Litcius/Paper detail

Tregs integrate native and CAR-mediated costimulatory signals for control of allograft rejection

Isaac Rosado‐Sánchez, Manjurul Haque, Kevin Salim, Madeleine Speck, Vivian Fung, Dominic A. Boardman, Majid Mojibian, Giorgio Raimondi, Megan K. Levings

2023JCI Insight34 citationsDOIOpen Access PDF

Abstract

Tregs expressing chimeric antigen receptors (CAR-Tregs) are a promising tool to promote transplant tolerance. The relationship between CAR structure and Treg function was studied in xenogeneic, immunodeficient mice, revealing advantages of CD28-encoding CARs. However, these models could underrepresent interactions between CAR-Tregs, antigen-presenting cells (APCs), and donor-specific Abs. We generated Tregs expressing HLA-A2-specific CARs with different costimulatory domains and compared their function in vitro and in vivo using an immunocompetent model of transplantation. In vitro, the CD28-encoding CAR had superior antigen-specific suppression, proliferation, and cytokine production. In contrast, in vivo, Tregs expressing CARs encoding CD28, ICOS, programmed cell death 1, and GITR, but not 4-1BB or OX40, all extended skin allograft survival. To reconcile in vitro and in vivo data, we analyzed effects of a CAR encoding CD3ζ but no costimulatory domain. These data revealed that exogenous costimulation from APCs can compensate for the lack of a CAR-encoded CD28 domain. Thus, Tregs expressing a CAR with or without CD28 are functionally equivalent in vivo, mediating similar extension of skin allograft survival and controlling the generation of anti-HLA-A2 alloantibodies. This study reveals a dimension of CAR-Treg biology and has important implications for the design of CARs for clinical use in Tregs.

Topics & Concepts

Control (management)Computer scienceChemistryImmunologyCancer researchMedicineArtificial intelligenceCAR-T cell therapy researchViral Infectious Diseases and Gene Expression in InsectsImmune Cell Function and Interaction