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Department of Chemistry, Stanford University, Stanford, CA 94305
Solution studies have demonstrated the existence of two
functionally distinct isomers of empty class II MHC: an active isomer
that binds peptide and an inactive isomer that does not. Empty MHC
molecules on the surface of APCs can load antigenic peptides directly
from the extracellular medium, facilitating the generation of a diverse
peptide repertoire for T cell presentation. In this report, we examine
I-Ek on the surface of Chinese hamster ovary cells with respect to the
active and inactive isomers. As in the case of purified soluble active
I-Ek, active I-Ek on the cell surface is unstable, decaying to the
inactive form in
14 min. Evidence is presented suggesting that at
steady state <1% of the total cell surface I-Ek is active and that a
significant fraction of these active molecules originates from
intracellular pools as well as reactivation of inactive cell surface
I-Ek.
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