VISTA.COMP — an engineered checkpoint receptor agonist that potently suppresses T cell–mediated immune responses
Aaron Prodeus, Aws Abdul-Wahid, Amanda Sparkes, Nicholas W. Fischer, Marzena Cydzik, Nicholas Chiang, Mays Alwash, Alessandra Ferzoco, Nathalie Vacaresse, Michael Julius, Reginald M. Gorczysnki, Jean Gariépy
Aaron Prodeus, Aws Abdul-Wahid, Amanda Sparkes, Nicholas W. Fischer, Marzena Cydzik, Nicholas Chiang, Mays Alwash, Alessandra Ferzoco, Nathalie Vacaresse, Michael Julius, Reginald M. Gorczysnki, Jean Gariépy
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Research Article Immunology Therapeutics

VISTA.COMP — an engineered checkpoint receptor agonist that potently suppresses T cell–mediated immune responses

Abstract

V-domain immunoglobulin suppressor of T cell activation (VISTA) is a recently discovered immune checkpoint ligand that functions to suppress T cell activity. The therapeutic potential of activating this immune checkpoint pathway to reduce inflammatory responses remains untapped, largely due to the inability to derive agonists targeting its unknown receptor. A dimeric construct of the IgV domain of VISTA (VISTA-Fc) was shown to suppress the activation of T cells in vitro. However, this effect required its immobilization on a solid surface, suggesting that VISTA-Fc may display limited efficacy as a VISTA-receptor agonist in vivo. Herein, we have designed a stable pentameric VISTA construct (VISTA.COMP) by genetically fusing its IgV domain to the pentamerization domain from the cartilage oligomeric matrix protein (COMP). In contrast to VISTA-Fc, VISTA.COMP does not require immobilization to inhibit the proliferation of CD4+ T cells undergoing polyclonal activation. Furthermore, we show that VISTA.COMP, but not VISTA-Fc, functions as an immunosuppressive agonist in vivo capable of prolonging the survival of skin allografts in a mouse transplant model as well as rescuing mice from acute concanavalin-A–induced hepatitis. Collectively, we believe our data demonstrate that VISTA.COMP is a checkpoint receptor agonist and the first agent to our knowledge targeting the putative VISTA-receptor to suppress T cell–mediated immune responses.

Authors

Aaron Prodeus, Aws Abdul-Wahid, Amanda Sparkes, Nicholas W. Fischer, Marzena Cydzik, Nicholas Chiang, Mays Alwash, Alessandra Ferzoco, Nathalie Vacaresse, Michael Julius, Reginald M. Gorczysnki, Jean Gariépy

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Figure 2

VISTA.COMP binds to a clonal T cell line and suppresses its activation.

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VISTA.COMP binds to a clonal T cell line and suppresses its activation. ...
(A) 2.10 clonal T cells were activated with immobilized anti-CD3 antibody (3 μg/ml) in the presence of immobilized or soluble VISTA-Fc or VISTA.COMP (10 μg/ml), and proliferation was measured by pulsing cells with 3H-thymidine in the last 6 hours of a 24-hour culture. As observed with primary CD4+ T cells, pentameric VISTA.COMP suppresses proliferation when immobilized or when added soluble in culture media, whereas VISTA-Fc only exhibits suppressive activity when immobilized (data represent mean ± SEM, ***P < 0.01 relative to anti-CD3 stimulated control by Student’s t test, n = 3). Data are representative of at least three independent experiments. (B) Titration of soluble VISTA.COMP (blue) or VISTA-Fc (red) on 2.10 cells activated as described in A. Data show a lack of an antiproliferative effect on cells by soluble VISTA-Fc at high concentrations (each point represents mean ± SEM). (C) FACS analysis of biotinylated COMP, biotinylated VISTA.COMP, and VISTA-Fc (shaded histogram) binding to 2.10 clonal T cells compared with unstained control (empty histograms). Data are representative of 3 independent experiments. (D) FACS-derived histograms of VISTA-Fc binding to 2.10 cells (shaded histograms) in the presence or absence of equimolar unlabeled VISTA.COMP. Empty histograms represent unstained cells. VISTA.COMP readily out competes VISTA-Fc binding to these cells.