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Metabolically intact nuclei are fluidized by the activity of the chromatin remodeling motor BRG1

  • Fitzroy J. Byfield
  • , Behnaz Eftekhari
  • , Kaeli Kaymak-Loveless
  • , Kalpana Mandal
  • , David Li
  • , Rebecca G. Wells
  • , Wenjun Chen
  • , Jasna Brujic
  • , Giulia Bergamaschi
  • , Gijs J.L. Wuite
  • , Alison E. Patteson
  • , Paul A. Janmey
  • University of Pennsylvania
  • Vrije Universiteit Amsterdam

Zinātniskās darbības rezultāts: Devums žurnālamZinātniskais raksts (žurnālā)koleģiāli recenzēts

6 Atsauces (Scopus)

Kopsavilkums

The structure and dynamics of the nucleus regulate cellular functions, with shape changes impacting cell motility. Although the nucleus is generally seen as the stiffest organelle in the cell, cells can nevertheless deform the nucleus to large strains by small mechanical stresses. Here, we show that the mechanical response of the cell nucleus exhibits active fluidization that is driven by the BRG1 motor of the SWI/SNF/BAF chromatin remodeling complex. Atomic force microscopy measurements show that the nucleus alters stiffness in response to the cell substrate stiffness, which is retained after the nucleus is isolated, and that the work of nuclear compression is mostly dissipated rather than elastically stored. Inhibiting BRG1 stiffens the nucleus and eliminates dissipation and nuclear remodeling both in isolated nuclei and in intact cells. These findings uncover a novel role of the BRG1 motor in nuclear mechanics, advancing our understanding of cell motility mechanisms.

OriģinālvalodaAngļu
Lapas (no-līdz)494-507
Lapu skaits14
ŽurnālsBiophysical Journal
Sējums124
Izdevuma numurs3
DOIs
Publikācijas statussPublicēts - 4 febr. 2025

OECD Zinātnes nozare

  • 1.3 Fizika un astronomija

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