A strategy to eradicate well-developed Krebs-2 ascites in mice

نویسندگان

  • Ekaterina A. Potter
  • Evgenia V. Dolgova
  • Anastasia S. Proskurina
  • Alexandra M. Minkevich
  • Yaroslav R. Efremov
  • Oleg S. Taranov
  • Vladimir V. Omigov
  • Valeriy P. Nikolin
  • Nelly A. Popova
  • Sergey I. Bayborodin
  • Alexander A. Ostanin
  • Elena R. Chernykh
  • Nikolay A. Kolchanov
  • Mikhail A. Shurdov
  • Sergey S. Bogachev
چکیده

We describe the strategy, which allows curing experimental mice engrafted with Krebs-2 ascites. The strategy is based on the facts that i) Krebs-2 tumor-initiating stem cells (TISCs) are naturally capable of internalizing fragments of extracellular double-stranded DNA (dsDNA); ii) upon delivery into TISCs, these dsDNA fragments interfere with the on-going DNA repair process so that TISCs either die or lose their tumorigenic potential. The following 3-step regimen of therapeutic procedures leading to eradication of Krebs-2 ascites is considered. Firstly, three timed injections of cyclophosphamide (CP) exactly matching the interstrand cross-link (ICL) repair phases that lead to synchronization of ascites cells in late S/G2/M. Secondly, additional treatment of ascites 18 hours post each CP injection (at NER/HR transition timepoint) with a composite dsDNA-based preparation interfering with the NER and HR repair pathways, so that tumorigenic properties of ascites cells are compromised. Thirdly, final treatment of mice with a combination of CP and dsDNA injections as ascites cells undergo apoptotic destruction, and the surviving TAMRA+ TISCs arrested in late S/G2/M phases massively enter into G1/S, when they regain sensitivity to CP+dsDNA treatment. Thus, this regimen assures that no viable cells, particularly Krebs-2 TISCs, remain.

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عنوان ژورنال:

دوره 7  شماره 

صفحات  -

تاریخ انتشار 2016