The transcription factor ERG recruits CCR4–NOT to control mRNA decay and mitotic progression

Rambout, Xavier; Detiffe, Cécile; Bruyr, Jonathan; Mariavelle, Emeline; Cherkaoui, Majid; Brohée, Sylvain; Demoitié, Pauline; Lebrun, Marielle; Soin, Romuald; Lesage, Bart; Guedri, Katia; Beullens, Monique; Bollen, Mathieu; Farazi, Thalia A.; Kettmann, Richard; Struman, Ingrid; Hill, David E.; Vidal, Marc; Kruys, Véronique; Simonis, Nicolas; Twizere, Jean-Claude; Dequiedt, Samuel

doi:10.1038/nsmb.3243

Cited by 35 publications

(37 citation statements)

References 61 publications

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“…CNOT2 encodes a subunit of the multi-component CCR4-NOT complex, involved in gene expression regulating mRNA synthesis, degradation, splicing, transport, and localization (Jeong, Kwon, Jeong, Sohn, & Kim, 2017;Rambout et al, 2016). According to its wide biological functions, it is ubiquitously expressed (https://www.genecards.org),…”

Section: Resultsmentioning

confidence: 99%

A heterozygous, intragenic deletion of CNOT2 recapitulates the phenotype of 12q15 deletion syndrome

Alesi

Loddo

Calì

et al. 2019

American J of Med Genetics Pt A

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Only a few individuals with 12q15 deletion have been described, presenting with a disorder characterized by learning disability, developmental delay, nasal speech, and hypothyroidism. The smallest region of overlap for this syndrome was included in a genomic segment spanning CNOT2, KCNMB4, and PTPRB genes. We report on an additional patient harboring a 12q15 microdeletion encompassing only part of CNOT2 gene, presenting with a spectrum of clinical features overlapping the 12q15 deletion syndrome phenotype. We propose CNOT2 as the phenocritical gene for 12q15 deletion syndrome and its haploinsufficiency being associated with an autosomal dominant disorder, presenting with developmental delay, hypotonia, feeding problems, learning difficulties, nasal speech, skeletal anomalies, and facial dysmorphisms. K E Y W O R D S 12q15, 12q deletion syndrome, CNOT2

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Section: Resultsmentioning

confidence: 99%

A heterozygous, intragenic deletion of CNOT2 recapitulates the phenotype of 12q15 deletion syndrome

Alesi

Loddo

Calì

et al. 2019

American J of Med Genetics Pt A

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“…Indirect effects of CNOT-mediated transcriptional repression could involve the association or regulation of transcription factors. Examples for such a mechanism are interactions of CNOT1 with estrogen receptor α, CNOT9 binding to c-Myb 20 and CNOT2 interaction with ERG 60 .…”

Section: Discussionmentioning

confidence: 99%

The CCR4-NOT complex contributes to repression of Major Histocompatibility Complex class II transcription

Rodríguez-Gil

Ritter

Saul

et al. 2017

Sci Rep

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The multi-subunit CCR4 (carbon catabolite repressor 4)-NOT (Negative on TATA) complex serves as a central coordinator of all different steps of eukaryotic gene expression. Here we performed a systematic and comparative analysis of cells where the CCR4-NOT subunits CNOT1, CNOT2 or CNOT3 were individually downregulated using doxycycline-inducible shRNAs. Microarray experiments showed that downregulation of either CNOT subunit resulted in elevated expression of major histocompatibility complex class II (MHC II) genes which are found in a gene cluster on chromosome 6. Increased expression of MHC II genes after knock-down or knock-out of either CNOT subunit was seen in a variety of cell systems and also in naïve macrophages from CNOT3 conditional knock-out mice. CNOT2-mediated repression of MHC II genes occurred also in the absence of the master regulator class II transactivator (CIITA) and did not cause detectable changes of the chromatin structure at the chromosomal MHC II locus. CNOT2 downregulation resulted in an increased de novo transcription of mRNAs whereas tethering of CNOT2 to a regulatory region governing MHC II expression resulted in diminished transcription. These results expand the known repertoire of CCR4-NOT members for immune regulation and identify CNOT proteins as a novel group of corepressors restricting class II expression.

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“…Although a new transcription-independent role of PER cannot be excluded, different mechanisms have been revealed that link transcription with the control of mRNA polyadenylation and stability (48,49). Notably, interactions between the transcription machinery and the CCR4-NOT complex indicate that mRNA deadenylation can be regulated at the transcriptional level (50)(51)(52)(53), raising the possibility that PER might interfere with POP2 activity through its role as a transcriptional repressor. For example, CBP/p300 acetylates CAF1 to promote its activity (52).…”

Section: Discussionmentioning

confidence: 99%

PERIOD-controlled deadenylation of the timeless transcript in the Drosophila circadian clock

Grima

Papin

Martin

et al. 2019

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

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The Drosophila circadian oscillator relies on a negative transcriptional feedback loop, in which the PERIOD (PER) and TIMELESS (TIM) proteins repress the expression of their own gene by inhibiting the activity of the CLOCK (CLK) and CYCLE (CYC) transcription factors. A series of posttranslational modifications contribute to the oscillations of the PER and TIM proteins but few posttranscriptional mechanisms have been described that affect mRNA stability. Here we report that down-regulation of the POP2 deadenylase, a key component of the CCR4-NOT deadenylation complex, alters behavioral rhythms. Downregulating POP2 specifically increases TIM protein and tim mRNA but not tim pre-mRNA, supporting a posttranscriptional role. Indeed, reduced POP2 levels induce a lengthening of tim mRNA poly(A) tail. Surprisingly, such effects are lost in per 0 mutants, supporting a PERdependent inhibition of tim mRNA deadenylation by POP2. We report a deadenylation mechanism that controls the oscillations of a core clock gene transcript. circadian rhythms | clock genes | mRNA poly(A) tail | CAF1/POP2 | CCR4-NOT complex

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The transcription factor ERG recruits CCR4–NOT to control mRNA decay and mitotic progression

Cited by 35 publications

References 61 publications

A heterozygous, intragenic deletion of CNOT2 recapitulates the phenotype of 12q15 deletion syndrome

A heterozygous, intragenic deletion of CNOT2 recapitulates the phenotype of 12q15 deletion syndrome

The CCR4-NOT complex contributes to repression of Major Histocompatibility Complex class II transcription

PERIOD-controlled deadenylation of the timeless transcript in the Drosophila circadian clock

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