Journal article

Tapasin-mediated retention and optimization of peptide ligands during the assembly of class I molecules

MJ Barnden, AW Purcell, JJ Gorman, J McCluskey

Journal of Immunology | AMER ASSOC IMMUNOLOGISTS | Published : 2000

Abstract

The murine class I H-2Kb molecule achieves high level surface expression in tapasin-deficient 721.220 human cells. Compared with their behavior in wild-type cells, Kb molecules expressed on 721.220 cells are more receptive to exogenous peptide, undergo more rapid surface decay, and fail to form macromolecular peptide loading complexes. As a result, they are rapidly transported to the cell surface, reflecting a failure of endoplasmic reticulum retention mechanisms in the absence of loading complex formation. Despite the failure of Kb molecules to colocalize to the TAP and their rapid egress to the cell surface, Kb is still capable of presenting TAP-dependent peptides in the absence of tapasin..

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University of Melbourne Researchers