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Selective expansion of regulatory T cells using an orthogonal IL-2/IL-2 receptor system facilitates transplantation tolerance

Toshihito Hirai, Teresa Lopes Ramos, Po‐Yu Lin, Federico Simonetta, Leon Su, Lora K. Picton, Jeanette Baker, Jian‐Xin Lin, Peng Li, Kinya Seo, Juliane K. Lohmeyer, Sara Bolivar-Wagers, Melissa Mavers, Warren J. Leonard, Bruce R. Blazar, K. Christopher García, Robert S. Negrin

2021Journal of Clinical Investigation71 citationsDOIOpen Access PDF

Abstract

Adoptive transfer of Tregs has been shown to improve alloengraftment in animal models. However, it is technically challenging to expand Tregs ex vivo for the purpose of infusing large numbers of cells in the clinic. We demonstrate an innovative approach to engineering an orthogonal IL-2/IL-2 receptor (IL-2R) pair, the parts of which selectively interact with each other, transmitting native IL-2 signals, but do not interact with the natural IL-2 or IL-2R counterparts, thereby enabling selective stimulation of target cells in vivo. Here, we introduced this orthogonal IL-2R into Tregs. Upon adoptive transfer in a murine mixed hematopoietic chimerism model, orthogonal IL-2 injection significantly promoted orthogonal IL-2R+Foxp3GFP+CD4+ cell proliferation without increasing other T cell subsets and facilitated donor hematopoietic cell engraftment followed by acceptance of heart allografts. Our data indicate that selective target cell stimulation enabled by the engineered orthogonal cytokine receptor improves Treg potential for the induction of organ transplantation tolerance.

Topics & Concepts

Adoptive cell transferImmunologyTransplantationHaematopoiesisCytokineT cellCell biologyBiologyIn vivoStem cellCancer researchImmune systemMedicineInternal medicineBiotechnologyT-cell and B-cell ImmunologyImmune Cell Function and InteractionHematopoietic Stem Cell Transplantation
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