Combinatorial library of moenomycin analogs and methods of producing same

Assignee

• Advanced Medicine, Inc. · US

Inventors

• Nigel Mark Allanson · Princeton, US
• Tin-Yau Chan · Edison, US
• Nicole T. Hatzenbuhler · Bound Brook, US
• Rakesh K. Jain · Penfield, US
• Ramesh Kakarla · Doylestown, US
• Rui Liang · Plainsboro, US
• Dashan Liu · East Brunswick Township, US
• Domingos J. Silva · Collegeville, US
• Michael Joseph Sofia · Carmel, US

Key dates

Classification

• Technology area (CPC C)Chemistry; Metallurgy
• CPC primaryC40B40/00
• WIPO fieldOrganic fine chemistry
• WIPO sectorChemistry

Abstract

A combinatorial chemical library of compounds structurally related to the moenomycin class of antibiotics has the formula ##STR1## wherein D is a donor mono- or disaccharide, A is an acceptor monosaccharide, and P-R is a lipophosphoglycerate mimetic group. Members of the library have a glycosidic linkage between the anomeric carbon of D and the C2 carbon of A, and the D-A moiety is in turn covalently linked through the anomeric carbon of A to the P-R group. Members of the library exhibit their greatest structural diversity in terms of substitutions occurring at the C3 position of the A residue, substitutions at the C2 position of the D residue, and different P-R groups used in assembling the compounds. Members of the library are preferably synthesized by solid phase techniques involving stepwise coupling of the respective units to a support, functionalizing the A and/or D saccharides either before or after immobilizing them on the support, and cleaving the assembled compounds from the support. Preferred functionalities attached to the sugar residues are amides, carbamates, ureas, sulfonamides, substituted amines, esters, carbonates, and sulfates. Exemplary P-R groups are derivative…