<i>TGFBI</i> Deficiency Predisposes Mice to Spontaneous Tumor Development

Zhang, Ye; Wen, Gengyun; Shao, Genze; Wang, Cuidong; Lin, Chyuan‐Sheng; Fang, Hongbo; Balajee, Adayabalam S.; Bhagat, Govind; Hei, Tom K.; Zhao, Yongliang

doi:10.1158/0008-5472.can-08-1648

Cited by 109 publications

(98 citation statements)

References 47 publications

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“…Thus, the physiological expression of PITX1, TGF␤I, and ELL2 mRNA negatively correlated with mtert mRNA expression in the B16F10 clones. TGF␤I encodes a secreted protein, transforming growth factor ␤ (TGF␤), that is known to be a regulator of telomerase activity through the repression of the hTERT gene (57). ELL2 encodes a member of the ELL family of RNA polymerase II elongation factors.…”

Section: Resultsmentioning

confidence: 99%

Identification of PITX1 as a TERT Suppressor Gene Located on Human Chromosome 5

Ohhira

Fujisaki

et al. 2011

Molecular and Cellular Biology

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Telomerase, a ribonucleoprotein enzyme that maintains telomere length, is crucial for cellular immortalization and cancer progression. Telomerase activity is attributed primarily to the expression of telomerase reverse transcriptase (TERT). Using microcell-mediated chromosome transfer (MMCT) into the mouse melanoma cell line B16F10, we previously found that human chromosome 5 carries a gene, or genes, that can negatively regulate TERT expression (H. Kugoh, K. Shigenami, K. Funaki, J. Barrett, and M. Oshimura, Genes Chromosome Cancer 36:37-47, 2003). To identify the gene responsible for the regulation of TERT transcription, we performed cDNA microarray analysis using parental B16F10 cells, telomerase-negative B16F10 microcell hybrids with a human chromosome 5 (B16F10MH5), and its revertant clones (MH5R) with reactivated telomerase. Here, we report the identification of PITX1, whose expression leads to the downregulation of mouse tert (mtert) transcription, as a TERT suppressor gene. Additionally, both human TERT (hTERT) and mouse TERT (mtert) promoter activity can be suppressed by PITX1. We show that three and one binding site within the hTERT and mtert promoters, respectively, that express a unique conserved region are responsible for the transcriptional activation of TERT. Furthermore, we showed that PITX1 binds to the TERT promoter both in vitro and in vivo. Thus, PITX1 suppresses TERT transcription through direct binding to the TERT promoter, which ultimately regulates telomerase activity.

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Section: Resultsmentioning

confidence: 99%

Identification of PITX1 as a TERT Suppressor Gene Located on Human Chromosome 5

Ohhira

Fujisaki

et al. 2011

Molecular and Cellular Biology

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“…␤ig-h3 protein suppresses human breast tumor progression and malignant transformation of cells (27, 34 -38). Mutation or altered expression of ␤ig-h3 has been linked to the pathogenesis of human corneal dystrophy and osteogenesis (39). However, the underlying molecular mechanism of ␤ig-h3 effects is not well understood.…”

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confidence: 99%

Matrix Metalloproteinase 9 (MMP-9)-dependent Processing of βig-h3 Protein Regulates Cell Migration, Invasion, and Adhesion

Kim

Kwon

Kim

2012

Journal of Biological Chemistry

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Background: Cell migration is involved in altering the cell and matrix interface on the cell surface. Results: ␤ig-h3 is cleaved by MMP-9, and its cleavage results in changes in its binding properties, cell adhesion, cell migration, FAK/Src signals, and chemoattractant effects. Conclusion: MMP-9-cleaved ␤ig-h3 modulates tumor cell and macrophage migration. Significance: The MMP-9-mediated ␤ig-h3 processing mechanism is crucial for understanding cell migration.

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“…One possibility that we examined is that BIGH3 functions as a tumor suppressor that diminishes tumor viability by induction of apoptosis. In support of this possibility TGFBI −/− mice are predisposed to form tumors when compared to wild type mice [10]. Other investigators have shown that BIGH3 is downregulated in tumors and tumor cells of mesenchyme origin, indicating a tumor suppressor role [9] [58] [59] [60] [61] [62].…”

Section: Discussionmentioning

confidence: 99%

“…TGFBI −/− mice exhibited predisposition to develop various tumors, underscoring BIGH3's tumor suppressing property. Isolated TGFBI −/− mouse embryonic fibroblasts showed chromosomal abnormalities, increased cyclin D1 synthesis, and cell proliferation [10].…”

Section: Introductionmentioning

confidence: 97%

BIGH3: A Negative Regulator of Human Osteosarcoma Large Multicellular Spheroids

Thoma¹,

Moritz²,

Rezapoor³

et al. 2016

IJCM

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Numerous studies have demonstrated a relationship between the extracellular matrix protein BIGH3 and variations in the malignant properties of different cancer cell types, including osteosarcoma cells. BIGH3 protein can suppress and promote tumor growth, even on the same cancer cell type, indicating that contextual cues regulate BIGH3-mediated divergent outcomes. We employed a multicellular tumor spheroid model to study the effects of BIGH3 with respect to physical and molecular features of three-dimensional tumor growth. The results demonstrated that exogenous recombinant BIGH3 blocked the development of multicellular large tumor spheroids so that only small spheroids formed. The effect was dependent on the BIGH3 concentration in the growth medium and the time of incubation of BIGH3 with the osteosarcoma cells in the spheroid model. TGF-β1 signaling induced multicellular tumor spheroids to synthesize a greater quantity of BIGH3 relative to non-treated spheroids. The TGF-β1-mediated increase in BIGH3 protein antagonized the development of multicellular large spheroids. Anti-BIGH3 antibody, and an inhibitor of TGF-β1 signaling, blocked the antagonistic effect induced through TGF-β1 stimulation and BIGH3 protein expression, resulting in the formation of multicellular large spheroids. Immunohistochemistry detected BIGH3 at cell bodies within the spheroid stroma, suggesting osteosarcoma cell-surface proteins bind BIGH3. Flow cytometry demonstrates that osteosarcoma cells interact with soluble BIGH3, and solid-phase cell adhesion assays show that osteosarcoma adhesion to BIGH3 substratum is mediated by integrin α4β1. However, anti-α4 antibody did not attenuate the BIGH3-mediated antagonism toward formation of multicellular large spheroids. We conclude that TGFβ1 and BIGH3 suppress the development of large osteosarcoma tumors.

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TGFBI Deficiency Predisposes Mice to Spontaneous Tumor Development

Cited by 109 publications

References 47 publications

Identification of PITX1 as a TERT Suppressor Gene Located on Human Chromosome 5

Identification of PITX1 as a TERT Suppressor Gene Located on Human Chromosome 5

Matrix Metalloproteinase 9 (MMP-9)-dependent Processing of βig-h3 Protein Regulates Cell Migration, Invasion, and Adhesion

BIGH3: A Negative Regulator of Human Osteosarcoma Large Multicellular Spheroids

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