33 results on '"Vilches, Clara"'
Search Results
2. Dysfunctional LAT2 Amino Acid Transporter Is Associated With Cataract in Mouse and Humans
- Author
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Knöpfel, Emilia Boiadjieva, Vilches, Clara, Camargo, Simone MR, Errasti-Murugarren, Ekaitz, Stäubli, Andrina, Mayayo, Clara, Munier, Francis L, Miroshnikova, Nataliya, Poncet, Nadège, Junza, Alexandra, Bhattacharya, Shomi S, Prat, Esther, Berry, Vanita, Berger, Wolfgang, Heon, Elise, Moore, Anthony T, Yanes, Óscar, Nunes, Virginia, Palacín, Manuel, Verrey, Francois, and Kloeckener-Gruissem, Barbara
- Subjects
Biomedical and Clinical Sciences ,Ophthalmology and Optometry ,Eye Disease and Disorders of Vision ,Aging ,Congenital Structural Anomalies ,Pediatric ,Genetics ,2.1 Biological and endogenous factors ,Aetiology ,amino acid transporters LAT2 and TAT1 ,gene expression ,cataract ,ocular tissues ,mouse model ,patient screen ,Physiology ,Medical Physiology ,Psychology ,Biochemistry and cell biology ,Medical physiology - Abstract
Cataract, the loss of ocular lens transparency, accounts for ∼50% of worldwide blindness and has been associated with water and solute transport dysfunction across lens cellular barriers. We show that neutral amino acid antiporter LAT2 (Slc7a8) and uniporter TAT1 (Slc16a10) are expressed on mouse ciliary epithelium and LAT2 also in lens epithelium. Correspondingly, deletion of LAT2 induced a dramatic decrease in lens essential amino acid levels that was modulated by TAT1 defect. Interestingly, the absence of LAT2 led to increased incidence of cataract in mice, in particular in older females, and a synergistic effect was observed with simultaneous lack of TAT1. Screening SLC7A8 in patients diagnosed with congenital or age-related cataract yielded one homozygous single nucleotide deletion segregating in a family with congenital cataract. Expressed in HeLa cells, this LAT2 mutation did not support amino acid uptake. Heterozygous LAT2 variants were also found in patients with cataract some of which showed a reduced transport function when expressed in HeLa cells. Whether heterozygous LAT2 variants may contribute to the pathology of cataract needs to be further investigated. Overall, our results suggest that defects of amino acid transporter LAT2 are implicated in cataract formation, a situation that may be aggravated by TAT1 defects.
- Published
- 2019
3. In vivo testing of gold nanoparticles using the Caenorhabditis elegans model organism
- Author
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Gonzalez-Moragas, Laura, Berto, Pascal, Vilches, Clara, Quidant, Romain, Kolovou, Androniki, Santarella-Mellwig, Rachel, Schwab, Yannick, Stürzenbaum, Stephen, Roig, Anna, and Laromaine, Anna
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- 2017
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4. Targeted hyperthermia with plasmonic nanoparticles
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Vilches, Clara, primary and Quidant, Romain, additional
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- 2020
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5. Standardization of In Vitro Studies for Plasmonic Photothermal therapy
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Villuendas, Helena, primary, Vilches, Clara, additional, and Quidant, Romain, additional
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- 2023
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6. The antioxidant l-Ergothioneine prevents cystine lithiasis in the Slc7a9-/- mouse model of cystinuria
- Author
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0000-0002-5747-9310, Mayayo-Vallverdú, Clara, López de Heredia, Miguel, Prat, Esther, González, Laura, Espino Guarch, Meritxell, Vilches, Clara, Muñoz, Lourdes, Asensi, Miguel A., Serra, Carmen, Llebaria, Amadeu, Casado, Mercedes, Artuch, Rafael, Garrabou, Gloria, Garcia-Roves, Pablo M., Pallardó, Federico V., Nunes, Virginia, 0000-0002-5747-9310, Mayayo-Vallverdú, Clara, López de Heredia, Miguel, Prat, Esther, González, Laura, Espino Guarch, Meritxell, Vilches, Clara, Muñoz, Lourdes, Asensi, Miguel A., Serra, Carmen, Llebaria, Amadeu, Casado, Mercedes, Artuch, Rafael, Garrabou, Gloria, Garcia-Roves, Pablo M., Pallardó, Federico V., and Nunes, Virginia
- Abstract
The high recurrence rate of cystine lithiasis observed in cystinuria patients highlights the need for new therapeutic options to address this chronic disease. There is growing evidence of an antioxidant defect in cystinuria, which has led to test antioxidant molecules as new therapeutic approaches. In this study, the antioxidant l-Ergothioneine was evaluated, at two different doses, as a preventive and long-term treatment for cystinuria in the Slc7a9-/- mouse model. l-Ergothioneine treatments decreased the rate of stone formation by more than 60% and delayed its onset in those mice that still developed calculi. Although there were no differences in metabolic parameters or urinary cystine concentration between control and treated mice, cystine solubility was increased by 50% in the urines of treated mice. We also demonstrate that l-Ergothioneine needs to be internalized by its transporter OCTN1 (Slc22a4) to be effective, as when administrated to the double mutant Slc7a9-/-Slc22a4-/- mouse model, no effect on the lithiasis phenotype was observed. In kidneys, we detected a decrease in GSH levels and an impairment of maximal mitochondrial respiratory capacity in cystinuric mice that l-Ergothioneine treatment was able to restore. Thus, l-Ergothioneine administration prevented cystine lithiasis in the Slc7a9-/- mouse model by increasing urinary cystine solubility and recovered renal GSH metabolism and mitochondrial function. These results support the need for clinical trials to test l-Ergothioneine as a new treatment for cystinuria.
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- 2023
7. Influence of Cell Type on the Efficacy of Plasmonic Photothermal Therapy
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Villuendas, Helena, primary, Vilches, Clara, additional, and Quidant, Romain, additional
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- 2022
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8. Treatment of Hepatic Fibrosis in Mice Based on Targeted Plasmonic Hyperthermia
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Ribera, Jordi, primary, Vilches, Clara, additional, Sanz, Vanesa, additional, de Miguel, Ignacio, additional, Portolés, Irene, additional, Córdoba-Jover, Bernat, additional, Prat, Esther, additional, Nunes, Virginia, additional, Jiménez, Wladimiro, additional, Quidant, Romain, additional, and Morales-Ruiz, Manuel, additional
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- 2021
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9. A toolbox for the comprehensive, real-time optimization of plasmonic photothermal therapy demonstrated on an orthotopic renal tumor model
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Fernández Esteberena, Pablo R., primary, Vilches, Clara, additional, Martínez Lozano, María del Mar, additional, de Miguel, Ignacio, additional, Casanovas, Oriol, additional, Quidant, Romain, additional, and Durduran, Turgut, additional
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- 2021
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10. Chapter 12 - Targeted hyperthermia with plasmonic nanoparticles
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Vilches, Clara and Quidant, Romain
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- 2020
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11. Dysfunctional LAT2 Amino Acid Transporter Is Associated With Cataract in Mouse and Humans
- Author
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Knöpfel, Emilia Boiadjieva, primary, Vilches, Clara, additional, Camargo, Simone M. R., additional, Errasti-Murugarren, Ekaitz, additional, Stäubli, Andrina, additional, Mayayo, Clara, additional, Munier, Francis L., additional, Miroshnikova, Nataliya, additional, Poncet, Nadège, additional, Junza, Alexandra, additional, Bhattacharya, Shomi S., additional, Prat, Esther, additional, Berry, Vanita, additional, Berger, Wolfgang, additional, Heon, Elise, additional, Moore, Anthony T., additional, Yanes, Óscar, additional, Nunes, Virginia, additional, Palacín, Manuel, additional, Verrey, Francois, additional, and Kloeckener-Gruissem, Barbara, additional
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- 2019
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12. Dysfunctional LAT2 Amino Acid Transporter Is Associated With Cataract in Mouse and Humans
- Author
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Boiadjieva Knöpfel, Emilia, Vilches, Clara, Camargo, Simone M R, Errasti-Murugarren, Ekaitz, Stäubli, Andrina, Mayayo, Clara, Munier, Francis L, Miroshnikova, Nataliya, Poncet, Nadège, Junza, Alexandra, Bhattacharya, Shomi S, Prat, Esther, Berry, Vanita, Berger, Wolfgang, Heon, Elise, Moore, Anthony T, Yanes, Óscar, Nunes, Virginia, Palacín, Manuel, Verrey, Francois, Kloeckener-Gruissem, Barbara, Boiadjieva Knöpfel, Emilia, Vilches, Clara, Camargo, Simone M R, Errasti-Murugarren, Ekaitz, Stäubli, Andrina, Mayayo, Clara, Munier, Francis L, Miroshnikova, Nataliya, Poncet, Nadège, Junza, Alexandra, Bhattacharya, Shomi S, Prat, Esther, Berry, Vanita, Berger, Wolfgang, Heon, Elise, Moore, Anthony T, Yanes, Óscar, Nunes, Virginia, Palacín, Manuel, Verrey, Francois, and Kloeckener-Gruissem, Barbara
- Abstract
Cataract, the loss of ocular lens transparency, accounts for ∼50% of worldwide blindness and has been associated with water and solute transport dysfunction across lens cellular barriers. We show that neutral amino acid antiporter LAT2 ) and uniporter TAT1 () are expressed on mouse ciliary epithelium and LAT2 also in lens epithelium. Correspondingly, deletion of LAT2 induced a dramatic decrease in lens essential amino acid levels that was modulated by TAT1 defect. Interestingly, the absence of LAT2 led to increased incidence of cataract in mice, in particular in older females, and a synergistic effect was observed with simultaneous lack of TAT1. Screening in patients diagnosed with congenital or age-related cataract yielded one homozygous single nucleotide deletion segregating in a family with congenital cataract. Expressed in HeLa cells, this LAT2 mutation did not support amino acid uptake. Heterozygous LAT2 variants were also found in patients with cataract some of which showed a reduced transport function when expressed in HeLa cells. Whether heterozygous LAT2 variants may contribute to the pathology of cataract needs to be further investigated. Overall, our results suggest that defects of amino acid transporter LAT2 are implicated in cataract formation, a situation that may be aggravated by TAT1 defects.
- Published
- 2019
13. Dysfunctional LAT2 amino acid transporter is associated with cataract in mouse and humans
- Author
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Hartmann Müller Foundation for Medical Research, Novartis Foundation for Sustainable Development, Swiss National Science Foundation, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), European Commission, Instituto de Salud Carlos III, Generalitat de Catalunya, Centro de Investigación Biomédica en Red Enfermedades Raras (España), Wellcome Trust, National Institute for Health Research (UK), Knöpfel, Emilia Boiadjieva, Vilches, Clara, Camargo, Simone M. R., Errasti-Murugarren, Ekaitz, Stäubli, Andrina, Mayayo, Clara, Munier, Francis L., Miroshnikova, Nataliya, Poncet, Nadège, Junza, Alexandra, Bhattacharya, Shom Shanker, Prat, Esther, Berry, Vanita, Berger, Wolfgang, Heon, Elise, Moore, Anthony T., Yanes, Óscar, Nunes, Virginia, Palacín, Manuel, Verrey, Francois, Kloeckener-Gruissem, Barbara, Hartmann Müller Foundation for Medical Research, Novartis Foundation for Sustainable Development, Swiss National Science Foundation, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), European Commission, Instituto de Salud Carlos III, Generalitat de Catalunya, Centro de Investigación Biomédica en Red Enfermedades Raras (España), Wellcome Trust, National Institute for Health Research (UK), Knöpfel, Emilia Boiadjieva, Vilches, Clara, Camargo, Simone M. R., Errasti-Murugarren, Ekaitz, Stäubli, Andrina, Mayayo, Clara, Munier, Francis L., Miroshnikova, Nataliya, Poncet, Nadège, Junza, Alexandra, Bhattacharya, Shom Shanker, Prat, Esther, Berry, Vanita, Berger, Wolfgang, Heon, Elise, Moore, Anthony T., Yanes, Óscar, Nunes, Virginia, Palacín, Manuel, Verrey, Francois, and Kloeckener-Gruissem, Barbara
- Abstract
Cataract, the loss of ocular lens transparency, accounts for ~50% of worldwide blindness and has been associated with water and solute transport dysfunction across lens cellular barriers. We show that neutral amino acid antiporter LAT2 (Slc7a8) and uniporter TAT1 (Slc16a10) are expressed on mouse ciliary epithelium and LAT2 also in lens epithelium. Correspondingly, deletion of LAT2 induced a dramatic decrease in lens essential amino acid levels that was modulated by TAT1 defect. Interestingly, the absence of LAT2 led to increased incidence of cataract in mice, in particular in older females, and a synergistic effect was observed with simultaneous lack of TAT1. Screening SLC7A8 in patients diagnosed with congenital or age-related cataract yielded one homozygous single nucleotide deletion segregating in a family with congenital cataract. Expressed in HeLa cells, this LAT2 mutation did not support amino acid uptake. Heterozygous LAT2 variants were also found in patients with cataract some of which showed a reduced transport function when expressed in HeLa cells. Whether heterozygous LAT2 variants may contribute to the pathology of cataract needs to be further investigated. Overall, our results suggest that defects of amino acid transporter LAT2 are implicated in cataract formation, a situation that may be aggravated by TAT1 defects.
- Published
- 2019
14. Non-invasive and quantitative in vivo monitoring of gold nanoparticle concentration and tissue hemodynamics by hybrid optical spectroscopies
- Author
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Mireles, Miguel, Morales-Dalmau, Jordi, Johansson, Johannes, Vidal-Rosas, Ernesto E., Vilches, Clara, Martinez-Lozano, Mar, Sanz, Vanesa, de Miguel, Ignacio, Casanovas, Oriol, Quidant, Romain, Durduran, Turgut, Mireles, Miguel, Morales-Dalmau, Jordi, Johansson, Johannes, Vidal-Rosas, Ernesto E., Vilches, Clara, Martinez-Lozano, Mar, Sanz, Vanesa, de Miguel, Ignacio, Casanovas, Oriol, Quidant, Romain, and Durduran, Turgut
- Abstract
Owing to their unique combination of chemical and physical properties, inorganic nanoparticles show a great deal of potential as suitable agents for early diagnostics and less invasive therapies. Yet, their translation to the clinic has been hindered, in part, by the lack of non-invasive methods to quantify their concentration in vivo while also assessing their effect on the tissue physiology. In this work, we demonstrate that diffuse optical techniques, employing near-infrared light, have the potential to address this need in the case of gold nanoparticles which support localized surface plasmons. An orthoxenograft mouse model of clear cell renal cell carcinoma was non-invasively assessed by diffuse reflectance and correlation spectroscopies before and over several days following a single intravenous tail vein injection of polyethylene glycol-coated gold nanorods (AuNRs-PEG). Our platform enables to resolve the kinetics of the AuNR-PEG uptake by the tumor in quantitative agreement with ex vivo inductively coupled plasma mass spectroscopy. Furthermore, it allows for the simultaneous monitoring of local tissue hemodynamics, enabling us to conclude that AuNRs-PEG do not significantly alter the animal physiology. We note that the penetration depth of this current probe was a few millimeters but can readily be extended to centimeters, hence gaining clinical relevance. This study and the methodology presented here complement the nanomedicine toolbox by providing a flexible platform, extendable to other absorbing agents that can potentially be translated to human trials., Funding Agencies|Fundacio CELLEX Barcelona (HYTH); Ministerio de Economia y Competitividad (PHOTODEMENTIA) [DPI2015-64358-C1, DPI2015-64358-C2]; Instituto de Salud Carlos III/FEDER [MEDPHOTAGE DTS16/00087]; "Severo Ochoa" Programme for Centres of Excellence in RD [SEV-2015-0522]; Obra social "La Caixa" Foundation (LlumMedBcn); Institucio CERCA; AGAUR-Generalitat [2017 SGR 1380]; LASERLAB-EUROPE IV [651448]; CONACYT [329661/306133]; Marie Curie IEF fellowship (FP7 MOBODICT); FPI fellowship program MINECO [BES-2013-064913]
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- 2019
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15. Non-invasive and quantitativein vivomonitoring of gold nanoparticle concentration and tissue hemodynamics by hybrid optical spectroscopies
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Mireles, Miguel, primary, Morales-Dalmau, Jordi, additional, Johansson, Johannes D., additional, Vidal-Rosas, Ernesto E., additional, Vilches, Clara, additional, Martínez-Lozano, Mar, additional, Sanz, Vanesa, additional, de Miguel, Ignacio, additional, Casanovas, Oriol, additional, Quidant, Romain, additional, and Durduran, Turgut, additional
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- 2019
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16. Quantification of gold nanoparticle accumulation in tissue by two-photon luminescence microscopy
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Morales-Dalmau, Jordi, primary, Vilches, Clara, additional, Sanz, Vanesa, additional, de Miguel, Ignacio, additional, Rodríguez-Fajardo, Valeria, additional, Berto, Pascal, additional, Martínez-Lozano, Mar, additional, Casanovas, Oriol, additional, Durduran, Turgut, additional, and Quidant, Romain, additional
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- 2019
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17. Cooperation of Antiporter LAT2/CD98hc with Uniporter TAT1 for Renal Reabsorption of Neutral Amino Acids
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Vilches, Clara, primary, Boiadjieva-Knöpfel, Emilia, additional, Bodoy, Susanna, additional, Camargo, Simone, additional, López de Heredia, Miguel, additional, Prat, Esther, additional, Ormazabal, Aida, additional, Artuch, Rafael, additional, Zorzano, Antonio, additional, Verrey, François, additional, Nunes, Virginia, additional, and Palacín, Manuel, additional
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- 2018
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18. Mutations in L-type amino acid transporter-2 support SLC7A8 as a novel gene involved in age-related hearing loss
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Generalitat de Catalunya, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, European Commission, Qatar National Research Fund, Espino Guarch, Meritxell, Font-Llitjós, Mariona, Murillo-Cuesta, Silvia, Errasti-Murugarren, Ekaitz, Celaya, Adelaida M., Girotto, Giorgia, Vuckovic, Dragana, Mezzavilla, Massimo, Vilches, Clara, Bodoy, Susanna, Sahún, Ignasi, González, Laura, Prat, Esther, Zorzano, Antonio, Dierssen, Mara, Varela-Nieto, Isabel, Gasparini, Paolo, Palacín, Manuel, Nunes, Virginia, Generalitat de Catalunya, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, European Commission, Qatar National Research Fund, Espino Guarch, Meritxell, Font-Llitjós, Mariona, Murillo-Cuesta, Silvia, Errasti-Murugarren, Ekaitz, Celaya, Adelaida M., Girotto, Giorgia, Vuckovic, Dragana, Mezzavilla, Massimo, Vilches, Clara, Bodoy, Susanna, Sahún, Ignasi, González, Laura, Prat, Esther, Zorzano, Antonio, Dierssen, Mara, Varela-Nieto, Isabel, Gasparini, Paolo, Palacín, Manuel, and Nunes, Virginia
- Abstract
Age-related hearing loss (ARHL) is the most common sensory deficit in the elderly. The disease has a multifactorial etiology with both environmental and genetic factors involved being largely unknown. SLC7A8/SLC3A2 heterodimer is a neutral amino acid exchanger. Here, we demonstrated that SLC7A8 is expressed in the mouse inner ear and that its ablation resulted in ARHL, due to the damage of different cochlear structures. These findings make SLC7A8 transporter a strong candidate for ARHL in humans. Thus, a screening of a cohort of ARHL patients and controls was carried out revealing several variants in SLC7A8, whose role was further investigated by in vitro functional studies. Significant decreases in SLC7A8 transport activity was detected for patient's variants (p.Val302Ile, p.Arg418His, p.Thr402Met and p.Val460Glu) further supporting a causative role for SLC7A8 in ARHL. Moreover, our preliminary data suggest that a relevant proportion of ARHL cases could be explained by SLC7A8 mutations.
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- 2018
19. La ablación del transportador de aminoácidos LAT2 (SLC7A8) causa hipoacusia asociada al envejecimiento en ratón
- Author
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Murillo-Cuesta, Silvia, Espino Guarch, Meritxell, Font-Llitjós, Mariona, Celaya, Adelaida M., Vilches, Clara, Bodoy, Susanna, Sahún, Ignasi, González, Laura, Prat, Esther, Dierssen, Mara, Palacín, Manuel, Nunes, Virginia, and Varela-Nieto, Isabel
- Abstract
Trabajo presentado a la X Reunión Científica Anual CIBERER, celebrada en San Lorenzo del Escorial del 23 al 24 de marzo de 2017.
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- 2017
20. Mutations in L-type amino acid transporter-2 support SLC7A8 as a novel gene involved in age-related hearing loss
- Author
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Espino Guarch, Meritxell, primary, Font-Llitjós, Mariona, additional, Murillo-Cuesta, Silvia, additional, Errasti- Murugarren, Ekaitz, additional, Celaya, Adelaida M, additional, Girotto, Giorgia, additional, Vuckovic, Dragana, additional, Mezzavilla, Massimo, additional, Vilches, Clara, additional, Bodoy, Susanna, additional, Sahún, Ignasi, additional, González, Laura, additional, Prat, Esther, additional, Zorzano, Antonio, additional, Dierssen, Mara, additional, Varela-Nieto, Isabel, additional, Gasparini, Paolo, additional, Palacín, Manuel, additional, and Nunes, Virginia, additional
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- 2018
- Full Text
- View/download PDF
21. Author response: Mutations in L-type amino acid transporter-2 support SLC7A8 as a novel gene involved in age-related hearing loss
- Author
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Espino Guarch, Meritxell, primary, Font-Llitjós, Mariona, additional, Murillo-Cuesta, Silvia, additional, Errasti- Murugarren, Ekaitz, additional, Celaya, Adelaida M, additional, Girotto, Giorgia, additional, Vuckovic, Dragana, additional, Mezzavilla, Massimo, additional, Vilches, Clara, additional, Bodoy, Susanna, additional, Sahún, Ignasi, additional, González, Laura, additional, Prat, Esther, additional, Zorzano, Antonio, additional, Dierssen, Mara, additional, Varela-Nieto, Isabel, additional, Gasparini, Paolo, additional, Palacín, Manuel, additional, and Nunes, Virginia, additional
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- 2018
- Full Text
- View/download PDF
22. Optimum morphology of gold nanorods for light-induced hyperthermia
- Author
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Morales-Dalmau, Jordi, primary, Vilches, Clara, additional, de Miguel, Ignacio, additional, Sanz, Vanesa, additional, and Quidant, Romain, additional
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- 2018
- Full Text
- View/download PDF
23. In vivo testing of gold nanoparticles using the Caenorhabditis elegans model organism
- Author
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Universitat Politècnica de Catalunya. Institut de Ciències Fotòniques, Gonzalez-Moragasa, Laura, Berto, Clara, Vilches, Clara, Quidant, Romain, Kolovouc, Androniki, Santarella-Mellwig, Rachel, Schwab, Yannick, Stürzenbaum, Stephen, Roig, Anna, Laromainea, Anna, Universitat Politècnica de Catalunya. Institut de Ciències Fotòniques, Gonzalez-Moragasa, Laura, Berto, Clara, Vilches, Clara, Quidant, Romain, Kolovouc, Androniki, Santarella-Mellwig, Rachel, Schwab, Yannick, Stürzenbaum, Stephen, Roig, Anna, and Laromainea, Anna
- Abstract
Gold nanoparticles (AuNPs) are present in many man-made products and cosmetics, and are also used by the food and medical industries. Tight regulations regarding the use of mammalian animals for product testing can hamper the study of the specific interactions between engineered nanoparticles and biological systems. Invertebrate models, such as the nematode Caenorhabditis elegans (C. elegans), can offer alternative approaches during the early phases of nanoparticle discovery. Here, we thoroughly evaluated the biodistribution of 11-nm and 150-nm citrate-capped AuNPs in the model organism C. elegans at multiple scales, moving from micrometric to nanometric resolution and from the organismal to cellular level. We confirmed that the nanoparticles were not able to cross the intestinal and dermal barriers. We investigated the effect of AuNPs on the survival and reproductive performance of C. elegans, and correlated these effects with the uptake of AuNPs in terms of their number, surface area, and metal mass. In general, exposure to 11-nm AuNPs resulted in a higher toxicity than the larger 150-nm AuNPs. NP aggregation inside C. elegans was determined using absorbance microspectroscopy, which allowed the plasmonic properties of AuNPs to be correlated with their confinement inside the intestinal lumen, where anatomical traits, acidic pH and the presence of biomolecules play an essential role on NP aggregation. Finally, quantitative PCR of selected molecular markers indicated that exposure to AuNPs did not significantly affect endocytosis and intestinal barrier integrity. Statement of significance This work highlights how the simple, yet information-rich, animal model C. elegans is ideally suited for preliminary screening of nanoparticles or chemicals mitigating most of the difficulties associated with mammalian animal models, namely the ethical issues, the high cost, and time constraints. This is of particular relevance to the cosmetic, food, and pharmaceutical industries, w, Peer Reviewed, Postprint (author's final draft)
- Published
- 2017
24. In vivo testing of gold nanoparticles using the Caenorhabditis elegans model organism
- Author
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Ministerio de Economía y Competitividad (España), Generalitat de Catalunya, European Commission, European Cooperation in Science and Technology, European Molecular Biology Laboratory, National Institutes of Health (US), González Moragas, Laura, Berto, Pascal, Vilches, Clara, Quidant, Romain, Kolovou, Androniki, Santarella-Mellwig, Rachel, Schwab, Yannick, Stürzenbaum, Stephen, Roig Serra, Anna, Laromaine, Anna, Ministerio de Economía y Competitividad (España), Generalitat de Catalunya, European Commission, European Cooperation in Science and Technology, European Molecular Biology Laboratory, National Institutes of Health (US), González Moragas, Laura, Berto, Pascal, Vilches, Clara, Quidant, Romain, Kolovou, Androniki, Santarella-Mellwig, Rachel, Schwab, Yannick, Stürzenbaum, Stephen, Roig Serra, Anna, and Laromaine, Anna
- Abstract
Gold nanoparticles (AuNPs) are present in many man-made products and cosmetics and are also used by the food and medical industries. Tight regulations regarding the use of mammalian animals for product testing can hamper the study of the specific interactions between engineered nanoparticles and biological systems. Invertebrate models, such as the nematode Caenorhabditis elegans (C. elegans), can offer alternative approaches during the early phases of nanoparticle discovery. Here, we thoroughly evaluated the biodistribution of 11-nm and 150-nm citrate-capped AuNPs in the model organism C. elegans at multiple scales, moving from micrometric to nanometric resolution and from the organismal to cellular level. We confirmed that the nanoparticles were not able to cross the intestinal and dermal barriers. We investigated the effect of AuNPs on the survival and reproductive performance of C. elegans, and correlated these effects with the uptake of AuNPs in terms of their number, surface area, and metal mass. In general, exposure to 11-nm AuNPs resulted in a higher toxicity than the larger 150-nm AuNPs. NP aggregation inside C. elegans was determined using absorbance microspectroscopy, which allowed the plasmonic properties of AuNPs to be correlated with their confinement inside the intestinal lumen, where anatomical traits, acidic pH and the presence of biomolecules play an essential role on NP aggregation. Finally, quantitative PCR of selected molecular markers indicated that exposure to AuNPs did not significantly affect endocytosis and intestinal barrier integrity.
- Published
- 2017
25. Simultaneous, non-invasive measurement of local tissue hemodynamics, oxygen metabolism and gold nanorod concentration in vivo
- Author
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Morales, Jordí, Mireles, Miguel, Johansson, Johannes D., Martínez Lozano, Mar, Vilches, Clara, Casanovas, Oriol, Quidant, Romain, Durduran, Turgut, Morales, Jordí, Mireles, Miguel, Johansson, Johannes D., Martínez Lozano, Mar, Vilches, Clara, Casanovas, Oriol, Quidant, Romain, and Durduran, Turgut
- Abstract
A hybrid broadband diffuse optical and diffuse correlation spectroscopy system is used to measure local tissue hemodynamics, oxygen metabolism and gold nanorod concentration. The objective is to provide real-time feed-back for photothermal therapy.
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- 2016
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26. Simultaneous, non-invasive measurement of local tissue hemodynamics, oxygen metabolism and gold nanorod concentration in vivo
- Author
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Morales-Dalmau, Jordi, primary, Mireles, Miguel, additional, Johansson, Johannes, additional, Martínez-Lozano, Mar, additional, Vilches, Clara, additional, Casanovas, Oriol, additional, Quidant, Romain, additional, and Durduran, Turgut, additional
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- 2016
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27. Digenic Inheritance in Cystinuria Mouse Model
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Espino, Meritxell, primary, Font-Llitjós, Mariona, additional, Vilches, Clara, additional, Salido, Eduardo, additional, Prat, Esther, additional, López de Heredia, Miguel, additional, Palacín, Manuel, additional, and Nunes, Virginia, additional
- Published
- 2015
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28. Cooperation of Basolateral Epithelial Amino Acid Transporters TAT1 and LAT2 Investigated in a Double Knockout Mouse Model
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Boiadjieva, Emilia, primary, Vilches, Clara, additional, Bodoy, Susanna, additional, Oparija, Lalita, additional, Jando, Julia, additional, Nunes, Virginia, additional, Verrey, François, additional, and Palacin, Manuel, additional
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- 2015
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29. Mutations in L-type amino acid transporter-2 support SLC7A8 as a novel gene involved in age-related hearing loss.
- Author
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Guarch, Meritxell Espino, Font-Llitjós, Mariona, Murillo-Cuesta, Silvia, Errasti- Murugarren, Ekaitz, Celaya, Adelaida M., Girotto, Giorgia, Vuckovic, Dragana, Mezzavilla, Massimo, Vilches, Clara, Bodoy, Susanna, Sahún, Ignasi, González, Laura, Prat, Esther, Zorzano, Antonio, Dierssen, Mara, Varela-Nieto, Isabel, Gasparini, Paolo, Palacín, Manuel, and Nunes, Virginia
- Published
- 2018
- Full Text
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30. Disrupting MLC1 and GlialCAM and ClC-2 interactions in leukodystrophy entails glial chloride channel dysfunction
- Author
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Hoegg-Beiler, Maja B., primary, Sirisi, Sònia, additional, Orozco, Ian J., additional, Ferrer, Isidre, additional, Hohensee, Svea, additional, Auberson, Muriel, additional, Gödde, Kathrin, additional, Vilches, Clara, additional, de Heredia, Miguel López, additional, Nunes, Virginia, additional, Estévez, Raúl, additional, and Jentsch, Thomas J., additional
- Published
- 2014
- Full Text
- View/download PDF
31. Mutations in L-type amino acid transporter-2 support SLC7A8 as a novel gene involved in age-related hearing loss
- Author
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Mara Dierssen, Clara Vilches, Esther Prat, Dragana Vuckovic, Giorgia Girotto, Isabel Varela-Nieto, Ekaitz Errasti-Murugarren, Mariona Font-Llitjós, Adelaida M. Celaya, Silvia Murillo-Cuesta, Laura González, Massimo Mezzavilla, Paolo Gasparini, Virginia Nunes, Susanna Bodoy, Antonio Zorzano, Ignasi Sahún, Manuel Palacín, Meritxell Espino Guarch, Universitat de Barcelona, Generalitat de Catalunya, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, European Commission, Qatar National Research Fund, Guarch, Meritxell Espino, Font-Llitjós, Mariona, Murillo-Cuesta, Silvia, Errasti-Murugarren, Ekaitz, Celaya, Adelaida M., Girotto, Giorgia, Vuckovic, Dragana, Mezzavilla, Massimo, Vilches, Clara, Bodoy, Susanna, Sahún, Ignasi, González, Laura, Prat, Esther, Zorzano, Antonio, Dierssen, Mara, Varela-Nieto, Isabel, Gasparini, Paolo, Palacín, Manuel, and Nunes, Virginia
- Subjects
0301 basic medicine ,Genetics and Molecular Biology (all) ,medicine ,Etiology ,Mouse ,Immunology and Microbiology (all) ,Disease ,Audiology ,Biochemistry ,Persones grans ,Mice ,knock-out mouse model ,0302 clinical medicine ,Medicine ,chromosome ,Biology (General) ,genes ,age-related hearing lo ,General Neuroscience ,Fusion Regulatory Protein 1, Light Chains ,human biology ,Human biology ,General Medicine ,hearing lo ,Presbycusis ,3. Good health ,age-related hearing loss ,medicine.anatomical_structure ,Genes and Chromosomes ,Etiologia ,medicine.symptom ,Research Article ,Human ,chromosomes ,medicine.medical_specialty ,Amino Acid Transport System y+ ,Hearing loss ,QH301-705.5 ,Science ,L-Type Amino Acid Transporter ,Age-related hearing loss ,General Biochemistry, Genetics and Molecular Biology ,Chromosomes ,Novel gene ,03 medical and health sciences ,Trastorns auditius ,otorhinolaryngologic diseases ,Animals ,Humans ,Inner ear ,human ,Genetic Testing ,LAT2 ,Slc7a8 ,auditory brainstem response ,hearing loss ,mouse ,Neuroscience (all) ,Biochemistry, Genetics and Molecular Biology (all) ,gene ,Human Biology and Medicine ,Gene ,General Immunology and Microbiology ,business.industry ,Mutació (Biologia) ,Mutation (Biology) ,Hearing disorders ,030104 developmental biology ,Auditory brainstem response ,Genes ,Mutation ,Older people ,business ,030217 neurology & neurosurgery ,Gene Deletion - Abstract
Age-related hearing loss (ARHL) is the most common sensory deficit in the elderly. The disease has a multifactorial etiology with both environmental and genetic factors involved being largely unknown. SLC7A8/SLC3A2 heterodimer is a neutral amino acid exchanger. Here, we demonstrated that SLC7A8 is expressed in the mouse inner ear and that its ablation resulted in ARHL, due to the damage of different cochlear structures. These findings make SLC7A8 transporter a strong candidate for ARHL in humans. Thus, a screening of a cohort of ARHL patients and controls was carried out revealing several variants in SLC7A8, whose role was further investigated by in vitro functional studies. Significant decreases in SLC7A8 transport activity was detected for patient’s variants (p.Val302Ile, p.Arg418His, p.Thr402Met and p.Val460Glu) further supporting a causative role for SLC7A8 in ARHL. Moreover, our preliminary data suggest that a relevant proportion of ARHL cases could be explained by SLC7A8 mutations., eLife digest Age-related hearing loss affects about one in three individuals between the ages of 65 and 74. The first symptom is difficulty hearing high-pitched sounds like children’s voices. The disease starts gradually and worsens over time. Changes in the ear, the nerve that connects it to the brain, or the brain itself can cause hearing loss. Sometimes all three play a role. Genetics, exposure to noise, disease, and aging may all contribute. The condition is so complex it is difficult for scientists to pinpoint a primary suspect or develop treatments. Now, Guarch, Font-Llitjós et al. show that errors in a protein called SLC7A8 cause age-related hearing loss in mice and humans. The SLC7A8 protein acts like a door that allows amino acids – the building blocks of proteins – to enter or leave a cell. This door is blocked in mice lacking SLC7A8 and damage occurs in the part of their inner ear responsible for hearing. As a result, the animals lose their hearing. Next, Guarch, Font-Llitjós et al. scanned the genomes of 147 people from isolated villages in Italy for mutations in the gene for SLC7A8. The people also underwent hearing tests. Mutations in the gene for SLC7A8 that partially block the door and prevent the flow of amino acids were found in people with hearing loss. Some mutations in SLC7A8 that allow the door to stay open where found in people who could hear. The experiments suggest that certain mutations in the gene for SLC7A8 are likely an inherited cause of age-related hearing loss. It is possible that other proteins that control the flow of amino acids into or out of cells also may play a role in hearing. More studies are needed to see if it is possible to fix errors in the SLC7A8 protein to delay or restore the hearing loss.
- Published
- 2018
32. Prediction of the response to antiangiogenic sunitinib therapy by non-invasive hybrid diffuse optics in renal cell carcinoma.
- Author
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Mireles M, Jiménez-Valerio G, Morales-Dalmau J, Johansson JD, Martínez-Lozano M, Vidal-Rosas EE, Navarro-Pérez V, Busch DR, Casanovas O, Durduran T, and Vilches C
- Abstract
In this work, broadband diffuse reflectance spectroscopy (DRS) and diffuse correlation spectroscopy (DCS) were used to quantify deep tissue hemodynamics in a patient-derived orthotopic xenograft mouse model of clear cell renal cancer undergoing antiangiogenic treatment. A cohort of twenty-two mice were treated with sunitinib and compared to thirteen control untreated mice, and monitored by DRS/DCS. A reduction in total hemoglobin concentration (THC, p = 0.03), oxygen saturation (SO
2, p = 0.03) and blood flow index (BFI, p = 0.02) was observed over the treatment course. Early changes in tumor microvascular blood flow and total hemoglobin concentration were correlated with the final microvessel density (p = 0.014) and tumor weight (p = 0.024), respectively. Higher pre-treatment tumor microvascular blood flow was observed in non-responder mice with respect to responder mice, which was statistically predictive of the tumor intrinsic resistance (p = 0.01). This hybrid diffuse optical technique provides a method for predicting tumor intrinsic resistance to antiangiogenic therapy and could be used as predictive biomarker of response to antiangiogenic therapies in pre-clinical models., Competing Interests: The authors declare no conflicts of interest. Author Contributions. GJV, MM, JMD, MML and JJ conducted experiments and processed data. MM, JJ, EEVR, VNP, DRB and CV contributed to data processing. CV, OC and TD conceived the study. GJV, MM and CV prepared the manuscript draft. All authors reviewed and approved the manuscript., (© 2024 Optica Publishing Group.)- Published
- 2024
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33. Non-invasive and quantitative in vivo monitoring of gold nanoparticle concentration and tissue hemodynamics by hybrid optical spectroscopies.
- Author
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Mireles M, Morales-Dalmau J, Johansson JD, Vidal-Rosas EE, Vilches C, Martínez-Lozano M, Sanz V, de Miguel I, Casanovas O, Quidant R, and Durduran T
- Subjects
- Animals, Carcinoma, Renal Cell pathology, Carcinoma, Renal Cell therapy, Cell Line, Tumor, Humans, Hyperthermia, Induced, Infrared Rays, Kidney Neoplasms pathology, Kidney Neoplasms therapy, Male, Mass Spectrometry, Mice, Mice, Nude, Phototherapy, Polyethylene Glycols chemistry, Transplantation, Heterologous, Gold chemistry, Hemodynamics, Metal Nanoparticles chemistry
- Abstract
Owing to their unique combination of chemical and physical properties, inorganic nanoparticles show a great deal of potential as suitable agents for early diagnostics and less invasive therapies. Yet, their translation to the clinic has been hindered, in part, by the lack of non-invasive methods to quantify their concentration in vivo while also assessing their effect on the tissue physiology. In this work, we demonstrate that diffuse optical techniques, employing near-infrared light, have the potential to address this need in the case of gold nanoparticles which support localized surface plasmons. An orthoxenograft mouse model of clear cell renal cell carcinoma was non-invasively assessed by diffuse reflectance and correlation spectroscopies before and over several days following a single intravenous tail vein injection of polyethylene glycol-coated gold nanorods (AuNRs-PEG). Our platform enables to resolve the kinetics of the AuNR-PEG uptake by the tumor in quantitative agreement with ex vivo inductively coupled plasma mass spectroscopy. Furthermore, it allows for the simultaneous monitoring of local tissue hemodynamics, enabling us to conclude that AuNRs-PEG do not significantly alter the animal physiology. We note that the penetration depth of this current probe was a few millimeters but can readily be extended to centimeters, hence gaining clinical relevance. This study and the methodology presented here complement the nanomedicine toolbox by providing a flexible platform, extendable to other absorbing agents that can potentially be translated to human trials.
- Published
- 2019
- Full Text
- View/download PDF
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