identified positions of SR-BI ectodomain that, by altering HCV binding, inhibit entry. Finally, we characterized alternative ectodomain determinants that, by reducing SR-BI cholesterol uptake and efflux functions, abolish HDL-mediated infection-enhancement. Altogether, we demonstrate that SR-BI is an essential HCV entry factor. Moreover, our results highlight specific SR-BI determinants required during HCV entry and physiological lipid transfer functions hijacked by HCV to favor infection

Public Library of Science (PLOS)

Crossref

Directory of Open Access Journals

PubMed Central

Intravenous regional block is similar to sympathetic ganglion block for pain management in patients with complex regional pain syndrome type I

Author: Ackerman WE
Bernard JM
Bonelli S
Brown DL
Carron H
Choyce A
Connelly NR
Eisenach JC
Elias M
Forouzanfar T
Forouzanfar T
Frade LC
Gintautas J
Hannington-Kiff JG
Harden RN
Hardy PA
Hilgenhurst G
Hoffman BB
Hord AH
Hord ED
J.G. Klamt
Karakurum G
Kopacz DJ
Kroin JS
Lake AP
Livingstone JA
M.S.A. Nascimento
McKain CW
Merskey H
Price DD
Quisel A
Reuben SS
Reuben SS
Reuben SS
Reuben SS
Sia S
Singelyn FJ
Taskaynatan MA
Toda K
Tountas AA
W.A. Prado
Wallace MS
Wasner G
Publication venue: 'FapUNIFESP (SciELO)'
Publication date
Field of study

Crossref

A Neptune-sized transiting planet closely orbiting a 5–10-million-year-old star

Author: A Claret
A McQuillan
A Vanderburg
AC Boley
ACS Readhead
AL Kraus
AL Kraus
AL Kraus
AL Kraus
AW Mann
BMS Hansen
BP Bowler
BT Montet
CD Dressing
CD Dressing
CH Chen
CL Slesnick
D Foreman-Mackey
DE Trilling
DL Nidever
DNC Lin
EA Petigura
EJ de Geus
EL Martín
GJ Herczeg
GP Kuiper
H Bouy
I Baraffe
IJM Crossfield
JD Scargle
JE Baldwin
JHJ de Bruijne
JM Carpenter
JM Carpenter
JN Connelly
K Mandel
KL Luhman
L Girardi
L Girardi
L Kreidberg
L Malavolta
L Yu
MC Wyatt
MJ Pecaut
MJ Pecaut
N Huélamo
N Lodieu
N Lodieu
NR Lomb
PG Tuthill
PJ Armitage
PR Allen
PT de Zeeuw
R Kolbl
R Kurosawa
RJ Jackson
RR Rafikov
S Chatterjee
S Hinkley
S Lépine
S Seager
SB Dieterich
SB Howell
SB Howell
SM Rucinski
SN Quinn
T Preibisch
T Preibisch
T Preibisch
TJ David
TJ David
W Kley
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/06/2016
Field of study

Theories of the formation and early evolution of planetary systems postulate that planets are born in circumstellar disks, and undergo radial migration during and after dissipation of the dust and gas disk from which they formed^1, 2. The precise ages of meteorites indicate that planetesimals—the building blocks of planets—are produced within the first million years of a star’s life^3. Fully formed planets are frequently detected on short orbital periods around mature stars. Some theories suggest that the in situ formation of planets close to their host stars is unlikely and that the existence of such planets is therefore evidence of large-scale migration^4, 5. Other theories posit that planet assembly at small orbital separations may be common^6, 7, 8. Here we report a newly born, transiting planet orbiting its star with a period of 5.4 days. The planet is 50 per cent larger than Neptune, and its mass is less than 3.6 times that of Jupiter (at 99.7 per cent confidence), with a true mass likely to be similar to that of Neptune. The star is 5–10 million years old and has a tenuous dust disk extending outward from about twice the Earth–Sun separation, in addition to the fully formed planet located at less than one-twentieth of the Earth–Sun separation

arXiv.org e-Print Archive

Crossref

ScholarSpace at University of Hawai'i at Manoa

Caltech Authors

University of Southern Queensland ePrints

Thrombus aspiration during primary percutaneous coronary intervention is associated with reduced myocardial edema, hemorrhage, microvascular obstruction and left ventricular remodeling

Abstract Background Thrombus aspiration (TA) has been shown to improve microvascular perfusion during primary percutaneous coronary intervention (PCI) for patients with ST-segment elevation myocardial infarction (STEMI). The objective of our study was to assess the relationship between TA and myocardial edema, myocardial hemorrhage, microvascular obstruction (MVO) and left ventricular remodeling in STEMI patients using cardiovascular magnetic resonance (CMR). Methods Sixty patients were enrolled post primary PCI and underwent CMR on a 1.5 T scanner at 48 hours and 6 months. Patients were retrospectively stratified into 2 groups: those that received TA (35 patients) versus that did not receive thrombus aspiration (NTA) (25 patients). Myocardial edema and myocardial hemorrhage were assessed by T2 and T2* quantification respectively. MVO was assessed via a contrast-enhanced T1-weighted inversion recovery gradient-echo sequence. Results At 48 hours, infarct segment T2 (NTA 57.9 ms vs. TA 52.1 ms, p = 0.022) was lower in the TA group. Also, infarct segment T2* was higher in the TA group (NTA 29.3 ms vs. TA 37.8 ms, p = 0.007). MVO incidence was lower in the TA group (NTA 88% vs. TA 54%, p = 0.013). At 6 months, left ventricular end-diastolic volume index (NTA 91.9 ml/m2 vs. TA 68.3 ml/m2, p = 0.013) and left ventricular end systolic volume index (NTA 52.1 ml/m2 vs. TA 32.4 ml/m2, p = 0.008) were lower and infarct segment systolic wall thickening was higher in the TA group (NTA 3.5% vs. TA 74.8%, p = 0.003). Conclusion TA during primary PCI is associated with reduced myocardial edema, myocardial hemorrhage, left ventricular remodeling and incidence of MVO after STEMI.</p

University of Toronto Research Repository

Crossref

Springer - Publisher Connector

Directory of Open Access Journals

PubMed Central

An agent-based simulation combined with group decision-making technique for improving the performance of an emergency department

Author: Ahmed MA
Brenner S
Chiavone PA
Connelly LG
Dawson D
Doyle SL
Eskandari H
Fülöp J
Gul M
Hancock WM
Herrera-Viedma E
Hoot NR
Kadri F
Lane DC
Laskowski M
Laskowski M
Mackway-Jones K
Paul SA
Ruohonen T
Samaha S
Shaikh SB
Taboada M
Taboada M
Taboada M
Trzeciak S
Uriarte AG
Van der Wulp I
Wilensky U
Publication venue: 'FapUNIFESP (SciELO)'
Publication date: 01/01/2017
Field of study

Crossref

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
Daly D
Daniels J
Das E
Das K
Datta U
Davies E
Davies G
Davies J
Davies P
Davis H
Davison C
Dawe V
Dawood S
Day L
De Cates C
De Freitas M
Dean S
Debnath D
Deekonda P
Deepak S
Deery L
Delvi A
Denley S
Dennahy IS
Dennis R
Dennis Y
Desai H
Desai K
Devalia S
Dhaliwal R
Dhillon AK
Dhillon P
Dhir T
Dhuna S
Diamond J
Dib NP
Dickson G
Dietrich A
Dindyal S
Dixon O
Do V
Dobrzynska M
Doherty C
Donaldson G
Donohoe C
Doshi A
Doull C
Downes C
Doyle C
Drake TM
Draper A
Dudley B
Duff F
Duffield J
Duggal A
Dumann E
Dunleavy K
Dunne E
Dupaguntla YS
Durand C
Durbacz M
Durham-Hall A
Durno J
Durrigan T
Duthie F
Dutta A
Dyal A
Dynes K
Easby S
Easdon S
Eastwood M
Ebhogiaye O
Eccles L
Ecclestone T
Eddama M
Edgerton K
Edozie F
Edwin C
Egan E
Eiben I
Eiben P
Eilon T
El Matary R
El Tokhy O
El-Sawy D
El-Taji O
Elangovan S
Elbuzidi M
Elder P
Elias J
Ellerby N
Elliot J
Elliott J
Elsaddig M
Elseedawy E
Emberton J
En BNW
Engledow A
English W
Epanomeritakis E
Episkopos C
Epstein J
Esmail R
Evans D
Evans E
Evans L
Evans R
Ezzat A
Fafemi O
Falamarzi A
Fam M
Faraj A
Farhan-Alanie MMH
Farmer N
Farooq M
Farooqi M
Farrar E
Farwana M
Faulkner S
Fawole A
Fearnhead N
Feldman M
Fenton K
Ferris B
Filipescu T
Finch E
Fitzgerald I
Fitzgerald JE
Fitzpatrick H
Flack V
Flamini T
Fletcher D
Foley MP
Fong J
Fowler AJ
Fox H
Fozard T
France B
Francis N
Francis S
Francois V
Francombe J
Freeman SK
Frere M
Frew K
Friend C
Froggatt P
Frost A
Frost J
Fung H
Gabriel R
Gaddah M
Gadsby C
Gaffing S
Galea M
Gallogly P
Galloway F
Gammeri E
Gani A
Ganyani R
Gao C
Gardner I
Gardner S
Gardner T
Garner C
Garsaa T
Gaukroger A
Ge Y
Gentry R
George A
George D
Gerard L
Ghaffar A
Ghag S
Ghailan N
Gharatya A
Gibbons D
Gibson W
Gidwani A
Gil H
Gilbert A
Gill A
Gill K
Gillespie H
Gimson A
Girdlestone T
Given A
Glace S
Glasbey J
Glasbey JC
Glen P
Glover M
Gnanappiragasam D
Goaman A
Goergen N
Goh C
Goh ET
Gohil J
Gokani S
Golding D
Gomaa A
Gonzalez-Ciscar A
Goodson R
Gopfert A
Gordon J
Gorman D
Gower T
Grace R
Graham CJ
Graham S
Grant A
Grant M
Gravell R
Green B
Green S
Greenan E
Greenhalgh S
Gregoriou K
Gregory C
Gresly J
Grey A
Gribbon C
Griffith J
Griffiths B
Griffiths H
Griffiths N
Gruhn A
Guevel B
Guillotte C
Gulzar I
Gundogan B
Gunwa T
Gupta A
Gupta R
Gurjar S
Gurung E
Guy C
Gwilym B
Gwozdz AM
Hack J
Hackney E
Haddad S
Hague M
Hair J
Hall M
Hall N
Hallan R
Hamdan K
Hamid H
Hammad A
Hanson M
Haq T
Haque A
Haray P
Hare L
Harinath G
Harlinska A
Harris A
Harris C
Harris L
Harris R
Harris S
Harrison E
Harrison EM
Harrison P
Harrogate S
Hart SJ
Harte J
Hartley J
Hartley M
Harty M
Hashemi R
Hassanin K
Hathaway C
Haughey B
Hawthorne T
Hayashi E
Hayat A
Hayat F
Hayes JDB
Haynes K
Haynes S
Hayward J
Haywood E
Hazeldine P
He YY
Hedley C
Helliwell R
Heng S
Henry J
Henshaw V
Herman A
Hernon J
Heywood E
Hickland P
Hill N
Hilton J
Hitchen C
Ho B
Ho C
Ho M
Ho W
Hodgson B
Hodgson S
Hogg G
Holdsworth R
Hole J
Hollington D
Holmes D
Holt F
Hopkins M
Horne L
Horseman C
Hosamuddin H
Hoskins T
Hossain M
Hossain S
Hough A
Houghton C
Houlton J
Howlader M
Hrvacic N
Hubert J
Hudson S
Hudson-Peacock N
Hughes B
Hughes EJ
Hughes J
Hughes K
Huisman L
Hull K
Hung YMA
Hungwe C
Hunt C
Huppatz IW
Huq T
Hurst P
Hussain A
Hussain M
Hussain SF
Hussain ST
Hussein N
Hutchinson S
Ibrahim B
Ibrahim I
Ijeomah A
Ikogho O
Ikram B
Ilenkovan N
Imam SZ
Imran H
Ingleton R
Ingram H
Innes R
Iqbal F
Iqbal S
Iroegbu U
Ishaq H
Islam Y
Ismail O
Ito G
Ivo T
Jackman T
Jackson CES
Jacob-Ramsdale B
Jain D
Jain P
Jamal S
James F
Javaid NR
Jawad L
Jawad ZAR
Jebakumar R
Jeffreys N
Jeyabaladevan S
Ji C
Jiang J
Jiao LR
John I
John N
Johnson S
Johnston R
Johnston S
Joji N
Jones A
Jones C
Jones D
Jones E
Jones H
Jones L
Jones M
Jones W
Jong B
Jordan P
Joseph R
Joyce H
Joyner C
Jull P
Kale A
Kamarajah S
Kambasha C
Kaminski F
Kanabar S
Kanapeckaite L
Kandage D
Kandhari N
Kandiah K
Kane D
Kane L
Kapp J
Kaptanis S
Karaj J
Karam E
Karbowiak M
Karim MA
Karim MJ
Karmarkar A
Karsan RB
Karunatilleke AS
Katira A
Katsaiti I
Kaur G
Kausar A
Kazmi Z
Keane K
Kee JY
Keelan G
Kelkar A
Kelly D
Kelly M
Kenefick N
Kennedy ED
Keogh C
Kerin M
Kerr M
Kerrigan K
Kersey T
Kershaw S
Keshvala C
Kethees A
Keyte A
Khadem N
Khalil M
Khaliq M
Khan A
Khan H
Khan K
Khan M
Khan S
Khatri C
Khaw J
Khawaja H
Khawar H
Khawari S
Khodatars K
Khoo E
Kiandee M
Kidanu D
Kiely A
Killington K
Kim P
Kim S
King J
King S
Kinnersley H
Kirby S
Kirk S
Kishore A
Klimach S
Knight C
Knight JS
Kokayi A
Komolafe O
Komoriyama A
Kong C
Kong CH
Kong JTH
Koo PY
Kopczynska M
Koshy R
Kossoff J
Kremel D
Krishna K
Krysztopik R
Kukran S
Kumar AP
Kumar KM
Kumar R
Lacy-Colson J
Ladha D
Lagzouli N
Laing C
Lake C
Lakin F
Lal K
Lalor P
Lam J
Lambotharan S
Lamptey E
Lang-Orsini M
Langasco N
Latter J
Lau J
Lau K
Lawday S
Laws J
Lazarou A
Leadholm N
Lee A
Lee G
Lee J
Lee S
Leer M
Leinhardt D
Leong A
Leong K
Leong S
Leong SH
Leptidis I
Leung E
Lewis N
Lex J
Li H
Liew I
Lim D
Lim H
Lim S
Lim SW
Lim ZC
Lim ZH
Limb C
Lingam G
Linley-Adams L
Linn T
Liu H
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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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Suri A
Svolkinas D
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Tang A
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Taribagil P
Tariq A
Tate S
Tayeh S
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Taylor O
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Taylor Z
Telfer R
Teng T
Tenters F
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Thachettu A
Thakrar D
Thatcher A
Theodoropoulou K
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Thoms BL
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Yang DD
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Yarham E
Yasin IH
Yasin T
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Ye W
Yeo A
Yeoh T
Yeung J
Yin ZD
Yip J
Yoganayagam N
Yogeswara T
York J
Yousaf A
Youssef H
Yu T
Yule A
Zaat S
Zanichelli D
Zaver V
Zeng R
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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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The University of Manchester - Institutional Repository

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Search for new phenomena in final states with an energetic jet and large missing transverse momentum in pp collisions at root s = 8 TeV with the ATLAS detector (vol 75, 299, 2015)

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Abbott B
Abdallah J
Abdinov O
Aben R
Abi B
Abolins M
AbouZeid OS
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Abreu H
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Acharya BS
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Agatonovic-Jovin T
Aguilar-Saavedra JA
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Ahlen SP
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Akesson TPA
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Alconada Verzini MJ
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Aleksandrov IN
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Alexandre G
Alexopoulos T
Alhroob M
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Alison J
Allbrooke BMM
Allison LJ
Allport PP
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Amaral Coutinho Y
Amelung C
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Amor Dos Santos SP
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Amundsen G
Anastopoulos C
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Anders CF
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Anisenkov AV
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Collaboration ATLAS
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Flowerdew MJ
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Gavrilenko IL
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Gee CNP
Geerts DAA
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Giordani MP
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Gorbounov PA
Gordon HA
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Goshaw AT
Gostkin MI
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Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2015
Field of study

Results of a search for new phenomena in final states with an energetic jet and large missing transverse momentum are reported. The search uses 20.3 fb−1 of √s=8 TeV data collected in 2012 with the ATLAS detector at the LHC. Events are required to have at least one jet with pT>120 GeV and no leptons. Nine signal regions are considered with increasing missing transverse momentum requirements between EmissT>150 GeV and EmissT>700 GeV. Good agreement is observed between the number of events in data and Standard Model expectations. The results are translated into exclusion limits on models with either large extra spatial dimensions, pair production of weakly interacting dark matter candidates, or production of very light gravitinos in a gauge-mediated supersymmetric model. In addition, limits on the production of an invisibly decaying Higgs-like boson leading to similar topologies in the final state are presented

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