| Literature DB >> 24731243 |
M Segovia1, C Louvet1, P Charnet2, A Savina3,4, G Tilly1, L Gautreau1, L Carretero-Iglesia1, G Beriou1, I Cebrian3,4, T Cens2, L Hepburn5, E Chiffoleau1, R A Floto5, I Anegon1, S Amigorena3,4, M Hill1, M C Cuturi1.
Abstract
The administration of autologous (recipient-derived) tolerogenic dendritic cells (ATDCs) is under clinical evaluation. However, the molecular mechanisms by which these cells prolong graft survival in a donor-specific manner is unknown. Here, we tested mouse ATDCs for their therapeutic potential in a skin transplantation model. ATDC injection in combination with anti-CD3 treatment induced the accumulation of CD8(+) CD11c(+) T cells and significantly prolonged allograft survival. TMEM176B is an intracellular protein expressed in ATDCs and initially identified in allograft tolerance. We show that Tmem176b(-/-) ATDCs completely failed to trigger both phenomena but recovered their effect when loaded with donor peptides before injection. These results strongly suggested that ATDCs require TMEM176B to cross-present antigens in a tolerogenic fashion. In agreement with this, Tmem176b(-/-) ATDCs specifically failed to cross-present male antigens or ovalbumin to CD8(+) T cells. Finally, we observed that a Tmem176b-dependent cation current controls phagosomal pH, a critical parameter in cross-presentation. Thus, ATDCs require TMEM176B to cross-present donor antigens to induce donor-specific CD8(+) CD11c(+) T cells with regulatory properties and prolong graft survival. © Copyright 2014 The American Society of Transplantation and the American Society of Transplant Surgeons.Entities:
Keywords: Autologous dendritic cells; cellular therapy; cross-presentation; ion channel
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Year: 2014 PMID: 24731243 PMCID: PMC4629416 DOI: 10.1111/ajt.12708
Source DB: PubMed Journal: Am J Transplant ISSN: 1600-6135 Impact factor: 8.086