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Centre dImmunologie de Marseille-Luminy, 13288 Marseille cedex 9, France
Exogenous Ags taken up from the fluid phase can be presented by
both newly synthesized and recycling MHC class II molecules. However,
the presentation of Ags internalized through the B cell receptor (BCR)
has not been characterized with respect to whether the class II
molecules with which they become associated are newly synthesized or
recycling. We show that the presentation of Ag taken up by the BCR
requires protein synthesis in splenic B cells and in B lymphoma cells.
Using B cells transfected with full-length I-Ak molecules
or molecules truncated in cytoplasmic domains of their
- or
ß-chains, we further show that when an Ag is internalized by the BCR,
the cytoplasmic tails of class II molecules differentially control the
presentation of antigenic peptides to specific T cells depending upon
the importance of proteolytic processing in the production of that
peptide. Integrity of the cytoplasmic tail of the I-Ak
ß-chain is required for the presentation of the hen egg lysozyme
determinant (4661) following BCR internalization, but that dependence
is not seen for the (3445) determinant derived from the same protein.
The tail of the ß-chain is also of importance for the dissociation of
invariant chain fragments from class II molecules. Our results
demonstrate that Ags internalized through the BCR are targeted to
compartments containing newly synthesized class II molecules and that
the tails of class II ß-chains control the loading of determinants
produced after extensive Ag processing.
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