Literature DB >> 11416145

Role for E2F in control of both DNA replication and mitotic functions as revealed from DNA microarray analysis.

S Ishida1, E Huang, H Zuzan, R Spang, G Leone, M West, J R Nevins.   

Abstract

We have used high-density DNA microarrays to provide an analysis of gene regulation during the mammalian cell cycle and the role of E2F in this process. Cell cycle analysis was facilitated by a combined examination of gene control in serum-stimulated fibroblasts and cells synchronized at G(1)/S by hydroxyurea block that were then released to proceed through the cell cycle. The latter approach (G(1)/S synchronization) is critical for rigorously maintaining cell synchrony for unambiguous analysis of gene regulation in later stages of the cell cycle. Analysis of these samples identified seven distinct clusters of genes that exhibit unique patterns of expression. Genes tend to cluster within these groups based on common function and the time during the cell cycle that the activity is required. Placed in this context, the analysis of genes induced by E2F proteins identified genes or expressed sequence tags not previously described as regulated by E2F proteins; surprisingly, many of these encode proteins known to function during mitosis. A comparison of the E2F-induced genes with the patterns of cell growth-regulated gene expression revealed that virtually all of the E2F-induced genes are found in only two of the cell cycle clusters; one group was regulated at G(1)/S, and the second group, which included the mitotic activities, was regulated at G(2). The activation of the G(2) genes suggests a broader role for E2F in the control of both DNA replication and mitotic activities.

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Year:  2001        PMID: 11416145      PMCID: PMC87143          DOI: 10.1128/MCB.21.14.4684-4699.2001

Source DB:  PubMed          Journal:  Mol Cell Biol        ISSN: 0270-7306            Impact factor:   4.272


  24 in total

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  235 in total

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3.  Use of chromatin immunoprecipitation to clone novel E2F target promoters.

Authors:  A S Weinmann; S M Bartley; T Zhang; M Q Zhang; P J Farnham
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Journal:  Mol Cell Biol       Date:  2003-04       Impact factor: 4.272

5.  Deregulation of Rb-E2F1 axis causes chromosomal instability by engaging the transactivation function of Cdc20-anaphase-promoting complex/cyclosome.

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6.  Jab1/CSN5 mediates E2F dependent expression of mitotic and apoptotic but not DNA replication targets.

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7.  Distinct mechanisms of E2F regulation by Drosophila RBF1 and RBF2.

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8.  Cell cycle-dependent and cell cycle-independent control of transcription by the Drosophila E2F/RB pathway.

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