Issue 8, 2025

Total synthesis of linear lipodepsipeptide kavaratamide A and its C25-epimer

Abstract

We report the stereoselective total synthesis of kavaratamide A, a linear lipodepsipeptide from the cyanobacterium Moorena bouillonii (collected in Kavaratti, India), and its unnatural C25-epimer. The convergent approach employs Keck asymmetric allylation to construct the chiral β-hydroxy carboxylic acid fragment [(3S)-HDA; 3-hydroxydecanoic acid], while the peptide unit was assembled from L-Val, N-Me-L-Ala, (S)-Hiva, and (S)-iPr-O-Me-pyr using well-orchestrated coupling methods to prevent racemization. Modifications to the Keck allylation conditions enabled the synthesis of the C25-epimer with good yield. Cytotoxicity of kavaratamide A and C25-epi-kavaratamide A, assessed using the MTT assay, demonstrated moderate activity against HepG2 and PANC-1 cell lines.

Graphical abstract: Total synthesis of linear lipodepsipeptide kavaratamide A and its C25-epimer

Supplementary files

Article information

Article type
Communication
Submitted
05 Dec 2024
Accepted
06 Jan 2025
First published
07 Jan 2025

Org. Biomol. Chem., 2025,23, 1819-1822

Total synthesis of linear lipodepsipeptide kavaratamide A and its C25-epimer

M. R. Sahu, S. R. Ingale and R. Kontham, Org. Biomol. Chem., 2025, 23, 1819 DOI: 10.1039/D4OB01970A

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