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. 2003 Oct 31;68(22):8465-70.
doi: 10.1021/jo034837z.

Synthesis and evaluation of macrocyclic transition state analogue inhibitors for alpha-chymotrypsin

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Synthesis and evaluation of macrocyclic transition state analogue inhibitors for alpha-chymotrypsin

Kristina K Hansen et al. J Org Chem. .

Abstract

Lactams 1 and 2 are readily formed from acyclic precursors in the presence of trypsin and chymotrypsin, respectively, identifying the macrocyclic ring system as a potential motif for constrained transition state analogue inhibitors of the serine peptidases. Ketone 3 was synthesized and shown to be a modest inhibitor of chymotrypsin (Ki = 220 microM), albeit 4-fold more potent than the acyclic hydroxy acid 25 (Ki = 1.5 mM as a mixture of epimers). A precursor (31) to the amino boronic acid 4 was also prepared; although this derivative was a potent inhibitor of chymotrypsin (Ki = 130 nM) by virtue of the boronic acid moiety, it showed no advantage over the des-amino analogue 32 (Ki = 120 nM), which is not capable of cyclizing.

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