4.1 Article

Inhibition of Galectins with Small Molecules

Journal

CHIMIA
Volume 65, Issue 1-2, Pages 18-23

Publisher

SWISS CHEMICAL SOC
DOI: 10.2533/chimia.2011.18

Keywords

Cancer; Galectin; Immunity; Inflammation; Inhibitor

Funding

  1. Swedish Research Council
  2. Royal Fysiographic Society, Lund

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Evidence that the galectin family of proteins plays crucial roles in cancer, inflammation, and immunity has accumulated over the last decade. The galectins have consequently emerged as interesting drug targets. A majority of galectin functions occurs by means of cross-linking glycoproteins and by doing so controlling gly-coproteirl cellular localization and residence times. The glycoprotein cross-linking occurs when galectin dimers or multimers, or galectins with two binding sites, bind galactose-containing glycans of the glycoproteins. Such galectin-glycan interactions have been successfully blocked with compounds having multivalent presentation of galactose, lactose, or N-acetyllactosamine, with peptides, and with small carbohydrate (galactose) derivatives. This review summarizes and analyzes attempts to develop efficient and selective small-molecule galectin inhibitors through derivatization of monosaccharides, mainly galactosides, with non-carbohydrate structures that protrude into subsites adjacent to the core-conserved galactose-recognizing site of the galectins.

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