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TARG-SUP

TARGETING TGF-Β ACTIVATION, LIKELY THE CORE MECHANISM OF IMMUNOSUPPRESSION BY HUMAN REGULATORY T CELLS

Regulatory T lymphocytes (Tregs) inhibit immune responses and are required to maintain immune tolerance. Tregs express membrane protein GARP, which displays latent TGF-β1 on the cell surface. Immunosuppression by human Tregs appears to require GARP-mediated activation of TGF-β1.

My objectives are to unravel the molecular aspects of TGF-β1 activation by GARP and determine the functional importance of this process in physiological and pathological conditions where Tregs or other GARP-expressing cells are present.


As this implies the development of new tools to modulate GARP-dependent TGF-β1 activation and Treg immunosuppression, we will also explore their potential for the treatment of immune-related human diseases, and notably cancer.

More specifically, I will:

  • Derive antibodies that modulate GARPmediated TGFβ1 production by human Tregs and perform structural analyses in the presence of these antibodies to identify tridimensional changes in GARP/TGFβ1 complexes that lead to the release of active TGFβ1.
  • Identify and characterize additional proteins implicated in TGFβ1 activation by human Tregs, as GARP is required but not sufficient for TGFβ1 activation by Tregs.
  • Determine the immunological and clinical impact of inhibitory antiGARP mAbs on cancer in mice. We will derive anti-murine GARP mAbs. As an alternative, we will generate mutant mice expressing a chimeric mouse/human GARP that is recognized by anti-human GARP mAbs. The antibodies will be tested in tumour-bearing mice treated or not with other immunotherapies including vaccines or immunostimulatory antibodies.
  • Determine whether blocking antiGARP mAbs improve immune responses to microbial vaccines or to chronic infections, as these represent important applications for transient inhibition of Treg activity in humans.
  • Analyse the expression and roles of GARP in nonTreg cells to better understand GARP functions, which remain largely unknown, and predict potential toxicities of antiGARP mAbs.

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This project has received funding from the European Research Council (ERC) under the European Union's Horizon 2020 research and innovation programme under the grant agreement number 682818.