Summary
Ageing is an unavoidable consequence of living and constitutes the highest risk factor for most human diseases in modern “western” societies. Despise the frequently observed correlation between metabolic alterations and cellular ageing, the molecular mechanisms linking these two complex processes are far from being understood. Here the EpiMetAgeing project proposes to take a novel approach to investigate cell decline linked to obesity and ageing through the lenses of RNA modifications, specifically TET2-mediated 5-hydroxymethylation of cytosines (5hmC). For that purpose, we will characterize the impact of obesity throughout ageing in: (1) the distribution and dynamics of 5hmC epitranscriptomic modification and (2) the key RNA-binding proteins that mediate TET2 function. Given that RNA modifications are reversible, the ultimate goal of this project is to develop novel strategies for cellular rejuvenation. To this end the ER will use cutting-edge technologies, including next-generation sequencing techniques, proteomics, CRISPR activation and repression systems, metabolic phenotyping and iPSC technology. EpiMetAgeing will provide a deeper understanding of the implication of a specific RNA chemical modification in orchestrating metabolism and ageing. Our research has the potential to facilitate the identification of potential druggable targets for therapeutic intervention in age-associated metabolic diseases.
EpiMetAgeing has been carefully designed by combining the ER and host expertise in a highly interdisciplinary research environment to boost her career opportunities, and enhance her possibilities to achieve a position of greater professional maturity and independence that will allow her transition to become a principal investigator in the European R&D system.
EpiMetAgeing has been carefully designed by combining the ER and host expertise in a highly interdisciplinary research environment to boost her career opportunities, and enhance her possibilities to achieve a position of greater professional maturity and independence that will allow her transition to become a principal investigator in the European R&D system.
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More information & hyperlinks
| Web resources: | https://cordis.europa.eu/project/id/895984 |
| Start date: | 15-09-2020 |
| End date: | 14-09-2022 |
| Total budget - Public funding: | 160 932,48 Euro - 160 932,00 Euro |
Cordis data
Original description
Ageing is an unavoidable consequence of living and constitutes the highest risk factor for most human diseases in modern “western” societies. Despise the frequently observed correlation between metabolic alterations and cellular ageing, the molecular mechanisms linking these two complex processes are far from being understood. Here the EpiMetAgeing project proposes to take a novel approach to investigate cell decline linked to obesity and ageing through the lenses of RNA modifications, specifically TET2-mediated 5-hydroxymethylation of cytosines (5hmC). For that purpose, we will characterize the impact of obesity throughout ageing in: (1) the distribution and dynamics of 5hmC epitranscriptomic modification and (2) the key RNA-binding proteins that mediate TET2 function. Given that RNA modifications are reversible, the ultimate goal of this project is to develop novel strategies for cellular rejuvenation. To this end the ER will use cutting-edge technologies, including next-generation sequencing techniques, proteomics, CRISPR activation and repression systems, metabolic phenotyping and iPSC technology. EpiMetAgeing will provide a deeper understanding of the implication of a specific RNA chemical modification in orchestrating metabolism and ageing. Our research has the potential to facilitate the identification of potential druggable targets for therapeutic intervention in age-associated metabolic diseases.EpiMetAgeing has been carefully designed by combining the ER and host expertise in a highly interdisciplinary research environment to boost her career opportunities, and enhance her possibilities to achieve a position of greater professional maturity and independence that will allow her transition to become a principal investigator in the European R&D system.
Status
TERMINATEDCall topic
MSCA-IF-2019Update Date
28-04-2024
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