Id3 is a novel regulator of p27kip1 mRNA in early G1 phase and is required for cell-cycle progression

Chassot, Anne-Amandine; Turchi, Laurent; Virolle, Thierry; Fitsialos, Giorgos; Batoz, M; Deckert, Marcel; Dulić, Vjekoslav; Meneguzzi, Guerríno; Buscà, Roser; Ponzio, Gilles

doi:10.1038/sj.onc.1210386

Cited by 30 publications

(28 citation statements)

References 50 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…This may explain the 13I effect on SH-EP cells, at least partly, as E47 activity prevents cell cycle progression in neuroblastoma cells (Rothschild et al, 2006). Finally, 13I affected the expression of the Id targets p27 kip1 and VEGF (Lasorella et al, 2005;Chassot et al, 2007), by turning the first on and the second off. Such a deregulation was reversed by over-producing ID2.…”

Section: Discussionmentioning

confidence: 98%

“…Through the HLH domain, Ids associate with the ubiquitous bHLHs, the E proteins, preventing DNA binding and complex formation with tissue-specific bHLHs (Ruzinova and Benezra, 2003). They also interact with non-bHLH proteins such as PAX, ETS, ELK and underphosphorylated RB (Iavarone et al, 1994;Ohtani et al, 2001;Roberts et al, 2001;Chassot et al, 2007).…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Targeting Id protein interactions by an engineered HLH domain induces human neuroblastoma cell differentiation

et al. 2009

View full text Add to dashboard Cite

Inhibitor of DNA-binding (Id) proteins prevent cell differentiation, promote growth and sustain tumour development. They do so by binding to E proteins and other transcription factors through the helix-loop-helix (HLH) domain, and inhibiting transcription. This makes HLH-mediated Id protein interactions an appealing therapeutic target. We have used the dominant interfering HLH dimerization mutant 13I to model the impact of Id inhibition in two human neuroblastoma cell lines: LA-N-5, similar to immature neuroblasts, and SH-EP, resembling more immature precursor cells. We have validated 13I as an Id inhibitor by showing that it selectively binds to Ids, impairs complex formation with RB, and relieves repression of E protein-activated transcription. Id inactivation by 13I enhances LA-N-5 neural features and causes SH-EP cells to acquire neuronal morphology, express neuronal proteins such as N-CAM and NF-160, proliferate more slowly, and become responsive to retinoic acid. Concomitantly, 13I augments the cell-cycle inhibitor p27 Kip1 and reduces the angiogenic factor vascular endothelial growth factor. These effects are Id specific, being counteracted by Id overexpression. Furthermore, 13I strongly impairs tumorigenic properties in agar colony formation and cell invasion assays. Targeting Id dimerization may therefore be effective for triggering differentiation and restraining neuroblastoma cell tumorigenicity.

show abstract

Section: Discussionmentioning

confidence: 98%

Section: Introductionmentioning

confidence: 99%

Targeting Id protein interactions by an engineered HLH domain induces human neuroblastoma cell differentiation

et al. 2009

View full text Add to dashboard Cite

show abstract

“…[56][57][58] Conversely, Id knockdown is associated in many cell types with increased expression of CDKIs. 53,56,[59][60][61][62][63] Recently we reported that E47 directly activates p57…”

Section: Discussionmentioning

confidence: 99%

Id3 upregulates BrdU incorporation associated with a DNA damage response, not replication, in human pancreatic β-cells

Lee

Hao

Levine

et al. 2011

Islets

View full text Add to dashboard Cite

“…Using a wounding model as an inducer of cell cycle entry for human dermal fibroblasts, when Id3 was silenced, the expected down-regulation of p27 did not occurred, suggesting that transcription repression of p27 was regulated by Id3. It was also found that both G1 phase progression and G1/S transition were blocked by Id3 depletion (14).…”

Section: Effect Of Id3 Suppression On the Sensitivity Of Cancer Cellsmentioning

confidence: 89%

“…These inhibitors sequestrate CDKs and therefore stop them from phosphorylating pRB, hence having an indirect anti-proliferation effect (13). Id3 specifically regulates P27 through an ETS domain factor called ELK1 (14). Id1 and Id3 have also been identified as downstream targets of MYC (15).…”

Section: Introductionmentioning

confidence: 99%

Inhibition of tumourigenicity of small cell lung cancer cells by suppressing Id3 expression

Kamalian

Forootan²,

Bao³

et al. 2010

Int J Oncol

View full text Add to dashboard Cite

Abstract.Id3 is over-expressed in small cell lung cancer (SCLC). To test whether the tumourigenicity of SCLC cells can be inhibited by suppressing Id3 expression, we transfected siRNA into SCLC cell line GLC-19 and established two sublines (G-Id3-1 and G-Id3-7) which expressed only 30% of the level of Id3 measured in control transfectants. Suppression of Id3 expression in both G-Id3-1 and G-Id3-7 cells produced significant reductions in proliferation rates and in numbers of colonies formed in soft agar assay. When G-Id3-1, G-Id3-7 and the control transfectants were inoculated subcutaneously into 3 groups (8 each) of nude mice, respectively, all (100%) inoculated animals produced tumours. Although there was no difference in tumour incidents amongst the 3 groups, significant reductions were observed in both size and weight of tumours produced by either G-Id3-1 or G-Id3-7 cells. While the final average volume of tumours produced in control group was 1012.1±394 mm 3 , it was significantly reduced (p<0.001, p<0.01) by 2.1-and 2.9-fold to 475.7±167 mm 3 and 354.3±218 mm 3 in groups inoculated with G-Id3-1 and G-Id3-7 cells, respectively. Similar differences were also observed in average weight of tumours. Upon induction of apoptosis by cytotoxin camptothecin, the percentages of apoptotic cells in G-Id3-1 and G-Id3-7 were, respectively >2.4-fold higher than that in control. The results in this study suggest that highly expressed Id3 in SCLC cells may be an important therapeutic target for tumour suppression.

show abstract

Id3 is a novel regulator of p27kip1 mRNA in early G1 phase and is required for cell-cycle progression

Cited by 30 publications

References 50 publications

Targeting Id protein interactions by an engineered HLH domain induces human neuroblastoma cell differentiation

Targeting Id protein interactions by an engineered HLH domain induces human neuroblastoma cell differentiation

Id3 upregulates BrdU incorporation associated with a DNA damage response, not replication, in human pancreatic β-cells

Inhibition of tumourigenicity of small cell lung cancer cells by suppressing Id3 expression

Contact Info

Product

Resources

About