Molecules (Feb 2018)

Probing the Influence of Linker Length and Flexibility in the Design and Synthesis of New Trehalase Inhibitors

  • Giampiero D’Adamio,
  • Matilde Forcella,
  • Paola Fusi,
  • Paolo Parenti,
  • Camilla Matassini,
  • Xhenti Ferhati,
  • Costanza Vanni,
  • Francesca Cardona

DOI
https://doi.org/10.3390/molecules23020436
Journal volume & issue
Vol. 23, no. 2
p. 436

Abstract

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This work aims to synthesize new trehalase inhibitors selective towards the insect trehalase versus the porcine trehalase, in view of their application as potentially non-toxic insecticides and fungicides. The synthesis of a new pseudodisaccharide mimetic 8, by means of a stereoselective α-glucosylation of the key pyrrolizidine intermediate 13, was accomplished. The activity of compound 8 as trehalase inhibitor towards C. riparius trehalase was evaluated and the results showed that 8 was active in the μM range and showed a good selectivity towards the insect trehalase. To reduce the overall number of synthetic steps, simpler and more flexible disaccharide mimetics 9–11 bearing a pyrrolidine nucleus instead of the pyrrolizidine core were synthesized. The biological data showed the key role of the linker chain’s length in inducing inhibitory properties, since only compounds 9 (α,β-mixture), bearing a two-carbon atom linker chain, maintained activity as trehalase inhibitors. A proper change in the glucosyl donor-protecting groups allowed the stereoselective synthesis of the β-glucoside 9β, which was active in the low micromolar range (IC50 = 0.78 μM) and 12-fold more potent (and more selective) than 9α towards the insect trehalase.

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