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165 research outputs found

Non-uniform recovery of left ventricular transmural mechanics in ST-segment elevation myocardial infarction

Author: AN Lieberman
DA Morrow
F David Fortuin
FE Rademakers
FJ Villarreal
G Olivetti
Giuseppe Caracciolo
GY Cho
H Lim
Haruhiko Abe
IJ LeGrice
J Chen
J Korinek
J Korinek
JE Moller
KA Reimer
KD Costa
KT Weber
Mackram F Eleid
Nisha Bhatia
P Gaudron
Partho P Sengupta
PP Sengupta
R Citro
R Mazhari
RA Nishimura
RG McKay
RM Lang
SA Mollema
Scipione Carerj
Susan Wilansky
T Vartdal
Y Li
Y Zhang
YH Park
Publication venue: BioMed Central
Publication date: 01/01/2010
Field of study

Abstract Background After a transient ischemic episode, the subendocardial region is more severely injured than outer subepicardial layers and may regain a proportionately greater degree of mechanical function in the longitudinal direction. We sought to explore left ventricular (LV) transmural mechanics in patients with ST-segment elevation myocardial infarction (STEMI) for determining the mechanism underlying recovery of global LV function after primary percutaneous coronary intervention (PCI). Methods A total of 42 patients (62 ± 11 years old, 71% male) with a first STEMI underwent serial assessments of LV longitudinal, circumferential and radial strains (LS, CS and RS) by selective tracking of subendocardial and subepicardial regions within 48 hours and a median of 5 months after PCI. LV mechanical parameters were compared with sixteen age and gender matched normal controls. Results In comparison with controls, endocardial and epicardial LS were markedly attenuated at 48 hours following PCI (P < 0.001). An improvement in LV ejection fraction (EF > 5%) following PCI was seen in 24 (57%) patients and was associated with improvement in endocardial and epicardial LS (P < 0.001 and P = 0.003, respectively) and endocardial CS (P = 0.01). Radial strain and wall motion score index, however, remained persistently abnormal. The change in endocardial LS (OR 1.2, 95% CI 1.03 to 1.42, P = 0.01) and the change in epicardial LS (OR 1.2, 95% 1.03 to 1.46, P = 0.02) were significantly associated with the improvement in LVEF, independent of the location of STEMI and the presence of underlying multivessel disease. Conclusions In patients with STEMI treated by PCI, the recovery of LV subendocardial shortening strain seen in the longitudinal direction underlies the improvement in LV global function despite persistent abnormalities in radial mechanics and wall motion score index.</p

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Directory of Open Access Journals

PubMed Central

Ultrafast Light and Electrons: Imaging the Invisible

Author: A Amunts
A Cavalleri
A Feist
A Howie
A Klug
A Sali
A Tonomura
A Tonomura
A Yurtsever
A Yurtsever
AH Zewail
AH Zewail
AH Zewail
AH Zewail
AH Zewail
AH Zewail
AH Zewail
AH Zewail
AH Zewail
AI Sabra
AV Crewe
AWP Fitzpatrick
AWP Fitzpatrick
B Barwick
B Barwick
B Steffens
C Bressler
DJ Flannigan
DJ Flannigan
E Fill
EW Müller
F Carbone
F Krausz
F Krausz
F Lépine
F Schotte
GF Mancini
H Lichte
HS Cho
HS Park
J Frank
JC Williamson
JCH Spence
JCH Spence
JM Cowley
JM Thomas
JM Thomas
JM Thomas
JM Thomas
JM Thomas
JM Thomas
JW Strutt
KT Kim
L Piazza
M Chergui
M Dantus
M Först
M Knoll
M Kociak
MA O’Keefe
MM Lin
MM Lin
MM Lin
MM Lin
MM Lin
MM Lin
MP Silverman
MT Hassan
N Gedik
N Jonge de
OH Kwon
OH Kwon
P Baum
P Baum
P Baum
PB Corkum
PD Nellist
PL Gai
PW Hawkes
R Henderson
R Henderson
R Hooke
RA Crowther
RM Glaeser
RM Glaeser
S Forsén
SA Hilbert
SR Leone
ST Park
ST Park
ST Park
TK Kim
TT Tsong
VK Jain
W Kühlbrandt
Publication venue: 'Springer Fachmedien Wiesbaden GmbH'
Publication date: 14/12/2016
Field of study

In this chapter, the evolutionary and revolutionary developments of microscopic imaging are overviewed with focus on ultrashort light and electrons pulses; for simplicity, we shall use the term “ultrafast” for both. From Alhazen’s camera obscura, to Hooke and van Leeuwenhoek’s optical micrography, and on to three- and four-dimensional (4D) electron microscopy, the developments over a millennium have transformed humans’ scope of visualization. The changes in the length and time scales involved are unimaginable, beginning with the visible shadows of candles at the centimeter and second scales, and ending with invisible atoms with space and time dimensions of sub-nanometer and femtosecond, respectively. With these advances it has become possible to determine the structures of matter and to observe their elementary dynamics as they fold and unfold in real time, providing the means for visualizing materials behavior and biological function, with the aim of understanding emergent phenomena in complex systems. Both light and light-generated electrons are now at the forefront of femtosecond and attosecond science and technology, and the scope of applications has reached beyond the nuclear motion as electron dynamics become accessible

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Caltech Authors

RNA interference approaches for treatment of HIV-1 infection

Author: A Fire
A Khvorova
A Michienzi
A Ono
A Prussia
A Singh
A Soejitno
AT Das
B Berkhout
BL Levine
BP Burke
CA Didigu
CB Wilen
D Boden
D Finzi
D Grimm
D Liu
D Siolas
D Stone
D Vlachakis
DA Maier
DA Persons
DB Kohn
DF Purcell
DH Kim
DL DiGiusto
DS Schwarz
E Cave
E Puerta-Fernandez
E Song
EB Schleifman
EE Perez
EJ Arts
EM Westerhout
F Boutimah
F Buchholz
F Christ
F Wong-Staal
G Hutter
G Hutter
GJ McIntyre
GJ McIntyre
GR Rettig
H Ebina
H Mitsuya
H Nishitsuji
H Siomi
HJ Unwalla
HP Bogerd
HS Christensen
I Sarkar
IB Hogue
J Anderson
J Chung
J Chung
J Lunzen van
J Nejepinska
J Yuan
J Zhou
J Zhou
J Zhou
J Zhou
JC Burnett
JC Burnett
JJ Eekels
JJ Eekels
JJ Eekels
JJ Rossi
JJ Rossi
JK Wong
JL Macpherson
JL Umbach
JM Jacque
JN Leonard
John C Burnett
John J Rossi
JS Pan
K Allers
K Bebenek
K Konopka
K Suzuki
K Suzuki
K Suzuki
KE Broderick
KJ Eije von
KT Gagnon
KV Morris
KV Morris
L Kordelas
L Li
L Mariyanna
L Ye
L Zaitseva
LA Wheeler
LQ Al-Mawsawi
M Aubert
M Ishaq
M Li
M Sano
M Sioud
M Tamhane
M Vaccari
M Yan
MA Kay
MA Kotterman
MA Martinez
Maggie L Bobbin
MD Krebs
MJ Buzon
MJ Li
MR Zamora
MS Souza de
MS Weinberg
MT Certo
N Holt
N Vazquez-Salat
NC Schopman
NC Schopman
NM Flynn
NM Snead
NM Snead
O Brake ter
O Brake ter
P Kumar
P Parameswaran
P Tebas
PR Gorry
PS Shah
PV Maillard
RJ Scarborough
RL Kanasty
RT Mitsuyasu
RT Mitsuyasu
S Akhtar
S Backes
S Backes
S Bivalkar-Mehla
S Knowling
S Omoto
S Rerks-Ngarm
S Shimizu
S Subramanya
S Subramanya
S Yang
SA Yukl
SD Rose
SG Deeks
SK Lee
SK Singh
SS Kim
SW Cho
T Kubo
T Nagawa
T Yamamoto
T Zhang
TA Karlsen
TJ Cradick
TL Symensma
TP Chendrimada
TS Lau
V Kulkarni
V Patel
VA Green
VR Sanghvi
W Hu
WS Park
WW Xu
X Zhang
Y Kashiwakura
Y Li
Y Pan
Y Takeuchi
YH Ping
YL Chiu
YP Liu
YP Liu
YP Liu
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2015
Field of study

HIV/AIDS is a chronic and debilitating disease that cannot be cured with current antiretroviral drugs. While combinatorial antiretroviral therapy (cART) can potently suppress HIV-1 replication and delay the onset of AIDS, viral mutagenesis often leads to viral escape from multiple drugs. In addition to the pharmacological agents that comprise cART drug cocktails, new biological therapeutics are reaching the clinic. These include gene-based therapies that utilize RNA interference (RNAi) to silence the expression of viral or host mRNA targets that are required for HIV-1 infection and/or replication. RNAi allows sequence-specific design to compensate for viral mutants and natural variants, thereby drastically expanding the number of therapeutic targets beyond the capabilities of cART. Recent advances in clinical and preclinical studies have demonstrated the promise of RNAi therapeutics, reinforcing the concept that RNAi-based agents might offer a safe, effective, and more durable approach for the treatment of HIV/AIDS. Nevertheless, there are challenges that must be overcome in order for RNAi therapeutics to reach their clinical potential. These include the refinement of strategies for delivery and to reduce the risk of mutational escape. In this review, we provide an overview of RNAi-based therapies for HIV-1, examine a variety of combinatorial RNAi strategies, and discuss approaches for ex vivo delivery and in vivo delivery

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PubMed Central

eScholarship - University of California

Approaches in biotechnological applications of natural polymers

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Publication venue: 'American Institute of Mathematical Sciences (AIMS)'
Publication date: 01/01/2016
Field of study

Natural polymers, such as gums and mucilage, are biocompatible, cheap, easily available and non-toxic materials of native origin. These polymers are increasingly preferred over synthetic materials for industrial applications due to their intrinsic properties, as well as they are considered alternative sources of raw materials since they present characteristics of sustainability, biodegradability and biosafety. As definition, gums and mucilages are polysaccharides or complex carbohydrates consisting of one or more monosaccharides or their derivatives linked in bewildering variety of linkages and structures. Natural gums are considered polysaccharides naturally occurring in varieties of plant seeds and exudates, tree or shrub exudates, seaweed extracts, fungi, bacteria, and animal sources. Water-soluble gums, also known as hydrocolloids, are considered exudates and are pathological products; therefore, they do not form a part of cell wall. On the other hand, mucilages are part of cell and physiological products. It is important to highlight that gums represent the largest amounts of polymer materials derived from plants. Gums have enormously large and broad applications in both food and non-food industries, being commonly used as thickening, binding, emulsifying, suspending, stabilizing agents and matrices for drug release in pharmaceutical and cosmetic industries. In the food industry, their gelling properties and the ability to mold edible films and coatings are extensively studied. The use of gums depends on the intrinsic properties that they provide, often at costs below those of synthetic polymers. For upgrading the value of gums, they are being processed into various forms, including the most recent nanomaterials, for various biotechnological applications. Thus, the main natural polymers including galactomannans, cellulose, chitin, agar, carrageenan, alginate, cashew gum, pectin and starch, in addition to the current researches about them are reviewed in this article.. }To the Conselho Nacional de Desenvolvimento Cientfíico e Tecnológico (CNPq) for fellowships (LCBBC and MGCC) and the Coordenação de Aperfeiçoamento de Pessoal de Nvíel Superior (CAPES) (PBSA). This study was supported by the Portuguese Foundation for Science and Technology (FCT) under the scope of the strategic funding of UID/BIO/04469/2013 unit, the Project RECI/BBB-EBI/0179/2012 (FCOMP-01-0124-FEDER-027462) and COMPETE 2020 (POCI-01-0145-FEDER-006684) (JAT)

Universidade do Minho: RepositoriUM

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Study of multi-muon events produced in p\bar{p} interactions at \sqrt{s}=1.96 TeV

Author: Aaltonen T
Adelman J
Ahmed S
Ahmed S
Ahmed S.
Alam M. S.
Alam MS
Alam MS
Albert J
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Amerio S
Amidei D
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Apresyan A
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Artikov A
Ashmanskas W
Azzolini V
Azzolini V
Azzolini V
Azzolini V.
Azzurri P
Badgett W
Band H. R.
Band HR
Band HR
Band HR
Band HR
Banerjee S
Banerjee S
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Banerjee S.w.
Barnett BA
Bartsch V
Beecher D
Behari S
Bellettini G
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Benitez JF
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Bhuyan B
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Bhuyan B
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Bizjak I
Blocker C
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Cabrera S
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Davies T
de Barbaro P
DELL'ORSO MAURO
Della Ricca G
Della Ricca G
Della Ricca G
Della Ricca G.
Demortier L
Deng J
Deninno M
di Giovanni GP
Di Ruzza B
Dingfelder JC
Dittmann JR
DONATI SIMONE
Donini J
Dorfan J
Dorigo T
Drummond B. W.
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Publication venue
Publication date: 01/01/2010
Field of study

68 pages, 46 figures, 11 tables. Submitted to Phys. Rev. D. Removed typos from the authors' listWe report the results of a study of multi-muon events produced at the Fermilab Tevatron collider and acquired with the CDF II detector using a dedicated dimuon trigger. The production cross section and kinematics of events in which both muon candidates are produced inside the beam pipe of radius 1.5 cm are successfully modeled by known processes which include heavy flavor production. In contrast, we are presently unable to fully account for the number and properties of the remaining events, in which at least one muon candidate is produced outside of the beam pipe, in terms of the same understanding of the CDF II detector, trigger, and event reconstruction.Peer reviewe

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A922 Sequential measurement of 1 hour creatinine clearance (1-CRCL) in critically ill patients at risk of acute kidney injury (AKI)

Author: Abbott TE
Abdallah RI
Abdel-Aal IR
Abdelmonem SA
Abdo WF
Abellan AN
Abellán AN
Abellán AN
Abellán AN
Abrams ST
Ackerley C
Acuña M
Adda M
Adhikari NK
Adriano G
Adrie C
Affatato R
Affatato R
Afonso-Rivero D
Agarossi A
Agarwal LK
Ageeva T
Agrawal R
Aguayo-DeHoyos E
Aguilar AL
Aguilar-Alonso E
Aguilar-Alonso E
Aguilar-Alonso E
Aguirregabyria M
Ahmadnia E
Ahn C
Ahn JY
Ahn JY
Ahn MY
Ahn MY
Aitken LM
Akalaev R
Akbarzadeh A
Akcan-Arikan A
Akhlagh SH
Akhtar N
AKI Research Group
Akiduki N
Akin S
Akizuki N
Akkoc T
Ala-Kokko T
Alanio A
Albaiceta GM
Albaladejo P
Alberto F
Albuisson E
Alcala MA
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Aldabo-Pallas T
Aldana NN
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Alegría L
Alejandro R
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Algieri I
Algora-Weber A
Alhamdi Y
Aliaga FA
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Almudena PM
Almudevar PM
Almudevar PM
Almudévar PM
Altıntas ND
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Alzola LM
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Amaro R
Amato MB
Ambler M
Amerongen MP
Amininejad T
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Anand RK
Andersen LW
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Annane D
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Antoniadou A
Antonio C
Antonucci E
Antón DG
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Appiani F
Aquevedo A
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Araujo NJ
Araujo VF
ARIAM registry of adult cardiac surgery
ARIAM-ANDALUCIA
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Cook DJ
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Cordeiro CP
Cordero M
Cordolcini V
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Corradi F
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Correa-Chamorro E
Corte FD
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Costanzo E
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Creagh-Brown B
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Crimella F
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Cuthbertson BH
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de Abreu MG
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de la Fuente MV
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de Molina FJ
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Filho CA
Filho CA
Filho CA
Filipe E
FINNRESUSCI Study Group
Fischer G
Fleischmann E
Fless K
Floccard B
Flowers E
Follin A
Follin A
Fong KY
Fontaiña LP
Fontana V
Fontenot T
Forel JM
Forni L
Forni L
Forni LG
Forni LG
Forni LG
Fournel E
Fox B
Franchi P
Francioni JE
Francioni JE
Franco JF
Frantzeskaki F
Frantzeskaki F
Frat JP
Frat JP
Frat JP
Freile MT
Frenzel T
Frigeni B
Frithiof R
Fritz C
FROG ICU Investigators
Fromentin M
Frontera PR
Fuentes M
Fumagalli F
Fumagalli F
Fumis RR
Fushimi K
Gabán-Díez Á
Gadgil S
Gaide-Chevronnay L
Gainnier M
Gaite FB
Gaizauskas E
Gajic O
Galache JA
Gallego-Corpa AI
Gameiro J
Gancedo CH
Gandini L
Gando S
Gando S
Gando S
Gando S
Gandola A
Gandolfi S
Ganuza MS
Garcia IP
Garcia IP
Garcia M
Garcia PK
Garcia-Alvarez JM
Garcia-Alvarez JM
Garcia-Delgado M
Garcia-Gigorro R
García MF
García-Martínez MV
García-Olivares P
Garnacho-Montero J
Garrido BB
Garrido BB
Garrido EM
Garrouste M
Gaspard N
Gasparovic V
Gattinoni L
Gaudard P
Gavranovic Z
Gavrychenko D
Gayat E
Geantot MA
Gemmell L
Gemmell LK
Genc D
Genève C
Georgopoulos D
Geri G
GETGAG Working Group
GETGAG/SEMICYUC
Ghabina S
Ghazal S
Gherli T
Gherli T
Ghosh S
Giannantonio M
Giannopoulos A
Giesinger RE
Gigorro RG
Gil EM
Gimenez J
Gimillo MR
Ginés AS
Gioia A
Girbes AR
Girotto V
Gkirkas K
Glogoski MZ
Gobert F
Godinho I
Godoy K
Goldsworthy M
Golovnya E
Gomes AA
Gomez C
Gomez SE
Gommers D
Gommers D
Gonzalez CA
Gonzalez JA
Gonzalez V
Gonzalez-Engroba R
González AS
González BS
González JC
González-Jiménez AI
Gonçalves B
Goodwin S
Gopcevic A
Gordillo-Brenes A
Gordo F
Gordon M
Gordon M
Gorjup V
Goto T
Goto T
Gottlieb J
Gouveia J
Gracia RM
Gradišek P
Granada RM
Granados PR
Grando M
Granger CL
Grangé S
Grangé S
Grangé S
Granillo JF
Grassi L
Grasso S
Greco E
Green RS
Greer M
Gregory S
Grelon F
Grelon F
Grelon F
Grevelink M
Grossestreuer A
Guanziroli M
Guarracino F
Guarracino F
Gubianas CM
Guerrero AP
Guerrero JE
Guerrero-Lopez F
Guerrero-López F
Guervilly C
Guidet B
Guillamon LN
Guillen JA
Guillot M
Guitard PG
Guitard PG
Guitard PG
Gul F
Gupta A
Gupta D
Gupta O
Gustad LT
Gutierrez LA
Gutiérrez-Pizarraya A
Guérin C
Guérin C
Guérin C
Gálvez V
Géri G
Gómez LC
Gómez-Jiménez C
Gómez-Jiménez C
Güven G
Ha JK
Hadley JS
Haghbin S
Haines R
Hala P
Hall D
Hallows G
Hallows G
Hamilton A
Han HS
Han SH
Han SH
Handler E
Hanekom S
Haniffa R
Hanna AA
Haritydi T
Harm S
Harridge SD
Harrison D
Harrison M
Hart N
Hart R
Hartmann J
Hashimoto Y
Hassanin H
Hatakeyama J
Hatib F
Hawkins K
Hayakawa M
Hayakawa M
Hayakawa M
Hayakawa M
Hayakawa M
Hayashi K
He X
Healey AJ
Hebert P
Hegazy S
Hellevuo H
Helmy TA
Helyar S
Helyar S
Hempel D
Henderson MA
Hendra H
Henschel B
Heras G
Hernandis V
Hernández A
Hernández AA
Hernández AA
Hernández AA
Hernández AA
Hernández AA
Hernández AA
Hernández G
Hernández-Tejedor A
Herpain A
Herrera AN
Herrera AN
Herrera AN
Herrera AN
Herrera AN
Herrera AN
Herruzo-Aviles A
Heunks LM
Hewitt H
Heyne T
Hickey S
Hidalgo C
Hikasa Y
Hillier SD
Himmel Y
Himpe D
Hinojosa-Perez R
Hirata A
Hirayama T
Hirohata S
Hodgson LE
Hodgson LE
Hofmeijer J
Hollands S
Hom H
Hopkins PA
Hopkins PA
Hoppu S
Hoppu S
Horkan CM
Horstmann C
Horton A
Horvat A
Hou DS
Houzé S
Houzé S
Howes D
Hozhabri K
Hrachovina M
Hraiech S
Hravnak M
Hu HC
Hua Y
Hualde JB
Hualde JB
Hualde JB
Hualde JB
Hualde JB
Hualde JB
Huang CH
Huang WC
Huang WC
Huang WC
Huang WC
Hubbard A
Huber W
Huddart S
Hull AM
Hung CY
Hung WT
Hung WT
Hung WT
Hung WT
Huot B
Husheer SL
Hutchings S
Hutchison R
Hwang GS
Hwang GS
Ibañes PG
Ibsen M
Idei M
Idei M
Idone FA
Iesu E
Iesu E
Iglesias-Santiago A
Ignacio ML
Iida A
Iijima H
Ilan R
Ilyina V
Imanaka H
Inaloo S
Ince C
Iotti GA
Iotti GA
Iotti GA
IPREA Study Group
Irazabal JM
Irazabal JM
Ishimatsu S
Itenov TS
Iwamoto M
Izawa M
Izdes S
Jaber S
Jacky A
Jacobs FM
Jacques T
Jaffal K
Jamali S
Jang BH
Janotka M
Janotka M
Janotka M
Jansen D
Jansen N
Japan Septic Disseminated Intravascular Coagulation (JSEPTIC DIC) study group
Jardim JJ
Jardim M
Jareño A
Javadpour S
Jayasinghe S
Jean-Baptiste S
Jean-Baptiste S
Jensen AE
Jensen JU
Jeon YD
Jeon YD
Jeong IY
Jeong IY
Jeong WY
Jeong WY
Jian Z
Jiao LR
Jibaja M
Jimenez-Herrera MF
Jiménez GJ
Jo YH
Joachim J
Jochmans S
John G
Jonas M
Jonas M
Jonas M
Jones C
Joshi R
Joshi V
Jovaisa T
JSEPTIC (Japanese Society of Education for Physicians and Trainees in Intensive Care) Clinical Trial Group
Juan WC
Juanas CA
Judickas S
Juez A
Juliarena A
Jun IG
Jun IG
Jung K
Jung KW
Junior JM
Kaczirek K
Kaese S
Kalani N
Kalenka A
Kalfon P
Kamali E
Kaminsky GE
Kaneko M
Kang M
Kang M
Kang PL
Kang PL
Kang PL
Kang PL
Kang Y
Kao KC
Kappler F
Kara A
Karachi F
Karanjia N
Karbing DS
Karsten E
Kasdan H
Kashiya S
Kashyap R
Katabami K
Katabami K
Katabami K
Katabami K
Katira BH
Kavanagh BP
Kawamura N
Kawano S
Kay FU
Kayaaslan B
Kayambu G
Kazutoshi F
Ke MW
Ke MW
Keep J
Keep J
Keller E
Kellner F
Kelly JM
Kenardy J
Keough E
Kerhuel L
Kerr C
Kezyte G
Khadjibaev A
Khaliq W
Khine H
Kim DJ
Kim HJ
Kim JM
Kim JM
Kim JW
Kim KS
Kim KS
Kim KS
Kim KS
Kim MH
Kim MH
Kim W
Kimmoun A
King HS
Kinnear J
Kirakli C
Kirakli C
Kirca H
Kirman M
Kirwan CJ
Kittnar O
Klapsing P
Klaus DA
Kleinpell R
Kluge S
Knafelj R
Knight LD
Ko JI
Ko SB
Kobayashi A
Koco E
Kodate A
Kodate A
Kodate A
Kokkini S
Kolnikova I
Komuro T
Kondili E
Kongpolprom N
Kooner G
Kostalas M
Kosuk ME
Kotsopoulos A
Kou PS
Kouatchet A
Kovacikova L
Kox M
Kraegpoeth A
Krenn CG
Krishna B
Kristof J
Kruger A
Kruger A
Krüger A
Ku NS
Ku NS
Kubik M
Kubota K
Kuebler WM
Kulaga EV
Kulkarni AP
Kumari BK
Kumbamu A
Kunze-Szikszay N
Kurmukov IA
Kurth T
Kurtz P
Kurtz P
Kwon HM
Kwon HM
Kwon WY
Kwon WY
Kwon WY
Kye YC
Kyle UG
Kyle UG
Labaune MA
Labra C
Lacerda P
Laerkner E
Lafaurie M
Lafuente E
Lagonidis D
Lagos R
Lahmer T
Lai CC
Lai CH
Lake K
Lan SK
Lapteva K
Lapteva K
Larsson JS
Latini R
Latini R
Latini R
Latorre J
Lattuada M
Lattuada M
Lau YH
Laurent A
Lauretta MP
Laureys S
Lavrentieva A
Lawrence N
Lazzeri EH
Le Brocque R
Lebherz-Eichinger D
Lebiedz P
Lebrón-Gallardo M
Lebut J
Lechner C
Lee C
Lee CT
Lee DS
Lee DS
Lee EY
Lee JH
Lee S
Lee SH
Lee SJ
Lee WY
Lee YJ
Lee YJ
Legrand M
Legrand M
Legrand M
Legriel S
Leitao AL
Leite RT
Leonard H
Leone M
Leone M
Lerma FA
Lesmes SP
Lesmes SP
Lesmes SP
Lesmes SP
Lesmes SP
Lesmes SP
Letizia T
Levrat Q
Levy B
León JL
León JP
León JP
León JP
Lheureux O
Lheureux O
Lheureux O
Lheureux O
Li R
Li SH
Liao X
Lichtenstein D
Lim TH
Limuti R
Lin KC
Lin KC
Lin KC
Lin KC
Lin KL
Lin PH
Lin SC
Lin SC
Lin SC
Lin SC
Lin WC
Lin WC
Lipcsey M
Lischinsky A
Lissonde F
Lissonde F
Litchfield K
Liu CP
Liu CP
Liu CP
Liu CP
Liu D
Llaurado-Serra M
Llorente B
Llorente MÁ
Lobato MS
Lobo-Civico A
Loizou C
Lombardo MD
Londoño JG
Longani N
Longhi L
Lopes JA
Lopez GD
Lopez R
Lopez-Caler C
Lopez-Gude MJ
Lorini L
Lortat-Jacob B
Lortat-Jacob B
Lotay R
Loudet CI
Louf-Durier A
Louf-Durier A
Louis B
Lourido CM
Lozano JA
Lozano JA
Lucendo AP
Lucendo MA
Luciani A
Lucinio NM
Luini M
Luján J
Lukaszewicz AC
Luna RR
Lundeg G
Lusk J
Lusk J
Ly H
Lázaro AS
López AR
López L
López MA
Macfarlane B
MacKay A
MacKay A
Mackey G
Mackey G
MacPhee I
Macrì M
Madueño VP
Maekawa K
Maekawa K
Maekawa K
Maekawa K
Maertens B
Maggiorini M
Maghsoudi B
Magnanimi E
Magnoni S
Magret M
Mainardi JL
Maistry N
Maitra S
Makiko S
Malagurski B
Malek F
Malo LR
Maly M
Malyshev A
Manca T
Manca T
Mancebo J
Mancebo J
Mancebo J
Mancino A
Mandal K
Mantz J
Mantz J
Mar GY
Mar GY
Mar GY
Mar GY
Marca L
Marca L
Marcos-Zambrano LJ
Mariani M
Mariman A
Marin-Mateos H
Marine-Vidal J
Mariotte E
Mariotti L
Marmanidou K
Marmanidou K
Marqués-Miñana MR
Marra C
Marrazzo F
Marshall P
Martin AD
Martin AD
Martin C
Martin S
Martin-Gallardo F
Martin-Villen L
Martin-Vivas A
Martinez AD
Martinez FH
Martinez M
Martinez MP
Martinez-Lopez P
Martinez-Reyes L
Martí AT
Martín MC
Martín-Loeches I
Martín-Loeches I
Martínez F
Martínez L
Martínez L
Martínez M
Martínez MP
Martínez MV
Martínez NA
Martínez-Carmona JF
Marín-Corral J
Mas A
Masclans JR
Masjedi M
Masjedi M
Maslove D
Masson S
Masson S
Masson S
Mata PJ
Matamis D
Matamis D
Matamis D
Mateos HM
Mates M
Mathew R
Matsuda Y
Matsukubo S
Mauri T
Mayr U
Mazo C
Mazurenko G
Mazza E
McCormick B
McCue C
McHugh L
Mckinlay J
McNamara PJ
McNelly AS
McPhail MJ
McWilliams D
Mebazaa A
Mebazaa A
Mecklenburg A
Medar S
Mehl A
Meissonnier J
Mejías CR
Mellis C
Melnyk L
Melo N
Mendes A
Mendez MC
Mendonca AV
Mendsaikhan N
Menendez R
Mengelle C
Mercat A
Mercat A
Mercat A
Mergulhão PJ
Merino-Vega D
Messenger D
Mezidi M
Mezidi M
Michel L
Midwinter MJ
Mignot T
Miguelena PR
Mihara Y
Millar M
Mimoun M
Mimoz O
Min A
Min HJ
Mingone D
Mion MM
Mira JP
Mirabella L
Miranda F
Miranda R
Mirković T
Mistry M
Mistry N
Mitchell M
Mitchell S
Mizobuchi S
Mizugaki A
Mizugaki A
Mlcek M
Moerer O
Moffatt S
Moggia F
Mohamed AN
Mohammed HM
Mohan R
Mohankumar L
Mojoli F
Mojoli F
Mojoli F
Moles SI
Molina JA
Molina R
Monchi M
Mongkolpun W
Mongodi S
Monnet X
Monroy NS
Monsalvo S
Montejo-González JC
Montenegro AP
Montenegro WS
Montero JG
Montero RM
Montesinos-Cerro N
Montgomery HE
Montini E
Montoya AA
Montravers P
Montravers P
Moon YJ
Moon YJ
Moore M
Mora-Ordoñez J
Mora-Ordóñez JM
Moraes RB
Morais CC
Morales RC
Moreira T
Morimatsu H
Morimoto T
Morman D
Moro F
Morán I
Motos A
Mouaci A
Mourad M
Mourvillier B
Moxham J
Muhammad JB
Mukherjee DN
Muncharaz AB
Munteanu G
Murakami H
Murakami H
Muscedere J
Muscedere J
Mutlu H
Muñoz JJ
Muñoz JM
Muñoz-Muñoz JL
Márquez MP
Mézière G
Møller MH
Na SJ
Nadel S
Nadkarni V
Nagib H
Naito T
Nakagawa S
Nakao A
Nakataki E
Nakataki E
Namiki M
Namiki M
Nandha R
Naran P
Nataf P
Naumann DN
Navarro-Guillamón L
Naz I
Neels H
Neto AS
Neuville M
Neuzil P
Neuzil P
Neves M
Ng L
Nicolini EA
Nicolini F
Nicolini F
Nieto B
Nieto OR
Nikhilesh J
Nishigaki A
Nishimura M
Nishimura M
Nisula S
Nobile L
Nobile L
Nobile L
Noda E
Nomura T
Nomura T
Noon A
Noon A
Noriega SK
Nosaka N
Nouer SA
Nouris C
Nouris C
Nouris C
Noursadeghi M
Noval RL
Novelli D
Noč M
Nseir S
Nuevo-Ortega P
Nunes J
Nunes RS
Nuvials X
Nuvials X
Nyunga M
Nóbrega JJ
O'Dwyer MJ
Obukhova O
Oddo M
Ode S
Oguzhan K
Oh J
Ohta Y
Oikonomou M
Oikonomou M
Okada Y
Okahara S
Okamoto H
Okayama Research Investigation Organizing Network (ORION)investigators
Olaechea P
Olavarria E
Olea-Jiménez V
Olivares F
Olkkola KT
Ong C
Ono Y
Ono Y
Ono Y
Ono Y
Onodera M
Onodera M
Oobayashi W
Orden VA
Ori C
Orlando A
Orlando A
Orlando A
Orlando S
Orlowski S
Orozco V
Ortiz AB
Ortolano F
Ostadal P
Ostadal P
Ostadal P
Ostermann M
Otani N
Oto J
Oto J
Otulakowski G
Ovnanian V
Ozkarakas H
Padeniya A
Padilla YS
Pakhare A
Paktoris-Papine S
Paldusová B
Palencia E
Palencia E
Pallás TA
Palomar M
Palomar M
Panafidina V
Panciera G
Pannu JK
Papazian L
Pappachan J
Paramythiotou E
Paramythiotou E
Park CM
Park CM
Park J
Park JS
Park M
Park MJ
Parker C
Parkin MS
Parlevliet KL
Parpibaev F
Parry SM
Parslow R
Pascual OA
Pascual OA
Pascual T
Pasha SA
Pastor EE
Patel B
Patel C
Patil VP
Patiño JA
Patrigeon RG
Patruno A
Pattnaik SK
Paul M
Paula MP
Paver N
Pawar S
Payen D
Payen JF
Payne D
Paños-Espinosa C
Peden C
Peiretti MA
Pekkarinen PT
Pelisson FG
Pellin-Ariño JI
Pelosi P
Peláez C
Penavic LV
Penichet SM
Pennisi MA
Peralvo-Bernat M
Perbet S
Pereira CA
Pereira M
Pereira SM
Pereira UV
Perez C
Perez JC
Perez JL
Perez LP
Perez M
Perez-Borrero L
Perez-Borrero L
Perez-Borrero L
Perez-Vela JL
Perinel S
Perinel S
Perivolioti E
Perner A
Perner A
Persona P
Pertuz ED
Pertuz ED
Pertuz ED
Pertuz ED
Pesonen E
Peters K
Petrova MV
Petsikas D
Pettilä V
Pettilä V
Pham T
Pham T
Pham T
Pham T
Philips BJ
Phongpagdi P
Pi-Guerrero M
Pickkers P
Pickkers P
Picoita F
PICS- HCPA: Programa Intrahospitalar de Combate à Sepse do Hospital de Clínicas de Porto Alegre
Pienovi R
Pierce C
Pifferi S
Pinsky M
Pinto JL
Piquilloud L
Piquilloud L
Piquilloud L
Pirracchio R
Pirracchio R
Pirracchio R
Piñol M
Piñol-Tena A
Plebani M
Plouhinec V
Plug Working Group
PLUG working group
PLUG Working Group
PLUG Working Group
PLUG Working Group
Plug working group
Podlepich V
Podlepich V
Pognuz ER
Poissy J
Poitou T
Pompeo MS
Pons S
Pont T
Portillo IP
Portillo JH
Post E
Post M
Pottecher J
Poukkanen M
Powell-Tuck J
Pozzebon S
Pozzi M
Pozzi M
Pozzi M
Prabu N
Prada DA
Pratikaki M
Pravettoni D
Prazeres PH
Preau S
Preece J
Preiser JC
Price RD
Prieto J
Privato E
Prosperi M
Prowle JR
Prīdāne S
PS-ICU Group
Psarologakis C
Puerto-Morlán A
Pugliese F
Pujol LM
Pulham RA
Pulitano' SM
Pusapati R
Puthucheary ZA
Puthucheary ZA
Putzu A
Puybasset L
Pérez A
Pérez AG
Pérez H
Pérez HR
Pérez HR
Pérez LP
Pérez LP
Pérez LP
Qiu H
Quinart A
Quintana S
Quintana S
Quintel M
Quinza A
Rabello L
Radjou A
Radu V
Rai S
Ramazanoglu A
Ramelli A
Ramelli A
Ramirez JR
Ramirez P
Ramirez P
Ramirez V
Ramnarayan P
Ramnarayan P
Ramos A
Ramos JV
Ramos JV
Ramos JV
Ramírez CS
Ramírez CS
Ramírez JR
Ranse K
Ranzani OT
Rapid Diagnosis of Infections in the Critically Ill Team
Rattray J
Raurich JM
Ravasi S
Rawal J
Ray B
Ray BR
Raymond T
Recker F
Recuerda M
Redfors B
Rees SE
Reeves E
Reginster JY
Reichenspurner H
Reinikainen M
Reis A
Reiter A
Rello J
Renault A
Renes-Carreño E
Renuka S
Repessé X
Resche-Rigon M
Restrepo MI
Reusch S
ReVA Research Network and the PROVE Network Investigators
Revel N
Revuelto-Rey J
Rey JR
Reyes LF
Rezai F
Riad Z
Rialp G
Richard C
Richard JC
Richard JC
Richard JC
Richard JC
Richard JC
Richard JC
Richardson S
Ricksten SE
Rico J
Rico T
Ridi S
Riera J
Riera J
Riera SQ
Rigal R
Righy C
Rigol M
Rigon MR
Rincon L
Rios-Toro JJ
Riozzi P
Riozzi P
Ristagno G
Ristagno G
Ristagno G
Rivas RF
Rivas RF
Riveiro M
Rivera-Fernandez R
Rivera-Fernandez R
Rivera-Romero L
Rizoli S
Rizos M
Roasio A
Robaglia D
Robert R
Robles CM
Roca JM
Rocha LL
Rodrigues DP
Rodrigues NJ
Rodriguez A
Rodriguez P
Rodriguez-Biendicho A
Rodriguez-Fernandez S
Rodríguez FG
Roesthuis L
Rogero S
Rolin N
Rolla F
Rolland-Debord C
Romero DG
Romero I
Romero JC
Romero JC
Romero JC
Romero JC
Romeu JD
Rood PJ
Ros Martínez J
Rosario LE
Rosario LE
Rosario LE
Rosario LE
Rosario LE
Rosario LE
Rossetti AO
Rossi S
Rossini P
Rosstalnaya A
Rota L
Roth GA
Rottoli MR
Rotzel HB
Rousseau AF
Routsi C
Rouw N
Rouzé A
Rowlerson A
Ruberto F
Rubiera M
Rubio RJ
Rudiger A
Ruffini C
Ruffini C
Ruijter A
Ruiz A
Ruiz BL
Ruiz FC
Ruiz J
Ruiz-Ramos J
Ruiz-Rodriguez JC
Ruiz-Rodríguez JC
Ruiz-Ruano RDEL
Runge I
Runge I
Runge I
Rutherford WB
Rutten AM
Rydingsward JE
Saadat F
Sabetian G
Sabeļņikovs O
Sabirov D
Sadamoto Y
Sadamoto Y
Sadamoto Y
Saeed S
Saha T
Saigal S
Saito M
Saito N
Saitou N
Sakai Y
Sakieva FI
Sakuma M
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Sales G
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Sawamura A
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Scala S
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Schmidt M
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Student Research Committee - Shiraz University of Medical Sciences
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Taccone FS
Taccone FS
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Taccone FS
Taggu A
Taggu A
Takahashi H
Takaki S
Takaki S
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Takeda M
Takei T
Takei T
Talan L
Tamura T
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Tanaka S
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Tapponnier R
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Tavazzi G
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Telli S
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Terzi N
Terzi N
Terzi N
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Tonetti T
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Torrent RL
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Torriglia F
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Torsvik M
Tosi F
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Trapp O
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Traynor T
Trefler S
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Vallverdu M
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Yamamoto H
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Zaien I
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Zani D
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Zepeda EM
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Zerva L
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Zhou JC
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Zogheib E
Zogheib E
Zogheib E
Zullino V
Zwaag J
Zýková I
Álvarez JT
Álvarez-Lerma F
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2016
Field of study

Meeting abstrac

University of Toronto Research Repository

Serveur académique lausannois

PEARL (Univ. of Plymouth)

Queen Mary Research Online

Crossref

Springer - Publisher Connector

VBN

Archivio istituzionale della ricerca - Alma Mater Studiorum Università di Bologna

Radboud Repository

St George's Online Research Archive

Iron Behaving Badly: Inappropriate Iron Chelation as a Major Contributor to the Aetiology of Vascular and Other Progressive Inflammatory and Degenerative Diseases

Author: A Abbott
A Abou-Raya
A Aljandali
A Ambesi-Impiombato
A Aydin
A Balcerczyk
A Besarab
A Brzezinski
A Campbell
A Carrillo-Vico
A Cavalli
A Chattopadhyay
A Chattopadhyay
A Cherubini
A Dey
A Doms
A Donovan
A Donovan
A Dávalos
A Gaeta
A Garny
A Gnjec
A Gomes
A Gopalakrishnan
A Hald
A Henney
A Hirayama
A Hoffmann
A Huber
A Hugman
A Iannetti
A Ide-Ektessabi
A Jacobs
A Jeyabalan
A Kahvejian
A Karrar
A Kasztler
A Kibel
A Kocyigit
A Kotha
A Kumral
A Lass
A Lecube
A Lewén
A Lotery
A Maggio
A Malek
A Malik
A Mantovani
A Matsuzawa
A Mitra
A Monge
A Murakami
A Murakami
A Murakami
A Murakami
A Mutti
A Nijnik
A Nunomura
A Nunomura
A Patt
A Persson
A Pietrangelo
A Piga
A Pirat
A Post
A Pradhan
A Protti
A Rattner
A Ravati
A Rehman
A Reynolds
A Richmond
A Roetto
A Roetto
A Rostom
A Rumbold
A Russo
A Rötig
A Saltelli
A Saltelli
A Sandek
A Sassano
A Scalbert
A Scalbert
A Scalbert
A Sica
A Smahi
A Sola
A Stintzi
A Szewczyk
A Taguchi
A Tedgui
A Terman
A Terman
A Terman
A Undas
A Virdis
A Wagner
A Wagner
A Wagner
A Wagner
A Wojas-Pelc
A Wong
A Xu
A Yoritaka
A Yoshimura
A-L Barabási
AA Andreadis
AA Borisy
AA Farooqui
AA Qutub
AA Qutub
AA Vlessis
AB Nathens
AB Parsons
AB Parsons
AB Thompson
AB Thomson
AC Bayne
AC Bharti
AC Cave
AC Mello Filho
AD d'Hardemare
AD de Silva
Ad hoc committee on systemic lupus erythematosus response criteria for fatigue
ADL van der
AE Aust
AE Baue
AE Finefrock
AE Heazell
AE Heazell
AE Kartikasari
AEC Ihekwaba
AEC Ihekwaba
AF Tramontano
AH Berg
AH Koeppen
AH Koeppen
AH Tong
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AI Bush
AI Bush
AI Bush
AI Faden
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AJ Ghio
AJ Ghio
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AL Beal
AL Hemdahl
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AL Hopkins
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AL Sirén
AL Takeda
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AM Borzychowski
AM Choi
AM Dolga
AM Elneihoum
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AM Feist
AM Harvey
AM Jenkinson
AM Lin
AM Samuni
AM Snyder
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AN Tabah
AP Bolger
AP Breen
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AR Kallianpur
AR Martin
AR Ness
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AS Wierzbicki
AT McKie
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AV Perkins
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AW Maresso
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AY Sun
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B Halliwell
B Halliwell
B Halliwell
B Halliwell
B Halliwell
B Halliwell
B Halliwell
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B Kwak
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B Pradines
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The Long-Term Intervention with Pravastatin in Ischaemic Disease (LIPID) Study Group
TJ Gibson
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TK Kvien
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V Adam-Vizi
V Adam-Vizi
V Atanasiu
V Braun
V Braun
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X Zhang
X Zhu
X Zhu
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XM Yuan
XM Yuan
XP Huang
Y Almog
Y Avramovich-Tirosh
Y Bao
Y Bdolah
Y Chen
Y Christen
Y Curin
Y Deugnier
Y Deugnier
Y Engin-Üstün
Y Ge
Y Gilgun-Sherki
Y Haruna
Y Honda
Y Hua
Y Ikeda
Y Jiao
Y Jung
Y Ke
Y Ke
Y Kohgo
Y Kohgo
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Y Li
Y Okatani
Y Okatani
Y Sai
Y Sai
Y Sun
Y Takada
Y Wang
Y Wang
Y Wei
Y Wei
Y Wu
Y Wu
Y Zhang
Y Zhang
Y Zhang
Y Zhao
Y Zheng
YE Henrotin
YF Chu
YH Lee
YH Suh
YH Wei
YJ Surh
YJ Surh
YJ Surh
YK Wu
YM Kim
YS Keum
YS Sohn
YX Ma
YZ Fang
Z Cai
Z Cai
Z Cheng
Z Pei
Z Serdar
Z Tong
Z Tong
Z Yu
Z Zhang
ZD Liu
ZD Liu
ZE Karanjawala
ZE Suntres
ZI Cabantchik
ZZ Chong
ZZ Chong
Publication venue
Publication date: 09/08/2008
Field of study

The production of peroxide and superoxide is an inevitable consequence of aerobic metabolism, and while these particular "reactive oxygen species" (ROSs) can exhibit a number of biological effects, they are not of themselves excessively reactive and thus they are not especially damaging at physiological concentrations. However, their reactions with poorly liganded iron species can lead to the catalytic production of the very reactive and dangerous hydroxyl radical, which is exceptionally damaging, and a major cause of chronic inflammation. We review the considerable and wide-ranging evidence for the involvement of this combination of (su)peroxide and poorly liganded iron in a large number of physiological and indeed pathological processes and inflammatory disorders, especially those involving the progressive degradation of cellular and organismal performance. These diseases share a great many similarities and thus might be considered to have a common cause (i.e. iron-catalysed free radical and especially hydroxyl radical generation). The studies reviewed include those focused on a series of cardiovascular, metabolic and neurological diseases, where iron can be found at the sites of plaques and lesions, as well as studies showing the significance of iron to aging and longevity. The effective chelation of iron by natural or synthetic ligands is thus of major physiological (and potentially therapeutic) importance. As systems properties, we need to recognise that physiological observables have multiple molecular causes, and studying them in isolation leads to inconsistent patterns of apparent causality when it is the simultaneous combination of multiple factors that is responsible. This explains, for instance, the decidedly mixed effects of antioxidants that have been observed, etc...Comment: 159 pages, including 9 Figs and 2184 reference

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Pan-cancer analysis of whole genomes

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The ICGC/TCGA Pan-Cancer Analysis of Whole Genomes Consortium View Correspondence (jump link)
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Publication date: 11/12/2019
Field of study

Cancer is driven by genetic change, and the advent of massively parallel sequencing has enabled systematic documentation of this variation at the whole-genome scale(1-3). Here we report the integrative analysis of 2,658 whole-cancer genomes and their matching normal tissues across 38 tumour types from the Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium of the International Cancer Genome Consortium (ICGC) and The Cancer Genome Atlas (TCGA). We describe the generation of the PCAWG resource, facilitated by international data sharing using compute clouds. On average, cancer genomes contained 4-5 driver mutations when combining coding and non-coding genomic elements; however, in around 5% of cases no drivers were identified, suggesting that cancer driver discovery is not yet complete. Chromothripsis, in which many clustered structural variants arise in a single catastrophic event, is frequently an early event in tumour evolution; in acral melanoma, for example, these events precede most somatic point mutations and affect several cancer-associated genes simultaneously. Cancers with abnormal telomere maintenance often originate from tissues with low replicative activity and show several mechanisms of preventing telomere attrition to critical levels. Common and rare germline variants affect patterns of somatic mutation, including point mutations, structural variants and somatic retrotransposition. A collection of papers from the PCAWG Consortium describes non-coding mutations that drive cancer beyond those in the TERT promoter(4); identifies new signatures of mutational processes that cause base substitutions, small insertions and deletions and structural variation(5,6); analyses timings and patterns of tumour evolution(7); describes the diverse transcriptional consequences of somatic mutation on splicing, expression levels, fusion genes and promoter activity(8,9); and evaluates a range of more-specialized features of cancer genomes(8,10-18).Peer reviewe

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Search for strongly interacting massive particles generating trackless jets in proton-proton collisions at s = 13 TeV

Author: Aarrestad TK
Aarup Petersen H
Abbaneo D
Abbiendi G
Abbrescia M
Abdullin S
Abercrombie D
Acharya H
Acosta D
Acosta JG
Adam W
Adams E
Adams MR
Adams T
Adloff C
Adzic P
Agapitos A
Agarwal G
Aggleton R
Agram J-L
Aguilar-Benitez M
Ahmad A
Ahmad M
Ahmed A
Ahuja S
Aime C
Akchurin N
Akgun B
Akpinar A
Albajar C
Albergo S
Albert A
Albrow M
Alcaraz Maestre J
Aldaya Martin M
Aldá Júnior WL
Aleksandrov A
Alexander J
Alhusseini M
Alimena J
Alison J
Allen B
Almond J
Alvarez Gonzalez B
Alverson G
Alves GA
Aly R
Alyari M
Amapane N
Amendola C
Amin N
Amram O
Amsler C
Anagnostou G
Andrea J
Andreev V
Andreev Y
Andrews MB
Androsov K
Antchev G
Antunovic Z
Apanasevich L
Apollinari G
Appelt E
Apresyan A
Apyan A
Araujo M
Arcaro D
Arcidiacono R
Arenton MW
Argiro S
Arneodo M
Aruta C
Asavapibhop B
Asawatangtrakuldee C
Asenov P
Asghar MI
Asilar E
Askew A
Asmuss P
Aspell P
Atakisi IO
Atanassov I
Ather MW
Attikis A
Auffray E
Aushev T
Auzinger G
Avati V
Avery P
Avila C
Awais A
Awan MIM
Ayala E
Ayala G
Aydogmus Sen F
Azarkin M
Azhgirey I
Aziz T
Azzi P
Azzurri P
Baarmand MM
Babaev A
Babounikau I
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Backhaus M
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Baginyan A
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Baldenegro Barrera C
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Široký J
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2022
Field of study

A search for dark matter in the form of strongly interacting massive particles (SIMPs) using the CMS detector at the LHC is presented. The SIMPs would be produced in pairs that manifest themselves as pairs of jets without tracks. The energy fraction of jets carried by charged particles is used as a key discriminator to suppress efficiently the large multijet background, and the remaining background is estimated directly from data. The search is performed using proton-proton collision data corresponding to an integrated luminosity of 16.1 fb - 1 , collected with the CMS detector in 2016. No significant excess of events is observed above the expected background. For the simplified dark matter model under consideration, SIMPs with masses up to 100 GeV are excluded and further sensitivity is explored towards higher masses

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