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1. Neuroblastoma in Spain: Linking the national clinical database and epidemiological registries – A study by the Joint Action on Rare Cancers

Author

Almazán, F, Benito, AI, Buedo, MI, Calvo, C, Cañete, A, Cruz, O, Esquembre, C, Fernández, M, Fernández-Teijeiro Álvarez, A, Fuster, JL, García, M, Gil López, C, Gómez, J, Gondra, A, González, M, González, H, Herrero, B, Lassaletta, A, López, R, López-Ibor Aliño, B, Madero, L, Maldonado, S, Mares, FJ, Márquez, C, Mateos, ME, Melwani, K, Mendoza, MC, Moreno, L, Moreno, ML, Muñoz, GM, Ortega, MJ, Panizo, E, Pisa Gatell, S, Portugal, R, Sagaseta, M, Salinas, JA, Sastre, A, Tallón, M, Torrent, M, Uriz, JJ, Varo, A, Vázquez, MA, Vílchez, JS, Villegas, JA, Vivanco, JL, Zamora, M, Alamo, R, Alemán, A, Chico, M, Chirlaque, MD, Galceran, J, Marcos, R, Mateos, A, Quirós, JR, Sanchez-Contador, C, Sabater, C, Cañete, Adela, Peris-Bonet, Rafael, Capocaccia, Riccardo, Pardo-Romaguera, Elena, Segura, Vanessa, Muñoz-López, Ana, Fernández-Teijeiro, Ana, Galceran-Padros, Jaume, and Gatta, Gemma

Published
2022
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4. Have there been changes in the application of mechanical ventilation in relation to scientific evidence? A multicenter observational study in Mexico

Author

Aguilera Almazán, F., Benítez Cortázar, M., Carrillo Speare, R., Castaño, R., Corral, R., D’Ector Lira, D.N., Díaz Polanco, G., Elizalde, J.J., Envila Fisher, R., Franco, G., García Balbuena, P., Gayoso Cruz, O., Green, L., Herrera Hoyos, J.O., Hinojosa, J., Huerta, J., Juárez, V.A., Loera, M., López Alzate, C., López Mora, E., Martínez Caro, S., Méndez Reyes, R., Mendoza, M., Narváez Porras, O., Ortiz, E., Padua, A., Poblano, M., Pureco Reyes, V., Querevalum, W., Quesada, A., Ramírez Rivera, A., Tamariz, A., Vargas, A., Vázquez, C., Cerda, P., Mercado, R., Albe Castañón, J., Villagómez Ortiz, A.J., Cruz Lozano, C., Maycotte Luna, Z., López Bacal, F., Cueto Robledo, G., Treviño Salinas, M.A., Martínez Zubieta, R., Olvera-Guzmán, C., Montes de Oca, Marco, Ñamendys-Silva, S.A., Martínez Cano, J.S., Baltazar Torres, J.A., Morales Muñoz, G., Villa Delgado, A., Ladape Martínez, J., Ortega Pérez, A., Chávez Morales, A., García Luna, A., Rugiero Cabrera, A., Rugerio Cabrera, A., Pérez-Calatayud, Á.A., Arellano, A., Velasco Gutiérrez, A., Longino Gómez, A.J., Tamariz Becerra Álvarez Calderón, Antonio, Álvarez Calderón Christus Mugerza, R., Reynoso Estrella, C.I., Déctor-Lira Espindola-Cruz, D., Gutiérrez-Zárate, D., Esmeralda, D., Anica Malagón, E.D., Monares Zepeda, E., Deloya, E., Manzo Palacios, E., de Jesús Montelongo, F., Flores Mejía, F.J., Ramírez Cervantes, M., Camarena Alejo, G., Vázquez de Anda, G., Vázquez, H., Larios Luna, C., Zamora, S.E., Magaña Solano, G., Sánchez González, J.I., Rosendo Sánchez Medina, J., Zaragoza, J.J., Buensuseso Alfaro, J.A., Dávila Fernández, J.C., Mijangos-Méndez, J.C., Martínez Medina, M., Chacón Gómez, M., Calyeca Sánchez, M.V., Martínez Soria, J.J., García Graullera, R.J., Rosas, R., Sanjuana Gómez Flores, S., Reyes Inurrigarro, S., Ñamendy-Silva, S.A., Sánchez Hurtado, L.A., Villegas Castellanos, L.L., Zalatiel Maycotte, L., Estrada Gutiérrez, A., León, M.A., Marín, M.C., Elizalde, J., Villagómez, A., Cerón, U., Palma-Lara, I., Sánchez, J.R., Monares, E., Muriel, A., Peñuelas, Ó., Frutos-Vivar, F., and Esteban, A.

Published
2020
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5. ¿Se han producido cambios en la aplicación de la ventilación mecánica en relación con la evidencia científica? Estudio multicéntrico en México

Author

Aguilera Almazán, F., Benítez Cortázar, M., Carrillo Speare, R., Castaño, R., Corral, R., D́Ector Lira, D.N., Díaz Polanco, G., Elizalde, J.J., Envila Fisher, R., Franco, G., García Balbuena, P., Gayoso Cruz, O., Green, L., Herrera Hoyos, J.O., Hinojosa, J., Huerta, J., Juárez, V.A., Loera, M., López Alzate, C., López Mora, E., Martínez Caro, S., Méndez Reyes, R., Mendoza, M., Narváez Porras, O., Ortiz, E., Padua, A., Poblano, M., Pureco Reyes, V., Querevalum, W., Quesada, A., Ramírez Rivera, A., Tamariz, A., Vargas, A., Vázquez, C., Cerda, P., Mercado, R., Albe Castañón, J., Villagómez Ortiz, A.J., Cruz Lozano, C., Maycotte Luna, Z., López Bacal, F., Cueto Robledo, G., Treviño Salinas, M.A., Martínez Zubieta, R., Olvera-Guzmán, C., Montes de Oca, Marco, Ñamendys-Silva, S.A., Martínez Cano, J.S., Baltazar Torres, J.A., Morales Muñoz, G., Villa Delgado, A., Ladape Martínez, J., Ortega Pérez, A., Chávez Morales, A., García Luna, A., Rugiero Cabrera, A., Rugerio Cabrera, A., Pérez-Calatayud, Á.A., Arellano, A., Velasco Gutiérrez, A., Longino Gómez, A.J., Tamariz Becerra Álvarez Calderón, Antonio, Álvarez Calderón Christus Mugerza, R., Reynoso Estrella, C.I., Déctor-Lira Espindola-Cruz, D., Gutiérrez-Zárate, D., Esmeralda, D., Anica Malagón, E.D., Monares Zepeda, E., Deloya, E., Manzo Palacios, E., de Jesús Montelongo, F., Flores Mejía, F.J., Ramírez Cervantes, M., Camarena Alejo, G., Vázquez de Anda, G., Vázquez, H., Larios Luna, C., Zamora, S.E., Magaña Solano, G., Sánchez González, J.I., Rosendo Sánchez Medina, J., Zaragoza, J.J., Buensuseso Alfaro, J.A., Dávila Fernández, J.C., Mijangos-Méndez, J.C., Martínez Medina, M., Chacón Gómez, M., Calyeca Sánchez, M.V., Martínez Soria, J.J., García Graullera, R.J., Rosas, R., Sanjuana Gómez Flores, S., Reyes Inurrigarro, S., Ñamendy-Silva, S.A., Sánchez Hurtado, L.A., Villegas Castellanos, L.L., Zalatiel Maycotte, L., Estrada Gutiérrez, A., León, M.A., Marín, M.C., Elizalde, J., Villagómez, A., Cerón, U., Palma-Lara, I., Sánchez, J.R., Monares, E., Muriel, A., Peñuelas, Ó., Frutos-Vivar, F., and Esteban, A.

Published
2020
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6. Neuroblastoma in Spain: Linking the national clinical database and epidemiological registries – A study by the Joint Action on Rare Cancers

Author

Cañete, Adela, primary, Peris-Bonet, Rafael, additional, Capocaccia, Riccardo, additional, Pardo-Romaguera, Elena, additional, Segura, Vanessa, additional, Muñoz-López, Ana, additional, Fernández-Teijeiro, Ana, additional, Galceran-Padros, Jaume, additional, Gatta, Gemma, additional, Almazán, F, additional, Benito, AI, additional, Buedo, MI, additional, Calvo, C, additional, Cañete, A, additional, Cruz, O, additional, Esquembre, C, additional, Fernández, M, additional, Fernández-Teijeiro Álvarez, A, additional, Fuster, JL, additional, García, M, additional, Gil López, C, additional, Gómez, J, additional, Gondra, A, additional, González, M, additional, González, H, additional, Herrero, B, additional, Lassaletta, A, additional, López, R, additional, López-Ibor Aliño, B, additional, Madero, L, additional, Maldonado, S, additional, Mares, FJ, additional, Márquez, C, additional, Mateos, ME, additional, Melwani, K, additional, Mendoza, MC, additional, Moreno, L, additional, Moreno, ML, additional, Muñoz, GM, additional, Ortega, MJ, additional, Panizo, E, additional, Pisa Gatell, S, additional, Portugal, R, additional, Sagaseta, M, additional, Salinas, JA, additional, Sastre, A, additional, Tallón, M, additional, Torrent, M, additional, Uriz, JJ, additional, Varo, A, additional, Vázquez, MA, additional, Vílchez, JS, additional, Villegas, JA, additional, Vivanco, JL, additional, Zamora, M, additional, Alamo, R, additional, Alemán, A, additional, Chico, M, additional, Chirlaque, MD, additional, Galceran, J, additional, Marcos, R, additional, Mateos, A, additional, Quirós, JR, additional, Sanchez-Contador, C, additional, and Sabater, C, additional

Published
2022
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7. CRISPR-Cas13d: a tool to fight RNA viruses

Author

Moreno-Sánchez, Ismael, Fernández, A., Polo, E., Almazán, F., Collado, M., Pino, P. del, Rodríguez Aguirre, Dolores, Montoliu, Lluís, and Moreno-Mateos, Miguel A.

Abstract

Trabajo presentado en Current Trends in Biomedicine Workshop, celebrado en Baeza (España) del 02 al 04 de noviembre de 2021., CRISPR-Cas13 is a family of class II type VI CRISPR systems which have been successfully used to induce RNA degradation in mammalian cells, plants and the fission yeast. We have recently optimized the use of CRISPR-RfxCas13d to efficiently induce mRNA knockdown in animal embryos, including zebrafish, medaka, killifish and mouse embryos. Since Cas13d is an efficient and specific RNA nuclease, it has been proposed the use of this system to target RNA viruses such as Influenza virus and the causative agent of Covid-19 pandemic, the novel coronavirus SARS-CoV-2. As a proof of principle, it has been demonstrated by other groups that the transgenic and constant expression of Cas13d with a combination of several gRNAs targeting nucleocapsid or RNA-dependent RNA polymerase genes from SARS-CoV-2 is able to reduce viral RNA in cells transfected with these gRNAs and challenged with SARS-CoV-2 virus. However, to use CRISPR-Cas13d as a potential antiviral therapy, a formulation able to be delivered in vivo and induce transient targeting is needed. Here, we show Cas13d-gRNA ribonucleoprotein (RNP) complex is able to efficiently target different RNAs from viruses belonging to the Nidovirales order including BEV torovirus, 229E coronavirus and SARS-CoV-2 when injected in zebrafish embryos as an in vivo model system. Finally, we have also achieved an efficient delivery approach based on fusogenic cellsomes which allows the entry of Cas13dgRNA RNPs in equine cell cultures infected with BEV torovirus leading to viral to a drastic reduction in viral protein expression and progeny virus production. We believe these preliminary but promising results support the future use of CRISPR-Cas13d RNPs as a potential antiviral therapy. Further analysis will show whether our optimized encapsulated RNP is able to degrade viral RNA in animal models infected with SARS-CoV-2 and other RNA viruses.

Published
2021

9. Have there been changes in the application of mechanical ventilation in relation to scientific evidence? A multicenter observational study in Mexico

Author

Marín, M.C., primary, Elizalde, J., additional, Villagómez, A., additional, Cerón, U., additional, Poblano, M., additional, Palma-Lara, I., additional, Sánchez, J.R., additional, Monares, E., additional, Arellano, A., additional, Muriel, A., additional, Peñuelas, Ó., additional, Frutos-Vivar, F., additional, Esteban, A., additional, Aguilera Almazán, F., additional, Benítez Cortázar, M., additional, Carrillo Speare, R., additional, Castaño, R., additional, Corral, R., additional, D’Ector Lira, D.N., additional, Díaz Polanco, G., additional, Elizalde, J.J., additional, Envila Fisher, R., additional, Franco, G., additional, García Balbuena, P., additional, Gayoso Cruz, O., additional, Green, L., additional, Herrera Hoyos, J.O., additional, Hinojosa, J., additional, Huerta, J., additional, Juárez, V.A., additional, Loera, M., additional, López Alzate, C., additional, López Mora, E., additional, Martínez Caro, S., additional, Méndez Reyes, R., additional, Mendoza, M., additional, Narváez Porras, O., additional, Ortiz, E., additional, Padua, A., additional, Pureco Reyes, V., additional, Querevalum, W., additional, Quesada, A., additional, Ramírez Rivera, A., additional, Tamariz, A., additional, Vargas, A., additional, Vázquez, C., additional, Cerda, P., additional, Mercado, R., additional, Albe Castañón, J., additional, Villagómez Ortiz, A.J., additional, Cruz Lozano, C., additional, Maycotte Luna, Z., additional, López Bacal, F., additional, Cueto Robledo, G., additional, Treviño Salinas, M.A., additional, Martínez Zubieta, R., additional, Olvera-Guzmán, C., additional, Montes de Oca, Marco, additional, Ñamendys-Silva, S.A., additional, Martínez Cano, J.S., additional, Baltazar Torres, J.A., additional, Morales Muñoz, G., additional, Villa Delgado, A., additional, Ladape Martínez, J., additional, Ortega Pérez, A., additional, Chávez Morales, A., additional, García Luna, A., additional, Rugiero Cabrera, A., additional, Rugerio Cabrera, A., additional, Pérez-Calatayud, Á.A., additional, Velasco Gutiérrez, A., additional, Longino Gómez, A.J., additional, Tamariz Becerra Álvarez Calderón, Antonio, additional, Álvarez Calderón Christus Mugerza, R., additional, Reynoso Estrella, C.I., additional, Déctor-Lira Espindola-Cruz, D., additional, Gutiérrez-Zárate, D., additional, Esmeralda, D., additional, Anica Malagón, E.D., additional, Monares Zepeda, E., additional, Deloya, E., additional, Manzo Palacios, E., additional, de Jesús Montelongo, F., additional, Flores Mejía, F.J., additional, Ramírez Cervantes, M., additional, Camarena Alejo, G., additional, Vázquez de Anda, G., additional, Vázquez, H., additional, Larios Luna, C., additional, Zamora, S.E., additional, Magaña Solano, G., additional, Sánchez González, J.I., additional, Rosendo Sánchez Medina, J., additional, Zaragoza, J.J., additional, Buensuseso Alfaro, J.A., additional, Dávila Fernández, J.C., additional, Mijangos-Méndez, J.C., additional, Martínez Medina, M., additional, Chacón Gómez, M., additional, Calyeca Sánchez, M.V., additional, Martínez Soria, J.J., additional, García Graullera, R.J., additional, Rosas, R., additional, Sanjuana Gómez Flores, S., additional, Reyes Inurrigarro, S., additional, Ñamendy-Silva, S.A., additional, Sánchez Hurtado, L.A., additional, Villegas Castellanos, L.L., additional, Zalatiel Maycotte, L., additional, Estrada Gutiérrez, A., additional, and León, M.A., additional

Published
2020
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10. ¿Se han producido cambios en la aplicación de la ventilación mecánica en relación con la evidencia científica? Estudio multicéntrico en México

Author

Marín, M.C., primary, Elizalde, J., additional, Villagómez, A., additional, Cerón, U., additional, Poblano, M., additional, Palma-Lara, I., additional, Sánchez, J.R., additional, Monares, E., additional, Arellano, A., additional, Muriel, A., additional, Peñuelas, Ó., additional, Frutos-Vivar, F., additional, Esteban, A., additional, Aguilera Almazán, F., additional, Benítez Cortázar, M., additional, Carrillo Speare, R., additional, Castaño, R., additional, Corral, R., additional, D́Ector Lira, D.N., additional, Díaz Polanco, G., additional, Elizalde, J.J., additional, Envila Fisher, R., additional, Franco, G., additional, García Balbuena, P., additional, Gayoso Cruz, O., additional, Green, L., additional, Herrera Hoyos, J.O., additional, Hinojosa, J., additional, Huerta, J., additional, Juárez, V.A., additional, Loera, M., additional, López Alzate, C., additional, López Mora, E., additional, Martínez Caro, S., additional, Méndez Reyes, R., additional, Mendoza, M., additional, Narváez Porras, O., additional, Ortiz, E., additional, Padua, A., additional, Pureco Reyes, V., additional, Querevalum, W., additional, Quesada, A., additional, Ramírez Rivera, A., additional, Tamariz, A., additional, Vargas, A., additional, Vázquez, C., additional, Cerda, P., additional, Mercado, R., additional, Albe Castañón, J., additional, Villagómez Ortiz, A.J., additional, Cruz Lozano, C., additional, Maycotte Luna, Z., additional, López Bacal, F., additional, Cueto Robledo, G., additional, Treviño Salinas, M.A., additional, Martínez Zubieta, R., additional, Olvera-Guzmán, C., additional, Montes de Oca, Marco, additional, Ñamendys-Silva, S.A., additional, Martínez Cano, J.S., additional, Baltazar Torres, J.A., additional, Morales Muñoz, G., additional, Villa Delgado, A., additional, Ladape Martínez, J., additional, Ortega Pérez, A., additional, Chávez Morales, A., additional, García Luna, A., additional, Rugiero Cabrera, A., additional, Rugerio Cabrera, A., additional, Pérez-Calatayud, Á.A., additional, Velasco Gutiérrez, A., additional, Longino Gómez, A.J., additional, Tamariz Becerra Álvarez Calderón, Antonio, additional, Álvarez Calderón Christus Mugerza, R., additional, Reynoso Estrella, C.I., additional, Déctor-Lira Espindola-Cruz, D., additional, Gutiérrez-Zárate, D., additional, Esmeralda, D., additional, Anica Malagón, E.D., additional, Monares Zepeda, E., additional, Deloya, E., additional, Manzo Palacios, E., additional, de Jesús Montelongo, F., additional, Flores Mejía, F.J., additional, Ramírez Cervantes, M., additional, Camarena Alejo, G., additional, Vázquez de Anda, G., additional, Vázquez, H., additional, Larios Luna, C., additional, Zamora, S.E., additional, Magaña Solano, G., additional, Sánchez González, J.I., additional, Rosendo Sánchez Medina, J., additional, Zaragoza, J.J., additional, Buensuseso Alfaro, J.A., additional, Dávila Fernández, J.C., additional, Mijangos-Méndez, J.C., additional, Martínez Medina, M., additional, Chacón Gómez, M., additional, Calyeca Sánchez, M.V., additional, Martínez Soria, J.J., additional, García Graullera, R.J., additional, Rosas, R., additional, Sanjuana Gómez Flores, S., additional, Reyes Inurrigarro, S., additional, Ñamendy-Silva, S.A., additional, Sánchez Hurtado, L.A., additional, Villegas Castellanos, L.L., additional, Zalatiel Maycotte, L., additional, Estrada Gutiérrez, A., additional, and León, M.A., additional

Published
2020
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16. Optical absorption spectroscopy measurement of the gap shrinkage due to thallium incorporation in GaInTlAs alloys.

Author

Sibai, A., Olivares, J., Guillot, G., Bremond, G., Sánchez-Almazán, F., Gendry, M., Regreny, P., and Hollinger, G.

Subjects
LOW temperatures, MOLECULAR beam epitaxy, PHOTOLUMINESCENCE, LIGHT absorption
Abstract

The optical properties of Ga[SUB(1-y)0.45] In[SUB(1-y)0.55] Tl[SUBy]As epilayers grown at low temperature (230°C) by solid-source molecular-beam epitaxy on InP substrates were characterized using optical absorption and photoluminescence techniques. Optical absorption measurements at room temperature show a gap shrinkage toward lower energies from 0.71 to 0.61 and 0.53 eV when the Tl content increases from 0% to 4%, and 8%, in good agreement with theoretical predictions. Low-temperature photoluminescence band-gap signals from GaInAs and GaInTlAs layers are only obtained after rapid thermal annealing performed in order to improve the electronic quality of the layers. A band gap decrease as much as 41 meV for GaInTlAs with 1.9% Tl incorporation is measured by photoluminescence at 8 K. [ABSTRACT FROM AUTHOR]

Published
2003
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17. Explosives Detection by Array of Si µ -Cantilevers Coated with Titanosilicate-Type Nanoporous Materials

Author

Pina Iritia, M.P., Almazán, F., Eguizábal, A., Pellejero, I., Urbiztondo, M., Sesé, J., Santamaría, J., García-Romeo, D., Calvo, B., and Medrano, N.

Abstract

An array comprising four Si µ -cantilevers coated with nanoporous functionalized ETS-10 crystals sub-micrometric in size has been developed as a multisensing platform for explosives recognition in vapor phase. The detection capabilities of the proposed device have been tested for common taggants such as 1-methyl-2-nitro-benzene (o-MNT)] and explosives (commercial detonation cord, a plastic tube filled with pentaerythritol tetranitrate (PETN); and C-4, a mixture of cyclotrimethylenetrinitramine (RDX), binders and plastifiers). The general strategy for the detection of explosives in vapor phase is based on the characteristic fingerprint each one produces as a result of the dissimilar chemical interactions between the ETS-10 coated µ -cantilevers and the target molecules emanating from the explosives and swept by ambient air. A portable lock-in amplifier has been implemented to exploit the truly benefits of the array in terms of portability, reduced size, and energy consumption. Such low-power electronic interface is capable of creating the excitation signal as well as obtaining the response values of four resonating µ -cantilevers simultaneously. The resulting sensing platform has successfully been applied for the o-MNT, PETN, and RDX detection at trace level.

Published
2016

18. Explosives detection by array of Si µ-cantilevers coated with titanosilicate type nanoporous materials

Author

Pina, M.P., Almazán, F., Eguizábal, A., Pellejero, I., Urbiztondo, M., Sesé, J., Santamaría, J., García-Romeo, D., Calvo, B., and Medrano, N.

Abstract

An array comprising 4 Si microcantilevers coated with nanoporous ETS-10 crystals sub-micrometric in size has been deployed as a multisensing platform for 2-nitrotoluene (an explosive related molecule) recognition. For such purposes, the adsorption properties of synthetic microporous ETS-10 titanosilicate type materials have been tailored by means of the Si/Ti ratio, and surface grafting with organic groups (amine, imidazol). Our general strategy for vapor detection of explosives involves the combination of Si based nanoporous solids as sensing materials and resonating Si cantilevers provided with self-heating elements as tiny microbalances (mass sensitivity factors ~18 Hz/ng). Particularly for this work, ETS-10 type titanosilicates with promoted basic properties (Si/Ti=4, -NH2 anchored on the external surface) exhibit the higher affinity towards nitroaromatic derivatives as electron defficient molecules. A high remarkable hydrophilic character is shown by titanosilicates modified by covalent linkage with imidazole based organosilane (above 17% wt. water uptake at room temperature). Accounting from such versatile sorption behavior, the family of nanoporous ETS-10 crystals has been deployed by microdropping technique over the 8 Si-microcantilevers chip. By means of a portable lowpower electronic interface capable of the simultaneous excitation and measurement of 4 sensor output signals, such multisensing platform has been successfully applied for 2-nitrotoluene detection at trace level.

Published
2014

20. Growth of GaInTlAsalloys on InP by low temperature molecular beam epitaxy

Author

Sánchez-Almazán, F., Gendry, Michel, Regreny, Philippe, Bergignat, E., Grenet, G., Hollinger, Guy, Olivares, Jose, Bremond, Georges, Marty, Olivier, Pitaval, Michel, Laboratoire d'électronique, optoélectronique et microsystèmes (LEOM), École Centrale de Lyon (ECL), Université de Lyon-Université de Lyon-Centre National de la Recherche Scientifique (CNRS), Laboratoire de physique de la matière (LPM), Institut National des Sciences Appliquées de Lyon (INSA Lyon), Institut National des Sciences Appliquées (INSA)-Université de Lyon-Institut National des Sciences Appliquées (INSA)-Université de Lyon-Centre National de la Recherche Scientifique (CNRS), Laboratoire d'Electronique, Nanotechnologies, Capteurs (LENAC), Université Claude Bernard Lyon 1 (UCBL), and Gendry, Michel

Subjects
[SPI.NANO] Engineering Sciences [physics]/Micro and nanotechnologies/Microelectronics, [SPI.NANO]Engineering Sciences [physics]/Micro and nanotechnologies/Microelectronics, ComputingMilieux_MISCELLANEOUS
Abstract

International audience

Published
2001

23. Growth of GaInTlAs layers on InP by molecular beam epitaxy

Author

Sánchez-Almazán, F., primary, Gendry, M., additional, Regreny, P., additional, Bergignat, E., additional, Grenet, G., additional, Hollinger, G., additional, Olivares, J., additional, Bremond, G., additional, Marty, O., additional, Pitaval, M., additional, and Canut, B., additional

Published
2001
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34. Prognostic significance of mutation type and chromosome fragility in Fanconi anemia.

Author

Ramírez MJ, Pujol R, Minguillón J, Bogliolo M, Persico I, Cavero D, de la Cal A, Río P, Navarro S, Casado JA, Bailador A, de la Fuente AS, de Heredia ML, Almazán F, Antelo ML, Argilés B, Badell I, Baragaño M, Beléndez C, Bermúdez M, Bernués M, Buedo MI, Carrasco E, Català A, Costa D, Cuesta I, Fernandez-Delgado R, Fernández-Teijeiro A, Figuera Á, García M, Gondra A, González M, Muñiz SG, Hernández-Rodríguez I, Ibañez F, Kelleher NJ, Lendínez F, López M, López-Almaraz R, Marchante I, Mendoza C, Nieto J, Ojeda E, Payán-Pernía S, Peláez I, de Soto IP, Portugal R, Ramos-Arroyo MA, Regueiro A, Rodríguez A, Rosell J, Saez R, Sánchez J, Sánchez M, Senent M, Tapia M, Trujillo-Quintero JP, Vagace JM, Verdú-Amorós J, Verdugo V, Vidales I, Villarreal J, Díaz-de-Heredia C, Sevilla J, Bueren JA, and Surrallés J

Subjects
Adolescent, Adult, Child, Child, Preschool, Female, Humans, Infant, Male, Middle Aged, Young Adult, Fanconi Anemia Complementation Group D2 Protein genetics, Follow-Up Studies, Neoplasms genetics, Prognosis, Chromosome Fragility, Fanconi Anemia genetics, Fanconi Anemia Complementation Group A Protein genetics, Fanconi Anemia Complementation Group G Protein genetics, Mutation
Abstract

Fanconi anemia (FA) is a rare genetic disease characterized by high phenotypic and genotypic heterogeneity, and extreme chromosome fragility. To better understand the natural history of FA, identify genetic risk and prognostic factors, and develop novel therapeutic strategies, the Spanish Registry of Patients with FA collects data on clinical features, chromosome fragility, genetic subtypes, and DNA sequencing with informed consent of participating individuals. In this article, we describe the clinical evolution of 227 patients followed up for up to 30 years, for whom our data indicate a cumulative cancer incidence of 86% by age 50. We found that patients with lower chromosome fragility had a milder malformation spectrum and better outcomes in terms of later-onset hematologic impairment, less severe bone marrow failure, and lower cancer risk. We also found that outcomes were better for patients with mutations leading to mutant FANCA protein expression (genetic hypomorphism) than for patients lacking this protein. Likewise, prognosis was consistently better for patients with biallelic mutations in FANCD2 (mainly hypomorphic mutations) than for patients with biallelic mutations in FANCA and FANCG, with the lack of the mutant protein in patients with biallelic mutations in FANCG contributing to their poorer outcomes. Our results regarding the clinical impact of chromosome fragility and genetic hypomorphism suggest that mutant FA proteins retain residual activity. This finding should encourage the development of novel therapeutic strategies aimed at partially or fully enhancing mutant FA function, thereby preventing or delaying bone marrow failure and cancer in patients with FA. Clinical Trial Registration number: NCT06490510., (© 2024 The Author(s). American Journal of Hematology published by Wiley Periodicals LLC.)

Published
2025
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35. Editorial for SARS-CoV-2 and COVID-19 Topical Collection.

Author

Martinez-Sobrido L and Almazán F

Subjects
Animals, Humans, SARS-CoV-2, Animals, Wild, China epidemiology, COVID-19
Abstract

A previously unknown coronavirus, severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), was isolated in Wuhan, China in December 2019, from a patient with a respiratory disease linked to potential contact with wild animals [...].

Published
2024
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36. Gold Nanoparticles Capped with a Novel Titanium(IV)-Containing Polyoxomolybdate Cluster: Selective and Enhanced Bactericidal Effect Against Escherichia coli.

Author

Paesa M, Almazán F, Yus C, Sebastián V, Arruebo M, Gandía LM, Reinoso S, Pellejero I, and Mendoza G

Subjects
Animals, Gold chemistry, Escherichia coli, Titanium pharmacology, Staphylococcus aureus, Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents chemistry, Microbial Sensitivity Tests, Mammals, Metal Nanoparticles chemistry, Anti-Infective Agents pharmacology, Staphylococcal Infections
Abstract

Bacterial infections are a public health threat of increasing concern in medical care systems; hence, the search for novel strategies to lower the use of antibiotics and their harmful effects becomes imperative. Herein, the antimicrobial performance of four polyoxometalate (POM)-stabilized gold nanoparticles (Au@POM) against Escherichia coli (E. coli) and Staphylococcus aureus (S. aureus) as Gram-negative and Gram-positive bacteria models, respectively, is studied. The bactericidal studies performed, both in planktonic and sessile forms, evidence the antimicrobial potential of these hybrid nanostructures with selectivity toward Gram-negative species. In particular, the Au@GeMoTi composite with the novel [Ti 2 (HGeMo 7 O 28 ) 2 ] 10- POM capping ligand exhibits outstanding bactericidal efficiency with a minimum inhibitory concentration of just 3.12 µm for the E. coli strain, thus outperforming the other three Au@POM counterparts. GeMoTi represents the fourth example of a water-soluble Ti IV -containing polyoxomolybdate, and among them, the first sandwich-type structure having heteroatoms in high-oxidation state. The evaluation of the bactericidal mechanisms of action points to the cell membrane hyperpolarization, disruption, and subsequent nucleotide leakage and the low cytotoxicity exerted on five different cell lines at antimicrobial doses demonstrates the antibiotic-like character. These studies highlight the successful design and development of a new POM-based nanomaterial able to eradicate Gram-negative bacteria without damaging mammalian cells., (© 2023 The Authors. Small published by Wiley-VCH GmbH.)

Published
2024
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37. Reverse Genetics of Zika Virus Using a Bacterial Artificial Chromosome.

Author

Nogales A, Martínez-Sobrido L, and Almazán F

Subjects
Animals, Humans, Chromosomes, Artificial, Bacterial genetics, Reverse Genetics methods, DNA, Complementary genetics, Virus Replication, Zika Virus genetics, Zika Virus Infection
Abstract

Zika virus (ZIKV) is a mosquito-borne member of the Flaviviridae family that has become a global threat to human health. Although ZIKV has been known to circulate for decades causing mild febrile illness, the more recent ZIKV outbreaks in the Americas and the Caribbean have been associated with severe neurological disorders and congenital abnormalities. The development of ZIKV reverse genetics approaches have allowed researchers to address key questions on the biology of ZIKV by genetically engineering infectious recombinant (r)ZIKV. This has resulted in a better understanding of the biology of ZIKV infections, including viral pathogenesis, molecular mechanisms of viral replication and transcription, or the interaction of viral and host factors, among others aspects. In addition, reverse genetics systems have facilitated the identification of anti-ZIKV compounds and the development of new prophylactic approaches to combat ZIKV infections. Different reverse genetics strategies have been implemented for the recovery of rZIKV. All these reverse genetics systems have faced and overcome multiple challenges, including the viral genome size, the toxicity of viral sequences in bacteria, etc. In this chapter we describe the generation of a ZIKV full-length complementary (c)DNA infectious clone based on the use of a bacterial artificial chromosome (BAC) and the experimental procedures for the successful recovery of rZIKV. Importantly, the protocol described in this chapter provides a powerful method for the generation of infectious clones of other flaviviruses with genomes that have stability problems during bacterial propagation., (© 2024. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published
2024
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38. Bacterial Artificial Chromosome Reverse Genetics Approaches for SARS-CoV-2.

Author

Chiem K, Nogales A, Almazán F, Ye C, and Martínez-Sobrido L

Subjects
Humans, Chromosomes, Artificial, Bacterial genetics, Reverse Genetics methods, Virus Replication genetics, SARS-CoV-2 genetics, COVID-19
Abstract

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is a new member of the Coronaviridae family responsible for the coronavirus disease 19 (COVID-19) pandemic. To date, SARS-CoV-2 has been accountable for over 624 million infection cases and more than 6.5 million human deaths. The development and implementation of SARS-CoV-2 reverse genetics approaches have allowed researchers to genetically engineer infectious recombinant (r)SARS-CoV-2 to answer important questions in the biology of SARS-CoV-2 infection. Reverse genetics techniques have also facilitated the generation of rSARS-CoV-2 expressing reporter genes to expedite the identification of compounds with antiviral activity in vivo and in vitro. Likewise, reverse genetics has been used to generate attenuated forms of the virus for their potential implementation as live-attenuated vaccines (LAV) for the prevention of SARS-CoV-2 infection. Here we describe the experimental procedures for the generation of rSARS-CoV-2 using a well-established and robust bacterial artificial chromosome (BAC)-based reverse genetics system. The protocol allows to produce wild-type and mutant rSARS-CoV-2 that can be used to understand the contribution of viral proteins and/or amino acid residues in viral replication and transcription, pathogenesis and transmission, and interaction with cellular host factors., (© 2024. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published
2024
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39. Spontaneous Interconversion between Different Narrowly Defined Shapes of Rotavirus Double-Layered Particles Studied in Real Time by High-Resolution Mobility Analysis.

Author

Fernandez de la Mora J, Almazán F, and Rodríguez JM

Subjects
Cryoelectron Microscopy, Capsid Proteins, Rotavirus chemistry
Abstract

Rotavirus double-layered particles (DLPs) are studied in the gas phase with a high-resolution differential mobility analyzer (DMA). DLPs were transferred to 10 mM aqueous ammonium acetate, electrosprayed into the gas phase, converted into primarily singly charged particles, and DMA-analyzed. Up to seven slightly different conformations were resolved, whose apparently random, fast (minutes), and reversible interconversions were followed in real time. They sometimes evolved into just two distinct structures, with periods of one dominating over the other and vice versa. Differences between the DLP structures in solution and in the gas phase are clearly revealed by the smaller DLP diameter found here (60 versus 70 nm). Nevertheless, we argue that the multiple gas-phase conformers observed originate in as many conformations pre-existing in solution. We further hypothesize that these conformers correspond to incomplete DLPs having lost some of the VP6 trimer quintets surrounding each of the 12 5-fold axes. Instances of this peculiar loss have been previously documented by cryoelectron microscopy for the rotavirus Wa strain, as well as via charge detection mass spectrometry for five other rotavirus strains included in the RotaTec vaccine. Evidence of this loss systematically found for all 7 rotavirus types so far studied in aqueous ammonium acetate may be a special feature of this electrolyte.

Published
2023
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40. On-chip monitoring of toxic gases: capture and label-free SERS detection with plasmonic mesoporous sorbents.

Author

Lafuente M, Almazán F, Bernad E, Florea I, Arenal R, Urbiztondo MA, Mallada R, and Pina MP

Abstract

The detection of the spread of toxic gas molecules in the air at low concentration in the field requires a robust miniaturized system combined with an analytical technique that is portable and able to detect and identify the molecules, as is the case with surface enhanced Raman scattering (SERS). This work aims to address capability gaps faced by first responders in real-time detection, identification and monitoring of neurotoxic gases by developing robust, reliable and reusable SERS microfluidic chips. Thus, the key performance attributes of a portable SERS detection system that must be addressed in detail are its limit of detection, response time and reusability. To this purpose, we integrate a 3D plasmonic architecture based on closely packed mesoporous silica (MCM48) nanospheres decorated with Au nanoparticle arrays, denoted as MCM48@Au, into a Si microfluidic chip designed and used for preconcentration and label-free detection of gases at a trace concentration level. The SERS performance of the plasmonic platform is thoroughly analyzed using DMMP as a model neurotoxic simulant over a 1 cm 2 SERS active area and over a range of concentrations from 100 ppbV to 2.5 ppmV. The preconcentration-based SERS signal amplification by the mesoporous silica moieties is evaluated against dense silica counterparts, denoted as Stöber@Au. To assess the potential for applications in the field, the microfluidic SERS chip has been interrogated with a portable Raman spectrometer, evaluated with temporal and spatial resolution and subjected to several gas detection/regeneration cycles. The reusable SERS chip shows exceptional performance for the label-free monitoring of 2.5 ppmV gaseous DMMP.

Published
2023
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42. In vivo rescue of recombinant Zika virus from an infectious cDNA clone and its implications in vaccine development.

Author

Ávila-Pérez G, Nogales A, Park JG, Vasquez DM, Dean DA, Barravecchia M, Perez DR, Almazán F, and Martínez-Sobrido L

Subjects
Animals, Chlorocebus aethiops, DNA, Complementary immunology, DNA, Viral genetics, DNA, Viral immunology, Disease Models, Animal, Female, Male, Mice, Receptor, Interferon alpha-beta genetics, Reverse Genetics, Vaccines, Attenuated administration & dosage, Vaccines, Attenuated immunology, Vero Cells, Viral Vaccines administration & dosage, Viral Vaccines immunology, Viremia genetics, Viremia immunology, Zika Virus immunology, Zika Virus Infection genetics, Zika Virus Infection immunology, Chromosomes, Artificial, Bacterial genetics, DNA, Complementary genetics, Genetic Vectors administration & dosage, Viremia prevention & control, Zika Virus genetics, Zika Virus Infection prevention & control
Abstract

Zika virus (ZIKV) is a mosquito-borne member of the Flaviviridae family that has been known to circulate for decades causing mild febrile illness. The more recent ZIKV outbreaks in the Americas and the Caribbean associated with congenital malformations and Guillain-Barré syndrome in adults have placed public health officials in high alert and highlight the significant impact of ZIKV on human health. New technologies to study the biology of ZIKV and to develop more effective prevention options are highly desired. In this study we demonstrate that direct delivery in mice of an infectious ZIKV cDNA clone allows the rescue of recombinant (r)ZIKV in vivo. A bacterial artificial chromosome containing the sequence of ZIKV strain Paraiba/2015 under the control of the cytomegalovirus promoter was complexed with a commercial transfection reagent and administrated using different routes in type-I interferon receptor deficient A129 mice. Clinical signs and death associated with ZIKV viremia were observed in mice. The rZIKV recovered from these mice remained fully virulent in a second passage in mice. Interestingly, infectious rZIKV was also recovered after intraperitoneal inoculation of the rZIKV cDNA in the absence of transfection reagent. Further expanding these studies, we demonstrate that a single intraperitoneal inoculation of a cDNA clone encoding an attenuated rZIKV was safe, highly immunogenic, and provided full protection against lethal ZIKV challenge. This novel in vivo reverse genetics method is a potentially suitable delivery platform for the study of wild-type and live-attenuated ZIKV devoid of confounding factors typical associated with in vitro systems. Moreover, our results open the possibility of employing similar in vivo reverse genetic approaches for the generation of other viruses and, therefore, change the way we will use reverse genetics in the future.

Published
2020
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43. Rescue of Recombinant Zika Virus from a Bacterial Artificial Chromosome cDNA Clone.

Author

Ávila-Pérez G, Park JG, Nogales A, Almazán F, and Martínez-Sobrido L

Subjects
Animals, Chlorocebus aethiops, Clone Cells, Genome, Viral, Humans, Vero Cells, Virion genetics, Zika Virus immunology, Zika Virus Infection virology, Chromosomes, Artificial, Bacterial genetics, DNA, Complementary genetics, Recombination, Genetic genetics, Zika Virus genetics
Abstract

The association of Zika virus (ZIKV) infection with neurological complications during the recent worldwide outbreak and the lack of approved vaccines and/or antivirals have underscored the urgent need to develop ZIKV reverse genetic systems to facilitate the study of ZIKV biology and the development of therapeutic and/or prophylactic approaches. However, like with other flaviviruses, the generation of ZIKV full-length infectious cDNA clones has been hampered due to the toxicity of viral sequences during its amplification in bacteria. To overcome this problem, we have developed a nontraditional approach based on the use of bacterial artificial chromosomes (BACs). Using this approach, the full-length cDNA copy of the ZIKV strain Rio Grande do Norte Natal (ZIKV-RGN) is generated from four synthetic DNA fragments and assembled into the single-copy pBeloBAC11 plasmid under the control of the human cytomegalovirus (CMV) immediate-early promoter. The assembled BAC cDNA clone is stable during propagation in bacteria, and infectious recombinant (r)ZIKV is recovered in Vero cells after transfection of the BAC cDNA clone. The protocol described here provides a powerful technique for the generation of infectious clones of flaviviruses, including ZIKV, and other positive-strand RNA viruses, particularly those with large genomes that have stability problems during bacterial propagation.

Published
2019
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44. Potent Inhibition of Zika Virus Replication by Aurintricarboxylic Acid.

Author

Park JG, Ávila-Pérez G, Madere F, Hilimire TA, Nogales A, Almazán F, and Martínez-Sobrido L

Abstract

Zika virus (ZIKV) is one of the recently emerging vector-borne viruses in humans and is responsible for severe congenital abnormalities such as microcephaly in the Western Hemisphere. Currently, only a few vaccine candidates and therapeutic drugs are being developed for the treatment of ZIKV infections, and as of yet none are commercially available. The polyanionic aromatic compound aurintricarboxylic acid (ATA) has been shown to have a broad-spectrum antimicrobial and antiviral activity. In this study, we evaluated ATA as a potential antiviral drug against ZIKV replication. The antiviral activity of ATA against ZIKV replication in vitro showed median inhibitory concentrations (IC 50 ) of 13.87 ± 1.09 μM and 33.33 ± 1.13 μM in Vero and A549 cells, respectively; without showing any cytotoxic effect in both cell lines (median cytotoxic concentration (CC 50 ) > 1,000 μM). Moreover, ATA protected both cell types from ZIKV-induced cytopathic effect (CPE) and apoptosis in a time- and concentration-dependent manner. In addition, pre-treatment of Vero cells with ATA for up to 72 h also resulted in effective suppression of ZIKV replication with similar IC 50 . Importantly, the inhibitory effect of ATA on ZIKV infection was effective against strains of the African and Asian/American lineages, indicating that this inhibitory effect was not strain dependent. Overall, these results demonstrate that ATA has potent inhibitory activity against ZIKV replication and may be considered as a potential anti-ZIKV therapy for future clinical evaluation.

Published
2019
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45. New Advances on Zika Virus Research.

Author

Martinez-Sobrido L and Almazán F

Subjects
Disease Outbreaks, Female, Humans, Mosquito Vectors virology, Pregnancy, Pregnancy Complications, Infectious virology, Zika Virus pathogenicity, Zika Virus Infection complications, Host Microbial Interactions, Research trends, Zika Virus Infection epidemiology
Abstract

Zika virus (ZIKV) is an emerging mosquito-borne member of the Flaviviridae family that has historically been known to cause sporadic outbreaks, associated with a mild febrile illness, in Africa and Southeast Asia [...].

Published
2019
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46. Reverse Genetic Approaches for the Generation of Recombinant Zika Virus.

Author

Ávila-Pérez G, Nogales A, Martín V, Almazán F, and Martínez-Sobrido L

Subjects
Animals, DNA, Complementary, Genome, Viral, Humans, Virus Replication, Zika Virus physiology, Recombination, Genetic, Reverse Genetics, Zika Virus genetics, Zika Virus Infection virology
Abstract

Zika virus (ZIKV) is an emergent mosquito-borne member of the Flaviviridae family that was responsible for a recent epidemic in the Americas. ZIKV has been associated with severe clinical complications, including neurological disorder such as Guillain-Barré syndrome in adults and severe fetal abnormalities and microcephaly in newborn infants. Given the significance of these clinical manifestations, the development of tools and reagents to study the pathogenesis of ZIKV and to develop new therapeutic options are urgently needed. In this respect, the implementation of reverse genetic techniques has allowed the direct manipulation of the viral genome to generate recombinant (r)ZIKVs, which have provided investigators with powerful systems to answer important questions about the biology of ZIKV, including virus-host interactions, the mechanism of transmission and pathogenesis or the function of viral proteins. In this review, we will summarize the different reverse genetic strategies that have been implemented, to date, for the generation of rZIKVs and the applications of these platforms for the development of replicon systems or reporter-expressing viruses.

Published
2018
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47. An Alanine-to-Valine Substitution in the Residue 175 of Zika Virus NS2A Protein Affects Viral RNA Synthesis and Attenuates the Virus In Vivo.

Author

Márquez-Jurado S, Nogales A, Ávila-Pérez G, Iborra FJ, Martínez-Sobrido L, and Almazán F

Subjects
A549 Cells, Amino Acid Substitution, Animals, Chlorocebus aethiops, Chromosomes, Artificial, Bacterial genetics, DNA, Complementary genetics, Female, Humans, Mice, Mice, Knockout, RNA, Viral genetics, Receptor, Interferon alpha-beta deficiency, Receptor, Interferon alpha-beta genetics, Reverse Genetics, Vaccines, Attenuated administration & dosage, Vaccines, Attenuated immunology, Vero Cells, Viral Vaccines administration & dosage, Viral Vaccines immunology, Virus Replication, Zika Virus immunology, Zika Virus Infection prevention & control, Viral Nonstructural Proteins genetics, Viral Proteins genetics, Zika Virus genetics, Zika Virus pathogenicity, Zika Virus Infection pathology, Zika Virus Infection virology
Abstract

The recent outbreaks of Zika virus (ZIKV), its association with Guillain⁻Barré syndrome and fetal abnormalities, and the lack of approved vaccines and antivirals, highlight the importance of developing countermeasures to combat ZIKV disease. In this respect, infectious clones constitute excellent tools to accomplish these goals. However, flavivirus infectious clones are often difficult to work with due to the toxicity of some flavivirus sequences in bacteria. To bypass this problem, several alternative approaches have been applied for the generation of ZIKV clones including, among others, in vitro ligation, insertions of introns and using infectious subgenomic amplicons. Here, we report a simple and novel DNA-launched approach based on the use of a bacterial artificial chromosome (BAC) to generate a cDNA clone of Rio Grande do Norte Natal ZIKV strain. The sequence was identified from the brain tissue of an aborted fetus with microcephaly. The BAC clone was fully stable in bacteria and the infectious virus was efficiently recovered in Vero cells through direct delivery of the cDNA clone. The rescued virus yielded high titers in Vero cells and was pathogenic in a validated mouse model (A129 mice) of ZIKV infection. Furthermore, using this infectious clone we have generated a mutant ZIKV containing a single amino acid substitution (A175V) in the NS2A protein that presented reduced viral RNA synthesis in cell cultures, was highly attenuated in vivo and induced fully protection against a lethal challenge with ZIKV wild-type. This BAC approach provides a stable and reliable reverse genetic system for ZIKV that will help to identify viral determinants of virulence and facilitate the development of vaccine and therapeutic strategies.

Published
2018
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48. Mitochondrial levels determine variability in cell death by modulating apoptotic gene expression.

Author

Márquez-Jurado S, Díaz-Colunga J, das Neves RP, Martinez-Lorente A, Almazán F, Guantes R, and Iborra FJ

Subjects
Algorithms, Apoptosis drug effects, Apoptosis Regulatory Proteins genetics, Apoptosis Regulatory Proteins metabolism, Cell Death genetics, Gene Expression drug effects, HeLa Cells, Humans, Mitochondria metabolism, Models, Genetic, Reactive Oxygen Species metabolism, Signal Transduction drug effects, TNF-Related Apoptosis-Inducing Ligand pharmacology, Apoptosis genetics, Gene Expression genetics, Mitochondria genetics, Signal Transduction genetics
Abstract

Fractional killing is the main cause of tumour resistance to chemotherapy. This phenomenon is observed even in genetically identical cancer cells in homogeneous microenvironments. To understand this variable resistance, here we investigate the individual responses to TRAIL in a clonal population of HeLa cells using live-cell microscopy and computational modelling. We show that the cellular mitochondrial content determines the apoptotic fate and modulates the time to death, cells with higher mitochondrial content are more prone to die. We find that all apoptotic protein levels are modulated by the mitochondrial content. Modelling the apoptotic network, we demonstrate that these correlations, and especially the differential control of anti- and pro-apoptotic protein pairs, confer mitochondria a powerful discriminatory capacity of apoptotic fate. We find a similar correlation between the mitochondria and apoptotic proteins in colon cancer biopsies. Our results reveal a different role of mitochondria in apoptosis as the global regulator of apoptotic protein expression.

Published
2018
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49. Generation of a DNA-Launched Reporter Replicon Based on Dengue Virus Type 2 as a Multipurpose Platform.

Author

Usme-Ciro JA, Lopera JA, Alvarez DA, Enjuanes L, and Almazán F

Abstract

Dengue viruses (DENV) have become the most important arthropod-borne viruses, causing dengue and severe dengue fever in at least 50-100 million cases each year, mainly in tropical and subtropical countries. During recent years, important advances in the molecular biology concerning the life cycle of these viruses have allowed the manipulation and generation of recombinant viruses and replicons with multiple applications, mainly in viral biology and the screening of antiviral compounds. In the present study, we describe the construction of an enhanced green fluorescent protein-bearing DENV replicon under the control of the cytomegalovirus immediate early promoter. Following a rational in silico design and cloning by standard molecular biology techniques, a reporter DENV-2 replicon and a replication-deficient mutant were constructed, and characterized by confocal microscopy and real-time RT-PCR. The results showed successful transcription, translation, and autonomous viral RNA replication of the DENV replicon from its DNA clone. This novel DENV replicon will allow the study of viral replication and testing of antiviral candidates without the need for in vitro transcription., (© 2017 S. Karger AG, Basel.)

Published
2016
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50. Continuous and Discontinuous RNA Synthesis in Coronaviruses.

Author

Sola I, Almazán F, Zúñiga S, and Enjuanes L

Subjects
Animals, Coronavirus metabolism, Humans, RNA, Viral metabolism, Transcription, Genetic, Coronavirus genetics, Coronavirus Infections virology, RNA, Viral genetics
Abstract

Replication of the coronavirus genome requires continuous RNA synthesis, whereas transcription is a discontinuous process unique among RNA viruses. Transcription includes a template switch during the synthesis of subgenomic negative-strand RNAs to add a copy of the leader sequence. Coronavirus transcription is regulated by multiple factors, including the extent of base-pairing between transcription-regulating sequences of positive and negative polarity, viral and cell protein-RNA binding, and high-order RNA-RNA interactions. Coronavirus RNA synthesis is performed by a replication-transcription complex that includes viral and cell proteins that recognize cis-acting RNA elements mainly located in the highly structured 5' and 3' untranslated regions. In addition to many viral nonstructural proteins, the presence of cell nuclear proteins and the viral nucleocapsid protein increases virus amplification efficacy. Coronavirus RNA synthesis is connected with the formation of double-membrane vesicles and convoluted membranes. Coronaviruses encode proofreading machinery, unique in the RNA virus world, to ensure the maintenance of their large genome size.

Published
2015
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