14 research outputs found
What makes a galaxy radio-loud?
- Author
- Publication venue
- 'Cambridge University Press (CUP)'
- Publication date
- 20/01/2012
- Field of study
Full text linkWe compare the Spectral Energy Distribution (SED) of radio-loud and
radio-quiet AGNs in three different samples observed with SDSS: radio-loud AGNs
(RLAGNs), Low Luminosity AGNs (LLAGNs) and AGNs in isolated galaxies (IG-AGNs).
All these galaxies have similar optical spectral characteristics. The median
SED of the RLAGNs is consistent with the characteristic SED of quasars, while
that of the LLAGNs and IG-AGNs are consistent with the SED of LINERs, with a
lower luminosity in the IG-AGNs than in the LLAGNs. We infer the masses of the
black holes (BHs) from the bulge masses. These increase from the IG-AGNs to the
LLAGNs and are highest for the RLAGNs. All these AGNs show accretion rates near
or slightly below 10% of the Eddington limit, the differences in luminosity
being solely due to different BH masses. Our results suggests there are two
types of AGNs, radio quiet and radio loud, differing only by the mass of their
bulges or BHs.Comment: 3 pages, 3 figures; to appear in Proceedings of IAU Symposium No.
284, The Spectral Energy Distribution of Galaxies (SED2011), Preston, UK, 5-9
sep. 201
ICAR: endoscopic skull‐base surgery
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- Publication venue
- Publication date
- 01/07/2019
- Field of study
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Clonal chromosomal mosaicism and loss of chromosome Y in elderly men increase vulnerability for SARS-CoV-2
- Author
- Abellán Javier
- Acosta-isaac René
- Aguado Jose María
- Aguilar Carlos
- Aguilera-albesa Sergio
- Ahmadi Sabbagh Abdolah
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- Albu Sergiu
- Alcalá-gallardo Karla A. M.
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- Alcolea Batres Sergio
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- Arribas López José Ramón
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- Dantas-komatsu Raquel C. S.
- Darnaude M. Teresa
- De Andrés Raimundo
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- De Juan Carmen
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- Gutiérrez-bautista Juan F.
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- Herrero María José
- Herrero-gonzález Antonio
- Herráez Belén
- Horcajada Juan P.
- Imaz-ayo Natale
- Intxausti-urrutibeaskoa Maider
- Jacomo Rafael H.
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- Jiménez Ángel
- Jiménez-alfaro Ignacio
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- Molina-roldán Elena
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- Perales Celia
- Perucho Teresa
- Pichardo Lisbeth A.
- Pinho Susana M. T.
- Pinsach-abuin Mel·lina
- Pinzón Luz Adriana
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- Pla-juncà Francesc
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- Pujol Aurora
- Pérez Alexandra
- Pérez César
- Pérez María Jazmín
- Pérez Patricia
- Pérez-de-nanclares Gustavo
- Pérez-garcía Felipe
- Pérez-jurado Luis A.
- Pérez-matute Patricia
- Pérez-tomás M. Elena
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- Quintela Inés
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- Rascado Sedes Pedro
- Recalde Delia
- Recio-fernández Emma
- Resino Salvador
- Riancho José A.
- Ribeiro Adriana P.
- Rivadeneira-chamorro Carlos S.
- Roa-agudelo Diana
- Robelo Pardo Montserrat
- Rodriguez Marilyn Johanna
- Rodriguez-nicolas Antonio
- Rodriguez-palmero Agustí
- Rodriguez-urrego Paula A.
- Rodríguez-artalejo Fernando
- Rodríguez-ferrer Marena
- Rodríguez-gallego Carlos
- Rodríguez-garcía José A.
- Rodríguez-hernández María A.
- Rodríguez-novoa German Ezequiel
- Rodríguez-ruiz Emilio
- Rojas-martinez Augusto
- Rojo Federico
- Romero-coronado Andrea
- Rondón-garcía Filomeno
- Rosa Lidia S.
- Rosales-castillo Antonio
- Rubio Cladelis
- Ruiz Montserrat
- Ruiz-cabello Francisco
- Ruiz-casares Eva
- Ruiz-cubillan Juan J.
- Ruiz-hornillos Javier
- Ryan Pablo
- Salamanca Hector D.
- Salazar-garcía Lorena
- Salgueiro-origlia Giorgina Gabriela
- Sancho-sainz Cristina
- Sande Esther
- Sangil Anna
- Santos Arnoldo
- Santos Ney P. C.
- Schlüter Agatha
- Scourge Cohort Group
- Segovia Sonia
- Serra-llovich Alex
- Sevil-puras Fernando
- Sevilla-porras Marta
- Sicolo Miguel A.
- Silbiger Vivian N.
- Silva Fabiola T. C.
- Silva Gabriela V.
- Silva Nayara S.
- Silván-fuentes Cristina
- Solé-violán Jordi
- Soria José Manuel
- Sorlí Jose V.
- Sousa Renata R.
- Souto Juan Carlos
- Souza Karla S. C.
- Souza Vanessa S.
- Sprockel John J.
- Suárez-rama José Javier
- Suárez-zamora David A.
- Sánchez López Antonio J.
- Sánchez Pedro-luis
- Sánchez-carpintero Abad María
- Sánchez-pablo Clara
- Sánchez-pernaute Olga
- Sánchez-prados María Concepción
- Sánchez-real Javier
- Sánchez-redondo Jorge
- Taboada-fraga Xiana
- Tamayo Eduardo
- Tamayo-velasco Alvaro
- Taracido-fernández Juan Carlos
- Tavares Nathali A. C.
- Tellería Carlos
- Tenorio-castaño Jair Antonio
- Teper Alejandro
- Torres-gutiérrez Ronald P.
- Torres-macho Juan
- Torres-tobar Lilian
- Troya Jesús
- Urioste Miguel
- Valencia-ramos Juan
- Valido Agustín
- Vargas-gallo Juan Pablo
- Varón Belén
- Vasconcelos Romero H. T.
- Vega Tomas
- Velasco-quirce Santiago
- Vidán-estévez Julia
- Vieitez-santiago Miriam
- Vilches Carlos
- Villalobos Lavinia
- Villar Felipe
- Villar-garcia Judit
- Villaverde Cristina
- Villoslada-blanco Pablo
- Virseda-berdices Ana
- Vélez-santamaría Valentina
- Víctor Virginia
- Yáñez Zuleima
- Zapatero-gaviria Antonio
- Zarate Ruth
- Zazo Sandra
- Álvarez Nuria
- Álvarez-benítez Yady
- Álvarez-navia Felipe
- Álvarez-sala Walther Rodolfo
- Íñigo-campos Antonio
- Íñiguez María
- Publication venue
- Springer Science and Business Media LLC
- Publication date
- 08/05/2024
- Field of study
Full text linkThe pandemic caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2, COVID-19) had an estimated overall case fatality ratio of 1.38% (pre-vaccination), being 53% higher in males and increasing exponentially with age. Among 9578 individuals diagnosed with COVID-19 in the SCOURGE study, we found 133 cases (1.42%) with detectable clonal mosaicism for chromosome alterations (mCA) and 226 males (5.08%) with acquired loss of chromosome Y (LOY). Individuals with clonal mosaic events (mCA and/or LOY) showed a 54% increase in the risk of COVID-19 lethality. LOY is associated with transcriptomic biomarkers of immune dysfunction, pro-coagulation activity and cardiovascular risk. Interferon-induced genes involved in the initial immune response to SARS-CoV-2 are also down-regulated in LOY. Thus, mCA and LOY underlie at least part of the sex-biased severity and mortality of COVID-19 in aging patients. Given its potential therapeutic and prognostic relevance, evaluation of clonal mosaicism should be implemented as biomarker of COVID-19 severity in elderly people. Among 9578 individuals diagnosed with COVID-19 in the SCOURGE study, individuals with clonal mosaic events (clonal mosaicism for chromosome alterations and/or loss of chromosome Y) showed an increased risk of COVID-19 lethality
Moonlighting Peptides with Emerging Function
- Author
- Alfredo Torres Larios
- AM Rea
- Amanda Villalón Rojas
- Antonio Peña Díaz
- BK Lee
- C Gancedo
- C Geourjon
- Carlos Amero
- Carlos Polanco Gonzalez
- CJ Jeffery
- CJ Jeffery
- CJ Jeffery
- CJ Jeffery
- CK Suzuki
- Dale E. Bredesen
- E Hazy
- FF Severin
- G del Rio
- Gabriel del Rio
- Gabriela Zarraga Granados
- Georgina Garza-Ramos
- H Muller
- HM Ellerby
- HM Ellerby
- Jonathan G. Rodríguez Plaza
- JS Gounarides
- K Kitada
- K Wakamatsu
- K Wakamatsu
- LH Hartwell
- M Das
- M Obeid
- Manuel Gutiérrez Aguilar
- María Teresa Lara Ortiz
- MG Abel
- MG Kolonin
- N Sreerama
- NN Zhang
- P Shenbagamurthi
- P Tompa
- Peter Csermely
- PS Low
- Roberto Coria
- Salvador Uribe Carvajal
- Sur Herrera
- Susana Castro-Obregon
- TE Rusten
- US Bhalla
- W Arap
- W Arap
- W Arap
- W Yang
- YL Zhang
- Publication venue
- 'Public Library of Science (PLoS)'
- Publication date
- Field of study
No full textPrevalent HLA Class II Alleles in Mexico City Appear to Confer Resistance to the Development of Amebic Liver Abscess
- Author
- A Arnaiz-Villena
- A Arnaiz-Villena
- A Moreno-Estrada
- A Nieto
- Alberto López-Reyes
- Alexandra Luna
- Alicia Valadez
- AM Borghans José
- AM Pérez-Miranda
- AV Hill
- C Alaez
- C Gorodezky
- C Sánchez
- Carmen Maldonado
- CD Huston
- Cecilia Ximénez
- D Aceves
- D Middleton
- D Mondal
- Edgar Rascón
- Enrique González
- Eric G. Hernández
- F del Puerto
- F Ramos
- F Williams
- Francisco J. Estrada
- G Choudhuri
- G Vargas-Alarcon
- G Vargas-Alarcón
- H Vivanco-Cid
- I Wong-Baeza
- J Arellano
- J Arellano
- J Klein
- J Zúñiga
- Julio Granados
- JY Lin
- K Cao
- Liliana Rojas
- M Camorlinga-Ponce
- M Carrington
- M Denis
- M Macías-Vega
- Miriam Nieves-Ramírez
- MV Camacho
- Mónica Escamilla-Tilch
- N Singh
- NH Deghaide
- O Valenzuela
- Olivia Valenzuela
- Oswaldo Partida-Rodríguez
- P Duggal
- P Duggal
- P Morán
- Patricia Morán
- R Barquera
- R Burgos-Vargas
- RM Maizels
- S Hernández-Gutiérrez
- SA Miller
- T Juárez-Cedillo
- T Moatter
- U Shankarkumar
- Ulises Magaña
- Zhi-Ying Wu
- Publication venue
- 'Public Library of Science (PLoS)'
- Publication date
- Field of study
No full textLandschaft, pueblo
- Author
- Acosta J.D.
- Acuña R.
- AGN
- Albores B.
- Alfonso-X
- Alonso M.
- Bernal-García M.-E.
- Bernal-García M.-E.
- Berque A.
- Berque A.
- Berque A.
- Berque A.
- Blázquez-Garbajosa A.
- Bolós M.D.
- Bonfil-Batalla G.
- Boone E.H.
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- Broda J.
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- Brown C.
- Carrasco D.
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- Chanfón-Olmos C.
- Chávez-Peón-Herrero A.E.
- Claval P.
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- Cline H.F.
- Corominas J.
- Corominas J.
- Cortelazzo M.
- Cortés H.
- Cosgrove D.
- Cosgrove D.E.
- Covarrubias-Orozco S.D.
- Crespo-Sanz A.
- Crespo-Sanz A.
- Crosby A.W.
- Delgado-Granados H.
- Deylen W.V.
- Donadieu P.
- Duncan J.S.
- Durán D.
- Díaz del Castillo B.
- Enfield G.H.
- Escalante P.
- Espinosa A.
- Federico Fernández-Christlieb
- Fernández-Christlieb F.
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- Florescano E.
- Galarza J.
- Galera-I-Monegal M.
- García-Guerra M.E.
- García-Martínez B.
- García-Martínez B.
- García-Romero A.
- García-Zambrano A.J.
- Gerhard P.
- Gibson C.
- González-Hermosillo F.
- González-Hermosillo F.
- Gruffund P.
- Haber W.
- Haverkamp-Begemann E.
- Jackson J.B.
- Kagan R.L.
- Kagan R.L.
- Kamen H.
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- Kobayashi T.
- Kubler G.
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- Leibsohn D.
- Licate J.A.
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- Lind M.
- Links J.G.
- Lockhart J.
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- Maderuelo J.
- Marcus J.
- Martínez H.
- McCafferty G.G.
- Melville E.G.K.
- Mitchell D.
- Molina A.D.
- Montero-García I.-A.
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- Nader H.
- Noguez X.
- Olwig K.R.
- Ramírez-Ruiz M.
- Ramírez-Ruiz M.
- Real Academia de la Historia
- Real Academia Española.
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- Reyes-García C.
- Roger A.
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- Publication venue
- 'Informa UK Limited'
- Publication date
- Field of study
No full textCandida bloodstream infections in intensive care units: analysis of the extended prevalence of infection in intensive care unit study
- Author
- 't Kindt H.
- Abbruzzese C.
- Abel P.
- Abulmagd M.
- Adén F.
- Afonso S.
- Aguilar G.
- Aguilar L.
- Aguirre G.
- Alan Javier Z.
- Alansary A.
- Albaya A.
- Aldrighi J.
- Alemparte-Pardavila E.
- Alhashemi J.
- Alheira-Rocha R.
- Ali A.
- Almeida E.
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- Amaro P.
- Ambike D.
- Amin P.
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- Anane S.
- Andrade C.
- Angstwurm Matthias
- Antonelli M.
- Antón Caraballo E.
- Arabi Y.
- Arias Antun A.
- Armaganidis A.
- Arribas M.
- Arroyo A.
- Assuncao M.
- Avila C.
- Azoulay Elie
- Azoulay Elie
- Bach F.
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- Bakshi C.
- Balasini S.
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- Banerjee A.
- Baptista M.
- Barahona D.
- Barbosa A.
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- Bartkowska-Sniatkowska A.
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- Publication venue
- 'Ovid Technologies (Wolters Kluwer Health)'
- Publication date
- 01/01/2011
- Field of study
No full textItem does not contain fulltextOBJECTIVES: To provide a global, up-to-date picture of the prevalence, treatment, and outcomes of Candida bloodstream infections in intensive care unit patients and compare Candida with bacterial bloodstream infection. DESIGN: A retrospective analysis of the Extended Prevalence of Infection in the ICU Study (EPIC II). Demographic, physiological, infection-related and therapeutic data were collected. Patients were grouped as having Candida, Gram-positive, Gram-negative, and combined Candida/bacterial bloodstream infection. Outcome data were assessed at intensive care unit and hospital discharge. SETTING: EPIC II included 1265 intensive care units in 76 countries. PATIENTS: Patients in participating intensive care units on study day. INTERVENTIONS: None. MEASUREMENT AND MAIN RESULTS: Of the 14,414 patients in EPIC II, 99 patients had Candida bloodstream infections for a prevalence of 6.9 per 1000 patients. Sixty-one patients had candidemia alone and 38 patients had combined bloodstream infections. Candida albicans (n = 70) was the predominant species. Primary therapy included monotherapy with fluconazole (n = 39), caspofungin (n = 16), and a polyene-based product (n = 12). Combination therapy was infrequently used (n = 10). Compared with patients with Gram-positive (n = 420) and Gram-negative (n = 264) bloodstream infections, patients with candidemia were more likely to have solid tumors (p < .05) and appeared to have been in an intensive care unit longer (14 days [range, 5-25 days], 8 days [range, 3-20 days], and 10 days [range, 2-23 days], respectively), but this difference was not statistically significant. Severity of illness and organ dysfunction scores were similar between groups. Patients with Candida bloodstream infections, compared with patients with Gram-positive and Gram-negative bloodstream infections, had the greatest crude intensive care unit mortality rates (42.6%, 25.3%, and 29.1%, respectively) and longer intensive care unit lengths of stay (median [interquartile range]) (33 days [18-44], 20 days [9-43], and 21 days [8-46], respectively); however, these differences were not statistically significant. CONCLUSION: Candidemia remains a significant problem in intensive care units patients. In the EPIC II population, Candida albicans was the most common organism and fluconazole remained the predominant antifungal agent used. Candida bloodstream infections are associated with high intensive care unit and hospital mortality rates and resource use
Candida bloodstream infections in intensive care units: analysis of the extended prevalence of infection in intensive care unit study
- Author
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- Publication venue
- Publication date
- 01/01/2011
- Field of study
No full textTo provide a global, up-to-date picture of the prevalence, treatment, and outcomes of Candida bloodstream infections in intensive care unit patients and compare Candida with bacterial bloodstream infection.
DESIGN:
A retrospective analysis of the Extended Prevalence of Infection in the ICU Study (EPIC II). Demographic, physiological, infection-related and therapeutic data were collected. Patients were grouped as having Candida, Gram-positive, Gram-negative, and combined Candida/bacterial bloodstream infection. Outcome data were assessed at intensive care unit and hospital discharge.
SETTING:
EPIC II included 1265 intensive care units in 76 countries.
PATIENTS:
Patients in participating intensive care units on study day.
INTERVENTIONS:
None.
MEASUREMENT AND MAIN RESULTS:
Of the 14,414 patients in EPIC II, 99 patients had Candida bloodstream infections for a prevalence of 6.9 per 1000 patients. Sixty-one patients had candidemia alone and 38 patients had combined bloodstream infections. Candida albicans (n = 70) was the predominant species. Primary therapy included monotherapy with fluconazole (n = 39), caspofungin (n = 16), and a polyene-based product (n = 12). Combination therapy was infrequently used (n = 10). Compared with patients with Gram-positive (n = 420) and Gram-negative (n = 264) bloodstream infections, patients with candidemia were more likely to have solid tumors (p < .05) and appeared to have been in an intensive care unit longer (14 days [range, 5-25 days], 8 days [range, 3-20 days], and 10 days [range, 2-23 days], respectively), but this difference was not statistically significant. Severity of illness and organ dysfunction scores were similar between groups. Patients with Candida bloodstream infections, compared with patients with Gram-positive and Gram-negative bloodstream infections, had the greatest crude intensive care unit mortality rates (42.6%, 25.3%, and 29.1%, respectively) and longer intensive care unit lengths of stay (median [interquartile range]) (33 days [18-44], 20 days [9-43], and 21 days [8-46], respectively); however, these differences were not statistically significant.
CONCLUSION:
Candidemia remains a significant problem in intensive care units patients. In the EPIC II population, Candida albicans was the most common organism and fluconazole remained the predominant antifungal agent used. Candida bloodstream infections are associated with high intensive care unit and hospital mortality rates and resource use
Enhanced infection prophylaxis reduces mortality in severely immunosuppressed HIV-infected adults and older children initiating antiretroviral therapy in Kenya, Malawi, Uganda and Zimbabwe: the REALITY trial
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- Publication venue
- 'International AIDS Society'
- Publication date
- 01/01/2016
- Field of study
Get PDFMeeting abstract FRAB0101LB from 21st International AIDS Conference 18–22 July 2016, Durban, South Africa.
Introduction: Mortality from infections is high in the first 6 months of antiretroviral therapy (ART) among HIV‐infected adults and children with advanced disease in sub‐Saharan Africa. Whether an enhanced package of infection prophylaxis at ART initiation would reduce mortality is unknown.
Methods:
The REALITY 2×2×2 factorial open‐label trial (ISRCTN43622374) randomized ART‐naïve HIV‐infected adults and children >5 years with CD4 <100 cells/mm3. This randomization compared initiating ART with enhanced prophylaxis (continuous cotrimoxazole plus 12 weeks isoniazid/pyridoxine (anti‐tuberculosis) and fluconazole (anti‐cryptococcal/candida), 5 days azithromycin (anti‐bacterial/protozoal) and single‐dose albendazole (anti‐helminth)), versus standard‐of‐care cotrimoxazole. Isoniazid/pyridoxine/cotrimoxazole was formulated as a scored fixed‐dose combination. Two other randomizations investigated 12‐week adjunctive raltegravir or supplementary food. The primary endpoint was 24‐week mortality.
Results:
1805 eligible adults (n = 1733; 96.0%) and children/adolescents (n = 72; 4.0%) (median 36 years; 53.2% male) were randomized to enhanced (n = 906) or standard prophylaxis (n = 899) and followed for 48 weeks (3.8% loss‐to‐follow‐up). Median baseline CD4 was 36 cells/mm3 (IQR: 16–62) but 47.3% were WHO Stage 1/2. 80 (8.9%) enhanced versus 108(12.2%) standard prophylaxis died before 24 weeks (adjusted hazard ratio (aHR) = 0.73 (95% CI: 0.54–0.97) p = 0.03; Figure 1) and 98(11.0%) versus 127(14.4%) respectively died before 48 weeks (aHR = 0.75 (0.58–0.98) p = 0.04), with no evidence of interaction with the two other randomizations (p > 0.8). Enhanced prophylaxis significantly reduced incidence of tuberculosis (p = 0.02), cryptococcal disease (p = 0.01), oral/oesophageal candidiasis (p = 0.02), deaths of unknown cause (p = 0.02) and (marginally) hospitalisations (p = 0.06) but not presumed severe bacterial infections (p = 0.38). Serious and grade 4 adverse events were marginally less common with enhanced prophylaxis (p = 0.06). CD4 increases and VL suppression were similar between groups (p > 0.2).
Conclusions:
Enhanced infection prophylaxis at ART initiation reduces early mortality by 25% among HIV‐infected adults and children with advanced disease. The pill burden did not adversely affect VL suppression. Policy makers should consider adopting and implementing this low‐cost broad infection prevention package which could save 3.3 lives for every 100 individuals treated
Vorapaxar in the secondary prevention of atherothrombotic events
- Author
- A. Ahsan
- A. Albirini
- A. Altschuller
- A. Antolick
- A. Arthur
- A. Bank
- A. Belemer
- A. Berni
- A. Betriu
- A. Biton
- A. Brady
- A. Brito
- A. Brock
- A. Bura-Riviere
- A. Caceres
- A. Cale
- A. Camp
- A. Campolongo
- A. Carvalho
- A. Centurion
- A. Cerny
- A. Claxton
- A. Cohen
- A. Comerota
- A. Csanyi
- A. Czlonkowska
- A. Da Silva
- A. DaCosta
- A. Dahlmans
- A. Del Rio Ligorit
- A. Desai
- A. Dijkshoorn
- A. Doerr
- A. Domzal-Stryga
- A. Don
- A. Elgasen
- A. Elis
- A. Engstrom
- A. Fallden-Gunnnarsson
- A. Fernandez
- A. Findik
- A. Fiscella
- A. Ford
- A. Frey
- A. Galla
- A. Gallino
- A. Garcia Pastor
- A. Gatkova
- A. Gavazzi
- A. Gil Nunez
- A. Giordano
- A. Glanz
- A. Goldhaber
- A. Gottsater
- A. Gruszka
- A. Guenther
- A. Guimaraes
- A. Gupta
- A. Habermeier
- A. Hakansson
- A. Hallmann
- A. Hamer
- A. Hellberg
- A. Hill
- A. Horak
- A. Howard
- A. Jakal
- A. Jaltier
- A. Joergensen
- A. Kaakkomaki
- A. Katz
- A. Kilian
- A. Kofmel
- A. Koralewska
- A. Korsnack
- A. Kubiak
- A. Kuhn
- A. Kuijper
- A. Labroo
- A. Lamy
- A. Lau-Sieckman
- A. Lazzari
- A. Ledda
- A. Ledger
- A. Lewis
- A. Linhart
- A. Linor
- A. Long
- A. Looney
- A. Loxton
- A. Lozada
- A. Manoj
- A. Martignoni
- A. Matoltsy
- A. McCann
- A. Milnerowicz
- A. Minisi
- A. Moore
- A. Morissette
- A. Mukherjee
- A. Munoz
- A. Murally
- A. Niederman
- A. Norden
- A. Odero
- A. Odhav
- A. Opdal
- A. Orozco
- A. Orpen
- A. Pande
- A. Pawlak
- A. Pedersen
- A. Peeters
- A. Pell
- A. Piti
- A. Podczeck-Schweighofer
- A. Prado
- A. Ramachandran
- A. Rees
- A. Rek
- A. Remes
- A. Renouf
- A. Revilla
- A. Rizzo
- A. Roach
- A. Roodt
- A. Rynkiewicz
- A. Salvador
- A. Sasaki
- A. Schaffranka
- A. Schlesinger
- A. Schmidt
- A. Scholtze
- A. Schut
- A. Shepler
- A. Shirwany
- A. Singhal
- A. Sjol
- A. Skene
- A. Slattery
- A. Souza
- A. Stilman
- A. Stoll
- A. Suzuki
- A. Szczudlik
- A. Tang
- A. Tarulla
- A. Teklinski
- A. Tilkian
- A. Turner
- A. Vadala
- A. Valikovics
- A. van der Spoel
- A. Vlastaris
- A. Walton
- A. Wardeh
- A. Whelan
- A. Wiseman
- A. Wojtarowicz
- A. Yoshioka
- A. Zangerle
- A.A. Chu
- A.B. Brum
- A.B. Chandler
- A.B. Teixeira
- A.H. Morsund
- A.H. Pereira
- A.J. Bradley
- A.J. Dalby
- A.J.O. Ophuis
- A.L. Marques
- A.L. Tetrault
- A.M. Kaalaas
- A.M. Zeiher
- A.O. Ophuis
- A.P. Horokosky
- A.P. Macagnan
- A.P. Vieira
- A.R. Alves
- A.R. Rajakumar
- A.S. Pandey
- A.S. Wong
- B. Abramson
- B. Amann-Vesti
- B. Aral-Becher
- B. Atkinson
- B. Bagnato
- B. Bertolet
- B. Birkeland
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- B. Blazejewska-Hyzorek
- B. Bozek
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- B. Palme
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- B. Singh
- B. Stein
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- B. Sussex
- B. Sutton
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- B.B. Kaspersen
- B.B. Olsen
- B.F. Lloyd
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- W.P. Klinke
- W.P. McGuinn
- W.R. Ardito
- W.R. Cashion
- W.W. Wilson
- X. Garcia-Moll
- X. Liu
- Y. Aladro Benito
- Y. Chandrashekhar
- Y. Cottin
- Y. Feldman
- Y. Hirano
- Y. Hiraoka
- Y. Honda
- Y. Lampl
- Y. Manabe
- Y. Niinuma
- Y. Okada
- Y. Oono
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- Y.K. Chan
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- Z. Kalita
- Z. Klimsa
- Z. Kornacewicz-Jach
- Z. Lorenc
- Z. Mohamed
- Z. Monhart
- Publication venue
- 'Massachusetts Medical Society'
- Publication date
- 01/01/2012
- Field of study
Get PDFItem does not contain fulltextBACKGROUND: Thrombin potently activates platelets through the protease-activated receptor PAR-1. Vorapaxar is a novel antiplatelet agent that selectively inhibits the cellular actions of thrombin through antagonism of PAR-1. METHODS: We randomly assigned 26,449 patients who had a history of myocardial infarction, ischemic stroke, or peripheral arterial disease to receive vorapaxar (2.5 mg daily) or matching placebo and followed them for a median of 30 months. The primary efficacy end point was the composite of death from cardiovascular causes, myocardial infarction, or stroke. After 2 years, the data and safety monitoring board recommended discontinuation of the study treatment in patients with a history of stroke owing to the risk of intracranial hemorrhage. RESULTS: At 3 years, the primary end point had occurred in 1028 patients (9.3%) in the vorapaxar group and in 1176 patients (10.5%) in the placebo group (hazard ratio for the vorapaxar group, 0.87; 95% confidence interval [CI], 0.80 to 0.94; P<0.001). Cardiovascular death, myocardial infarction, stroke, or recurrent ischemia leading to revascularization occurred in 1259 patients (11.2%) in the vorapaxar group and 1417 patients (12.4%) in the placebo group (hazard ratio, 0.88; 95% CI, 0.82 to 0.95; P=0.001). Moderate or severe bleeding occurred in 4.2% of patients who received vorapaxar and 2.5% of those who received placebo (hazard ratio, 1.66; 95% CI, 1.43 to 1.93; P<0.001). There was an increase in the rate of intracranial hemorrhage in the vorapaxar group (1.0%, vs. 0.5% in the placebo group; P<0.001). CONCLUSIONS: Inhibition of PAR-1 with vorapaxar reduced the risk of cardiovascular death or ischemic events in patients with stable atherosclerosis who were receiving standard therapy. However, it increased the risk of moderate or severe bleeding, including intracranial hemorrhage. (Funded by Merck; TRA 2P-TIMI 50 ClinicalTrials.gov number, NCT00526474.)
