Multiple elements regulate nuclear/cytoplasmic shuttling of FOXO1: characterization of phosphorylation- and 14-3-3-dependent and -independent mechanisms

Zhao, Xiangshan; Gan, Lixia; Pan, Haiyun; Kan, Donghui; Majeski, Michael W.; Adam, Stephen A.; Unterman, Terry G.

doi:10.1042/bj20031450

Cited by 204 publications

(205 citation statements)

References 37 publications

(72 reference statements)

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“…shRNA CD44 inhibited Ser241 phosphorylation of PDK1. This inhibition of the PDK1/Akt molecule is an important signal for cell survival (27). GSK3β is the target of PDK1/Akt signal transduction.…”

Section: Discussionmentioning

confidence: 99%

“…The loss of GSK3 protein explains the stable accumulation of nonphosphorylated β-catenin that is accessible to the adherens junction at the cell periphery (47). The Wnt/β-catenin pathway was very recently reported to protect cells from p53-mediated FoxO1-induced apoptosis, a mechanism involving the activation of the Akt survival pathway (27,29). Silencing of CD44 expression in SW620 cells, indicating decreased β-catenin, increased wild-type p53 and FoxO1 expression.…”

Section: Discussionmentioning

confidence: 99%

“…Silencing of CD44 expression in SW620 cells, indicating decreased β-catenin, increased wild-type p53 and FoxO1 expression. Activation of FoxO1 induces apoptosis by up-regulating a number of cell death genes, including those encoding the ligand for the death receptor (Fas) and the Bcl-2-interacting mediator (Bim) of cell death, and the tumor necrosis factor-related apoptosis-inducing ligand (27,33). Sub-cellular localization of wild-type FoxO1 is controlled primarily by phosphorylation, leading to nuclear export and subsequent repression of transcriptional activity (25,26).…”

Section: Discussionmentioning

confidence: 99%

“…Nuclear localization of forkhead box transcription factor O (FoxO) proteins is required for transcriptional regulatory functions, which include the control of genes involved in apoptosis, such as Bim (18,19) and FasL (20), and genes involved in cell cycle regulation, such as p27 (21,22) and cyclin D1 and D2 (23,24). As major direct substrates of FoxO factors are negatively regulated by Akt phosphorylation in the presence of growth factor signaling (25,26), which results in binding to 14-3-3 proteins followed by nuclear export (27). Akt is recruited to the plasma membrane through the binding of its pleckstrin homology domain to the phosphatidylinositol 3,4,5-triphosphate (PIP3), which is a product of PI3K that is anchored to the plasma membrane.…”

Section: Introductionmentioning

confidence: 99%

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shRNA against CD44 inhibits cell proliferation, invasion and migration, and promotes apoptosis of colon carcinoma cells

Park

Huh²,

Lee³

et al. 2011

Oncol Rep

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Abstract. CD44 is a causal factor for tumor invasion, metastasis and acquisition of resistance to apoptosis. CD44 knockdown using inducible short hairpin RNA (shRNA) significantly reduces cell growth and invasion. Short hairpin RNA against CD44 and pGFP-V-RS-vector was used for knockdown of CD44 expression in SW620 colon cancer cells. Cell growth, invasion and migration assay, immunofluorescence for β-catenin expression and Western blotting for Wnt signaling molecules were analyzed. Cell cycle analysis and Western blot analysis for apoptotic molecules were evaluated. Short hairpin RNA against CD44 reduced the expression of CD44. Cell proliferation, migration and invasion were markedly inhibited and apoptosis was increased in shRNA CD44-transfected cells. Knockdown of CD44 decreased the phosphorylation of PDK1, Akt and GSK3β, and β-catenin levels. Decreased phosphorylated Akt led to an increase in phosphorylated FoxO1 and induced cell cycle arrest in the G 0 -G 1 phase and a decrease in the S phase. The levels of Bcl-2 and Bcl-xL expression were down-regulated, while the levels of BAX expression and cleaved caspase-3, -8 and -9 were increased. CD44 knockdown by way of shRNA inhibited cell proliferation and induced cell apoptosis. This can be used as a therapeutic intervention with the anti-survival/pro-apoptotic machinery in human colon cancer.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

shRNA against CD44 inhibits cell proliferation, invasion and migration, and promotes apoptosis of colon carcinoma cells

Park

Huh²,

Lee³

et al. 2011

Oncol Rep

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“…Nuclear/cytoplasmic shuttling of members of the forkhead protein family (ie FOXO1) has been reported to occur as a result of protein phosphorylation. 28 Phosphorylation of FKHRL1 via a phosphatidylinositol 3-kinase/Akt kinase results in cytoplasmic shuttling of the protein, 29 which suggests that similar mechanisms may be also involved in FOXP1 cytoplasmic localization. Given that hypoxia both enhances Act activity 30 and induces HIF-1a and -2a overexpression, the significant association between the cytoplasmic localization of FOXP1 and HIF-1a overexpression may be the result of a single cause, namely hypoxia.…”

Section: Discussionmentioning

confidence: 99%

Loss of expression and nuclear/cytoplasmic localization of the FOXP1 forkhead transcription factor are common events in early endometrial cancer: relationship with estrogen receptors and HIF-1α expression

et al. 2006

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The FOXP1 gene has been identified as a new member of the winged helix family of transcription factors that have important roles in cellular transformation, differentiation and proliferation. In this study, we examined the expression of FOXP1 in the normal and malignant endometrium (stage I endometrioid adenocarcinoma cases), showing a frequent deregulation of its expression in cancer. Proliferative endometrium showed predominantly nuclear localization of FOXP1, while exclusively weak cytoplasmic staining was present in the secretory phase. Loss of nuclear expression was the most striking event in endometrial adenocarcinoma. Nuclear expression ranged from 0 to 20% (median 0%). Cytoplasmic expression was noted more frequently, ranging from 0 to 90% of cancer cells (median 30%). Overall, 24/82 cases (29.3%) were observed to lack both nuclear and cytoplasmic FOXP1 expression. Tumors with exclusively cytoplasmic expression of FOXP1 were linked with deep myometrial invasion and hypoxia-inducible factors 1a (HIF-1a) expression. On the other hand, the presence of nuclear FOXP1 expression was significantly linked with ER-a reactivity. Survival analysis did not reveal significant differences among patients grouped by FOXP1 expression, presumably due to the high curability of stage I disease. This study provides evidence on pathways to be investigated to elucidate the interplay between FOXP1, ER-a and HIF-1a in hormone dependent cancers.

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FOXO transcription factors at the interface of metabolism and cancer

Link

Fernández-Marcos

2017

Intl Journal of Cancer

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Diabetes refers to a group of metabolic diseases characterized by impaired insulin signalling and high blood glucose. A growing body of epidemiological evidence links diabetes to several types of cancer but the underlying molecular mechanisms are poorly understood. The signalling cascade connecting insulin and FOXO proteins provides a compelling example for a conserved pathway at the interface between insulin signalling and cancer. FOXOs are transcription factors that orchestrate programs of gene expression known to control a variety of processes in response to cellular stress. Genes regulated by this family of proteins are involved in the regulation of cellular energy production, oxidative stress resistance and cell viability and proliferation. Accordingly, FOXO factors have been shown to play an important role in the suppression of tumour growth and in the regulation of metabolic homeostasis. There is emerging evidence that deregulation of FOXO factors might account for the association between insulin resistance-related metabolic disorders and cancer.

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Multiple elements regulate nuclear/cytoplasmic shuttling of FOXO1: characterization of phosphorylation- and 14-3-3-dependent and -independent mechanisms

Cited by 204 publications

References 37 publications

shRNA against CD44 inhibits cell proliferation, invasion and migration, and promotes apoptosis of colon carcinoma cells

shRNA against CD44 inhibits cell proliferation, invasion and migration, and promotes apoptosis of colon carcinoma cells

Loss of expression and nuclear/cytoplasmic localization of the FOXP1 forkhead transcription factor are common events in early endometrial cancer: relationship with estrogen receptors and HIF-1α expression

FOXO transcription factors at the interface of metabolism and cancer

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