Pim-selective inhibitor DHPCC-9 reveals Pim kinases as potent stimulators of cancer cell migration and invasion

Santio, Niina M.; Vahakoski, Riitta L.; Rainio, Eeva-Marja; Sandholm, Jouko; Virtanen, Sanna S.; Prudhomme, Michelle; Anizon, Fabrice; Moreau, Pascale; Koskinen, Päivi J.

doi:10.1186/1476-4598-9-279

Cited by 64 publications

(89 citation statements)

References 36 publications

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“…Loss of nuclear expression and gain of cytoplasmic expression appear to be the likely mechanisms of oncogenesis in gastric cancers, although further work will be needed to verify this hypothesis. Our finding that cytoplasmic PIM1 expression correlates inversely with the presence of lymphovascular invasion is potentially interesting in view of a recent report that implicates PIM1 in invasion and metastasis [33]. The identification of high-level PIM1 genomic amplification by aCGH suggests that overexpression and subsequent gain of PIM1 function might occur in a subset of gastric cancers.…”

Section: Discussionsupporting

confidence: 58%

Clinical and therapeutic relevance of PIM1 kinase in gastric cancer

et al. 2011

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Background Gastric cancer is a leading cause of cancerrelated mortality, and chemotherapeutic options are currently limited. PIM1 kinase, an oncogene that promotes tumorigenesis in several cancer types, might represent a novel therapeutic target in gastric cancer. Methods We studied the expression and genomic status of PIM1 in human primary gastric normal and tumor tissue samples by immunohistochemistry and array-based comparative genomic hybridization (aCGH). To ascertain whether PIM1 expression predicted susceptibility to PIM1 kinase-specific inhibition, the cytotoxic effect of a previously reported PIM1-specific small molecular inhibitor (K00135) was investigated in two gastric cancer cell lines with high (IM95) and undetectable (NUGC-4) PIM1 expression levels. Results PIM1 expression was exclusively nuclear in normal gastric epithelial cells, while aberrant expression/ localization (decreased nuclear and/or increased cytoplasmic expression) was observed in 75.6% (68/90) of the human gastric cancer tissue samples, with a significant inverse correlation between nuclear and cytoplasmic expression levels. Clinicopathological analyses revealed that decreased nuclear PIM1 expression correlated with poorer survival and greater depth of tumor invasion, while increased cytoplasmic PIM1 expression correlated inversely with the presence of lymphovascular invasion. Highlevel PIM1 amplification was identified in 10.5% of gastric cancers by aCGH. K00135 impaired the survival of IM95, while it had no significant effect on NUGC-4 survival. Conclusion Our findings demonstrate the clinical and therapeutic relevance of PIM1 in gastric cancers, and suggest that PIM1 represents a potential therapeutic target.

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Section: Discussionsupporting

confidence: 58%

Clinical and therapeutic relevance of PIM1 kinase in gastric cancer

et al. 2011

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“…Interestingly, while PIM1 did not alter BAD phosphorylation levels, both PIM2 and PIM3 reduced BAD phosphorylation and total BAD levels after PIM2 knockdown (Fig. 9D), which might explain the proapoptotic effects seen after knockdown of PIM2 and PIM3 (32,(46)(47)(48). Taken together, the proapoptotic effects of PIM inhibitors and their effect on CXCR4 downregulation from the cell surface are mediated by different PIM kinases, with PIM1 regulating the CXCR4 surface expression and PIM2/PIM3 supporting survival of CLL cells.…”

Section: Four Irradiated Rag2mentioning

confidence: 73%

PIM Kinases Are Essential for Chronic Lymphocytic Leukemia Cell Survival (PIM2/3) and CXCR4-Mediated Microenvironmental Interactions (PIM1)

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Finter

Forde

et al. 2014

Molecular Cancer Therapeutics

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Overexpression of the CXCR4 receptor is a hallmark of chronic lymphocytic leukemia (CLL) and is important for CLL cell survival, migration, and interaction with their protective microenvironment. In acute myelogenous leukemia (AML), PIM1 was shown to regulate the surface expression of the CXCR4 receptor. Here, we show that PIM (proviral integration site for Moloney murine leukemia virus) kinases 1-3 are overexpressed and that the CXCR4 receptor is hyperphosphorylated on Ser339 in CLL compared with normal lymphocytes. Furthermore, CXCR4 phosphorylation correlates with PIM1 protein expression and PIM1 transcript levels in CLL. PIM kinase inhibition with three different PIM kinase inhibitors induced apoptosis in CLL cells independent of the presence of protective stromal cells. In addition, PIM inhibition caused dephosphorylation of the CXCR4 receptor on Ser339, resulting in enhanced ligand-dependent CXCR4 internalization and reduced re-externalization after withdrawal of CXCL12. Furthermore, PIM inhibition in CLL cells blocked CXCR4 functions, such as migration toward CXCL12-or CXCL12-induced extracellular signal-regulated kinase (ERK) phosphorylation. In concordance, pretreatment of CLL cells with PIM kinase inhibitors strongly reduced homing of CLL cells toward the bone marrow and the spleen of Rag2

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“…Among other activities, PIM1 and PIM3 act by repressing apoptosis 30,39,40 and by stimulating the invasion activity of cancer cells. 41 These characteristics are reflected in the gene silencing experiments shown here, where downregulation of PIM1 and PIM3 expression determines cell death and a decrease of invasiveness. In particular, as far as GBM cells are concerned, PIM3 seems to be more relevant than PIM1.…”

Section: Discussionmentioning

confidence: 98%