NKG2D and CD94 bind to multimeric α2,3-linked N-acetylneuraminic acid

Abstract

Killer lectin-like receptors on natural killer cells mediate cytotoxicity through glycans on target cells including the sialyl Lewis X antigen (sLeX). We investigated whether NK group 2D (NKG2D) and CD94 can bind to sialylated N-linked glycans, using recombinant glutathione S-transferase-fused extracellular lectin-like domains of NKG2D (rNKG2Dlec) and CD94 (rCD94lec). Both rNKG2Dlec and rCD94lec bound to plates coated with high-sLeX-expressing transferrin secreted by HepG2 cells (HepTF). The binding of rNKG2Dlec and rCD94lec to HepTF was markedly suppressed by treatment of HepTF with neuraminidase and in the presence of N-acetylneuraminic acid. Moreover, rNKG2Dlec and rCD94lec bound to α2,3-sialylated human α 1-acid glycoprotein (AGP) but not to α2,6-sialylated AGP. Mutagenesis revealed that 152Y of NKG2D and 144F and 160N of CD94 were critical for HepTF binding. This is the first report that NKG2D and CD94 bind to α2,3-sialylated but not to α2,6-sialylated multi-antennary N-glycans.