Summary of 273-Kaise-NeuralStemCell

SSBD:database
SSBD:database URL
Title
Bioluminescent time-lapse imaging of Ascl1-Luciferse reporter mice's brain slices after iPaD virus injection
Description
-
Relase date
2024-11-25
Updated date
-
License
CC BY
Kind
Image data based on Experiment
Number of Datasets
2 ( Image datasets: 2, Quantitative data datasets: 0 )
Size of Datasets
242.0 MB ( Image datasets: 242.0 MB, Quantitative data datasets: 0 bytes )

Organism(s)
Mus musculus

Datatype
-
Molecular Function (MF)
Biological Process (BP)
stem cell differentiation, neurogenesis
Cellular Component (CC)
Biological Imaging Method
fluorescence microscopy, time lapse microscopy
X scale
-
Y scale
-
Z scale
-
T scale
10 minutes per time interval

Image Acquisition
Experiment type
-
Microscope type
-
Acquisition mode
-
Contrast method
-
Microscope model
-
Detector model
-
Objective model
-
Filter set
-

Related paper(s)

Takashi Kaise, Masahiro Fukui, Risa Sueda, Wenhui Piao, Mayumi Yamada, Taeko Kobayashi, Itaru Imayoshi, Ryoichiro Kageyama (2022) Functional rejuvenation of aged neural stem cells by Plagl2 and anti-Dyrk1a activity., Genes & development, Volume 36, Number 1-2, pp. 23-37

Published in 2022 Jan 1 (Electronic publication in Dec. 16, 2021, midnight )

(Abstract) The regenerative potential of neural stem cells (NSCs) declines during aging, leading to cognitive dysfunctions. This decline involves up-regulation of senescence-associated genes, but inactivation of such genes failed to reverse aging of hippocampal NSCs. Because many genes are up-regulated or down-regulated during aging, manipulation of single genes would be insufficient to reverse aging. Here we searched for a gene combination that can rejuvenate NSCs in the aged mouse brain from nuclear factors differentially expressed between embryonic and adult NSCs and their modulators. We found that a combination of inducing the zinc finger transcription factor gene Plagl2 and inhibiting Dyrk1a, a gene associated with Down syndrome (a genetic disorder known to accelerate aging), rejuvenated aged hippocampal NSCs, which already lost proliferative and neurogenic potential. Such rejuvenated NSCs proliferated and produced new neurons continuously at the level observed in juvenile hippocampi, leading to improved cognition. Epigenome, transcriptome, and live-imaging analyses indicated that this gene combination induces up-regulation of embryo-associated genes and down-regulation of age-associated genes by changing their chromatin accessibility, thereby rejuvenating aged dormant NSCs to function like juvenile active NSCs. Thus, aging of NSCs can be reversed to induce functional neurogenesis continuously, offering a way to treat age-related neurological disorders.
(MeSH Terms)

Contact
Ryoichiro Kageyama , RIKEN , RIKEN Center for Brain Science
Contributors
Risa Sueda


Dataset List of 273-Kaise-NeuralStemCell

#
Dataset ID
Kind
Size
4D View
SSBD:OMERO
Download BDML
Download Images
# 11550
Dataset Kind Image data
Dataset Size 121.0 MB
4D view
SSBD:OMERO
Download BDML
Download Image data

# 11551
Dataset Kind Image data
Dataset Size 121.0 MB
4D view
SSBD:OMERO
Download BDML
Download Image data