High affinity soluble ILT2 receptor: a potent inhibitor of CD8(+) T cell activation.

Ruth K Moysey; Yi LI; Samantha J Paston; Emma E Baston; Malkit S Sami; Brian J Cameron; Jessie Gavarret; Penio Todorov; Annelise Vuidepot; Steven M Dunn; Nicholas J Pumphrey; Katherine J Adams; Fang Yuan; Rebecca E Dennis; Deborah H Sutton; Andy D Johnson; Joanna E Brewer; Rebecca Ashfield; Nikolai M Lissin; Bent K Jakobsen

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High affinity soluble ILT2 receptor: a potent inhibitor of CD8(+) T cell activation.

Author: Ruth K MOYSEY ¹ ; Yi LI ; Samantha J PASTON ; Emma E BASTON ; Malkit S SAMI ; Brian J CAMERON ; Jessie GAVARRET ; Penio TODOROV ; Annelise VUIDEPOT ; Steven M DUNN ; Nicholas J PUMPHREY ; Katherine J ADAMS ; Fang YUAN ; Rebecca E DENNIS ; Deborah H SUTTON ; Andy D JOHNSON ; Joanna E BREWER ; Rebecca ASHFIELD ; Nikolai M LISSIN ; Bent K JAKOBSEN
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1. Immunocore Limited, 57c Milton Park, Abingdon, Oxon, OX14 4RX, UK.
Publication Type:Journal Article
MeSH: Amino Acid Sequence; Antigens, CD; chemistry; genetics; pharmacology; Autoimmunity; Biological Assay; Cell Line; Cytotoxicity, Immunologic; genetics; immunology; Dose-Response Relationship, Immunologic; Humans; Immunoglobulins; immunology; metabolism; Immunologic Factors; chemistry; genetics; pharmacology; Kinetics; Leukocyte Immunoglobulin-like Receptor B1; Lymphocyte Activation; genetics; immunology; Major Histocompatibility Complex; genetics; immunology; Molecular Sequence Data; Molecular Targeted Therapy; Mutagenesis, Site-Directed; Peptide Library; Polyethylene Glycols; Protein Binding; genetics; immunology; Receptors, Immunologic; chemistry; genetics; Recombinant Fusion Proteins; genetics; metabolism; T-Lymphocytes, Cytotoxic; immunology; metabolism
From: Protein & Cell 2010;1(12):1118-1127
CountryChina
Language:English
Abstract: Using directed mutagenesis and phage display on a soluble fragment of the human immunoglobulin super-family receptor ILT2 (synonyms: LIR1, MIR7, CD85j), we have selected a range of mutants with binding affinities enhanced by up to 168,000-fold towards the conserved region of major histocompatibility complex (MHC) class I molecules. Produced in a dimeric form, either by chemical cross-linking with bivalent polyethylene glycol (PEG) derivatives or as a genetic fusion with human IgG Fc-fragment, the mutants exhibited a further increase in ligand-binding strength due to the avidity effect, with resident half-times (t(1/2)) on the surface of MHC I-positive cells of many hours. The novel compounds antagonized the interaction of CD8 co-receptor with MHC I in vitro without affecting the peptide-specific binding of T-cell receptors (TCRs). In both cytokine-release assays and cell-killing experiments the engineered receptors inhibited the activation of CD8(+) cytotoxic T lymphocytes (CTLs) in the presence of their target cells, with subnanomolar potency and in a dose-dependent manner. As a selective inhibitor of CD8(+) CTL responses, the engineered high affinity ILT2 receptor presents a new tool for studying the activation mechanism of different subsets of CTLs and could have potential for the development of novel autoimmunity therapies.