Synthesis of full length and truncated microcin B17 analogues as DNA gyrase poisons.

نویسندگان

  • Robert E Thompson
  • Frédéric Collin
  • Anthony Maxwell
  • Katrina A Jolliffe
  • Richard J Payne
چکیده

Microcin B17 (MccB17) is a post-translationally modified peptide containing thiazole and oxazole heterocycles that interrupt the peptide backbone. MccB17 is capable of poisoning DNA gyrase through stabilization of the gyrase-DNA cleavage complex and has therefore attracted significant attention. Using a combination of Fmoc-strategy solid-phase peptide synthesis and solution-phase fragment assembly we have prepared a library of full-length and truncated MccB17 analogues to investigate key structural requirements for gyrase-poisoning activity. Synthetic peptides lacking the glycine-rich N-terminal portion of the full-length sequence showed strong stabilization of the gyrase-DNA cleavage complex with increased potency relative to the full-length sequences. This truncation, however, led to a decrease in antibacterial activity of these analogues relative to their full-length counterparts indicating a potential role of the N-terminal region of the natural product for cellular uptake.

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عنوان ژورنال:
  • Organic & biomolecular chemistry

دوره 12 10  شماره 

صفحات  -

تاریخ انتشار 2014