| Literature DB >> 28931757 |
Aaron Prodeus1,2, Aws Abdul-Wahid2, Amanda Sparkes2, Nicholas W Fischer1,2, Marzena Cydzik2, Nicholas Chiang2,3, Mays Alwash2,3, Alessandra Ferzoco2,4, Nathalie Vacaresse2, Michael Julius1,2,4, Reginald M Gorczysnki3,5, Jean Gariépy1,2,3.
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.Entities:
Keywords: Immunology; Immunotherapy; Therapeutics
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Year: 2017 PMID: 28931757 PMCID: PMC5621893 DOI: 10.1172/jci.insight.94308
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708