Dataset Information

Nuclear envelope deformation controls cell cycle progression in response to mechanical force.

ABSTRACT: The shape of the cell nucleus can vary considerably during developmental and pathological processes; however, the impact of nuclear morphology on cell behavior is not known. Here, we observed that the nuclear envelope flattens as cells transit from G1 to S phase and inhibition of myosin II prevents nuclear flattening and impedes progression to S phase. Strikingly, we show that applying compressive force on the nucleus in the absence of myosin II-mediated tension is sufficient to restore G1 to S transition. Using a combination of tools to manipulate nuclear morphology, we observed that nuclear flattening activates a subset of transcription factors, including TEAD and AP1, leading to transcriptional induction of target genes that promote G1 to S transition. In addition, we found that nuclear flattening mediates TEAD and AP1 activation in response to ROCK-generated contractility or cell spreading. Our results reveal that the nuclear envelope can operate as a mechanical sensor whose deformation controls cell growth in response to tension.

SUBMITTER: Aureille J

PROVIDER: S-EPMC6726894 | biostudies-literature | 2019 Sep

REPOSITORIES: biostudies-literature

ACCESS DATA

Publications

Nuclear envelope deformation controls cell cycle progression in response to mechanical force.

Aureille Julien J Buffière-Ribot Valentin V Harvey Ben E BE Boyault Cyril C Pernet Lydia L Andersen Tomas T Bacola Gregory G Balland Martial M Fraboulet Sandrine S Van Landeghem Laurianne L Guilluy Christophe C

EMBO reports 20190801 9

The shape of the cell nucleus can vary considerably during developmental and pathological processes; however, the impact of nuclear morphology on cell behavior is not known. Here, we observed that the nuclear envelope flattens as cells transit from G1 to S phase and inhibition of myosin II prevents nuclear flattening and impedes progression to S phase. Strikingly, we show that applying compressive force on the nucleus in the absence of myosin II-mediated tension is sufficient to restore G1 to S ...[more]

PMID: 31368207

Dataset Information

Nuclear envelope deformation controls cell cycle progression in response to mechanical force.

Publications

Nuclear envelope deformation controls cell cycle progression in response to mechanical force.

Similar Datasets

OmicsDI is part of the ELIXIR infrastructure

Similar Datasets

ESCRT-III controls nuclear envelope deformation induced by progerin.
| S-EPMC7606583 | biostudies-literature

Nuclear Deformation in Response to Mechanical Confinement is Cell Type Dependent.
| S-EPMC6563141 | biostudies-literature

KDP-1 is a nuclear envelope KASH protein required for cell-cycle progression.
| S-EPMC2724607 | biostudies-literature

Mitochondrial Deformation During the Cardiac Mechanical Cycle.
| S-EPMC6312496 | biostudies-literature

Kv1.3 Controls Mitochondrial Dynamics during Cell Cycle Progression.
| S-EPMC8431373 | biostudies-literature

ESCRT-III controls nuclear envelope reformation.
| S-EPMC4471131 | biostudies-literature

ATR mediates a checkpoint at the nuclear envelope in response to mechanical stress.
| S-EPMC4121522 | biostudies-literature

Simian virus 40 induces lamin A/C fluctuations and nuclear envelope deformation during cell entry.
| S-EPMC3260569 | biostudies-literature

Force-specific activation of Smad1/5 regulates vascular endothelial cell cycle progression in response to disturbed flow.
| S-EPMC3356658 | biostudies-literature

Perinuclear force regulates SUN2 dynamics and distribution on the nuclear envelope for proper nuclear mechanotransduction
2022-10-12 | GSE214854 | GEO