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Use of a Phosphonate Methyltransferase in the Identification of the Fosfazinomycin Biosynthetic Gene Cluster
Authors:Dr. Jiangtao Gao  Dr. Kou‐San Ju  Xiaomin Yu  Dr. Juan E. Velásquez  Subha Mukherjee  Dr. Jaeheon Lee  Dr. Changming Zhao  Dr. Bradley S. Evans  Dr. James R. Doroghazi  Prof. William W. Metcalf  Prof. Wilfred A. van der Donk
Affiliation:1. Institute for Genomic Biology, University of Illinois at Urbana‐Champaign (USA);2. University of Illinois at Urbana‐Champaign, Department of Microbiology, 601 South Goodwin Avenue, Urbana, IL 61801 (USA);3. University of Illinois at Urbana‐Champaign, Howard Hughes Medical Institute and Department of Chemistry, 600 South Mathews Avenue, Urbana, IL 61801 (USA)
Abstract:Natural product discovery has been boosted by genome mining approaches, but compound purification is often still challenging. We report an enzymatic strategy for “stable isotope labeling of phosphonates in extract” (SILPE) that facilitates their purification. We used the phosphonate methyltransferase DhpI involved in dehydrophos biosynthesis to methylate a variety of phosphonate natural products in crude spent medium with a mixture of labeled and unlabeled S‐adenosyl methionine. Mass‐guided fractionation then allowed straightforward purification. We illustrate its utility by purifying a phosphonate that led to the identification of the fosfazinomycin biosynthetic gene cluster. This unusual natural product contains a hydrazide linker between a carboxylic acid and a phosphonic acid. Bioinformatic analysis of the gene cluster provides insights into how such a structure might be assembled.
Keywords:antibiotics  biosynthesis  hydrazine  natural products
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