Literature

Abstract

The second-generation synthesis of 3'-hydroxypacidamycin D (2) has been accomplished via an Ugi-four component reaction at a late stage of the synthesis. This approach provided ready access to a range of analogues including diastereomers of the diaminobutylic acid residue and hybrid-type analogues of mureidomycins. Biological evaluations of these analogues indicated that the stereochemistry at the diaminobutylic acid residue has a crucial impact on both the MraY biochemical inhibition and whole-cell antibacterial activity.

DOI： 10.1016/j.bmcl.2012.05.050

Synthesis of pacidamycin analogues via an Ugi-multicomponent reaction

Bioorganic & Medicinal Chemistry Letters 2012.0

Synthesis and Biological Evaluation of Muraymycin Analogues Active against Anti-Drug-Resistant Bacteria

ACS Medicinal Chemistry Letters 2010.0

Synthetic dihydropacidamycin antibiotics

Bioorganic & Medicinal Chemistry Letters 2003.0

Mechanistic Analysis of Muraymycin Analogues: A Guide to the Design of MraY Inhibitors

Journal of Medicinal Chemistry 2011.0

One-pot synthesis and biological evaluation of aspergillamides and analogues

Bioorganic & Medicinal Chemistry Letters 2000.0

Synthesis and preliminary biological evaluation of a small library of hybrid compounds based on Ugi isocyanide multicomponent reactions with a marine natural product scaffold