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Design and synthesis of 2-acetamidomethyl derivatives of isofagomine as potential inhibitors of human lysosomal beta-hexosaminidases
Authors:van den Berg Richard J B H N  Donker-Koopman Wilma  van Boom Jacques H  Aerts Hans M F G  Noort Daan
Affiliation:Leiden Institute of Chemistry, Gorlaeus Laboratories, University of Leiden, PO Box 9502, Leiden NL-2300 RA, The Netherlands.
Abstract:As part of a program towards the development of specific inhibitors of human lysosomal beta-hexosaminidase for use as chemical chaperones in therapy of G(M2) gangliosidosis related diseases, the synthesis of 2-acetamidomethyl derivatives of isofagomine has been undertaken. Key event in this synthesis is the conversion of a C-2 substituted gluconolactone derivative into the corresponding lactam, followed by reduction to the corresponding amine. The 1-N-imino-2 acetamidomethyl derivative 5 proved to be a rather selective inhibitor with a K(i) of 2.4 microM for homogenate of human spleen lysosomal beta-hexosaminidase.
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