Detail of Fig5j_spines_SIM_EGFP_tagRFP-dEVH1_10
Project
Title
SIM images of spines from individual neurons expressing EGFP and tagRFP-ΔEVH1.
Description
SIM images of spines from individual neurons expressing EGFP and tagRFP-ΔEVH1.
Release, Updated
2022-03-31
License
CC-BY
Kind
Image data
File Formats
.tif
Data size
126.2 MB
Protein tags
EGFP, tagRFP
Datatype
-
Molecular Function (MF)
-
Biological Process (BP)
dendritic spine development
(
GO:0060996
)
synapse organization
(
GO:0050808
)
Cellular Component (CC)
dendritic spine
(
GO:0043197
)
Biological Imaging Method
structured illumination microscopy
(
Fbbi:00000332
)
X scale
0.032 micrometer/pixel
Y scale
0.032 micrometer/pixel
Z scale
0.12 micrometer/slice
T scale
NA (single image)
Image Acquisition
Experiment type
-
Microscope type
-
Acquisition mode
-
Contrast method
-
Microscope model
-
Detector model
-
Objective model
-
Filter set
-
Summary of Methods
See details in Iwasaki K, et. al. (2020) Eur J Neurosci., 51(3):806-821.
Related paper(s)
Kanako Iwasaki, Kazuki Obashi, Shigeo Okabe (2020) Vasodilator-stimulated phosphoprotein (VASP) is recruited into dendritic spines via G-actin-dependent mechanism and contributes to spine enlargement and stabilization., The European journal of neuroscience, Volume 51, Number 3, pp. 806-821
Published in 2020 Feb (Electronic publication in Dec. 18, 2019, midnight )
- doi: 10.1111/ejn.14634
-
pmid: 31793065
(Abstract) Actin organization and dynamics are modulated by diverse actin regulators during dendritic spine development. To understand the molecular network that regulates actin organization and spine morphology, it is important to investigate dynamic redistribution of actin regulators during spine development. One of the actin regulators, vasodilator-stimulated phosphoprotein (VASP), has multiple functions in actin regulation and is known to regulate spine morphology. However, dynamics and temporal regulation of VASP during spine development have not been clarified. In this study, we performed time-lapse imaging of mouse hippocampal dissociated neurons to analyse the change in localization of VASP during spine development. We found that accumulation of VASP within spines precedes the start of persistent F-actin increase, which are temporally coupled with spine enlargement. Using domain deletion or mutation constructs of VASP, we revealed that the interaction with G-actin is important for the preceding accumulation of VASP. Furthermore, we showed that accumulation of VASP contributes to actin enrichment within spines and stabilization of spine morphology by dominant negative experiments. These data suggest that G-actin-dependent VASP recruitment has dual functions in spine development, enlargement and stabilization, through the interaction with actin and other cytoskeletal regulators.(MeSH Terms)
Contact
Shigeo Okabe
, The University of Tokyo
, Department of Cellular Neurobiology, Graduate School of Medicine
Contributors
OMERO Dataset
OMERO Project
Source