Journal article

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

TV Nheu, H He, Y Hirokawa, K Tamaki, L Florin, ML Schmitz, I Suzuki-Takahashi, RN Jorissen, AW Burgess, S Nishimura, J Wood, H Maruta

Cancer Journal | Published : 2002

DOI: 10.1097/00130404-200207000-00009

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 inhib..

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University of Melbourne Researchers

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Keywords

Science & Technology
Cdk2
Protein-Kinase
Biotechnology
Ras
Atp Antagonists
Life Sciences & Biomedicine
K252a Dimer
Signal Therapy
Complex
Pp1
Paks
Transformation
Activation
Cancer
In-Vitro
Staurosporine Derivatives
32 Biomedical and Clinical Sciences
2.1 Biological and Endogenous Factors
3211 Oncology and Carcinogenesis
5.1 Pharmaceuticals
Cep-1347
Oncology
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