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1. In Vitro Antifungal Activity of Ibrexafungerp (SCY-078) Against Contemporary Blood Isolates From Medically Relevant Species of Candida: A European Study

Author

Farmacología, Inmunología, microbiología y parasitología, Farmakologia, Immunologia, mikrobiologia eta parasitologia, Quindós Andrés, Guillermo, Miranda Cadena, Katherine, San Millán Gutiérrez, Rosario María, Borroto Esoda, Katyna, Cantón, Emilia, Linares Sicilia, María José, Hamprecht, Axel Georg, Montesinos, Isabel, Tortorano, Anna Maria, Prigitano, Anna, Vidal García, Matxalen, Marcos Arias, Cristina, Guridi Cortaberria, Andrea, Sánchez Reus, Ferrán, Machuca Bárcena, Jesús, Rodríguez Iglesias, Manuel Antonio, Martín Mazuelos, Estrella, Castro Méndez, Carmen, López Soria, Leyre, Ruiz Gaitán, Alba, Fernández Rivero, Marcelo, Lorenzo, Damaris, Capilla, Javier, Rezusta, Antonio, Pemán, Javier, Guarro, Josep, Pereira, Joana, Célia, Pais, Romeo, Orazio, Ezpeleta Lobato, Guillermo, Jaureguizar Albonigamayor, Nerea, Angulo, David, Eraso Barrio, María Elena, Farmacología, Inmunología, microbiología y parasitología, Farmakologia, Immunologia, mikrobiologia eta parasitologia, Quindós Andrés, Guillermo, Miranda Cadena, Katherine, San Millán Gutiérrez, Rosario María, Borroto Esoda, Katyna, Cantón, Emilia, Linares Sicilia, María José, Hamprecht, Axel Georg, Montesinos, Isabel, Tortorano, Anna Maria, Prigitano, Anna, Vidal García, Matxalen, Marcos Arias, Cristina, Guridi Cortaberria, Andrea, Sánchez Reus, Ferrán, Machuca Bárcena, Jesús, Rodríguez Iglesias, Manuel Antonio, Martín Mazuelos, Estrella, Castro Méndez, Carmen, López Soria, Leyre, Ruiz Gaitán, Alba, Fernández Rivero, Marcelo, Lorenzo, Damaris, Capilla, Javier, Rezusta, Antonio, Pemán, Javier, Guarro, Josep, Pereira, Joana, Célia, Pais, Romeo, Orazio, Ezpeleta Lobato, Guillermo, Jaureguizar Albonigamayor, Nerea, Angulo, David, and Eraso Barrio, María Elena

Abstract

BackgroundIbrexafungerp (SCY-078) is the newest oral and intravenous antifungal drug with broad activity, currently undergoing clinical trials for invasive candidiasis. ObjectiveThe aim of this study was to assess the in vitro activity of ibrexafungerp and comparators against a collection of 434 European blood isolates of Candida. MethodsIbrexafungerp, caspofungin, fluconazole, and micafungin minimum inhibitory concentrations (MICs) were collected from 12 European laboratories for 434 blood isolates, including 163 Candida albicans, 108 Candida parapsilosis, 60 Candida glabrata, 40 Candida tropicalis, 29 Candida krusei, 20 Candida orthopsilosis, 6 Candida guilliermondii, 2 Candida famata, 2 Candida lusitaniae, and 1 isolate each of Candida bracarensis, Candida catenulata, Candida dubliniensis, and Candida kefyr. MICs were determined by the EUCAST broth microdilution method, and isolates were classified according to recommended clinical breakpoints and epidemiological cutoffs. Additionally, 22 Candida auris from different clinical specimens were evaluated. ResultsIbrexafungerp MICs ranged from 0.016 to >= 8 mg/L. The lowest ibrexafungerp MICs were observed for C. albicans (geometric MIC 0.062 mg/L, MIC range 0.016-0.5 mg/L) and the highest ibrexafungerp MICs were observed for C. tropicalis (geometric MIC 0.517 mg/L, MIC range 0.06->= 8 mg/L). Modal MICs/MIC(50)s (mg/L) against Candida spp. were 0.125/0.06 for C. albicans, 0.5/0.5 for C. parapsilosis, 0.25/0.25 for C. glabrata, 0.5/0.5 for C. tropicalis, 1/1 for C. krusei, 4/2 for C. orthopsilosis, and 0.5/0.5 for C. auris. Ibrexafungerp showed activity against fluconazole- and echinocandin-resistant isolates. If adopting wild-type upper limits, a non-wild-type phenotype for ibrexafungerp was only observed for 16/434 (3.7%) isolates: 11 (4.6%) C. parapsilosis, 4 (5%) C. glabrata, and 1 (2.5%) C. tropicalis. ConclusionIbrexafungerp showed a potent in vitro activity against Candida.

Published
2022

2. In Vitro Antifungal Activity of Ibrexafungerp (SCY-078) Against Contemporary Blood Isolates From Medically Relevant Species of Candida: A European Study

Author

Farmacología, Inmunología, microbiología y parasitología, Farmakologia, Immunologia, mikrobiologia eta parasitologia, Quindós Andrés, Guillermo, Miranda Cadena, Katherine, San Millán Gutiérrez, Rosario María, Borroto Esoda, Katyna, Cantón, Emilia, Linares Sicilia, María José, Hamprecht, Axel Georg, Montesinos, Isabel, Tortorano, Anna Maria, Prigitano, Anna, Vidal García, Matxalen, Marcos Arias, Cristina, Guridi Cortaberria, Andrea, Sánchez Reus, Ferrán, Machuca Bárcena, Jesús, Rodríguez Iglesias, Manuel Antonio, Martín Mazuelos, Estrella, Castro Méndez, Carmen, López Soria, Leyre, Ruiz Gaitán, Alba, Fernández Rivero, Marcelo, Lorenzo, Damaris, Capilla, Javier, Rezusta, Antonio, Pemán, Javier, Guarro, Josep, Pereira, Joana, Célia, Pais, Romeo, Orazio, Ezpeleta Lobato, Guillermo, Jauregizar Albonigamayor, Nerea, Angulo, David, Eraso Barrio, María Elena, Farmacología, Inmunología, microbiología y parasitología, Farmakologia, Immunologia, mikrobiologia eta parasitologia, Quindós Andrés, Guillermo, Miranda Cadena, Katherine, San Millán Gutiérrez, Rosario María, Borroto Esoda, Katyna, Cantón, Emilia, Linares Sicilia, María José, Hamprecht, Axel Georg, Montesinos, Isabel, Tortorano, Anna Maria, Prigitano, Anna, Vidal García, Matxalen, Marcos Arias, Cristina, Guridi Cortaberria, Andrea, Sánchez Reus, Ferrán, Machuca Bárcena, Jesús, Rodríguez Iglesias, Manuel Antonio, Martín Mazuelos, Estrella, Castro Méndez, Carmen, López Soria, Leyre, Ruiz Gaitán, Alba, Fernández Rivero, Marcelo, Lorenzo, Damaris, Capilla, Javier, Rezusta, Antonio, Pemán, Javier, Guarro, Josep, Pereira, Joana, Célia, Pais, Romeo, Orazio, Ezpeleta Lobato, Guillermo, Jauregizar Albonigamayor, Nerea, Angulo, David, and Eraso Barrio, María Elena

Abstract

BackgroundIbrexafungerp (SCY-078) is the newest oral and intravenous antifungal drug with broad activity, currently undergoing clinical trials for invasive candidiasis. ObjectiveThe aim of this study was to assess the in vitro activity of ibrexafungerp and comparators against a collection of 434 European blood isolates of Candida. MethodsIbrexafungerp, caspofungin, fluconazole, and micafungin minimum inhibitory concentrations (MICs) were collected from 12 European laboratories for 434 blood isolates, including 163 Candida albicans, 108 Candida parapsilosis, 60 Candida glabrata, 40 Candida tropicalis, 29 Candida krusei, 20 Candida orthopsilosis, 6 Candida guilliermondii, 2 Candida famata, 2 Candida lusitaniae, and 1 isolate each of Candida bracarensis, Candida catenulata, Candida dubliniensis, and Candida kefyr. MICs were determined by the EUCAST broth microdilution method, and isolates were classified according to recommended clinical breakpoints and epidemiological cutoffs. Additionally, 22 Candida auris from different clinical specimens were evaluated. ResultsIbrexafungerp MICs ranged from 0.016 to >= 8 mg/L. The lowest ibrexafungerp MICs were observed for C. albicans (geometric MIC 0.062 mg/L, MIC range 0.016-0.5 mg/L) and the highest ibrexafungerp MICs were observed for C. tropicalis (geometric MIC 0.517 mg/L, MIC range 0.06->= 8 mg/L). Modal MICs/MIC(50)s (mg/L) against Candida spp. were 0.125/0.06 for C. albicans, 0.5/0.5 for C. parapsilosis, 0.25/0.25 for C. glabrata, 0.5/0.5 for C. tropicalis, 1/1 for C. krusei, 4/2 for C. orthopsilosis, and 0.5/0.5 for C. auris. Ibrexafungerp showed activity against fluconazole- and echinocandin-resistant isolates. If adopting wild-type upper limits, a non-wild-type phenotype for ibrexafungerp was only observed for 16/434 (3.7%) isolates: 11 (4.6%) C. parapsilosis, 4 (5%) C. glabrata, and 1 (2.5%) C. tropicalis. ConclusionIbrexafungerp showed a potent in vitro activity against Candida.

Published
2022

3. A Mucoralean White Collar-1 Photoreceptor Controls Virulence by Regulating an Intricate Gene Network during Host Interactions

Author

Universitat Rovira i Virgili, Perez-Arques, Carlos; Navarro-Mendoza, Maria Isabel; Murcia, Laura; Lax, Carlos; Sanchis, Marta; Capilla, Javier; Navarro, Eusebio; Garre, Victoriano; Nicolas, Francisco Esteban, Universitat Rovira i Virgili, and Perez-Arques, Carlos; Navarro-Mendoza, Maria Isabel; Murcia, Laura; Lax, Carlos; Sanchis, Marta; Capilla, Javier; Navarro, Eusebio; Garre, Victoriano; Nicolas, Francisco Esteban

Abstract

Mucolares are an ancient group of fungi encompassing the causal agents for the lethal infection mucormycosis. The high lethality rates, the emerging character of this disease, and the broad antifungal resistance of its causal agents are mucormycosis features that are alarming clinicians and researchers. Thus, the research field around mucormycosis is currently focused on finding specific weaknesses and targets in Mucorales for developing new treatments. In this work, we tested the role of the white-collar genes family in the virulence potential of Mucor lusitanicus. Study of the three genes of this family, mcwc-1a, mcwc-1b, and mcwc-1c, resulted in a marked functional specialization, as only mcwc-1a was essential to maintain the virulence potential of M. lusitanicus. The traditional role of wc-1 genes regulating light-dependent responses is a thoroughly studied field, whereas their role in virulence remains uncharacterized. In this work, we investigated the mechanism involving mcwc-1a in virulence from an integrated transcriptomic and functional approach during the host-pathogen interaction. Our results revealed mcwc-1a as a master regulator controlling an extensive gene network. Further dissection of this gene network clustering its components by type of regulation and functional criteria disclosed a multifunctional mechanism depending on diverse pathways. In the absence of phagocytic cells, mcwc-1a controlled pathways related to cell motility and the cytoskeleton that could be associated with the essential tropism during tissue invasion. After phagocytosis, several oxidative response pathways dependent on mcwc-1a were activated during the germination of M. lusitanicus spores inside phagocytic cells, which is the first stage of the infection. The third relevant group o

Published
2021

4. Antifungal and Antiparasitic Drug Delivery

Author

Torrado Durán, Juan José, Serrano López, Dolores Remedios, Capilla, Javier, Torrado Durán, Juan José, Serrano López, Dolores Remedios, and Capilla, Javier

Abstract

Fungal and parasitic diseases affect more than a billion people across the globe, one-sixth of the world’s population, mostly located in developing countries. The lack of effective and safer treatments combined with a deficient diagnosis lead to serious chronic illness or even death. There is a mismatch between the rate of drug resistance and the development of new medicines. Formulation of antifungal and antiparasitic drugs adapted to different administration routes is challenging, bearing in mind their poor water solubility, which limits their bioavailability and efficacy. Hence, there is an unmet clinical need to develop vaccines and novel formulations and drug delivery strategies that can improve the bioavailability and therapeutic effect by enhancing their dissolution, increasing their chemical potency, stabilising the drug and targeting high concentration of drug to the infection sites. This Editorial regards the ten research contributions presented in the Special Issue “Antifungal and Antiparasitic Drug Delivery”., Depto. de Farmacia Galénica y Tecnología Alimentaria, Fac. de Farmacia, TRUE, pub

Published
2020

5. Cu transporter protein CrpF protects against Cu-induced toxicity inFusarium oxysporum

Author

Universitat Rovira i Virgili, Lorenzo-Gutierrez, Damaris; Gomez-Gil, Lucia; Guarro, Josep; Roncero, M. Isabel G.; Capilla, Javier; Lopez-Fernandez, Loida, Universitat Rovira i Virgili, and Lorenzo-Gutierrez, Damaris; Gomez-Gil, Lucia; Guarro, Josep; Roncero, M. Isabel G.; Capilla, Javier; Lopez-Fernandez, Loida

Abstract

Cu is an essential trace element for cell growth and proliferation. However, excess of Cu accumulation leads to cellular toxicity. Thus, precise and tight regulation of Cu homeostasis processes, including transport, delivery, storage, detoxification, and efflux machineries, is required. Moreover, the maintenance of Cu homeostasis is critical for the survival and virulence of fungal pathogens. Cu homeostasis has been extensively studied in mammals, bacteria, and yeast, but it has not yet been well documented in filamentous fungi. In the present work, we investigated Cu tolerance in the filamentous fungusFusarium oxysporumby analysing the Cu transporter coding genecrpF, previously studied inAspergillus fumigatus. The expression studies demonstrated thatcrpFis upregulated in the presence of Cu and its deletion leads to severe sensitivity to low levels of CuSO(4)inF. oxysporum. Targeted deletion ofcrpFdid not significantly alter the resistance of the fungus to macrophage killing, nor its pathogenic behaviour on the tomato plants. However, the targeted deletion mutant Delta crpFshowed increased virulence in a murine model of systemic infection compared to wild-type strain (wt).

Published
2020

6. Increased Efficacy of Oral Fixed-Dose Combination of Amphotericin B and AHCC® Natural Adjuvant against Aspergillosis

Author

Pérez-Cantero, Alba, Serrano López, Dolores Remedios, Navarro Rodríguez, Patricia, Schätzlein, Andreas G., Uchegbu, Ijeoma F., Torrado Durán, Juan José, Capilla, Javier, Pérez-Cantero, Alba, Serrano López, Dolores Remedios, Navarro Rodríguez, Patricia, Schätzlein, Andreas G., Uchegbu, Ijeoma F., Torrado Durán, Juan José, and Capilla, Javier

Abstract

Invasive pulmonary aspergillosis represents one of the most serious fungal infections among immunocompromised patients. In this study, we aimed to analyze the in vivo e_cacy of prophylactic oral amphotericin B (AMB) encapsulated in modified chitosan-nanoparticles (Nanomerics’ Molecular Envelope Technology (MET)) supplemented with a standardized extract of cultured Lentinula edodes mycelia (AHCC®) in a murine model of pulmonary aspergillosis. We determined fungal burden and survival of mice and additionally, we carried out a cytokine analysis in an attempt to understand the immunomodulation of the extract. Our results evidenced equivalent e_cacy between orally administered AMB-MET and the intravenous liposomal AMB marketed formulation. Addition of the AHCC® supplement significantly improved e_cacy in terms of burden reduction and survival increase of both oral and intravenous AMB therapies compared to the untreated control group. Moreover, a protective e_ect of the extract was observed in terms of weight loss. Regarding the cytokine profiles, the Th1 immune response was stimulated in treated animals when compared to the control group. This response was marked by an enhancement in the MCP-1, GM-CSF, VEGF, RANTES and IL-17 levels and a decrease in the IL-6, a biomarker related to the severity of the infection., Universidad Complutense de Madrid, UCL School of Pharmacy, University of London, Generalitat de Catalunya, Depto. de Farmacia Galénica y Tecnología Alimentaria, Fac. de Farmacia, TRUE, pub

Published
2019

8. Scedosporium and Lomentospora: An updated overview of underrated opportunists

Author

Ramirez-Garcia, Andoni, Pellon, Aize, Rementeria, Aitor, Buldain, Idoia, Barreto-Bergter, Eliana, Rollin-Pinheiro, Rodrigo, De Meirelles, Jardel Vieira, Xisto, Mariana Ingrid D.S., Ranque, Stephane, Havlicek, Vladimir, Vandeputte, Patrick, Govic, Yohann Le, Bouchara, Jean Philippe, Giraud, Sandrine, Chen, Sharon, Rainer, Johannes, Alastruey-Izquierdo, Ana, Martin-Gomez, Maria Teresa, López-Soria, Leyre M., Peman, Javier, Schwarz, Carsten, Bernhardt, Anne, Tintelnot, Kathrin, Capilla, Javier, Martin-Vicente, Adela, Cano-Lira, Jose, Nagl, Markus, Lackner, Michaela, Irinyi, Laszlo, Meyer, Wieland, De Hoog, Sybren, Hernando, Fernando L., Ramirez-Garcia, Andoni, Pellon, Aize, Rementeria, Aitor, Buldain, Idoia, Barreto-Bergter, Eliana, Rollin-Pinheiro, Rodrigo, De Meirelles, Jardel Vieira, Xisto, Mariana Ingrid D.S., Ranque, Stephane, Havlicek, Vladimir, Vandeputte, Patrick, Govic, Yohann Le, Bouchara, Jean Philippe, Giraud, Sandrine, Chen, Sharon, Rainer, Johannes, Alastruey-Izquierdo, Ana, Martin-Gomez, Maria Teresa, López-Soria, Leyre M., Peman, Javier, Schwarz, Carsten, Bernhardt, Anne, Tintelnot, Kathrin, Capilla, Javier, Martin-Vicente, Adela, Cano-Lira, Jose, Nagl, Markus, Lackner, Michaela, Irinyi, Laszlo, Meyer, Wieland, De Hoog, Sybren, and Hernando, Fernando L.

Abstract

Species of Scedosporium and Lomentospora are considered as emerging opportunists, affecting immunosuppressed and otherwise debilitated patients, although classically they are known from causing trauma-associated infections in healthy individuals. Clinical manifestations range from local infection to pulmonary colonization and severe invasive disease, in which mortality rates may be over 80%. These unacceptably high rates are due to the clinical status of patients, diagnostic difficulties, and to intrinsic antifungal resistance of these fungi. In consequence, several consortia have been founded to increase research efforts on these orphan fungi. The current review presents recent findings and summarizes the most relevant points, including the Scedosporium/Lomentospora taxonomy, environmental distribution, epidemiology, pathology, virulence factors, immunology, diagnostic methods, and therapeutic strategies.

Published
2018

9. Scedosporium and Lomentospora: An updated overview of underrated opportunists

Author

Ramirez-Garcia, Andoni, Pellon, Aize, Rementeria, Aitor, Buldain, Idoia, Barreto-Bergter, Eliana, Rollin-Pinheiro, Rodrigo, De Meirelles, Jardel Vieira, Xisto, Mariana Ingrid D.S., Ranque, Stephane, Havlicek, Vladimir, Vandeputte, Patrick, Govic, Yohann Le, Bouchara, Jean Philippe, Giraud, Sandrine, Chen, Sharon, Rainer, Johannes, Alastruey-Izquierdo, Ana, Martin-Gomez, Maria Teresa, López-Soria, Leyre M., Peman, Javier, Schwarz, Carsten, Bernhardt, Anne, Tintelnot, Kathrin, Capilla, Javier, Martin-Vicente, Adela, Cano-Lira, Jose, Nagl, Markus, Lackner, Michaela, Irinyi, Laszlo, Meyer, Wieland, De Hoog, Sybren, Hernando, Fernando L., Ramirez-Garcia, Andoni, Pellon, Aize, Rementeria, Aitor, Buldain, Idoia, Barreto-Bergter, Eliana, Rollin-Pinheiro, Rodrigo, De Meirelles, Jardel Vieira, Xisto, Mariana Ingrid D.S., Ranque, Stephane, Havlicek, Vladimir, Vandeputte, Patrick, Govic, Yohann Le, Bouchara, Jean Philippe, Giraud, Sandrine, Chen, Sharon, Rainer, Johannes, Alastruey-Izquierdo, Ana, Martin-Gomez, Maria Teresa, López-Soria, Leyre M., Peman, Javier, Schwarz, Carsten, Bernhardt, Anne, Tintelnot, Kathrin, Capilla, Javier, Martin-Vicente, Adela, Cano-Lira, Jose, Nagl, Markus, Lackner, Michaela, Irinyi, Laszlo, Meyer, Wieland, De Hoog, Sybren, and Hernando, Fernando L.

Abstract

Species of Scedosporium and Lomentospora are considered as emerging opportunists, affecting immunosuppressed and otherwise debilitated patients, although classically they are known from causing trauma-associated infections in healthy individuals. Clinical manifestations range from local infection to pulmonary colonization and severe invasive disease, in which mortality rates may be over 80%. These unacceptably high rates are due to the clinical status of patients, diagnostic difficulties, and to intrinsic antifungal resistance of these fungi. In consequence, several consortia have been founded to increase research efforts on these orphan fungi. The current review presents recent findings and summarizes the most relevant points, including the Scedosporium/Lomentospora taxonomy, environmental distribution, epidemiology, pathology, virulence factors, immunology, diagnostic methods, and therapeutic strategies.

Published
2018

10. Scedosporium and Lomentospora: an updated overview of underrated opportunists

Author

Inmunología, microbiología y parasitología, Immunologia, mikrobiologia eta parasitologia, Ramírez García, Andoni, Pellón Rodríguez, Aize, Rementeria Ruiz, Aitor Domingo, Buldain Garriz, Idoia, Barreto-Bergter, Eliana, Rollin-Pinheiro, Rodrigo, Vieira de Meirelles, Jardel, Xisto, Mariana Ingrid D. S., Ranque, Stephane, Havlicek, Vladimir, Vandeputte, Patrick, Le Govic, Yohann, Bouchara, Jean Philippe, Giraud, Sandrine, Chen, Sharon, Rainer, Johannes, Alastruey-Izquierdo, Ana, Martín Gómez, María Teresa, López Soria, Leyre, Pemán, Javier, Schwarz, Carsten, Bernhardt, Anne, Tintelnot, Kathrin, Capilla, Javier, Martin-Vicente, Adela, Cano-Lira, Jose, Nagl, Markus, Lackner, Michaela, Irinyi, Laszlo, Meyer, Wieland, de Hoog, Sybren, Hernando, Fernando Luis, Inmunología, microbiología y parasitología, Immunologia, mikrobiologia eta parasitologia, Ramírez García, Andoni, Pellón Rodríguez, Aize, Rementeria Ruiz, Aitor Domingo, Buldain Garriz, Idoia, Barreto-Bergter, Eliana, Rollin-Pinheiro, Rodrigo, Vieira de Meirelles, Jardel, Xisto, Mariana Ingrid D. S., Ranque, Stephane, Havlicek, Vladimir, Vandeputte, Patrick, Le Govic, Yohann, Bouchara, Jean Philippe, Giraud, Sandrine, Chen, Sharon, Rainer, Johannes, Alastruey-Izquierdo, Ana, Martín Gómez, María Teresa, López Soria, Leyre, Pemán, Javier, Schwarz, Carsten, Bernhardt, Anne, Tintelnot, Kathrin, Capilla, Javier, Martin-Vicente, Adela, Cano-Lira, Jose, Nagl, Markus, Lackner, Michaela, Irinyi, Laszlo, Meyer, Wieland, de Hoog, Sybren, and Hernando, Fernando Luis

Abstract

Species of Scedosporium and Lomentospora are considered as emerging opportunists, affecting immunosuppressed and otherwise debilitated patients, although classically they are known from causing trauma-associated infections in healthy individuals. Clinical manifestations range from local infection to pulmonary colonization and severe invasive disease, in which mortality rates may be over 80%. These unacceptably high rates are due to the clinical status of patients, diagnostic difficulties, and to intrinsic antifungal resistance of these fungi. In consequence, several consortia have been founded to increase research efforts on these orphan fungi. The current review presents recent findings and summarizes the most relevant points, including the Scedosporium/Lomentospora taxonomy, environmental distribution, epidemiology, pathology, virulence factors, immunology, diagnostic methods, and therapeutic strategies.

Published
2018

11. Multicenter, International Study of MIC/MEC Distributions for Definition of Epidemiological Cutoff Values for Sporothrix Species Identified by Molecular Methods

Author

Espinel Ingroff, A., Abreu, D. P. B., Almeida Paes, R., Brilhante, R. S. N., Chakrabarti, A., Chowdhary, A., Hagen, F., Córdoba, S., González González, Gloria María, Govender, N. P., Guarro, Josep, Johnson, E. M., Kidd, S. E., Pereira, S. A., Rodrigues, A. M., Rozental, S., Szeszs, M. W., Ballesté Alaniz, R., Bonifaz, Alexandro, Bonfietti, L. X., Borba Santos, L. P., Capilla, Javier, Colombo, A. L., Dolande, M., Isla, M. G., Melhem, M. S. C., Mesa Arango, A. C., Oliveira, M. M. E., Panizo, M. M., Pires de Camargo, Z., Zancope Oliveira, R. M., Meis, J. F., Turnidge, J., Espinel Ingroff, A., Abreu, D. P. B., Almeida Paes, R., Brilhante, R. S. N., Chakrabarti, A., Chowdhary, A., Hagen, F., Córdoba, S., González González, Gloria María, Govender, N. P., Guarro, Josep, Johnson, E. M., Kidd, S. E., Pereira, S. A., Rodrigues, A. M., Rozental, S., Szeszs, M. W., Ballesté Alaniz, R., Bonifaz, Alexandro, Bonfietti, L. X., Borba Santos, L. P., Capilla, Javier, Colombo, A. L., Dolande, M., Isla, M. G., Melhem, M. S. C., Mesa Arango, A. C., Oliveira, M. M. E., Panizo, M. M., Pires de Camargo, Z., Zancope Oliveira, R. M., Meis, J. F., and Turnidge, J.

Abstract

Clinical and Laboratory Standards Institute (CLSI) conditions for testing the susceptibilities of pathogenic Sporothrix species to antifungal agents are based on a collaborative study that evaluated five clinically relevant isolates of Sporothrix schenckii sensu lato and some antifungal agents. With the advent of molecular identification, there are two basic needs: to confirm the suitability of these testing conditions for all agents and Sporothrix species and to establish species-specific epidemiologic cutoff values (ECVs) or breakpoints (BPs) for the species. We collected available CLSI MICs/minimal effective concentrations (MECs) of amphotericin B, five triazoles, terbinafine, flucytosine, and caspofungin for 301 Sporothrix schenckii sensu stricto, 486 S. brasiliensis, 75S. globosa, and 13 S. mexicana molecularly identified isolates. Data were obtained in 17 independent laboratories (Australia, Europe, India, South Africa, and South and North America) using conidial inoculum suspensions and 48 to 72 h of incubation at 35°C. Sufficient and suitable data (modal MICs within 2-fold concentrations) allowed the proposal of the following ECVs for S. schenckii and S. brasiliensis, respectively: amphotericin B, 4 and 4 g/ml; itraconazole, 2 and 2 g/ml; posaconazole, 2 and 2 g/ml; and voriconazole, 64 and 32 g/ml. Ketoconazole and terbinafine ECVs for S. brasiliensis were 2 and 0.12 g/ml, respectively. Insufficient or unsuitable data precluded the calculation of ketoconazole and terbinafine (or any other antifungal agent) ECVs for S. schenckii, as well as ECVs for S. globosa and S. mexicana. These ECVs could aid the clinician in identifying potentially resistant isolates (non-wild type) less likely to respond to therapy.

Published
2017

12. Multicenter, International Study of MIC/MEC Distributions for Definition of Epidemiological Cutoff Values for Sporothrix Species Identified by Molecular Methods

Author

Espinel Ingroff, A., Abreu, D. P. B., Almeida Paes, R., Brilhante, R. S. N., Chakrabarti, A., Chowdhary, A., Hagen, F., Córdoba, S., González González, Gloria María, Govender, N. P., Guarro, Josep, Johnson, E. M., Kidd, S. E., Pereira, S. A., Rodrigues, A. M., Rozental, S., Szeszs, M. W., Ballesté Alaniz, R., Bonifaz, Alexandro, Bonfietti, L. X., Borba Santos, L. P., Capilla, Javier, Colombo, A. L., Dolande, M., Isla, M. G., Melhem, M. S. C., Mesa Arango, A. C., Oliveira, M. M. E., Panizo, M. M., Pires de Camargo, Z., Zancope Oliveira, R. M., Meis, J. F., Turnidge, J., Espinel Ingroff, A., Abreu, D. P. B., Almeida Paes, R., Brilhante, R. S. N., Chakrabarti, A., Chowdhary, A., Hagen, F., Córdoba, S., González González, Gloria María, Govender, N. P., Guarro, Josep, Johnson, E. M., Kidd, S. E., Pereira, S. A., Rodrigues, A. M., Rozental, S., Szeszs, M. W., Ballesté Alaniz, R., Bonifaz, Alexandro, Bonfietti, L. X., Borba Santos, L. P., Capilla, Javier, Colombo, A. L., Dolande, M., Isla, M. G., Melhem, M. S. C., Mesa Arango, A. C., Oliveira, M. M. E., Panizo, M. M., Pires de Camargo, Z., Zancope Oliveira, R. M., Meis, J. F., and Turnidge, J.

Abstract

Clinical and Laboratory Standards Institute (CLSI) conditions for testing the susceptibilities of pathogenic Sporothrix species to antifungal agents are based on a collaborative study that evaluated five clinically relevant isolates of Sporothrix schenckii sensu lato and some antifungal agents. With the advent of molecular identification, there are two basic needs: to confirm the suitability of these testing conditions for all agents and Sporothrix species and to establish species-specific epidemiologic cutoff values (ECVs) or breakpoints (BPs) for the species. We collected available CLSI MICs/minimal effective concentrations (MECs) of amphotericin B, five triazoles, terbinafine, flucytosine, and caspofungin for 301 Sporothrix schenckii sensu stricto, 486 S. brasiliensis, 75S. globosa, and 13 S. mexicana molecularly identified isolates. Data were obtained in 17 independent laboratories (Australia, Europe, India, South Africa, and South and North America) using conidial inoculum suspensions and 48 to 72 h of incubation at 35°C. Sufficient and suitable data (modal MICs within 2-fold concentrations) allowed the proposal of the following ECVs for S. schenckii and S. brasiliensis, respectively: amphotericin B, 4 and 4 g/ml; itraconazole, 2 and 2 g/ml; posaconazole, 2 and 2 g/ml; and voriconazole, 64 and 32 g/ml. Ketoconazole and terbinafine ECVs for S. brasiliensis were 2 and 0.12 g/ml, respectively. Insufficient or unsuitable data precluded the calculation of ketoconazole and terbinafine (or any other antifungal agent) ECVs for S. schenckii, as well as ECVs for S. globosa and S. mexicana. These ECVs could aid the clinician in identifying potentially resistant isolates (non-wild type) less likely to respond to therapy.

Published
2017

13. Voriconazole MICs are predictive for the outcome of experimental disseminated scedosporiosis

Author

Martin Vicente, Adela, Guarro, Josep, González González, Gloria María, Lass Flörl, Cornelia, Lackner, Michaela, Capilla, Javier, Martin Vicente, Adela, Guarro, Josep, González González, Gloria María, Lass Flörl, Cornelia, Lackner, Michaela, and Capilla, Javier

Abstract

Scedosporiosis is associated with a mortality rate of up to 90% in patients suffering from disseminated infections. Recommended first-line treatment is voriconazole, but epidemiological cut-off values and clinical breakpoints have not been determined. Objectives: To correlate voriconazole treatment response in mice suffering from disseminated scedosporiosis with MIC values determined using CLSI broth microdilution, Etest (bioMe´rieux) and disc diffusion

Published
2016

14. Detección de errores en ortofotogramas mediante la visión estéreo

Author

Universitat Politècnica de Catalunya. Departament d'Enginyeria Civil i Ambiental, Prades Valls, Albert, Muñoz Capilla, Javier, Sousa Vilchez, Héctor, Universitat Politècnica de Catalunya. Departament d'Enginyeria Civil i Ambiental, Prades Valls, Albert, Muñoz Capilla, Javier, and Sousa Vilchez, Héctor

Abstract

En este proyecto se ha implementado un programa para ayudar en la detección de errores de ortofotogramas mediante la visión estéreo. Se ha usado el lenguaje C++ con el apoyo de las librerías Open Graphic Library (OpenGL) para el procesamiento de imágenes y Microsoft Foundation Classes (MFC) para la interfaz gráfica. El programa nos permite visualizar en estéreo un par de ortoimágenes que comparten una zona de solapamiento. Si el modelo y las imágenes son correctos, se espera una visualización plana y sin relieves. En el caso de que existan discrepancias, entonces el operador podrá acotar rápidamente las zonas con problemas y podrá corregirlas apropiadamente. El trabajo se divide en tres apartados. El primero donde se explican los conceptos teóricos necesarios, un segundo apartado donde se expone cómo configurar la computadora para la visualización 3D. Por último, la parte práctica que corresponde al diseño e implementación de los diferentes módulos, donde se muestra el funcionamiento del programa y la exposición de los resultados obtenidos.

Published
2016

15. Voriconazole MICs are predictive for the outcome of experimental disseminated scedosporiosis

Author

Martin Vicente, Adela, Guarro, Josep, González González, Gloria María, Lass Flörl, Cornelia, Lackner, Michaela, Capilla, Javier, Martin Vicente, Adela, Guarro, Josep, González González, Gloria María, Lass Flörl, Cornelia, Lackner, Michaela, and Capilla, Javier

Abstract

Scedosporiosis is associated with a mortality rate of up to 90% in patients suffering from disseminated infections. Recommended first-line treatment is voriconazole, but epidemiological cut-off values and clinical breakpoints have not been determined. Objectives: To correlate voriconazole treatment response in mice suffering from disseminated scedosporiosis with MIC values determined using CLSI broth microdilution, Etest (bioMe´rieux) and disc diffusion

Published
2016

16. Voriconazole MICs are predictive for the outcome of experimental disseminated scedosporiosis

Author

Martin Vicente, Adela, Guarro, Josep, González González, Gloria María, Lass Flörl, Cornelia, Lackner, Michaela, Capilla, Javier, Martin Vicente, Adela, Guarro, Josep, González González, Gloria María, Lass Flörl, Cornelia, Lackner, Michaela, and Capilla, Javier

Abstract

Scedosporiosis is associated with a mortality rate of up to 90% in patients suffering from disseminated infections. Recommended first-line treatment is voriconazole, but epidemiological cut-off values and clinical breakpoints have not been determined. Objectives: To correlate voriconazole treatment response in mice suffering from disseminated scedosporiosis with MIC values determined using CLSI broth microdilution, Etest (bioMe´rieux) and disc diffusion

Published
2016

17. Oral Particle Uptake and Organ Targeting Drives the Activity of Amphotericin B Nanoparticles

Author

Ciències Mèdiques Bàsiques, Universitat Rovira i Virgili, Serrano, Dolores R.; Lalatsa, Aikaterini; Auxiliadora Dea-Ayuela, M.; Bilbao-Ramos, Pablo E.; Garrett, Natalie L.; Moger, Julian; Guarro, Josep; Capilla, Javier; Paloma Ballesteros, M.; Schaetzlein, Andreas G.; Bolas, Francisco; Torrado, Juan J.; Uchegbu, Ijeoma F., Ciències Mèdiques Bàsiques, Universitat Rovira i Virgili, and Serrano, Dolores R.; Lalatsa, Aikaterini; Auxiliadora Dea-Ayuela, M.; Bilbao-Ramos, Pablo E.; Garrett, Natalie L.; Moger, Julian; Guarro, Josep; Capilla, Javier; Paloma Ballesteros, M.; Schaetzlein, Andreas G.; Bolas, Francisco; Torrado, Juan J.; Uchegbu, Ijeoma F.

Abstract

There are very few drug delivery systems that target key organs via the oral route, as oral delivery advances normally address gastrointestinal drug dissolution, permeation, and stability. Here we introduce a nanomedicine in which nanoparticles, while also protecting the drug from gastric degradation, are taken up by the gastrointestinal epithelia and transported to the lung, liver, and spleen, thus selectively enhancing drug bioavailability in these target organs and diminishing kidney exposure (relevant to nephrotoxic drugs). Our work demonstrates, for the first time, that oral particle uptake and translocation to specific organs may be used to achieve a beneficial therapeutic response. We have illustrated this using amphotericin B, a nephrotoxic drug encapsulated within N-palmitoyl-N-methyl-N,N-dimethyl-N,N,N-trimethyl-6-O-glycol chitosan (GCPQ) nanoparticles, and have evidenced our approach in three separate disease states (visceral leishmaniasis, candidiasis, and aspergillosis) using industry standard models of the disease in small animals. The oral bioavailability of AmB-GCPQ nanoparticles is 24%. In all disease models, AmB-GCPQ nanoparticles show comparable efficacy to parenteral liposomal AmB (AmBisome). Our work thus paves the way for others to use nanoparticles to achieve a specific targeted delivery of drug to key organs via the oral route. This is especially important for drugs with a narrow therapeutic index.

Published
2015

18. Pithomyces species (Montagnulaceae) from clinical specimens: Identification and antifungal susceptibility profiles

Author

UCL - SST/ELI/ELIM - Applied Microbiology, Da Cunha, Keith Cássia, Guarro, Josep, Wiederhold, Nathan P., Decock, Cony, Madrid, Hugo, Capilla, Javier, Cano, Josep, Gené, Josepa, Sutton, Deanna A., UCL - SST/ELI/ELIM - Applied Microbiology, Da Cunha, Keith Cássia, Guarro, Josep, Wiederhold, Nathan P., Decock, Cony, Madrid, Hugo, Capilla, Javier, Cano, Josep, Gené, Josepa, and Sutton, Deanna A.

Abstract

The fungal genus Pithomyces comprises numerous dematiaceous saprobic species commonly found on dead leaves and stems of a great variety of plants. Occasionally, they have been recovered from clinical specimens. We morphologically and molecularly (rDNA sequences) investigated a set of 42 isolates tentatively identified as Pithomyces recovered from clinical specimens in the United States. The predominant species were P. chartarum and P. sacchari (33.3% each), followed by Pithomyces sp. I (28.6%) and P. maydicus (4.8%). Most of the isolates were obtained from samples of superficial tissue (50%), the respiratory tract (21.4%), and the nasal region (19%). In general, these fungi were highly susceptible in vitro to the eight antifungal agents tested.

Published
2014

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