Proteasome isoforms exhibit only quantitative differences in cleavage and 
epitope generation.

Mishto, M.; Liepe, J.; Textoris-Taube, K.; Keller, C.; Henklein, P.; Weberruss, M.; Dahlmann, B.; Enenkel, C.; Voigt, A.; Kuckelkorn, U.; Stumpf, M. P. H.; Kloetzel, P. M.

doi:10.1002/eji.201444902

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Proteasome isoforms exhibit only quantitative differences in cleavage and epitope generation.

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Liepe, J.
Research Group of Quantitative and System Biology, MPI for Biophysical Chemistry, Max Planck Society;

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Citation

Mishto, M., Liepe, J., Textoris-Taube, K., Keller, C., Henklein, P., Weberruss, M., et al. (2014). Proteasome isoforms exhibit only quantitative differences in cleavage and epitope generation. European Journal of Immunology, 44(12), 3508-3521. doi:10.1002/eji.201444902.

Cite as: https://hdl.handle.net/11858/00-001M-0000-002D-FFF7-E

Abstract

Immunoproteasomes are considered to be optimised to process Ags and to alter the peptide repertoire by generating a qualitatively different set of MHC class I epitopes. Whether the immunoproteasome at the biochemical level, influence the quality rather than the quantity of the immuno-genic peptide pool is still unclear. Here, we quantified the cleavage-site usage by human standard- and immunoproteasomes, and proteasomes from immuno-subunit-deficient mice, as well as the peptides generated from model polypeptides. We show in this study that the different proteasome isoforms can exert significant quantitative differences in the cleavage-site usage and MHC class I restricted epitope production. However, independent of the proteasome isoform and substrates studied, no evidence was obtained for the abolishment of the specific cleavage-site usage, or for differences in the quality of the peptides generated. Thus, we conclude that the observed differences in MHC class I restricted Ag presentation between standard- and immunoproteasomes are due to quantitative differences in the proteasome-generated antigenic peptides.