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Abstract
Oncogenic RAS mutants such as v-Ha-RAS induce cell cycling, in particular the G1 to S transition, by up-regulating cyclin D1 and down-regulating p27, an inhibitor for cyclin-dependent kinases (CDKs). PI-3 kinase appears to be involved in the regulation of both cyclin D1 and p27. In this report, using two distinct inhibitors specific for PAK1-3 (CEP-1347 and WR-PAK18), we present the first evidence indicating that the PIX/Rac/CDC42-dependent Ser/Thr kinases PAK1-3, acting downstream of PI-3 kinase and up-stream of the Raf/MEK/ERKs kinase cascade, is essential for RAS-induced up-regulation of cyclin D1, but not down-regulation of p27. Since these PAK-inhibitors block selectively the malignant growth of RAS transformants, in which PAK1 is constitutively activated, but not normal cell growth, it is suggested that RAS transformants are addicted to the high levels of PAK1 for their malignant entry to S phase.