Satoshi Ishido, Stuart K. Calderwood, Cristina Bonorino, Benjamin J. Lang, João Ismael Budelon Gonçalves, Priscila Vianna, Naoka Murakami, Rafael Fernandes Zanin, Laura M. Bellan, Jeoung-Sook Shin, Thiago J. Borges, Krist Helen Antunes, Mayuko Uehara, Felipe D. Machado, María José Pérez-Sáez, Gabriel Birrane, Ana Paula de Souza, Rafael Lopes, Reza Abdi, Ayesha Murshid, Leonardo V. Riella, and Jamil Azzi
In transplantation, donor dendritic cells (do-DCs) initiate the alloimmune response either by direct interaction with host T cells or by transferring intact donor MHC to host DCs. However, how do-DCs can be targeted for improving allograft survival is still unclear. Here we show CD103+ DCs are the major do-DC subset involved in the acute rejection of murine skin transplants. In the absence of CD103+ do-DCs, less donor MHC-II is carried to host lymph nodes, fewer allogenic T cells are primed and allograft survival is prolonged. Incubation of skin grafts with the anti-inflammatory mycobacterial protein DnaK reduces donor MHC-II on CD103+DCs and prolongs graft survival. This effect is mediated through IL-10-induced March1, which ubiquitinates and decreases MHC-II levels. Importantly, in vitro pre-treatment of human DCs with DnaK reduces their ability to prime alloreactive T cells. Our findings demonstrate a novel therapeutic approach to dampen alloimmunity by targeting donor MHC-II on CD103+DCs., Donor-derived dendritic cells (do-DC) in the graft can contribute to the induction of alloimmunity and tissue rejection, but how do-DC can be targeted for improving graft survival is unclear. Here the authors show that reducing MHC-II expression on do-DCs by DnaK pre-treatment can decrease the priming of alloimmunity and prolong graft survival in mouse models.