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dc.contributor.authorRaimondi, C.
dc.contributor.authorFalasca, Marco
dc.date.accessioned2017-01-30T12:49:49Z
dc.date.available2017-01-30T12:49:49Z
dc.date.created2015-10-29T04:09:53Z
dc.date.issued2011
dc.identifier.citationRaimondi, C. and Falasca, M. 2011. Targeting PDK1 in cancer. Current Medicinal Chemistry. 18 (18): pp. 2763-2769.
dc.identifier.urihttp://hdl.handle.net/20.500.11937/25718
dc.identifier.doi10.2174/092986711796011238
dc.description.abstract

Abnormal activation of phosphoinositide 3-kinase (PI3K) signalling is very common in cancer, leading to deregulation of several intracellular processes normally controlled by this enzyme, including cell survival, growth, proliferation and migration. Mutations in the gene encoding the tumour suppressor phosphatase and tensin homologue deleted on chromosome 10 (PTEN), which leads to uncontrolled activation of the PI3K pathway, are reported in different cancers. Among the downstream effectors of PI3Ks, 3-phosphoinositide- dependent protein kinase 1 (PDK1) and protein kinase B (PKB)/Akt have a key role in several cancer types. More recent data indicate that alteration of PDK1 is a critical component of oncogenic PI3K signalling in breast cancer, suggesting that inhibition of PDK1 can inhibit breast cancer progression. PDK1 has an essential role in regulating cell migration especially in the context of PTEN deficiency. Downregulation of PDK1 levels inhibits migration and experimental metastasis of human breast cancer cells. PDK1 activates a large number of proteins, including Akt, some PKC isoforms, S6K and SGK. Data also reveal that PDK1 is oncogenic and this is dependent on PI3K pathway. Therefore, accumulating evidence demonstrates that PDK1 is a valid therapeutic target and suggests that PDK1 inhibitors may be useful to prevent cancer progression and abnormal tissue dissemination. This review will focus on published data on the role of PDK1 in cancer and approaches used to inhibit PDK1. © 2011 Bentham Science Publishers Ltd.

dc.titleTargeting PDK1 in cancer
dc.typeJournal Article
dcterms.source.volume18
dcterms.source.number18
dcterms.source.startPage2763
dcterms.source.endPage2769
dcterms.source.issn0929-8673
dcterms.source.titleCurrent Medicinal Chemistry
curtin.departmentSchool of Biomedical Sciences
curtin.accessStatusFulltext not available


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