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Epitranscriptomics & Cancer Adaptation : A.David

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Our research work focuses on the contribution of post-transcriptional mechanisms on cancer cell adaptation, in particular RNA epigenetic & translational control.

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Added by eric_julien
Group name EquipeEJ
Item Type Journal Article
Title The transcription factor E4F1 coordinates CHK1-dependent checkpoint and mitochondrial functions
Creator Rodier et al.
Author Geneviève Rodier
Author Olivier Kirsh
Author Martín Baraibar
Author Thibault Houlès
Author Matthieu Lacroix
Author Hélène Delpech
Author Elodie Hatchi
Author Stéphanie Arnould
Author Dany Severac
Author Emeric Dubois
Author Julie Caramel
Author Eric Julien
Author Bertrand Friguet
Author Laurent Le Cam
Author Claude Sardet
Abstract Recent data support the notion that a group of key transcriptional regulators involved in tumorigenesis, including MYC, p53, E2F1, and BMI1, share an intriguing capacity to simultaneously regulate metabolism and cell cycle. Here, we show that another factor, the multifunctional protein E4F1, directly controls genes involved in mitochondria functions and cell-cycle checkpoints, including Chek1, a major component of the DNA damage response. Coordination of these cellular functions by E4F1 appears essential for the survival of p53-deficient transformed cells. Acute inactivation of E4F1 in these cells results in CHK1-dependent checkpoint deficiency and multiple mitochondrial dysfunctions that lead to increased ROS production, energy stress, and inhibition of de novo pyrimidine synthesis. This deadly cocktail leads to the accumulation of uncompensated oxidative damage to proteins and extensive DNA damage, ending in cell death. This supports the rationale of therapeutic strategies simultaneously targeting mitochondria and CHK1 for selective killing of p53-deficient cancer cells.
Publication Cell Reports
Volume 11
Issue 2
Pages 220-233
Date Apr 14, 2015
Journal Abbr Cell Rep
Language eng
DOI 10.1016/j.celrep.2015.03.024
ISSN 2211-1247
Library Catalog PubMed
Extra PMID: 25843721
Tags Animals, Cell Survival, Checkpoint Kinase 1, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, Humans, Mice, Mouse Embryonic Stem Cells, Neoplasms, original, Protein Kinases, Pyrimidines, Stress, Physiological, Transcription Factors, Tumor Suppressor Protein p53
Date Added 2018/09/26 - 15:46:19
Date Modified 2019/05/28 - 13:57:51


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Located in the Parc Euromédecine, the Institut de Recherche en Cancérologie de Montpellier (U1194) is located on the Val d'Aurelle Campus (ICM, Institut régional du Cancer Montpellier/ Val d'Aurelle).

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