부산대학교 도서관

Galectin-1 is a component of the extracellular matrix as well as a ligand of cell surface counter receptors such as [beta]-galactoside-containing glycolipids, however, the molecular mechanism of galectin-1 secretion has remained elusive. Based on a nonbiased screen for galectin-1 export mutants we have identified 26 single amino acid changes that cause a defect of both export and binding to counter receptors. When wild-type galectin-1 was analyzed in CHO clone 13 cells, a mutant cell line incapable of expressing functional galectin-1 counter receptors, secretion was blocked. Intriguingly, we also find that a distant relative of galectin-1, the fungal lectin CGL-2, is a substrate for nonclassical export from Chinese hamster ovary (CHO) cells. Alike mammalian galectin-1, a CGL-2 mutant defective in [beta]-galactoside binding, does not get exported from CHO cells. We conclude that the [beta]-galactoside binding site represents the primary targeting motif of galectins defining a galectin export machinery that makes use of [beta]-galactoside-containing surface molecules as export receptors for intracellular galectin-1.