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33 research outputs found

Analysing Dynamical Behavior of Cellular Networks via Stochastic Bifurcations

Author: A Koseska
A Koseska
A Kuznetsov
A Nakajima
A Pikovsky
Aneta Koseska
Anna Zakharova
AS Zakharova
BP Kramer
CW Gardiner
D Gonze
D Lloyd
IA Khovanov
J Stricker
Jürgen Kurths
K Kaneko
K Tsaneva-Atanasova
Kumar Selvarajoo
L Arnold
L Schimansky-Geier
M Atkinson
M Elowitz
M Samoilov
M Tigges
N Sri Namachchivaya
OV Ushakov
PE Kloeden
R Lefever
S Huang
S Huang
SA Kaufmann
Tatyana Vadivasova
TS Gardner
W Ebeling
W Horsthemke
Y Hirata
Z Wang
Publication venue: Public Library of Science
Publication date: 01/01/2011
Field of study

The dynamical structure of genetic networks determines the occurrence of various biological mechanisms, such as cellular differentiation. However, the question of how cellular diversity evolves in relation to the inherent stochasticity and intercellular communication remains still to be understood. Here, we define a concept of stochastic bifurcations suitable to investigate the dynamical structure of genetic networks, and show that under stochastic influence, the expression of given proteins of interest is defined via the probability distribution of the phase variable, representing one of the genes constituting the system. Moreover, we show that under changing stochastic conditions, the probabilities of expressing certain concentration values are different, leading to different functionality of the cells, and thus to differentiation of the cells in the various types

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Repositorium für Naturwissenschaften und Technik (TIB Hannover)

MPG.PuRe

A Tri-Oceanic Perspective: DNA Barcoding Reveals Geographic Structure and Cryptic Diversity in Canadian Polychaetes

Author: A Arndt
A Chao
A Hobæk
A Nygren
A Nygren
A Rohfritsch
AE Radulovici
AG Glover
AR Templeton
B Pernet
C Arvanitidis
C Bleidorn
CE Hernández
Christina M. Carr
CJ Glasby
CM Carr
D Davenport
D Martin
DP Shorthouse
F Maltagliati
F Pleijel
G Wörheide
GJ Vermeij
GP Manchenko
GW Rouse
IA Jirkov
J Mallet
J Provan
JC Briggs
JC Briggs
JDS Witt
JJ Dodson
Jonathan H. Badger
K Dunton
K Fauchald
K Fauchald
K Tamura
KCR Kerr
M Bhaud
M Clement
M Kimura
M Nei
M Sato
MA Olson
MA Smith
MA Smith
MJH van Oppen
MR Bhaud
MT Jolly
MW Hart
N Knowlton
N Knowlton
NV Ivanova
NV Ivanova
P Chevaldonne
P Hutchings
P Pocklington
PA Quijón
Paul D. N. Hebert
PB Marko
PDN Hebert
PDN Hebert
PDN Hebert
PJ Stabeno
PV Ushakov
R Barroso
R Bastrop
R Bastrop
R Floyd
R Nikula
RA Moreno
RK Colwell
RK Wayne
S Ratnasingham
SA Rice
Sarah M. Hardy
SM Hardy
SR Palumbi
SR Palumbi
T Webb III
TA Sørensen
Tanya M. Brown
Tara A. Macdonald
W Westheide
X Zhou
Publication venue: Public Library of Science
Publication date: 14/07/2011
Field of study

Although polychaetes are one of the dominant taxa in marine communities, their distributions and taxonomic diversity are poorly understood. Recent studies have shown that many species thought to have broad distributions are actually a complex of allied species. In Canada, 12% of polychaete species are thought to occur in Atlantic, Arctic, and Pacific Oceans, but the extent of gene flow among their populations has not been tested.Sequence variation in a segment of the mitochondrial cytochrome c oxidase I (COI) gene was employed to compare morphological versus molecular diversity estimates, to examine gene flow among populations of widespread species, and to explore connectivity patterns among Canada's three oceans. Analysis of 1876 specimens, representing 333 provisional species, revealed 40 times more sequence divergence between than within species (16.5% versus 0.38%). Genetic data suggest that one quarter of previously recognized species actually include two or more divergent lineages, indicating that richness in this region is currently underestimated. Few species with a tri-oceanic distribution showed genetic cohesion. Instead, large genetic breaks occur between Pacific and Atlantic-Arctic lineages, suggesting their long-term separation. High connectivity among Arctic and Atlantic regions and low connectivity with the Pacific further supports the conclusion that Canadian polychaetes are partitioned into two distinct faunas.Results of this study confirm that COI sequences are an effective tool for species identification in polychaetes, and suggest that DNA barcoding will aid the recognition of species overlooked by the current taxonomic system. The consistent geographic structuring within presumed widespread species suggests that historical range fragmentation during the Pleistocene ultimately increased Canadian polychaete diversity and that the coastal British Columbia fauna played a minor role in Arctic recolonization following deglaciation. This study highlights the value of DNA barcoding for providing rapid insights into species distributions and biogeographic patterns in understudied groups

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Effects of alirocumab on types of myocardial infarction: insights from the ODYSSEY OUTCOMES trial

Author: Abbas J
Abbate A
Abdullakutty J
Abhyanakar AD
Aboyans V
Abrantes JAM
Abu-Fadel M
Acevedo M
Adamkova V
Adhyapak S
Agarwal H
Aggarwal R
Aggarwal RK
Aguirre A
Ahmed H
Ahremark U
Ahuad Guerrero RA
Aidar Ayoub JC
Airaksinen JK
Aitken D
Akatova E
Akhter F
Ako J
Akright L
Akyea-Djamson A
Al Joundi T
Al-Windy NYY
Alan D
Alcocer Gamba MA
Alexander JH
Alexander K
Alexandru TM
Alings M
Alonso Martin JJ
Alvarisqueta AF
Alves De Lima AE
Amarasekera S
Amarasena N
Amir O
Amlani M
Amosova E
Amuchastegui M
Andersen K
Andersen R
Anderson J
Ando K
Angel Hominal M
Annam S
Anscombe R
Apostolovic SR
Appel K-F
Arandjelovic A
Araneda G
Arango Benecke JL
Arbel Y
Arif I
Armaganijan L
Arroyo JAC
Arstall MA
Asanin MR
Atar S
Athyros V
Auguadro C
Ayala CAC
Aylward PE
Azizad MM
Bagai A
Bagriy A
Bahit MC
Bai F
Balaguer Recena J
Baldari D
Balinovac J
Ball E
Bang LE
Banuru S
Barakovic F
Baranov E
Baranova E
Barbarash OL
Barbato E
Barna OM
Barone-Rochette G
Barr C
Barrucco R
Bartels GL
Bashir R
Basson MMDV
Bastos JM
Bata I
Batushkin V
Bayat J
Bayram Llamas EA
Bayron C
Beauloye C
Bednarski J
Behrens S
Belhassane A
Benedicto A
Bengus CM
Benov HO
Berger R
Berglund S
Berk M
Berland J
Berli MA
Berlowitz M
Berman B
Bernan A
Berti S
Bhagwat A
Bhagwat R
Bhansali P
Bhatt DL
Binder R
Birchem J
Bittner VA
Blicharski T
Blok T
Blumberg EDS
Boccara F
Bodanese LC
Bodi Peris V
Boecker D
Bojovski S
Bokarev I
Bokern MJJA
Bonfanti AJC
Bono JOE
Bordonava AP
Borse R
Bortnick A
Bos RJ
Botas Rodriguez J
Botelho A
Botelho RV
Botia DCL
Bottcher M
Bourgeois R
Brabham D
Braganza D
Braun-Dullaeus R
Breedveld RW
Brennan JM
Brodison A
Bronzwaer PNA
Brueren BRG
Bruguera Cortada J
Budaj A
Bugan V
Busmane A
Bustamante Labarta MH
Busz-Papiez B
Butler R
Bystryk L
Caccavo A
Caime GD
Calabro P
Camprubi Potau M
Camsari A
Caraco Y
Carey C
Carlson E
Carnero GS
Carranza Madrigal J
Carrillo Calvillo J
Carroll PA
Cartasegna LR
Carter L
Caruso OC
Cassimjee S
Castadot M
Cavallini C
Cequier Fillat AR
Cerqueira MJAG
Cestari HG
Cevc M
Cha J
Chae I-H
Chaitman B
Chalavarya G
Chaleff F
Chambilla JMC
Chandna H
Chane M
Chang M
Chaudhary S
Chavez V-CER
Chen D
Chen J
Chen Y
Cheng S-C
Cheng X
Chiang C-E
Chiang C-E
Chizhov P
Chopda M
Chopra VK
Christenson S
Chu A
Chua T
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Chumburidze V
Civeira Murillo F
Claeys M
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Clerc J
Cleveland D
Clifford P
Clifton S
Coching RM
Codutti OR
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Colombo HR
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Commerford PJ
Concha YMR
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Constantinescu MCA
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Cornel JH
Correa Flores RM
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Cosin Sales J
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Coste P
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Coverdale SGM
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Cruz Fernandez JM
Cuccia C
Cui L
Cyster HP
Czerski T
D'Urso M
Daboul N
Dagher G
Dahl C
Dai K
Dalby AJ
Dalby AJ
Danchin N
Dandillaya R
Daniels C
Das S
Davidovic G
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Davies R
Davis W
De Berrazueta Fernandez JR
De Cesare NB
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de Santos MON
de Silva HA
de Souza JA
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Delarche N
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Demirtas M
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DeVore AD
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Diaz R
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Dilic M
Dimkovic S
Dimov BI
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Ding C
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El-Ahdab F
Elias M
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Elliott J
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Erglis A
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Faes D
Faggiano P
Fairlamb J
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Farhat N
Farrar M
Fausto Ovando SR
Fazekas F
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Fernandez Portales J
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Filardi PP
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Fisher D
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Franek E
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Friedman D
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Gelormini J
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Gerber R
Ghitis A
Ghlonti R
Gibson P
Gielen S
Giesler G
Gil-Extremera B
Gilbert JM
Gillespie E
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Gimple L
Giordano JA
Giorgeto FE
Gislason G
Giuliano ME
Gniot J
Goch A
Goloborodko B
Gomez Vilamajo OA
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Gonzalez Diaz B
Gonzalez Salas LG
Gonzalez-Juanatey C
Gonzalez-Juanatey JR
Goodman SG
Goodman SG
Gordeev I
Gordienko A
Gorny J
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Gosselink ATM
Gotcheva NN
Gotcheva NN
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Goyal NK
Gremmler U
Grewal JS
Griffiths H
Gring C
Groenemeijer BE
Groutars RGEJ
Guardigli G
Guerrero De Leon M
Guha S
Gullestad L
Guneri S
Guneri S
Guo Y
Gurevich V
Gusi Tragant G
Guzman PN
Haddad T
Hagstrom E
Hagstrom E
Hahalis PIG
Halabi M
Halcox J
Hald F
Haldis T
Hall J
Halvorsen S
Hameed A
Haniffa R
Hanotin C
Hansen O
Haraguchi T
Harding S
Harkut P
Harrington RA
Harris B
Harris B
Hart H
Hata Y
Hattler B
Hedman A
Heidenreich L
Heinc P
Heitzer T
Hemetsberger R
Henderson D
Henkin Y
Herath JI
Herazo AS
Hermans K
Hermans WRM
Hernandez HAA
Herrman JPR
Hersbach FMRJ
Hess CN
Higashikata T
Higuera JD
Hii CLS
Hirayama A
Hirooka K
Hlatky MA
Hoag G
Hodes Z
Hoffer E
Hoffman D
Hong T
Hoogslag PAM
Hoppe U
Horak D
Horowitz J
Horvath I
Horwitz P
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Hranai M
Hsieh I-C
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Huang S
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II TC
III DG
III KG
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Iqbal SMR
Irimpen A
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Ito K
Ivanov IG
Ivanova R
Ivanovic N
Iyengar SS
Izzo M
Jacoby D
Jafar Z
Jaffrani N
Jain D
Janik M
Janosik D
Jaramillo N
Jatin FGM
Jaworska K
Jayawardena J
Jensen SA
Jensen SA
Jeong MH
Jeppesen J
Jeserich M
Jiang W
Jintapakorn W
Johansen PB
Jonas M
Jones WS
Jordan JD
Jortveit J
Joshi AB
Joshi P
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Jr WD
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Jukema JW
Juonala M
Jure HO
Jurgaitiene R
Kadr H
Kaewsuwanna P
Kahali D
Kaikkonen K
Kaiser S
Kalashetti S
Kalil R
Kamensky G
Kamiya H
Kandasamy B
Kapin T
Kaplan R
Kapp IE
Karalis I
Karlsberg R
Karna S
Karpenko O
Karpenko Y
Karpov Y
Karpov Y
Kartalis A
Kasim S
Katona A
Katsuda Y
Katz A
Kaucak V
Kavaliauskiene R
Kawasaki T
Ke Y
Keating F
Kedev S
Keen W
Kehasukcharoen W
Kelsey SF
Kerkar P
Khabeishvili G
Khaira AS
Khaisheva L
Khan A
Khan A
Khan M
Khasanov N
Khintibidze I
Khurana S
Kibarskis A
Kichukov KN
Killat H
Kim C
Kim HS
Kim MH
Kim S-H
Kimmelstiel C
Kimura K
Kimura T
King M
Kirma C
Kishi K
Kiss RG
Kiss RG
Kiviniemi T
Kjovkaroski A
Klancke K
Klantsa A
Klausen IC
Kline G
Klutstein M
Knickelbine T
Knowles JW
Knutson T
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Kobalava Z
Kobayashi J
Koike A
Koldas L
Kolls BJ
Kondo NI
Kong DF
Kopytsya M
Koren M
Kormann A
Kornder J
Kornowski R
Korol M
Kosinski E
Kosmachova E
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Kotha P
Kouz S
Kovalskyi I
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Krasowski W
Krawczyk J
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Kristensen KS
Kubica J
Kubilius R
Kuchar J
Kuhlman P
Kultursay H
Kumar A
Kumar P
Kumbla M
Kumkumian G
Kuo J-Y
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Kushnir M
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Laufs U
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Leaes PE
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Lee K
Lee K
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Leggewie S
Lehman SJ
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Lekakis J
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Leone A
Lepage S
Lepor N
Leshchuk O
Lester FM
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Li H
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Liew HB
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Lin J
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Senaratne V
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Zrazhevsky K
Zuniga JDH
Zurakowski A
Zuran I
Zweiker R
Publication venue: 'Oxford University Press (OUP)'
Publication date: 01/01/2019
Field of study

Aims The third Universal Definition of Myocardial Infarction (MI) Task Force classified MIs into five types: Type 1, spontaneous; Type 2, related to oxygen supply/demand imbalance; Type 3, fatal without ascertainment of cardiac biomarkers; Type 4, related to percutaneous coronary intervention; and Type 5, related to coronary artery bypass surgery. Low-density lipoprotein cholesterol (LDL-C) reduction with statins and proprotein convertase subtilisin–kexin Type 9 (PCSK9) inhibitors reduces risk of MI, but less is known about effects on types of MI. ODYSSEY OUTCOMES compared the PCSK9 inhibitor alirocumab with placebo in 18 924 patients with recent acute coronary syndrome (ACS) and elevated LDL-C (≥1.8 mmol/L) despite intensive statin therapy. In a pre-specified analysis, we assessed the effects of alirocumab on types of MI. Methods and results Median follow-up was 2.8 years. Myocardial infarction types were prospectively adjudicated and classified. Of 1860 total MIs, 1223 (65.8%) were adjudicated as Type 1, 386 (20.8%) as Type 2, and 244 (13.1%) as Type 4. Few events were Type 3 (n = 2) or Type 5 (n = 5). Alirocumab reduced first MIs [hazard ratio (HR) 0.85, 95% confidence interval (CI) 0.77–0.95; P = 0.003], with reductions in both Type 1 (HR 0.87, 95% CI 0.77–0.99; P = 0.032) and Type 2 (0.77, 0.61–0.97; P = 0.025), but not Type 4 MI. Conclusion After ACS, alirocumab added to intensive statin therapy favourably impacted on Type 1 and 2 MIs. The data indicate for the first time that a lipid-lowering therapy can attenuate the risk of Type 2 MI. Low-density lipoprotein cholesterol reduction below levels achievable with statins is an effective preventive strategy for both MI types.For complete list of authors see http://dx.doi.org/10.1093/eurheartj/ehz299</p

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Use of anticoagulants and antiplatelet agents in stable outpatients with coronary artery disease and atrial fibrillation. International CLARIFY registry

Author: A. L. R. Ng
Abardia Oliva F. J.
Abdel Malak S.
Abdel Wahab H.
Abdul Kareem B. B.
Abdul Manap H.
Abdul Rahim A. A.
Abdulkader F.
Abdulla A. H. K.
AbdulWahab M. Z.
Abduvalieva V.
Abele S.
Aboyans V.
Abreu P. E.
Adam-Blanpain M.
Adamaszek K.
Adamczyk-Kot D.
Adamkiewicz-Piejko A.
Adda M.
Aftab A.
Agrawal A.
Aguiar C.
Ahuad Guerrero A.
Ahuja R.
Ai F.
Aimouch N.
Aiyegbayo O.
Ajani A.
Akbar M.
Aksyutina N.
Al Dhanki M.
Al Ghool S.
Al Kandari F.
Al Lawati A.
Al Mahmeed W.
Al Radaideh G.
Al Rashdan I.
Al Sousi A.
Al Suwaidi J.
Al Tamimi F.
Al Wahshi Y.
Al Yazeedi J.
Al Zaibag M.
Al-Baker H.
Al-Faleh H.
Al-Hersi A.
Al-Khalidi B.
Al-Shamiri M.
Al-Zaibag M.
Alam A.
Alanazy M.
Alanbaei M.
Albero Martinez V.
Alberto Ramirez Reyes H.
Albuquerque A.
Alcaravela J.
Alcocer Gamba M.
Alegret Colomer J. M.
Alegria Ezquerra E.
Alekseenko V.
Alekseeva T.
Alexanderson E.
Alexopoulos I.
Alford K.
Alitto F.
Alizon F.
Allcock A.
Almeida Fernandez C. A.
Altevogt B. -M.
Altmann U.
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Alvarez Aunon A.
Alvarez Garcia P.
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Publication date: 01/01/2015
Field of study

Florence Research

CDC42 switches IRSp53 from inhibition of actin growth to elongation by clustering of VASP

Author: Abbott MA
Abou-Kheir W
Adams JC
Ahmed S
Akin O
Andrea Disanza
Andrea Palamidessi
Applewhite DA
Bachmann C
Barzik M
Bear JE
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Breitsprecher D
Breitsprecher D
Chan CE
Christophe Ampè
David Kast
Davy Waterschoot
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Dmitry S Ushakov
Faix J
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Francesca Milanesi
Gabbiani G
Gates J
Gertler FB
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Giorgio Scita
Goh WI
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Guillaume Romet-Lemonne
Hans-Michael Müller
Hansen SD
Huttelmaier S
Jan Faix
Jegou A
Joern Linkner
Koestler SA
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Lim KB
Marie-France Carlier
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Moritz Winterhoff
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Paola Marighetti
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Roberto Dominguez
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Scita G
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Temmerman K
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Vignjevic D
Vignjevic D
Walter Nickel
Weiss SM
Wiesner S
Wu C
Yamagishi A
Yang C
Yang C
Yang C
Yang C
Zhao H
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

Effect of alirocumab on mortality after acute coronary syndromes. An analysis of the ODYSSEY OUTCOMES randomized clinical trial

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Abbate A
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Abhyanakar AD
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Abrantes JAM
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Al-Windy NYY
Alan D
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Alexander JH
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Alexandru TM
Alexopoulos D
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Alonso Martin JJ
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Alsweiler C
Alvarisqueta AF
Alves De Lima AE
Amarasekera S
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Amir O
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Amuchastegui M
Anchante Hernandez HA
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Apostolovic SR
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Arroyo JAC
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Asanin MR
Atar S
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Auguadro C
Aylward P
Aylward PE
Aylward PE
Azizad MM
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Bartels GL
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Zweiker R
Publication venue: 'Ovid Technologies (Wolters Kluwer Health)'
Publication date: 04/01/2019
Field of study

Background: Previous trials of PCSK9 (proprotein convertase subtilisin-kexin type 9) inhibitors demonstrated reductions in major adverse cardiovascular events, but not death. We assessed the effects of alirocumab on death after index acute coronary syndrome. Methods: ODYSSEY OUTCOMES (Evaluation of Cardiovascular Outcomes After an Acute Coronary Syndrome During Treatment With Alirocumab) was a double-blind, randomized comparison of alirocumab or placebo in 18 924 patients who had an ACS 1 to 12 months previously and elevated atherogenic lipoproteins despite intensive statin therapy. Alirocumab dose was blindly titrated to target achieved low-density lipoprotein cholesterol (LDL-C) between 25 and 50 mg/dL. We examined the effects of treatment on all-cause death and its components, cardiovascular and noncardiovascular death, with log-rank testing. Joint semiparametric models tested associations between nonfatal cardiovascular events and cardiovascular or noncardiovascular death. Results: Median follow-up was 2.8 years. Death occurred in 334 (3.5%) and 392 (4.1%) patients, respectively, in the alirocumab and placebo groups (hazard ratio [HR], 0.85; 95% CI, 0.73 to 0.98; P=0.03, nominal P value). This resulted from nonsignificantly fewer cardiovascular (240 [2.5%] vs 271 [2.9%]; HR, 0.88; 95% CI, 0.74 to 1.05; P=0.15) and noncardiovascular (94 [1.0%] vs 121 [1.3%]; HR, 0.77; 95% CI, 0.59 to 1.01; P=0.06) deaths with alirocumab. In a prespecified analysis of 8242 patients eligible for ≥3 years follow-up, alirocumab reduced death (HR, 0.78; 95% CI, 0.65 to 0.94; P=0.01). Patients with nonfatal cardiovascular events were at increased risk for cardiovascular and noncardiovascular deaths (P<0.0001 for the associations). Alirocumab reduced total nonfatal cardiovascular events (P<0.001) and thereby may have attenuated the number of cardiovascular and noncardiovascular deaths. A post hoc analysis found that, compared to patients with lower LDL-C, patients with baseline LDL-C ≥100 mg/dL (2.59 mmol/L) had a greater absolute risk of death and a larger mortality benefit from alirocumab (HR, 0.71; 95% CI, 0.56 to 0.90; Pinteraction=0.007). In the alirocumab group, all-cause death declined wit h achieved LDL-C at 4 months of treatment, to a level of approximately 30 mg/dL (adjusted P=0.017 for linear trend). Conclusions: Alirocumab added to intensive statin therapy has the potential to reduce death after acute coronary syndrome, particularly if treatment is maintained for ≥3 years, if baseline LDL-C is ≥100 mg/dL, or if achieved LDL-C is low. Clinical Trial Registration: URL: https://www.clinicaltrials.gov. Unique identifier: NCT01663402

Spiral - Imperial College Digital Repository

A review of bipolarity concepts: history and examples from Radiolaria and Medusozoa (Cnidaria)

Author: Afanasieva MS
Aita Y
Alvarino A
Amon EO
Amon EO
Andriashev AP
Andriashev AP
Andriashev AP
Andriashev AP
Andriashev AP
Andriashev AP
Andriashev AP
Antsulevitch AE
Antsulevitch AE
Arai M
Averintsev VG
Bailey JW
Barnard JL
Beers JR
Beklemishev KV
Beljaev GM
Benson RN
Bergh LS
Bergh LS
Bergh LS
Bergh LS
Bergh LS
Beshbeeshy ML
Birstein YA
Birstein YA
Bjørklund KR
Bjørklund KR
Bjørklund KR
Blanko OM
Blanko OM
Blanko OM
Blanko OM
Blanko OM
Blanko OM
Blanko OM
Blanko OM
Boero F
Bogorov VG
Boltovskoy D
Borgert A
Bouillon J
Bouillon J
Bouillon J
Bouillon J
Bouillon J
Bouillon J
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Bouillon J
Brandt K
Briggs EA
Brinckmann A
Brinckmann-Voss A
Brinton E
Broch H
Brundin L
Cachon J
Calder DR
Calder DR
Calder DR
Calder DR
Calder DR
Calder DR
Calder DR
Calder DR
Calder DR
Calder DR
Candolle A.d
Casey RE
Chapligina SF
Chapligina SF
Chen PH
Christiansen BO
Chun C
Cleve PT
Cleve PT
Cleve PT
Cornelius PFS
Cornelius PFS
Cornelius PFS
Cornelius PFS
Cornelius PFS
Cornelius PFS
Cornelius PFS
Cornelius PFS
Cornelius PFS
Cornelius PFS
Crame JA
Crame JA
Dana JD
Darwin C
Dayton PK
De Vries AL
De Wever P
Derjugin KM
Dogiel VA
Dunbar MJ
Ehrenberg CG
Ehrenberg CG
Ehrenberg CG
Ekman S
Es'kov KY
Fraser CM
Fraser CM
Fraser CM
Fraser CM
Fraser CM
G. Cortese
Geptner VG
Gibbons MJ
Golikov AN
Gravier-Bonnet N
Gravier-Bonnet N
Gruzov EN
Haeckel E
Haeckel E
Haecker V
Haecker V.
Hasle GR
Helland-Hansen B
Hesse R
Hirai E
Hirai E
Hirohito ES
Hirohito ES
Hirohito TIES
Hirohito TIES
Hubbs CL
Hülsemann K
Jansen E
Jarms G
Jarms G
Jarms G
Jarms G.
Jørgensen E
Jørgensen E
K. R. Bjørklund
Kafanov AI
Keany J
Kling SA
Kling SA
Knudsen J
Kozlova GE.
Kramp PL
Kramp PL
Kramp PL
Kramp PL
Kramp PL
Kramp PL
KrasheninNIkov VA
Kruglikova SB
Kruglikova SB
Kruglikova SB
Kruglikova SB
Kruglikova SB
Kruglikova SB
Kruglikova SB
Kruglikova SB
Kruglikova SB
Kubota S
Kubota S
Kubota S
Kubota S
Kubota S
Kubota S
Kubota S
Kubota S
Kussakin OG
Larson RJ
Larson RJ
Lazarus D
Levushkin SI
Ling HY
Ling HY
Maas O
Maas O
Maas O
Mangerud J
Manton SM
Mapstone GM
Margulis RY
Margulis RY
Margulis RY
Marques AC
Marques AC
Marques AC
Marques AC
Matul A
Matul A
Matul A.
McGinitie GE
Mead GW
Medel MD
Medel MD
Medel MD
Meisenheimer J
Meunier A
Migotto AE
Migotto AE
Mileykovskyi SA
Millard NAH
Millard NAH
Millard NAH
Murray J
Nakaseko K
Namikawa H
Namikawa H
Naumov DV
Naumov DV
Nigrini C
Nigrini C
Nigrini C
Nishimura A
Orlov DV
Ortmann AE
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Page FC
Pages F
Pages F
Pages F
Panteleeva NN
Pasternak FA
Petrushevskaya MG
Petrushevskaya MG
Petrushevskaya MG
Petrushevskaya MG
Petrushevskaya MG
Petrushevskaya MG
Petrushevskaya MG
Petrushevskaya MG
Petrushevskaya MG
Petrushevskaya MG
Petrushevskaya MG
Peña Cantero AL
Pfeffer G
Pierrot-Bults AC
Ramil F
Ramil F
Rasnitzin AP
Rasnitzin AP.
Rass TS
Rass TS
Rees WJ
Renz GW
Reshetnjak VV
Reshetnjak VV
Reshetnjak VV
Reshetnjak VV
Riedel WR
Riedel WR
Riedel WR
Riedel WR
Robins MW
Ross GA
Russel FS
Russel FS
Ryland JS
S. B. Kruglikova
S. D. Stepanjants
Schneppenheim R
Schröder O
Schröder O
Schröder O
Schröder-Ritzrau A
Schuchert P
Schuchert P
Schuchert P
Schwarz SS
Segonzac M
Semenov VN
Sheiko OV
Sheiko OV
Stechow E
Stepanjants SD
Stepanjants SD
Stepanjants SD
Stepanjants SD
Stepanjants SD
Stepanjants SD
Stepanjants SD
Stepanjants SD
Stepanjants SD
Stepanjants SD
Stepanjants SD
Stepanjants SD
Stepanjants SD
Stepanjants SD
Stepanjants SD
Stepanjants SD
Stepanjants SD
Svetovidov AN
Svoboda A
Svoboda A
Takahashi K
Tibbs JF
Ushakov PV
Vanhöffen E
Vanhöffen E
Vervoort W
Vervoort W
Vervoort W
Vervoort W
Vervoort W
Vervoort W
Vinogradov ME
Vinogradov ME
Vinogradova NG
Vinogradova NG
Vishnevskaya VS
Voronov AG
Watson JE
Watson JE
Watson JE
Watson JE
Weaver FM
Yamada M
Zenkevitch LA
Zenkevitch LA
Publication venue: 'Informa UK Limited'
Publication date: 01/01/2006
Field of study

Crossref

Electronic Publication Information Center

Modelling and Optimization of Spacecrafts’ Systems Design

Author: A Antamoshkin
E Semenkin
M Volovik
M Volovik
O Semenkina
SA Ushakov
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/1996
Field of study

Crossref

Effect of Bi substitution on the cationic vacancy ordering in SrMoO4-based complex oxides: Structure and properties

Author: Abrahams I
Komleva EV
Mikhaylovskaya ZA
Pankrushina EA
Petrova SA
Streltsov SV
Ushakov AV
Publication venue
Publication date: 01/01/2022
Field of study

ePubs: the open archive for STFC research publications

Effect of Bi substitution on the cationic vacancy ordering in SrMoO<inf>4</inf>-based complex oxides: Structure and properties

Author: Abrahams I
Komleva EV
Mikhaylovskaya ZA
Pankrushina EA
Petrova SA
Streltsov SV
Ushakov AV
Publication venue: 'Elsevier BV'
Publication date: 04/05/2022
Field of study

The electronic and crystal structures of the Sr1−3xBi2xФxMoO4 series (0.025 ≤ x ≤ 0.30, where Ф represents cation vacancies) were studied. The 0.025 ≤ x ≤ 0.15 compositions showed a defect scheelite structure. Powder X-ray and neutron diffraction patterns for compositions with 0.15 < x ≤ 0.225 exhibited a tetragonal supercell with asup ≈ √5a, csup ≈ c where a and c are the tetragonal scheelite cell parameters. Strong distortion of MoO4 polyhedra was shown by Raman spectroscopy and described by the calculated phonon spectra of “virtual crystals” of Bi2+[MoO4] and Ф2+[MoO4]. The electronic structures were calculated for both types of structure. The decrease of the calculated energy gap is consistent with experimental data from Kubelka-Munk measurements. The electroconductive properties were measured by A.C. impedance spectroscopy. For Sr1−3xBi2xФxMoO4 compositions conductivity increases with increasing x-value, with maximum values of conductivity at 948 K of 2.82 × 10−5S cm−1 for the x = 0.20 composition

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