Contractile and mechanical properties in epithelia with perturbed actomyosin dynamics
Mechanics has an important role during morphogenesis, both in the generation of forces driving cell shape changes and in determining the effective material properties of cells and tissues. Drosophila dorsal closure (DC) has emerged as a model system for studying the interplay between tissue mechanic...
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Main Authors | , , , , , , |
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Format | Journal Article |
Language | English |
Published |
24.03.2014
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Subjects | |
Online Access | Get full text |
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Summary: | Mechanics has an important role during morphogenesis, both in the generation
of forces driving cell shape changes and in determining the effective material
properties of cells and tissues. Drosophila dorsal closure (DC) has emerged as
a model system for studying the interplay between tissue mechanics and cellular
activity. Thereby, the amnioserosa (AS) generates one of the major forces that
drive DC through the apical contraction of its constituent cells. We combined
quantitation of live data, genetic and mechanical perturbation and cell
biology, to investigate how mechanical properties and contraction rate emerge
from cytoskeletal activity. We found that a decrease in Myosin phosphorylation
induces a fluidization of AS cells which become more compliant. Conversely, an
increase in Myosin phosphorylation and an increase in actin linear
polymerization induce a solidification of cells. Contrary to expectation, these
two perturbations have an opposite effect on the strain rate of cells during
DC. While an increase in actin polymerization increases the contraction rate of
AS cells, an increase in Myosin phosphorylation gives rise to cells that
contract very slowly. The quantification of how the perturbation induced by
laser ablation decays throughout the tissue revealed that the tissue in these
two mutant backgrounds reacts very differently. We suggest that the differences
in the strain rate of cells in situations where Myosin activity or actin
polymerization is increased arise from changes in how the contractile forces
are transmitted and coordinated across the tissue through ECadherin mediated
adhesion. Our results show that there is an optimal level of Myosin activity to
generate efficient contraction and suggest that the architecture of the actin
cytoskeleton and the dynamics of adhesion complexes are important parameters
for the emergence of coordinated activity throughout the tissue. |
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DOI: | 10.48550/arxiv.1403.5878 |