AI Article Synopsis
- The study investigates how certain viral peptides, particularly PA(224-233), can stimulate CD8(+) T cell responses, highlighting the unusual properties of this peptide.
- It reveals that PA(224-233) forms a large pool in the cytoplasm for extended periods, which aids in its effective presentation despite the inhibition of protein synthesis.
- The research suggests that the lack of strong immune responses from natural proteasome products is due to their rapid degradation, rather than an inability to be presented by antigen-presenting cells.
Article Abstract
The nature of crosspriming immunogens for CD8(+) T cell responses is highly controversial. By using a panel of T cell receptor-like antibodies specific for viral peptides bound to mouse D(b) major histocompatibility complex class I molecules, we show that an exceptional peptide (PA(224-233)) expressed as a viral minigene product formed a sizeable cytosolic pool continuously presented for hours after protein synthesis was inhibited. PA(224-233) pool formation required active cytosolic heat-shock protein 90 but not ER g96 and uniquely enabled crosspriming by this peptide. These findings demonstrate that exceptional class I binding oligopeptides that escape proteolytic degradation are potent crosspriming agents. Thus, the feeble immunogenicity of natural proteasome products in crosspriming can be attributed to their evanescence in donor cells and not an absolute inability of cytosolic oligopeptides to be transferred to and presented by professional antigen-presenting cells.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2587262 | PMC |
| http://dx.doi.org/10.1016/j.immuni.2008.04.015 | DOI Listing |
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