De novo macrolide-glycolipid macrolactone hybrids: Synthesis, structure and antibiotic activity of carbohydrate-fused macrocycles

Richard T Desmond; Anniefer N Magpusao; Chris Lorenc; Jeremy B Alverson; Nigel Priestley; Mark W Peczuh

doi:10.3762/bjoc.10.229

De novo macrolide-glycolipid macrolactone hybrids: Synthesis, structure and antibiotic activity of carbohydrate-fused macrocycles

Beilstein J Org Chem. 2014 Sep 17:10:2215-21. doi: 10.3762/bjoc.10.229. eCollection 2014.

Authors

Richard T Desmond¹, Anniefer N Magpusao¹, Chris Lorenc¹, Jeremy B Alverson², Nigel Priestley², Mark W Peczuh¹

Affiliations

¹ Department of Chemistry, University of Connecticut, 55 N. Eagleville Road, U3060, Storrs, CT 06269, USA, +1-860-486-1605 FAX: +1-860-486-2981.
² Department of Chemistry and Biochemistry, University of Montana, Missoula, MT 59812, USA.

Abstract

Natural product-like macrocycles were designed as potential antibacterial compounds. The macrocycles featured a D-glucose unit fused into a 12- or 13-member macrolactone. The rings are connected via the C6' and anomeric (C1') positions of the monosaccharide. The new macrocycles/macrolides were characterized by X-ray crystallography. Their structures showed that, in addition to the ester and alkene units, the dihedral angle about the glycosidic linkage (exo-anomeric effect) influenced the overall shape of the molecules. Glycosylation of an available hydroxy group on the macrocycle gave a hybrid macrolide with features common to erythromycin and sophorlipid macrolactone. Weak antibiotic activity (MICs <100 μg/mL) was observed for several of the compounds.

Keywords: antibiotic; carbohydrate; exo-anomeric effect; macrolide; structure; synthesis.