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Nuclear deformability and telomere dynamics are regulated by cell geometric constraints. | LitMetric

Nuclear deformability and telomere dynamics are regulated by cell geometric constraints.

Proc Natl Acad Sci U S A

Mechanobiology Institute, National University of Singapore, Singapore 117411; Department of Biological Sciences, National University of Singapore, Singapore 117543; Institute of Molecular Oncology, Italian Foundation for Cancer Research, 20139 Milan, Italy

Published: January 2016

AI Article Synopsis

  • Forces from the cytoskeleton are linked to the nucleus and influence its shape and dynamics, with the study revealing that different cell shapes affect nuclear deformability.
  • The research showed that cells with less organized cytoskeletal fibers (constrained and isotropic) have more flexible nuclei compared to elongated cells, and this flexibility changes based on cytoskeletal manipulation and lamin A/C protein levels.
  • Additionally, it was found that the geometry of the cell influences the movement of chromatin, indicating that active cytoskeletal forces and the structural support from the nucleoskeleton work together to manage chromatin dynamics, which plays a significant role in gene regulation and cell behavior.

Article Abstract

Forces generated by the cytoskeleton can be transmitted to the nucleus and chromatin via physical links on the nuclear envelope and the lamin meshwork. Although the role of these active forces in modulating prestressed nuclear morphology has been well studied, the effect on nuclear and chromatin dynamics remains to be explored. To understand the regulation of nuclear deformability by these active forces, we created different cytoskeletal states in mouse fibroblasts using micropatterned substrates. We observed that constrained and isotropic cells, which lack long actin stress fibers, have more deformable nuclei than elongated and polarized cells. This nuclear deformability altered in response to actin, myosin, formin perturbations, or a transcriptional down-regulation of lamin A/C levels in the constrained and isotropic geometry. Furthermore, to probe the effect of active cytoskeletal forces on chromatin dynamics, we tracked the spatiotemporal dynamics of heterochromatin foci and telomeres. We observed increased dynamics and decreased correlation of the heterochromatin foci and telomere trajectories in constrained and isotropic cell geometry. The observed enhanced dynamics upon treatment with actin depolymerizing reagents in elongated and polarized geometry were regained once the reagent was washed off, suggesting an inherent structural memory in chromatin organization. We conclude that active forces from the cytoskeleton and rigidity from lamin A/C nucleoskeleton can together regulate nuclear and chromatin dynamics. Because chromatin remodeling is a necessary step in transcription control and its memory, genome integrity, and cellular deformability during migration, our results highlight the importance of cell geometric constraints as critical regulators in cell behavior.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4711833PMC
http://dx.doi.org/10.1073/pnas.1513189113DOI Listing

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