Essential roles of FoxM1 in Ras-induced liver cancer progression and in cancer cells with stem cell features

Kopanja, Dragana; Pandey, Ankur; Kiefer, Megan M.; Wang, Zebin; Chandan, Neha; Carr, Janai R.; Franks, Roberta; Yu, Dae Yeul; Guzman, Grace; Maker, Ajay V.; Raychaudhuri, Pradip

doi:10.1016/j.jhep.2015.03.023

Cited by 77 publications

(84 citation statements)

References 32 publications

(52 reference statements)

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“…Its over-expression coincides with high-grade progression in almost all types of cancers, including those in breast12, liver34, lung56, prostate78, pancreas910, ovary11, brain12, nasopharynx13, esophagus14, and also in certain leukemia15. Moreover, a study that analyzed 18,000 human tumors with outcomes for 39 different malignancies identified over-expression of FoxM1 as a major predictor for poor prognosis16.…”

mentioning

confidence: 99%

Plk1 Regulates the Repressor Function of FoxM1b by inhibiting its Interaction with the Retinoblastoma Protein

Mukhopadhyay

Chand

Pandey

et al. 2017

Sci Rep

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FoxM1b is a cell cycle-regulated transcription factor, whose over-expression is a marker for poor outcome in cancers. Its transcriptional activation function requires phosphorylation by Cdk1 or Cdk2 that primes FoxM1b for phosphorylation by Plk1, which triggers association with the co-activator CBP. FoxM1b also possesses transcriptional repression function. It represses the mammary differentiation gene GATA3 involving DNMT3b and Rb. We investigated what determines the two distinct functions of FoxM1b: activation and repression. We show that Rb binds to the C-terminal activation domain of FoxM1b. Analyses with phospho-defective and phospho-mimetic mutants of FoxM1b identified a critical role of the Plk1 phosphorylation sites in regulating the binding of FoxM1b to Rb and DNMT3b. That is opposite of what was seen for the interaction of FoxM1b with CBP. We show that, in addition to GATA3, FoxM1b also represses the mammary luminal differentiation marker FoxA1 by promoter-methylation, and that is regulated by the Plk1 phosphorylation sites in FoxM1b. Our results show that the Plk1 phosphorylation sites in FoxM1b serve as a regulator for its repressor function, and they provide insights into how FoxM1b inhibits differentiation genes and activates proliferation genes during cancer progression.

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confidence: 99%

Plk1 Regulates the Repressor Function of FoxM1b by inhibiting its Interaction with the Retinoblastoma Protein

Mukhopadhyay

Chand

Pandey

et al. 2017

Sci Rep

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“…Secondly, FoxM1 is not expressed, or is expressed at very low levels in normal tissues [21]. Thirdly, FoxM1 plays an essential role in HCC cell migration, invasion, as well as liver cancer progression and in cancer cells with stem cell features [15, 22]. Fourthly, clinicopathologic studies suggest that FoxM1 expression correlated with poorly-differentiated HCC tumors with intrahepatic metastasis, which is a leading cause of post-surgical recurrence and low survival rate [20, 29].…”

Section: Discussionmentioning

confidence: 99%

“…Previous studies have shown that FoxM1 was essential for development of HCC, and overexpression of FoxM1 was associated with aggressive tumor features and poor prognosis [20]. In fact, FoxM1 could induce an epithelial-mesenchymal-like transition phenotype in HCC cells, increase cell migration, and induce premetastatic niche at the distal organ of metastasis [21, 22]. Down-regulation of FoxM1 could suppress the proliferation of HCC cells and inhibit HCC growth [23].…”

Section: Introductionmentioning

confidence: 99%

Immunotherapy based on dendritic cells pulsed with CTPFoxM1 fusion protein protects against the development of hepatocellular carcinoma

Zheng

et al. 2016

Oncotarget

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Application of dendritic cells (DCs) pulsed with tumor-associated antigens is considered attractive in immunotherapy for hepatocellular carcinoma (HCC). In order to efficiently prime tumor-associated antigens specific for cytotoxic T lymphocytes (CTLs), it is important that DCs present tumor-associated antigens on MHC class I. MHC class I generally present endogenous antigens expressed in the cytosol. In this study, we developed a new antigen delivery tool based on cross presentation of exogenous antigens in DCs by using cytoplasmic transduction peptide (CTP). CTP protein could transduce FoxM1 tumor antigen into the cytosol of DCs, and CTP-FoxM1 fusion protein could stimulate activation and maturation of DCs. DCs pulsed with CTP-FoxM1 could induce specific CTLs. More importantly, the immunity induced by DCs loaded with CTP-FoxM1 could significantly inhibit tumor growth and metastasis in HCC-bearing mice, which was more potent than that induced by DCs loaded with FoxM1 or CTP, alone. Our results indicate that DCs pulsed with CTP-FoxM1 might be a promising vaccine candidate for HCC therapy and provide new insight into the design of DC-based immunotherapy.

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“…Further encouraged by new evidence indicating that FOXM1 (1) drives tumor development and progression 15–19 by virtue of a complex mechanism that includes enhanced cell proliferation, migration and invasion 6 , regulation of the DNA damage response 20 and changes in the cancer epigenome 21 , (2) promotes cancer-cell resistance to ionizing radiation 22 and cytotoxic drugs 23 , (3) governs, in part, the survival and tissue-regenerating capacity of both normal hematopoietic stem cells 24 and malignant stem cell-like cells 25 , (4) links acquired resistance to cancer therapy with cancer stemness 26 and (5) owing to the development of specific small-molecule inhibitors 27 , may soon be targeted more effectively than possible in the past 28 , we here decided to evaluate whether FOXM1 might play an important but heretofore overlooked role in plasma cell myeloma.…”

Section: Introductionmentioning

confidence: 99%

FOXM1 is a therapeutic target for high-risk multiple myeloma

Yang

Sompallae

et al. 2015

Leukemia

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The transcription factor forkhead box M1 (FOXM1) is a validated oncoprotein in solid cancers, but its role in malignant plasma cell tumors such as multiple myeloma (MM) is unknown. We analyzed publicly available MM datasets and found that overexpression of FOXM1 prognosticates inferior outcome in a subset (~15%) of newly diagnosed cases, particularly patients with high-risk disease based on global gene expression changes. Follow-up studies using human myeloma cell lines (HMCLs) as the principal experimental model system demonstrated that enforced expression of FOXM1 increased growth, survival and clonogenicity of myeloma cells, whereas knockdown of FOXM1 abolished these features. In agreement with that, constitutive up-regulation of FOXM1 promoted HMCL xenografts in laboratory mice, whereas inducible knockdown of FOXM1 led to growth inhibition. Expression of cyclin dependent kinase 6 (CDK6) and NIMA-related kinase 2 (NEK2) was co-regulated with FOXM1 in both HMCLs and myeloma patient samples, suggesting interaction of these 3 genes in a genetic network that may lend itself to targeting with small-drug inhibitors for new approaches to myeloma therapy and prevention. These results establish FOXM1 as high-risk myeloma gene and provide support for the design and testing of FOXM1-targeted therapies specifically for the FOXM1High subset of myeloma.

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Essential roles of FoxM1 in Ras-induced liver cancer progression and in cancer cells with stem cell features

Cited by 77 publications

References 32 publications

Plk1 Regulates the Repressor Function of FoxM1b by inhibiting its Interaction with the Retinoblastoma Protein

Plk1 Regulates the Repressor Function of FoxM1b by inhibiting its Interaction with the Retinoblastoma Protein

Immunotherapy based on dendritic cells pulsed with CTPFoxM1 fusion protein protects against the development of hepatocellular carcinoma

FOXM1 is a therapeutic target for high-risk multiple myeloma

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