Publication: Identification of common cardiometabolic alterations and deregulated pathways in mouse and pig models of aging.
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Publication date
2020-07-30
Authors
Fanjul, Victor CNIC
Jorge, Inmaculada CNIC 



Camafeita, Emilio CNIC 





Macias, Alvaro CNIC 





Barettino, Ana CNIC
Dorado, Beatriz CNIC
Rivera-Torres, Jose CNIC
Vazquez, Jesus CNIC 





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Wiley
Abstract
Aging is the main risk factor for cardiovascular and metabolic diseases, which have become a global concern as the world population ages. These diseases and the aging process are exacerbated in Hutchinson-Gilford progeria syndrome (HGPS or progeria). Here, we evaluated the cardiometabolic disease in animal models of premature and normal aging with the aim of identifying alterations that are shared or specific to each condition. Despite differences in body composition and metabolic markers, prematurely and normally aging mice developed heart failure and similar cardiac electrical abnormalities. High-throughput proteomics of the hearts of progeric and normally aged mice revealed altered protein oxidation and glycation, as well as dysregulated pathways regulating energy metabolism, proteostasis, gene expression, and cardiac muscle contraction. These results were corroborated in the hearts of progeric pigs, underscoring the translational potential of our findings, which could help in the design of strategies to prevent or slow age-related cardiometabolic disease.
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Bibliographic citation
Aging Cell. 2020; 19(9):e13203