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Abstract
A two-step route to MK-4482 (EIDD-2801, 1) was developed consisting of an
esterification and hydroxamination of cytidine.
The reactions can be conducted in either order with overall yields of
67% (first step—esterification) and 37% (first step—hydroxamination). Selective
esterification of the nucleoside’s primary alcohol by enzymatic means
eliminated the need for diol protection/deprotection, and direct transamination
with hydroxylamine precluded the necessity of activating the nucleobase for
amine coupling. This results in a significant
advancement over the reported synthesis which is formed in at best 17%
yield. The step count is reduced from
five transformation to two, and the more expensive uridine is replaced with the
more available cytidine.
Supplementary materials
Title
2020 08 17 Supporting Information
Description
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