Abstract
Background: Qa-2 is a nonclassical MHC Ib antigen, which has been implicated in both innate and adaptive immune responses, as well as embryonic development. Qa-2 has an unusual peptide binding specificity in that it requires two dominant C-terminal anchor residues and is capable of associating with a substantially more diverse array of peptide sequences than other nonclassical MHC. Results: We have determined the crystal structure, to 2.3 Å, of the Q9 gene of murine Qa-2 complexed with a self-peptide derived from the L19 ribosomal protein, which is abundant in the pool of peptides eluted from the Q9 groove. The 9 amino acid peptide is bound high in a shallow, hydrophobic binding groove of Q9, which is missing a C pocket. The peptide makes few specific contacts and exhibits extremely poor shape complementarity to the MHC groove, which facilitates the presentation of a degenerate array of sequences. The L19 peptide is in a centrally bulged conformation that is stabilized by intramolecular interactions from the invariant P7 histidine anchor residue and by a hydrophobic core of preferred secondary anchor residues that have minimal interaction with the MHC. Conclusions: Unexpectedly, the preferred secondary peptide residues that exhibit tenuous contact with Q9 contribute significantly to the overall stability of the peptide-MHC complex. The structure of this complex implies a "conformational" selection by Q9 for peptide residues that optimally stabilize the large bulge rather than making intimate contact with the MHC pockets.
Original language | English (US) |
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Pages (from-to) | 1213-1224 |
Number of pages | 12 |
Journal | Structure |
Volume | 9 |
Issue number | 12 |
DOIs | |
State | Published - 2001 |
Funding
We thank D.-C. Chow for assistance with data collection, E.J. Adams for comments on the manuscript, I.A. Wilson for discussion, and the staff of the Stanford Synchrotron Radiation Laboratory for beamline resources and support. K.C.G. is funded by National Institutes of Health grant RO1 AI48540, the March of Dimes, the Multiple Sclerosis Society, and the Rita Allen Foundation. X.H. is supported by the American Heart Association and the California Cancer Research Program. I.S. is supported by National Institutes of Health grants RO1 AI 19624 and PO1 AI 37818.
Keywords
- Immune recognition
- MHC
- Nonclassical
- Structure
- X-ray crystallography
ASJC Scopus subject areas
- Structural Biology
- Molecular Biology