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Glycosylation of an N-Acetylated Glucosamine Disaccharide Using an Orthogonally Protected 3-Iodo-Kdo Fluoride Donor.

作者信息

Goto Takaaki, Blaukopf Markus, Stöger Berthold, Pantophlet Ralph, Kerner Lukáš, Kosma Paul

机构信息

Institute of Organic Chemistry, University of Natural Resources and Life Sciences-Vienna, Muthgasse 18, A-1190, Vienna, Austria.

X-Ray Center (XRC), University of Technology Vienna, Lehargasse 4, A-1060, Vienna, Austria.

出版信息

ChemistryOpen. 2025 Apr 14:e2500141. doi: 10.1002/open.202500141.

DOI:10.1002/open.202500141
PMID:40223430
Abstract

Kdo (3-Deoxy-d-manno-oct-2-ulosonic acid) is an essential sugar found in bacterial lipopolysaccharides with significant biomedical relevance. This study introduces an orthogonally protected 3-iodo-Kdo fluoride donor and demonstrates its coupling to a pre-synthesized β-(1→6)-linked N-acetylglucosamine disaccharide acceptor as an example. Nuclear magnetic resonance data indicates the presence of an intraresidue hydrogen bond in the distal glucosamine unit. Two complementary glycosylation approaches are explored with an emphasis on achieving high stereoselectivity and minimizing protecting-group manipulation. The orthogonal protection of 3-iodo Kdo fluoride donor offers insights into tailoring Kdo-based donors for specific biomedical applications. While yields vary depending on the approach, they are sufficient to demonstrate the donor's applicability. These findings enable the design of advanced glycomimetic constructs for therapeutic and vaccine research.

摘要

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