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51 research outputs found

The doubly inelastic contribution to electron loss: H0 and He0 (0,5 MeV u-1) in collision with Ar

Author: Farmery B. W.
Groeneveld K. O.
Heil O.
Jakubaßa-Amundsen Doris H.
Kuzel M.
Lucas M. W.
Maier R.
Publication venue
Publication date: 01/01/1992
Field of study

Genomic evolution of breast cancer metastasis and relapse

A.G.L. and J.H.R.F. were supported by a Cancer Research UK Program Grant to Simon Tavaré (C14303/A17197).Patterns of genomic evolution between primary and metastatic breast cancer have not been studied in large numbers, despite patients with metastatic breast cancer having dismal survival. We sequenced whole genomes or a panel of 365 genes on 299 samples from 170 patients with locally relapsed or metastatic breast cancer. Several lines of analysis indicate that clones seeding metastasis or relapse disseminate late from primary tumors, but continue to acquire mutations, mostly accessing the same mutational processes active in the primary tumor. Most distant metastases acquired driver mutations not seen in the primary tumor, drawing from a wider repertoire of cancer genes than early drivers. These include a number of clinically actionable alterations and mutations inactivating SWI-SNF and JAK2-STAT3 pathways.Publisher PDFPeer reviewe

DI-fusion

The University of Manchester - Institutional Repository

Erasmus University Digital Repository

Institute of Cancer Research Repository

Crossref

EUR Research Repository

Oxford University Research Archive

King's Research Portal

University of St. Andrews - Pure

St Andrews Research Repository

The Role of Presenilin and its Interacting Proteins in the Biogenesis of Alzheimer’s Beta Amyloid

Author: A Alberici
A Bergman
A Bergman
A Capell
A Georgakopoulos
A Herreman
A Lleo
A Lleo
A Smine
A Takashima
A Weidemann
AA Johnsingh
AL Mah
AS Crystal
B Stahl
B Strooper De
B Strooper De
BJ Passer
C Dumanchin
C Goutte
C Lilliehook
C Lilliehook
C Yu
CA Lemere
D Beher
D Cai
D Edbauer
D Edbauer
D Levitan
D Seiffert
DE Kang
DE Kang
DG Jo
DG Jo
DG Jo
DM McLoughlin
DM McLoughlin
DR Borchelt
DS Yang
E Levy-Lahad
E Pack-Chung
EH Schroeter
EI Rogaev
EK Choi
EM Hansson
F Chen
FA Barr
G Gassen Van
G Levesque
G Ma
G Periz
G Prihar
G Thinakaran
G Verdile
G Verdile
G Yu
G Yu
G Yu
G Zhao
G Zhao
Giuseppe Verdile
H Hasegawa
H Laudon
H Lopez-Schier
H Steiner
H Steiner
H Steiner
H Tanahashi
H Tanahashi
HM Chung
HQ Wang
HS Kim
I Hayashi
I Imafuku
I Raurell
J Li
J Shen
J Zhou
JD Buxbaum
JD Buxbaum
JP Borg
JY Leem
K Shinozaki
K Shirotani
K Shirotani
K Stromberg
K Suga
K Suga
KF Lau
L Pellegrini
L Zhang
LK Massey
LK Massey
M Niimura
M Niwa
M Okochi
M Sastre
M Sastre
M Seeger
MA Leissring
MA Liz
MB Podlisny
MJ LaVoie
MR Farmery
MS Wolfe
MS Wolfe
MS Wolfe
MT Lai
N Takasugi
N Watanabe
O Berezovska
O Berezovska
O Nyabi
P Mastrangelo
PC Fraering
PC Wong
PH Reddy
Q Chen
R Blum
R Francis
R Roncarati
R Rozmahel
Ralph N. Martins
S Cervantes
S Gandy
S Gupta
S Prokop
S Shah
S Tomita
S Urban
Samuel E Gandy
SF Lee
SF Lee
SH Kim
SH Kim
SK Smith
SM Stabler
SX Zhang
T Katayama
T Li
T Ogura
T Takeda
T Tomita
VA Morais
VK Lazarov
W Scheper
W Xia
W Xia
W Xia
W Zhang
WG Annaert
WJ Luo
WJ Ray
WP Esler
WT Kimberly
WT Kimberly
WT Kimberly
X Xu
Y Araki
Y Gu
Y Hu
Y Hu
Y Morohashi
Y Zhou
YM Li
YM Li
Z Zhang
Publication venue: Kluwer Academic Publishers-Plenum Publishers
Publication date: 01/01/2006
Field of study

The biogenesis and accumulation of the beta amyloid protein (Aβ) is a key event in the cascade of oxidative and inflammatory processes that characterises Alzheimer’s disease. The presenilins and its interacting proteins play a pivotal role in the generation of Aβ from the amyloid precursor protein (APP). In particular, three proteins (nicastrin, aph-1 and pen-2) interact with presenilins to form a large multi-subunit enzymatic complex (γ-secretase) that cleaves APP to generate Aβ. Reconstitution studies in yeast and insect cells have provided strong evidence that these four proteins are the major components of the γ-secretase enzyme. Current research is directed at elucidating the roles that each of these protein play in the function of this enzyme. In addition, a number of presenilin interacting proteins that are not components of γ-secretase play important roles in modulating Aβ production. This review will discuss the components of the γ-secretase complex and the role of presenilin interacting proteins on γ-secretase activity

Crossref

Springer - Publisher Connector

PubMed Central

Research Online @ ECU

espace@Curtin

Jefferson Digital Commons

The structure and function of Alzheimer's gamma secretase enzyme complex

Author: Anders L
Andersson CX
Araki Y
Artavanis-Tsakonas S
Barr FA
Bartus RT
Baumeister R
Beher D
Bentahir M
Berezovska O
Berezovska O
Best JD
Blum R
Bonn S
Britschgi M
Brown MS
Brunkan AL
Cai J
Capell A
Capell A
Carey BW
Cervantes S
Chen F
Citron M
Cowan JW
David Groth
De Keersmaecker K.
De Strooper B
De Strooper B
De Strooper B.
Duff K
Dyczynska E
Edbauer D
Eggert S
Endres K
Evin G
Farmery MR
Fluhrer R
Fortini ME.
Fortna RR
Fraering PC
Francis R
Friedmann E
Gandy S
Georgakopoulos A
Giuseppe Verdile
Gowrishankar K
Green RC
Gu Y
Gu Y
Haapasalo A
Haas IG
Hampe W
Hansson EM
Hasegawa H
Hayashi I
Hemming ML
Hiesberger T
Ho A
Hoe HS
Hu Y
Ikeuchi T
Ishii K
Kasuga K
Kidd PM.
Kim AC
Kim DY
Kim SH
Kim SH
Kimberly WT
Kimberly WT
Kuhn PH
Kumar-Singh S
Lai MT
Lammich S
Lanz TA
Lao JI
Laudon H
LaVoie MJ
LaVoie MJ
Lazarov VK
Lee HJ
Lee SF
Lee SF
Lemberg MK
Lemere CA
Leuchtenberger S
Levitan D
Levy-Lahad E
Li T
Li YM
Li YM
Limbikani Kanyenda
Litterst C
Liu CX
Lleo A
Luo WJ
Marambaud P
Marambaud P
Maretzky T
Martys-Zage JL
Mastrangelo P
May P
McElroy B
Meyer EL
Mi K
Mizutani T
Mumm JS
Murakami D
Murayama O
Netzer WJ
Ni CY
Ni CY
Nyabi O
Nyborg AC
Nyborg AC
Ogura T
Okamoto I
Okochi M
Okochi M
Parks AL
Placanica L
Podlisny MB
Ponting CP
Prokop S
Qi-Takahara Y
Raina P
Ralph N Martins
Raychaudhuri M
Reddy PH.
Rogaev EI
Rozmahel R
Saleh AZ
Sanchez-Irizarry C
Sastre M
Sato T
Saxena MT
Schellenberg GD
Scheuner D
Schroeter EH
Schroeter EH
Schulte A
Schulz JG
Searfoss GH
Seeger M
Seiffert D
Shah S
Shearman MS
Shen J
Sherrington R
Shimizu K
Shirotani K
Spasic D
St George-Hyslop P
Steiner H
Steiner H
Steiner H
Sudarsan Krishnaswamy
Takasugi N
Taniguchi Y
Thinakaran G
Tomita T
Tousseyn T
Uemura K
Urban S
Urra S
Vassar R
Verdile G
Verdile G
Verdile G
Vetrivel KS
von Arnim CA
Wakabayashi T
Walsh DM
Wang R
Wang Y
Watanabe N
Weidemann A
Weihofen A
Wilhelmsen K
Winblad B
Winkler E
Wolfe MS
Wolfe MS
Wolfe MS.
Wolfe MS.
Wong HK
Xia W
Xiong K
Yao J
Yarden Y
Yu C
Yu G
Zekanowski C
Zhang L
Zhang YW
Zhao G
Zhao G
Zhou S
Zou Z
Publication venue: 'Informa UK Limited'
Publication date: 01/01/2009
Field of study

The production and accumulation of the beta amyloid protein (Aβ) is a key event in the cascade of oxidative and inflammatory processes that characterizes Alzheimer’s disease (AD). A multi-subunit enzyme complex, referred to as gamma (γ) secretase, plays a pivotal role in the generation of Aβ from its parent molecule, the amyloid precursor protein (APP). Four core components (presenilin, nicastrin, aph-1, and pen-2) interact in a high-molecular-weight complex to perform intramembrane proteolysis on a number of membrane-bound proteins, including APP and Notch. Inhibitors and modulators of this enzyme have been assessed for their therapeutic benefit in AD. However, although these agents reduce Aβ levels, the majority have been shown to have severe side effects in pre-clinical animal studies, most likely due to the enzymes role in processing other proteins involved in normal cellular function. Current research is directed at understanding this enzyme and, in particular, at elucidating the roles that each of the core proteins plays in its function. In addition, a number of interacting proteins that are not components of γ-secretase also appear to play important roles in modulating enzyme activity. This review will discuss the structural and functional complexity of the γ-secretase enzyme and the effects of inhibiting its activity

Crossref

Research Online @ ECU

espace@Curtin

Telomerecat: A ploidy-agnostic method for estimating telomere length from whole genome sequencing data (vol 8, 1300, 2018)

Author: Afzal M
Aitman T
Alachkar H
Alavijeh OS
Ali S
Ali S
Allen HL
Allen L
Allsup D
Ambegaonkar G
Ancliff P
Anderson J
Antrobus R
Armstrong R
Arno G
Arumugakani G
Ashford S
Astle W
Attwood A
Austin S
Babbs C
Bacchelli C
Bakchoul T
Bariana TK
Baxendale H
Bennett D
Bethune C
Bibi S
Bitner-Glindzicz M
Bleda M
Boggard HJ
Bolton-Maggs P
Booth C
Bradley JR
Brady A
Brown M
Browning M
Bryson C
Burns S
Calleja P
Canham N
Carmichael J
Carss K
Caulfield M
Chalmers E
Chandra A
Chinnery P
Chitre M
Chong S
Church C
Clement E
Clements-Brod N
Clowes V
Coghlan G
Colby E
Collins J
Collins P
Cook HT
Cookson V
Cooper N
Corris PA
Creaser-Myers A
DaCosta R
Daugherty L
Davies S
Davis J
De Vries M
Deegan P
Deevi SVV
Deshpande C
Devlin L
Dewhurst E
Dixon P
Doffinger R
Dolling H
Dormand N
Drewe E
Edgar D
Egner W
Emmerson I
Erber WN
Erwood M
Everington T
Eyries M
Farmery JHR
Favier R
Firth H
Fletcher D
Flinter F
Frary A
French C
Freson K
Furie B
Furnell A
Gale D
Gall H
Gardham A
Gattens M
Gebhart J
Ghali N
Ghataorhe PK
Ghio S
Ghofrani A
Ghurye R
Gibbs JSR
Gilmour K
Ginsberg L
Girerd B
Gissen P
Goddard S
Gomez K
Gordins P
Gosal D
Graf S
Greene D
Greenhalgh A
Greinacher A
Gresele P
Grigoriadou S
Grozeva D
Hackett S
Hadden R
Hadinnapola C
Hague R
Haimel M
Halmagyi C
Hammerton T
Harper L
Hart D
Hayman G
Heemskerk JWM
Henderson R
Hensiek A
Henskens Y
Herwadkar A
Holden S
Holder M
Holder S
Horvath R
Houweling AC
Hu F
Hudson G
Huissoon A
Humbert M
Hurst J
in't Veld AH
James R
Johnson S
Jolles S
Josifova D
Kazmi R
Keeling D
Kelleher P
Kelly AM
Kennedy F
Kiely DG
Kingston N
Kovacs G
Koziell A
Krishnakumar D
Kuijpers T
Kuijpers TW
Kumararatne D
Kurian M
Laffan MA
Lambert MP
Lango-Allen H
Lawrie A
Layton M
Lear S
Lees M
Lentaigne C
Levine AP
Liesner R
Linger R
Longhurst H
Lorenzo L
Louka E
Lynch AG
Machado R
MackenzieRoss RV
MacLaren R
Mahdi-Rogers M
Maher E
Maimaris J
Makris M
Mangles S
Manson A
Manzur A
Mapeta R
Markus HS
Marshall A
Martin J
Martin JM
Masati L
Mathias M
Matser V
Matthews E
Maw A
McCarthy M
McDermott E
McGowan S
McJannet C
Meacham S
Mead A
Meehan S
Megy K
Mehta S
Michaelides M
Millar CM
Moledina S
Montani D
Moore A
Morrell NW
Mumford A
Murng S
Murphy E
Nejentsev S
Noorani S
Noordegraaf AV
Nurden P
Oksenhendler E
Ormondroyd L
Othman S
Ouwehand WH
Papadia S
Park S-M
Parker A
Pasi J
Patch C
Paterson J
Payne J
Peacock AJ
Peerlinck K
Penkett CJ
Pepke-Zaba J
Perry DJ
Pollock V
Polwarth G
Ponsford M
Qasim W
Quinti I
Ranganathan L
Rankin J
Rankin S
Raymond FL
Rayner-Matthews P
Rehnstrom K
Reid E
Reilly M
Renton T
Revel-Vilk S
Rhodes CJ
Rice A
Richards M
Richardson S
Richter A
Roberts I
Rondina M
Rosser E
Roughley C
Roy N
Rue-Albrecht K
Saleem M
Samarghitean C
Sanchis-Juan A
Sandford R
Santra S
Sargur R
Savic S
Scelsi L
Schotte G
Schulman S
Schulze H
Scott R
Scully M
Seneviratne S
Sewell C
Shamardina O
Shipley D
Simeoni I
Sivapalaratnam S
Smith KGC
Smith ML
Sohal A
Soubrier F
Southgate L
Staines S
Staples E
Stark H
Stauss H
Stein P
Stephens J
Stirrups K
Stock S
Stubbs M
Suntharalingam J
Tait RC
Talks K
Tan R
Tan Y
Thachil J
Thaventhiran J
Themistocleous A
Thomas E
Thomas M
Thompson D
Thrasher A
Tischkowitz M
Titterton C
Toh C-H
Toshner M
Treacy CM
Trembath R
Tuna S
Turek W
Turro E
Vale T
Van Geet C
Van Zuydam N
Veltman M
Vogt J
von Ziegenweldt J
Wakeling E
Walker S
Walker S
Wanjiku I
Warner TQ
Wassmer E
Watkins H
Watson H
Watt C
Webster A
Wei W
Welch S
Westbury S
Wharton J
Whitehorn D
Whitworth J
Wilkins M
Willcocks L
Williamson C
Wong EKS
Woods G
Wort SJ
Yates K
Yeatman N
Yong P
Young T
Yu P
Yu-Wai-Man P
Publication venue: NATURE PUBLISHING GROUP
Publication date: 03/09/2018
Field of study

UCL Discovery

Dimethyl fumarate in patients admitted to hospital with COVID-19 (RECOVERY): a randomised, controlled, open-label, platform trial

Author: Abbas M.
Abdul Rasheed A.
Abdul A.
Abdul-Kadir R.
Abdusamad K.
Abernethy K.
Aboelela H.
Abouzaid M.
Abraham M.
Abraham T.
Abrams J.
Abu H.
Abu-Arafeh A.
Acton C.
Adam F.
Adam M.
Adams C.
Adams C.
Adams D.
Adams L.
Addo A.
Adedeji O.
Adegoke K.
Adewunmi E.
Adeyemo T.
Agbeko R.
Aggarwal S.
Ahmad S.
Ahmed A.
Ahmed I.
Ahmed M.
Ahmed R.
Ahmed R.
Ainsworth M.
Ajmi A.
Akili S.
Al Aaraj A.
Al Balushi A.
Al-Asadi A.
Al-Khalil M.
Al-Ramadhani B.
Al-Saadi Z.
Al-Shahi Salman R.
Al-Sheklly B.
Albert P.
Alegria A.
Alexander A.
Alexander P.
Alhabsha O.
Ali M.
Ali M.
Aliberti E.
Alin J.
Aliyuda F.
Alkhudhayri A.
Allan N.
Allanson A.
Allen E.
Allen L.
Alshaer I.
Altaf S.
Amezaga M.
Amin A.
Amit B.
Anand A.
Anantapatnaikuni S.
Anderson L.
Anderson M.
Anderson M.
Anderson N.
Anderson R.
Andrews A.
Ang A.
Anguvaa L.
Aniruddhan K.
Antonina Z.
Araujo M.
Archer A.
Archer S.
Arimoto R.
Arkley C.
Armah C.
Armistead J.
Armstrong C.
Arnison-Newgass C.
Arora D.
Arya A.
Arya R.
Asghar A.
Ashbrook-Raby C.
Asher G.
Ashley D.
Ashraf S.
Ashton D.
Ashworth R.
Aslam A.
Atomode A.
Attubato E.
Aubrey P.
Aujayeb A.
Aung N.
Avery M.
Avram C.
Aya A.
Ayaz E.
Aziz G.
Babatunde F.
Babington G.
Bachour M.
Badhan G.
Bae J.
Bagley G.
Bagshaw L.
Bailey A.
Baillie J.
Baillie J.K.
Baird D.
Bajandouh A.
Baker D.
Baker K.
Bakere H.
Bakhai A.
Balasingam P.
Balaskas T.
Balasubramaniam M.
Balcombe A.
Baldwin A.
Baldwin-Jones R.
Balfour J.
Balmforth C.
Baluwala A.
Bamford A.
Bancroft H.
Banda J.
Banks H.
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Bannister O.
Baptist M.
Barclay C.
Barker D.
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Barker-Williams K.
Barnacle J.
Barnard A.
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Barnett-Vanes A.
Barr A.
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Bartholomew J.
Bartlett G.
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Baruah R.
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Bashyal A.
Basoglu A.
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Batra D.
Baxter M.
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Beacham L.
Beadon K.
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Beddall H.
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Biggs S.
Biju A.
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Bridgwood G.
Bright J.
Broadhurst R.
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Brodsky M.
Brokke F.
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Brraka A.
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Brudlo W.
Buch M.H.
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Buck A.
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Bugg G.
Bujazia R.
Bullock E.
Burda D.
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Burgess S.
Burman A.
Burston C.
Burton A.
Butler E.
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Buttress D.
Byrne J.
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Byrne-Watts V.
Cale E.
Calisti G.
Callens C.
Cameron E.
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Camm C.
Cammack R.
Campbell Hewson Q.
Campbell B.
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Cann A.
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Cantliff J.
Caplin B.
Capp A.
Carey C.
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Carnahan M.
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Carson R.
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Chadwick J.
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Chaudhuri N.
Chauhan R.
Chawla V.
Chen F.
Cheng F.
Cherrie M.
Cheung E.
Cheyne C.
Chilcott S.
Chilvers A.
Chin K.
Chineka R.
Chinonso E.
Chisnall B.
Chiswick C.
Chivima B.
Chmiel C.
Chrisopoulou A.
Christian P.
Christides A.
Christmas D.
Church E.
Cianci N.
Cicconi P.
Clare E.
Clark E.
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Clark L.
Clark R.
Clarke A.
Clarke R.
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Clay K.
Clayton-Smith J.
Cleaver C.
Clemente de la Torre C.
Clifford S.
Coakley M.
Cobain K.
Cochrane P.
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Coe A.
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Cohen D.
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Coker O.
Cole J.
Coleman G.
Coles H.
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Collini P.
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Collins V.
Colton H.
Condliffe R.
Connell E.
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Connelly K.
Connolly G.
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Conteh V.
Conway R.
Cook E.
Cooke G.
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Cooper D.
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Cooray S.
Corbett C.
Corbishley A.
Cornwell J.
Corr A.
Corredera M.
Corrigan R.
Cosier T.
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Cotterill D.
Coull A.
Courtney E.
Cowen L.
Cowman S.
Cox E.
Coy K.
Cradduck-Bamford A.
Crasta S.
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Crawford A.
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Crawshaw S.
Creagh-Brown B.
Cremona J.
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Crichton C.
Crisp L.
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Crosby H.
Cross T.
Crotty S.
Cruickshank C.
Cruise J.
Cryans D.
Cui G.
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Publication venue: Springer Science and Business Media LLC
Publication date: 31/01/2024
Field of study

Dimethyl fumarate (DMF) inhibits inflammasome-mediated inflammation and has been proposed as a treatment for patients hospitalised with COVID-19. This randomised, controlled, open-label platform trial (Randomised Evaluation of COVID-19 Therapy [RECOVERY]), is assessing multiple treatments in patients hospitalised for COVID-19 (NCT04381936, ISRCTN50189673). In this assessment of DMF performed at 27 UK hospitals, adults were randomly allocated (1:1) to either usual standard of care alone or usual standard of care plus DMF. The primary outcome was clinical status on day 5 measured on a seven-point ordinal scale. Secondary outcomes were time to sustained improvement in clinical status, time to discharge, day 5 peripheral blood oxygenation, day 5 C-reactive protein, and improvement in day 10 clinical status. Between 2 March 2021 and 18 November 2021, 713 patients were enroled in the DMF evaluation, of whom 356 were randomly allocated to receive usual care plus DMF, and 357 to usual care alone. 95% of patients received corticosteroids as part of routine care. There was no evidence of a beneficial effect of DMF on clinical status at day 5 (common odds ratio of unfavourable outcome 1.12; 95% CI 0.86-1.47; p = 0.40). There was no significant effect of DMF on any secondary outcome

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