AI Article Synopsis

  • Asukamycin, an antimicrobial and potential antitumor agent, is isolated from Streptomyces nodosus and its biosynthetic gene cluster has been successfully cloned and expressed in Streptomyces lividans.
  • The biosynthetic pathway involves multiple genes (asuA-D) that contribute to the formation of key building blocks, leading to the creation of the intermediate protoasukamycin and its conversion to the final product through specific enzymes.
  • Branched acyl CoA units from amino acids Val, Leu, and Ile are utilized in the production of asukamycin variants, while a type II thioesterase helps regulate cellular fatty acid levels and membrane stability.

Article Abstract

Asukamycin, a member of the manumycin family metabolites, is an antimicrobial and potential antitumor agent isolated from Streptomyces nodosus subsp. asukaensis. The entire asukamycin biosynthetic gene cluster was cloned, assembled, and expressed heterologously in Streptomyces lividans. Bioinformatic analysis and mutagenesis studies elucidated the biosynthetic pathway at the genetic and biochemical level. Four gene sets, asuA-D, govern the formation and assembly of the asukamycin building blocks: a 3-amino-4-hydroxybenzoic acid core component, a cyclohexane ring, two triene polyketide chains, and a 2-amino-3-hydroxycyclopent-2-enone moiety to form the intermediate protoasukamycin. AsuE1 and AsuE2 catalyze the conversion of protoasukamycin to 4-hydroxyprotoasukamycin, which is epoxidized at C5-C6 by AsuE3 to the final product, asukamycin. Branched acyl CoA starter units, derived from Val, Leu, and Ile, can be incorporated by the actions of the polyketide synthase III (KSIII) AsuC3/C4 as well as the cellular fatty acid synthase FabH to produce the asukamycin congeners A2-A7. In addition, the type II thioesterase AsuC15 limits the cellular level of omega-cyclohexyl fatty acids and likely maintains homeostasis of the cellular membrane.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2915727PMC
http://dx.doi.org/10.1074/jbc.M110.128850DOI Listing

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