ANALOGS OF SIALIC ACIDS AS POTENTIAL SIALIDASE INHIBITORS - SYNTHESIS OF 2-C-HYDROXYMETHYL DERIVATIVES OF N-ACETYL-6-AMINO-2,6-DIDEOXY-NEURAMINIC ACID

The intramolecular cycloaddition of the previously described azidoalkene 16, the related diacetates 7 and 13, and the monoacetate 8 led diastereoselectivity to the (2R)‐ and (2S)‐configurated hydropyridotriazoles 17, 9 and 11, 14 and 15, and 10 and 12, respectively (Scheme 1). Thermolysis of 16 gave also the aziridine 18, its proportion increasing with reaction time. The diastereoselectivity of the cycloaddition‐ is rationalized on the basis of steric interactions and of Hbonds in the transition state. Photolysis in benzene partially transformed 9 into the aziridine 19. Treatment of 9 with aqueous AcOH gave 19 and the tetrahydrofuran 20, with AcOH in benzene 20 and the triacetate 23, and with aqueous H2SO4 in THF, the primary alcohol 22 (room temperature) or 19 and 22 (0°). Deacetylation of 9 followed by reaction with pyridinium hydrochloride led to the tetrahydrofuran 21 and the chloride 24 (Scheme 2). The diacetate 22 and the triacetate 23 gave the tripl 25 which was deprotected to 26. Reduction of the keto‐aziridine 18 (NaBH4) gave the alcohols 27 and 29 which were acetylated to give 28 and 19, respectively (Scheme 3). Treatment of the aziridine 28 with AcOH in benzene followed by deacetylation gave 30 and hence 31. AcOH in benzene transformed the triazoline 15 first into the aziridine 32 and hence into 33, which was deprotected to give the triol 34 and hence 35. The 2‐(hydroxymethyl)piperidines 26, 31, and 35 inhibited Vibrio cholerae sialidase with K1 = 3.8 · 10−2 M, 3.4 · 10−3 M, and 1.5 · 10−4 M, respectively. The conformation of the glycerol side chain of these compounds and of the unbranched piperidines 2–4 deviates from the one of Neu5Ac (and Neu2en5Ac). This finding is rationalized by an H‐bond between OHC(8) and NHC(6). The conformations and the K1 values of 26, 31, and 35 correlate with each other. Copyright © 1990 Verlag GmbH & Co. KGaA, Weinheim