Recipient nonhematopoietic antigen-presenting cells are sufficient to induce lethal acute graft-versus-host disease | Zendy

Motoko Koyama | Zendy; Rachel D. Kuns | Zendy; Stuart D. Olver | Zendy; Neil C. Raffelt | Zendy; Yana A. Wilson | Zendy; Alistair L. J. Don | Zendy; Katie E. Lineburg | Zendy; Melody Cheong | Zendy; Renee J. Robb | Zendy; Kate A. Markey | Zendy; Antiopi Varelias | Zendy; Bernard Malissen | Zendy; Günter J. Hämmerling | Zendy; Andrew D. Clouston | Zendy; Christian Engwerda | Zendy; Purnima Bhat | Zendy; Kelli P. A. MacDonald | Zendy; Geoffrey R. Hill | Zendy

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Recipient nonhematopoietic antigen-presenting cells are sufficient to induce lethal acute graft-versus-host disease

Author(s) -

Motoko Koyama,

Rachel D. Kuns,

Stuart D. Olver,

Neil C. Raffelt,

Yana A. Wilson,

Alistair L. J. Don,

Katie E. Lineburg,

Melody Cheong,

Renee J. Robb,

Kate A. Markey,

Antiopi Varelias,

Bernard Malissen,

Günter J. Hämmerling,

Andrew D. Clouston,

Christian Engwerda,

Purnima Bhat,

Kelli P. A. MacDonald,

Geoffrey R. Hill

Publication year - 2011

Publication title -

nature medicine

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 19.536

H-Index - 547

eISSN - 1546-170X

pISSN - 1078-8956

DOI - 10.1038/nm.2597

Subject(s) - immunology , graft versus host disease , major histocompatibility complex , antigen presentation , bone marrow , haematopoiesis , antigen presenting cell , t cell , hematopoietic stem cell transplantation , antigen , immune system , medicine , biology , stem cell , disease , pathology , microbiology and biotechnology

The presentation pathways by which allogeneic peptides induce graft-versus-host disease (GVHD) are unclear. We developed a bone marrow transplant (BMT) system in mice whereby presentation of a processed recipient peptide within major histocompatibility complex (MHC) class II molecules could be spatially and temporally quantified. Whereas donor antigen presenting cells (APCs) could induce lethal acute GVHD via MHC class II, recipient APCs were 100-1,000 times more potent in this regard. After myeloablative irradiation, T cell activation and memory differentiation occurred in lymphoid organs independently of alloantigen. Unexpectedly, professional hematopoietic-derived recipient APCs within lymphoid organs had only a limited capacity to induce GVHD, and dendritic cells were not required. In contrast, nonhematopoietic recipient APCs within target organs induced universal GVHD mortality and promoted marked alloreactive donor T cell expansion within the gastrointestinal tract and inflammatory cytokine generation. These data challenge current paradigms, suggesting that experimental lethal acute GVHD can be induced by nonhematopoietic recipient APCs.

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