Structure of NKp65 bound to its keratinocyte ligand reveals basis for genetically linked recognition in natural killer gene complex

The natural killer (NK) gene complex (NKC) encodes numerous C-type lectin-like receptors that govern the activity of NK cells. Although some of these receptors (Ly49s, NKG2D, CD94/NKG2A) recognize MHC or MHC-like molecules, others (Nkrp1, NKRP1A, NKp80, NKp65) instead bind C-type lectin-like ligands...

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Published in:Proceedings of the National Academy of Sciences - PNAS 2013-07, Vol.110 (28), p.11505-11510
Main Authors: Li, Yili, Wang, Qian, Chen, Sharon, Brown, Patrick H., Mariuzza, Roy A.
Format: Article
Language:English
Subjects:
Amino Acid Sequence
Atoms
B lymphocytes
Biochemistry
Biological Sciences
Crystal structure
Dimers
Genetics
Human genetics
Humans
Hydrogen bonds
Keratinocytes - metabolism
Ligands
Models, Molecular
Molecular biology
Molecular Sequence Data
Molecules
Mutation
Natural killer cells
Protein Conformation
Proteins
Receptors
Receptors, NK Cell Lectin-Like - chemistry
Receptors, NK Cell Lectin-Like - genetics
Receptors, NK Cell Lectin-Like - metabolism
Sequence Homology, Amino Acid
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Summary:The natural killer (NK) gene complex (NKC) encodes numerous C-type lectin-like receptors that govern the activity of NK cells. Although some of these receptors (Ly49s, NKG2D, CD94/NKG2A) recognize MHC or MHC-like molecules, others (Nkrp1, NKRP1A, NKp80, NKp65) instead bind C-type lectin-like ligands to which they are genetically linked in the NKC. To understand the basis for this recognition, we determined the structure of human NKp65, an activating receptor implicated in the immunosurveillance of skin, bound to its NKC-encoded ligand keratinocyte-associated C-type lectin (KACL). Whereas KACL forms a homodimer resembling other C-type lectin-like dimers, NKp65 is monomeric. The binding mode in the NKp65–KACL complex, in which a monomeric receptor engages a dimeric ligand, is completely distinct from those used by Ly49s, NKG2D, or CD94/NKG2A. The structure explains the exceptionally high affinity of the NKp65–KACL interaction compared with other cell–cell interaction pairs (K D = 6.7 × 10 ⁻¹⁰ M), which may compensate for the monomeric nature of NKp65 to achieve cell activation. This previously unreported structure of an NKC-encoded receptor–ligand complex, coupled with mutational analysis of the interface, establishes a docking template that is directly applicable to other genetically linked pairs in the NKC, including Nkrp1–Clr, NKRP1A–LLT1, and NKp80–AICL.
ISSN:0027-8424
1091-6490
DOI:10.1073/pnas.1303300110