Summary of 84-Ito-CellDyn

SSBD:database
SSBD:database URL
Title
Timelapse images of different types HT29 cells during nocodazole treatment
Description
-
Relase date
2018-11-14
Updated date
-
License
CC BY
Kind
Image data based on Experiment
Number of Datasets
7 ( Image datasets: 7, Quantitative data datasets: 0 )
Size of Datasets
638.0 MB ( Image datasets: 638.0 MB, Quantitative data datasets: 0 bytes )

Organism(s)
H. sapiens
Strain(s)
HT29
Protein name(s)
MLC2
Protein tag(s)
EGFP

Datatype
cell dynamics
Molecular Function (MF)
Biological Process (BP)
-
Cellular Component (CC)
apical junction complex
Biological Imaging Method
-
XYZ Scale
XY: 353 micrometer/pixel, Z: NA micrometer/slice
T scale
300 second for each time interval, 120 second for each time interval, 60 second for each time interval

Image Acquisition
Experiment type
TimeLapse
Microscope type
ConfocalMicroscope
Acquisition mode
LaserScanningConfocalMicroscopy
Contrast method
DIC
Microscope model
Olympus LCV100 or Olympus IX81 + Yokogawa CSU-W1
Detector model
Olympus DP30 or ImagEM-IK
Objective model
Olympus UAPOx40/340 or PLANAPO N x60/1.42 oil lens
Filter set
interference filter

Related paper(s)

Shoko Ito, Satoru Okuda, Masako Abe, Mari Fujimoto, Tetsuo Onuki, Tamako Nishimura, Masatoshi Takeichi (2017) Induced cortical tension restores functional junctions in adhesion-defective carcinoma cells., Nature communications, Volume 8, Number 1, pp. 1834

Published in 2017 Nov 28 (Electronic publication in Nov. 28, 2017, midnight )

(Abstract) Normal epithelial cells are stably connected to each other via the apical junctional complex (AJC). AJCs, however, tend to be disrupted during tumor progression, and this process is implicated in cancer dissemination. Here, using colon carcinoma cells that fail to form AJCs, we investigated molecular defects behind this failure through a search for chemical compounds that could restore AJCs, and found that microtubule-polymerization inhibitors (MTIs) were effective. MTIs activated GEF-H1/RhoA signaling, causing actomyosin contraction at the apical cortex. This contraction transmitted force to the cadherin-catenin complex, resulting in a mechanosensitive recruitment of vinculin to cell junctions. This process, in turn, recruited PDZ-RhoGEF to the junctions, leading to the RhoA/ROCK/LIM kinase/cofilin-dependent stabilization of the junctions. RhoGAP depletion mimicked these MTI-mediated processes. Cells that normally organize AJCs did not show such MTI/RhoA sensitivity. Thus, advanced carcinoma cells require elevated RhoA activity for establishing robust junctions, which triggers tension-sensitive reorganization of actin/adhesion regulators.
(MeSH Terms)

Contact
Masatoshi Takeichi , RIKEN , Center for Biosystems Dynamics Research , Laboratory for Cell Adhesion and Tissue Patterning
Contributors
Shoko Ito, Satoru Okuda, Masako Abe, Mari Fujimoto, Tetsuo Onuki, Tamako Nishimura, Masatoshi Takeichi


Dataset List of 84-Ito-CellDyn

#
Dataset ID
Kind
Size
4D View
SSBD:OMERO
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# 4082
Datast ID fig1e
Dataset Kind Image data
Dataset Size 48.1 MB
4D view
SSBD:OMERO
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# 4083
Datast ID fig5e
Dataset Kind Image data
Dataset Size 37.4 MB
4D view
SSBD:OMERO
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# 4084
Datast ID fig6a_lower
Dataset Kind Image data
Dataset Size 45.9 MB
4D view
SSBD:OMERO
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# 4085
Datast ID fig6a_upper
Dataset Kind Image data
Dataset Size 45.9 MB
4D view
SSBD:OMERO
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# 4086
Datast ID figS1c_left
Dataset Kind Image data
Dataset Size 225.0 MB
4D view
SSBD:OMERO
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# 4087
Datast ID figS1c_right
Dataset Kind Image data
Dataset Size 225.0 MB
4D view
SSBD:OMERO
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# 4088
Datast ID figS2a
Dataset Kind Image data
Dataset Size 10.5 MB
4D view
SSBD:OMERO
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