Major Histocompatibility Complex class I heavy chains localize in both cytoplasmic and nuclear compartment

Author:

Gómez-Herranz Maria,Dziadosz Alicja,Mikac Sara,Rychłowski Michał,Fahraeus Robin,Marek-Trzonkowska Natalia,Chruściel Elżbieta,Urban-Wójciuk Zuzanna,Papak Ines,Arcimowicz Łukasz,Marjanski Tomasz,Rzyman Witold,Sznarkowska AlicjaORCID

Abstract

AbstractThe Major Histocompatibility Complex class I (MHC-I) molecules present antigenic peptides (AP) to CD8+T cells for self versus non-self recognition. Loading of AP on MHC-I takes place in the endoplasmic reticulum (ER), upon shuttling of cytoplasmic AP substrates to the ER. Understanding of this process has been influenced by the view that MHC-I antigens are produced from the proteasomal degradation of cellular proteins. Recent observations on the intronic and untranslated region-derived peptides as well as on the non-AUG translation products presented on the MHC-I open the possibility that antigenic peptides can derive from pre-spliced mRNAs translated in the nuclear compartment. In this brief report, we show that a fraction of human MHC-I molecules (human leukocyte antigens type A, HLA-A) is present in the nuclei of cells, in the proximity of histone H2B. With this finding, we hope to initiate a new direction of research on the nuclear role of MHC-I and ask whether the loading of antigens can take place in the nuclear compartment.

Publisher

Cold Spring Harbor Laboratory

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