An Efficient Method for the In Vitro Production of Azol(in)e-Based Cyclic Peptides**

نویسندگان

  • Wael E Houssen
  • Andrew F Bent
  • Andrew R McEwan
  • Nathalie Pieiller
  • Jioji Tabudravu
  • Jesko Koehnke
  • Greg Mann
  • Rosemary I Adaba
  • Louise Thomas
  • Usama W Hawas
  • Huanting Liu
  • Ulrich Schwarz-Linek
  • Margaret C M Smith
  • James H Naismith
  • Marcel Jaspars
چکیده

Heterocycle-containing cyclic peptides are promising scaffolds for the pharmaceutical industry but their chemical synthesis is very challenging. A new universal method has been devised to prepare these compounds by using a set of engineered marine-derived enzymes and substrates obtained from a family of ribosomally produced and post-translationally modified peptides called the cyanobactins. The substrate precursor peptide is engineered to have a non-native protease cleavage site that can be rapidly cleaved. The other enzymes used are heterocyclases that convert Cys or Cys/Ser/Thr into their corresponding azolines. A macrocycle is formed using a macrocyclase enzyme, followed by oxidation of the azolines to azoles with a specific oxidase. The work is exemplified by the production of 17 macrocycles containing 6-9 residues representing 11 out of the 20 canonical amino acids.

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عنوان ژورنال:

دوره 53  شماره 

صفحات  -

تاریخ انتشار 2014