Your search keyword '"Ramírez, Sara Pérez"' showing total 3 results

1. Anthracycline-induced cardiovascular toxicity: validation of the Heart Failure Association and International Cardio-Oncology Society risk score.

Author

Rivero-Santana, Borja, Saldaña-García, Jesús, Caro-Codón, Juan, Zamora, Pilar, Moliner, Pedro, Monzonis, Amparo Martínez, Zatarain, Eduardo, Álvarez-Ortega, Carlos, Gómez-Prieto, Pilar, Pernas, Sonia, Rodriguez, Isabel, Soto, Antonio Buño, Cadenas, Rosalía, Ozores, Patricia Palacios, Ramírez, Sara Pérez, Salvador, María Merino, Valbuena, Silvia, Gasso, Lucía Fernández, Juárez, Victor, and Severo, Andrea

Abstract

Background and Aims Baseline cardiovascular toxicity risk stratification is critical in cardio-oncology. The Heart Failure Association (HFA) and International Cardio-Oncology Society (ICOS) score aims to assess this risk but lacks real-life validation. This study validates the HFA-ICOS score for anthracycline-induced cardiovascular toxicity. Methods Anthracycline-treated patients in the CARDIOTOX registry (NCT02039622) were stratified by the HFA-ICOS score. The primary endpoint was symptomatic or moderate to severe asymptomatic cancer therapy-related cardiac dysfunction (CTRCD), with all-cause mortality and cardiovascular mortality as secondary endpoints. Results The analysis included 1066 patients (mean age 54 ± 14 years; 81.9% women; 24.5% ≥65 years). According to the HFA-ICOS criteria, 571 patients (53.6%) were classified as low risk, 333 (31.2%) as moderate risk, 152 (14.3%) as high risk, and 10 (0.9%) as very high risk. Median follow-up was 54.8 months (interquartile range 24.6–81.8). A total of 197 patients (18.4%) died, and 718 (67.3%) developed CTRCD (symptomatic: n = 45; moderate to severe asymptomatic: n = 24; and mild asymptomatic: n = 649). Incidence rates of symptomatic or moderate to severe symptomatic CTRCD and all-cause mortality significantly increased with HFA-ICOS score [hazard ratio 28.74, 95% confidence interval (CI) 9.33–88.5; P <.001, and hazard ratio 7.43, 95% CI 3.21–17.2; P <.001) for very high-risk patients. The predictive model demonstrated good calibration (Brier score 0.04, 95% CI 0.03–0.05) and discrimination (area under the curve 0.78, 95% CI 0.70–0.82; Uno's C -statistic 0.78, 95% CI 0.71–0.84) for predicting symptomatic or severe/moderate asymptomatic CTRCD at 12 months. Conclusions The HFA-ICOS score effectively categorizes patients by cardiovascular toxicity risk and demonstrates strong predictive ability for high-risk anthracycline-related cardiovascular toxicity and all-cause mortality. [ABSTRACT FROM AUTHOR]

Published

2025

2. 8. ¿CUÁL ES EL PAPEL DE LA IMAGEN CARDIACA EN LA VALORACIÓN BASAL DE PACIENTES QUE VAN A RECIBIR INMUNOTERAPIA? ANÁLISIS DEL REGISTRO SIR-CVT

Author

López, Silvia C. Valbuena, García, Jesús Saldaña, de los Monteros, Belén Terol Espinosa, de Castro Carpeño, Javier, Ramírez, Sara Pérez, García, Ana Martín, del Barco, Edel, Lozano, Teresa, Banaclocha, Natividad Martínez, Muñoz, Marinela Chaparro, Ibañez, Borja, Tocchetti, Carlo Gabrielle, Monzonís, Amparo Martínez, Nicolás, Eduardo Zataraín, and Fernández, Teresa López

Published

2023

3. Pharmacological cancer treatment and venous thromboembolism risk.

Author

Muñoz Martín AJ, Ramírez SP, Morán LO, Zamorano MR, Benéitez MCV, Salcedo IA, Escobar IG, and Fernández JMS

Abstract

Risk factors for cancer-associated thrombosis are commonly divided into three categories: patient-, cancer-, and treatment-related factors. Currently, different types of drugs are used in cancer treatment. Chemotherapy has been identified as an independent risk factor for venous thromboembolism (VTE). However, it should be noted, that the risk of VTE is not consistent among all cytotoxic agents. In addition, different supportive care drugs, such as erythropoiesis stimulating agents or granulocyte colony stimulating factors, and hormonotherapy have been associated to an increased risk of VTE. Immunotherapy and molecular-targeted therapies have significantly changed the treatment of cancer over the past decade. The main subtypes include tyrosine-kinase inhibitors, monoclonal antibodies, small molecules, and immunomodulatory agents. The relationship between VTE and targeted therapies remains largely unknown., (Published on behalf of the European Society of Cardiology. © The Author(s) 2020.)

Published

2020