[R01] Role of Tregs in the acquisition and maintenance of Tconv anergy in transplantation tolerance
Ente: National Institute of Allergy and Infectious Diseases
Scadenza: 2030-06-30
Importo max: 766.265 EUR
Paese: US
Descrizione
Summary
Donor-specific transplantation tolerance is an important goal for improving the quality of life of transplant
patients, as it eliminates side-effects from chronic immunosuppression. Transient regimens that use a blocking
CD154 antibody have been shown to promote donor-specific transplantation tolerance in mice and non-human
primates. Although initial clinical trials testing CD154 had been halted due to thromboembolic complications in
humans, new humanized Fc-mutated antibodies avoid FcR cross-linking and platelet aggregation and are safe.
Three such antibodies are in clinical trials, frexalimab (Sanofi), tegoprubart (AT-1501, Eledon Pharmaceuticals),
and TNX-1500, with both TNX-1500 and AT-1501 being slated to start phase 2 trials in kidney transplantation.
As such, there is considerable renewed interest in mechanistic experiments to fully understand the
consequences of CD154 therapy. We and others have shown that transient administration of CD154, when
in combination with injection of donor splenocytes (DST) as a source of systemic alloantigen, results in long-
term donor-specific transplantation tolerance of fully mismatched cardiac allografts in mice. This treatment
expands Tregs, prevents germinal center formation and therefore development of donor-specific antibodies
(DSA), and results in a hypofunctional state of alloreactive conventional T cells (Tconvs) akin to anergy. We have
shown that acquisition of this T cell anergic state requires both blockade of CD154/CD40 interactions and
persistent expression of the cognate alloantigen in the graft. Our preliminary results also show that
CD154+DST-mediated graft acceptance and expansion of Tregs both depend on the presence of classical
dendritic cells 1 (cDC1), as they fail to occur in IRF832 mice that lack cDC1s. Although we initially thought that
Tregs would function as suppressor cells in this model (reducing the activation of functional Tconvs), our
preliminary results reveal an exciting new property of Tregs: their ability to program and maintain anergy in
alloreactive Tconvs. Indeed, CD154+DST fails to induce alloreactive Tconv anergy in mice lacking Tregs, and
Treg depletion long after establishment of tolerance reinvigorates Tconvs, along with de novo DSA development.
We hypothesize that the crosstalk between Tregs, cDC1s and Tconvs during the induction of transplantation
tolerance is essential to program alloreactive Tconvs into an anergic state, as well as to maintain this state when
established. This hypothesis will be tested in the context of the following Specific Aims.
Specific Aim 1. To elucidate the mechanisms by which Tregs program alloreactive T cell anergy
during the induction phase of transplantation tolerance. Specific Aim 2. To establish the mechanisms by
which elimination of Tregs at the maintenance phase of tolerance triggers alloreactive T cell
reinvigoration. This project will define a new property of Tregs (driving Tconv anergy) and establish the ro
Istituzione: UNIVERSITY OF CHICAGO
PI: Maria-Luisa Alegre
Progetto: 5R01AI194499-02
Settori: National Institute of Allergy and Infectious Diseases
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