Oxidative stress affects the availability of key-regulators of vascular homeostasis and controls a number of signaling pathways relevant to myocardial and vascular disease. Reactive oxygen species are generated by different intracellular molecular pathways principally located in mitochondria. The notion that mice carrying a targeted mutation of the p66 Shc gene display prolonged lifespan, reduced production of intracellular oxidants, and increased resistance to oxidative stress–induced apoptosis prompted a series of studies aimed at defining the biochemical function of p66 Shc and its possible implication in cardiovascular diseases. Indeed, p66 Shc/ mice are protected against vascular, cardiac, and renal impairment attributable to hypercholesterolemia, aging, diabetes, and ischemia/reperfusion. The present review focuses on the biochemical and physiological function of the p66 Shc adaptor protein as well as on the mechanisms linking p66 Shc -associated generation of free radicals to the pathophysiology of aging and cardiovascular disease. On the whole, the evidence so far reported and here discussed supports the concept that pharmacological modulation of p66 Shc expression and activity may be a novel and effective target for the treatment of atherosclerotic vascular disease as well as myocardial adaptation to hypertrophic, inflammatory and neuro-hormonal stimuli in the overloaded heart.

Final common molecular pathways of aging and cardiovascular disease: role of the p66Shc protein / Cosentino, Francesco; Francia, Pietro; Camici, Gg; Pelicci, Pg; Lüscher, Tf; Volpe, Massimo. - In: ARTERIOSCLEROSIS, THROMBOSIS, AND VASCULAR BIOLOGY. - ISSN 1079-5642. - 28:(2008), pp. 622-628. [10.1161/ATVBAHA.107.156059]

Final common molecular pathways of aging and cardiovascular disease: role of the p66Shc protein.

COSENTINO, Francesco;FRANCIA, Pietro;VOLPE, Massimo
2008

Abstract

Oxidative stress affects the availability of key-regulators of vascular homeostasis and controls a number of signaling pathways relevant to myocardial and vascular disease. Reactive oxygen species are generated by different intracellular molecular pathways principally located in mitochondria. The notion that mice carrying a targeted mutation of the p66 Shc gene display prolonged lifespan, reduced production of intracellular oxidants, and increased resistance to oxidative stress–induced apoptosis prompted a series of studies aimed at defining the biochemical function of p66 Shc and its possible implication in cardiovascular diseases. Indeed, p66 Shc/ mice are protected against vascular, cardiac, and renal impairment attributable to hypercholesterolemia, aging, diabetes, and ischemia/reperfusion. The present review focuses on the biochemical and physiological function of the p66 Shc adaptor protein as well as on the mechanisms linking p66 Shc -associated generation of free radicals to the pathophysiology of aging and cardiovascular disease. On the whole, the evidence so far reported and here discussed supports the concept that pharmacological modulation of p66 Shc expression and activity may be a novel and effective target for the treatment of atherosclerotic vascular disease as well as myocardial adaptation to hypertrophic, inflammatory and neuro-hormonal stimuli in the overloaded heart.
2008
01 Pubblicazione su rivista::01a Articolo in rivista
Final common molecular pathways of aging and cardiovascular disease: role of the p66Shc protein / Cosentino, Francesco; Francia, Pietro; Camici, Gg; Pelicci, Pg; Lüscher, Tf; Volpe, Massimo. - In: ARTERIOSCLEROSIS, THROMBOSIS, AND VASCULAR BIOLOGY. - ISSN 1079-5642. - 28:(2008), pp. 622-628. [10.1161/ATVBAHA.107.156059]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/381383
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