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Intracellular trafficking of HLA-E and its regulation.


ABSTRACT: Interest in MHC-E-restricted CD8+ T cell responses has been aroused by the discovery of their efficacy in controlling simian immunodeficiency virus (SIV) infection in a vaccine model. The development of vaccines and immunotherapies utilizing human MHC-E (HLA-E)-restricted CD8+ T cell response requires an understanding of the pathway(s) of HLA-E transport and antigen presentation, which have not been clearly defined previously. We show here that, unlike classical HLA class I, which rapidly exits the endoplasmic reticulum (ER) after synthesis, HLA-E is largely retained because of a limited supply of high-affinity peptides, with further fine-tuning by its cytoplasmic tail. Once at the cell surface, HLA-E is unstable and is rapidly internalized. The cytoplasmic tail plays a crucial role in facilitating HLA-E internalization, which results in its enrichment in late and recycling endosomes. Our data reveal distinctive transport patterns and delicate regulatory mechanisms of HLA-E, which help to explain its unusual immunological functions.

SUBMITTER: He W 

PROVIDER: S-EPMC10165540 | biostudies-literature | 2023 Aug

REPOSITORIES: biostudies-literature

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Intracellular trafficking of HLA-E and its regulation.

He Wanlin W   Gea-Mallorquí Ester E   Colin-York Huw H   Fritzsche Marco M   Gillespie Geraldine M GM   Brackenridge Simon S   Borrow Persephone P   McMichael Andrew J AJ  

The Journal of experimental medicine 20230504 8


Interest in MHC-E-restricted CD8+ T cell responses has been aroused by the discovery of their efficacy in controlling simian immunodeficiency virus (SIV) infection in a vaccine model. The development of vaccines and immunotherapies utilizing human MHC-E (HLA-E)-restricted CD8+ T cell response requires an understanding of the pathway(s) of HLA-E transport and antigen presentation, which have not been clearly defined previously. We show here that, unlike classical HLA class I, which rapidly exits  ...[more]

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