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• W2899691505 endingPage "26" @default.
• W2899691505 startingPage "1" @default.
• W2899691505 abstract "Mitochondria are highly dynamic and regulated organelles that historically have been defined based on their crucial role in cell metabolism. However, they are implicated in a variety of other important functions, making mitochondrial dysfunction an important axis in several pathological contexts. Despite that conventional biochemical and molecular biology approaches have provided significant insight into mitochondrial functionality, innovative techniques that provide a global view of the mitochondrion are still necessary. Proteomics fulfils this need by enabling accurate, systems-wide quantitative analysis of protein abundance. More importantly, redox proteomics approaches offer unique opportunities to tackle oxidative stress, a phenomenon that is intimately linked to aging, cardiovascular disease, and cancer. In addition, cutting-edge proteomics approaches reveal how proteins exert their functions in complex interaction networks where even subtle alterations stemming from early pathological states can be monitored. Here, we describe the proteomics approaches that will help to deepen the role of mitochondria in health and disease by assessing not only changes to mitochondrial protein composition but also alterations to their redox state and how protein interaction networks regulate mitochondrial function and dynamics. This review is aimed at showing the reader how the application of proteomics approaches during the last 20 years has revealed crucial mitochondrial roles in the context of aging, neurodegenerative disorders, metabolic disease, and cancer." @default.
• W2899691505 created "2018-11-16" @default.
• W2899691505 creator A5033161729 @default.
• W2899691505 creator A5054407791 @default.
• W2899691505 creator A5057650956 @default.
• W2899691505 creator A5061921382 @default.
• W2899691505 date "2018-11-08" @default.
• W2899691505 modified "2023-10-15" @default.
• W2899691505 title "Mitoproteomics: Tackling Mitochondrial Dysfunction in Human Disease" @default.
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