Structural elucidation of the m157 mouse cytomegalovirus ligand for Ly49 natural killer cell receptors
| Autor: | K. Christopher Garcia, Erin J. Adams, Rayna Takaki Venook, Lewis L. Lanier, Hisashi Arase, Martin J. Boulanger, Z. Sean Juo |
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| Rok vydání: | 2007 |
| Předmět: |
Models
Molecular Muromegalovirus Protein Conformation Viral protein chemical and pharmacologic phenomena Crystallography X-Ray Ligands Lymphoma T-Cell Major histocompatibility complex medicine.disease_cause Protein Structure Secondary Natural killer cell Mice Antigen Cell Line Tumor MHC class I medicine Animals Antigens Ly Lectins C-Type Disulfides Receptors Immunologic Receptor Binding Sites Multidisciplinary biology Histocompatibility Antigens Class I Hydrogen Bonding Biological Sciences MHC restriction Ligand (biochemistry) Protein Structure Tertiary Cell biology Killer Cells Natural medicine.anatomical_structure biology.protein Baculoviridae NK Cell Lectin-Like Receptor Subfamily A Protein Binding Receptors NK Cell Lectin-Like |
| Zdroj: | Proceedings of the National Academy of Sciences. 104:10128-10133 |
| ISSN: | 1091-6490 0027-8424 |
| Popis: | Natural killer (NK) cells express activating and inhibitory receptors that, in concert, survey cells for proper expression of cell surface major histocompatibility complex (MHC) class I molecules. The mouse cytomegalovirus encodes an MHC-like protein, m157, which is the only known viral antigen to date capable of engaging both activating (Ly49H) and inhibitory (Ly49I) NK cell receptors. We have determined the 3D structure of m157 and studied its biochemical and cellular interactions with the Ly49H and Ly49I receptors. m157 has a characteristic MHC-fold, yet possesses several unique structural features not found in other MHC class I-like molecules. m157 does not bind peptides or other small ligands, nor does it associate with β2-microglobulin. Instead, m157 engages in extensive intra- and intermolecular interactions within and between its domains to generate a compact minimal MHC-like molecule. m157's binding affinity for Ly49I (Kd≈ 0.2 μM) is significantly higher than that of classical inhibitory Ly49–MHC interactions. Analysis of viral escape mutations on m157 that render it resistant to NK killing reveals that it is likely to be recognized by Ly49H in a binding mode that differs from Ly49/MHC-I. In addition, Ly49H+ NK cells can efficiently lyse RMA cells expressing m157, despite the presence of native MHC class I. Collectively, our results show that m157 represents a structurally divergent form of MHC class I-like proteins that directly engage Ly49 receptors with appreciable affinity in a noncanonical fashion. |
| Databáze: | OpenAIRE |
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