Crawford Jason M, Thomas Paul M, Scheerer Jonathan R, Vagstad Anna L, Kelleher Neil L, Townsend Craig A
Department of Chemistry, Johns Hopkins University, Baltimore, MD21218, USA.
Science. 2008 Apr 11;320(5873):243-6. doi: 10.1126/science.1154711.
PksA, which initiates biosynthesis of the environmental carcinogen aflatoxin B1, is one of the multidomain iterative polyketide synthases (IPKSs), a large, poorly understood family of biosynthetic enzymes. We found that dissection of PksA and its reconstitution from selected sets of domains allows the accumulation and characterization of advanced octaketide intermediates bound to the enzyme, permitting the reactions controlled by individual catalytic domains to be identified. A product template (PT) domain unites with the ketosynthase and thioesterase in this IPKS system to assemble precisely seven malonyl-derived building blocks to a hexanoyl starter unit and mediate a specific cyclization cascade. Because the PT domain is common among nonreducing IPKSs, these mechanistic features should prove to be general for IPKS-catalyzed production of aromatic polyketides.
启动环境致癌物黄曲霉毒素B1生物合成的PksA是多结构域迭代聚酮合酶(IPKS)之一,这是一类庞大且了解甚少的生物合成酶家族。我们发现,对PksA进行拆分并从选定的结构域集合中进行重组,可以积累和表征与该酶结合的高级八酮中间体,从而确定由各个催化结构域控制的反应。在这个IPKS系统中,一个产物模板(PT)结构域与酮合成酶和硫酯酶结合,将七个丙二酰衍生的结构单元精确组装到一个己酰起始单元上,并介导特定的环化级联反应。由于PT结构域在非还原型IPKS中很常见,这些机制特征应该对IPKS催化的芳香族聚酮化合物的生产具有普遍意义。
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