Structural basis of latent TGF-β1 presentation and activation by GARP on human regulatory T cells

Author:

Liénart Stéphanie1ORCID,Merceron Romain23,Vanderaa Christophe1ORCID,Lambert Fanny1,Colau Didier4,Stockis Julie15ORCID,van der Woning Bas6,De Haard Hans6,Saunders Michael6,Coulie Pierre G.15,Savvides Savvas N.23ORCID,Lucas Sophie15ORCID

Affiliation:

1. de Duve Institute, UCLouvain, 1200 Brussels, Belgium.

2. Department of Biochemistry and Microbiology, Ghent University, 9052 Ghent, Belgium.

3. VIB Center for Inflammation Research, 9052 Ghent, Belgium.

4. Ludwig Cancer Research, Brussels, Belgium.

5. Walloon Excellence in Lifesciences and Biotechnology, 1300 Wavre, Belgium.

6. argenx, 9052 Zwijnaarde, Belgium.

Abstract

Visualizing TGF-β1 regulation by GARP Regulatory T cells (T regs ) can suppress immune responses through a variety of mechanisms. One such mechanism involves the activation of a surface-bound latent form of the cytokine transforming growth factor–β1 (TGF-β1). Within the cell, newly synthesized pro-TGF-β1 homodimers form disulfide bonds with the transmembrane protein GARP, which acts to chaperone and orient the cytokine for activation at the cell surface. Liénart et al. reveal how GARP interacts with TGF-β1, using a crystal structure in which the complex was stabilized using a Fab fragment from a monoclonal antibody (MHG-8) that binds to the complex. In so doing, they also demonstrate how MHG-8 prevents membrane-associated TGF-β1 release. These structural and mechanistic insights may inform treatments of diseases with altered TGF-β1 functionality and dysfunctional T reg activity, including cancer immunotherapy. Science , this issue p. 952

Funder

H2020 European Research Council

Fonds De La Recherche Scientifique - FNRS

Publisher

American Association for the Advancement of Science (AAAS)

Subject

Multidisciplinary

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