Total synthesis of antifungal lipopeptide iturin A analogues and evaluation of their bioactivity against F. graminearum

Author:

Karamanis Periklis12,Muldoon Jimmy1,Murphy Cormac D.23,Rubini Marina12ORCID

Affiliation:

1. UCD School of Chemistry University College Dublin Dublin Ireland

2. BiOrbic Bioeconomy SFI Research Centre University College Dublin Dublin Ireland

3. UCD School of Biomolecular and Biomedical Science University College Dublin Dublin Ireland

Abstract

The pursuit of novel antifungal agents is imperative to tackle the threat of antifungal resistance, which poses major risks to both human health and to food security. Iturin A is a cyclic lipopeptide, produced by Bacillus sp., with pronounced antifungal properties against several pathogens. Its challenging synthesis, mainly due to the laborious synthesis of the β‐amino fatty acid present in its structure, has hindered the study of its mode of action and the development of more potent analogues. In this work, a facile synthesis of bioactive iturin A analogues containing an alkylated cysteine residue is presented. Two analogues with opposite configurations of the alkylated cysteine residue were synthesized, to evaluate the role of the stereochemistry of the newly introduced amino acid on the bioactivity. Antifungal assays, conducted against F. graminearum, showed that the novel analogues are bioactive and can be used as a synthetic model for the design of new analogues and in structure–activity relationship studies. The assays also highlight the importance of the β‐amino acid in the natural structure and the role of the stereochemistry of the amino fatty acid, as the analogue with the D configuration showed stronger antifungal properties than the one with the L configuration.

Funder

Science Foundation Ireland

Publisher

Wiley

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