Ovarian cancer cells that coexpress endogenous Rb and p16 are insensitive to overexpression of functional p16 protein

Todd, Maria C.; Sclafani, Robert A.; Langan, Thomas A.

doi:10.1038/sj.onc.1203289

Cited by 26 publications

(32 citation statements)

References 42 publications

(52 reference statements)

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“…They also observed that p16 expression induced transcriptional downregulation of the RB gene (19). Ovarian cancer cell lines coexpressing p16 and RB are insensitive to p16 overexpression, suggesting that tumors that express both genes may be unresponsive to p16 gene therapy (21). Loss of expression of the p16 tumor suppressor occurs more often in ovarian cancers lacking p53 mutations (22), consistent with the paradigm that inactivation of p53 is less important in ovarian carcinogenesis when another G 1 regulatory gene has already been inactivated.…”

Section: G 1 Regulatorssupporting

confidence: 63%

“…These findings are in accordance with the knowledge that RB and p16 tumor suppressor genes function in the same pathway of cell cycle control. Investigations regarding the pRb/ cyclin D1/p16 pathway showed that coexpression of pRb, p16, and cyclin D1 is present in 82% of ovarian cancer tissues and cell lines, suggesting that defects in the pRb/cyclin D1/p16 pathway, other than the loss of pRb or p16, may play a major role in the development of ovarian cancer (21). Nieman et al (44) showed that for most ovarian carcinomas, RB alteration is not necessary for the development of a malignant phenotype, and RB mutation, when it does occur, may represent a sporadic event in ovarian carcinogenesis.…”

Section: G 1 -S Regulatorsmentioning

confidence: 99%

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Cell Cycle Genes in Ovarian Cancer

D’Andrilli

Kumar

Scambia

et al. 2004

Clinical Cancer Research

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Human malignant tumors are characterized by abnormal proliferation resulting from alterations in cell cycleregulatory mechanisms. The regulatory pathways controlling cell cycle phases include several oncogenes and tumor suppressor genes that display a range of abnormalities with potential usefulness as markers of evolution or treatment response in ovarian cancer. This review summarizes the current knowledge about these aberrations in malignant tumors of the ovary. We sought to divide cell cycle-regulatory genes into four subgroups on the basis of their predominant role in a specific phase or during the transition between two phases of the cell cycle.

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Section: G 1 Regulatorssupporting

confidence: 63%

Section: G 1 -S Regulatorsmentioning

confidence: 99%

Cell Cycle Genes in Ovarian Cancer

D’Andrilli

Kumar

Scambia

et al. 2004

Clinical Cancer Research

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“…As mentioned earlier, we previously reported the insensitivity of RB + /p16 + ovarian cancer cell lines to adenoviralmediated overexpression of p16 protein (7). The inability of p16 to induce a G1 arrest in one of the cell lines, NIH-OVCAR-3, was associated with the persistence of RB phosphorylation, suggesting deregulation of G1 cyclin-associated kinase activity in these cells.…”

Section: Introductionmentioning

confidence: 96%

“…1). Indeed, we have previously shown that 82% of ovarian tumors and cell lines retain the expression of both RB and p16 proteins with the majority overexpressing p16 protein (7). Despite the presence of these two negative regulators of G1-phase, however, RB + /p16 + ovarian cancer cell lines are defective with regard to G1/S regulation as indicated by their insensitivity to the growth suppressive effects of ectopically overexpressed functional p16 protein (7).…”

Section: Introductionmentioning

confidence: 99%

Small interference RNA-mediated suppression of overexpressed cyclin E protein restores G1/S regulation in NIH-OVCAR-3 ovarian cancer cells

Todd

Spruill²,

Meerbrey³

2009

Int J Oncol

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Abstract. The development of ovarian cancer, unlike that of most human tumors, is rarely dependent upon the mutually exclusive loss of RB and p16 cell cycle proteins. RB + /p16 + ovarian cancer cell lines are, however, insensitive to the growth-suppressive effects of ectopically expressed p16 protein, which suggests that they harbor as yet unidentified defects that compromise cell cycle regulation in late G1/S. In the current study, we used Western blotting to analyze cyclin E protein expression in a panel of normal and tumor ovarian tissues and ovarian cancer cell lines (including the p16-insensitive RB + /p16 + ovarian cancer cell line, NIH-OVCAR-3). Both the NIH-OVCAR-3 cell line and 70% of RB + /p16 + ovarian tumors showed abnormally elevated levels of the full-length cyclin E protein (EL1) in addition to several low molecular weight (LMW) isoforms of cyclin E. Using small interference RNA (siRNA), we have inhibited the synthesis of cyclin EL1 protein by approximately 80% and eliminated the LMW isoforms in NIH-OVCAR-3 ovarian cancer cells. Associated with the down-regulation of cyclin E expression, we observed both a marked shift in RB protein expression to the active, hypophosphorylated state and barely detectable expression of cyclin A (which is usually expressed upon entry into S-phase). Consistent with the protein expression data, cell cycle distribution analysis indicated that the NIH-OVCAR-3 cells had undergone a marked accumulation in G1 phase of the cell cycle. These data indicate the therapeutic potential of targeted RNA interference in the treatment of ovarian cancer patients whose tumors overexpress cyclin E protein.

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“…37 Although the status of p16Ink4 in COLO 357 has not been described, nearly all pancreatic adenocarcinomas that have been tested lack normal p16 expression. 38 The SK -OV3 (Rb positive, p16 null ) 39 ovarian carcinoma cell line, the SAOS -2 (Rb negative) 40 and U2OS (Rb positive, low p16 ) 41 osteosarcoma cell lines, the MDA -MB -453 (Rb positive, 42 cyclin D1 amplification 43 ) breast carcinoma cell line, the WI38 normal human fibroblast cell line, and the 293 cell line were obtained from American Type Culture Collection. All of the cell lines express p84N5 detectable by Western blot analysis ( data not shown), although the relative level of expression varies by as much as 5 -fold from high -expressing lines (U2OS) to lowexpressing lines (WI38 ).…”

Section: Cell Culture and Animal Modelsmentioning

confidence: 99%

Adenovirus-mediated N5 gene transfer inhibits tumor growth and metastasis of human carcinoma in nude mice

Yin

Wang

Xie³

et al. 2002

Cancer Gene Ther

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The therapeutic effectiveness of cancer therapy often relies on induction of apoptotic cell death. Gene -therapy -mediated induction of apoptosis, therefore, may provide an effective means to kill cancer cells. The N5 gene encodes a death -domain -containing protein ( p84N5 ) that can trigger atypical apoptosis from within the nucleus, suggesting it may be a candidate for use as a gene therapy for cancer. In the present study, we test the potential utility of a recombinant adenovirus designed to express the N5 gene ( AdN5 ) for the treatment of a variety of human cancers using in vitro and animal models. In vitro, adenoviral -mediated N5 gene transfer inhibits the growth of five different tumor cell lines, but not a normal diploid fibroblast cell line. Adenoviral -mediated N5 gene transfer also reduces the growth and metastasis of primary human tumors in subcutaneous and orthotopic xenograft mouse models. Reduction in tumor cell growth in vitro and in vivo correlates with increased expression of p84N5 and induction of apoptosis. The relative sensitivity of different human cancer cells to AdN5 or Adp53 varies, suggesting that AdN5 may be effective in tumors relatively resistant to p53 gene therapy. We conclude that N5 has potential utility for the gene therapy of cancer.

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Ovarian cancer cells that coexpress endogenous Rb and p16 are insensitive to overexpression of functional p16 protein

Cited by 26 publications

References 42 publications

Cell Cycle Genes in Ovarian Cancer

Cell Cycle Genes in Ovarian Cancer

Small interference RNA-mediated suppression of overexpressed cyclin E protein restores G1/S regulation in NIH-OVCAR-3 ovarian cancer cells

Adenovirus-mediated N5 gene transfer inhibits tumor growth and metastasis of human carcinoma in nude mice

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