Characterization of a Carcinogenesis Rat Model of Ovarian Preneoplasia and Neoplasia

Stewart, Sherri L.; Querec, Troy D.; Ochman, Alexander R.; Gruver, Briana N.; Bao, Rong; Babb, James S.; Wong, Thang S.; Koutroukides, Theodoros; Pinnola, Aaron D.; Klein‐Szanto, Andres J.; Hamilton, Thomas C.; Patriotis, Christos

doi:10.1158/0008-5472.can-04-1702

Cited by 63 publications

(74 citation statements)

References 37 publications

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“…Furthermore, we also observed that the basal levels of the p53 protein were also increased in the MAD2DC-agar cells (Figure 5a). It is possible that DMBA treatment may have caused mutations on the p53 gene as previously reported (Stewart et al, 2004) which leads to stabilization of this protein. However, sequencing analysis of the p53 gene showed no evidence of mutation, suggesting that the increased p53 expression is not the result of DMBA-induced mutation.…”

Section: Mad2dc Promotes Carcinogen-induced Transformationmentioning

confidence: 78%

“…For example, der(1)t(1;16) was observed in over 87% of the MAD2DC-agar cells while this aberration was not detected in the MAD2DC cells (see white circles in Figure 2a). Since the carcinogenic effect of DMBA is believed to be through its mutagenic effect on the genome (Stewart et al, 2004), it is not a surprise to observe the increased chromosomal structural alterations in the MAD2DC-agar cells. Cell cycle analysis revealed a similar pattern between MAD2DC and MAD2DC-agar cells before and after exposure to nocodazole (Figure 3a) and suggested that the polyploidy MAD2DC-agar cells were also able to undergo cell division in the presence on microtubule disruption.…”

Section: Mad2dc Promotes Carcinogen-induced Transformationmentioning

confidence: 99%

“…Role of p53 and MEK pathways in the MAD2DC-induced transformation Carcinogens such as DMBA promotes tumorigenesis through inactivation of tumor suppressor pathways such as the p53 pathway possibly through induction of gene mutations (Stewart et al, 2004). Although the HPV E6 oncogene is able to inactivate p53 through premature degradation of this protein (Kessis et al, 1993), a functional p53 pathway has been reported in certain HPV E6/E7-immortalized cell lines (Butz et al, 1995).…”

Section: Mad2dc Promotes Carcinogen-induced Transformationmentioning

confidence: 99%

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MAD2ΔC induces aneuploidy and promotes anchorage-independent growth in human prostate epithelial cells

Cheung

et al. 2007

Oncogene

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The mitotic arrest deficient 2 (MAD2) is suggested to play a key role in a functional mitotic checkpoint because of its inhibitory effect on anaphase-promoting complex/cyclosome (APC/C) during mitosis. The binding of MAD2 to mitotic checkpoint regulators MAD1 and Cdc20 is thought to be crucial for its function and loss of which leads to functional inactivation of the MAD2 protein. However, little is known about the biological significance of this MAD2 mutant in human cells. In this study, we stably transfected a C-terminal-deleted MAD2 gene (MAD2DC) into a human prostate epithelial cell line, Hpr-1 and studied its effect on chromosomal instability, cell proliferation, mitotic checkpoint control and soft agar colony-forming ability. We found that MAD2DC was able to induce aneuploidy through promoting chromosomal duplication, which was a result of an impaired mitotic checkpoint and cytokinesis, suggesting a crucial role of MAD2-mediated mitotic checkpoint in chromosome stability in human cells. In addition, the MAD2DC-transfected cells displayed anchorage-independent growth in soft agar after challenged by 7,12-dimethylbenz[A]anthracene (DMBA), demonstrating a cancer-promoting effect of a defective mitotic checkpoint in human cells. Furthermore, the DMBA-induced transformation was accompanied by a complete loss of DNA damage-induced p53 response and activation of the MAPK pathway in MAD2DC cells. These results indicate that a defective mitotic checkpoint alone is not a direct cause of tumorigenesis, but it may predispose human cells to carcinogen-induced malignant transformation. The evidence presented here provides a link between MAD2 inactivation and malignant transformation of epithelial cells.

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Section: Mad2dc Promotes Carcinogen-induced Transformationmentioning

confidence: 78%

Section: Mad2dc Promotes Carcinogen-induced Transformationmentioning

confidence: 99%

Section: Mad2dc Promotes Carcinogen-induced Transformationmentioning

confidence: 99%

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MAD2ΔC induces aneuploidy and promotes anchorage-independent growth in human prostate epithelial cells

Cheung

et al. 2007

Oncogene

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“…The direct application of DMBA to the ovary has been shown to result in selective development of ovarian malignancies in both rats and mice. 2,[6][7][8][9][10] The development of a post-menopausal animal model for ovarian cancer may prove useful in evaluating diagnostic tools to aid in differentiating benign and malignant ovarian pathology and provide better understanding of features characteristic of early cancers to improve their detection. Optical coherence tomography is an emerging, non-destructive imaging modality using near-infrared light to create cross-sectional images of tissue structure with near histological resolution (2-20 µm) with the advantage of up to 2 mm penetration depth compared to other optical technologies which may only have 100 micron or less penetration.…”

Section: Resultsmentioning

confidence: 99%

Simultaneous optical coherence tomography and laser induced fluorescence imaging in rat model of ovarian carcinogenesis

Hariri

Liebmann

Marion

et al. 2010

Cancer Biology & Therapy

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pathologic changes in the ovary, specifically the characterization of precursor lesions to malignant transformation.The incidence of all types of ovarian cancer except germ cell neoplasms increases approximately ten-fold in post-menopausal women, 1 thus the availability of an animal ovarian cancer model mimicking the post-menopausal state would be most applicable to epithelial and stromal ovarian tumors. Recently, a rodent model was developed to mirror the post-menopausal state, utilizing 4-vinylcyclohexene diepoxide (VCD) to accelerate atresia of ovarian follicles. VCD selectively eradicates primordial and primary follicles from the ovary without direct effect on larger, more mature follicles resulting in a gradual onset of ovarian failure with accompanying hormonal changes emulating the human peri-menopausal state.

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“…O gene ras, quando alterado (oncogen ras), o que ocorre em cerca de 10% a 20% dos tumores de mama (Stewart et al, 2004;De Vita et al, 2004) Rogers et al (1998) e Russo et al (1990Russo et al ( , 2005a.…”

Section: R Re Ev VI Is Sã ãO O D Da a L Li It Te Er Ra At Tu Ur Ra A unclassified

Efeitos morfológicos, histológicos e moleculares dos moduladores seletivos dos receptores de estrogênios tamoxifeno e raloxifeno na prevenção primária de tumores mamários quimicamente induzidos em ratas

Mori¹

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Characterization of a Carcinogenesis Rat Model of Ovarian Preneoplasia and Neoplasia

Cited by 63 publications

References 37 publications

MAD2ΔC induces aneuploidy and promotes anchorage-independent growth in human prostate epithelial cells

MAD2ΔC induces aneuploidy and promotes anchorage-independent growth in human prostate epithelial cells

Simultaneous optical coherence tomography and laser induced fluorescence imaging in rat model of ovarian carcinogenesis

Efeitos morfológicos, histológicos e moleculares dos moduladores seletivos dos receptores de estrogênios tamoxifeno e raloxifeno na prevenção primária de tumores mamários quimicamente induzidos em ratas

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