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3. Cardiac complications in a geriatric population hospitalized with COVID-19: The OCTA-COVID cohort

Author

Ramos-Sánchez Mónica, Quezada-Feijoó Maribel, Jaramillo Javier, Lozano-Montoya Isabel, Toro Rocío, Ayala Rocío, and Gómez-Pavón Francisco Javier

Subjects
Aged, 80 and over, Heart Failure, Male, Aging, geriatric population, población geriatrica, pulmonary embolism, insuficiencia cardiaca, Medicine (miscellaneous), COVID-19, fibrilación auricular, Article, Hospitalization, congestive heart failure, Humans, Female, atrial fibrillation, Hospital Mortality, Acute Coronary Syndrome, Geriatrics and Gerontology, Aged, tromboembolismo pulmonar
Abstract

Introducción: La población geriátrica es especialmente vulnerable a la enfermedad por coronavirus (COVID-19) y sus posibles complicaciones. Nos propusimos analizar la incidencia de complicaciones cardiológicas en una población anciana hospitalizada por COVID-19. Métodos: Estudio longitudinal observacional prospectivo que incluyó a pacientes ≥ 75 años con diagnóstico de COVID-19 ingresados en el Servicio de Geriatría de marzo a mayo de 2020. Se recogieron variables epidemiológicas, geriátricas, clínicas y de laboratorio. Se documentaron eventos cardiovasculares, que incluyen fibrilación auricular (FA) de novo, síndrome coronario agudo (SCA), insuficiencia cardíaca congestiva (ICC), embolia pulmonar y muerte intrahospitalaria. Se realizó un seguimiento a los 12 meses, mediante entrevista telefónica y accediendo a la historia clínica electronica, recogiendo eventos cardíacos y mortalidad. Resultados: Se incluyeron 305 pacientes; 190 (62,3%) eran mujeres, con una mediana de edad de 87 años (RIQ (82 - 91)). Más de la mitad de los pacientes tenían antecedentes de enfermedad cardíaca, siendo la FA la más frecuente y afectando a 85 (27,9%) pacientes. Durante la hospitalización fallecieron 112 (36,7%) pacientes. Ochenta y nueve (29,2%) pacientes presentaron complicaciones cardíacas. La ICC aguda fue la más prevalente (46; 15,1%), seguida de la FA de nueva aparición (20; 6,5%), la embolia pulmonar (17; 5,6%) y el SCA (5; 1,6%). Los pacientes con complicaciones cardíacas tuvieron una estancia hospitalaria más prolongada (p

Published
2022

4. Peripheral microRNA panels to guide the diagnosis of familial cardiomyopathy

Author

Belmonte, Thalia, Mangas, Alipio, Calderón‐Domínguez, María, Quezada-Feijoo, Maribel, Ramos-Sánchez, Mónica, Campuzano, Oscar, Gómez, Silvia, Peña-Peña, María Luisa, Cubillos-Arango, Andres M., Domínguez, Fernando, Llorente-Cortés, Vicenta, Gonzalo-Calvo, David de, Toro, Rocío, Belmonte, Thalia, Mangas, Alipio, Calderón‐Domínguez, María, Quezada-Feijoo, Maribel, Ramos-Sánchez, Mónica, Campuzano, Oscar, Gómez, Silvia, Peña-Peña, María Luisa, Cubillos-Arango, Andres M., Domínguez, Fernando, Llorente-Cortés, Vicenta, Gonzalo-Calvo, David de, and Toro, Rocío

Abstract

Etiology-based diagnosis of dilated cardiomyopathy (DCM) is challenging. We evaluated whether peripheral microRNAs (miRNAs) could be used to characterize the DCM etiology. We investigated the miRNA plasma profiles of 254 subjects that comprised 5 groups: Healthy subjects (n = 70), idiopathic DCM patients (n = 55), ischemic DCM patients (n = 60) and 2 groups of patients with pathogenic variants responsible for familial DCM in the LMNA (LMNA, n = 37) and BAG3 (BAG3, n = 32) genes. Diagnostic performance was assessed using receiver operating characteristic curves. In a screening study (n = 30), 179 miRNAs robustly detected in plasma samples were profiled in idiopathic DCM and carriers of pathogenic variants. After filtering, 26 miRNA candidates were selected for subsequent quantification in the whole study population. In the validation study, a 6-miRNA panel identified familial DCM with an AUC (95% confidence interval [CI]) of 87.8 (82.0–93.6). The 6-miRNA panel also distinguished between specific DCM etiologies with AUCs ranging from 85.9 to 89.9. Only 1 to 10 of the subjects in the first and second tertiles of the 6-miRNA panel were patients with familial DCM. Additionally, a 5-miRNA panel showed an AUC (95% CI) of 87.5 (80.4–94.6) for the identification of carriers with pathogenic variants who were phenotypically negative for DCM. The 5-miRNA panel discriminated between carriers and healthy controls with AUCs ranging from 83.2 to 90.8. Again, only 1 to 10 of the subjects in the lowest tertiles of the 5-miRNA panel were carriers of pathogenic variants. In conclusion, miRNA signatures could be used to rule out patients with pathogenic variants responsible for DCM.

Published
2020

5. Emerging role of microRNAs in dilated cardiomyopathy: evidence regarding etiology

Author

Junta de Andalucía, European Commission, Ministerio de Economía y Competitividad (España), Calderón‐Domínguez, María, Belmonte, Thalia, Quezada-Feijoo, Maribel, Ramos-Sánchez, Mónica, Fernandez-Armenta, J., Pérez-Navarro, Amparo, Cesar, Sergi, Peña-Peña, María Luisa, Vea, Ángela, Llorente-Cortés, Vicenta, Mangas, Alipio, Gonzalo-Calvo, David de, Toro, Rocío, Junta de Andalucía, European Commission, Ministerio de Economía y Competitividad (España), Calderón‐Domínguez, María, Belmonte, Thalia, Quezada-Feijoo, Maribel, Ramos-Sánchez, Mónica, Fernandez-Armenta, J., Pérez-Navarro, Amparo, Cesar, Sergi, Peña-Peña, María Luisa, Vea, Ángela, Llorente-Cortés, Vicenta, Mangas, Alipio, Gonzalo-Calvo, David de, and Toro, Rocío

Abstract

Dilated cardiomyopathy (DCM) is a heart muscle disease characterized by ventricular dilation and systolic dysfunction in the absence of abnormal loading conditions or coronary artery disease. This cardiac disorder is a major health problem due to its high prevalence, morbidity, and mortality. DCM is a complex disease with a common phenotype but heterogeneous pathological mechanisms. Early etiological diagnosis and prognosis stratification is crucial for the clinical management of the patient. Advances in imaging technology and genetic tests have provided useful tools for clinical practice. Nevertheless, the assessment of the disease remains challenging. Novel noninvasive indicators are still needed to assist in decision-making. microRNAs (miRNAs), a group of small noncoding RNAs, have been identified as key mediators of cell biology. They are found in a stable form in body fluids and their concentration is altered in response to stress. Previous research has suggested that the miRNA signature constitutes a novel source of noninvasive biomarkers for a wide array of cardiovascular diseases. Specifically, several studies have reported the potential role of miRNAs as clinical indicators among the etiologies of DCM. However, this field has not been reviewed in detail. Here, we summarize the evidence of intracellular and circulating miRNAs in DCM and their usefulness in the development of novel diagnostic, prognostic and therapeutic approaches, with a focus on DCM etiology. Although the findings are still preliminary, due to methodological and technical limitations and the lack of robust population-based studies, miRNAs constitute a promising tool to assist in the clinical management of DCM.

Published
2020

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