Actin-ring segment switching drives nonadhesive gap closure

Gap closure to eliminate physical discontinuities and restore tissue integrity is a fundamental process in normal development and repair of damaged tissues and organs. Here, we demonstrate a nonadhesive gap closure model in which collective cell migration, large-scale actin-network fusion, and purse...

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Published inProceedings of the National Academy of Sciences - PNAS Vol. 117; no. 52; pp. 33263 - 33271
Main Authors Wei, Qiong, Shi, Xuechen, Zhao, Tiankai, Cai, Pingqiang, Chen, Tianwu, Zhang, Yao, Huang, Changjin, Yang, Jian, Chen, Xiaodong, Zhang, Sulin
Format Journal Article
LanguageEnglish
Published United States National Academy of Sciences 29.12.2020
Subjects
Actins - metabolism
Animals
Biological Sciences
Biomechanical Phenomena
Cell Adhesion
Cell Proliferation
Cell Shape
Dogs
Imaging, Three-Dimensional
Kinetics
Madin Darby Canine Kidney Cells
Microscopy, Atomic Force
Models, Biological
Time Factors
Wound Healing
traction force microscopy
gap closure
actin ring
cell patterning
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ISSN0027-8424
1091-6490
1091-6490
DOI10.1073/pnas.2010960117

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Summary:Gap closure to eliminate physical discontinuities and restore tissue integrity is a fundamental process in normal development and repair of damaged tissues and organs. Here, we demonstrate a nonadhesive gap closure model in which collective cell migration, large-scale actin-network fusion, and purse-string contraction orchestrate to restore the gap. Proliferative pressure drives migrating cells to attach onto the gap front at which a pluricellular actin ring is already assembled. An actin-ring segment switching process then occurs by fusion of actin fibers from the newly attached cells into the actin cable and defusion from the previously lined cells, thereby narrowing the gap. Such actin-cable segment switching occurs favorably at high curvature edges of the gap, yielding size-dependent gap closure. Cellular force microscopies evidence that a persistent rise in the radial component of inward traction force signifies successful actin-cable segment switching. A kinetic model that integrates cell proliferation, actin fiber fusion, and purse-string contraction is formulated to quantitatively account for the gap-closure dynamics. Our data reveal a previously unexplored mechanism in which cells exploit multifaceted strategies in a highly cooperative manner to close nonadhesive gaps.
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Edited by Philip LeDuc, Carnegie Mellon University, Pittsburgh, PA, and accepted by Editorial Board Member John A. Rogers November 6, 2020 (received for review June 7, 2020)
Author contributions: Q.W., X.S., C.H., and S.Z. designed research; Q.W., X.S., T.Z., P.C., T.C., and Y.Z. performed research; Q.W., X.S., T.Z., P.C., J.Y., X.C., and S.Z. contributed new reagents/analytic tools; Q.W., X.S., T.Z., P.C., and S.Z. analyzed data; and Q.W., X.S., and S.Z. wrote the paper.
1Q.W. and X.S. contributed equally to this work.
ISSN:0027-8424
1091-6490
1091-6490
DOI:10.1073/pnas.2010960117