The atypical E2F family member E2F7 couples the p53 and RB pathways during cellular senescence

Aksoy, Ozlem; Chicas, Agustin; Zeng, Tianying; Zhao, Zhen; McCurrach, Mila E.; Wang, Xiaowo; Lowe, Scott W.

doi:10.1101/gad.196238.112

Cited by 114 publications

(108 citation statements)

References 59 publications

(82 reference statements)

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“…Further, these E2Fs have now been shown to function as repressors of the very genes that are induced by the activator E2Fs (16,17). Such a regulatory relationship has been described as an incoherent feed-forward mechanism in which an activator induces a target but at the same time also induces a repressor of the target, thus limiting the extent of the induction (39).…”

Section: Discussionmentioning

confidence: 99%

“…ChIP-sequencing analysis reveals that E2F7 binds to multiple G 1 /S-regulated genes and represses their transcription (16). E2F7 is induced by p53 and is involved in cell cycle arrest response to DNA damage and cellular senescence (17)(18)(19). Recent studies using mouse model systems also show that the atypical E2Fs are involved in angiogenesis, polyploidization, and placental development (20 -23).…”

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confidence: 99%

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Interaction of E2F7 Transcription Factor with E2F1 and C-terminal-binding Protein (CtBP) Provides a Mechanism for E2F7-dependent Transcription Repression

Liu

Shats

Gatza

et al. 2013

Journal of Biological Chemistry

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Background: E2F7 is a transcription factor that controls cell cycle by repressing the expression of G 1 /S genes in late S phase. Results: E2F7 forms a heterodimer with E2F1, and it recruits the co-repressor CtBP to repress G 1 /S transcription. Conclusion: E2F7 represses gene transcription by interacting with E2F1 and co-repressor CtBP. Significance: These findings suggest a mechanism for the repression of transcription by E2F7.

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

Interaction of E2F7 Transcription Factor with E2F1 and C-terminal-binding Protein (CtBP) Provides a Mechanism for E2F7-dependent Transcription Repression

Liu

Shats

Gatza

et al. 2013

Journal of Biological Chemistry

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“…The correct regulation of the E2F7 alternative exon is likely important for the cell, because use of the exon changes the reading frame and alters the C terminus of the protein, which is necessary for the transcriptional activation of its target genes. E2F7 has antiproliferative properties (61,62), and it is possible that SNORD27 changes observed in cancer influence E2F7-dependent cell cycle regulation.…”

Section: Discussionmentioning

confidence: 99%

Dual function of C/D box small nucleolar RNAs in rRNA modification and alternative pre-mRNA splicing

Falaleeva

Pagès

Matuszek

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

165

152

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C/D box small nucleolar RNAs (SNORDs) are small noncoding RNAs, and their best-understood function is to target the methyltransferase fibrillarin to rRNA (for example, SNORD27 performs 2′-Omethylation of A27 in 18S rRNA). Unexpectedly, we found a subset of SNORDs, including SNORD27, in soluble nuclear extract made under native conditions, where fibrillarin was not detected, indicating that a fraction of the SNORD27 RNA likely forms a protein complex different from canonical snoRNAs found in the insoluble nuclear fraction. As part of this previously unidentified complex, SNORD27 regulates the alternative splicing of the transcription factor E2F7 pre-mRNA through direct RNA-RNA interaction without methylating the RNA, likely by competing with U1 small nuclear ribonucleoprotein (snRNP). Furthermore, knockdown of SNORD27 activates previously "silent" exons in several other genes through base complementarity across the entire SNORD27 sequence, not just the antisense boxes. Thus, some SNORDs likely function in both rRNA and pre-mRNA processing, which increases the repertoire of splicing regulators and links both processes.alternative splicing | gene regulation | snoRNAs | pre-mRNA processing S mall nucleolar RNAs (snoRNAs) are 60-to 300-nt-long noncoding RNAs that accumulate in the nucleolus. Based on conserved sequence elements, snoRNAs are classified as C/D box small nucleolar RNAs (SNORDs) or H/ACA box snoRNAs (SNORAs). SNORDs contain sequence elements termed C (RUGAUGA) and D (CUGA) boxes, usually present in duplicates (C′ and D′ boxes), and up to two antisense boxes that hybridize to the target RNA (1). In humans, SNORDs are usually derived from introns. After the splicing reaction, introns are excised as lariats, which are then opened by the debranching enzyme and subsequently degraded. Intronic SNORDs escape this degradation by forming a protein complex that consists of non-histone chromosome protein 2-like 1 (NHP2L1, 15.5K, SNU13), nucleolar protein 5A (NOP56), nucleolar protein 5 (NOP58), and fibrillarin (2-4). The SNORD protein complex forms through the entry of the snoRNA and fibrillarin to a complex containing NHP2L1, NOP58, and at least five assembly factors (5). The SNORD acts as a scaffold for the final protein complex formation and also controls recognition of other RNAs using the antisense boxes. The antisense boxes recognize sequences in rRNA, resulting in the fifth nucleotide upstream of the D or D′ box being 2′-O-methylated by fibrillarin (1). Structural studies indicate that the active form of SNORDs is dimeric (6).The conserved overall structure of SNORDs allows the identification of their putative target RNA binding sites. However, numerous SNORDs without obvious target RNAs have been identified (7-10) and are termed "orphan snoRNAs." Genome-wide deep sequencing experiments identified shorter but stable SNORD fragments that were found in all species tested, ranging from mammals to the protozoan Giardia lamblia (11) and EpsteinBarr virus (12). Fragments longer than 27 nt generated by SNORDs will ...

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“…A senescent phenotype of the syncytiotrophoblast, including high DCR2 expression, might contribute to this inactivation and thus support the viability of these cells. Of note, knockout of genes that can regulate senescence (pRb or E2F7) leads to disorganization of the trophoblast in mice and even causes embryonic lethality (Narita et al 2003;Wu et al 2003;Aksoy et al 2012;Ouseph et al 2012). Placenta-specific ablation of pRb, for example, causes embryonic lethality, and placenta malfunction is the defect responsible for the embryonic lethality of pRb knockout mice (Wu et al 2003).…”

Section: Discussionmentioning

confidence: 99%

Cell fusion induced by ERVWE1 or measles virus causes cellular senescence

et al. 2013

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Cellular senescence limits proliferation of potentially detrimental cells, preventing tumorigenesis and restricting tissue damage. However, the function of senescence in nonpathological conditions is unknown. We found that the human placental syncytiotrophoblast exhibited the phenotype and expressed molecular markers of cellular senescence. During embryonic development, ERVWE1-mediated cell fusion results in formation of the syncytiotrophoblast, which serves as the maternal/fetal interface at the placenta. Expression of ERVWE1 caused cell fusion in normal and cancer cells, leading to formation of hyperploid syncytia exhibiting features of cellular senescence. Infection by the measles virus, which leads to cell fusion, also induced cellular senescence in normal and cancer cells. The fused cells activated the main molecular pathways of senescence, the p53-and p16-pRbdependent pathways; the senescence-associated secretory phenotype; and immune surveillance-related proteins. Thus, fusion-induced senescence might be needed for proper syncytiotrophoblast function during embryonic development, and reuse of this senescence program later in life protects against pathological expression of endogenous fusogens and fusogenic viral infections.

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The atypical E2F family member E2F7 couples the p53 and RB pathways during cellular senescence

Cited by 114 publications

References 59 publications

Interaction of E2F7 Transcription Factor with E2F1 and C-terminal-binding Protein (CtBP) Provides a Mechanism for E2F7-dependent Transcription Repression

Interaction of E2F7 Transcription Factor with E2F1 and C-terminal-binding Protein (CtBP) Provides a Mechanism for E2F7-dependent Transcription Repression

Dual function of C/D box small nucleolar RNAs in rRNA modification and alternative pre-mRNA splicing

Cell fusion induced by ERVWE1 or measles virus causes cellular senescence

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