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Site-selective bromination of vancomycin.

Journal of the American Chemical Society (2012-04-03)
Tejas P Pathak, Scott J Miller
ABSTRACT

We report the site-selective bromination of vancomycin to produce, with substantial efficiency, previously unknown monobromovancomycins, a dibromovancomycin, and a tribromovancomycin. We document the inherent reactivity of native vancomycin toward N-bromophthalimide. We then demonstrate significant rate acceleration and perturbation of the inherent product distribution in the presence of a rationally designed peptide-based promoter. Alternative site selectivity is observed as a function of solvent and replacement of the peptide with guanidine.

MATERIALS
Product Number
Brand
Product Description

Sigma-Aldrich
N-Bromophthalimide, 95%