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Mapping the life histories of T cells

Objectif

T cells display many different phenotypes and functions, depending on the nature of previously encountered signals. If we want to understand how these different T cell subsets arise, we need to be able to follow individual T cells and their progeny through time. With the aim to map the life histories of individual T cells we have developed unique technologies that allow us to determine whether different T cell populations arise from common or distinct progenitors.

Within this project we will utilize genetic reporter systems to determine:
1. How T cell recruitment, proliferation and death shape antigen-specific T cell responses
2. At which stage the resulting T cells commit to the effector or the memory T cell lineage
3. The self renewal potential of the tissue-resident memory T cells that remain after infection is cleared

By following T cells and their progeny through time, this project will describe the regulation of cell fate in antigen-specific T cell responses. Furthermore, this project will lead to the creation of novel reporters of cellular history that will be of broad value to analyze cell fate and kinship for a variety of cell types.

Appel à propositions

ERC-2010-AdG_20100317
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Régime de financement

ERC-AG - ERC Advanced Grant

Institution d’accueil

STICHTING HET NEDERLANDS KANKER INSTITUUT-ANTONI VAN LEEUWENHOEK ZIEKENHUIS
Contribution de l’UE
€ 2 499 640,00
Adresse
PLESMANLAAN 121
1066 CX Amsterdam
Pays-Bas

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Région
West-Nederland Noord-Holland Groot-Amsterdam
Type d’activité
Research Organisations
Contact administratif
Henri Van Luenen (Dr.)
Chercheur principal
Antonius Nicolaas Maria Schumacher (Prof.)
Liens
Coût total
Aucune donnée

Bénéficiaires (1)