Your search keyword '"José María Aguado Caballero"' showing total 2 results

1. Influence of non-osteoporotic treatments in patients on active anti-osteoporotic therapy: evidence from the OSTEOMED registry.

Author

Coco-Martín, María Begoña, Leal-Vega, Luis, Blázquez-Cabrera, José Antonio, Navarro, Amalia, Moro, María Jesús, Arranz-García, Francisca, Amérigo, María José, Sosa-Henríquez, Manuel, Vázquez, María Ángeles, Montoya, María José, Díaz-Curiel, Manuel, Olmos, José Manuel, Ruiz-Mambrilla, Marta, Filgueira-Rubio, José, Pérez-Castrillón, José Luis, on behalf of the OSTEOMED Group, Hernández-de Sosa, Nerea, Calero-Bernal, María Luz, Armengol-Sucarrats, Dolors, and de Escalante-Yanguas, Begoña

Subjects

DIPHOSPHONATES, DRUG therapy, BONE fracture prevention, OSTEOPOROSIS prevention, BONE metabolism, DRUG efficacy, ANTIHYPERTENSIVE agents, DIURETICS, STATINS (Cardiovascular agents), REPORTING of diseases, ANTIANDROGENS, THYROID hormones, ADRENOCORTICAL hormones, LETROZOLE, SEROTONIN uptake inhibitors, TERIPARATIDE, RETROSPECTIVE studies, OSTEOPOROSIS, RISK assessment, DISEASE relapse, PROTON pump inhibitors, BENZODIAZEPINES, GONADOTROPIN releasing hormone, DRUGS, DESCRIPTIVE statistics, LOGISTIC regression analysis, AROMATASE, ODDS ratio, ANABOLIC steroids, BONE fractures, LONGITUDINAL method, TRANQUILIZING drugs, DISEASE risk factors, EVALUATION

Abstract

Purpose: To evaluate the effect of different non-osteoporotic drugs on the increase or decrease in the risk of incident fragility fractures (vertebral, humerus or hip) in a cohort of patients diagnosed with osteoporosis on active anti-osteoporotic therapy. Methods: For this retrospective longitudinal study, baseline and follow-up data on prescribed non-osteoporotic treatments and the occurrence of vertebral, humerus or hip fractures in 993 patients from the OSTEOMED registry were analyzed using logistic regression models. The drugs evaluated with a possible beneficial effect were thiazides and statins, while the drugs evaluated with a possible harmful effect were antiandrogens, aromatase inhibitors, proton pump inhibitors, selective serotonin reuptake inhibitors, benzodiazepines, GnRH agonists, thyroid hormones, and oral and inhaled corticosteroids. Results: Logistic regression analyses indicated that no treatment significantly improved fracture risk, with the only treatments that significantly worsened fracture risk being letrozole (OR = 0.18, p-value = 0.03) and oral corticosteroids at doses ≤ 5 mg/day (OR = 0.16, p-value = 0.03) and > 5 mg/day (OR = 0.27, p-value = 0.04). Conclusion: The potential beneficial or detrimental effects of the different drugs evaluated on fracture risk are masked by treatment with anabolic or antiresorptive drugs that have a more potent action on bone metabolism, with two exceptions: letrozole and oral corticosteroids. These findings may have important clinical implications, as patients receiving these treatments are not fully protected by bisphosphonates, which may imply the need for more potent anti-osteoporotic drugs such as denosumab or teriparatide. [ABSTRACT FROM AUTHOR]

Published

2023

2. Comorbidity and osteoporotic fracture: approach through predictive modeling techniques using the OSTEOMED registry.

Author

Coco Martín, María Begoña, Leal Vega, Luis, Blázquez Cabrera, José Antonio, Navarro, Amalia, Moro, María Jesús, Arranz García, Francisca, Amérigo, María José, Sosa Henríquez, Manuel, Vázquez, María Ángeles, Montoya, María José, Díaz Curiel, Manuel, Olmos, José Manuel, Pérez Castrillón, José Luis, OSTEOMED Group, Filgueira Rubio, José, Sánchez Molini, Pilar, Aguado Caballero, José María, Armengol Sucarrats, Dolors, Calero Bernal, María Luz, and de Escalante Yanguas, Begoña

Subjects

THERAPEUTIC use of vitamin D, OSTEOPOROSIS treatment, REPORTING of diseases, PATIENT aftercare, SCIENTIFIC observation, AGE distribution, RETROSPECTIVE studies, TREATMENT effectiveness, SEX distribution, COMPARATIVE studies, DESCRIPTIVE statistics, STATISTICAL models, ARTIFICIAL neural networks, LOGISTIC regression analysis, ODDS ratio, BONE fractures, COMORBIDITY

Abstract

Purpose: To examine the response to anti-osteoporotic treatment, considered as incident fragility fractures after a minimum follow-up of 1 year, according to sex, age, and number of comorbidities of the patients. Methods: For this retrospective observational study, data from baseline and follow-up visits on the number of comorbidities, prescribed anti-osteoporotic treatment and vertebral, humerus or hip fractures in 993 patients from the OSTEOMED registry were analyzed using logistic regression and an artificial network model. Results: Logistic regression showed that the probability of reducing fractures for each anti-osteoporotic treatment considered was independent of sex, age, and the number of comorbidities, increasing significantly only in males taking vitamin D (OR = 7.918), patients without comorbidities taking vitamin D (OR = 4.197) and patients with ≥ 3 comorbidities taking calcium (OR = 9.412). Logistic regression correctly classified 96% of patients (Hosmer–Lemeshow = 0.492) compared with the artificial neural network model, which correctly classified 95% of patients (AUC = 0.6). Conclusion: In general, sex, age and the number of comorbidities did not influence the likelihood that a given anti-osteoporotic treatment improved the risk of incident fragility fractures after 1 year, but this appeared to increase when patients had been treated with risedronate, strontium or teriparatide. The two models used classified patients similarly, but predicted differently in terms of the probability of improvement, with logistic regression being the better fit. [ABSTRACT FROM AUTHOR]

Published

2022