113 results on '"Murcia, L."'
Search Results
2. On a bi-stability regime and the existence of odd subharmonics in a Comb-drive MEMS model with cubic stiffness
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Núñez, D. and Murcia, L.
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- 2023
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3. Stable periodic oscillations in simple parallel-plate MEMS based on a family of graphene-like materials
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Núñez, D., Galán-Vioque, J., and Murcia, L.
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- 2023
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4. Odd periodic oscillations in Comb-drive finger actuators
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Núñez, D., Larreal, O., and Murcia, L.
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- 2021
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5. Density assessment and reporting for Phlebotomus perniciosus and other sand fly species in periurban residential estates in Spain
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Muñoz, C., Risueño, J., Pérez-Cutillas, P., Bernal, L. J., Ortiz, J. M., Ruiz de Ybáñez, R., Sánchez-López, P. F., Martínez-Carrasco, C., Del Río, L., De la Rúa, P., García-Martínez, J. D., Gonzálvez, M., Murcia, L., Collantes, F., Goyena, E., Spitzova, T., Elshanat, S., and Berriatua, E.
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- 2021
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6. Stable periodic oscillations in simple parallel-plate MEMS based on a family of graphene-like materials
- Author
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Universidad de Sevilla. Departamento de Matemática Aplicada II (ETSI), Universidad de Sevilla. TIC130: Investigación en sistemas dinámicos en ingeniería, Pontificia Universidad Javeriana Cali Capital Semilla, Colombia, Núñez, Daniel E., Galán Vioque, Jorge Francisco, Murcia, L., Universidad de Sevilla. Departamento de Matemática Aplicada II (ETSI), Universidad de Sevilla. TIC130: Investigación en sistemas dinámicos en ingeniería, Pontificia Universidad Javeriana Cali Capital Semilla, Colombia, Núñez, Daniel E., Galán Vioque, Jorge Francisco, and Murcia, L.
- Abstract
In this paper we study the existence, multiplicity and the stability properties of lateral (positive) periodic oscillations in a class of simple parallel-plate MEM devices based on graphene and graphene-like materials with a non-constant -periodic input voltage, which are modeled by Duffing equations. We also complete some partial results previously obtained in Kadyrov et al., (2021) for this kind of models and show analytically the existence of a positive asymptotically locally stable -periodic oscillation, in particular for the graphene-based model. These results could be an approach to a design principle for stabilizing the device without an external controller by means of a tuning of the input voltage. Numerical continuation and simulations are also provided in order to illustrate theoretical results and to reveal the robustness of the graphene-based MEMS compared to the traditional ones.
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- 2023
7. Stable periodic oscillations in simple parallel-plate MEMS based on a family of graphene-like materials
- Author
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Núñez, Daniel E., Galán Vioque, Jorge Francisco, Murcia, L., Universidad de Sevilla. Departamento de Matemática Aplicada II (ETSI), Universidad de Sevilla. TIC130: Investigación en sistemas dinámicos en ingeniería, and Pontificia Universidad Javeriana Cali Capital Semilla, Colombia
- Subjects
MEMS ,Lower and upper solutions method ,Periodic solutions ,Linear stability ,Graphene - Abstract
In this paper we study the existence, multiplicity and the stability properties of lateral (positive) periodic oscillations in a class of simple parallel-plate MEM devices based on graphene and graphene-like materials with a non-constant -periodic input voltage, which are modeled by Duffing equations. We also complete some partial results previously obtained in Kadyrov et al., (2021) for this kind of models and show analytically the existence of a positive asymptotically locally stable -periodic oscillation, in particular for the graphene-based model. These results could be an approach to a design principle for stabilizing the device without an external controller by means of a tuning of the input voltage. Numerical continuation and simulations are also provided in order to illustrate theoretical results and to reveal the robustness of the graphene-based MEMS compared to the traditional ones.
- Published
- 2023
8. Evidence for widespread Leishmania infantum infection among wild carnivores in L. infantum periendemic northern Spain
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Del Río, L., Chitimia, L., Cubas, A., Victoriano, I., De la Rúa, P., Gerrikagoitia, X., Barral, M., Muñoz-García, C.I., Goyena, E., García-Martínez, D., Fisa, R., Riera, C., Murcia, L., Segovia, M., and Berriatua, E.
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- 2014
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9. Success of benznidazole chemotherapy in chronic Trypanosoma cruzi-infected patients with a sustained negative PCR result
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Murcia, L., Carrilero, B., Ferrer, F., Roig, M., Franco, F., and Segovia, M.
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- 2016
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10. Cryptic Leishmaniosis by Leishmania infantum, a feature of canines only? A study of natural infection in wild rabbits, humans and dogs in southeastern Spain
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Chitimia, L., Muñoz-García, C.I., Sánchez-Velasco, D., Lizana, V., del Río, L., Murcia, L., Fisa, R., Riera, C., Giménez-Font, P., Jiménez-Montalbán, P., Martínez-Ramírez, Á., Meseguer-Meseguer, J.M., García-Bacete, I., Sánchez-Isarria, M.A., Sanchis-Monsonís, G., García-Martínez, J.D., Vicente, V., Segovia, M., and Berriatua, E.
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- 2011
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11. La educaci��n superior mediante plataformas tecnol��gicas, un medio para generar ambientes de aprendizaje virtuales
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Ric��rdez Jim��nez, Jer��nimo D., Murcia L��pez, Leticia, and Quijano Hern��ndez, Oliveth Maithe
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educaci��n ,plataformas tecnol��gicas ,aprendizaje virtual ,comunicaci��n virtual - Abstract
El sistema de educaci��n superior en M��xico ofrece distintas opciones de formaci��n para garantizar el desarrollo profesional, sin embargo, a ra��z de la pandemia por COVID-19 la situaci��n de la educaci��n en M��xico y en el mundo ha implicado un reto para los modelos educativos del pa��s. La necesidad de las instituciones de educaci��n superior para adecuar los sistemas tradicionales de educaci��n a una modalidad virtual ha modificado la cotidianidad de los estudiantes y docentes, a raz��n del uso imprescindible de las plataformas tecnol��gicas educativas a fin de que los estudiantes contin��en adquiriendo las competencias fundamentales para su formaci��n. La adopci��n de plataformas tecnol��gicas en el ��mbito educativo involucra el uso de diferentes tipos de herramientas destinadas para promover ambientes de aprendizaje, teniendo como objetivo facilitar la adquisici��n de conocimientos, creando materiales electr��nicos que complementen un entorno educativo virtual de calidad para garantizar que las y los j��venes adquieran habilidades t��cnicas y vocacionales. Las plataformas tecnol��gicas educativas constituyen los medios para la transmisi��n y adquisici��n del conocimiento, para cumplir con las unidades de competencia propuestas en los modelos educativos, fomentando las t��cnicas de autoaprendizaje por medio de la tecnolog��a. Por lo anterior, es necesario hacer una identificaci��n de las plataformas m��s efectivas, tomando en cuenta la aceptaci��n, conveniencia y el impacto que reflejan en el desarrollo de los nuevos modelos de educaci��n, evaluando su funcionalidad y flexibilidad para el uso de estudiantes y docentes.
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- 2021
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12. LA AUDITOR��A CONTINUA: EL NUEVO RETO DE LA FISCALIZACI��N EN M��XICO
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Hern��ndez Villa, Xochitl Citlali. and Murcia L��pez, Leticia.
- Abstract
El objetivo de la presente investigaci��n es describir la utilidad de la auditoria continua en el contexto de la fiscalizaci��n de entes p��blicos en M��xico; a trav��s de un enfoque descriptivo y anal��tico. Las organizaciones a nivel mundial est��n siendo transformadas por las Tecnolog��as de Informaci��n y Comunicaci��n (TIC), lo que ha permitido que no existan fronteras de espacio ni de tiempo para desarrollar las organizaciones, haci��ndolas incluso virtuales. El ��ndice de percepci��n de corrupci��n a nivel internacional, elaborado por Transparencia Internacional en el a��o 2020, ubica a M��xico en el puesto 124 de 180 pa��ses. Uno de los problemas actuales en M��xico es que las funciones de resarcimiento del da��o causado al patrimonio p��blico, no se favorecen con la actual estructura y medios ineficientes. Es claro que el control no debe ser ni previo, ni posterior; tiene que ser en tiempo real y, para avanzar hacia la consecuci��n de este prop��sito, es necesario estandarizar los procesos y procedimientos de control; acudir a herramientas como las TIC, con lo cual se puede garantizar un mayor control, que impacta de manera significativa, sus procesos estrat��gicos, misionales y de apoyo.
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- 2021
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13. Biodversidad subterránea y epigea de los sistemas cársticos de El Peñón (Andes), Santander, Colombia
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Natalia Vargas, Maribel Arias-Mañosca, Daniela Martínez, Lina M. Mesa S., Angélica Benítez, Nubia Strella Santamaría Patiño, Magnolia Longo, Teddy Angarita-Sierra, Johanna Dulcey-Ulloa, Justo Arosemena, Johann E. Cárdenas-Bautista, José Andrés Deosa, Roman Hapka, Silvia Restrepo, Alejandro Lopera-Toro, Carlos Mario López-Orozco, Felipe Villegas, Angie Mayerli Vargas Barrera, Wilber González, Dan Straley, Humberto Mendoza-Cifuentes, Andrea Benavides-Calderón, Osvaldo Villareal, Juan David Rodríguez-Torres, Arley Davinsson Ruíz, Javier Jérez Aguilar, Jesús Fernández-Auderset, Diego Casallas-Pabón, Mario Andrés Murcia L., Edwin González Patiño, Diana Morales-B., Delfina Moreno-Ariza, Sleyder Galeano Ruíz, Andrés Romero, Camila Durán, Camilo Martínez-Martínez, Maykol Galeano Ruíz, Ricardo Pinto, Braddy Merrit, Mario Andrés García-Mora, María del Socorro Sierra, Camilo Chica, Berenice Vásquez Vargas, Karen Lorena Peña González, Ciro Alfonso Jerez, Yilver Galeano Ruíz, Javier C. Barriga, Angélica Díaz-Pulido, Andrés R. Acosta-Galvis, Carlos A. Lasso, Nicolás Valdivieso, Edison Duarte, Laura Castañeda, Jonnathan Galeano Ruíz, Sergio Córdoba Córdoba, Yaneth Muñoz-Saba, Jorge E. García-Melo, and Laura Pineda
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- 2020
14. Fixed places, shifting distances: remittance houses and migrants’ negotiation of home in Ecuador
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Boccagni, P and Pérez-Murcia, L. E.
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- 2020
15. Chemical composition and bioactivity potential of the new endosequence BC Sealer formulación hiflow
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Rodríguez Lozano, Francisco Javier, López-García, Sergio, García-Bernal, David, Tomás-Catalá, C.J., Santos, J.M., Llena Puy, María Carmen, Lozano, A., Murcia, L., and Forner Navarro, Leopoldo
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Odontologia - Abstract
Aim To evaluate in a laboratory setting the effects of Endosequence BC Sealer HiFlow (Brasseler USA, Savannah, GA, USA), a novel calcium silicate-based sealer developed for use in warm canal filling techniques, on human periodontal ligament stem cells (hPDLSCs). Methodology Eluates of EndoSequence BC Sealer HiFlow (BCHiF) (Brasseler USA), EndoSequence BC Sealer (BCS) (Brasseler USA) and AH Plus (AHP) (Dentsply DeTrey GmbH, Konstanz, Germany), were placed in contact with hPDLSCs. The characterisation of the chemical elements of the root canal sealers was assessed using Scanning Electron Microscopy and Energy Dispersive X-ray analysis (SEM-EDX). Inductively Coupled Plasma Mass Spectrometry (ICP-MS) was used to determine the ion release of the sealers. MTT assay and wound healing techniques were used to determine cell viability and migration, respectively. Cell morphology and cell attachment were assessed using a direct contact technique of hPDLSCs onto the surface of the sealers and analysed by SEM. The bioactivity potential was carried out with the Alizarin Red and qPCR testing methods. The statistical differences were evaluated using one-way ANOVA and Tukey´s test (p0.05). Both BCS and BCHiF had similar rates of cell migration to the control group at 24 and 48 hours. Cell morphology and adhesion capacity were also similar for BCS and BCHiF groups, while the AHP group was associated with reduced adhesion capacity. The Alizarin Red assay revealed a significant difference between the BCS and the control group (p
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- 2020
16. Chemical composition and bioactivity potential of the new Endosequence BC Sealer formulation HiFlow
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Rodríguez‐Lozano, F. J., primary, López‐García, S., additional, García‐Bernal, D., additional, Tomás‐Catalá, C. J., additional, Santos, J. M., additional, Llena, C., additional, Lozano, A., additional, Murcia, L., additional, and Forner, L., additional
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- 2020
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17. A non-canonical RNAi pathway controls virulence and genome stability in Mucorales
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Pérez-Arques, C., primary, Navarro-Mendoza, M.I., additional, Murcia, L., additional, Navarro, E., additional, Garre, V., additional, and Nicolás, F., additional
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- 2020
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18. Mucor circinelloides Thrives inside the Phagosome through an Atf-Mediated Germination Pathway.
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Chowdhary, A, Pérez-Arques, C, Navarro-Mendoza, MI, Murcia, L, Lax, C, Martínez-García, P, Heitman, J, Nicolás, FE, Garre, V, Chowdhary, A, Pérez-Arques, C, Navarro-Mendoza, MI, Murcia, L, Lax, C, Martínez-García, P, Heitman, J, Nicolás, FE, and Garre, V
- Abstract
Mucormycosis is an emerging fungal infection that is often lethal due to the ineffectiveness of current therapies. Here, we have studied the first stage of this infection-the germination of Mucor circinelloides spores inside phagocytic cells-from an integrated transcriptomic and functional perspective. A relevant fungal gene network is remodeled in response to phagocytosis, being enriched in crucial functions to survive and germinate inside the phagosome, such as nutritional adaptation and response to oxidative stress. Correspondingly, the phagocytic cells induced a specific proinflammatory and apoptotic response to the pathogenic strain. Deletion of fungal genes encoding putative transcription factors (atf1, atf2, and gcn4), extracellular proteins (chi1 and pps1), and an aquaporin (aqp1) revealed that these genes perform important roles in survival following phagocytosis, germination inside the phagosome, and virulence in mice. atf1 and atf2 play a major role in these pathogenic processes, since their mutants showed the strongest phenotypes and both genes control a complex gene network of secondarily regulated genes, including chi1 and aqp1 These new insights into the initial phase of mucormycosis define genetic regulators and molecular processes that could serve as pharmacological targets.IMPORTANCE Mucorales are a group of ancient saprophytic fungi that cause neglected infectious diseases collectively known as mucormycoses. The molecular processes underlying the establishment and progression of this disease are largely unknown. Our work presents a transcriptomic study to unveil the Mucor circinelloides genetic network triggered in fungal spores in response to phagocytosis by macrophages and the transcriptional response of the host cells. Functional characterization of differentially expressed fungal genes revealed three transcription factors and three extracellular proteins essential for the fungus to survive and germinate inside the phagosome and to cause diseas
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- 2019
19. An observational longitudinal study to evaluate tools and strategies available for the diagnosis of Congenital Chagas Disease in a non-endemic country
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Simón, M., Gil-Gallardo, L.J., Asunción Iborra, M., Carrilero, B., López López, Manuel Carlos, Romay-Barja, M., Murcia, L., Thomas, María del Carmen, Benito, A., Segovia, M., Simón, M., Gil-Gallardo, L.J., Asunción Iborra, M., Carrilero, B., López López, Manuel Carlos, Romay-Barja, M., Murcia, L., Thomas, María del Carmen, Benito, A., and Segovia, M.
- Abstract
Objectives: Congenital Chagas Disease (CCD) has become a global health problem. Early diagnosis and treatment is essential for the cure of the disease. Our aim was to evaluate techniques and samples used for the diagnosis of CCD in order to improve diagnostic strategies. Methods: A total of 181 children born in Spain from Latin American Chagas-infected mothers were consecutively enrolled and studied by microhematocrit, PCR and serology tests at 0–2, 6 and 9–12 months of age and followed up when it was required. Samples of cord blood and peripheral blood were collected for T. cruzi detection by PCR. Parasite culture was performed in patients with a positive PCR. Results: Of 181 children, 7 children (3.9%) were lost to follow-up. A total of 174 children completed follow-up, 12 were diagnosed with CCD (6.9%) and 162 (93.1%) as uninfected children (negative serology tests at the end of the follow-up). Traditional parasitological diagnosis by microhematocrit had a poor performance (sensitivity was 10%), while PCR in peripheral blood showed high sensitivity (90.9%) and specificity (100%), allowing the early diagnosis of 9 infected children during the first 6-months-old. In the other 3 congenital cases, diagnosis was only possible at 12 months by serological and molecular techniques. However, PCR in cord blood showed low sensitivity (33.3%) and less specificity (96.4%) for the diagnosis. Conclusion: PCR in peripheral blood has proven to be the most adequate strategy for the diagnosis of CCD, allowing an early and reliable diagnosis.
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- 2019
20. Cytocompatibility, bioactivity potential, and ion release of three premixed calcium silicate-based sealers
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López-García, S., primary, Myong-Hyun, Baek, additional, Lozano, A., additional, García-Bernal, D., additional, Forner, L., additional, Llena, C., additional, Guerrero-Gironés, J., additional, Murcia, L., additional, and Rodríguez-Lozano, F. J., additional
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- 2019
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21. Evaluation of changes in ion release and biological properties of NeoMTA‐Plus and Endocem‐MTA exposed to an acidic environment
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Rodríguez‐Lozano, F. J., primary, Collado‐González, M., additional, López‐García, S., additional, García‐Bernal, D., additional, Moraleda, J. M., additional, Lozano, A., additional, Forner, L., additional, Murcia, L., additional, and Oñate‐Sánchez, R. E., additional
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- 2019
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22. GuttaFlow Bioseal promotes spontaneous differentiation of human periodontal ligament stem cells into cementoblast-like cells
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Rodríguez-Lozano, F.J., primary, Collado-González, M., additional, Tomás-Catalá, C.J., additional, García-Bernal, D., additional, López, S., additional, Oñate-Sánchez, R.E., additional, Moraleda, J.M., additional, and Murcia, L., additional
- Published
- 2019
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23. Cytocompatibility, bioactivity potential, and ion release of three premixed calcium silicate-based sealers.
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López-García, S., Myong-Hyun, Baek, Lozano, A., García-Bernal, D., Forner, L., Llena, C., Guerrero-Gironés, J., Murcia, L., and Rodríguez-Lozano, F. J.
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CELL morphology ,CELL migration ,PERIODONTAL ligament ,SURFACE sealers ,CALCIUM ,CYTOCOMPATIBILITY - Abstract
Objective: Compositional modifications may alter the biological and physicochemical characteristics of calcium silicate-based sealers (CSBS) and, ultimately, their bioactivity. The main objective of this study was to evaluate the biological properties of three CSBS: EndoSequence BC Sealer, Ceraseal, and Endoseal mineral trioxide aggregate. Materials and methods: Human periodontal ligament stem cells (hPDLSCs) were exposed to several eluates of CSBS. The ion release profile and pH were determined, and metabolic activity and cell migration were assessed using the MTT and wound healing assays. hPDLSCs were cultured in direct contact with the surface of each material, and cell morphology and attachment were analyzed by scanning electron microscopy (SEM). Bioactivity potential was assessed by RT-qPCR and mineralization assays. Statistical differences between biomaterials were assessed using one- or two-way ANOVA (α < 0.05). Results: All materials showed an alkaline pH, although Endoseal exhibited a significantly higher pH compared with the other CSBS (p < 0.05). Ceraseal released significantly more Ca
2+ (p < 0.05) than EndoSequence BC Sealer and Endoseal. Interestingly, Endoseal induced a significant reduction in cell viability and cell migration compared with the control (p < 0.001). Moreover, SEM showed abundant cells adhering to EndoSequence BC Sealer and Ceraseal surfaces, whereas very few round cells were detected on the surface of Endoseal. Finally, Ceraseal and EndoSequence induced ALP, CAP, and CEMP-1 expression and a significantly higher mineralization capacity than Endoseal (***p < 0.001). Conclusions: The eluates from EndoSequence BC Sealer and Ceraseal displayed higher cell viability, cell attachment, cell migration rates, and ion release rates than Endoseal. Ceraseal and EndoSequence BC Sealer exhibited significantly more gene expression and mineralization capacity than Endoseal. Clinical relevance: The results obtained in the present work suggest that EndoSequence BC Sealer and Ceraseal possess biological properties that make them suitable materials for root canal treatment. [ABSTRACT FROM AUTHOR]- Published
- 2020
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24. Pratiques alimentaires dans la petite enfance et caractéristiques du sommeil entre 2 et 5–6 ans dans la cohorte EDEN
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Murcia, L., primary, Reynaud, E., additional, Davisse-Paturet, C., additional, Forhan, A., additional, Heude, B., additional, Charles, M.A., additional, De Lauzon-Guillain, B., additional, and Plancoulaine, S., additional
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- 2018
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25. Abstracts from Hydrocephalus 2016.
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Adam, A, Robison, J, Lu, J, Jose, R, Badran, N, Vivas-Buitrago, T, Rigamonti, D, Sattar, A, Omoush, O, Hammad, M, Dawood, M, Maghaslah, M, Belcher, T, Carson, K, Hoffberger, J, Jusué Torres, I, Foley, S, Yasar, S, Thai, Q A, Wemmer, J, Klinge, P, Al-Mutawa, L, Al-Ghamdi, H, Carson, K A, Asgari, M, de Zélicourt, D, Kurtcuoglu, V, Garnotel, S, Salmon, S, Balédent, O, Lokossou, A, Page, G, Balardy, L, Czosnyka, Z, Payoux, P, Schmidt, E A, Zitoun, M, Sevestre, M A, Alperin, N, Baudracco, I, Craven, C, Matloob, S, Thompson, S, Haylock Vize, P, Thorne, L, Watkins, L D, Toma, A K, Bechter, Karl, Pong, A C, Jugé, L, Bilston, L E, Cheng, S, Bradley, W, Hakim, F, Ramón, J F, Cárdenas, M F, Davidson, J S, García, C, González, D, Bermúdez, S, Useche, N, Mejía, J A, Mayorga, P, Cruz, F, Martinez, C, Matiz, M C, Vallejo, M, Ghotme, K, Soto, H A, Riveros, D, Buitrago, A, Mora, M, Murcia, L, Bermudez, S, Cohen, D, Dasgupta, D, Curtis, C, Domínguez, L, Remolina, A J, Grijalba, M A, Whitehouse, K J, Edwards, R J, Eleftheriou, A, Lundin, F, Fountas, K N, Kapsalaki, E Z, Smisson, H F, Robinson, J S, Fritsch, M J, Arouk, W, Garzon, M, Kang, M, Sandhu, K, Baghawatti, D, Aquilina, K, James, G, Thompson, D, Gehlen, M, Schmid Daners, M, Eklund, A, Malm, J, Gomez, D, Guerra, M, Jara, M, Flores, M, Vío, K, Moreno, I, Rodríguez, S, Ortega, E, Rodríguez, E M, McAllister, J P, Guerra, M M, Morales, D M, Sival, D, Jimenez, A, Limbrick, D D, Ishikawa, M, Yamada, S, Yamamoto, K, Junkkari, A, Häyrinen, A, Rauramaa, T, Sintonen, H, Nerg, O, Koivisto, A M, Roine, R P, Viinamäki, H, Soininen, H, Luikku, A, Jääskeläinen, J E, Leinonen, V, Kehler, U, Lilja-Lund, O, Kockum, K, Larsson, Elna-Marie, Riklund, K, Söderström, L, Hellström, P, Laurell, K, Kojoukhova, M, Sutela, A, Vanninen, R, Vanha, K I, Timonen, M, Rummukainen, J, Korhonen, V, Helisalmi, S, Solje, E, Remes, A M, Huovinen, J, Paananen, J, Hiltunen, M, Kurki, M, Martin, B, Loth, F, Luciano, M, Luikku, A J, Hall, A, Herukka, S K, Mattila, J, Lötjönen, J, Alafuzoff, Irina, Jurjević, I, Miyajima, M, Nakajima, M, Murai, H, Shin, T, Kawaguchi, D, Akiba, C, Ogino, I, Karagiozov, K, Arai, H, Reis, R C, Teixeira, M J, Valêncio, C G, da Vigua, D, Almeida-Lopes, L, Mancini, M W, Pinto, F C G, Maykot, R H, Calia, G, Tornai, J, Silvestre, S S S, Mendes, G, Sousa, V, Bezerra, B, Dutra, P, Modesto, P, Oliveira, M F, Petitto, C E, Pulhorn, H, Chandran, A, McMahon, C, Rao, A S, Jumaly, M, Solomon, D, Moghekar, A, Relkin, N, Hamilton, M, Katzen, H, Williams, M, Bach, T, Zuspan, S, Holubkov, R, Rigamonti, A, Clemens, G, Sharkey, P, Sanyal, A, Sankey, E, Rigamonti, K, Naqvi, S, Hung, A, Schmidt, E, Ory-Magne, F, Gantet, P, Guenego, A, Januel, A C, Tall, P, Fabre, N, Mahieu, L, Cognard, C, Gray, L, Buttner-Ennever, J A, Takagi, K, Onouchi, K, Thompson, S D, Thorne, L D, Tully, H M, Wenger, T L, Kukull, W A, Doherty, D, Dobyns, W B, Moran, D, Vakili, S, Patel, M A, Elder, B, Goodwin, C R, Crawford, J A, Pletnikov, M V, Xu, J, Blitz, A, Herzka, D A, Guerrero-Cazares, H, Quiñones-Hinojosa, A, Mori, S, Saavedra, P, Treviño, H, Maitani, K, Ziai, W C, Eslami, V, Nekoovaght-Tak, S, Dlugash, R, Yenokyan, G, McBee, N, Hanley, D F, Adam, A, Robison, J, Lu, J, Jose, R, Badran, N, Vivas-Buitrago, T, Rigamonti, D, Sattar, A, Omoush, O, Hammad, M, Dawood, M, Maghaslah, M, Belcher, T, Carson, K, Hoffberger, J, Jusué Torres, I, Foley, S, Yasar, S, Thai, Q A, Wemmer, J, Klinge, P, Al-Mutawa, L, Al-Ghamdi, H, Carson, K A, Asgari, M, de Zélicourt, D, Kurtcuoglu, V, Garnotel, S, Salmon, S, Balédent, O, Lokossou, A, Page, G, Balardy, L, Czosnyka, Z, Payoux, P, Schmidt, E A, Zitoun, M, Sevestre, M A, Alperin, N, Baudracco, I, Craven, C, Matloob, S, Thompson, S, Haylock Vize, P, Thorne, L, Watkins, L D, Toma, A K, Bechter, Karl, Pong, A C, Jugé, L, Bilston, L E, Cheng, S, Bradley, W, Hakim, F, Ramón, J F, Cárdenas, M F, Davidson, J S, García, C, González, D, Bermúdez, S, Useche, N, Mejía, J A, Mayorga, P, Cruz, F, Martinez, C, Matiz, M C, Vallejo, M, Ghotme, K, Soto, H A, Riveros, D, Buitrago, A, Mora, M, Murcia, L, Bermudez, S, Cohen, D, Dasgupta, D, Curtis, C, Domínguez, L, Remolina, A J, Grijalba, M A, Whitehouse, K J, Edwards, R J, Eleftheriou, A, Lundin, F, Fountas, K N, Kapsalaki, E Z, Smisson, H F, Robinson, J S, Fritsch, M J, Arouk, W, Garzon, M, Kang, M, Sandhu, K, Baghawatti, D, Aquilina, K, James, G, Thompson, D, Gehlen, M, Schmid Daners, M, Eklund, A, Malm, J, Gomez, D, Guerra, M, Jara, M, Flores, M, Vío, K, Moreno, I, Rodríguez, S, Ortega, E, Rodríguez, E M, McAllister, J P, Guerra, M M, Morales, D M, Sival, D, Jimenez, A, Limbrick, D D, Ishikawa, M, Yamada, S, Yamamoto, K, Junkkari, A, Häyrinen, A, Rauramaa, T, Sintonen, H, Nerg, O, Koivisto, A M, Roine, R P, Viinamäki, H, Soininen, H, Luikku, A, Jääskeläinen, J E, Leinonen, V, Kehler, U, Lilja-Lund, O, Kockum, K, Larsson, Elna-Marie, Riklund, K, Söderström, L, Hellström, P, Laurell, K, Kojoukhova, M, Sutela, A, Vanninen, R, Vanha, K I, Timonen, M, Rummukainen, J, Korhonen, V, Helisalmi, S, Solje, E, Remes, A M, Huovinen, J, Paananen, J, Hiltunen, M, Kurki, M, Martin, B, Loth, F, Luciano, M, Luikku, A J, Hall, A, Herukka, S K, Mattila, J, Lötjönen, J, Alafuzoff, Irina, Jurjević, I, Miyajima, M, Nakajima, M, Murai, H, Shin, T, Kawaguchi, D, Akiba, C, Ogino, I, Karagiozov, K, Arai, H, Reis, R C, Teixeira, M J, Valêncio, C G, da Vigua, D, Almeida-Lopes, L, Mancini, M W, Pinto, F C G, Maykot, R H, Calia, G, Tornai, J, Silvestre, S S S, Mendes, G, Sousa, V, Bezerra, B, Dutra, P, Modesto, P, Oliveira, M F, Petitto, C E, Pulhorn, H, Chandran, A, McMahon, C, Rao, A S, Jumaly, M, Solomon, D, Moghekar, A, Relkin, N, Hamilton, M, Katzen, H, Williams, M, Bach, T, Zuspan, S, Holubkov, R, Rigamonti, A, Clemens, G, Sharkey, P, Sanyal, A, Sankey, E, Rigamonti, K, Naqvi, S, Hung, A, Schmidt, E, Ory-Magne, F, Gantet, P, Guenego, A, Januel, A C, Tall, P, Fabre, N, Mahieu, L, Cognard, C, Gray, L, Buttner-Ennever, J A, Takagi, K, Onouchi, K, Thompson, S D, Thorne, L D, Tully, H M, Wenger, T L, Kukull, W A, Doherty, D, Dobyns, W B, Moran, D, Vakili, S, Patel, M A, Elder, B, Goodwin, C R, Crawford, J A, Pletnikov, M V, Xu, J, Blitz, A, Herzka, D A, Guerrero-Cazares, H, Quiñones-Hinojosa, A, Mori, S, Saavedra, P, Treviño, H, Maitani, K, Ziai, W C, Eslami, V, Nekoovaght-Tak, S, Dlugash, R, Yenokyan, G, McBee, N, and Hanley, D F
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- 2017
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26. Abstracts from Hydrocephalus 2016
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Adam, A., primary, Robison, J., additional, Lu, J., additional, Jose, R., additional, Badran, N., additional, Vivas-Buitrago, T., additional, Rigamonti, D., additional, Sattar, A., additional, Omoush, O., additional, Hammad, M., additional, Dawood, M., additional, Maghaslah, M., additional, Belcher, T., additional, Carson, K., additional, Hoffberger, J., additional, Jusué Torres, I., additional, Foley, S., additional, Yasar, S., additional, Thai, Q. A., additional, Wemmer, J., additional, Klinge, P., additional, Al-Mutawa, L., additional, Al-Ghamdi, H., additional, Carson, K. A., additional, Asgari, M., additional, de Zélicourt, D., additional, Kurtcuoglu, V., additional, Garnotel, S., additional, Salmon, S., additional, Balédent, O., additional, Lokossou, A., additional, Page, G., additional, Balardy, L., additional, Czosnyka, Z., additional, Payoux, P., additional, Schmidt, E. A., additional, Zitoun, M., additional, Sevestre, M. A., additional, Alperin, N., additional, Baudracco, I., additional, Craven, C., additional, Matloob, S., additional, Thompson, S., additional, Haylock Vize, P., additional, Thorne, L., additional, Watkins, L. D., additional, Toma, A. K., additional, Bechter, Karl, additional, Pong, A. C., additional, Jugé, L., additional, Bilston, L. E., additional, Cheng, S., additional, Bradley, W., additional, Hakim, F., additional, Ramón, J. F., additional, Cárdenas, M. F., additional, Davidson, J. S., additional, García, C., additional, González, D., additional, Bermúdez, S., additional, Useche, N., additional, Mejía, J. A., additional, Mayorga, P., additional, Cruz, F., additional, Martinez, C., additional, Matiz, M. C., additional, Vallejo, M., additional, Ghotme, K., additional, Soto, H. A., additional, Riveros, D., additional, Buitrago, A., additional, Mora, M., additional, Murcia, L., additional, Bermudez, S., additional, Cohen, D., additional, Dasgupta, D., additional, Curtis, C., additional, Domínguez, L., additional, Remolina, A. J., additional, Grijalba, M. A., additional, Whitehouse, K. J., additional, Edwards, R. J., additional, Eleftheriou, A., additional, Lundin, F., additional, Fountas, K. N., additional, Kapsalaki, E. Z., additional, Smisson, H. F., additional, Robinson, J. S., additional, Fritsch, M. J., additional, Arouk, W., additional, Garzon, M., additional, Kang, M., additional, Sandhu, K., additional, Baghawatti, D., additional, Aquilina, K., additional, James, G., additional, Thompson, D., additional, Gehlen, M., additional, Schmid Daners, M., additional, Eklund, A., additional, Malm, J., additional, Gomez, D., additional, Guerra, M., additional, Jara, M., additional, Flores, M., additional, Vío, K., additional, Moreno, I., additional, Rodríguez, S., additional, Ortega, E., additional, Rodríguez, E. M., additional, McAllister, J. P., additional, Guerra, M. M., additional, Morales, D. M., additional, Sival, D., additional, Jimenez, A., additional, Limbrick, D. D., additional, Ishikawa, M., additional, Yamada, S., additional, Yamamoto, K., additional, Junkkari, A., additional, Häyrinen, A., additional, Rauramaa, T., additional, Sintonen, H., additional, Nerg, O., additional, Koivisto, A. M., additional, Roine, R. P., additional, Viinamäki, H., additional, Soininen, H., additional, Luikku, A., additional, Jääskeläinen, J. E., additional, Leinonen, V., additional, Kehler, U., additional, Lilja-Lund, O., additional, Kockum, K., additional, Larsson, E. M., additional, Riklund, K., additional, Söderström, L., additional, Hellström, P., additional, Laurell, K., additional, Kojoukhova, M., additional, Sutela, A., additional, Vanninen, R., additional, Vanha, K. I., additional, Timonen, M., additional, Rummukainen, J., additional, Korhonen, V., additional, Helisalmi, S., additional, Solje, E., additional, Remes, A. M., additional, Huovinen, J., additional, Paananen, J., additional, Hiltunen, M., additional, Kurki, M., additional, Martin, B., additional, Loth, F., additional, Luciano, M., additional, Luikku, A. J., additional, Hall, A., additional, Herukka, S. K., additional, Mattila, J., additional, Lötjönen, J., additional, Alafuzoff, I., additional, Jurjević, I., additional, Miyajima, M., additional, Nakajima, M., additional, Murai, H., additional, Shin, T., additional, Kawaguchi, D., additional, Akiba, C., additional, Ogino, I., additional, Karagiozov, K., additional, Arai, H, additional, Reis, R. C., additional, Teixeira, M. J., additional, Valêncio, C. G., additional, da Vigua, D., additional, Almeida-Lopes, L., additional, Mancini, M. W., additional, Pinto, F. C. G., additional, Maykot, R. H., additional, Calia, G., additional, Tornai, J., additional, Silvestre, S. S. S., additional, Mendes, G., additional, Sousa, V., additional, Bezerra, B., additional, Dutra, P., additional, Modesto, P., additional, Oliveira, M. F., additional, Petitto, C. E., additional, Pulhorn, H., additional, Chandran, A., additional, McMahon, C., additional, Rao, A. S., additional, Jumaly, M., additional, Solomon, D., additional, Moghekar, A., additional, Relkin, N., additional, Hamilton, M., additional, Katzen, H., additional, Williams, M., additional, Bach, T., additional, Zuspan, S., additional, Holubkov, R., additional, Rigamonti, A., additional, Clemens, G., additional, Sharkey, P., additional, Sanyal, A., additional, Sankey, E., additional, Rigamonti, K., additional, Naqvi, S., additional, Hung, A., additional, Schmidt, E., additional, Ory-Magne, F., additional, Gantet, P., additional, Guenego, A., additional, Januel, A. C., additional, Tall, P., additional, Fabre, N., additional, Mahieu, L., additional, Cognard, C., additional, Gray, L., additional, Buttner-Ennever, J. A., additional, Takagi, K., additional, Onouchi, K, additional, Thompson, S. D., additional, Thorne, L. D., additional, Tully, H. M., additional, Wenger, T. L., additional, Kukull, W. A., additional, Doherty, D., additional, Dobyns, W. B., additional, Moran, D., additional, Vakili, S., additional, Patel, M. A., additional, Elder, B., additional, Goodwin, C. R., additional, Crawford, J. A., additional, Pletnikov, M. V., additional, Xu, J., additional, Blitz, A., additional, Herzka, D. A., additional, Guerrero-Cazares, H., additional, Quiñones-Hinojosa, A., additional, Mori, S., additional, Saavedra, P., additional, Treviño, H., additional, Maitani, K., additional, Ziai, W. C., additional, Eslami, V., additional, Nekoovaght-Tak, S., additional, Dlugash, R., additional, Yenokyan, G., additional, McBee, N., additional, and Hanley, D. F., additional
- Published
- 2017
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27. 0980 RELATIONS BETWEEN INFANT FEEDING PRACTICES AND SLEEP QUALITY OR DURATION AT AGE 2 IN THE FRENCH EDEN BIRTH COHORT
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Murcia, L, primary, de Lauzon Guillain, B, additional, Forhan, A, additional, Heude, B, additional, Charles, M, additional, and Plancoulaine, S, additional
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- 2017
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28. Side effects of benznidazole treatment in a cohort of patients with Chagas disease in non-endemic country
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Carrilero B, Murcia L, Martínez-Lage L, and Segovia M
- Subjects
Adult ,Male ,Gastrointestinal Diseases ,Arthritis ,Trypanosoma cruzi ,Middle Aged ,Trypanocidal Agents ,Cohort Studies ,Nitroimidazoles ,Spain ,Humans ,Chagas Disease ,Female ,Drug Eruptions ,Prospective Studies - Abstract
Chagas disease is a disease endemic in Latin America, caused by the parasite Trypanosoma cruzi. Benznidazole is the most commonly used drug for the etiological treatment of the disease although its effectiveness varies according to the phase of the same and toxic side effects are frequent. This prospective study describes the side effects of benznidazole treatment of a cohort of 373 chronic patients. Of these 40.2% presented adverse reactions. The most frequent side effect were dermatological reactions 32.4% (121 of 373) followed by digestive intolerance 9.1% (34 of 373). Surprisingly, three cases of migratory arthritis were observed. Patients treated with benznidazole must be followed up so that the long term incidence of side effects can be studied.
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- 2011
29. Spatial distribution of human asymptomatic Leishmania infantum infection in southeast Spain: A study of environmental, demographic and social risk factors
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Pérez-Cutillas, P., primary, Goyena, E., additional, Chitimia, L., additional, De la Rúa, P., additional, Bernal, L.J., additional, Fisa, R., additional, Riera, C., additional, Iborra, A., additional, Murcia, L., additional, Segovia, M., additional, and Berriatua, E., additional
- Published
- 2015
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30. Social Policy or Reparative Justice? Challenges for Reparations in Contexts of Massive Displacement and Related Serious Human Rights Violations
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Perez Murcia, L. E., primary
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- 2013
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31. Comparative value of microscopy, serology and real time pcr in the diagnosis of asymptomatic canine Leishmania infantum infection
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Risueño, J., primary, Bermejo, E., additional, Muñoz García, C. I., additional, Chitimia, I., additional, Del Río, L., additional, García Martínez, J. D., additional, Goyena, E., additional, Fisa, R., additional, Riera, C., additional, Jiménez Montalbán, P., additional, Martínez Ramírez, A., additional, Meseguer Meseguer, J. M., additional, Murcia, L., additional, Segovia, M., additional, and Berriatua, E., additional
- Published
- 2012
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32. Usefulness of PCR for monitoring benznidazole response in patients with chronic Chagas' disease: a prospective study in a non-disease-endemic country
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Murcia, L., primary, Carrilero, B., additional, Munoz, M. J., additional, Iborra, M. A., additional, and Segovia, M., additional
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- 2010
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33. Comportamiento de factores ambientales y socioculturales en pacientes con labio y/o paladar hendido que asistieron a la XI Jornada de Healing The Children 2002-HUN (CH-HUN)
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Ostos-Alfonso, H., Murcia, L., Aparicio, S., Parra, E., Ostos-Alfonso, H., Murcia, L., Aparicio, S., and Parra, E.
- Abstract
Determinar la relación de factores ambientales y socioculturales con la presencia de labio y paladar hendido en pacientes asistentes a HC-HUN.
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- 2001
34. Crustal contamination in northern Andean volcanics
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James, D. and Murcia, L. Armando
- Abstract
Late Cenozoic andesitic rocks of the Colombian Andes are characterized by small but systematic and well-correlated variations in 87Sr/86Sr, 143Nd/144Nd, and δ18O that reflect significant crustal contamination. The range in isotopic ratios measured in northern Andean andesites is most pronounced for oxygen, relatively much more subtle for Sr and Nd. Pb isotopic data, so diagnostic of crustal contamination in central Andean lavas, exhibit minimal variation in the northern Andean volcanics. Trace element trends and phenocryst populations suggest dominantly mafic mineral fractionation, although plagioclase fractionation may be significant in later-stage differentiation. An assimilation-fractional crystallization model is constructed to match measured isotopic data. The results of that modelling indicate that the andesitic magmas of Galeras and Ruiz volcanoes may have assimilated up to 10-20% of crustal material. Correlated variations in measured isotopic ratios can be modelled satisfactorily by assuming a crustal contaminant of composition δ18O=10 per mil, 87Sr/86Sr=0.710-0.712 (Sr≈90 ppm), and 143Nd/144Nd=0.5120-0.5122 (Nd≈20-30 ppm). We estimate that the composition of the primary magma (prior to crustal contamination) was in the range δ18O=6.5 per mil, 87Sr/86Sr=0.704, and 143Nd/144Nd=0.51285, values that may suggest an additional crustal component was present in the primary magma. If we assume the added crustal component was derived from partial melting of subducted continental sedimentary material and/or oceanic crust (source contamination), then model calculations suggest that crustal material comprises less than 10 to 15 wt% of the primary magma. This model-dependent effect of source contamination is to shift isotopic ratios to the right on the Sr-Nd plot (see also Hawkesworth et al. 1977), whereas crustal contamination of the magma during ascent through the Andean crust appears to have produced isotopic trajectories that cut downward and through the mantle array.
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- 1984
35. Mitigating lipopolysaccharide-induced impairment in human dental pulp stem cells with tideglusib-doped nanoparticles: Enhancing osteogenic differentiation and mineralization.
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Osorio R, Rodríguez-Lozano FJ, Toledano M, Toledano-Osorio M, García-Bernal D, Murcia L, and López-García S
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- Humans, Cells, Cultured, Real-Time Polymerase Chain Reaction, Cell Movement drug effects, Calcification, Physiologic drug effects, In Vitro Techniques, Dental Pulp cytology, Dental Pulp drug effects, Lipopolysaccharides pharmacology, Cell Differentiation drug effects, Osteogenesis drug effects, Stem Cells drug effects, Cell Survival drug effects, Nanoparticles, Cell Proliferation drug effects
- Abstract
Objective: Drug-loaded non-resorbable polymeric nanoparticles (NPs) are proposed as an adjunctive treatment for pulp regenerative strategies. The present in vitro investigation aimed to evaluate the effectiveness of tideglusib-doped nanoparticles (TDg-NPs) in mitigating the adverse effects of bacterial lipopolysaccharide endotoxin (LPS) on the viability, morphology, migration, differentiation and mineralization potential of human dental pulp stem cells (hDPSCs)., Methods: Cell viability, proliferation, and differentiation were assessed using a MTT assay, cell migration evaluation, cell cytoskeleton staining analysis, Alizarin Red S staining and expression of the odontogenic related genes by a real-time quantitative polymerase chain reaction (RT-qPCR) were also performed. Cells were tested both with and without stimulation with LPS at various time points. One-way ANOVA and Tukey's test were employed for statistical analysis (p < 0.05)., Results: Adequate cell viability was encountered in all groups and at every tested time point (24, 48, 72 and 168 h), without differences among the groups (p > 0.05). The analysis of cell cytoskeleton showed nuclear alteration in cultures with undoped NPs after LPS stimulation. These cells exhibited an in blue diffuse and multifocal appearance. Some nuclei looked fragmented and condensed. hDPSCs after LPS stimulation but in the presence of TDg-NPs exhibited less nuclei changes. LPS induced down-regulation of Alkaline phosphatase, Osteonectin and Collagen1 gene markers, after 21d. LPS half-reduced the cells production of calcium deposits in all groups (p < 0.05), except in the group with TDg-NPs (decrease about 10 %)., Significance: LPS induced lower mineral deposition and cytoskeletal disorganization in hDPSCs. These effects were counteracted by TDg-NPs, enhancing osteogenic differentiation and mineralization., Competing Interests: Declaration of Competing Interest The authors declare that they have no conflict of interest., (Copyright © 2024. Published by Elsevier Inc.)
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- 2024
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36. Biological Effects of New Chemical-Mechanical Caries Removal Products on Human Dental Pulp Stem Cells.
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López-García S, Pérez-Guzmán N, Rodríguez-Lozano FJ, Pecci-Lloret MP, García-Bernal D, Murcia L, Oñate-Sánchez RE, and Llena C
- Abstract
Introduction: The aim of this study was to compare the biological effects of four chemical caries removal materials and to assess their cytotoxicity using human dental pulp stem cells (hDPSCs)., Methods: The products evaluated are: 1 - papain-based product (BRIX 3000®); 2 - papain/chloramine based products (NATURAL-CARE and Papacárie Duo®); and 3 - chloramine based product (Cariesolut). The following in vitro experiments were carried out: IC50 measurement, cell metabolic activity (MTT) assay, cell migration, immunofluorescence experiment, cell apoptosis analysis, and reactive oxygen species (ROS) production analysis. Statistical analyses were performed using one-way ANOVA followed by Tukey's post hoc test (p < 0.05)., Results: The IC50 values were: Brix 3000: 0.596%; Papacárie Duo: 0.052%; NATURAL CARE: 1.034%; and Cariesolut: 0.020%. The MTT assays showed non-adequate cell viability of all chemical-mechanical caries removal tested at 2% at 24, 48, and 72 h (p < 0.001). The same behaviour was observed at 0.1% in the Papacárie Duo and Cariesolut groups. In contrast, 0.1% of Brix 3000 at all times and NATURAL CARE at 24 h treated cells showed cell viability rates similar to the control group. At 0.01% only Brix 3000 did not show statistically significant differences at any time. Delayed cell migration was observed in all hDPSCs treated with Papacárie Duo and Cariesolut (p < 0.01 and p < 0.001). Phalloidin staining images showed a high confluence of cells in the presence of NATURAL CARE, similar to the control group. On the contrary, no cells were observed in Brix 3000 and Cariesolut at 2% and 0.1% concentrations. Papacárie Duo showed cells at all concentrations, but hDPSCs treated at 0.01% concentration exhibited better proliferation and spreading than those in the control group. Apoptosis essay showed that Brix 3000 at both 0.1% and 0.01% had a percentage of live cells higher than 99%, with 68.4% live cells at 2%, 3.69% early apoptotic cells, and 27.9% late apoptotic cells. Conversely, the rest of the materials showed an abundance of apoptotic cells, even at low concentrations. 0.1% and 0.01% of BRIX 3000 did not affect the ROS production levels, while 2% of BRIX 3000 counterpart very significantly increased the percentage of CM-H2DCFDA positive cells. Again, all concentrations of Cariesolut showed significantly higher levels of ROS production than those observed in control cells., Conclusion: Our results suggest that Brix 3000 would be the most suitable material for chemical caries removal, with Papacárie Duo and NATURAL CARE also being good options, and discourage the use of Cariesolut due to its low cytocompatibility on dental pulp stem cells., (© 2024 S. Karger AG, Basel.)
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- 2024
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37. The polygenic implication of clopidogrel responsiveness: Insights from platelet reactivity analysis and next-generation sequencing.
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Echeverría O, Angulo-Aguado M, Vela R, Calderón-Ospina C, Parra K, Contreras N, Morel A, Cabrera R, Restrepo C, Ramírez-Santana C, Ortega-Recalde O, Rojas-Quintana ME, Murcia L, Gaviria-Sabogal CC, Valero N, and Fonseca-Mendoza DJ
- Subjects
- Humans, Male, Female, Middle Aged, Aged, Multifactorial Inheritance genetics, Ticlopidine analogs & derivatives, Ticlopidine therapeutic use, Ticlopidine pharmacology, Clopidogrel therapeutic use, Clopidogrel pharmacology, Polymorphism, Single Nucleotide, High-Throughput Nucleotide Sequencing methods, Platelet Aggregation Inhibitors therapeutic use, Platelet Aggregation Inhibitors pharmacology, Blood Platelets drug effects, Blood Platelets metabolism
- Abstract
Clopidogrel is widely used worldwide as an antiplatelet therapy in patients with acute coronary disease. Genetic factors influence interindividual variability in response. Some studies have explored the polygenic contributions in the drug response, generating pharmacogenomic risk scores (PgxPRS). Importantly, these factors are less explored in underrepresented populations, such as Latin-American countries. Identifying patients at risk of high-on-treatment platelet reactivity (HTPR) is highly valuable in translational medicine. In this study we used a custom next-generation sequencing (NGS) panel composed of 91 single nucleotide polymorphisms (SNPs) and 28 genes related to clopidogrel metabolism, to analyze 70 patients with platelet reactivity values, assessed through closure time (CT). Our results demonstrated the association of SNPs with HTPR and non-HTPR, revealing the strongest associations with rs2286823 (OR: 5,0; 95% CI: 1,02-24,48; p: 0,03), rs2032582 (OR: 4,41; 95% CI: 1,20-16,12; p: 0,019), and rs1045642 (OR: 3,38; 95% CI: 0,96-11,9; p: 0,05). Bivariate regression analysis demonstrated the significant association of several SNPs with the CT value, a "surrogate" biomarker of clopidogrel response. Exploratory results from the LASSO regression model showed a high discriminatory capacity between HTPR and non-HTPR patients (AUC: 0,955), and the generated PgxPRS demonstrated a significant negative association between the risk score, CT value, and the condition of HTPR and non-HTPR. To our knowledge, our study addresses for the first time the analysis of the polygenic contribution in platelet reactivity using NGS and establishes PgxPRS derived from the LASSO model. Our results demonstrate the polygenic implication of clopidogrel response and offer insights applicable to the translational medicine of antiplatelet therapy in an understudied population., Competing Interests: The authors have declared that no competing interests exist., (Copyright: © 2024 Echeverría et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.)
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- 2024
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38. Premixed calcium silicate-based ceramic sealers promote osteogenic/cementogenic differentiation of human periodontal ligament stem cells: A microscopy study.
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López-García S, Sánchez-Bautista S, García-Bernal D, Lozano A, Forner L, Sanz JL, Murcia L, Rodríguez-Lozano FJ, and Oñate-Sánchez RE
- Subjects
- Humans, Cells, Cultured, Cell Adhesion drug effects, Cell Movement drug effects, Cell Survival drug effects, Cementogenesis drug effects, Microscopy, Electron, Scanning, Periodontal Ligament cytology, Periodontal Ligament drug effects, Calcium Compounds pharmacology, Calcium Compounds chemistry, Silicates pharmacology, Silicates chemistry, Cell Differentiation drug effects, Ceramics chemistry, Stem Cells drug effects, Stem Cells cytology, Osteogenesis drug effects
- Abstract
To evaluate the effects of premixed calcium silicate based ceramic sealers on the viability and osteogenic/cementogenic differentiation of human periodontal ligament stem cells (hPDLSCs). The materials evaluated were TotalFill BC Sealer (TFbc), AH Plus Bioceramic Sealer (AHPbc), and Neosealer Flo (Neo). Standardized discs and 1:1, 1:2, and 1:4 eluates of the tested materials were prepared. The following in vitro experiments were carried out: ion release, cell metabolic activity 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) assay, cell migration, immunofluorescence experiment, cell attachment, gene expression, and mineralization assay. Statistical analyses were performed using one-way ANOVA followed by Tukey's post hoc test (p < .05). Increased Ca
2+ release was detected in TFbc compared to AHPbc and Neo (*p < .05). Biological assays showed a discrete cell metabolic activity and cell migration in Neo-treated cell, whereas scanning electronic microscopy assay exhibited that TFbc group had a better cell adhesion process of substrate attachment, spreading, and cytoskeleton development on the niche-like structures of the cement than AHPbc and Neo. The sealers tested were able to induce overexpression of the CEMP-1, ALP, and COL1A1 genes in the first days of exposure, particularly in the case of TFbc (***p < .001). All materials tested significantly increased the mineralization of hPDLSCs when compared to the negative control, although more pronounced calcium deposition was observed in the TFbc-treated cells (***p < .001). Our results suggested that TFbc promotes cell differentiation, both by increasing the expression of key osteo/odontogenic genes and by promoting mineralization of the extracellular matrix, whereas this phenomenon was less evident in Neo and AHPbc. RESEARCH HIGHLIGHTS: TFbc group had a better cell adhesion process of substrate attachment, spreading, and cytoskeleton development on the niche-like structures of the cement than AHPbc and Neo. The sealers tested were able to induce overexpression of the CEMP-1, ALP, and COL1A1 genes in the first days of exposure, particularly in the case of TFbc. All materials tested significantly increased the mineralization of hPDLSCs when compared to the negative control, although more pronounced calcium deposition was observed in the TFbc-treated cells., (© 2024 The Authors. Microscopy Research and Technique published by Wiley Periodicals LLC.)- Published
- 2024
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39. Assessment of the anti-inflammatory and biological properties of Bioroot Flow: A novel bioceramic sealer.
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López-García S, Sanz JL, Murcia L, García-Bernal D, Lozano A, Forner L, Rodríguez-Lozano FJ, and Oñate-Sánchez RE
- Subjects
- Humans, Root Canal Filling Materials pharmacology, Periodontal Ligament cytology, Periodontal Ligament drug effects, Periodontal Ligament metabolism, Stem Cells drug effects, Stem Cells metabolism, Cell Proliferation drug effects, Ceramics pharmacology, Biocompatible Materials pharmacology, Biocompatible Materials chemistry, Cell Movement drug effects, Cell Adhesion drug effects, Cell Differentiation drug effects, Anti-Inflammatory Agents pharmacology
- Abstract
Introduction: BioRoot Flow (BRF) is a novel premixed bioceramic sealer indicated for endodontic treatments, but the biological and immunomodulatory effects of this endodontic sealer on human periodontal ligament stem cells (hPDLSCs) have not been elucidated., Methods: To ascertain the biological impact of BRF, TotalFill BC Sealer (TFbc), and AH Plus (AHP) on human Periodontal Ligament Stem Cells (hPDLSCs), assessments were conducted to evaluate the cytocompatibility, cellular proliferation, migratory capacity, osteo/cementogenic differentiation potential, the ability to form mineralized nodules, and the immunomodulatory characteristics of hPDLSCs following treatment with these endodontic sealers., Results: Biological assays showed adequate cell metabolic activity and cell migration in BRF, while SEM assay evidenced that TFbc and BRF groups demonstrated a superior cell adhesion process, including substrate adhesion, cytoskeleton development, and spreading on the niche-like structures of the cement as compared to the AHP group. TFbc and BRF-treated groups exhibited a significantly lower IL6 and IL8 production than AHP (* p <.05). The bioceramic sealers stimulated heightened expression of BSP, CEMP-1, and CAP genes within a 7-14 day period. Notably, BRF and TFbc demonstrated a significant enhancement in the mineralization of hPDLSCs when compared to the negative control. Among these, cells treated with BRF showed a more substantial accumulation of calcium (*** p < .001)., Conclusions: Taken together, these findings indicate that BRF can potentially enhance cell differentiation by promoting the expression of essential genes related to bone and cement formation. In addition, BRF and TFbc displayed anti-inflammatory effects., Competing Interests: Declaration of Competing Interest The authors declare that they have no competing interests., (Copyright © 2024 The Authors. Published by Elsevier Ltd.. All rights reserved.)
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- 2024
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40. Comparative Cytotoxicity of Menthol and Eucalyptol: An In Vitro Study on Human Gingival Fibroblasts.
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Puig-Herreros C, Sanz JL, García-Bernal D, Rodríguez-Lozano FJ, Murcia L, Forner L, Ghilotti J, Oñate-Sánchez RE, and López-García S
- Abstract
The aim of this study was to assess the influence of eucalyptol and menthol on the cell viability, migration, and reactive oxygen species production of human gingival fibroblasts (GFs) in vitro. Three different concentrations of eucalyptol and menthol were prepared following ISO 10993-5 guidelines (1, 5, and 10 mM). GFs were isolated from extracted teeth from healthy donors. The following parameters were assessed: cell viability via MTT, Annexin-V-FITC and 7-AAD staining, and IC
50 assays; cell migration via horizontal scratch wound assay; and cell oxidative stress via reactive oxygen species assay. Data were analyzed using one-way ANOVA and Tukey's post hoc test. Statistical significance was established at p < 0.05. Eucalyptol and Menthol exhibited high cytotoxicity on gingival fibroblasts, as evidenced by cytotoxicity assays. Eucalyptol showed lower levels of cytotoxicity than menthol, compared to the control group. The cytotoxicity of the tested substances increased in a concentration-dependent manner. The same occurred in a time-dependent manner, although even 10 min of exposure to the tested substances showed a high cytotoxicity to the GFs. Commercially available products for oral application with these substances in their composition should be tested for cytotoxicity before their use.- Published
- 2024
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41. Comparative bioactivity and immunomodulatory potential of the new Bioroot Flow and AH Plus Bioceramic sealer: An in vitro study on hPDLSCs.
- Author
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Sanz JL, López-García S, García-Bernal D, Rodríguez-Lozano FJ, Forner L, Lozano A, and Murcia L
- Subjects
- Humans, Cytokines, Periodontal Ligament, Epoxy Resins, Alopecia congenital, Root Canal Filling Materials, Calcium Compounds, Silicates
- Abstract
Objectives: To evaluate the cytocompatibility, bioactivity, and anti-inflammatory potential of the new pre-mixed calcium silicate cement-based sealers Bioroot Flow (BrF) and AH Plus Bioceramic Sealer (AHPbcs) on human periodontal ligament stem cells (hPDLSCs) compared to the epoxy resin-based sealer AH Plus (AHP)., Materials and Methods: Standardized discs and 1:1, 1:2, and 1:4 eluates of BrF, AHPbcs and AHP after setting were prepared. The following assays were performed: cell attachment and morphology via SEM, cell viability via a MTT assay, cell migration/proliferation via a wound-healing assay, cytoskeleton organization via immunofluorescence staining; cytokine release via ELISA; osteo/cemento/odontogenic marker expression via RT-qPCR, and cell mineralized nodule formation via Alizarin Red S staining. HPDLSCs were isolated from extracted third molars from healthy patients. Comparisons were made with hPDLSCs cultured in unconditioned (negative control) or osteogenic (positive control) culture media. Statistical significance was established at p < 0.05., Results: Both BrF and AHPbcs showed significantly positive results in the cytocompatibility assays (cell metabolic activity, migration, attachment, morphology, and cytoskeleton organization) compared with a negative control group, while AHP showed significant negative results. BrF exhibited an upregulation of at least one osteo/cementogenic marker compared to the negative and positive control groups. BrF showed a significantly higher calcified nodule formation than AHPbcs, the negative and positive control groups, while AHPbcs was higher than the negative control group. Both were also significantly higher than AHP group., Conclusion: BrF and AHPbcs exhibit adequate and comparable cytocompatibility on hPDLSCs. BrF also promoted the osteo/cementogenic differentiation of hPDLSCs. Both calcium silicate-based sealers favored the downregulation of the inflammatory cytokine IL-6 and the calcified nodule formation from hPDLSCs. BrF exerted a significantly higher influence on cell mineralization than AHPbcs., Clinical Relevance: This is the first study to elucidate the biological properties and immunomodulatory potential of Bioroot Flow and AH Plus Bioceramic Sealer. The results act as supporting evidence for their use in root canal treatment., (© 2024. The Author(s).)
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- 2024
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42. Direct oral challenge for immediate and non-immediate beta-lactam allergy in children: A real-world multicenter study.
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Moral L, Toral T, Muñoz C, Marco N, García-Avilés B, Murcia L, Forniés MJ, González MC, Canals F, Bragado E, Martínez Olmos J, García-Magán C, Moure González JD, Cortés N, Giménez M, Gómez C, Rodríguez AB, Moreno A, Lucas JM, Quevedo S, Blasco C, and Aliaga Y
- Subjects
- Child, Humans, beta-Lactams, Anti-Bacterial Agents adverse effects, Skin Tests methods, Monobactams, Anaphylaxis chemically induced, Drug Hypersensitivity diagnosis, Drug Hypersensitivity epidemiology
- Abstract
Background: Allergy to beta-lactam antibiotics (BLA) is frequently suspected in children, but a drug provocation test (DPT) rules it out in over 90% of cases. Direct oral DPT (DODPT), without skin or other previous tests, is increasingly been used to delabel non-immediate BLA reactions. This real-world study aimed to assess the safety and effectiveness of DODPT in children with immediate and non-immediate reactions to BLAs., Methods: Ambispective registry study in children (<15 years), attended between 2016 and 2023 for suspected BLA allergy in 15 hospitals in Spain that routinely perform DODPT., Results: The study included 2133 patients with generally mild reactions (anaphylaxis 0.7%). Drug provocation test with the implicated BLA was performed in 2014 patients (94.4%): 1854 underwent DODPT (86.9%, including 172 patients with immediate reactions). One hundred forty-five (7.2%) had symptoms associated with DPT, although only four reactions were severe: two episodes of anaphylaxis and two of drug-induced enterocolitis syndrome, which resolved rapidly with treatment. Of the 141 patients with mild reactions in the first DPT, a second DPT was considered in 87 and performed in 57, with 52 tolerating it without symptoms. Finally, BLA allergy was ruled out in 90.9% of the sample, confirmed in 3.4%, and remained unverified, usually due to loss to follow-up, in 5.8%., Conclusions: Direct oral DPT is a safe, effective procedure even in immediate mild reactions to BLA. Many reactions observed in DPT are doubtful and require confirmation. Severe reactions are exceptional and amenable to treatment. Direct oral DPT can be considered for BLA allergy delabeling in pediatric primary care., (© 2024 European Academy of Allergy and Clinical Immunology and John Wiley & Sons Ltd.)
- Published
- 2024
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43. In vitro biocompatibility of ammonia-free silver fluoride products on human dental pulp stem cells.
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López-García S, Sanz JL, Oñate-Sánchez RE, Forner L, García-Bernal D, Murcia L, Rodríguez-Lozano FJ, and Llena C
- Subjects
- Humans, Adolescent, Young Adult, Adult, Dental Pulp, Reactive Oxygen Species, Dentin, Potassium Iodide therapeutic use, Stem Cells, Dental Caries drug therapy, Fluorides, Silver Compounds
- Abstract
Objectives: Silver fluoride (SF) is a preventive and therapeutic option for dental pathological processes involving structural alterations of the hard tissues, either during their formation or those caused by caries or other pathological reasons. This study aimed to compare the biological properties of two commercial SF products, one of them with ammonium (Riva Star; SDF) and the other ammonium-free (Riva Star Aqua; AgF), both with or without potassium iodide (KI), by the assessment of the cytotoxicity of the materials' eluates., Methods: Human dental pulp stem cells (hDPSCs) were obtained from healthy 18-23-year-old donors. Three dilutions were prepared for the tested materials (0.005%, 0.0005%, and 0.0001%). The following groups were assessed: (AgF, AgF+KI, SDF, SDF+KI, KI, negative control). A series of cytocompatibility assays were performed: MTT assay, IC50 assay, wound healing (migration) assay, cell cytoskeleton staining, analysis of cell apoptosis and necrosis, and reactive oxygen species production. The normality in the distribution of the data was previously confirmed via a Q-Q plot. Statistical significance was tested using one way ANOVA and Tukey's post hoc test., Results: The incorporation of KI improved the cytocompatibility of both SF products in terms of viability, migration, morphology, apoptosis, and reactive oxygen species production. This difference was higher in the AgF group. The lowest dilutions of SF+KI and AgF+KI showed a similar cytocompatibility to that of the control group (MTT assay (p > 0.05 after 24, 48, and 72 h of culture); migration assay (p > 0.05 after 24, 48, and 72 h of culture); reactive oxygen species production (p > 0.05 after 72 h of culture)., Significance: Riva Star Aqua shows lower cytotoxicity than Riva Star on hDPSCs. It can be considered as a good alternative in the conservative treatment of dental caries and in the preservation and remineralisation of viable dentine tissue., Competing Interests: Declaration of Competing Interest The authors declare that they have no conflict of interest., (Copyright © 2023 The Authors. Published by Elsevier Ltd.. All rights reserved.)
- Published
- 2024
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44. Oral Manifestations of Mucormycosis: A Systematic Review.
- Author
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Mora-Martínez A, Murcia L, and Rodríguez-Lozano FJ
- Abstract
Mucormycosis is a rare, opportunistic, and emerging fungal infection that can rapidly develop into a severe, highly fatal clinical picture. In most cases, it is caused by fungi of the order Mucorales, which are usually avirulent but become pathogenic when the host's immune system is compromised. This systematic review was conducted according to PRISMA guidelines. The databases searched included PubMed, Scopus, and Web of Science. We chose articles that analyzed the oral manifestations of patients with mucormycosis, were published between 2018 and 2023, and met our search terms. The risk of bias in the articles was assessed using the CARE guideline for case reports and STROBE for a cross-sectional study. After the selection process, 20 articles were included in this review, all containing information about the different oral manifestations presented by people with mucormycosis. The most common oral manifestations are mainly bone exposures and oral ulcers, halitosis, pus discharge, gingival thickening, and periodontitis. However, despite the importance of recognizing these oral manifestations in the early stages of mucormycotic infection, providing early treatment, and reducing the high mortality rate of the infection, more studies are needed.
- Published
- 2023
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45. Biological properties of Ceraputty as a retrograde filling material: an in vitro study on hPDLSCs.
- Author
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López-García S, Rodríguez-Lozano FJ, Sanz JL, Forner L, Pecci-Lloret MP, Lozano A, Murcia L, Sánchez-Bautista S, and Oñate-Sánchez RE
- Subjects
- Humans, Materials Testing, Periodontal Ligament, Calcium Compounds pharmacology, Silicates pharmacology, Stem Cells, Cells, Cultured, Root Canal Filling Materials pharmacology
- Abstract
Objectives: To assess the cytocompatibility and bioactive potential of the new calcium silicate-based cement Ceraputty on human periodontal ligament stem cells (hPDLSCs) compared to Biodentine and Endosequence BC root repair material (ERRM)., Materials and Methods: hPDLSCs were isolated from extracted third molars from healthy donors. Standardized sample discs and 1:1, 1:2, and 1:4 eluates of the tested materials were prepared. The following assays were performed: surface element distribution via SEM-EDX, cell attachment and morphology via SEM, cell viability via a MTT assay, osteo/cemento/odontogenic marker expression via RT-qPCR, and cell calcified nodule formation via Alizarin Red S staining. hPDLSCs cultured in unconditioned or osteogenic media were used as negative and positive control groups, respectively. Statistical analysis was performed using one-way ANOVA or two-way ANOVA and Tukey's post hoc test. Statistical significance was established at p < 0.05., Results: The highest Ca
2+ peak was detected from Biodentine samples, followed by ERRM and Ceraputty. hPDLSC viability was significantly reduced in Ceraputty samples (p < 0.001), while 1:2 and 1:4 Biodentine and ERRM samples similar results to that of the negative control (p > 0.05). Biodentine and ERRM exhibited an upregulation of at least one cemento/odonto/osteogenic marker compared to the negative and positive control groups. Cells cultured with Biodentine produced a significantly higher calcified nodule formation than ERRM and Ceraputty (p < 0.001), which were also higher than the control groups (p < 0.001)., Conclusion: Ceraputty evidenced a reduced cytocompatibility towards hPDLSCs on its lowest dilutions compared to the other tested cements and the control group. Biodentine and ERRM promoted a significantly higher mineralization and osteo/cementogenic marker expression on hPDLSCs compared with Ceraputty. Further studies are necessary to verify the biological properties of this new material and its adequacy as a retrograde filling material., Clinical Relevance: This is the first study to elucidate the adequate biological properties of Ceraputty for its use as a retrograde filling material., (© 2023. The Author(s).)- Published
- 2023
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46. Role of the Non-Canonical RNAi Pathway in the Antifungal Resistance and Virulence of Mucorales.
- Author
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Cánovas-Márquez JT, Navarro-Mendoza MI, Pérez-Arques C, Lax C, Tahiri G, Pérez-Ruiz JA, Lorenzo-Gutiérrez D, Calo S, López-García S, Navarro E, Nicolás FE, Garre V, and Murcia L
- Subjects
- Antifungal Agents pharmacology, Mucorales drug effects, Mucorales genetics, RNA Stability, RNA, Fungal genetics, RNA, Messenger chemistry, Signal Transduction, Drug Resistance, Fungal, Mucorales pathogenicity, RNA Interference
- Abstract
Mucorales are the causal agents for the lethal disease known as mucormycosis. Mortality rates of mucormycosis can reach up to 90%, due to the mucoralean antifungal drug resistance and the lack of effective therapies. A concerning urgency among the medical and scientific community claims to find targets for the development of new treatments. Here, we reviewed different studies describing the role and machinery of a novel non-canonical RNAi pathway (NCRIP) only conserved in Mucorales. Its non-canonical features are the independence of Dicer and Argonaute proteins. Conversely, NCRIP relies on RNA-dependent RNA Polymerases (RdRP) and an atypical ribonuclease III (RNase III). NCRIP regulates the expression of mRNAs by degrading them in a specific manner. Its mechanism binds dsRNA but only cuts ssRNA. NCRIP exhibits a diversity of functional roles. It represses the epimutational pathway and the lack of NCRIP increases the generation of drug resistant strains. NCRIP also regulates the control of retrotransposons expression, playing an essential role in genome stability. Finally, NCRIP regulates the response during phagocytosis, affecting the multifactorial process of virulence. These critical NCRIP roles in virulence and antifungal drug resistance, along with its exclusive presence in Mucorales, mark this pathway as a promising target to fight against mucormycosis.
- Published
- 2021
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47. The RNAi Mechanism Regulates a New Exonuclease Gene Involved in the Virulence of Mucorales.
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Pérez-Arques C, Navarro-Mendoza MI, Murcia L, Navarro E, Garre V, and Nicolás FE
- Subjects
- Gene Expression Regulation, Fungal, Genes, Fungal, Mutation genetics, RNA, Fungal genetics, RNA, Fungal metabolism, Transcriptome genetics, Virulence genetics, Exonucleases genetics, Mucorales genetics, Mucorales pathogenicity, RNA Interference
- Abstract
Mucormycosis is a lethal disease caused by Mucorales, which are emerging as human causes that explain the high mortality for this disease. Consequently, the research community is searching for virulence determinants that could be repurposed as targets to develop new treatments against mucormycosis. Our work explores an RNA interference (RNAi)-based approach to find targets involved in the virulence of Mucorales. A transcriptomewide analysis compared sRNAs and their target mRNAs in two Mucor lusitanicus different pathotypes, virulent and avirulent, generating a list of 75 loci selected by their differential sRNA accumulation in these strains. As a proof of concept and validity, an experimental approach characterized two loci showing opposite behavior, confirming that RNAi activity causes their differential expression in the two pathotypes. We generated deletion mutants for two loci and a knockin-strain overexpressing for one of these loci. Their functional analysis in murine virulence assays identified the gene wex1, a putative DEDDy exonuclease with RNase domains, as an essential factor for virulence. The identification of wex1 showed the potential of our approach to discover virulence factors not only in Mucorales but also in any other fungal model with an active RNAi machinery. More importantly, it adds a new layer to the biological processes controlled by RNAi in M. lusitanicus , confirming that the Dicer-dependent RNAi pathway can silence gene expression to promote virulence.
- Published
- 2021
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48. A Mucoralean White Collar-1 Photoreceptor Controls Virulence by Regulating an Intricate Gene Network during Host Interactions.
- Author
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Pérez-Arques C, Navarro-Mendoza MI, Murcia L, Lax C, Sanchis M, Capilla J, Navarro E, Garre V, and Nicolás FE
- Abstract
Mucolares are an ancient group of fungi encompassing the causal agents for the lethal infection mucormycosis. The high lethality rates, the emerging character of this disease, and the broad antifungal resistance of its causal agents are mucormycosis features that are alarming clinicians and researchers. Thus, the research field around mucormycosis is currently focused on finding specific weaknesses and targets in Mucorales for developing new treatments. In this work, we tested the role of the white-collar genes family in the virulence potential of Mucor lusitanicus . Study of the three genes of this family, mcwc-1a , mcwc-1b , and mcwc-1c , resulted in a marked functional specialization, as only mcwc-1a was essential to maintain the virulence potential of M. lusitanicus . The traditional role of wc-1 genes regulating light-dependent responses is a thoroughly studied field, whereas their role in virulence remains uncharacterized. In this work, we investigated the mechanism involving mcwc-1a in virulence from an integrated transcriptomic and functional approach during the host-pathogen interaction. Our results revealed mcwc-1a as a master regulator controlling an extensive gene network. Further dissection of this gene network clustering its components by type of regulation and functional criteria disclosed a multifunctional mechanism depending on diverse pathways. In the absence of phagocytic cells, mcwc-1a controlled pathways related to cell motility and the cytoskeleton that could be associated with the essential tropism during tissue invasion. After phagocytosis, several oxidative response pathways dependent on mcwc-1a were activated during the germination of M. lusitanicus spores inside phagocytic cells, which is the first stage of the infection. The third relevant group of genes involved in virulence and regulated by mcwc-1a belonged to the "unknown function," indicating that new and hidden pathways are involved in virulence. The unknown function category is especially pertinent in the study of mucormycosis, as it is highly enriched in specific fungal genes that represent the most promising targets for developing new antifungal compounds. These results unveil a complex multifunctional mechanism used by wc-1 genes to regulate the pathogenic potential in Mucorales that could also apply to other fungal pathogens.
- Published
- 2021
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49. A non-canonical RNAi pathway controls virulence and genome stability in Mucorales.
- Author
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Pérez-Arques C, Navarro-Mendoza MI, Murcia L, Navarro E, Garre V, and Nicolás FE
- Subjects
- Antifungal Agents pharmacology, Drug Resistance, Fungal genetics, Epigenesis, Genetic genetics, Fungal Proteins genetics, Gene Expression Regulation, Fungal genetics, Genomic Instability drug effects, Host-Pathogen Interactions genetics, Mucorales pathogenicity, Mucormycosis microbiology, Mutation genetics, RNA, Messenger genetics, Signal Transduction drug effects, Virulence genetics, Mucorales genetics, Mucormycosis genetics, RNA Interference, Ribonuclease III genetics
- Abstract
Epimutations in fungal pathogens are emerging as novel phenomena that could explain the fast-developing resistance to antifungal drugs and other stresses. These epimutations are generated by RNA interference (RNAi) mechanisms that transiently silence specific genes to overcome stressful stimuli. The early-diverging fungus Mucor circinelloides exercises a fine control over two interacting RNAi pathways to produce epimutants: the canonical RNAi pathway and a new RNAi degradative pathway. The latter is considered a non-canonical RNAi pathway (NCRIP) because it relies on RNA-dependent RNA polymerases (RdRPs) and a novel ribonuclease III-like named R3B2 to degrade target transcripts. Here in this work, we uncovered the role of NCRIP in regulating virulence processes and transposon movements through key components of the pathway, RdRP1 and R3B2. Mutants in these genes are unable to launch a proper virulence response to macrophage phagocytosis, resulting in a decreased virulence potential. The transcriptomic profile of rdrp1Δ and r3b2Δ mutants revealed a pre-exposure adaptation to the stressful phagosomal environment even when the strains are not confronted by macrophages. These results suggest that NCRIP represses key targets during regular growth and releases its control when a stressful environment challenges the fungus. NCRIP interacts with the RNAi canonical core to protect genome stability by controlling the expression of centromeric retrotransposable elements. In the absence of NCRIP, these retrotransposons are robustly repressed by the canonical RNAi machinery; thus, supporting the antagonistic role of NCRIP in containing the epimutational pathway. Both interacting RNAi pathways might be essential to govern host-pathogen interactions through transient adaptations, contributing to the unique traits of the emerging infection mucormycosis., Competing Interests: The authors have declared that no competing interests exist.
- Published
- 2020
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50. Mucorales Species and Macrophages.
- Author
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Nicolás FE, Murcia L, Navarro E, Navarro-Mendoza MI, Pérez-Arques C, and Garre V
- Abstract
Mucormycosis is an emerging fungal infection caused by Mucorales with an unacceptable high mortality rate. Mucorales is a complex fungal group, including eleven different genera that can infect humans. This heterogeneity is associated with species-specific invasion pathways and responses to the host defense mechanisms. The host innate immune system plays a major role in preventing Mucorales growth and host invasion. In this system, macrophages are the main immune effector cells in controlling these fungi by rapid and efficient phagocytosis of the spores. However, Mucorales have evolved mechanisms to block phagosomal maturation and species-specific mechanisms to either survive as dormant spores inside the macrophage, as Rhizopus species, or geminate and escape, as Mucor species. Classical fungal models of mucormycosis, mostly Rhizopus , have made important contributions to elucidate key aspects of the interaction between Mucorales and macrophages, but they lack robust tools for genetic manipulation. The recent introduction of the genetically tractable Mucor circinelloides as a model of mucormycosis offers the possibility to analyze gene function. This has allowed the identification of regulatory pathways that control the fungal response to phagocytosis, including a non-canonical RNAi pathway (NCRIP) that regulates the expression of most genes regulated by phagocytosis.
- Published
- 2020
- Full Text
- View/download PDF
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