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1. Chimeric Peptide Species Contribute to Divergent Dipeptide Repeat Pathology in c9ALS/FTD and SCA36

Author

McEachin, Zachary T., Gendron, Tania F., Raj, Nisha, García-Murias, María, Banerjee, Anwesha, Purcell, Ryan H., Ward, Patricia J., Todd, Tiffany W., Merritt-Garza, Megan E., Jansen-West, Karen, Hales, Chadwick M., García-Sobrino, Tania, Quintáns, Beatriz, Holler, Christopher J., Taylor, Georgia, San Millán, Beatriz, Teijeira, Susana, Yamashita, Toru, Ohkubo, Ryuichi, Boulis, Nicholas M., Xu, Chongchong, Wen, Zhexing, Streichenberger, Nathalie, Fogel, Brent L., Kukar, Thomas, Abe, Koji, Dickson, Dennis W., Arias, Manuel, Glass, Jonathan D., Jiang, Jie, Tansey, Malú G., Sobrido, María-Jesús, Petrucelli, Leonard, Rossoll, Wilfried, and Bassell, Gary J.

Published
2020
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2. Autoantibody screening in Guillain–Barré syndrome

Author

Lleixà, Cinta, Martín-Aguilar, Lorena, Pascual-Goñi, Elba, Franco, Teresa, Caballero, Marta, de Luna, Noemí, Gallardo, Eduard, Suárez-Calvet, Xavier, Martínez-Martínez, Laura, Diaz-Manera, Jordi, Rojas-García, Ricard, Cortés-Vicente, Elena, Turón, Joana, Casasnovas, Carlos, Homedes, Christian, Gutiérrez-Gutiérrez, Gerardo, Jimeno-Montero, María Concepción, Berciano, José, Sedano-Tous, Maria José, García-Sobrino, Tania, Pardo-Fernández, Julio, Márquez-Infante, Celedonio, Rojas-Marcos, Iñigo, Jericó-Pascual, Ivonne, Martínez-Hernández, Eugenia, Morís de la Tassa, Germán, Domínguez-González, Cristina, Juárez, Cándido, Illa, Isabel, and Querol, Luis

Published
2021
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4. Clinical and therapeutic features of myasthenia gravis in adults based on age at onset

Author

Cortés-Vicente, Elena, Álvarez-Velasco, Rodrigo, Segovia, Sonia, Paradas, Carmen, Casasnovas, Carlos, Guerrero-Sola, Antonio, Pardo, Julio, Ramos-Fransi, Alba, Sevilla, Teresa, López de Munain, Adolfo, Gómez, Maria Teresa, Jericó, Ivonne, Gutiérrez-Gutiérrez, Gerardo, Pelayo-Negro, Ana Lara, Martín, María Asunción, Mendoza, María Dolores, Morís, Germán, Rojas-Garcia, Ricard, Díaz-Manera, Jordi, Querol, Luis, Gallardo, Eduard, Vélez, Beatriz, Albertí, María Antonia, Galán, Lucía, García-Sobrino, Tania, Martínez-Piñeiro, Alicia, Lozano-Veintimilla, Ana, Fernández-Torrón, Roberto, Cano-Abascal, Ángel, and Illa, Isabel

Published
2020
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5. Characterizing SOD1 mutations in Spain. The impact of genotype, age, and sex in the natural history of the disease

Author

Instituto de Salud Carlos III, European Commission, Comunidad de Madrid, Ministerio de Sanidad (España), Centro de Investigación Biomédica en Red Enfermedades Raras (España), Centro Investigación Biomédica en Red Enfermedades Neurodegenerativas (España), Pérez-Tur, Jordi [0000-0002-9111-1712], Vázquez-Costa, Juan F., Borrego-Hernández, Daniel, Paradas, Carmen, Gómez-Caravaca, María Teresa, Rojas-García, Ricardo, Varona, Luis, Povedano, Mónica, García-Sobrino, Tania, Jericó Pascual, Ivonne, Gutierrez, Antonio, Riancho, Javier, Turón-Sans, Janina, Assialioui, Abdelilah, Pérez-Tur, Jordi, Sevilla, Teresa, Esteban Pérez, Jesús, García-Redondo, Alberto, Instituto de Salud Carlos III, European Commission, Comunidad de Madrid, Ministerio de Sanidad (España), Centro de Investigación Biomédica en Red Enfermedades Raras (España), Centro Investigación Biomédica en Red Enfermedades Neurodegenerativas (España), Pérez-Tur, Jordi [0000-0002-9111-1712], Vázquez-Costa, Juan F., Borrego-Hernández, Daniel, Paradas, Carmen, Gómez-Caravaca, María Teresa, Rojas-García, Ricardo, Varona, Luis, Povedano, Mónica, García-Sobrino, Tania, Jericó Pascual, Ivonne, Gutierrez, Antonio, Riancho, Javier, Turón-Sans, Janina, Assialioui, Abdelilah, Pérez-Tur, Jordi, Sevilla, Teresa, Esteban Pérez, Jesús, and García-Redondo, Alberto

Abstract

Introduction: The aim of this study is to describe the frequency and distribution of SOD1 mutations in Spain, and to explore those factors contributing to their phenotype and prognosis. Methods: Seventeen centres shared data on amyotrophic lateral sclerosis (ALS) patients carrying pathogenic or likely pathogenic SOD1 variants. Multivariable models were used to explore prognostic modifiers. Results: In 144 patients (from 88 families), 29 mutations (26 missense, 2 deletion/insertion and 1 frameshift) were found in all 5 exons of SOD1, including 7 novel mutations. 2.6% of ALS patients (including 17.7% familial and 1.3% sporadic) were estimated to carry SOD1 mutations. Its frequency varied considerably between regions, due to founder events. The most frequent mutation was p.Gly38Arg (n = 58), followed by p.Glu22Gly (n = 11), p.Asn140His (n = 10), and the novel p.Leu120Val (n = 10). Most mutations were characterized by a protracted course, and some of them by atypical phenotypes. Older age of onset was independently associated with faster disease progression (exp(Estimate) = 1.03 [0.01, 0.05], p = 0.001) and poorer survival (HR = 1.05 [1.01, 1.08], p = 0.007), regardless of the underlying mutation. Female sex was independently associated to faster disease progression (exp(Estimate) = 2.1 [1.23, 3.65], p = 0.012) in patients carrying the p.Gly38Arg mutation, resulting in shorter survival compared with male carriers (236 vs 301 months). Conclusions: These data may help to evaluate the efficacy of SOD1 targeted treatments, and to expand the number of patients that might benefit from these treatments.

Published
2023

7. Drug-refractory myasthenia gravis: Clinical characteristics, treatments, and outcome

Author

Neurociencias, Neurozientziak, Cortés Vicente, Elena, Álvarez Velasco, Rodrigo, Pla Junca, Francesc, Rojas García, Ricard, Paradas, Carmen, Sevilla, Teresa, Casasnovas, Carlos, Gómez Caravaca, María Teresa, Pardo Fernández, Julio, Ramos Fransi, Alba, Pelayo Negro, Ana Lara, Gutiérrez Gutiérrez, G., Turón Sans, Janina, López de Munain Arregui, Adolfo José, Guerrero Sola, Antonio, Jericó, Ivonne, Martín, María Asunción, Mendoza, María Dolores, Morís de la Tassa, G., Vélez Gómez, Beatriz, García Sobrino, Tania, Pascual Goñi, Elba, Reyes Leiva, David, Illa, Isabel, Gallardo, Eduard, Neurociencias, Neurozientziak, Cortés Vicente, Elena, Álvarez Velasco, Rodrigo, Pla Junca, Francesc, Rojas García, Ricard, Paradas, Carmen, Sevilla, Teresa, Casasnovas, Carlos, Gómez Caravaca, María Teresa, Pardo Fernández, Julio, Ramos Fransi, Alba, Pelayo Negro, Ana Lara, Gutiérrez Gutiérrez, G., Turón Sans, Janina, López de Munain Arregui, Adolfo José, Guerrero Sola, Antonio, Jericó, Ivonne, Martín, María Asunción, Mendoza, María Dolores, Morís de la Tassa, G., Vélez Gómez, Beatriz, García Sobrino, Tania, Pascual Goñi, Elba, Reyes Leiva, David, Illa, Isabel, and Gallardo, Eduard

Abstract

[EN] Objective: To describe the clinical characteristics and outcomes in patients with refractory myasthenia gravis (MG) and to determine the effectiveness and side effects of the drugs used for their treatment. Methods: This observational retrospective cross-sectional multicenter study was based on data from the Spanish MG Registry (NMD-ES). Patients were considered refractory when their MG Foundation of America post-interventional status (MGFA-PIS) was unchanged or worse after corticosteroids and two or more other immunosuppressive agents. Clinical and immunologic characteristics of drug-refractory patients, efficiency and toxicity of drugs used, and outcome (MGFA-PIS) at end of follow-up were studied. Results: We included 990 patients from 15 hospitals. Eighty-four patients (68 of 842 anti-acetylcholine receptor [AChR], 5 of 26 anti-muscle-specific tyrosine kinase [MusK], 10 of 120 seronegative, and 1 of 2 double-seropositive patients) were drug refractory. Drug-refractory patients were more frequently women (p < 0.0001), younger at onset (p < 0.0001), and anti-MuSK positive (p = 0.037). Moreover, they more frequently presented a generalized form of the disease, bulbar symptoms, and life-threatening events (p < 0.0001; p = 0.018; and p = 0.002, respectively) than non-drug-refractory patients. Mean follow-up was 9.8 years (SD 4.5). Twenty-four (50%) refractory patients had side effects to one or more of the drugs. At the end of follow-up, 42.9% of drug-refractory patients (42.6% of anti-AChR, 100% of anti-MuSK, and 10% of seronegative patients) and 79.8% of non-drug-refractory patients (p < 0.0001) achieved remission or had minimal manifestations. Eighty percent of drug-refractory-seronegative patients did not respond to any drug tested. Interpretation: In this study, 8.5% of MG patients were drug-refractory. New more specific drugs are needed to treat drug-refractory MG patients.

Published
2022

8. Drug-refractory myasthenia gravis: Clinical characteristics, treatments, and outcome

Author

Instituto de Salud Carlos III, European Commission, Centro de Investigación Biomédica en Red Enfermedades Raras (España), Cortés-Vicente, Elena [0000-0002-1428-1072], Casasnovas, Carlos0000-0003-1170-2676, Pascual-Goñi, Elba [0000-0001-7336-4305], Cortés-Vicente, Elena, Álvarez-Velasco, Rodrigo, Pla Junca, Francesc, Rojas-Garcia, Ricard, Paradas, Carmen, Sevilla, Teresa, Casasnovas, Carlos, Gómez-Caravaca, María Teresa, Pardo, Julio, Ramos-Fransi, Alba, Pelayo-Negro, Ana L., Gutiérrez-Gutiérrez, Gerardo, Turon-Sans, Janina, López de Munain, Adolfo, Guerrero-Sola, Antonio, Jericó, Ivonne, Martín, María Asunción, Mendoza, María Dolores, Moris, Germán, Vélez Gómez, Beatriz, García-Sobrino, Tania, Pascual-Goñi, Elba, Reyes-Leiva, David, Illa, Isabel, Gallardo, Eduard, Instituto de Salud Carlos III, European Commission, Centro de Investigación Biomédica en Red Enfermedades Raras (España), Cortés-Vicente, Elena [0000-0002-1428-1072], Casasnovas, Carlos0000-0003-1170-2676, Pascual-Goñi, Elba [0000-0001-7336-4305], Cortés-Vicente, Elena, Álvarez-Velasco, Rodrigo, Pla Junca, Francesc, Rojas-Garcia, Ricard, Paradas, Carmen, Sevilla, Teresa, Casasnovas, Carlos, Gómez-Caravaca, María Teresa, Pardo, Julio, Ramos-Fransi, Alba, Pelayo-Negro, Ana L., Gutiérrez-Gutiérrez, Gerardo, Turon-Sans, Janina, López de Munain, Adolfo, Guerrero-Sola, Antonio, Jericó, Ivonne, Martín, María Asunción, Mendoza, María Dolores, Moris, Germán, Vélez Gómez, Beatriz, García-Sobrino, Tania, Pascual-Goñi, Elba, Reyes-Leiva, David, Illa, Isabel, and Gallardo, Eduard

Abstract

[Objective] To describe the clinical characteristics and outcomes in patients with refractory myasthenia gravis (MG) and to determine the effectiveness and side effects of the drugs used for their treatment., [Methods] This observational retrospective cross-sectional multicenter study was based on data from the Spanish MG Registry (NMD-ES). Patients were considered refractory when their MG Foundation of America post-interventional status (MGFA-PIS) was unchanged or worse after corticosteroids and two or more other immunosuppressive agents. Clinical and immunologic characteristics of drug-refractory patients, efficiency and toxicity of drugs used, and outcome (MGFA-PIS) at end of follow-up were studied., [Results] We included 990 patients from 15 hospitals. Eighty-four patients (68 of 842 anti-acetylcholine receptor [AChR], 5 of 26 anti-muscle-specific tyrosine kinase [MusK], 10 of 120 seronegative, and 1 of 2 double-seropositive patients) were drug refractory. Drug-refractory patients were more frequently women (p < 0.0001), younger at onset (p < 0.0001), and anti-MuSK positive (p = 0.037). Moreover, they more frequently presented a generalized form of the disease, bulbar symptoms, and life-threatening events (p < 0.0001; p = 0.018; and p = 0.002, respectively) than non-drug-refractory patients. Mean follow-up was 9.8 years (SD 4.5). Twenty-four (50%) refractory patients had side effects to one or more of the drugs. At the end of follow-up, 42.9% of drug-refractory patients (42.6% of anti-AChR, 100% of anti-MuSK, and 10% of seronegative patients) and 79.8% of non-drug-refractory patients (p < 0.0001) achieved remission or had minimal manifestations. Eighty percent of drug-refractory-seronegative patients did not respond to any drug tested., [Interpretation] In this study, 8.5% of MG patients were drug-refractory. New more specific drugs are needed to treat drug-refractory MG patients.

Published
2022

9. Characterizing SOD1 mutations in Spain: The impact of genotype, age and sex in the natural history of the disease.

Author

Vázquez‐Costa, Juan F., Borrego‐Hernández, Daniel, Paradas, Carmen, Gómez‐Caravaca, María Teresa, Rojas‐Garcia, Ricardo, Varona, Luis, Povedano, Mónica, García‐Sobrino, Tania, Jericó Pascual, Ivonne, Gutiérrez, Antonio, Riancho, Javier, Turon‐Sans, Janina, Assialioui, Abdelilah, Pérez‐Tur, Jordi, Sevilla, Teresa, Esteban Pérez, Jesús, García‐Redondo, Alberto, López, Alberto Andrés, Calabria, M. Dolores, and Díaz‐Marín, Carmen

Subjects
AMYOTROPHIC lateral sclerosis, GENETIC mutation, SERVER farms (Computer network management), GENOTYPES, MOTOR neuron diseases
Abstract

Background and purpose: The aim of this study was to describe the frequency and distribution of SOD1 mutations in Spain, and to explore factors contributing to their phenotype and prognosis. Methods: Seventeen centres shared data on amyotrophic lateral sclerosis (ALS) patients carrying pathogenic or likely pathogenic SOD1 variants. Multivariable models were used to explore prognostic modifiers. Results: In 144 patients (from 88 families), 29 mutations (26 missense, 2 deletion/insertion and 1 frameshift) were found in all five exons of SOD1, including seven novel mutations. A total of 2.6% of ALS patients (including 17.7% familial and 1.3% sporadic) were estimated to carry SOD1 mutations. The frequency of this mutation varied considerably among regions, due to founder events. The most frequent mutation was p.Gly38Arg (n = 58), followed by p.Glu22Gly (n = 11), p.Asn140His (n = 10), and the novel p.Leu120Val (n = 10). Most mutations were characterized by a protracted course, and some of them by atypical phenotypes. Older age of onset was independently associated with faster disease progression (exp[Estimate] = 1.03 [0.01, 0.05], p = 0.001) and poorer survival (hazard ratio 1.05 [1.01, 1.08], p = 0.007), regardless of the underlying mutation. Female sex was independently associated with faster disease progression (exp[Estimate] = 2.1 [1.23, 3.65], p = 0.012) in patients carrying the p.Gly38Arg mutation, resulting in shorter survival compared with male carriers (236 vs. 301 months). Conclusions: These data may help to evaluate the efficacy of SOD1 targeted treatments, and to expand the number of patients that might benefit from these treatments. [ABSTRACT FROM AUTHOR]

Published
2023
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10. Enfermedad de Charcot-Marie-Tooth: caracterización clínica, electrofisiológica y molecular en población Gallega

Author

García Sobrino, Tania, Castillo Sánchez, José, Pardo Fernández, Julio, Universidade de Santiago de Compostela. Escola de Doutoramento Internacional (EDIUS), and Universidade de Santiago de Compostela. Programa de Doutoramento en Investigación Clínica en Medicina

Subjects
Enfermedad de Charcot-Marie-Tooth, Investigación::32 Ciencias médicas::3205 Medicina interna::320507 Neurología [Materias], CMT1A, CMT, prevalencia, polineuropatía sensitivo motora hereditaria
Abstract

La enfermedad de Charcot-Marie-Tooth (CMT) es la neuropatía hereditaria más frecuente, con una prevalencia de 28 casos/100.000 habitantes. CMT es uno de los síndromes neurodegenerativos más complejos, con más de 80 genes identificados. OBJETIVO: Analizar la epidemiología genética de CMT en Galicia. Realizar una descripción fenotípica, electrofisiológica y molecular de la población con CMT en Galicia. Proponer un protocolo de diagnóstico genético para su aplicación en la práctica clínica. Estudio descriptivo de CMT en población adulta (>18 años) en Galicia. Se incluyen pacientes con CMT y seguimiento clínico en el servicio de Neurología de las diferentes Gerencias de Gestión. RESULTADOS: Identificamos 232 casos de CMT en Galicia (142 familias). La prevalencia de CMT fue de 10 casos/100.000 habitantes. La prevalencia de CMT desmielinizante fue de 6 casos/100.000 habitantes y para CMT axonal 3 casos/100.000 habitantes. El 60% de los casos mostró una herencia autosómica dominante y un 35% una herencia autosómica recesiva o fueron casos esporádicos. La causa más frecuente de CMT fue CMT1A (57%). Otras causas de CMT identificadas fueron CMTX1 (9%), CMT1B (7%), CMT2A (6%) y CMT2K (6%). Las formas desmielinizantes de CMT se agruparon en CMT1A (75%), CMT1B (9.2%), CMT4G (4%) y CMT1D (4%). En CMT2 observamos una amplia heterogeneidad clínica y genética, resultando CMT2A (26%), CMT2K (26%), CMTX1 (26%), mutaciones en BSCL2 (13%) y CMT2T (5.3%) las causas más frecuentes. Alcanzamos el diagnóstico molecular en el 93% de CMT desmielinizante y en un 47.5% de CMT axonal.

Published
2021

11. Charcot–Marie–Tooth disease due to MORC2 mutations in Spain

Author

Sivera, Rafael, primary, Lupo, Vincenzo, additional, Frasquet, Marina, additional, Argente‐Escrig, Herminia, additional, Alonso‐Pérez, Jorge, additional, Díaz‐Manera, Jordi, additional, Querol, Luis, additional, Mar García‐Romero, María, additional, Ignacio Pascual, Samuel, additional, García‐Sobrino, Tania, additional, Paradas, Carmen, additional, Francisco Vázquez‐Costa, Juan, additional, Muelas, Nuria, additional, Millet, Elvira, additional, Jesús Vílchez, Juan, additional, Espinós, Carmen, additional, and Sevilla, Teresa, additional

Published
2021
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12. Enfermedad de Charcot-Marie-Tooth: caracterización clínica, electrofisiológica y molecular en población Gallega

Author

Castillo Sánchez, José, Pardo Fernández, Julio, Universidade de Santiago de Compostela. Escola de Doutoramento Internacional (EDIUS), Universidade de Santiago de Compostela. Programa de Doutoramento en Investigación Clínica en Medicina, García Sobrino, Tania, Castillo Sánchez, José, Pardo Fernández, Julio, Universidade de Santiago de Compostela. Escola de Doutoramento Internacional (EDIUS), Universidade de Santiago de Compostela. Programa de Doutoramento en Investigación Clínica en Medicina, and García Sobrino, Tania

Abstract

La enfermedad de Charcot-Marie-Tooth (CMT) es la neuropatía hereditaria más frecuente, con una prevalencia de 28 casos/100.000 habitantes. CMT es uno de los síndromes neurodegenerativos más complejos, con más de 80 genes identificados. OBJETIVO: Analizar la epidemiología genética de CMT en Galicia. Realizar una descripción fenotípica, electrofisiológica y molecular de la población con CMT en Galicia. Proponer un protocolo de diagnóstico genético para su aplicación en la práctica clínica. Estudio descriptivo de CMT en población adulta (>18 años) en Galicia. Se incluyen pacientes con CMT y seguimiento clínico en el servicio de Neurología de las diferentes Gerencias de Gestión. RESULTADOS: Identificamos 232 casos de CMT en Galicia (142 familias). La prevalencia de CMT fue de 10 casos/100.000 habitantes. La prevalencia de CMT desmielinizante fue de 6 casos/100.000 habitantes y para CMT axonal 3 casos/100.000 habitantes. El 60% de los casos mostró una herencia autosómica dominante y un 35% una herencia autosómica recesiva o fueron casos esporádicos. La causa más frecuente de CMT fue CMT1A (57%). Otras causas de CMT identificadas fueron CMTX1 (9%), CMT1B (7%), CMT2A (6%) y CMT2K (6%). Las formas desmielinizantes de CMT se agruparon en CMT1A (75%), CMT1B (9.2%), CMT4G (4%) y CMT1D (4%). En CMT2 observamos una amplia heterogeneidad clínica y genética, resultando CMT2A (26%), CMT2K (26%), CMTX1 (26%), mutaciones en BSCL2 (13%) y CMT2T (5.3%) las causas más frecuentes. Alcanzamos el diagnóstico molecular en el 93% de CMT desmielinizante y en un 47.5% de CMT axonal.

Published
2021

13. Serum neurofilament light chain predicts long-term prognosis in Guillain-Barré syndrome patients

Author

Martín-Aguilar, Lorena, primary, Camps-Renom, Pol, additional, Lleixà, Cinta, additional, Pascual-Goñi, Elba, additional, Díaz-Manera, Jordi, additional, Rojas-García, Ricardo, additional, De Luna, Noemi, additional, Gallardo, Eduard, additional, Cortés-Vicente, Elena, additional, Muñoz, Laia, additional, Alcolea, Daniel, additional, Lleó, Alberto, additional, Casasnovas, Carlos, additional, Homedes, Christian, additional, Gutiérrez-Gutiérrez, Gerardo, additional, Jimeno-Montero, María Concepción, additional, Berciano, José, additional, Sedano-Tous, María José, additional, García-Sobrino, Tania, additional, Pardo-Fernández, Julio, additional, Márquez-Infante, Celedonio, additional, Rojas-Marcos, Iñigo, additional, Jericó-Pascual, Ivonne, additional, Martínez-Hernández, Eugenia, additional, Morís de la Tassa, Germán, additional, Domínguez-González, Cristina, additional, Illa, Isabel, additional, and Querol, Luis, additional

Published
2020
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14. Muscle MRI in a large cohort of patients with oculopharyngeal muscular dystrophy

Author

Alonso-Jimenez, Alicia, Kroon, Rosemarie H M J M, Alejaldre-Monforte, Aida, Nuñez-Peralta, Claudia, Horlings, Corinne G C, van Engelen, Baziel G M, Olivé, Montse, González, Laura, Verges-Gil, Enric, Paradas, Carmen, Márquez, Celedonio, Garibaldi, Matteo, Gallano, Pía, Rodriguez, Maria José, Gonzalez-Quereda, Lidia, Dominguez Gonzalez, Cristina, Vissing, John, Fornander, Freja, Eisum, Anne-Sofie Vibæk, García-Sobrino, Tania, Pardo, Julio, García-Figueiras, Roberto, Muelas, Nuria, Vilchez, Juan Jesús, Kapetanovic, Solange, Tasca, Giorgio, Monforte, Mauro, Ricci, Enzo, Gomez, María Teresa, Bevilacqua, Jorge Alfredo, Diaz-Jara, Jorge, Zamorano, Ivonne Ingrid, Carlier, Robert Yves, Laforet, Pascal, Pelayo-Negro, Ana, Ramos-Fransi, Alba, Martínez, Amaia, Marini-Bettolo, Chiara, Straub, Volker, Gutiérrez, Gerardo, Stojkovic, Tanya, Martín, María Asunción, Morís, Germán, Fernández-Torrón, Roberto, Lopez De Munaín, Adolfo, Cortes-Vicente, Elena, Querol, Luis, Rojas-García, Ricardo, Illa, Isabel, Diaz-Manera, Jordi, Alonso-Jimenez, Alicia, Kroon, Rosemarie H M J M, Alejaldre-Monforte, Aida, Nuñez-Peralta, Claudia, Horlings, Corinne G C, van Engelen, Baziel G M, Olivé, Montse, González, Laura, Verges-Gil, Enric, Paradas, Carmen, Márquez, Celedonio, Garibaldi, Matteo, Gallano, Pía, Rodriguez, Maria José, Gonzalez-Quereda, Lidia, Dominguez Gonzalez, Cristina, Vissing, John, Fornander, Freja, Eisum, Anne-Sofie Vibæk, García-Sobrino, Tania, Pardo, Julio, García-Figueiras, Roberto, Muelas, Nuria, Vilchez, Juan Jesús, Kapetanovic, Solange, Tasca, Giorgio, Monforte, Mauro, Ricci, Enzo, Gomez, María Teresa, Bevilacqua, Jorge Alfredo, Diaz-Jara, Jorge, Zamorano, Ivonne Ingrid, Carlier, Robert Yves, Laforet, Pascal, Pelayo-Negro, Ana, Ramos-Fransi, Alba, Martínez, Amaia, Marini-Bettolo, Chiara, Straub, Volker, Gutiérrez, Gerardo, Stojkovic, Tanya, Martín, María Asunción, Morís, Germán, Fernández-Torrón, Roberto, Lopez De Munaín, Adolfo, Cortes-Vicente, Elena, Querol, Luis, Rojas-García, Ricardo, Illa, Isabel, and Diaz-Manera, Jordi

Abstract

BACKGROUND AND OBJECTIVE: Oculopharyngeal muscular dystrophy (OPMD) is a genetic disorder caused by an abnormal expansion of GCN triplets within the PABPN1 gene. Previous descriptions have focused on lower limb muscles in small cohorts of patients with OPMD, but larger imaging studies have not been performed. Previous imaging studies have been too small to be able to correlate imaging findings to genetic and clinical data.METHODS: We present cross-sectional, T1-weighted muscle MRI and CT-scan data from 168 patients with genetically confirmed OPMD. We have analysed the pattern of muscle involvement in the disease using hierarchical analysis and presented it as heatmaps. Results of the scans were correlated with genetic and clinical data.RESULTS: Fatty replacement was identified in 96.7% of all symptomatic patients. The tongue, the adductor magnus and the soleus were the most commonly affected muscles. Muscle pathology on MRI correlated positively with disease duration and functional impairment.CONCLUSIONS: We have described a pattern that can be considered characteristic of OPMD. An early combination of fat replacement in the tongue, adductor magnus and soleus can be helpful for differential diagnosis. The findings suggest the natural history of the disease from a radiological point of view. The information generated by this study is of high diagnostic value and important for clinical trial development.

Published
2019

15. Proceso asistencial integrado de esclerosis lateral amiotrófica

Author

Antelo Pose, Ana María, Blanco Vázquez, Olga Patricia, Barreiro Mosquera, José Luis, Cantón Blanco, Ana, Castro Vieites, José Luis, Dieguez Varela, Carina, Domínguez Martínez, Damaris, Escobar Lago, May, Fernández Benito, José, Ferro Gómez, Belén, Fraga Bau, Arturo, Garabal, Jessica, García Álvarez, Miguel Anxo, García Estévez, Daniel Apolinar, García Sobrino, Tania, Guijarro del Amo, Mónica, Hermida Porto, Leticia, Lorenzo González, José Ramón, Mederer Hengstl, Susana, Mosteiro Añón, María del Mar, Naveiro Soneira, Jesús Javier, Núñez del Río, Inés, Pardo Fernández, Julio, Perez Sousa, María Celia, Pérez Tenreiro, Marina, Prieto González, José María, Ricoy Gabaldón, Jorge, Tovar Bobo, Margarita, Valiño Lopez, Paz, and Zamarrón Sanz, Carlos

Subjects
Adult, Coordinación asistencial, Social Work, Sclerosis, protocolos clínicos, respiración artificial, Rehabilitation, Amyotrophic Lateral Sclerosis, Psychology, Clinical, psicología clínica, esclerosis, Nutritional Status, enfermedad de la neurona motora, Enfermedades de la médula espinal, rehabilitación, adulto, Respiration, Artificial, trabajo social, Enfermedades neurodegenerativas, Diagnosis, Differential, estado nutricional, Clinical Protocols, esclerosis lateral amiotrófica, Motor Neuron Disease, diagnóstico diferencial
Abstract

O proceso asistencial integrado da esclerose lateral amiotrófica, elaborouse co obxectivo de crear un proceso de traballo común en todas as áreas para facilitar a asistencia sanitaria ás persoas diagnosticadas desta enfermidade. Establécense actuacións como o asesoramento continuo, as consultas en acto único, a coordinación asistencial, tanto entre especialidades como coa atención primaria e a coordinación administrativa do sistema socio sanitario. Neste proceso participaron profesionais das diferentes áreas sanitarias especialistas en neuroloxía, endocrinoloxía, neumoloxía, psicoloxía clínica, rehabilitación, traballo social e hospitalización a domicilio El proceso asistencial integrado de la esclerosis lateral amiotrófica, se elaboró con el objetivo de crear un proceso de trabajo común en todas las áreas para facilitar la asistencia sanitaria a las personas diagnosticadas de esta enfermedad. Se establecen actuaciones como el asesoramiento continuo, las consultas en acto único, la coordinación asistencial, tanto entre especialidades como con la atención primaria y la coordinación administrativa del sistema socio sanitario. En este proceso participaron profesionales de las diferentes áreas sanitarias especialistas en neurología, endocrinología, neumología, psicología clínica, rehabilitación, trabajo social y hospitalización a domicilio

Published
2018

16. Serum neurofilament light chain predicts long-term prognosis in Guillain-Barré syndrome patients.

Author

Martín-Aguilar, Lorena, Camps-Renom, Pol, Lleixà, Cinta, Pascual-Goñi, Elba, Díaz-Manera, Jordi, Rojas-García, Ricardo, De Luna, Noemi, Gallardo, Eduard, Cortés-Vicente, Elena, Muñoz, Laia, Alcolea, Daniel, Lleó, Alberto, Casasnovas, Carlos, Homedes, Christian, Gutiérrez-Gutiérrez, Gerardo, Concepción Jimeno-Montero, María, Berciano, José, José Sedano-Tous, María, García-Sobrino, Tania, and Pardo-Fernández, Julio

Subjects
POLYNEUROPATHIES, GUILLAIN-Barre syndrome, CYTOPLASMIC filaments, FORECASTING, INSTITUTIONAL review boards, PROGNOSIS
Published
2021
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17. Muscle MRI in a large cohort of patients with oculopharyngeal muscular dystrophy

Author

Alonso-Jimenez, Alicia, primary, Kroon, Rosemarie H M J M, additional, Alejaldre-Monforte, Aida, additional, Nuñez-Peralta, Claudia, additional, Horlings, Corinne G C, additional, van Engelen, Baziel G M, additional, Olivé, Montse, additional, González, Laura, additional, Verges-Gil, Enric, additional, Paradas, Carmen, additional, Márquez, Celedonio, additional, Garibaldi, Matteo, additional, Gallano, Pía, additional, Rodriguez, Maria José, additional, Gonzalez-Quereda, Lidia, additional, Dominguez Gonzalez, Cristina, additional, Vissing, John, additional, Fornander, Freja, additional, Eisum, Anne-Sofie Vibæk, additional, García-Sobrino, Tania, additional, Pardo, Julio, additional, García-Figueiras, Roberto, additional, Muelas, Nuria, additional, Vilchez, Juan Jesús, additional, Kapetanovic, Solange, additional, Tasca, Giorgio, additional, Monforte, Mauro, additional, Ricci, Enzo, additional, Gomez, María Teresa, additional, Bevilacqua, Jorge Alfredo, additional, Diaz-Jara, Jorge, additional, Zamorano, Ivonne Ingrid, additional, Carlier, Robert Yves, additional, Laforet, Pascal, additional, Pelayo-Negro, Ana, additional, Ramos-Fransi, Alba, additional, Martínez, Amaia, additional, Marini-Bettolo, Chiara, additional, Straub, Volker, additional, Gutiérrez, Gerardo, additional, Stojkovic, Tanya, additional, Martín, María Asunción, additional, Morís, Germán, additional, Fernández-Torrón, Roberto, additional, Lopez De Munaín, Adolfo, additional, Cortes-Vicente, Elena, additional, Querol, Luis, additional, Rojas-García, Ricardo, additional, Illa, Isabel, additional, and Diaz-Manera, Jordi, additional

Published
2018
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18. Characterising the phenotype and mode of inheritance of patients with inherited peripheral neuropathies carrying MME mutations

Author

Lupo, Vincenzo, primary, Frasquet, Marina, additional, Sánchez-Monteagudo, Ana, additional, Pelayo-Negro, Ana Lara, additional, García-Sobrino, Tania, additional, Sedano, María José, additional, Pardo, Julio, additional, Misiego, Mercedes, additional, García-García, Jorge, additional, Sobrido, María Jesús, additional, Martínez-Rubio, María Dolores, additional, Chumillas, María José, additional, Vílchez, Juan Jesús, additional, Vázquez-Costa, Juan Francisco, additional, Espinós, Carmen, additional, and Sevilla, Teresa, additional

Published
2018
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19. Distribution and genotype-phenotype correlation of GDAP1 mutations in Spain

Author

Sivera, Rafael, primary, Frasquet, Marina, additional, Lupo, Vincenzo, additional, García-Sobrino, Tania, additional, Blanco-Arias, Patricia, additional, Pardo, Julio, additional, Fernández-Torrón, Roberto, additional, de Munain, Adolfo López, additional, Márquez-Infante, Celedonio, additional, Villarreal, Liliana, additional, Carbonell, Pilar, additional, Rojas-García, Ricard, additional, Segovia, Sonia, additional, Illa, Isabel, additional, Frongia, Anna Lia, additional, Nascimento, Andrés, additional, Ortez, Carlos, additional, García-Romero, María del Mar, additional, Pascual, Samuel Ignacio, additional, Pelayo-Negro, Ana Lara, additional, Berciano, José, additional, Guerrero, Antonio, additional, Casasnovas, Carlos, additional, Camacho, Ana, additional, Esteban, Jesús, additional, Chumillas, María José, additional, Barreiro, Marisa, additional, Díaz, Carmen, additional, Palau, Francesc, additional, Vílchez, Juan Jesús, additional, Espinós, Carmen, additional, and Sevilla, Teresa, additional

Published
2017
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20. Distribution and genotype-phenotype correlation of GDAP1 mutations in Spain

Author

Sivera, Rafael, Frasquet, Marina, Lupo, Vincenzo, García-Sobrino, Tania, Blanco-Arias, Patricia, Pardo, Julio, Fernández-Torrón, Roberto, de Munain, Adolfo López, Márquez-Infante, Celedonio, Villarreal, Liliana, Carbonell, Pilar, Rojas-Garcia, Ricard, Segovia, Sonia, Illa, Isabel, Frongia, Anna Lia, Nascimento, Andrés, Ortez, Carlos, García-Romero, María del Mar, Pascual, Samuel Ignacio, Pelayo-Negro, Ana Lara, Berciano, José, Guerrero, Antonio, Casasnovas, Carlos, Camacho, Ana, Esteban, Jesús, Chumillas, María José, Barreiro, Marisa, Díaz, Carmen, Palau, Francesc, Vílchez, Juan J, Espinós, Carmen, Sevilla, Teresa, Universitat Autònoma de Barcelona, Sivera, Rafael, Frasquet, Marina, Lupo, Vincenzo, García-Sobrino, Tania, Blanco-Arias, Patricia, Pardo, Julio, Fernández-Torrón, Roberto, de Munain, Adolfo López, Márquez-Infante, Celedonio, Villarreal, Liliana, Carbonell, Pilar, Rojas-Garcia, Ricard, Segovia, Sonia, Illa, Isabel, Frongia, Anna Lia, Nascimento, Andrés, Ortez, Carlos, García-Romero, María del Mar, Pascual, Samuel Ignacio, Pelayo-Negro, Ana Lara, Berciano, José, Guerrero, Antonio, Casasnovas, Carlos, Camacho, Ana, Esteban, Jesús, Chumillas, María José, Barreiro, Marisa, Díaz, Carmen, Palau, Francesc, Vílchez, Juan J, Espinós, Carmen, Sevilla, Teresa, and Universitat Autònoma de Barcelona

Abstract

Mutations in the GDAP1 gene can cause Charcot-Marie-Tooth disease. These mutations are quite rare in most Western countries but not so in certain regions of Spain or other Mediterranean countries. This cross-sectional retrospective multicenter study analyzed the clinical and genetic characteristics of patients with GDAP1 mutations across Spain. 99 patients were identified, which were distributed across most of Spain, but especially in the Northwest and Mediterranean regions. The most common genotypes were p.R120W (in 81% of patients with autosomal dominant inheritance) and p.Q163X (in 73% of autosomal recessive patients). Patients with recessively inherited mutations had a more severe phenotype, and certain clinical features, like dysphonia or respiratory dysfunction, were exclusively detected in this group. Dominantly inherited mutations had prominent clinical variability regarding severity, including 29% of patients who were asymptomatic. There were minor clinical differences between patients harboring specific mutations but not when grouped according to localization or type of mutation. This is the largest clinical series to date of patients with GDAP1 mutations, and it contributes to define the genetic distribution and genotype-phenotype correlation in this rare form of CMT.

Published
2017

26. Neuropathy in Tangier disease mimicking leprosy

Author

Pardo Fernández, Julio, Beiras Iglesias, Andrés, Lema Bouzas, Manuela, García Sobrino, Tania, Rabuñal Martínez, María, and Montiel Carracedo, María Dolores

Published
2014

29. Which hand moves our patients with temporal lobe epilepsy?

Author

Corredera García, Enrique, Rodríguez Osorio, Xiana, Pardo Parrado, María, Peleteiro Fernández, Manuel, López Ferreiro, Ana, García Sobrino, Tania, Santamaría Cadavid, María, and Fernández Pajarín, Gustavo

Published
2013

36. Caracterización clínica y hallazgos en la biopsia cutánea de una serie de pacientes con neuropatía de fibra fina

Author

Mederer Fernández, Tania Isabel, Pardo Fernández, Julio, Sopeña Pérez-Argüelles, Bernardo, García Sobrino, Tania, and Universidade de Santiago de Compostela. Facultade de Medicina e Odontoloxía

Subjects
NFF, Neuropatía de fibra fina, SFN, Sistema nervioso periférico, Small fiber neuropathy, Peripheral nerve system
Abstract

Traballo de Fin de Grao en Medicina. Curso 2019-2020. La neuropatía de fibra fina (NFF) es un trastorno del sistema nervioso periférico en el que se afectan de forma selectiva las fibras nerviosas mielínicas finas (Ad) y amielínicas (C). Clínicamente cursa con dolor neuropático y síntomas autonómicos y la exploración neurológica es, con frecuencia, anodina. Los estudios de conducción nerviosa son, por definición, normales, y la prueba diagnóstica de elección es la biopsia cutánea, que permite el estudio de la densidad de fibras nerviosas intraepidérmicas (DFNIE). Objetivos: El objetivo del trabajo es analizar el perfil demográfico, clínico y la DFNIE de una serie de pacientes diagnosticados de NFF. También se analizarán las posibles asociaciones entre las variables recogidas y los distintos subgrupos de pacientes en función de su etiología, patrón de neuropatía y existencia de fibromialgia. Material y métodos: Estudio descriptivo, retrospectivo de una serie de 18 pacientes diagnosticados de NFF mediante biopsia cutánea en la Unidad de Enfermedades Neuromusculares del Hospital Clínico de Santiago de Compostela entre 2017 y 2019. Se recogieron datos sociodemográficos, tiempo de evolución, datos de la historia clínica (antecedentes, tratamientos recibidos para el control del dolor, síntomas, exploración neurológica) y resultados de las pruebas complementarias. Resultados y conclusiones: EL 72% de los pacientes eran varones y la edad media de la serie fue de 57 años. Para controlar el dolor, los pacientes recibieron una media de 8.6 fármacos. El patrón longituddependiente fue el más frecuentemente identificado (67%). En un 61% de los pacientes no se logró identificar una causa subyacente y fueron diagnosticados de NFF idiopática. Un 22% de los casos tenían un diagnóstico previo de fibromialgia. La NFF tiene un marcado retraso diagnóstico (4.6 años de media), probablemente debido a la escasa disponibilidad de la infraestructura necesaria para el estudio de la DFNIE, el actual gold standard para el diagnóstico de esta entidad. A neuropatía de fibra fina ( NFF) é un trastorno do sistema nervioso periférico no que se afectan de forma selectiva as fibras nerviosas mielínicas finas (Ad) e amielínicas ( C). Clinicamente cursa con dor neuropática e síntomas autonómicos e a exploración neurolóxica é, con frecuencia, anodina. Os estudos de condución nerviosa son, por definición, normais, e a proba diagnóstica de elección é a biopsia cutánea, que permite o estudo da densidade de fibras nerviosas intraepidérmicas (DFNIE). Obxectivos: O obxectivo do traballo é analizar o perfil demográfico, clínico e a DFNIE dunha serie de pacientes diagnosticados de NFF. Tamén se analizarán as posibles asociacións entre as variables recollidas e os distintos subgrupos de pacientes en función da súa etioloxía, patrón da neuropatía e existencia de fibromialxia. Material e métodos: Estudo descritivo, retrospectivo dunha serie de 18 pacientes diagnosticados de NFF mediante biopsia cutánea na Unidade de Enfermidades Neuromusculares do Hospital Clínico de Santiago de Compostela entre 2017 e 2019. Recolléronse datos sociodemográficos, tempo de evolución, datos da historia clínica (antecedentes, tratamentos recibidos para o control da dor, síntomas, exploración neurolóxica) e resultados das probas complementarias. Resultados e conclusións: A maioría dos pacientes eran homes (72%) e a idade media da serie foi de 57 anos. Para o control da dor, os pacientes recibiron unha media de 8.6 fármacos. O patrón lonxitudedependente foi o máis frecuentemente identificado (67%). Nun 61% dos pacientes non se logrou identificar unha causa subxacente e foron diagnosticados de NFF idiopática. Un 22% dos casos tiñan un diagnóstico previo de fibromialxia. A NFF ten un marcado atraso diagnóstico (4.6 anos de media), probablemente debido á escasa dispoñibilidade da infraestrutura necesaria para o estudo da DFNIE, o actual gold standard para o diagnóstico desta entidade. Small fiber neuropathy (SFN) is a disorder of the peripheral nerve system characterized by selective damage of the thinly myelinated Aδ and unmyelinated C fibers, which causes neuropathic pain and autonomic symptoms. Neurological examination is usually unrewarding. Nerve Conduction Studies are typically normal and currently the skin biopsy with intraepidermal nerve fiber density (IENFD) measurements is the diagnostic modality of choice. Objectives: The aim of our work is to analyze the clinical, epidemiological and IENFD findings in a series of patients with definite SFN. Possible associations between the variables collected and the different patient subgroups in terms of etiology, neuropathy pattern, and the existence of fibromyalgia will also be analyzed. Material and Methods: A series of 18 patients diagnosed with SFN were seen between 2017 and 2019 and studied retrospectively in the Neuromuscular Unit of the University Hospital of Santiago de Compostela. All of them underwent detailed clinical history recording and sociodemographic data were collected, as well as data on time course, clinical characteristics, treatments received for neuropathic pain management, findings on the neurological examination and the results of the performed tests. Particular interest was placed in the IENFD quantification obtained via skin biopsy. Results and Conclusion: Most of the patients were males (72%) and the mean age was 57 years. To manage pain, patients received an average of 8.6 different drugs. The length-dependent pattern was the most frequently found in skin biopsy (67%). In 61% of the whole series no specific cause could be found and patients were therefore labelled as idiopathic SFN. 22% of the cases had been previously diagnosed with fibromyalgia. The diagnostic delay (mean 4.6 years) associated with SFN is probably due to the lack of diagnostic facilities required for the intra-epidermal nerve fiber density measurement, the current gold standard technique for the diagnosis of SFN.

Published
2020

37. Muscle MRI in a large cohort of patients with oculopharyngeal muscular dystrophy.

Author

Alonso-Jimenez A, Kroon RHMJM, Alejaldre-Monforte A, Nuñez-Peralta C, Horlings CGC, van Engelen BGM, Olivé M, González L, Verges-Gil E, Paradas C, Márquez C, Garibaldi M, Gallano P, Rodriguez MJ, Gonzalez-Quereda L, Dominguez Gonzalez C, Vissing J, Fornander F, Eisum AV, García-Sobrino T, Pardo J, García-Figueiras R, Muelas N, Vilchez JJ, Kapetanovic S, Tasca G, Monforte M, Ricci E, Gomez MT, Bevilacqua JA, Diaz-Jara J, Zamorano II, Carlier RY, Laforet P, Pelayo-Negro A, Ramos-Fransi A, Martínez A, Marini-Bettolo C, Straub V, Gutiérrez G, Stojkovic T, Martín MA, Morís G, Fernández-Torrón R, Lopez De Munaín A, Cortes-Vicente E, Querol L, Rojas-García R, Illa I, and Diaz-Manera J

Subjects
Adult, Cohort Studies, Cross-Sectional Studies, Female, Humans, Magnetic Resonance Imaging, Male, Middle Aged, Muscle, Skeletal pathology, Muscular Dystrophy, Oculopharyngeal complications, Muscular Dystrophy, Oculopharyngeal pathology, Tomography, X-Ray Computed, Muscle, Skeletal diagnostic imaging, Muscular Dystrophy, Oculopharyngeal diagnostic imaging
Abstract

Background and Objective: Oculopharyngeal muscular dystrophy (OPMD) is a genetic disorder caused by an abnormal expansion of GCN triplets within the PABPN1 gene. Previous descriptions have focused on lower limb muscles in small cohorts of patients with OPMD, but larger imaging studies have not been performed. Previous imaging studies have been too small to be able to correlate imaging findings to genetic and clinical data., Methods: We present cross-sectional, T1-weighted muscle MRI and CT-scan data from 168 patients with genetically confirmed OPMD. We have analysed the pattern of muscle involvement in the disease using hierarchical analysis and presented it as heatmaps. Results of the scans were correlated with genetic and clinical data., Results: Fatty replacement was identified in 96.7% of all symptomatic patients. The tongue, the adductor magnus and the soleus were the most commonly affected muscles. Muscle pathology on MRI correlated positively with disease duration and functional impairment., Conclusions: We have described a pattern that can be considered characteristic of OPMD. An early combination of fat replacement in the tongue, adductor magnus and soleus can be helpful for differential diagnosis. The findings suggest the natural history of the disease from a radiological point of view. The information generated by this study is of high diagnostic value and important for clinical trial development., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2019. No commercial re-use. See rights and permissions. Published by BMJ.)

Published
2019
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38. [Rapidly progressing paraparesis secondary to a fibrosarcoma].

Author

García-Sobrino T, Rodríguez-Osorio X, Pardo M, Santamaría-Cadavid M, and Arias M

Subjects
Blood Loss, Surgical, Disease Progression, Fatal Outcome, Female, Fibrosarcoma blood supply, Fibrosarcoma diagnostic imaging, Fibrosarcoma pathology, Fibrosarcoma surgery, Hemorrhage etiology, Humans, Middle Aged, Neck Injuries complications, Neoplasm Invasiveness, Radiography, Skin Neoplasms blood supply, Skin Neoplasms diagnostic imaging, Skin Neoplasms pathology, Skin Neoplasms surgery, Subcutaneous Tissue pathology, Thoracic Vertebrae diagnostic imaging, Urinary Incontinence etiology, Fibrosarcoma complications, Paraparesis etiology, Skin Neoplasms complications, Spinal Cord Compression etiology, Thoracic Vertebrae pathology
Published
2014

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