An Unusual Role for a Mobile Flavin in StaC-like Indolocarbazole Biosynthetic Enzymes

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• 作者：Peter?J. Goldman ; Katherine?S. Ryan ; Michael?J. Hamill ; Annaleise?R. Howard-Jones ; Christopher?T. Walsh ; Sean?J. Elliott ; Catherine?L. Drennan
• 刊名：Chemistry & Biology
• 出版年：2012
• 出版时间：27 July, 2012
• 年：2012
• 卷：19
• 期：7
• 页码：855-865
• 全文大小：1960 K

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Summary

The indolocarbazole biosynthetic enzymes StaC, InkE, RebC, and AtmC mediate the degree of oxidation of chromopyrrolic acid on route to the natural products staurosporine, K252a, rebeccamycin, and AT2433-A1, respectively. Here, we show that StaC and InkE, which mediate a net 4-electron oxidation, bind FAD with a micromolar K_d, whereas RebC and AtmC, which mediate a net 8-electron oxidation, bind FAD with a nanomolar K_d while displaying the same FAD redox properties. We further create RebC-10x, a RebC protein with ten StaC-like amino acid substitutions outside of previously characterized FAD-binding motifs and the complementary StaC-10x. We find that these mutations mediate both FAD affinity and product specificity, with RebC-10x displaying higher StaC activity than StaC itself. X-ray structures of this StaC catalyst identify the substrate of StaC as 7-carboxy-K252c and suggest a unique mechanism for this FAD-dependent enzyme.