Please use this identifier to cite or link to this item: https://doi.org/10.1172/JCI83408
Title: The chromatin remodeling factor CHD7 controls cerebellar development by regulating reelin expression
Authors: Whittaker, D.E
Riegman, K.L.H
Kasah, S
Mohan, C
Yu, T
Sala, B.P
Hebaishi, H
Caruso, A
Marques, A.C
Michetti, C
Smachetti, M.E.S
Shah, A
Sabbioni, M
Kulhanci, O
Tee, W.-W 
Reinberg, D
Scattoni, M.L
Volk, H
McGonnell, I
Wardle, F.C
Fernandes, C
Basson, M.A
Keywords: caspase
reelin
Chd7 protein, mouse
DNA binding protein
nerve cell adhesion molecule
nerve protein
reelin protein
scleroprotein
serine proteinase
animal cell
animal experiment
animal model
animal tissue
Article
brain development
BrdU assay
cell differentiation
cell proliferation
cell survival
cerebellum
cerebellum hypoplasia
CHD7 gene
chromatin assembly and disassembly
chromatin immunoprecipitation
controlled study
developmental disorder
experimental behavioral test
female
gene
gene expression
gene mutation
immunohistochemistry
in situ hybridization
male
motor coordination
motor dysfunction
mouse
nonhuman
polymerase chain reaction
protein expression
reelin gene
Western blotting
abnormalities
animal
cerebellum
embryology
gene expression regulation
gene locus
genetics
genome-wide association study
human
metabolism
nervous system development
nervous system malformation
neural stem cell
transgenic mouse
Animals
Cell Adhesion Molecules, Neuronal
Cerebellum
Developmental Disabilities
DNA-Binding Proteins
Extracellular Matrix Proteins
Gene Expression Regulation, Developmental
Genetic Loci
Genome-Wide Association Study
Humans
Mice
Mice, Transgenic
Motor Disorders
Nerve Tissue Proteins
Nervous System Malformations
Neural Stem Cells
Neurogenesis
Serine Endopeptidases
Issue Date: 2017
Publisher: American Society for Clinical Investigation
Citation: Whittaker, D.E, Riegman, K.L.H, Kasah, S, Mohan, C, Yu, T, Sala, B.P, Hebaishi, H, Caruso, A, Marques, A.C, Michetti, C, Smachetti, M.E.S, Shah, A, Sabbioni, M, Kulhanci, O, Tee, W.-W, Reinberg, D, Scattoni, M.L, Volk, H, McGonnell, I, Wardle, F.C, Fernandes, C, Basson, M.A (2017). The chromatin remodeling factor CHD7 controls cerebellar development by regulating reelin expression. Journal of Clinical Investigation 127 (3) : 874-887. ScholarBank@NUS Repository. https://doi.org/10.1172/JCI83408
Rights: Attribution 4.0 International
Abstract: The mechanisms underlying the neurodevelopmental deficits associated with CHARGE syndrome, which include cerebellar hypoplasia, developmental delay, coordination problems, and autistic features, have not been identified. CHARGE syndrome has been associated with mutations in the gene encoding the ATP-dependent chromatin remodeler CHD7. CHD7 is expressed in neural stem and progenitor cells, but its role in neurogenesis during brain development remains unknown. Here we have shown that deletion of Chd7 from cerebellar granule cell progenitors (GCps) results in reduced GCp proliferation, cerebellar hypoplasia, developmental delay, and motor deficits in mice. Genome-wide expression profiling revealed downregulated expression of the gene encoding the glycoprotein reelin (Reln) in Chd7-deficient GCps. Recessive RELN mutations have been associated with severe cerebellar hypoplasia in humans. We found molecular and genetic evidence that reductions in Reln expression contribute to GCp proliferative defects and cerebellar hypoplasia in GCp-specific Chd7 mouse mutants. Finally, we showed that CHD7 is necessary for maintaining an open, accessible chromatin state at the Reln locus. Taken together, this study shows that Reln gene expression is regulated by chromatin remodeling, identifies CHD7 as a previously unrecognized upstream regulator of Reln, and provides direct in vivo evidence that a mammalian CHD protein can control brain development by modulating chromatin accessibility in neuronal progenitors.
Source Title: Journal of Clinical Investigation
URI: https://scholarbank.nus.edu.sg/handle/10635/179226
ISSN: 00219738
DOI: 10.1172/JCI83408
Rights: Attribution 4.0 International
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