1. Academic Validation
  2. The K252a derivatives, inhibitors for the PAK/MLK kinase family selectively block the growth of RAS transformants

The K252a derivatives, inhibitors for the PAK/MLK kinase family selectively block the growth of RAS transformants

  • Cancer J. 2002 Jul-Aug;8(4):328-36. doi: 10.1097/00130404-200207000-00009.
Thao V Nheu 1 Hong He Yumiko Hirokawa Kazuhiko Tamaki Lore Florin M Lienhard Schmitz Ikuko Suzuki-Takahashi Robert N Jorissen Antony W Burgess Susumu Nishimura John Wood Hiroshi Maruta
Affiliations

Affiliation

  • 1 Ludwig Institute for Cancer Research, Royal Melbourne Hospital, Parkville, Australia.
Abstract

Background: Oncogenic Ras mutants such as v-Ha-RAS activate members of Rac/CDC42-dependent kinases (PAKs) and appear to contribute to the development of more than 30% of all human cancers. PAK1 activation is essential for oncogenic Ras transformation, and several chemical compounds that inhibit Tyr kinases essential for the RAS-induced activation of PAK1 strongly suppress Ras transformation either in Cell Culture or in vivo (nude mice). Although we have developed a cell-permeable PAK-specific peptide inhibitor called WR-PA18, so far no chemical (metabolically stable) compound has been developed that directly inhibits PAK1 in a highly selective manner. Thus, we have explored such a PAK1 Inhibitor(s) among synthetic derivatives of an adenosine triphosphate antagonist.

Results: From the naturally occurring adenosine triphosphate antagonist K252a, we have developed two bulky derivatives, called CEP-1347 and KT D606 (a K252a dimer), which selectively inhibit PAKs or mixed-lineage kinases both in vitro and in Cell Culture and convert v-Ha-RAS-transformed NIH 3T3 cells to flat fibroblasts similar to the parental normal cells. Furthermore, these two K252a analogues suppress the proliferation of v-Ha-RAS transformants, but not the normal cells.

Conclusion: These bulky adenosine triphosphate antagonists derived from K252a or related indolocarbazole compounds such as staurosporine would be potentially useful for the treatment of Ras/ PAK1-induced cancers, once their anti-PAK1 activity is significantly potentiated by a few additional chemical modifications at the sugar ring suggested in this paper.

Figures
Products
  • Cat. No.
    Product Name
    Description
    Target
    Research Area
  • HY-164488
    PAK 抑制剂
    PAK