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Role of Immunoproteasomes in Cross-Presentation
Author(s) -
Michael J. Palmowski,
Uzi Gileadi,
Mariolina Salio,
Awen Gallimore,
Maggie Millrain,
Edward James,
Caroline Addey,
Diane Scott,
Julian Dyson,
Elizabeth Simpson,
Vincenzo Cerundolo
Publication year - 2006
Publication title -
the journal of immunology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.737
H-Index - 372
eISSN - 1550-6606
pISSN - 0022-1767
DOI - 10.4049/jimmunol.177.2.983
Subject(s) - epitope , proteasome , antigen presentation , priming (agriculture) , mhc class i , immunology , biology , in vivo , antigen processing , peptide , microbiology and biotechnology , major histocompatibility complex , t cell , immune system , antigen , genetics , biochemistry , botany , germination
The evidence that proteasomes are involved in the processing of cross-presented proteins is indirect and based on the in vitro use of proteasome inhibitors. It remains, therefore, unclear whether cross-presentation of MHC class I peptide epitopes can occur entirely within phagolysosomes or whether it requires proteasome degradation. To address this question, we studied in vivo cross-presentation of an immunoproteasome-dependent epitope. First, we demonstrated that generation of the immunodominant HY Uty(246-254) epitope is LMP7 dependent, resulting in the lack of rejection of male LMP7-deficient (LMP7(-/-)) skin grafts by female LMP7(-/-) mice. Second, we ruled out an altered Uty(246-254)-specific T cell repertoire in LMP7(-/-) female mice and demonstrated efficient Uty(246-254) presentation by re-expressing LMP7 in male LMP7(-/-) cells. Finally, we observed that LMP7 expression significantly enhanced cross-priming of Uty(246-254)-specific T cells in vivo. The observations that male skin grafts are not rejected by LMP7(-/-) female mice and that presentation of a proteasome-dependent peptide is not efficiently rescued by alternative cross-presentation pathways provide strong evidence that proteasomes play an important role in cross-priming events.

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