46 research outputs found
Identificación de los pólenes en la flora ornamental de la ciudad de Granada (I)
- Publication venue
- Universidad de Granada, Facultad de Farmacia.
- Publication date
- 20/12/1987
- Field of study
Get PDFSe ha confeccionado una clave dicotómica para identificar los pólenes de la flora
ornamental de la ciudad de Granada, y un glosario de términos que incluye los rasgos
morfológicos más destacables de los mismos.A dichotomous key has been designed to identify the pollens from ornamental
flora found in the city of Granada, as well as a glossary of terms describing the most
outstanding !TIorphological characteristics of each
Identificación de los pólenes en la flora ornamental de la ciudad de Granada (I)
- Publication venue
- Editorial Universidad de Granada
- Publication date
- 20/12/1987
- Field of study
Get PDFA dichotomous key has been designed to identify the pollens from ornamental flora found in the city of Granada, as well as a glossary of terms describing the most outstanding morphological characteristics of each.Se ha confeccionado una clave dicotómica para identificar los pólenes de la flora ornamental de la ciudad de Granada, y un glosario de términos que incluye los rasgos morfológicos más destacables de los mismos
Aerobiological dynamics of the Cupressaceae pollen in Spain, 1992-98
- Author
- Publication venue
- Universidad de Córdoba, Departamento de Biología Vegetal y Ecología; Asociación de Palinólogos de Lengua Española
- Publication date
- 01/01/1999
- Field of study
Get PDFDetailed Characterization of Mesenchymal Stem/Stromal Cells from a Large Cohort of AML Patients Demonstrates a Definitive Link to Treatment Outcomes
- Author
- Anguita Eduardo
- Blanco Maria L.
- Bueno Clara
- Castaño Cardoso Julio
- Chaparro Alberto
- Delgado Julio
- Díaz de la Guardia Rafael
- Fuster Jose Luis
- Gómez-Casares Maite
- Juan Manel
- Lavoie Jessie R.
- Lopez-Millan Belen
- Menéndez Pablo
- Nomdedeu Josep
- Palomo Sanchis Laura
- Rosu-Myles Michael
- Universitat Autònoma de Barcelona
- Vives Susana
- Publication venue
- 'Elsevier BV'
- Publication date
- 01/01/2017
- Field of study
Get PDFAltres ajuts: Health Canada's Genomics Research and Development Initiative Phase VI (H4080-144541-2014-2019); Obra Social La Caixa-Fundació Josep Carreras and the Generalitat de Catalunya (SGR330); Asociación Española Contra el Cáncer (AECC-CI-2015)Bone marrow mesenchymal stem/stromal cells (BM-MSCs) are key components of the hematopoietic niche thought to have a direct role in leukemia pathogenesis. BM-MSCs from patients with acute myeloid leukemia (AML) have been poorly characterized due to disease heterogeneity. We report a functional, genetic, and immunological characterization of BM-MSC cultures from 46 AML patients, stratified by molecular/cytogenetics into low-risk (LR), intermediate-risk (IR), and high-risk (HR) subgroups. Stable MSC cultures were successfully established and characterized from 40 of 46 AML patients irrespective of the risk subgroup. AML-derived BM-MSCs never harbored tumor-specific cytogenetic/molecular alterations present in blasts, but displayed higher clonogenic potential than healthy donor (HD)-derived BM-MSCs. Although HD- and AML-derived BM-MSCs equally provided chemoprotection to AML cells in vitro, AML-derived BM-MSCs were more immunosuppressive/anti-inflammatory, enhanced suppression of lymphocyte proliferation, and diminished secretion of pro-inflammatory cytokines. Multivariate analysis revealed that the level of interleukin-10 produced by AML-derived BM-MSCs as an independent prognostic factor negatively affected overall survival. Collectively our data show that AML-derived BM-MSCs are not tumor related, but display functional differences contributing to therapy resistance and disease evolution. In this article, Díaz de la Guardia and colleagues report a functional, genetic, and immunological characterization of BM-MSC cultures from 46 AML patients, stratified by molecular/cytogenetics into low-risk (LR), intermediate-risk (IR), and high-risk (HR) subgroups. BM-MSCs never harbored tumor-specific cytogenetic/molecular alterations present in blasts, and IL-10 produced by AML-derived BM-MSCs is an independent prognostic factor negatively impacting on overall survival
Caribbean Corals in Crisis: Record Thermal Stress, Bleaching, and Mortality in 2005
- Author
- Alvarez-Filip Lorenzo
- Baca Bart
- Bartels Erich
- Bastidas Carolina
- Bouchon Claude
- Brandt Marilyn
- Bruckner Andrew W.
- Bunkley-Williams Lucy
- Cameron Andrew
- Causey Billy D.
- Chiappone Mark
- Christensen Tyler R. L.
- Crabbe M. James C
- Day Owen
- de la Guardia Elena
- DiResta Daniel
- Díaz-Pulido Guillermo
- Eakin C. Mark
- Gil-Agudelo Diego L.
- Gilliam David S.
- Ginsburg Robert N.
- Gore Shannon
- Guzmán Héctor M.
- Hendee James C.
- Hernández-Delgado Edwin A.
- Heron Scott F.
- Husain Ellen
- Jeffrey Christopher F. G.
- Jones Ross J.
- Jordán-Dahlgren Eric
- Kaufman Les S.
- Kline David I.
- Kramer Philip A.
- Lang Judith C.
- Lirman Diego
- Liu Gang
- Mallela Jennie
- Manfrino Carrie
- Marks Ken
- Maréchal Jean-Philippe
- Mihaly Jennifer
- Miller W. Jeff
- Morgan Jessica A.
- Mueller Erich M.
- Muller Erinn M.
- Orozco Toro Carlos A.
- Oxenford Hazel A.
- Ponce-Taylor Daniel
- Quinn Norman
- Ramírez Alberto Rodríguez
- Ritchie Kim B.
- Roberson Kimberly Woody
- Rodríguez Sebastián
- Romano Sandra
- Samhouri Jameal F.
- Schmahl George P.
- Shank Burton V.
- Skirving William J.
- Smith Tyler B.
- Steiner Sascha C. C.
- Sánchez Juan A.
- Villamizar Estrella
- Walsh Sheila M.
- Walter Cory
- Weil Ernesto
- Williams Ernest H.
- Yusuf Yusri
- Publication venue
- 'Public Library of Science (PLoS)'
- Publication date
- 10/12/2015
- Field of study
Get PDFBACKGROUND The rising temperature of the world's oceans has become a major threat to coral reefs globally as the severity and frequency of mass coral bleaching and mortality events increase. In 2005, high ocean temperatures in the tropical Atlantic and Caribbean resulted in the most severe bleaching event ever recorded in the basin. METHODOLOGY/PRINCIPAL FINDINGS Satellite-based tools provided warnings for coral reef managers and scientists, guiding both the timing and location of researchers' field observations as anomalously warm conditions developed and spread across the greater Caribbean region from June to October 2005. Field surveys of bleaching and mortality exceeded prior efforts in detail and extent, and provided a new standard for documenting the effects of bleaching and for testing nowcast and forecast products. Collaborators from 22 countries undertook the most comprehensive documentation of basin-scale bleaching to date and found that over 80% of corals bleached and over 40% died at many sites. The most severe bleaching coincided with waters nearest a western Atlantic warm pool that was centered off the northern end of the Lesser Antilles. CONCLUSIONS/SIGNIFICANCE Thermal stress during the 2005 event exceeded any observed from the Caribbean in the prior 20 years, and regionally-averaged temperatures were the warmest in over 150 years. Comparison of satellite data against field surveys demonstrated a significant predictive relationship between accumulated heat stress (measured using NOAA Coral Reef Watch's Degree Heating Weeks) and bleaching intensity. This severe, widespread bleaching and mortality will undoubtedly have long-term consequences for reef ecosystems and suggests a troubled future for tropical marine ecosystems under a warming climate.This work was partially supported by salaries from the NOAA Coral Reef Conservation Program to the NOAA Coral Reef Conservation Program authors. NOAA provided funding to Caribbean ReefCheck investigators to undertake surveys of bleaching and mortality. Otherwise, no funding from outside authors' institutions was necessary for the undertaking of this study. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript
Calcium renal lithiasis: metabolic diagnosis and medical treatment
- Author
- Alapont Pérez FM
- Annuk M
- Areses Trapote R
- Arrabal Martín M
- Arrabal Martín M
- Arrabal-Martín M
- Arrabal-Polo MA
- Arrabal-Polo MA
- Asplin JR
- Bek-Jensen H
- Bihl G
- Blackwood AM
- Bushinsky DA
- Chandhoke PJ
- Cirillo M
- Daudon M
- Eliahou R
- Evan A
- Evan AP
- Evan AP
- Fernández-Rodríguez A
- Fink HA
- Frick KK
- Giusti A
- Gomes SA
- Grases F
- Grases F
- Grases F
- Hall PM
- Hermida Pérez JA
- Hoppe B
- Hoppe B
- Jiménez Verdejo A
- Juan Garrido-Gomez
- Lancina Martín JA
- Lancina Martín JA
- Lewandowski S
- Madore F
- Madore F
- Matlaga BR
- Miguel Angel Arrabal-Polo
- Miguel Arrabal-Martin
- Ossandón Salas E
- Pak CY
- Pak CY
- Park S
- Parmar MS
- Pietrow PR
- Reed BY
- Reina Ruiz CM
- Sakhaee K
- Sakhaee K
- Schwille PO
- Siva S
- Soucie JM
- Stechman MJ
- Straub M
- Tiselius HG
- Tiselius HG
- Tsujihata M
- Valle Díaz de la Guardia F
- Worcester EM
- Worcester EM
- Yuen JW
- Zerwekh JE
- Zimmerer T
- Publication venue
- 'FapUNIFESP (SciELO)'
- Publication date
- Field of study
Full text linkA922 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
- Alcázar L
- Aldabo-Pallas T
- Aldana NN
- Aldecoa C
- Alegría L
- Alejandro R
- Alejo GC
- Alejos RM
- Alexandrova E
- Algarte R
- Algarte R
- Algieri I
- Algora-Weber A
- Alhamdi Y
- Aliaga FA
- Aliberti S
- Alkan A
- Almudena PM
- Almudevar PM
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- Altıntas ND
- Alvarez J
- Alves SC
- Alzola LM
- Amargianitakis V
- Amaro R
- Amato MB
- Ambler M
- Amerongen MP
- Amininejad T
- Amor LL
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- Anand RK
- Andersen LW
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- Araujo NJ
- Araujo VF
- ARIAM registry of adult cardiac surgery
- ARIAM-ANDALUCIA
- Arias CC
- Arias N
- Arias-Verdu MD
- Arias-Verdu MD
- Arias-Verdu MD
- Armaganidis A
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- Arrigo M
- Arslantas MK
- Artiguenave M
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- Avilés-Jurado FX
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- CAPCRI Study
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- Castañeda DP
- Castellana D
- Castellanos A
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- Castillo-Lorente E
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- Cavalcanti D
- Cavalheiro AM
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- Cavicchi FZ
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- Chernyshuk S
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- Chou W
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- Chouvarda I
- Christopher KB
- Chrétien JM
- Chrétien JM
- Chrétien JM
- Chumaev A
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- Cinnella G
- Citerio G
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- Clemente EA
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- Cordón J
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- Curiel-Balsera E
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- Curtis A
- Cuthbertson BH
- Cutuli SL
- Câmara M
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- da Silva SL
- da Silva VZ
- Daga-Ruiz D
- Dalhuisen A
- Dalorzo M
- Damas P
- Dambrosio M
- Damås JK
- Das Neves A
- David H
- Davis C
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- Day A
- de Abreu MG
- De Backer A
- De Brito-Ashurst I
- De Cassai A
- De Freitas FF
- De Gasperi A
- de Hoyos EA
- De la Calle-Pedrosa N
- de la Fuente MV
- De La Fuente-Martos C
- De La Fuente-Martos C
- De La Rica AS
- De la Torre MA
- De Maglie M
- De Maglie M
- de Molina FJ
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- de Oca Sandoval MA
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- de Vera AP
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- Dimopoulou IK
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- Elbers PW
- Elgendy M
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- Engelberts D
- ENVIN-HELICS Study Group
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- Escoval A
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- Ferrón FR
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- Fiks T
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- Fileković S
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- Filho CA
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- FINNRESUSCI Study Group
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- FROG ICU Investigators
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- Garcia-Alvarez JM
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- Gattinoni L
- Gaudard P
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- 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
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- Gherli T
- Ghosh S
- Giannantonio M
- Giannopoulos A
- Giesinger RE
- Gigorro RG
- Gil EM
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- Gimillo MR
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- Gioia A
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- Godinho I
- Godoy K
- Goldsworthy M
- Golovnya E
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- Gommers D
- Gommers D
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- Gonzalez-Engroba R
- González AS
- González BS
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- González-Jiménez AI
- Gonçalves B
- Goodwin S
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- Gordillo-Brenes A
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- Gordon M
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- Gouveia J
- Gracia RM
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- Granada RM
- Granados PR
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- Granillo JF
- Grassi L
- Grasso S
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- Green RS
- Greer M
- Gregory S
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- Grossestreuer A
- Guanziroli M
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- Haniffa R
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- Hayakawa M
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- Herruzo-Aviles A
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- Hewitt H
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- Hidalgo C
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- Hirayama T
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- Horstmann C
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- Howes D
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- Jardim JJ
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- Jonas M
- Jonas M
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- Jovaisa T
- JSEPTIC (Japanese Society of Education for Physicians and Trainees in Intensive Care) Clinical Trial Group
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- Kaczirek K
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- Kalenka A
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- Kleinpell R
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- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- 01/01/2016
- Field of study
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Guidelines for the use and interpretation of assays for monitoring autophagy (4th edition)1.
- Author
- Abdel-Aziz AK
- Abdelfatah S
- Abdellatif M
- Abdoli A
- Abel S
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- Zwerschke W
- Álvarez ÉMC
- Ávalos Y
- Önal G
- Üstün S
- Čolić M
- Đokić J
- Žerovnik E
- Publication venue
- 'Informa UK Limited'
- Publication date
- 01/01/2021
- Field of study
Get PDFIn 2008, we published the first set of guidelines for standardizing research in autophagy. Since then, this topic has received increasing attention, and many scientists have entered the field. Our knowledge base and relevant new technologies have also been expanding. Thus, it is important to formulate on a regular basis updated guidelines for monitoring autophagy in different organisms. Despite numerous reviews, there continues to be confusion regarding acceptable methods to evaluate autophagy, especially in multicellular eukaryotes. Here, we present a set of guidelines for investigators to select and interpret methods to examine autophagy and related processes, and for reviewers to provide realistic and reasonable critiques of reports that are focused on these processes. These guidelines are not meant to be a dogmatic set of rules, because the appropriateness of any assay largely depends on the question being asked and the system being used. Moreover, no individual assay is perfect for every situation, calling for the use of multiple techniques to properly monitor autophagy in each experimental setting. Finally, several core components of the autophagy machinery have been implicated in distinct autophagic processes (canonical and noncanonical autophagy), implying that genetic approaches to block autophagy should rely on targeting two or more autophagy-related genes that ideally participate in distinct steps of the pathway. Along similar lines, because multiple proteins involved in autophagy also regulate other cellular pathways including apoptosis, not all of them can be used as a specific marker for bona fide autophagic responses. Here, we critically discuss current methods of assessing autophagy and the information they can, or cannot, provide. Our ultimate goal is to encourage intellectual and technical innovation in the field
