Promiscuous Antigen Presentation by the Nonclassical MHC Ib Qa-2 is Enabled by a Shallow, Hydrophobic Groove and Self-stabilized Peptide Conformation

Overview

Journal Structure

Publisher Cell Press

Specialties Biochemistry
Biotechnology
Cell Biology
Molecular Biology

Date 2001 Dec 12

PMID 11738047

Citations 18

Authors

X He

P Tabaczewski

J Ho

I Stroynowski

K C Garcia

Affiliations

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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 A, 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.

Citing Articles

New Insights Into the Role of Qa-2 and HLA-G Non-classical MHC-I Complexes in Malignancy.

da Silva I, Montero-Montero L, Ferreira E, Quintanilla M Front Immunol. 2018; 9:2894.

PMID: 30574154 PMC: 6292030. DOI: 10.3389/fimmu.2018.02894.

Recognition of the Major Histocompatibility Complex (MHC) Class Ib Molecule H2-Q10 by the Natural Killer Cell Receptor Ly49C.

Sullivan L, Berry R, Sosnin N, Widjaja J, Deuss F, Balaji G J Biol Chem. 2016; 291(36):18740-52.

PMID: 27385590 PMC: 5009249. DOI: 10.1074/jbc.M116.737130.

The role of MHC class Ib-restricted T cells during infection.

Anderson C, Brossay L Immunogenetics. 2016; 68(8):677-91.

PMID: 27368413 PMC: 5003733. DOI: 10.1007/s00251-016-0932-z.

Expression and alternative splicing of classical and nonclassical MHCI genes in the hippocampus and neuromuscular junction.

Tetruashvily M, Melson J, Park J, Peng X, Boulanger L Mol Cell Neurosci. 2016; 72:34-45.

PMID: 26802536 PMC: 4821772. DOI: 10.1016/j.mcn.2016.01.005.

Peptide immunization elicits polyomavirus-specific MHC class ib-restricted CD8 T cells in MHC class ia allogeneic mice.

Hofstetter A, Evavold B, Lukacher A Viral Immunol. 2013; 26(1):109-13.

PMID: 23374150 PMC: 3578367. DOI: 10.1089/vim.2012.0052.