Literature DB >> 15798191

dDP is needed for normal cell proliferation.

Maxim V Frolov1, Nam-Sung Moon, Nicholas J Dyson.   

Abstract

To gain insight into the essential functions of E2F, we have examined the phenotypes caused by complete inactivation of E2F and DP family members in Drosophila. Our results show that dDP requires dE2F1 and dE2F2 for DNA-binding activity in vitro and in vivo. In tissue culture cells and in mutant animals, the levels of dE2F and dDP proteins are strongly interdependent. In the absence of dDP, the levels of dE2F1 and dE2F2 decline dramatically, and vice versa. Accordingly, the cell cycle and transcriptional phenotypes caused by targeting dDP mimic the effects of targeting both dE2F1 and dE2F2 and are indistinguishable from the effects of inactivating all three proteins. Although trans-heterozygous dDP mutant animals develop to late pupal stages, the analysis of somatic mutant clones shows that dDP mutant cells are at a severe proliferative disadvantage when compared directly with wild-type neighbors. Strikingly, the timing of S-phase entry or exit is not delayed in dDP mutant clones, nor is the accumulation of cyclin A or cyclin B. However, the maximal level of bromodeoxyuridine incorporation is reduced in dDP mutant clones, and RNA interference experiments show that dDP-depleted cells are prone to stall in S phase. In addition, dDP mutant clones contain reduced numbers of mitotic cells, indicating that dDP mutant cells have a defect in G2/M-phase progression. Thus, dDP is not essential for developmental control of the G1-to-S transition, but it is required for normal cell proliferation, for optimal DNA synthesis, and for efficient G2/M progression.

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Year:  2005        PMID: 15798191      PMCID: PMC1069608          DOI: 10.1128/MCB.25.8.3027-3039.2005

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


  40 in total

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Journal:  Mol Cell Biol       Date:  2001-07       Impact factor: 4.272

Review 4.  The E2F family: specific functions and overlapping interests.

Authors:  Claire Attwooll; Eros Lazzerini Denchi; Kristian Helin
Journal:  EMBO J       Date:  2004-11-11       Impact factor: 11.598

5.  Novel function of the cyclin A binding site of E2F in regulating p53-induced apoptosis in response to DNA damage.

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8.  Drosophila E2f2 promotes the conversion from genomic DNA replication to gene amplification in ovarian follicle cells.

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5.  Loss of dE2F compromises mitochondrial function.

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6.  A robust cell cycle control mechanism limits E2F-induced proliferation of terminally differentiated cells in vivo.

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7.  Tuberous sclerosis complex 1 regulates dE2F1 expression during development and cooperates with RBF1 to control proliferation and survival.

Authors:  Ting-Chiu Hsieh; Brandon N Nicolay; Maxim V Frolov; Nam-Sung Moon
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8.  Paradoxical instability-activity relationship defines a novel regulatory pathway for retinoblastoma proteins.

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9.  Protein phosphatase 2A promotes the transition to G0 during terminal differentiation in Drosophila.

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10.  dE2F2-independent rescue of proliferation in cells lacking an activator dE2F1.

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Journal:  Mol Cell Biol       Date:  2007-10-08       Impact factor: 4.272

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