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6. Introducción

Author

Ochoa Villanueva, Euridice Minerva, Rengifo Mattos, Karina, and Sánchez Aguilar, Alejandra

Published
2023

7. Legales

Author

Ochoa Villanueva, Euridice Minerva, Rengifo Mattos, Karina, and Sánchez Aguilar, Alejandra

Published
2023

8. Prólogo

Author

Ochoa Villanueva, Euridice Minerva, Rengifo Mattos, Karina, and Sánchez Aguilar, Alejandra

Published
2023

10. Agradecimientos

Author

Ochoa Villanueva, Euridice Minerva, Rengifo Mattos, Karina, and Sánchez Aguilar, Alejandra

Published
2023

15. Euclid preparation: XIII. Forecasts for galaxy morphology with the Euclid Survey using Deep Generative Models

Author

Euclid Collaboration, Bretonnière, H., Huertas-Company, M., Boucaud, A., Lanusse, F., Jullo, E., MERLIN, Emiliano, Tuccillo, D., CASTELLANO, MARCO, Brinchmann, J., Conselice, C. J., Poncet, M., Popa, L., POZZETTI, Lucia, Raison, F., Rebolo, R., Rhodes, J., Roncarelli, M., Rossetti, E., Saglia, R., Schneider, P., Dole, H., Secroun, A., Seidel, G., Sirignano, C., Sirri, G., Stanco, L., Starck, J. -L., Tallada-Crespí, P., Taylor, A. N., Tereno, I., Toledo-Moreo, R., Cabanac, R., Torradeflot, F., Valentijn, E. A., VALENZIANO, LUCA, Wang, Y., Welikala, N., Weller, J., Zamorani, G., Zoubian, J., Baldi, M., BARDELLI, Sandro, Courtois, H. M., Camera, S., FARINELLI, Ruben, Medinaceli, E., Mei, S., Polenta, G., Romelli, Erik, Tenti, M., Vassallo, T., ZACCHEI, Andrea, ZUCCA, Elena, Castander, F. J., Baccigalupi, C., Balaguera-Antolínez, A., BIVIANO, ANDREA, BORGANI, STEFANO, Bozzo, E., BURIGANA, CARLO, CAPPI, Alberto, Carvalho, C. S., Casas, S., Castignani, G., Duc, P. A., Colodro-Conde, C., Coupon, J., de la Torre, S., Fabricius, M., FARINA, Maria, Ferreira, P. G., Flose-Reimberg, P., Fotopoulou, S., GALEOTTA, Samuele, Ganga, K., Fosalba, P., Garcia-Bellido, J., Gaztanaga, E., Gozaliasl, G., Hook, I. M., Joachimi, B., Kansal, V., Kashlinsky, A., Keihanen, E., Kirkpatrick, C. C., Lindholm, V., Guinet, D., Mainetti, G., Maino, D., Maoli, R., Martinelli, M., Martinet, N., McCracken, H. J., Metcalf, R. B., MORGANTE, GIANLUCA, Morisset, N., Nightingale, J., Kruk, S., Nucita, A., Patrizii, L., Potter, D., Renzi, A., RICCIO, GIUSEPPE, Sánchez, A. G., Sapone, D., Schirmer, M., Schultheis, M., Scottez, V., Kuchner, U., SEFUSATTI, Emiliano, Teyssier, R., Tutusaus, I., Valiviita, J., VIEL, MATTEO, Whittaker, L., Knapen, J. H., Serrano, S., Soubrie, E., Tramacere, A., Wang, L., Amara, A., AURICCHIO, NATALIA, Bender, R., Bodendorf, C., BONINO, Donata, Branchini, Enzo, Brau-Nogue, S., BRESCIA, Massimo, Capobianco, Vito, CARBONE, Carmelita, Carretero, J., CAVUOTI, STEFANO, Cimatti, A., Cledassou, R., Congedo, G., Conversi, L., Copin, Y., CORCIONE, Leonardo, Costille, A., Cropper, M., Da Silva, A., Degaudenzi, H., Douspis, M., Dubath, F., Duncan, C. A. J., Dupac, X., Dusini, S., Farrens, S., Ferriol, S., FRAILIS, Marco, FRANCESCHI, ENRICO, FUMANA, Marco, GARILLI, BIANCA MARIA ROSA, Gillard, W., Gillis, B., GIOCOLI, Carlo, GRAZIAN, Andrea, Grupp, F., Haugan, S. V. H., Holmes, W., Hormuth, F., Hudelot, P., Jahnke, K., Kermiche, S., Kiessling, A., Kilbinger, M., Kitching, T., Kohley, R., Kümmel, M., Kunz, M., Kurki-Suonio, H., LIGORI, Sebastiano, Lilje, P. B., Lloro, I., MAIORANO, Elisabetta, MANSUTTI, Oriana, Marggraf, O., Markovic, K., Marulli, F., Massey, R., Maurogordato, S., Melchior, M., MENEGHETTI, MASSIMO, Meylan, G., Moresco, M., Morin, B., Moscardini, L., Munari, Emiliano, Nakajima, R., Niemi, S. M., Padilla, C., Paltani, S., Pasian, F., Pedersen, K., Pettorino, V., Pires, S., Astrophysique Interprétation Modélisation (AIM (UMR_7158 / UMR_E_9005 / UM_112)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Institut national des sciences de l'Univers (INSU - CNRS)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS)-Université de Paris (UP), Laboratoire de Cosmologie et Statistiques (LCS - COSMOSTAT), Institut de Recherches sur les lois Fondamentales de l'Univers (IRFU), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay, Lanusse, Francois, UAM. Departamento de Física Teórica, Bretonniere, H., Huertas-Company, M., Boucaud, A., Lanusse, F., Jullo, E., Merlin, E., Tuccillo, D., Castellano, M., Brinchmann, J., Conselice, C. J., Dole, H., Cabanac, R., Courtois, H. M., Castander, F. J., Duc, P. A., Fosalba, P., Guinet, D., Kruk, S., Kuchner, U., Serrano, S., Soubrie, E., Tramacere, A., Wang, L., Amara, A., Auricchio, N., Bender, R., Bodendorf, C., Bonino, D., Branchini, E., Brau-Nogue, S., Brescia, M., Capobianco, V., Carbone, C., Carretero, J., Cavuoti, S., Cimatti, A., Cledassou, R., Congedo, G., Conversi, L., Copin, Y., Corcione, L., Costille, A., Cropper, M., Da Silva, A., Degaudenzi, H., Douspis, M., Dubath, F., Duncan, C. A. J., Dupac, X., Dusini, S., Farrens, S., Ferriol, S., Frailis, M., Franceschi, E., Fumana, M., Garilli, B., Gillard, W., Gillis, B., Giocoli, C., Grazian, A., Grupp, F., Haugan, S. V. H., Holmes, W., Hormuth, F., Hudelot, P., Jahnke, K., Kermiche, S., Kiessling, A., Kilbinger, M., Kitching, T., Kohley, R., Kummel, M., Kunz, M., Kurki-Suonio, H., Ligori, S., Lilje, P. B., Lloro, I., Maiorano, E., Mansutti, O., Marggraf, O., Markovic, K., Marulli, F., Massey, R., Maurogordato, S., Melchior, M., Meneghetti, M., Meylan, G., Moresco, M., Morin, B., Moscardini, L., Munari, E., Nakajima, R., Niemi, S. M., Padilla, C., Paltani, S., Pasian, F., Pedersen, K., Pettorino, V., Pires, S., Poncet, M., Popa, L., Pozzetti, L., Raison, F., Rebolo, R., Rhodes, J., Roncarelli, M., Rossetti, E., Saglia, R., Schneider, P., Secroun, A., Seidel, G., Sirignano, C., Sirri, G., Stanco, L., Starck, J. -L., Tallada-Crespi, P., Taylor, A. N., Tereno, I., Toledo-Moreo, R., Torradeflot, F., Valentijn, E. A., Valenziano, L., Wang, Y., Welikala, N., Weller, J., Zamorani, G., Zoubian, J., Baldi, M., Bardelli, S., Camera, S., Farinelli, R., Medinaceli, E., Mei, S., Polenta, G., Romelli, E., Tenti, M., Vassallo, T., Zacchei, A., Zucca, E., Baccigalupi, C., Balaguera-Antolinez, A., Biviano, A., Borgani, S., Bozzo, E., Burigana, C., Cappi, A., Carvalho, C. S., Casas, S., Castignani, G., Colodro-Conde, C., Coupon, J., De La Torre, S., Fabricius, M., Farina, M., Ferreira, P. G., Flose-Reimberg, P., Fotopoulou, S., Galeotta, S., Ganga, K., Garcia-Bellido, J., Gaztanaga, E., Gozaliasl, G., Hook, I. M., Joachimi, B., Kansal, V., Kashlinsky, A., Keihanen, E., Kirkpatrick, C. C., Lindholm, V., Mainetti, G., Maino, D., Maoli, R., Martinelli, M., Martinet, N., Mccracken, H. J., Metcalf, R. B., Morgante, G., Morisset, N., Nightingale, J., Nucita, A., Patrizii, L., Potter, D., Renzi, A., Riccio, G., Sanchez, A. G., Sapone, D., Schirmer, M., Schultheis, M., Scottez, V., Sefusatti, E., Teyssier, R., Tutusaus, I., Valiviita, J., Viel, M., Whittaker, L., Knapen, J. H., Bretonniere H., Huertas-Company M., Boucaud A., Lanusse F., Jullo E., Merlin E., Tuccillo D., Castellano M., Brinchmann J., Conselice C.J., Dole H., Cabanac R., Courtois H.M., Castander F.J., Duc P.A., Fosalba P., Guinet D., Kruk S., Kuchner U., Serrano S., Soubrie E., Tramacere A., Wang L., Amara A., Auricchio N., Bender R., Bodendorf C., Bonino D., Branchini E., Brau-Nogue S., Brescia M., Capobianco V., Carbone C., Carretero J., Cavuoti S., Cimatti A., Cledassou R., Congedo G., Conversi L., Copin Y., Corcione L., Costille A., Cropper M., Da Silva A., Degaudenzi H., Douspis M., Dubath F., Duncan C.A.J., Dupac X., Dusini S., Farrens S., Ferriol S., Frailis M., Franceschi E., Fumana M., Garilli B., Gillard W., Gillis B., Giocoli C., Grazian A., Grupp F., Haugan S.V.H., Holmes W., Hormuth F., Hudelot P., Jahnke K., Kermiche S., Kiessling A., Kilbinger M., Kitching T., Kohley R., Kummel M., Kunz M., Kurki-Suonio H., Ligori S., Lilje P.B., Lloro I., Maiorano E., Mansutti O., Marggraf O., Markovic K., Marulli F., Massey R., Maurogordato S., Melchior M., Meneghetti M., Meylan G., Moresco M., Morin B., Moscardini L., Munari E., Nakajima R., Niemi S.M., Padilla C., Paltani S., Pasian F., Pedersen K., Pettorino V., Pires S., Poncet M., Popa L., Pozzetti L., Raison F., Rebolo R., Rhodes J., Roncarelli M., Rossetti E., Saglia R., Schneider P., Secroun A., Seidel G., Sirignano C., Sirri G., Stanco L., Starck J.-L., Tallada-Crespi P., Taylor A.N., Tereno I., Toledo-Moreo R., Torradeflot F., Valentijn E.A., Valenziano L., Wang Y., Welikala N., Weller J., Zamorani G., Zoubian J., Baldi M., Bardelli S., Camera S., Farinelli R., Medinaceli E., Mei S., Polenta G., Romelli E., Tenti M., Vassallo T., Zacchei A., Zucca E., Baccigalupi C., Balaguera-Antolinez A., Biviano A., Borgani S., Bozzo E., Burigana C., Cappi A., Carvalho C.S., Casas S., Castignani G., Colodro-Conde C., Coupon J., De La Torre S., Fabricius M., Farina M., Ferreira P.G., Flose-Reimberg P., Fotopoulou S., Galeotta S., Ganga K., Garcia-Bellido J., Gaztanaga E., Gozaliasl G., Hook I.M., Joachimi B., Kansal V., Kashlinsky A., Keihanen E., Kirkpatrick C.C., Lindholm V., Mainetti G., Maino D., Maoli R., Martinelli M., Martinet N., McCracken H.J., Metcalf R.B., Morgante G., Morisset N., Nightingale J., Nucita A., Patrizii L., Potter D., Renzi A., Riccio G., Sanchez A.G., Sapone D., Schirmer M., Schultheis M., Scottez V., Sefusatti E., Teyssier R., Tutusaus I., Valiviita J., Viel M., Whittaker L., Knapen J.H., Astronomy, Bretonniere, H, Huertas-Company, M, Boucaud, A, Lanusse, F, Jullo, E, Merlin, E, Tuccillo, D, Castellano, M, Brinchmann, J, Conselice, Cj, Dole, H, Cabanac, R, Courtois, Hm, Castander, Fj, Duc, Pa, Fosalba, P, Guinet, D, Kruk, S, Kuchner, U, Serrano, S, Soubrie, E, Tramacere, A, Wang, L, Amara, A, Auricchio, N, Bender, R, Bodendorf, C, Bonino, D, Branchini, E, Brau-Nogue, S, Brescia, M, Capobianco, V, Carbone, C, Carretero, J, Cavuoti, S, Cimatti, A, Cledassou, R, Congedo, G, Conversi, L, Copin, Y, Corcione, L, Costille, A, Cropper, M, Da Silva, A, Degaudenzi, H, Douspis, M, Dubath, F, Duncan, Caj, Dupac, X, Dusini, S, Farrens, S, Ferriol, S, Frailis, M, Franceschi, E, Fumana, M, Garilli, B, Gillard, W, Gillis, B, Giocoli, C, Grazian, A, Grupp, F, Haugan, Svh, Holmes, W, Hormuth, F, Hudelot, P, Jahnke, K, Kermiche, S, Kiessling, A, Kilbinger, M, Kitching, T, Kohley, R, Kummel, M, Kunz, M, Kurki-Suonio, H, Ligori, S, Lilje, Pb, Lloro, I, Maiorano, E, Mansutti, O, Marggraf, O, Markovic, K, Marulli, F, Massey, R, Maurogordato, S, Melchior, M, Meneghetti, M, Meylan, G, Moresco, M, Morin, B, Moscardini, L, Munari, E, Nakajima, R, Niemi, Sm, Padilla, C, Paltani, S, Pasian, F, Pedersen, K, Pettorino, V, Pires, S, Poncet, M, Popa, L, Pozzetti, L, Raison, F, Rebolo, R, Rhodes, J, Roncarelli, M, Rossetti, E, Saglia, R, Schneider, P, Secroun, A, Seidel, G, Sirignano, C, Sirri, G, Stanco, L, Starck, Jl, Tallada-Crespi, P, Taylor, An, Tereno, I, Toledo-Moreo, R, Torradeflot, F, Valentijn, Ea, Valenziano, L, Wang, Y, Welikala, N, Weller, J, Zamorani, G, Zoubian, J, Baldi, M, Bardelli, S, Camera, S, Farinelli, R, Medinaceli, E, Mei, S, Polenta, G, Romelli, E, Tenti, M, Vassallo, T, Zacchei, A, Zucca, E, Baccigalupi, C, Balaguera-Antolinez, A, Biviano, A, Borgani, S, Bozzo, E, Burigana, C, Cappi, A, Carvalho, C, Casas, S, Castignani, G, Colodro-Conde, C, Coupon, J, de la Torre, S, Fabricius, M, Farina, M, Ferreira, Pg, Flose-Reimberg, P, Fotopoulou, S, Galeotta, S, Ganga, K, Garcia-Bellido, J, Gaztanaga, E, Gozaliasl, G, Hook, Im, Joachimi, B, Kansal, V, Kashlinsky, A, Keihanen, E, Kirkpatrick, Cc, Lindholm, V, Mainetti, G, Maino, D, Maoli, R, Martinelli, M, Martinet, N, Mccracken, Hj, Metcalf, Rb, Morgante, G, Morisset, N, Nightingale, J, Nucita, A, Patrizii, L, Potter, D, Renzi, A, Riccio, G, Sanchez, Ag, Sapone, D, Schirmer, M, Schultheis, M, Scottez, V, Sefusatti, E, Teyssier, R, Tutusaus, I, Valiviita, J, Viel, M, Whittaker, L, Knapen, Jh, Department of Physics, Research Program in Systems Oncology, and Helsinki Institute of Physics

Subjects
INFORMATION, structure [Galaxies], FOS: Physical sciences, Techniques: image processing, Morphology (biology), observation [Cosmology], Astrophysics, Astrophysics::Cosmology and Extragalactic Astrophysics, Surveys, Cosmology: observation, 01 natural sciences, Settore FIS/05 - Astronomia e Astrofisica, DEPENDENCE, Galaxies: structure, galaxies, evolution, 0103 physical sciences, image processing [Techniques], structure, Survey, 010303 astronomy & astrophysics, Astrophysics::Galaxy Astrophysics, COSMOS, Physics, 010308 nuclear & particles physics, galaxie, Cosmology: observations, [PHYS.ASTR.GA] Physics [physics]/Astrophysics [astro-ph]/Galactic Astrophysics [astro-ph.GA], Galaxies: evolution, Física, Astronomy and Astrophysics, technique, 115 Astronomy, Space science, evolution [Galaxies], Astrophysics - Astrophysics of Galaxies, techniques, image processing, surveys, cosmology, observations, Galaxy, [PHYS.ASTR.GA]Physics [physics]/Astrophysics [astro-ph]/Galactic Astrophysics [astro-ph.GA], Space and Planetary Science, Astrophysics of Galaxies (astro-ph.GA), SIMULATION, Generative grammar
Abstract

Artículo escrito por un elevado número de autores, sólo se referencian el que aparece en primer lugar, los autores pertenecientes a la UAM y el nombre del grupo de colaboración, si lo hubiere., We present a machine learning framework to simulate realistic galaxies for the Euclid Survey, producing more complex and realistic galaxies than the analytical simulations currently used in Euclid. The proposed method combines a control on galaxy shape parameters offered by analytic models with realistic surface brightness distributions learned from real Hubble Space Telescope observations by deep generative models. We simulate a galaxy field of 0.4 deg2 as it will be seen by the Euclid visible imager VIS, and we show that galaxy structural parameters are recovered to an accuracy similar to that for pure analytic Sérsic profiles. Based on these simulations, we estimate that the Euclid Wide Survey (EWS) will be able to resolve the internal morphological structure of galaxies down to a surface brightness of 22.5 mag arcsec-2, and the Euclid Deep Survey (EDS) down to 24.9 mag arcsec-2. This corresponds to approximately 250 million galaxies at the end of the mission and a 50% complete sample for stellar masses above 1010.6 M (resp. 109.6 M) at a redshift z ∼ 0.5 for the EWS (resp. EDS). The approach presented in this work can contribute to improving the preparation of future high-precision cosmological imaging surveys by allowing simulations to incorporate more realistic galaxies

Published
2021

16. Ethical considerations for genetic research in low-income countries: perceptions of informed consent, data sharing, and expectations in Nicaragua.

Author

Delgado IS, Outterson A, Ramesh V, Amador Sanchez AG, Boza AC, Lopez-Pilarte D, Amador Velázquez JJ, Friedman DJ, Brooks DR, Scammell MK, and Wang C

Subjects
Humans, Nicaragua, Female, Male, Adult, Developing Countries, Middle Aged, Informed Consent ethics, Information Dissemination ethics, Genetic Research ethics
Abstract

Genetic research presents numerous ethical, legal, and social implications (ELSI), particularly when the research involves collaborations between investigators in high and low-income countries. Some ELSI issues are universal, and others are specific to context and culture. This study investigates perceptions of genetic research in Nicaragua, Central America, where local and U.S. based researchers have collaborated for over a decade. A total of 43 residents from northwestern Nicaragua, a region with high mortality rates attributed to chronic kidney disease of non-traditional causes (CKDnt), were interviewed, including research participants in ongoing studies (n = 36), health professionals (n = 3), labor leaders (n = 2), and family members of research participants (n = 2). Questions focused on informed consent, data-sharing, and post-study expectations. Audio recordings of interviews conducted in Spanish were transcribed and translated into English. English transcripts were coded and analyzed using NVivo 12 software. The lack of familiarity with terms in the consent form presented a barrier to participant comprehension of key elements of the genetic research study, raising concerns about the validity of informed consent. Research participants often viewed their participation as access to health care. Health professionals emphasized the importance of long-term partnerships between foreign-based researchers and local health institutions. Leaders and family members recommended that they be informed of research studies and allowed the opportunity to consent, as they felt the benefits and risks of research also apply to them. Our findings identified genetic research practices to be improved upon in order to be more responsive to the contextual realities of collaborators living in low-resource settings., (© 2023. The Author(s).)

Published
2024
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17. Targeting Relevant HDACs to Support the Survival of Cone Photoreceptors in Inherited Retinal Diseases: Identification of a Potent Pharmacological Tool with In Vitro and In Vivo Efficacy.

Author

Carullo G, Orsini N, Piano I, Pozzetti L, Papa A, Fontana A, Napoli D, Corsi F, Marco BD, Galante A, Marotta L, Panzeca G, O'Brien J, Sanchez AG, Doherty H, Mahon N, Clarke L, Contri C, Pasquini S, Gorelli B, Saponara S, Valoti M, Vincenzi F, Varani K, Ramunno A, Brogi S, Butini S, Gemma S, Kennedy BN, Gargini C, Strettoi E, and Campiani G

Subjects
Animals, Humans, Mice, Retinitis Pigmentosa metabolism, Retinitis Pigmentosa drug therapy, Retinitis Pigmentosa pathology, Histone Deacetylases metabolism, Histone Deacetylase 6 antagonists & inhibitors, Histone Deacetylase 6 metabolism, Cell Survival drug effects, Disease Models, Animal, Structure-Activity Relationship, Retinal Cone Photoreceptor Cells metabolism, Retinal Cone Photoreceptor Cells drug effects, Retinal Cone Photoreceptor Cells pathology, Zebrafish, Histone Deacetylase Inhibitors pharmacology, Histone Deacetylase Inhibitors chemistry, Histone Deacetylase Inhibitors therapeutic use
Abstract

Inherited retinal diseases, which include retinitis pigmentosa, are a family of genetic disorders characterized by gradual rod-cone degeneration and vision loss, without effective pharmacological treatments. Experimental approaches aim to delay disease progression, supporting cones' survival, crucial for human vision. Histone deacetylases (HDACs) mediate the activation of epigenetic and nonepigenetic pathways that modulate cone degeneration in RP mouse models. We developed new HDAC inhibitors ( 5a - p ), typified by a tetrahydro-γ-carboline scaffold, characterized by high HDAC6 inhibition potency with balanced physicochemical properties for in vivo studies. Compound 5d ( repistat , IC 50 HDAC6 = 6.32 nM) increased the levels of acetylated α-tubulin compared to histone H3 in ARPE-19 and 661W cells. 5d promoted vision rescue in the atp6v0e1 -/- zebrafish model of photoreceptor dysfunction. A single intravitreal injection of 5d in the rd10 mouse model of RP supported morphological and functional preservation of cone cells and maintenance of the retinal pigment epithelium array.

Published
2024
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18. Strathclyde minor groove binders (S-MGBs) with activity against Acanthamoeba castellanii.

Author

Mcgee LMC, Carpinteyro Sanchez AG, Perieteanu M, Eskandari K, Bian Y, Mackie L, Young L, Beveridge R, Suckling CJ, Roberts CW, and Scott FJ

Subjects
Humans, HEK293 Cells, Escherichia coli drug effects, Antiprotozoal Agents pharmacology, Trypanosoma brucei brucei drug effects, Staphylococcus aureus drug effects, Microbial Sensitivity Tests, Parasitic Sensitivity Tests, Cell Survival drug effects, Acanthamoeba castellanii drug effects
Abstract

Background: Acanthamoeba spp. is the causative agent of Acanthamoeba keratitis and granulomatous amoebic encephalitis. Strathclyde minor groove binders (S-MGBs) are a promising new class of anti-infective agent that have been shown to be effective against many infectious organisms., Objectives: To synthesize and evaluate the anti-Acanthamoeba activity of a panel of S-MGBs, and therefore determine the potential of this class for further development., Methods: A panel of 12 S-MGBs was synthesized and anti-Acanthamoeba activity was determined using an alamarBlue™-based trophocidal assay against Acanthamoeba castellanii. Cross-screening against Trypanosoma brucei brucei, Staphylococcus aureus and Escherichia coli was used to investigate selective potency. Cytotoxicity against HEK293 cells allowed for selective toxicity to be measured. DNA binding studies were carried out using native mass spectrometry and DNA thermal shift assays., Results and Discussion: S-MGB-241 has an IC50 of 6.6 µM against A. castellanii, comparable to the clinically used miltefosine (5.6 µM) and negligible activity against the other organisms. It was also found to have an IC50 > 100 µM against HEK293 cells, demonstrating low cytotoxicity. S-MGB-241 binds to DNA as a dimer, albeit weakly compared to other S-MGBs previously studied. This was confirmed by DNA thermal shift assay with a ΔTm = 1 ± 0.1°C., Conclusions: Together, these data provide confidence that S-MGBs can be further optimized to generate new, potent treatments for Acanthameoba spp. infections. In particular, S-MGB-241, has been identified as a 'hit' compound that is selectively active against A. castellanii, providing a starting point from which to begin optimization of DNA binding and potency., (© The Author(s) 2024. Published by Oxford University Press on behalf of British Society for Antimicrobial Chemotherapy.)

Published
2024
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19. SuRxgWell: study protocol for a randomized controlled trial of telemedicine-based digital cognitive behavioral intervention for high anxiety and depression among patients undergoing elective hip and knee arthroplasty surgery.

Author

Kaynar AM, Lin C, Sanchez AG, Lavage DR, Monroe A, Zharichenko N, Strassburger M, Saucier K, Groff YJ, Klatt BA, O'Malley MJ, Szigethy E, Wasan AD, and Chelly JE

Subjects
Humans, Quality of Life, Depression diagnosis, Depression etiology, Depression therapy, Analgesics, Opioid, Anxiety diagnosis, Anxiety etiology, Anxiety prevention & control, Anxiety Disorders, Pain, Postoperative diagnosis, Pain, Postoperative etiology, Pain, Postoperative prevention & control, Cognition, Treatment Outcome, Randomized Controlled Trials as Topic, Arthroplasty, Replacement, Knee adverse effects, Arthroplasty, Replacement, Knee psychology, Osteoarthritis, Hip, Telemedicine
Abstract

Background: Mood disorders (anxiety, depression), sleep disorders, and catastrophizing lead to increased post-operative pain perception, increase in postoperative opioid consumption, decreased engagement with physical activity, and increased resource utilization in surgical patients. Psychosocial disorders significantly affect postoperative outcome. Unfortunately, studies focused on perioperative psychological assessment and treatment are scarce. We propose to test whether digital cognitive behavioral intervention (dCBI) can help surgical patients. dCBI such as RxWell™ is a proven treatment for mood disorders in medical patients such as reducing depression in patients with inflammatory bowel disease. We hypothesize that RxWell™ will also be effective in surgical patients. This study aims to test whether RxWell™ can improve preoperative mood disorders and subsequently reduce postoperative pain and opioid requirement in patients scheduled for primary total hip and knee arthroplasty (THA, TKA). We named the trial as the SuRxgWell trial., Methods: This is a randomized, controlled trial that will enroll primary and unilateral THA or TKA patients with anxiety and/or depression symptoms before surgery to receive the SuRxgWell dCBI program and investigate its impact on postoperative outcomes including postoperative pain, anxiety, depression, sleep disorder, and catastrophizing. After signing an informed consent, subjects will be screened using the PROMIS questionnaires, and subjects with a T-score of ≥ 60 on the short Patient-Reported Outcomes Measurement Information System (PROMIS) 4a Anxiety and/or short PROMIS 4a Depression questionnaires will be randomized to either usual care (control group) or the cognitive behavioral intervention, RxWell™, plus usual care (intervention group). The control group will receive information on how to locate tools to address anxiety and depression, whereas the intervention group will have access to SuRxgWell 1 month prior to surgery and up to 3 months after surgery. The allocation will be 3:1 (intervention to control). Investigators will be blinded, but research coordinators approaching patients and research subjects will not. The primary outcome will be day of surgery anxiety or depression symptoms measured with the PROMIS Short Form v1.0 -Anxiety 4a/Depression and Generalized Anxiety Disorder Measure (GAD-7) and Patient Health Questionnaire (PHQ-8). Secondary end points include measuring other health-related quality of life outcomes including sleep disturbance, fatigue, ability to participate in social roles, pain interference, cognitive function, pain catastrophizing, and physical function. Other secondary outcomes include collecting data about preoperative and postoperative pain scores, and pain medication usage, and orthopedic functional recovery at baseline, day of surgery, and 1, 2, and 3 months after the surgery with the Pain Catastrophizing Scale, the Knee injury and Osteoarthritis Outcome Score (KOOS), and Hip injury and Osteoarthritis Outcome Score (HOOS). In addition, subjects will be asked to complete a GAD-7 and PHQ-8 questionnaires bi-weekly (via the RxWell™ app for the interventional group or REDCAP for the control group). Data about postsurgical complications, and resource utilization will also be recorded. We will also receive monthly reports measuring the usage and engagement of RxWell use for each participant randomized to that arm. The primary hypotheses will be assessed with intention-to-treat estimates, and differences in primary outcome will be tested using independent two sample t-tests. This trial is registered to the ClinicalTrials.gov database (NCT05658796) and supported by the DAPM, UPMC Health Plan, and the NIH., Discussion: Our trial will evaluate the feasibility of digital cognitive behavioral intervention as a perioperative tool to improve anxiety and depression before and after major orthopedic surgery in comparison to education. If digital cognitive behavioral intervention proves to be effective, this might have important clinical implications, reducing the incidence of chronic postsurgical pain and improving outcomes., (© 2023. The Author(s).)

Published
2023
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20. Should Advanced Friedreich's Ataxia Be a Contraindication for Heart Transplantation? A Case Report of a Successful Procedure in a 58-Year-Old Patient.

Author

Valero MJ, Muñoz-Blanco JL, Sanchez AG, Cuerpo G, Castrodeza J, Navas P, Sousa I, Villa A, Fernández-Avilés F, and Martínez-Sellés M

Abstract

The information on heart transplantation (HT) in patients with Friedreich's Ataxia (FA) is scarce, and the few published case reports are limited to young patients with mild neurological manifestations. We present the case of a 58-year-old patient with advanced FA (Scale for the Assessment and Rating of Ataxia [SARA] score 30/40), wheelchair-bound for the last 16 years and had urinary incontinence, dysarthria, and neurosensorial deafness. The patient was admitted for a refractory arrhythmic storm and had previous hypertrophic cardiomyopathy that evolved to dilated cardiomyopathy with severely reduced left ventricular ejection fraction and recurrent ventricular arrhythmias. A multidisciplinary team discussed the HT option. The patient was aware of the risks and benefits and considered worthy of the intervention, so he was listed for HT. After a successful surgical intervention, the patient had a long postoperative stay in ICU. He required a high dose of vasopressors, underwent hemofiltration for one month, suffered critical illness myopathy, had several respiratory infections and delayed tracheal extubation. Two and a half months after HT and almost five months at the hospital, the patient was successfully discharged. FA patients with severe heart conditions should be carefully evaluated by a multidisciplinary team to decide the candidacy for HT.

Published
2022
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21. Surface Disinfection using Ultraviolet Lightwith a Mobile Manipulation Robot.

Author

Sanchez AG and Smart WD

Abstract

Robots are being increasingly used in the fight against highly-infectious diseases such as Ebola, MERS, and SARS-COV-2. Many of the robots that are being used employ ultraviolet lights mounted on a mobile base to inactivate the pathogens. However, these lights are often mounted in a fixed configuration and do not provide adequate decontamination of horizontal surfaces, which can be a major source of cross-contamination. In the paper, we describe the design, implementation, and testing of an Ultraviolet Germicidal Irradiation (UVGI) system implemented on a mobile manipulation robot. A human supervisor designates a surface for disinfection, the robot autonomously plans and executes an end-effector trajectory to disinfect the surface to the required certainty, and then displays the results for the human supervisor to verify. We also provide some background information on UVGI and describe how we constructed and validated mathematical models of Ultraviolet (UV) radiation propagation and accumulation. Finally, we describe our implementation on a Fetch mobile manipulation platform, and discuss how the practicalities of implementation on a real robot affect our models.

Published
2021

22. Design and Implementation of a Germicidal UVC-LED Lamp.

Author

Juarez-Leon FA, Soriano-Sanchez AG, Rodriguez-Licea MA, and Perez-Pinal FJ

Abstract

In the last years, low pressure ozone UVC mercury germicidal lamps have been widely used to decontaminate air, surfaces, and water. This technology is mature, and it has been widely used during the pandemic as a measure against SARS-CoV-2 , the coronavirus that causes COVID-19; because the exposure of this virus to the wavelength wave of 254 nm has been proven to be an effective way to eliminate it. However, the Minamata Convention in 2013 decided to limit mercury lamps by 2020; therefore, the development of new technology devices based on UVC-LEDs (short-wave ultraviolet, light-emitting diodes) are receiving a lot of attention. Today, this technology is commercially available from 265 to 300 nm peak wavelengths, and recently up to 254 nm. Notwithstanding, due to the characteristics of these LEDs, arrangements with a precisely dosed power supply are regularly required to provide effective decontamination. Thus, this article reports the design and implementation of a power electronic converter for an array of 254 nm UVC-LEDs, which can be used to decontaminate from SARS-CoV-2 in a safe way., (This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 License. For more information, see https://creativecommons.org/licenses/by-nc-nd/4.0/.)

Published
2020
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23. Investigations of Sulfur Chemical Status with Synchrotron Micro Focused X-ray fluorescence and X-ray Absorption Spectroscopy.

Author

Castillo-Michel HA, Diaz-Sanchez AG, Martinez-Martinez A, and Hesse B

Subjects
Animals, Humans, Oxidation-Reduction, Proteins chemistry, Proteins radiation effects, Synchrotrons, Spectrometry, X-Ray Emission instrumentation, Sulfur chemistry, X-Ray Absorption Spectroscopy instrumentation
Abstract

Sulfur (S) is an essential macronutrient for all living organisms. A variety of organic and inorganic S species with oxidation states ranging from -2 to +6 exist. Today few spectroscopic and biochemical methods are used to investigate sulfur oxidation state and reactivity in biological samples. X-ray absorption near edge spectroscopy (XANES) is a very well suited spectroscopic technique to probe the oxidation state and the surrounding chemical environment of sulfur. Microspectroscopy beamlines, operating at almost all synchrotron facilities, allow the combination of XANES with X-ray fluorescence mapping (µXRF). Using this approach distribution maps of S in complex biological samples (intact parts of tissue, or individual cells) can be obtained using µXRF and its oxidation state can be probed in-situ (µXANES). Moreover, µXRF mapping at specific energies enables for chemical contrast of S at different oxidation states without the need of staining chemicals. This review introduces the basic concepts of synchrotron µXRF and µXANES and discusses the most recent applications in life science. Important methodological and technical issues will be discussed and results obtained in different complex biological samples will be presented.

Published
2016
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24. Osteoprotegerin Polymorphisms in a Mexican Population with Rheumatoid Arthritis and Generalized Osteoporosis: A Preliminary Report.

Author

Zavala-Cerna MG, Moran-Moguel MC, Cornejo-Toledo JA, Gonzalez-Montoya NG, Sanchez-Corona J, Salazar-Paramo M, Nava-Zavala AH, Aguilar-Chavez EA, Alcaraz-Lopez MF, Gonzalez-Sanchez AG, Gonzalez-Lopez L, and Gamez-Nava JI

Subjects
Adult, Aged, Alleles, Bone Density genetics, Case-Control Studies, Cross-Sectional Studies, Female, Genotype, Humans, Mexico, Middle Aged, RANK Ligand genetics, Receptor Activator of Nuclear Factor-kappa B genetics, Risk Factors, Young Adult, Arthritis, Rheumatoid genetics, Osteoporosis genetics, Osteoprotegerin genetics, Polymorphism, Single Nucleotide genetics
Abstract

Bone disease in rheumatoid arthritis (RA) is a complex phenomenon where genetic risk factors have been partially evaluated. The system formed by receptor activator for nuclear factor-κB (RANK), receptor activator for nuclear factor-κB ligand (RANKL), and osteoprotegerin (OPG): RANK/RANKL/OPG is a crucial molecular pathway for coupling between osteoblasts and osteoclasts, since OPG is able to inhibit osteoclast differentiation and activation. We aim to evaluate the association between SNPs C950T (rs2073617), C209T (rs3134069), T245G (rs3134070) in the TNFRSF11B (OPG) gene, and osteoporosis in RA. We included 81 women with RA and 52 healthy subjects in a cross-sectional study, genotyped them, and measured bone mineral density (BMD) at the lumbar spine and the femoral neck. Mean age in RA was 50 ± 12 with disease duration of 12 ± 8 years. According to BMD results, 23 (33.3%) were normal and 46 (66.7%) had osteopenia/osteoporosis. We found a higher prevalence of C allele for C950T SNP in RA. Polymorphisms C209T and T245G did not reach statistical significance in allele distribution. Further studies including patients from other regions of Latin America with a multicenter design to increase the sample size are required to confirm our findings and elucidate if C950T SNP could be associated with osteoporosis in RA.

Published
2015
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25. Recent advances on Ilex paraguariensis research: minireview.

Author

Bracesco N, Sanchez AG, Contreras V, Menini T, and Gugliucci A

Subjects
Animals, Anti-Inflammatory Agents pharmacology, Antimutagenic Agents pharmacology, Antioxidants pharmacology, Humans, Hypolipidemic Agents pharmacology, Plant Extracts pharmacology, Plant Leaves, Anti-Inflammatory Agents therapeutic use, Antimutagenic Agents therapeutic use, Antioxidants therapeutic use, Hypolipidemic Agents therapeutic use, Ilex paraguariensis chemistry, Phytotherapy, Plant Extracts therapeutic use
Abstract

Ilex paraguariensis dried and minced leaves are made into a brewed tea, prepared in a sui generis manner by large populations in South America, having evolved from a tea drunk by the Guarani ethnic group to a beverage that has a social and almost ritualistic role in some South American modern societies. It is used both as a source of caffeine, in lieu or in parallel with tea and coffee, but also as a therapeutic agent for its alleged pharmacological properties. Although with some exceptions, research on biomedical properties of this herb has had a late start and strongly lags behind the impressive amount of literature on green tea and coffee. However, in the past 15 years, there was a several-fold increase in the literature studying Ilex paraguariensis properties showing effects such as antioxidant properties in chemical models and ex vivo lipoprotein studies, vaso-dilating and lipid reduction properties, antimutagenic effects, controversial association with oropharyngeal cancer, anti-glycation effects and weight reduction properties. Lately, promising results from human intervention studies have surfaced and the literature offers several developments on this area. The aim of this review is to provide a concise summary of the research published in the past three years, with an emphasis on translational studies, inflammation and lipid metabolism. Ilex paraguariensis reduces LDL-cholesterol levels in humans with Ilex paraguariensis dyslipoproteinemia and the effect is synergic with that of statins. Plasma antioxidant capacity as well as expression of antioxidant enzymes is positively modulated by intervention with Ilex paraguariensis in human cohorts. A review on the evidence implicating Ilex paraguariensis heavy consumption with some neoplasias show data that are inconclusive but indicate that contamination with alkylating agents during the drying process of the leaves should be avoided. On the other hand, several new studies confirm the antimutagenic effects of Ilex paraguariensis in different models, from DNA double breaks in cell culture models to mice studies. Novel interesting work has emerged showing significant effect on weight reduction both in mice and in rat models. Some mechanisms involved are inhibition of pancreatic lipase, activation of AMPK and uncoupling of electron transport. Intervention studies in animals have provided strong evidence of anti-inflammatory effects of Ilex paraguariensis, notably protecting cigarette-induced lung inflammation acting on macrophage migration and inactivating matrix-metalloproteinase. Research on the effects of Ilex paraguariensis in health and disease has confirmed its antioxidant, anti-inflammatory, antimutagenic and lipid-lowering activities. Although we are still waiting for the double-blind, randomized prospective clinical trial, the evidence seems to provide support for beneficial effects of mate drinking on chronic diseases with inflammatory component and lipid metabolism disorders., (Copyright © 2010 Elsevier Ireland Ltd. All rights reserved.)

Published
2011
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26. Lobular carcinoma of the breast in a patient with Klinefelter's syndrome. A case with bilateral, synchronous, histologically different breast tumors.

Author

Sanchez AG, Villanueva AG, and Redondo C

Subjects
Breast Neoplasms genetics, Carcinoma in Situ genetics, Carcinoma, Intraductal, Noninfiltrating genetics, Humans, Karyotyping, Male, Mastectomy, Middle Aged, Phenotype, Receptors, Estrogen analysis, Receptors, Progesterone analysis, Breast Neoplasms complications, Carcinoma in Situ complications, Carcinoma, Intraductal, Noninfiltrating complications, Klinefelter Syndrome complications, Neoplasms, Multiple Primary
Abstract

A case of bilateral breast cancer in a patient with a Klinefelter mosaic syndrome is presented. The tumor in the left breast was an infiltrating lobular carcinoma with characteristic in situ component. To the knowledge of the authors, this is the first case in the English literature of lobular carcinoma of the breast in a phenotypic man. In fact, it was the pathologic diagnosis which led to the study of the chromosomal abnormality.

Published
1986
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