Mitotic progression, arrest, exit or death relies on centromere structural integrity, rather than de novo transcription

Novais-Cruz, Marco; Abad, Maria Alba; IJcken, Wilfred F. J. van; Galjart, Niels; Jeyaprakash, A. Arockia; Maiato, Hélder; Ferrás, Cristina

doi:10.7554/elife.36898

Cited by 18 publications

(28 citation statements)

References 75 publications

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“…Retention of elongating RNAPII at centromeres has been observed in metaphase chromosomes of human, fly and frog cells (Blower, 2016;Chan et al, 2012;Molina et al, 2016;Rosic et al, 2014), and several roles for mitotic centromere transcription have been proposed (Blower, 2016;Chan et al, 2012;Liu et al, 2015). However, a recent study has questioned the role of mitotic transcription for accurate chromosome segregation (Novais-Cruz et al, 2018). Our results demonstrate that elongating RNAPII is passively retained at centromeres in mitosis as a byproduct of cohesin retention.…”

Section: Mitotic Centromere Transcriptionmentioning

confidence: 47%

“…Importantly, this nascent-RNA signal on mitotic chromosomes in WAPL-AID cells was eliminated by treatment with triptolide, an inhibitor of RNAPII transcription initiation (Titov et al, 2011) (Fig. 2F-G), likely through RNAPII degradation following extended triptolide treatment (Novais-Cruz et al, 2018).…”

Section: Aid Cells Was Dependent On the Presence Of Cohesin As Co-depmentioning

confidence: 98%

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Cohesin removal reprograms gene expression upon mitotic entry

Perea-Resa

Bury

Cheeseman

et al. 2019

Preprint

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Highlights• Mitotic centromere transcription requires cohesin • Cohesin removal releases elongating RNA Pol II and nascent RNA from chromatin • The prophase pathway reprograms gene expression during mitosis SummaryEntering mitosis, the genome is restructured to facilitate chromosome segregation, accompanied by dramatic changes in gene expression. However, the mechanisms that underlie mitotic transcriptional regulation are unclear. In contrast to transcribed genes, centromere regions retain transcriptionally active RNA Polymerase II (RNAPII) in mitosis. Here, we demonstrate that chromatin-bound cohesin is sufficient to retain RNAPII at centromeres while WAPL-mediated removal of cohesin during prophase is required for RNAPII dissociation from chromosome arms. Failure to remove cohesin from chromosome arms results in a failure to release elongating RNAPII and nascent transcripts from mitotic chromosomes and dramatically alters gene expression. We propose that prophase cohesin removal is the key step in reprogramming gene expression as cells transition from G2 to mitosis, and is temporally coupled with chromosome condensation to coordinate chromosome segregation with changes in gene expression.

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Section: Mitotic Centromere Transcriptionmentioning

confidence: 47%

Section: Aid Cells Was Dependent On the Presence Of Cohesin As Co-depmentioning

confidence: 98%

Cohesin removal reprograms gene expression upon mitotic entry

Perea-Resa

Bury

Cheeseman

et al. 2019

Preprint

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“…Several studies show that inhibited transcription or splicing in mitosis or degradation of centromeric RNAs results in reduced CENP-C intensity on the kinetochore, anaphase extension, and chromosome segregation errors [22,[73][74][75]. However, a recent study suggested that transcription in mitosis was not required for mitotic progression in human cells [24]. The importance of transcripts in centromeric DNA has been reported for many species, including humans [75], maize [21,76], budding yeast [77], fission yeast [78], and flies [72].…”

Section: The Role Of Ncrnas In the Assembly And Function Of Kinetochoresmentioning

confidence: 99%

“…Since centromeric RNAs are transcribed and accumulated during mitosis [69,80], inhibiting transcription in mitosis affects kinetochore function [69,70]. However, a recent study suggested that transcription in mitosis was not required for mitotic progression [24]. The authors reported that DNA-intercalating drugs (α-amanitin) reduce localization of aurora-B in the centromere without reducing the amount of centromeric RNAs [24].…”

Section: The Role Of Ncrnas In the Assembly And Function Of Kinetochoresmentioning

confidence: 99%

“…The function of ncRNAs transcribed from the centromere region (centromeric RNAs) at the kinetochore has been studied since 2004 and 2007 with maize and human cells, respectively [21,22] Centromeric RNAs are associated with critical kinetochore proteins, recruiting and regulating them at the kinetochore [23]. At present, distinguishing the function of centromeric transcripts and transcription itself in kinetochore formation comes into question [24]. Compared with centrosomes and kinetochores, the function of ncRNAs on the mitotic spindle is poorly understood.…”

Section: Introductionmentioning

confidence: 99%

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The Emerging Role of ncRNAs and RNA-Binding Proteins in Mitotic Apparatus Formation

Ito

Watanabe

Kitagawa

2020

ncRNA

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Mounting experimental evidence shows that non-coding RNAs (ncRNAs) serve a wide variety of biological functions. Recent studies suggest that a part of ncRNAs are critically important for supporting the structure of subcellular architectures. Here, we summarize the current literature demonstrating the role of ncRNAs and RNA-binding proteins in regulating the assembly of mitotic apparatus, especially focusing on centrosomes, kinetochores, and mitotic spindles.

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An emerging role of transcription in chromosome segregation: Ongoing centromeric transcription maintains centromeric cohesion

Chen

Liu

2021

BioEssays

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Non-coding centromeres, which dictate kinetochore formation for proper chromosome segregation, are extremely divergent in DNA sequences across species but are under active transcription carried out by RNA polymerase (RNAP) II. The RNAP IImediated centromeric transcription has been shown to facilitate the deposition of the centromere protein A (CENP-A) to centromeres, establishing a conserved and critical role of centromeric transcription in centromere maintenance. Our recent work revealed another role of centromeric transcription in chromosome segregation: maintaining centromeric cohesion during mitosis. Interestingly, this role appears to be fulfilled through ongoing centromeric transcription rather than centromeric transcripts.In addition, we found that centromeric transcription may not require some of the traditional transcription initiation factors, suggestive of "uniqueness" in its regulation. In this review, we discuss the novel role and regulation of centromeric transcription as well as the potential underlying mechanisms.

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Mitotic progression, arrest, exit or death relies on centromere structural integrity, rather than de novo transcription

Cited by 18 publications

References 75 publications

Cohesin removal reprograms gene expression upon mitotic entry

Cohesin removal reprograms gene expression upon mitotic entry

The Emerging Role of ncRNAs and RNA-Binding Proteins in Mitotic Apparatus Formation

An emerging role of transcription in chromosome segregation: Ongoing centromeric transcription maintains centromeric cohesion

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