AI Article Synopsis

  • The activation of cytotoxic T lymphocytes (CTLs) relies on their recognition of peptides presented by MHC molecules on antigen-presenting cells (APCs).
  • This study shows that differential RNA splicing of antigen-encoding genes can reduce the amount of antigen available in APCs and impact the response of memory CTLs in humans.
  • Specifically, splicing altered the presentation of a crucial HLA-B8-restricted epitope from EBV, leading to lower expansion and effectiveness of CTLs, which was not due to a variety of TCR clonotypes but rather a decrease in cytotoxicity against target cells.

Article Abstract

The activation of CTLs is dependent on the recognition of MHC-bound peptide present on the surface of APCs. We give evidence in this study that differential splicing of Ag-encoding RNA can decrease the antigenic dose in APCs and regulate the recall of human memory CTLs. Differential splicing of RNA that encoded an immunodominant HLA-B8-restricted CTL epitope of EBV reduced the functional presentation of this epitope, and consequently the in vitro expansion and activity of CTLs, as measured by MHC/peptide-tetramer staining and cytotoxicity assays. The reduced activity of the stimulated CTLs was not only due to lower numbers of Ag-specific CTLs but, surprisingly, was also characterized by decreased cytotoxicity of the CTLs to target cells presenting limiting amounts of the peptide epitope. As indicated by TCR repertoire analysis, the reduction in CTL activity was not caused by stimulation of distinct populations of TCR clonotypes. This study demonstrates how a common eukaryotic posttranscriptional mechanism of gene regulation can modulate the endogenous presentation of Ag and ultimately contribute to the fine tuning of immunological memory cells, which are important in the fight against pathogens and tumors and in autoimmunity.

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Source
http://dx.doi.org/10.4049/jimmunol.165.4.1840DOI Listing

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