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Total Synthesis and Antibacterial Investigation of Plusbacin A3.

Akira KatsuyamaAtmika PaudelSuresh PantheeHiroshi HamamotoToru KawakamiHironobu HojoFumika YakushijiSatoshi Ichikawa
Published in: Organic letters (2017)
The total synthesis of plusbacin A3 (1) has been accomplished using a solvent-dependent diastereodivergent Joullié-Ugi three-component reaction (JU-3CR) as a key step. Two trans-3-hydroxy-l-proline residues were constructed by combining the JU-3CR with a convertible isocyanide strategy. Subsequent peptide coupling and macrolactamization afforded plusbacin A3. Investigating the antibacterial activity of 1 compared with that of its dideoxy analogue revealed that the threo-β-hydroxyaspartic acid residues are essential for antibacterial activity. Notably, there is a low potential for the development of resistance in S. aureus against plusbacin A3.
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