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PAK4 interacts with p85 alpha: implications for pancreatic cancer cell migration.


ABSTRACT: It has been reported that p21-activated kinase 4 (PAK4) is amplified in pancreatic cancer tissue. PAK4 is a member of the PAK family of serine/threonine kinases, which act as effectors for several small GTPases, and has been specifically identified to function downstream of HGF-mediated c-Met activation in a PI3K dependent manner. However, the functionality of PAK4 in pancreatic cancer and the contribution made by HGF signalling to pancreatic cancer cell motility remain to be elucidated. We now find that elevated PAK4 expression is coincident with increased expression levels of c-Met and the p85? subunit of PI3K. Furthermore, we demonstrate that pancreatic cancer cells have a specific motility response to HGF both in 2D and 3D physiomimetic organotypic assays; which can be suppressed by inhibition of PI3K. Significantly, we report a specific interaction between PAK4 and p85? and find that PAK4 deficient cells exhibit a reduction in Akt phosphorylation downstream of HGF signalling. These results implicate a novel role for PAK4 within the PI3K pathway via interaction with p85?. Thus, PAK4 could be an essential player in PDAC progression representing an interesting therapeutic opportunity.

SUBMITTER: King H 

PROVIDER: S-EPMC5312077 | biostudies-literature | 2017 Feb

REPOSITORIES: biostudies-literature

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PAK4 interacts with p85 alpha: implications for pancreatic cancer cell migration.

King Helen H   Thillai Kiruthikah K   Whale Andrew A   Arumugam Prabhu P   Eldaly Hesham H   Kocher Hemant M HM   Wells Claire M CM  

Scientific reports 20170216


It has been reported that p21-activated kinase 4 (PAK4) is amplified in pancreatic cancer tissue. PAK4 is a member of the PAK family of serine/threonine kinases, which act as effectors for several small GTPases, and has been specifically identified to function downstream of HGF-mediated c-Met activation in a PI3K dependent manner. However, the functionality of PAK4 in pancreatic cancer and the contribution made by HGF signalling to pancreatic cancer cell motility remain to be elucidated. We now  ...[more]

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