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research article

A nuclear jamming transition in vertebrate organogenesis

Kim, Sangwoo  
•
Amini, Rana
•
Yen, Shuo-Ting
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August 12, 2024
Nature Materials

Jamming of cell collectives and associated rigidity transitions have been shown to play a key role in tissue dynamics, structure and morphogenesis. Cellular jamming is controlled by cellular density and the mechanics of cell-cell contacts. However, the contribution of subcellular organelles to the physical state of the emergent tissue is unclear. Here we report a nuclear jamming transition in zebrafish retina and brain tissues, where physical interactions between highly packed nuclei restrict cellular movements and control tissue mechanics and architecture. Computational modelling suggests that the nuclear volume fraction and anisotropy of cells control the emerging tissue physical state. Analysis of tissue architecture, mechanics and nuclear movements during eye development show that retina tissues undergo a nuclear jamming transition as they form, with increasing nuclear packing leading to more ordered cellular arrangements, reminiscent of the crystalline cellular packings in the functional adult eye. Our results reveal an important role of the cell nucleus in tissue mechanics and architecture. Developing zebrafish retina and brain tissues undergo a nuclear jamming transition that induces crystalline-like cellular ordering, with the emergent tissue stiffness controlled by nuclear mechanics.

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Type
research article
DOI
10.1038/s41563-024-01972-3
Web of Science ID

WOS:001289962000001

PubMed ID

39134649

Author(s)
Kim, Sangwoo  

École Polytechnique Fédérale de Lausanne

Amini, Rana

Technische Universitat Dresden

Yen, Shuo-Ting

Technische Universitat Dresden

Pospisil, Petr

Technische Universitat Dresden

Boutillon, Arthur

Technische Universitat Dresden

Deniz, Ilker Ali

Technische Universitat Dresden

Campas, Otger

Technische Universitat Dresden

Date Issued

2024-08-12

Publisher

NATURE PORTFOLIO

Published in
Nature Materials
Volume

23

Issue

11

Subjects

IN-VIVO

•

CELL

•

MORPHOGENESIS

•

MECHANICS

•

PROGENITORS

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Science & Technology

•

Physical Sciences

•

Technology

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
MESOBIO  
FunderFunding(s)Grant NumberGrant URL

U.S. Department of Health & Human Services | NIH | Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD)

R01HD095797

United States Department of Health & Human Services

German Research Foundation (DFG)

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Available on Infoscience
February 1, 2025
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/246196
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