Rb family proteins as modulators of gene expression and new aspects regarding the interaction with chromatin remodeling enzymes

Macaluso, Marcella; Montanari, Micaela; Giordano, Antonio

doi:10.1038/sj.onc.1209680

Cited by 121 publications

(112 citation statements)

References 81 publications

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“…The down regulation of CDK2 and pRb might be responsible for chromatin remodeling [35] that might contribute to sustained down regulation of survivin, the overexpression of which could enhance malignant potential of glioblastomas [36,37]. One of the interesting observations made in the present study was the down regulation of survivin in glioblastoma cells after treatment with 4-HPR alone and also in combination with IFN-γ (Fig.…”

Section: Discussionsupporting

confidence: 59%

N-(4-Hydroxyphenyl)retinamide induced differentiation with repression of telomerase and cell cycle to increase interferon-γ sensitivity for apoptosis in human glioblastoma cells

2008

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Glioblastoma is the most malignant and prevalent brain tumor in humans. It is composed of heterogenic abnormal astroglial cells that avoid differentiation, maintain proliferation, and reluctant to apoptosis. N-(4-Hydroxyphenyl) retinamide (4-HPR) induced astrocytic differentiation and increased sensitivity to interferon-gamma (IFN-γ) for apoptosis in human glioblastoma A172, LN18, and SNB19 cells. Combination of 4-HPR and IFN-γ significantly inhibited human telomerase reverse transcriptase (hTERT), cyclin dependent kinase 2 (CDK2), and survivin to upregulate caspase-8, caspase-9, and caspase-3 for increasing apoptosis in all glioblastoma cell lines. Hence, combination of 4-HPR and IFN-γ should be considered for controlling growth of different human glioblastoma cells.

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Section: Discussionsupporting

confidence: 59%

N-(4-Hydroxyphenyl)retinamide induced differentiation with repression of telomerase and cell cycle to increase interferon-γ sensitivity for apoptosis in human glioblastoma cells

2008

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“…Consistent with this finding, The functional consequence of FoxO-mediated disruption of cyclin-CDK complex formation is to decrease the phosphorylation of the pRB family proteins, and hence E2F transcriptional activity. However, FoxO may also directly target the pRB family members p107 and p130 (also called pRB2) (Bandara et al, 1994;Giacinti and Giordano, 2006;Macaluso et al, 2006); mammalian FoxO3a and FoxO4 have been shown to directly activate the transcription of the p130 gene, which can induce cells to undergo cell cycle arrest and enter a quiescent state (Kops et al, 2002b). Interestingly, some cell cycle regulators, including p107, pRB, E2F1-3, cyclin D1, cyclin E1/2, cyclin A1/2, CDK2 and CDC2 are themselves transcriptional targets of E2F-and pRBrelated proteins (Dalton, 1992;Furukawa et al, 1994;Shan et al, 1994;Ohtani et al, 1995;Schulze et al, 1995;Sears et al, 1997;Araki et al, 2003;Cobrinik, 2005).…”

Section: Foxo and The G1/s Phase Transitionmentioning

confidence: 99%

Many forks in the path: cycling with FoxO

2008

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FoxO transcription factors are an evolutionary conserved subfamily of the forkhead transcription factors, characterized by the forkhead DNA-binding domain. FoxO factors regulate a number of cellular processes involved in cell-fate decisions in a cell-type-and environment-specific manner, including metabolism, differentiation, apoptosis and proliferation. A key mechanism by which FoxO determines cell fate is through regulation of the cell cycle machinery, and as such the cellular consequence of FoxO deregulation is often manifested through perturbation of the cell cycle. Consequently, the deregulation of FoxO factors is implicated in the development of numerous proliferative diseases, in particular cancer.

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“…This family includes the product of the Rb susceptibility gene, the pRb/p105 protein and the related p107 and pRb2/130 proteins (Mayol et al, 1993;Du and Pogoriler, 2006;Merola et al, 2006). They share the ability to recruit chromatin-remodeling enzymes and their best characterized targets are the members of the E2F/DP family of transcription factors, generally referred to as E2F (Cinti et al, 2005;Tosi et al, 2005;Genovese et al, 2006;Macaluso et al, 2006;Purev et al, 2006). Both pRb2/p130 and p107 are able to bind cdk2/ cyclins A and E (Claudio et al, 1996).…”

Section: Introductionmentioning

confidence: 99%

A small molecule based on the pRb2/p130 spacer domain leads to inhibition of cdk2 activity, cell cycle arrest and tumor growth reduction in vivo

et al. 2006

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One strategy in the development of anticancer therapeutics has been to arrest malignant proliferation through inhibition of the enzymatic activity of cyclin-dependent kinases (cdks), which are key regulatory molecules of the cell cycle. Over the past few years, numerous compounds with remarkable cdk inhibitory activity have been studied in cancer therapy, although it is very difficult to point out the best cdk to target. An excellent candidate appears to be cdk2, whose alteration is a pathogenic hallmark of tumorigenesis. The small molecule described in our study showed an inhibitory effect on the kinase activity of cdk2, a significant growth arrest observed in a colony formation assay and a reduction in the size of the tumor in nude mice, thus suggesting its potential role as a promising new type of mechanism-based antitumor drug, also for the treatment of hyperproliferative disorders.

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Rb family proteins as modulators of gene expression and new aspects regarding the interaction with chromatin remodeling enzymes

Cited by 121 publications

References 81 publications

N-(4-Hydroxyphenyl)retinamide induced differentiation with repression of telomerase and cell cycle to increase interferon-γ sensitivity for apoptosis in human glioblastoma cells

N-(4-Hydroxyphenyl)retinamide induced differentiation with repression of telomerase and cell cycle to increase interferon-γ sensitivity for apoptosis in human glioblastoma cells

Many forks in the path: cycling with FoxO

A small molecule based on the pRb2/p130 spacer domain leads to inhibition of cdk2 activity, cell cycle arrest and tumor growth reduction in vivo

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