Frailty syndrome often coexists with multimorbidity, sharing several risk factors and outcomes. Therefore, considering multimorbidity when exploring frailty biomarkers may deepen our understanding of these conditions’ pathophysiology. In this regard, most studies focused on inflammation, but markers of mitochondrial dysfunction, such as mitochondrial DNA damage, cell respiratory impairment, and oxidative stress, are less explored. The FRAMITO project aims to evaluate mitochondrial dysfunction in frailty, with and without multimorbidity. This cross-sectional study will enroll 75 individuals aged ≥65 years from inpatient and outpatient clinics at the Geriatrics Units of the University Hospital of Ferrara (Ferrara, Italy) and Fondazione IRCCS San Gerardo dei Tintori (Monza, Italy). Participants will be categorized into three groups: 25 without frailty and multimorbidity, 25 with frailty but not multimorbidity, and 25 with frailty and multimorbidity. Blood samples will be collected to isolate Peripheral Blood Mononuclear Cells. Frailty biomarkers will be identified using untargeted metabolomics and functional studies on mitochondrial dysfunctions in PBMCs and their subpopulations, evaluating mitochondrial DNA damage, mitochondrial and glycolytic cellular bioenergetics, and intracellular reactive oxygen species. This project will advance our understanding of mitochondrial dysfunctions in frailty, particularly when combined with multimorbidity, revealing potential synergistic effects.

Locatelli, E., Torsello, B., De Marco, S., Lombardi, M., Remelli, F., Pampolini, G., et al. (2025). Mitochondrial dysfunction as a biomarker of frailty: The FRAMITO study protocol. ARCHIVES OF GERONTOLOGY AND GERIATRICS, 133(June 2025) [10.1016/j.archger.2025.105803].

Mitochondrial dysfunction as a biomarker of frailty: The FRAMITO study protocol

Torsello, Barbara;De Marco, Sofia;Lombardi, Martina
;
Pasquale, Valentina;Ducci, Giacomo;Navaei, Ouldouz;Ferrara, Maria Cristina;Guo, Wenxiang;Cucini, Eleonora;Bellelli, Giuseppe;Sacco, Elena;Paglia, Giuseppe;Mazzola, Paolo;Bernasconi, Davide Paolo;Bianchi, Cristina;
2025

Abstract

Frailty syndrome often coexists with multimorbidity, sharing several risk factors and outcomes. Therefore, considering multimorbidity when exploring frailty biomarkers may deepen our understanding of these conditions’ pathophysiology. In this regard, most studies focused on inflammation, but markers of mitochondrial dysfunction, such as mitochondrial DNA damage, cell respiratory impairment, and oxidative stress, are less explored. The FRAMITO project aims to evaluate mitochondrial dysfunction in frailty, with and without multimorbidity. This cross-sectional study will enroll 75 individuals aged ≥65 years from inpatient and outpatient clinics at the Geriatrics Units of the University Hospital of Ferrara (Ferrara, Italy) and Fondazione IRCCS San Gerardo dei Tintori (Monza, Italy). Participants will be categorized into three groups: 25 without frailty and multimorbidity, 25 with frailty but not multimorbidity, and 25 with frailty and multimorbidity. Blood samples will be collected to isolate Peripheral Blood Mononuclear Cells. Frailty biomarkers will be identified using untargeted metabolomics and functional studies on mitochondrial dysfunctions in PBMCs and their subpopulations, evaluating mitochondrial DNA damage, mitochondrial and glycolytic cellular bioenergetics, and intracellular reactive oxygen species. This project will advance our understanding of mitochondrial dysfunctions in frailty, particularly when combined with multimorbidity, revealing potential synergistic effects.
Articolo in rivista - Articolo scientifico
frailty, mtDNA damage, oxidative stress, mitochondrial dysfunction, metabolomics
English
26-feb-2025
2025
133
June 2025
105803
open
Locatelli, E., Torsello, B., De Marco, S., Lombardi, M., Remelli, F., Pampolini, G., et al. (2025). Mitochondrial dysfunction as a biomarker of frailty: The FRAMITO study protocol. ARCHIVES OF GERONTOLOGY AND GERIATRICS, 133(June 2025) [10.1016/j.archger.2025.105803].
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/10281/543981
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