Differentially Active Origins of DNA Replication in Tumor versus Normal Cells

Paola, Domenic Di; Price, Gerald B.; Zannis‐Hadjopoulos, Maria

doi:10.1158/0008-5472.can-05-3951

Cited by 18 publications

(38 citation statements)

References 52 publications

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“…Indeed, increased activity of DNA replication origins in tumor cells or SV-40 transformed cells have been reported, suggesting that transformation may induce greater frequency of initiation of origins at certain loci. [39][40][41][42] The increased origin activity in tumor/transformed cells compared to normal cells may be influenced by many parameters including concentration and activity of initiation factors, chromatin structure and nuclear organization. 41 Potentially, FA proteins might be involved in these processes to regulate initiation of DNA replication.…”

Section: Discussionmentioning

confidence: 99%

A novel role for fanconi anemia (FA) pathway effector protein FANCD2 in cell cycle progression of untransformed primary human cells

Song¹,

Barkley²,

Day³

et al. 2010

Cell Cycle

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Section: Discussionmentioning

confidence: 99%

A novel role for fanconi anemia (FA) pathway effector protein FANCD2 in cell cycle progression of untransformed primary human cells

Song¹,

Barkley²,

Day³

et al. 2010

Cell Cycle

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“…Moreover, the origin activity in the tumor-transformed cells is two-to threefold higher than that of normal cells. 30 In chromosomal DNA replication, a plausible supermolecular assembly, the origin recognition complex, and the replisomes are thought to function in DNA replication initiation and the elongation of the DNA strands, respectively. The cell cycle starts from a Go quiescent state.…”

Section: Chromosomal Dna Duplication and Cell Divisionmentioning

confidence: 99%

Molecular basis for the actions of Hsp90 inhibitors and cancer therapy

et al. 2011

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Heat-shock protein 90 (Hsp90) inhibitor downregulates c-Myc expression and upregulates the expression of tumor repressor proteins such as p53 and pRB, inhibiting the G1/S transition and causing G2/M arrest during cell cycle progression. The cycle progression is extensively controlled by the pRB/E2F signaling pathway. E2F is released from the pRB/E2F complex with the phosphorylation of pRB by cyclin-cyclin-dependent kinase (CDK) complexes. The released E2F promotes the transcription of target genes involved in cell cycle progression. The pRB/E2F signaling pathway is controlled by DNA methyltransferase-1 (Dnmt-1). The elevated expression of Dnmt-1 has been reported in carcinomas of the colon, lung and prostate. A defect of pRB expression in RbÀ/À cancer cells is caused by the aberrant methylation of CpG in the Rb promoter. The Hsp90 inhibitor disrupts the Dnmt-1/Hsp90 association and upregulates pRB expression. In this review, the Hsp90 inhibitors that show promise for cancer therapy are summarized.

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“…A twofold increase in origin activity across the same 12.5 kb region of the human c-myc locus was also found in the isogenic cell lines WI38 and their transformed counterpart WI38 (SV40) [Tao et al, 2001], ruling out the possibility that cell type effects were the cause of the differential origin usage found in HeLa and NSF cells. It was thus concluded that the increased origin activities were the result of cellular transformation.More recent studies have found two-to threefold higher origin activities in transformed/tumor cells compared to normal cells, suggesting higher activation of these origins located across this $211 kb region on human chromosome 19q13 [Di Paola et al, 2006]. Again, use of the isogenic cell lines of WI38 and WI38(SV40) showed that the origins are at least twice as active in the transformed cell line (WI38(SV40)) compared to that of its normal counterpart (WI38), ruling out the possibility that cell type effects were responsible for increased frequency of initiation.…”

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confidence: 95%

“…The distribution of this 20mer consensus over 1 Mb of human chromosomal DNA is similar, quantitatively and qualitatively to the distribution of the ARS consensus sequence (ACS) on S. cerevisiae chromosomes . Finally, six versions of the 20mer which were analyzed ectopically and endogenously were found to act as origins of DNA replication in plasmids as well as in situ, at their chromosomal loci, suggesting that the 20-bp consensus sequence can be used to predict chromosomal regions that contain replication origins [Di Paola et al, 2006]. …”

mentioning

confidence: 99%

“…The increased origin activity across the $211 kb region in tumor/transformed cells compared to normal cells may be influenced by one or many parameters regulating DNA replication, such as the concentration and conformation of initiator proteins [McNairn and Gilbert, 2005;Lau et al, 2007;Blow and Gillespie, 2008], specific DNA sequences within the initiation sites having differential affinities for ORC [Bell, 2002], gene transcription [DePamphilis, 1993], chromatin structure [Melendy and Li, 2001;Aladjem, 2007], nuclear organization [Taddei et al, 2004;Ottaviani et al, 2008], and nucleotide pool levels [Anglana et al, 2003]. Previous work suggests that there are at least two types of malignant changes in regulation of DNA replication, the unexpected increase in origin activity at some loci [Tao et al, 1997[Tao et al, , 2000[Tao et al, , 2001Di Paola et al, 2006] and activation of silent origins [Martin and Oppenheim, 1977;Oppenheim and Martin, 1978]. Thus, it appears that there are at least three subsets of origins; those that are normal and remain unchanged, those with increased activity in immortalized or malignant cells, and those that are activated solely in tumor cells.…”

mentioning

confidence: 99%

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Metazoan origins of DNA replication: Regulation through dynamic chromatin structure

Rampakakis

Arvanitis

Paola

et al. 2009

J of Cellular Biochemistry

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DNA replication in eukaryotes is initiated at multiple replication origins distributed over the entire genome, which are normally activated once per cell cycle. Due to the complexity of the metazoan genome, the study of metazoan replication origins and their activity profiles has been less advanced than in simpler genome systems. DNA replication in eukaryotes involves many protein-protein and protein-DNA interactions, occurring in multiple stages. As in prokaryotes, control over the timing and frequency of initiation is exerted at the initiation site. A prerequisite for understanding the regulatory mechanisms of eukaryotic DNA replication is the identification and characterization of the cis-acting sequences that serve as replication origins and the trans-acting factors (proteins) that interact with them. Furthermore, in order to understand how DNA replication may become deregulated in malignant cells, the distinguishing features between normal and malignant origins of DNA replication as well as the proteins that interact with them must be determined. Based on advances that were made using simple genome model systems, several proteins involved in DNA replication have been identified. This review summarizes the current findings about metazoan origins of DNA replication and their interacting proteins as well as the role of chromatin structure in their regulation. Furthermore, progress in origin identification and isolation procedures as well as potential mechanisms to inhibit their activation in cancer development and progression are discussed.

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Differentially Active Origins of DNA Replication in Tumor versus Normal Cells

Cited by 18 publications

References 52 publications

A novel role for fanconi anemia (FA) pathway effector protein FANCD2 in cell cycle progression of untransformed primary human cells

A novel role for fanconi anemia (FA) pathway effector protein FANCD2 in cell cycle progression of untransformed primary human cells

Molecular basis for the actions of Hsp90 inhibitors and cancer therapy

Metazoan origins of DNA replication: Regulation through dynamic chromatin structure

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