Radicicol-sensitive Peptide Binding to the N-terminal Portion of GRP94
GRP94 is a molecular chaperone that carries immunologically relevant peptides from cell to cell, transferring them to major histocompatibility proteins for presentation to T cells. Here we examine the binding of several peptides to recombinant GRP94 and study the regulation and site of peptide bindi...
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Veröffentlicht in: | The Journal of biological chemistry 2002-10, Vol.277 (43), p.40742-40750 |
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Sprache: | eng |
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Zusammenfassung: | GRP94 is a molecular chaperone that carries immunologically relevant peptides from cell to cell, transferring them to major
histocompatibility proteins for presentation to T cells. Here we examine the binding of several peptides to recombinant GRP94
and study the regulation and site of peptide binding. We show that GRP94 contains a peptide-binding site in its N-terminal
355 amino acids. A number of peptides bind to this site with low on- and off-rates and with specificity that is distinct from
that of another endoplasmic reticulum chaperone, BiP/GRP78. Binding to the N-terminal fragment is sufficient to account for
the peptide binding activity of the entire molecule. Peptide binding is inhibited by radicicol, a known inhibitor of the chaperone
activities of HSP90-family proteins. However, the peptide-binding site is distinct from the radicicol-binding pocket, because
both can bind to the N-terminal fragment simultaneously. Furthermore, peptide binding does not cause the same conformational
change as does binding of radicicol. When the latter binds to the N-terminal domain, it induces a conformational change in
the downstream, acidic domain of GRP94, as measured by altered gel mobility and loss of an antibody epitope. These results
relate the peptide-binding activity of GRP94 to its other function as a chaperone. |
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ISSN: | 0021-9258 1083-351X |
DOI: | 10.1074/jbc.M205323200 |