Introduction of a point mutation into an HLA class i single-chain trimer induces enhancement of CTL priming and antitumor immunity

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Abstract

We previously discovered one particular HLA-A∗02:01 mutant that enhanced peptide-specific cytotoxic T lymphocyte (CTL) recognition in vitro compared to wild-type HLA-A∗02:01. This mutant contains a single amino acid substitution from histidine to leucine at position 74 (H74L) that is located in the peptide-binding groove. To investigate the effect of the H74L mutation on the in vivo CTL priming, we took advantage of the technology of the HLA class I single-chain trimer (SCT) in which three components involving a peptide, β2 microglobulin and the HLA class I heavy chain are joined together via flexible linkers. We generated recombinant adenovirus expressing SCT comprised influenza A matrix protein (FMP)-derived peptide, β2 microglobulin and the H74L heavy chain. HLA-A∗02:01 transgenic mice were immunized with the adenovirus, and the induction of peptide-specific CTLs and antitumor immunity was investigated. It was clearly shown that the H74L mutation enabled the HLA-A∗02:01 SCT molecule to dramatically enhance both in vivo priming of FMP-specific CTLs and protection against a lethal challenge of tumor cells expressing FMP. These data present the first evidence that a simple point mutation in the HLA class I heavy chain of SCT is beneficial for improving CTL-based immunotherapy and prophylaxis to control tumors.

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Matsui, M., Kawano, M., Matsushita, S., & Akatsuka, T. (2014). Introduction of a point mutation into an HLA class i single-chain trimer induces enhancement of CTL priming and antitumor immunity. Molecular Therapy Methods and Clinical Development, 1, 14027. https://doi.org/10.1038/mtm.2014.27

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