Chemical Glucosylation of Labile Natural Products Using a (2-Nitrophenyl)acetyl-Protected Glucosyl Acetimidate Donor

Julia Weber; Markus Schwarz; Andrea Schiefer; Christian Hametner; Georg Häubl; Johannes Fröhlich; Hannes Mikula

doi:10.1002/ejoc.201800260

Chemical Glucosylation of Labile Natural Products Using a (2-Nitrophenyl)acetyl-Protected Glucosyl Acetimidate Donor

European J Org Chem. 2018 Jun 7;2018(20-21):2701-2706. doi: 10.1002/ejoc.201800260. Epub 2018 Apr 26.

Authors

Julia Weber¹, Markus Schwarz¹, Andrea Schiefer¹, Christian Hametner¹, Georg Häubl², Johannes Fröhlich¹, Hannes Mikula¹

Affiliations

¹ Institute of Applied Synthetic Chemistry Vienna University of Technology (TU Wien) Getreidemarkt 9 1060 Vienna Austria.
² Romer Labs Technopark 1 3430 Tulln/Donau Austria.

Abstract

The synthesis of (2-nitrophenyl)acetyl (NPAc)-protected glucosyl donors is described that were designed for the neighboring-group assisted glucosylation of base-labile natural products also being sensitive to hydrogenolysis. Glycosylation conditions were optimized using a trichloroacetimidate glucosyl donor, and cyclohexylmethanol and (+)-menthol as model acceptors. The approach was then extended to a one-pot procedure for the synthesis of 1,2-trans-glycosides. This method was finally applied for improved synthesis of the masked mycotoxin T2-O-β,d-glucoside.

Keywords: Diastereoselectivity; Glycosylation; Natural products; Neighboring‐group effects; Protecting groups.