Optimizing natural products by biosynthetic engineering: Discovery of nonquinone Hsp90 inhibitors

Ming Qiang Zhang; Sabine Gaisser; Mohammad Nur-E-Alam; Lesley S. Sheehan; William A. Vousden; Nikolaos Gaitatzis; Gerrard Peck; Nigel J. Coates; Steven J. Moss; Markus Radzom; Teresa A. Foster; Rose M. Sheridan; Matthew A. Gregory; S. Mark Roe; Chrisostomos Prodromou; Laurence Pearl; Susan M. Boyd; Barrie Wilkinson; Christine J. Martin

Journal Article

Optimizing natural products by biosynthetic engineering: Discovery of nonquinone Hsp90 inhibitors

Journal of Medicinal Chemistry (2008) 51(18) 5494-5497

DOI: 10.1021/jm8006068

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Abstract

A biosynthetic medicinal chemistry approach was applied to the optimization of the natural product Hsp90 inhibitor macbecin. By genetic engineering, mutants have been created to produce novel macbecin analogues including a nonquinone compound (5) that has significantly improved binding affinity to Hsp90 (Kd 3 nM vs 240 nM for macbecin) and reduced toxicity (MTD ≥ 250 mg/kg). Structural flexibility may contribute to the preorganization of 5 to exist in solution in the Hsp90-bound conformation. © 2008 American Chemical Society.

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Zhang, M. Q., Gaisser, S., Nur-E-Alam, M., Sheehan, L. S., Vousden, W. A., Gaitatzis, N., … Martin, C. J. (2008). Optimizing natural products by biosynthetic engineering: Discovery of nonquinone Hsp90 inhibitors. Journal of Medicinal Chemistry, 51(18), 5494–5497. https://doi.org/10.1021/jm8006068

Optimizing natural products by biosynthetic engineering: Discovery of nonquinone Hsp90 inhibitors

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