4.5 Article

Polarized interfacial tension induces collective migration of cells, as a cluster, in a 3D tissue

期刊

BIOPHYSICAL JOURNAL
卷 121, 期 10, 页码 1856-1867

出版社

CELL PRESS
DOI: 10.1016/j.bpj.2022.04.018

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资金

  1. Japan Science and Technology Agency (JST), CREST [JPMJCR 1921]
  2. Japan Agency for Medical Research and Development (AMED) [21bm0704065h0001]
  3. Japan Society for the Promotion of Science (JSPS), KAKENHI [21H01209, 20K20958, 20K03871, 18H01135]
  4. Global Station for Soft Matter at Hokkaido University
  5. Research Program of Five-star Alliance in NJRC Mater. Dev.
  6. Uehara Memorial Foundation, Japan
  7. NOVARTIS Foundation (Japan) for the Promotion of Science
  8. Brain Science Foundation
  9. World Premier International Research Center Initiative (WPI), Ministry of Education, Culture, Sports, Science and Technology (MEXT), Japan
  10. Grants-in-Aid for Scientific Research [21H01209, 20K20958, 20K03871] Funding Source: KAKEN

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This study investigates the mechanisms of collective cell migration in 3D tissues. Numerical simulations using a 3D vertex model reveal that polarized interfacial tension between cells enables cluster migration without cell rearrangement. The strength of polarity, adhesion, and noise determines different migratory modes, including single cell migration, cluster migration, and string-like alignment observed in embryogenesis and cancer invasion.
In embryogenesis and cancer invasion, cells collectively migrate as a cluster in 3D tissues. Many studies have elucidated mechanisms of either individual or collective cell migration on 2D substrates; however, it remains unclear how cells collectively migrate as a cluster through 3D tissues. To address this issue, we considered the interfacial tension at cell-cell boundaries expressing cortical actomyosin contractions and cell-cell adhesive interactions. The strength of this tension is polarized; i.e., spatially biased within each cell according to a chemoattractant gradient. Using a 3D vertex model, we performed numerical simulations of multicellular dynamics in 3D space. The simulations revealed that the polarized interfacial tension enables cells to migrate collectively as a cluster through a 3D tissue. In this mechanism, interfacial tension induces unidirectional flow of each cell surface from the front to the rear along the cluster surface. Importantly, this mechanism does not necessarily require convection of cells, i.e., cell rearrangement, within the cluster. Moreover, several migratory modes were induced, depending on the strengths of polarity, adhesion, and noise; i.e., cells migrate either as single cells, as a cluster, or aligned like beads on a string, as occurs in embryogenesis and cancer invasion. These results indicate that the simple expansion and contraction of cell-cell boundaries enables cells to move directionally forward and to produce the variety of collective migratory movements observed in living systems.

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