Hoffmann, R. A wiki for the life sciences where authorship matters. Nature Genetics (2008)

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Gene: FOXO1 - forkhead box O1

Homo sapiens

Synonyms: FKH1, FKHR, forkhead box O1A (rhabdomyosarcoma), Forkhead box protein O1A, Forkhead in rhabdomyosarcoma, FOXO1A

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Kim, J.J., Dong, X.Y., Kim, J.J., Schuur, E.R., Begum, S., et al.

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Disease relevance of FOXO1

In addition, FOXO1A was transcriptionally down-regulated in some prostate cancers [1].
Human endometrial fibroblasts (HuF) expressed FOXO1A, progesterone receptor A (PGRA), and progesterone receptor B (PGRB) proteins, whereas the endometrial adenocarcinoma cell line, HEC-1B cells, expressed only FOXO1A and no detectable PGR proteins [2].
Furthermore, expression of the FOXO1 protein is lost in a mouse lymphoma model, where Skp2 is overexpressed [3].
We determined whether expression of Pax3-FKHR in the mouse germ line would render these animals prone to the development of rhabdomyosarcomas [4].
Since Pax3 induced a mesenchymal to epithelial transition (MET) in human SaOS-2 osteosarcomas, we hypothesized that Pax3/FKHR would also induce a morphological change in SaOS-2 cells [5].

Psychiatry related information on FOXO1

Analysis of hippocampi from patients with intractable epilepsy revealed that Bim levels were significantly lower than in controls and FKHR was inhibited; we were able to reproduce these results experimentally in rats by evoking multiple brief, noninjurious electroshock seizures [6].

High impact information on FOXO1

In C. elegans, removing the germ cells extends life span by triggering the nuclear localization and activation of the DAF-16/FOXO transcription factor in the intestine [7].
Thus, forkhead factor(s) play a critical role in the development of muscle atrophy, and inhibition of Foxo factors is an attractive approach to combat muscle wasting [8].
Here, we show that in cultured myotubes undergoing atrophy, the activity of the PI3K/AKT pathway decreases, leading to activation of Foxo transcription factors and atrogin-1 induction [8].
These findings indicate that the t(2;13) generates a potentially tumorigenic fusion transcription factor consisting of intact PAX3 DNA binding domains, a truncated fork head DNA binding domain and C-terminal FKHR regions [9].
Polymerase chain reaction analysis demonstrates that a 5'PAX3-3' FKHR chimaeric transcript is expressed in all eight alveolar rhabdomyosarcomas investigated [9].

Chemical compound and disease context of FOXO1

The effect of H(2)O(2) on downstream Akt targets was examined by Western blot using antibody against phosphorylated forkhead in rhabdomyosarcoma (FKHR) and phosphorylated glycogen synthase kinase (GSK)-3beta [10].
Estrogen regulation of Pak1 and FKHR pathways in breast cancer cells [11].
Intracerebroventricular injection of orthovanadate 30 minutes before ischemia inhibited dephosphorylation of FKHR after reperfusion, and blocked delayed neuronal death in the CA1 region [12].
To the extent that this model reflects human disease, these data suggest that FOXO function may be compromised with androgen-independent progression of human prostate cancer [13].

Biological context of FOXO1

Functionally, ectopic expression of FOXO1A inhibited, and its knockdown promoted, cell proliferation or survival [1].
Consistent with the understanding of FOXO1A biology, our findings suggest that FOXO1A is the 13q14 tumor suppressor gene, at least in prostate cancer [1].
Overexpressing FOXO1A also caused a change in cell shape, in that the stromal fibroblasts acquired a rounded, epithelioid appearance [14].
When FOXO1A expression was silenced using small interference RNA, IGFBP1 expression decreased in both HuF and HEC-1B cells [2].
The human forkhead box O1A (FOXO1A) gene on chromosome 13q14.1 is a key transcription factor in insulin signaling in liver and adipose tissue and plays a central role in the regulation of key pancreatic beta-cell genes including IPF1 [15].

Anatomical context of FOXO1

Deletion at FOXO1A was detected in 31% to 34% in 6 cell lines, 27 xenografts, and 72 clinical specimens of prostate cancer, and was significantly more frequent than deletions at surrounding loci [1].
FKHR, a FOXO forkhead transcription factor, stimulates IGFBP-1 promoter activity in liver cells through the insulin response sequences (IRSs) [16].
Here we show that FKHR and HOXA10 are expressed in baboon endometrium during the menstrual cycle and pregnancy [16].
Among metastatic ARMS, bone marrow involvement was significantly higher in PAX3-FKHR-positive patients [17].
Similarly, SH2-Bbeta stimulated the accumulation of FKHR in the cytoplasm of 293T and COS-7 cells, whereas SH2-Bbeta(R555E) enhanced its accumulation in the nucleus [18].

Associations of FOXO1 with chemical compounds

Furthermore, FOXO1A inhibited androgen- and androgen receptor-mediated gene regulation and cell proliferation [1].
Reporter studies demonstrated that whereas liganded PGRA or PGRB increased a progesterone response element-linked reporter construct, pPRE/ GRE.E1b.Luc, coexpression of FOXO1A inhibited the PGRB response in HuF and synergistically increased PGRA and PGRB response in HEC-1B cells [2].
The ER alpha-FKHR interaction depends on beta-estradiol and is reduced significantly in the absence of hormone or the presence of Tamoxifen [19].
The FKHR interaction was specific to ER alpha and was not detected with other ligand-activated steroid receptors [19].
Protein kinase B-alpha inhibits human pyruvate dehydrogenase kinase-4 gene induction by dexamethasone through inactivation of FOXO transcription factors [20].

Physical interactions of FOXO1

Induction of cyclin D2 in rat granulosa cells requires FSH-dependent relief from FOXO1 repression coupled with positive signals from Smad [21].
The t(2;13) chromosomal translocation in alveolar rhabdomyosarcoma tumors (ARMS) creates an oncogenic transcriptional activator by fusion of PAX3 DNA binding motifs to a COOH-terminal activation domain derived from the FKHR gene [22].
We find that FKHR can bind in vitro to the insulin-responsive sequence (IRS) in the insulin-like growth factor-binding protein 1 promoter and can activate transcription from a reporter plasmid containing multiple copies of the IRS [23].
FKHR interacted with the DNA binding domain of HNF-4 and inhibited HNF-4 binding to the cognate DNA [24].

Enzymatic interactions of FOXO1

These experiments suggest that DYRK1A may phosphorylate FKHR at Ser(329) in vivo [25].
FKHR is phosphorylated by protein kinase B (PKB) at Thr24, Ser256 and Ser319 in response to growth factors, stimulating the nuclear exit and inactivation of this transcription factor [26].
CDK2 specifically phosphorylated FOXO1 at serine-249 (Ser(249)) in vitro and in vivo [27].
Expression of a constitutively active form of FKHR that cannot be phosphorylated by Akt produces the same effect as reconstitution of PTEN on PTEN-deficient tumor cells [28].
Furthermore, the binding affinity of HNF-4 with phosphorylated FKHR significantly decreased in comparison to that with unphosphorylated FKHR [24].

Regulatory relationships of FOXO1

Conversely, ER alpha repressed FKHR-mediated transactivation through an insulin response sequence, and cell cycle arrest induced by FKHRL1 in MCF7 cells was abrogated by estradiol [19].
We demonstrate here that Pax3/FKHR more potently induces a MET in SaOS-2 cells than Pax3 [5].
Reporter gene studies reveal that FKHR stimulates both baboon and human IGFBP-1 promoter activity, whereas HOXA10 alone has a relatively weak effect [16].
These results indicate that TNF induces activation of the FOXO1 transcription factor, which acts as a master switch to control apoptosis [29].
Our results indicated that the interaction of FKHR with 14-3-3 proteins was not required for IGF-1-stimulated exclusion of FKHR from the nucleus [30].

Other interactions of FOXO1

Although PAX3-FKHR exhibits transforming activity in immortalized fibroblast cell lines, a direct role of this fusion protein in tumorigenesis in vivo has not been shown [4].
Insulin suppresses the hPDK4 induction by glucocorticoids through inactivation of the FOXO factors [20].
TIMP3 and CNR1 levels decreased even further in response to H+dbcAMP compared with FOXO1A alone [14].
Furthermore, in HEC-1B cells, FOXO1A increased IGFBP1 promoter activity, and coexpression of PGRA or PGRB further increased the promoter activity in a cooperative manner [2].
When FKHR and HOXA10 are expressed together, promoter activity is markedly up-regulated, which is indicative of cooperativity [16].

Analytical, diagnostic and therapeutic context of FOXO1

In addition, immunoprecipitation of HuF nuclear proteins with a PGR antibody followed by immunoblotting with anti-FOXO1A revealed that these two proteins interact in these cells [2].
By microarray analysis, we determined that Pax3/FKHR altered the expression of gene targets in a manner quantitatively and qualitatively distinct from Pax3 [5].
Using pulsed-field and fluorescence in situ hybridization analyses, we demonstrate that the 130kb FKHR intron 1 is rearranged in t(2;13)-containing alveolar rhabdomyosarcomas [31].
Fork-head box class-O 1 (FOXO1) was strongly activated, which was confirmed in vitro and in vivo by electrophoretic mobility shift assay [29].
Both alveolar and embryonal components of the mixed ARMS/ERMS subtype were negative for PAX3, PAX7, and FKHR rearrangements, a surprising finding confirmed by RT-PCR and/or conventional karyotyping [32].

References

FOXO1A is a candidate for the 13q14 tumor suppressor gene inhibiting androgen receptor signaling in prostate cancer. Dong, X.Y., Chen, C., Sun, X., Guo, P., Vessella, R.L., Wang, R.X., Chung, L.W., Zhou, W., Dong, J.T. Cancer Res. (2006)
Role of FOXO1A in the regulation of insulin-like growth factor-binding protein-1 in human endometrial cells: interaction with progesterone receptor. Kim, J.J., Buzzio, O.L., Li, S., Lu, Z. Biol. Reprod. (2005)
Skp2 inhibits FOXO1 in tumor suppression through ubiquitin-mediated degradation. Huang, H., Regan, K.M., Wang, F., Wang, D., Smith, D.I., van Deursen, J.M., Tindall, D.J. Proc. Natl. Acad. Sci. U.S.A. (2005)
Pax3-FKHR knock-in mice show developmental aberrations but do not develop tumors. Lagutina, I., Conway, S.J., Sublett, J., Grosveld, G.C. Mol. Cell. Biol. (2002)
Cell-type-specific regulation of distinct sets of gene targets by Pax3 and Pax3/FKHR. Begum, S., Emani, N., Cheung, A., Wilkins, O., Der, S., Hamel, P.A. Oncogene (2005)
Bim regulation may determine hippocampal vulnerability after injurious seizures and in temporal lobe epilepsy. Shinoda, S., Schindler, C.K., Meller, R., So, N.K., Araki, T., Yamamoto, A., Lan, J.Q., Taki, W., Simon, R.P., Henshall, D.C. J. Clin. Invest. (2004)
Germ-cell loss extends C. elegans life span through regulation of DAF-16 by kri-1 and lipophilic-hormone signaling. Berman, J.R., Kenyon, C. Cell (2006)
Foxo transcription factors induce the atrophy-related ubiquitin ligase atrogin-1 and cause skeletal muscle atrophy. Sandri, M., Sandri, C., Gilbert, A., Skurk, C., Calabria, E., Picard, A., Walsh, K., Schiaffino, S., Lecker, S.H., Goldberg, A.L. Cell (2004)
Fusion of a fork head domain gene to PAX3 in the solid tumour alveolar rhabdomyosarcoma. Galili, N., Davis, R.J., Fredericks, W.J., Mukhopadhyay, S., Rauscher, F.J., Emanuel, B.S., Rovera, G., Barr, F.G. Nat. Genet. (1993)
Oxidant-mediated Akt Activation in Human RPE Cells. Yang, P., Peairs, J.J., Tano, R., Jaffe, G.J. Invest. Ophthalmol. Vis. Sci. (2006)
Estrogen regulation of Pak1 and FKHR pathways in breast cancer cells. Mazumdar, A., Kumar, R. FEBS Lett. (2003)
Decreased akt activity is associated with activation of forkhead transcription factor after transient forebrain ischemia in gerbil hippocampus. Kawano, T., Morioka, M., Yano, S., Hamada, J., Ushio, Y., Miyamoto, E., Fukunaga, K. J. Cereb. Blood Flow Metab. (2002)
The progression of LNCaP human prostate cancer cells to androgen independence involves decreased FOXO3a expression and reduced p27KIP1 promoter transactivation. Lynch, R.L., Konicek, B.W., McNulty, A.M., Hanna, K.R., Lewis, J.E., Neubauer, B.L., Graff, J.R. Mol. Cancer Res. (2005)
FOXO1A differentially regulates genes of decidualization. Buzzio, O.L., Lu, Z., Miller, C.D., Unterman, T.G., Kim, J.J. Endocrinology (2006)
Analysis of FOXO1A as a candidate gene for type 2 diabetes. Karim, M.A., Craig, R.L., Wang, X., Hale, T.C., Elbein, S.C. Mol. Genet. Metab. (2006)
Regulation of insulin-like growth factor binding protein-1 promoter activity by FKHR and HOXA10 in primate endometrial cells. Kim, J.J., Taylor, H.S., Akbas, G.E., Foucher, I., Trembleau, A., Jaffe, R.C., Fazleabas, A.T., Unterman, T.G. Biol. Reprod. (2003)
PAX3-FKHR and PAX7-FKHR gene fusions are prognostic indicators in alveolar rhabdomyosarcoma: a report from the children's oncology group. Sorensen, P.H., Lynch, J.C., Qualman, S.J., Tirabosco, R., Lim, J.F., Maurer, H.M., Bridge, J.A., Crist, W.M., Triche, T.J., Barr, F.G. J. Clin. Oncol. (2002)
SH2-B is a positive regulator of nerve growth factor-mediated activation of the Akt/Forkhead pathway in PC12 cells. Wang, X., Chen, L., Maures, T.J., Herrington, J., Carter-Su, C. J. Biol. Chem. (2004)
Ligand-dependent interaction of estrogen receptor-alpha with members of the forkhead transcription factor family. Schuur, E.R., Loktev, A.V., Sharma, M., Sun, Z., Roth, R.A., Weigel, R.J. J. Biol. Chem. (2001)
Protein kinase B-alpha inhibits human pyruvate dehydrogenase kinase-4 gene induction by dexamethasone through inactivation of FOXO transcription factors. Kwon, H.S., Huang, B., Unterman, T.G., Harris, R.A. Diabetes (2004)
Induction of cyclin D2 in rat granulosa cells requires FSH-dependent relief from FOXO1 repression coupled with positive signals from Smad. Park, Y., Maizels, E.T., Feiger, Z.J., Alam, H., Peters, C.A., Woodruff, T.K., Unterman, T.G., Lee, E.J., Jameson, J.L., Hunzicker-Dunn, M. J. Biol. Chem. (2005)
An engineered PAX3-KRAB transcriptional repressor inhibits the malignant phenotype of alveolar rhabdomyosarcoma cells harboring the endogenous PAX3-FKHR oncogene. Fredericks, W.J., Ayyanathan, K., Herlyn, M., Friedman, J.R., Rauscher, F.J. Mol. Cell. Biol. (2000)
Negative regulation of the forkhead transcription factor FKHR by Akt. Tang, E.D., Nuñez, G., Barr, F.G., Guan, K.L. J. Biol. Chem. (1999)
Hepatocyte nuclear factor-4 is a novel downstream target of insulin via FKHR as a signal-regulated transcriptional inhibitor. Hirota, K., Daitoku, H., Matsuzaki, H., Araya, N., Yamagata, K., Asada, S., Sugaya, T., Fukamizu, A. J. Biol. Chem. (2003)
The kinase DYRK1A phosphorylates the transcription factor FKHR at Ser329 in vitro, a novel in vivo phosphorylation site. Woods, Y.L., Rena, G., Morrice, N., Barthel, A., Becker, W., Guo, S., Unterman, T.G., Cohen, P. Biochem. J. (2001)
Two novel phosphorylation sites on FKHR that are critical for its nuclear exclusion. Rena, G., Woods, Y.L., Prescott, A.R., Peggie, M., Unterman, T.G., Williams, M.R., Cohen, P. EMBO J. (2002)
CDK2-Dependent Phosphorylation of FOXO1 as an Apoptotic Response to DNA Damage. Huang, H., Regan, K.M., Lou, Z., Chen, J., Tindall, D.J. Science (2006)
Forkhead transcription factors are critical effectors of cell death and cell cycle arrest downstream of PTEN. Nakamura, N., Ramaswamy, S., Vazquez, F., Signoretti, S., Loda, M., Sellers, W.R. Mol. Cell. Biol. (2000)
FOXO1 functions as a master switch that regulates gene expression necessary for tumor necrosis factor-induced fibroblast apoptosis. Alikhani, M., Alikhani, Z., Graves, D.T. J. Biol. Chem. (2005)
Roles of the forkhead in rhabdomyosarcoma (FKHR) phosphorylation sites in regulating 14-3-3 binding, transactivation and nuclear targetting. Rena, G., Prescott, A.R., Guo, S., Cohen, P., Unterman, T.G. Biochem. J. (2001)
Structural characterization of the FKHR gene and its rearrangement in alveolar rhabdomyosarcoma. Davis, R.J., Bennicelli, J.L., Macina, R.A., Nycum, L.M., Biegel, J.A., Barr, F.G. Hum. Mol. Genet. (1995)
Use of a novel FISH assay on paraffin-embedded tissues as an adjunct to diagnosis of alveolar rhabdomyosarcoma. Nishio, J., Althof, P.A., Bailey, J.M., Zhou, M., Neff, J.R., Barr, F.G., Parham, D.M., Teot, L., Qualman, S.J., Bridge, J.A. Lab. Invest. (2006)