Abstract
The first total synthesis of the alkaloid brevianamide S has been achieved in eight steps. This natural product, isolated from Aspergillus versicolor, exhibits selective antibacterial activity against Bacille Calmette-Guérin (BCG), a commonly used surrogate for Mycobacterium tuberculosis. Brevianamide S is proposed to act through a novel, yet-to-be-elucidated mechanism, making it a promising lead in the development of next-generation antitubercular agents. Our approach employs a bidirectional synthetic strategy, involving a bespoke alkenyl-alkenyl Stille cross-coupling reaction and a double aldol condensation. This represents a flexible and efficient platform for the future synthesis of structurally diverse analogues.
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CITATION STYLE
Lockyer, A. R., Jones, H. E., Green, N. J., Godfrey, R. C., Demertzidou, V. P., Nichol, G. S., & Lawrence, A. L. (2025). Total Synthesis of Brevianamide S. Organic Letters. https://doi.org/10.1021/acs.orglett.5c00860
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