Tuning of NK-Specific HLA-C Expression by Alternative mRNA Splicing

A complex system regulating HLA-C expression in NK cells, driven by an NK-specific promoter that produces alternatively spliced variants of the 5'-UTR has been recently identified. Exon content of the NK-specific 5'-UTR varies strikingly across alleles, with some exons being allele specifi...

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Bibliographic Details
Published in:Frontiers in immunology 2020-01, Vol.10, p.3034-3034
Main Authors: Goodson-Gregg, Frederick J, Rothbard, Brian, Zhang, Amy, Wright, Paul W, Li, Hongchuan, Walker-Sperling, Victoria E, Carrington, Mary, Anderson, Stephen K
Format: Article
Language:English
Subjects:
alternative splicing
HLA-C
human
Immunology
NK-promoter
peptide loading
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Summary:A complex system regulating HLA-C expression in NK cells, driven by an NK-specific promoter that produces alternatively spliced variants of the 5'-UTR has been recently identified. Exon content of the NK-specific 5'-UTR varies strikingly across alleles, with some exons being allele specific. In order to investigate the possibility that allelic variation in the 5'-UTR modulates HLA-C expression levels, cDNAs containing several distinct classes of 5'-UTR were compared. Subtle changes in 5'-UTR content had a significant effect on the expression of and cDNA clones, suggesting that alternative splicing can fine-tune the level of protein expression. The allele was found to be highly expressed in relation to the other alleles studied. However, its increased expression was primarily associated with differences in the peptide-binding groove. Although the impact of allele-specific alternative splicing of NK-Pro transcripts on protein levels can be modest when compared with the effect of changes in peptide-loading, alternative splicing may represent an additional regulatory mechanism to fine-tune HLA-C levels within NK cells in distinct tissue environments or at different stages of maturation in order to achieve optimal levels of missing-self recognition.
ISSN:1664-3224
1664-3224
DOI:10.3389/fimmu.2019.03034