The fate of extra centrosomes in newly formed tetraploid cells: should I stay, or should I go?

Bloomfield, Mathew; Cimini, Daniela

doi:10.3389/fcell.2023.1210983

Front. Cell Dev. Biol.

2023

DOI: 10.3389/fcell.2023.1210983

|Get access via publisher |Summarize |Cite

|

Sign up to set email alerts

The fate of extra centrosomes in newly formed tetraploid cells: should I stay, or should I go?

Mathew Bloomfield

¹

,

Daniela Cimini

²

Abstract: An increase in centrosome number is commonly observed in cancer cells, but the role centrosome amplification plays along with how and when it occurs during cancer development is unclear. One mechanism for generating cancer cells with extra centrosomes is whole genome doubling (WGD), an event that occurs in over 30% of human cancers and is associated with poor survival. Newly formed tetraploid cells can acquire extra centrosomes during WGD, and a generally accepted model proposes that centrosome amplification i… Show more

Help me understand this report

Cited by 11 publications

(3 citation statements)

References 226 publications

Supporting

1

Mentioning

2

Contrasting

0

Unclassified

0

Order By: Relevance

“…We have demonstrated using 1 day treatment with AZD2811 to produced tetraploid cells that these can form viable colonies and have long term proliferative potential as diploid and tetraploid colonies. This supports the detailed fate studies of enforced tetraploid cells demonstrating reduced long term proliferative potential but stable tetraploid progeny is a potential outcome [37,45], and the genomics data demonstrating that tetraploidy can be tolerated by tumour cells [9], and In contrast to tetraploid cells, cells that undergo >2 failed cytokinesis and accumulate >8n DNA content and a corresponding increase in centrosome number have lost colony forming ability and long term proliferative potential. Indeed, in many of these experiments, exposure to AURKBi for the initial 2-3 days was sufficient to drive continued endomitotic cycles of failed cytokinesis.…”

Section: Discussionsupporting

confidence: 73%

“…It also appears that once cells have failed cytokinesis twice, they will continue to undergo further endomitotic cycles with failed cytokinesis in the absence of AURKBi. The increased centrosomes numbers and their ability to form individual mitotic spindles at each mitosis, rather than cluster to form pseudo-bipolar spindles that have been shown to enable relatively normal mitosis although commonly leading to cell death in subsequent mitosis [36,43,45]. The loss requirement for continued AURKBi treatment after 2-3 days is likely to be due to an inability of the mitotic, multipolar (>8 poles), hyper-polyploid (>8n DNA) cells to satisfy the spindle assembly checkpoint and undergo mitotic slippage without cytokinesis.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Aurora B inhibition promotes a hyper-polyploid state and continued endomitotic cycles in RB and p53 defective cells

Vora

¹

,

Andrew

²

,

Kumar

³

et al. 2024

Preprint

1

0

Get access via publisher Add to dashboard Cite

Exaggerated anticipatory anxiety is common in social anxiety disorder (SAD). Neuroimaging studies have revealed altered neural activity in response to social stimuli in SAD, but fewer studies have examined neural activity during anticipation of feared social stimuli in SAD. The current study examined the time course and magnitude of activity in threat processing brain regions during speech anticipation in socially anxious individuals and healthy controls (HC). Method Participants (SAD n = 58; HC n = 16) underwent functional magnetic resonance imaging (fMRI) during which they completed a 90s control anticipation task and 90s speech anticipation task.

show abstract

“…We have demonstrated using 1 day treatment with AZD2811 to produced tetraploid cells that these can form viable colonies and have long term proliferative potential as diploid and tetraploid colonies. This supports the detailed fate studies of enforced tetraploid cells demonstrating reduced long term proliferative potential but stable tetraploid progeny is a potential outcome [37,45], and the genomics data demonstrating that tetraploidy can be tolerated by tumour cells [9], and In contrast to tetraploid cells, cells that undergo >2 failed cytokinesis and accumulate >8n DNA content and a corresponding increase in centrosome number have lost colony forming ability and long term proliferative potential. Indeed, in many of these experiments, exposure to AURKBi for the initial 2-3 days was sufficient to drive continued endomitotic cycles of failed cytokinesis.…”

Section: Discussionsupporting

confidence: 73%

“…It also appears that once cells have failed cytokinesis twice, they will continue to undergo further endomitotic cycles with failed cytokinesis in the absence of AURKBi. The increased centrosomes numbers and their ability to form individual mitotic spindles at each mitosis, rather than cluster to form pseudo-bipolar spindles that have been shown to enable relatively normal mitosis although commonly leading to cell death in subsequent mitosis [36,43,45]. The loss requirement for continued AURKBi treatment after 2-3 days is likely to be due to an inability of the mitotic, multipolar (>8 poles), hyper-polyploid (>8n DNA) cells to satisfy the spindle assembly checkpoint and undergo mitotic slippage without cytokinesis.…”

Section: Discussionmentioning

confidence: 99%

Aurora B inhibition promotes a hyper-polyploid state and continued endomitotic cycles in RB and p53 defective cells

Vora

¹

,

Andrew

²

,

Kumar

³

et al. 2024

Preprint

1

0

Get access via publisher Add to dashboard Cite

Exaggerated anticipatory anxiety is common in social anxiety disorder (SAD). Neuroimaging studies have revealed altered neural activity in response to social stimuli in SAD, but fewer studies have examined neural activity during anticipation of feared social stimuli in SAD. The current study examined the time course and magnitude of activity in threat processing brain regions during speech anticipation in socially anxious individuals and healthy controls (HC). Method Participants (SAD n = 58; HC n = 16) underwent functional magnetic resonance imaging (fMRI) during which they completed a 90s control anticipation task and 90s speech anticipation task.

show abstract

“…Cells with too many centrioles might divide abnormally and/or undergo cell cycle arrest, leading to reduced proliferation or even cell death. Thus, centriole numbers appear to be maintained at an equilibrium by a balance of centriole overproduction and negative selection acting on cells with extra centrioles 26,33 . However, most studies are limited to investigating short-term effects and transient centriole number alterations.…”

Section: Introductionmentioning

confidence: 99%

Adaptation of human cell populations to different levels of centriole amplification

Peneda

¹

,

Bank

²

,

Louro

³

et al. 2024

Preprint

0

Get access via publisher Add to dashboard Cite

Exaggerated anticipatory anxiety is common in social anxiety disorder (SAD). Neuroimaging studies have revealed altered neural activity in response to social stimuli in SAD, but fewer studies have examined neural activity during anticipation of feared social stimuli in SAD. The current study examined the time course and magnitude of activity in threat processing brain regions during speech anticipation in socially anxious individuals and healthy controls (HC). Method Participants (SAD n = 58; HC n = 16) underwent functional magnetic resonance imaging (fMRI) during which they completed a 90s control anticipation task and 90s speech anticipation task.

show abstract

Mechanisms of whole-genome doubling in cancer evolution

McKenney

¹

,

Regot

²

2026

Trends in Cancer

1

0

Get access via publisher Add to dashboard Cite

Exaggerated anticipatory anxiety is common in social anxiety disorder (SAD). Neuroimaging studies have revealed altered neural activity in response to social stimuli in SAD, but fewer studies have examined neural activity during anticipation of feared social stimuli in SAD. The current study examined the time course and magnitude of activity in threat processing brain regions during speech anticipation in socially anxious individuals and healthy controls (HC). Method Participants (SAD n = 58; HC n = 16) underwent functional magnetic resonance imaging (fMRI) during which they completed a 90s control anticipation task and 90s speech anticipation task.

Scite is an AI-powered platform that helps researchers discover and evaluate scientific literature through Smart Citations, showing whether studies support or contradict a claim. Now part of Research Solutions, Scite has indexed 1.6B+ citations, partners with 30+ publishers, and serves 2M users worldwide.

Contact Info

customersupport@researchsolutions.com

10624 S. Eastern Ave., Ste. A-614

Henderson, NV 89052, USA