Several polyhydroxyperhydroazepines have been obtained either by
chemoenzymatic or chemical synthesis.
Condensation of (±)-3-azido-2-hydroxypropanaldehyde and
dihydroxyacetone phosphate (DHAP) in the presence
of a DHAP dependent aldolase followed by treatment with acid
phosphatase and an isomerase gave a 6-azido-6-deoxyaldopyranose, which upon reductive amination afforded the title
compound. The iminocyclitols can also be
obtained by chemical manipulations of aldopyranoses, protected as
benzyl glycosides or diisopropylidene ethers.
Thus, d-galactose leads to a
meso-3,4,5,6-tetrahydroxyperhydroazepine,
d-mannose to a derivative with a C
2
symmetry
axis, and N-acetylglucosamine to a 6-acetamidoiminocyclitol.
Asymmetrization of the meso azasugar was
carried
out by chemical means, to yield a 3-methoxy-4,5,6-trihydroxyazepane.
An attempted enzymatic synthesis of the
methoxy derivatives of these azasugars was unsuccessful, leading,
however, to both enantiomers of 1-deoxy-2-O-methylmannojirimycin. Some of these compounds display significant
activity as glycosidase inhibitors, with
K
i
values from moderate to low micromolar range. Though all these
iminocyclitols do not inhibit the mechanistically
related HIV protease, the 3,6-dibenzyl derivative 30 showed
moderate inhibition. The X-ray structure of 7
indicates
a pseudochair conformation.
Several sialyl Lewis X (SLex) mimics that contain the
essential functional groups for receptor interaction
and a negative charge or a hydrophobic group have been developed as
inhibitors of E-, P-, and L-selectins. Some
of the mimics exhibit selectin inhibition activities
103−104-fold more potent than does the
natural ligand tetrasaccharide,
with IC50 in the low micromolar to high nanomolar range.
The syntheses of these mimics are relatively simple,
using TMSOTf-Ac2O mediated C-glycosylation with
concurrent selective deprotection of the primary benzyl
group
and enzymatic aldol addition reactions as key steps.
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