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In situ recruitment of regulatory T cells promotes donor-specific tolerance in vascularized composite allotransplantation

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CCL22-releasing microparticles recruit suppressive immune cells to transplanted rat limbs to promote long-term graft survival. Vascularized composite allotransplantation (VCA) encompasses face and limb transplantation, but as with organ transplantation, it… Click to show full abstract

CCL22-releasing microparticles recruit suppressive immune cells to transplanted rat limbs to promote long-term graft survival. Vascularized composite allotransplantation (VCA) encompasses face and limb transplantation, but as with organ transplantation, it requires lifelong regimens of immunosuppressive drugs to prevent rejection. To achieve donor-specific immune tolerance and reduce the need for systemic immunosuppression, we developed a synthetic drug delivery system that mimics a strategy our bodies naturally use to recruit regulatory T cells (Treg) to suppress inflammation. Specifically, a microparticle-based system engineered to release the Treg-recruiting chemokine CCL22 was used in a rodent hindlimb VCA model. These “Recruitment-MP” prolonged hindlimb allograft survival indefinitely (>200 days) and promoted donor-specific tolerance. Recruitment-MP treatment enriched Treg populations in allograft skin and draining lymph nodes and enhanced Treg function without affecting the proliferative capacity of conventional T cells. With implications for clinical translation, synthetic human CCL22 induced preferential migration of human Treg in vitro. Collectively, these results suggest that Recruitment-MP promote donor-specific immune tolerance via local enrichment of suppressive Treg.

Keywords: tolerance; regulatory cells; composite allotransplantation; vascularized composite; specific tolerance; donor specific

Journal Title: Science Advances
Year Published: 2020

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