Triostin A Derived Cyclopeptide as Architectural Template for the Alignment of Four Recognition Units**

نویسندگان

  • Ursula M Kotyrba
  • Kevin Pröpper
  • Eike-F Sachs
  • Anastasiya Myanovska
  • Tobias Joppe
  • Friederike Lissy
  • George M Sheldrick
  • Konrad Koszinowski
  • Ulf Diederichsen
چکیده

The DNA bisintercalator triostin A is structurally based on a disulfide-bridged depsipeptide scaffold that provides preorganization of two quinoxaline units in 10.5 Å distance. Triostin A analogues are synthesized with nucleobase recognition units replacing the quinoxalines and containing two additional recognition units in between. Thus, four nucleobase recognition units are organized on a rigid template, well suited for DNA double strand interactions. The new tetra-nucleobase binders are synthesized as aza-TANDEM derivatives lacking the N-methylation of triostin A and based on a cyclopeptide backbone. Synthesis of two tetra-nucleobase aza-TANDEM derivatives is established, DNA interaction analyzed by microscale thermophoresis, cytotoxic activity studied and a nucleobase sequence dependent self-aggregation investigated by mass spectrometry.

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عنوان ژورنال:

دوره 3  شماره 

صفحات  -

تاریخ انتشار 2014