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Distinct, dosage-sensitive requirements for the autism-associated factor CHD8 during cortical development
by
Scattoni, Maria Luisa
, Brock, Olivier
, Delogu, Alessio
, Michetti, Caterina
, Evans, Romy
, Hurley, Shaun
, Rudari, Fabrizio
, Caruso, Angela
, Lerch, Jason P.
, Mohan, Conor
, Ellegood, Jacob
, Fernandes, Cathy
, Ellingford, Robert
, Riegman, Kimberley L. H.
, Suetterlin, Philipp
, Basson, M. Albert
in
Animals
/ Animals, Newborn
/ Antibodies
/ Apoptosis
/ Autism
/ Autistic Disorder - genetics
/ Behavior, Animal
/ Brain
/ Brain - diagnostic imaging
/ Brain - embryology
/ Brain - growth & development
/ Brain research
/ Cell Proliferation
/ Cerebral cortex
/ CHD8
/ Chromatin
/ Cortex
/ Deoxyribonucleic acid
/ Development and progression
/ Disease Models, Animal
/ DNA
/ DNA-Binding Proteins - deficiency
/ DNA-Binding Proteins - genetics
/ Embryonic development
/ Female
/ Gene expression
/ Gene Expression Regulation, Developmental
/ Gene mutations
/ Genetic aspects
/ Genetic transcription
/ Health aspects
/ Human Genetics
/ Hypomorph
/ Laboratories
/ Medicine
/ Medicine & Public Health
/ Mice, Transgenic
/ Molecular weight
/ Mutation
/ Neurology
/ Neuropsychology
/ Neurosciences
/ Pediatrics
/ Phenotype
/ Pregnancy
/ Proteins
/ Psychiatry
/ Risk factors
/ Stem Cells
/ TBR2
/ Tumor Suppressor Protein p53 - genetics
2021
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Distinct, dosage-sensitive requirements for the autism-associated factor CHD8 during cortical development
by
Scattoni, Maria Luisa
, Brock, Olivier
, Delogu, Alessio
, Michetti, Caterina
, Evans, Romy
, Hurley, Shaun
, Rudari, Fabrizio
, Caruso, Angela
, Lerch, Jason P.
, Mohan, Conor
, Ellegood, Jacob
, Fernandes, Cathy
, Ellingford, Robert
, Riegman, Kimberley L. H.
, Suetterlin, Philipp
, Basson, M. Albert
in
Animals
/ Animals, Newborn
/ Antibodies
/ Apoptosis
/ Autism
/ Autistic Disorder - genetics
/ Behavior, Animal
/ Brain
/ Brain - diagnostic imaging
/ Brain - embryology
/ Brain - growth & development
/ Brain research
/ Cell Proliferation
/ Cerebral cortex
/ CHD8
/ Chromatin
/ Cortex
/ Deoxyribonucleic acid
/ Development and progression
/ Disease Models, Animal
/ DNA
/ DNA-Binding Proteins - deficiency
/ DNA-Binding Proteins - genetics
/ Embryonic development
/ Female
/ Gene expression
/ Gene Expression Regulation, Developmental
/ Gene mutations
/ Genetic aspects
/ Genetic transcription
/ Health aspects
/ Human Genetics
/ Hypomorph
/ Laboratories
/ Medicine
/ Medicine & Public Health
/ Mice, Transgenic
/ Molecular weight
/ Mutation
/ Neurology
/ Neuropsychology
/ Neurosciences
/ Pediatrics
/ Phenotype
/ Pregnancy
/ Proteins
/ Psychiatry
/ Risk factors
/ Stem Cells
/ TBR2
/ Tumor Suppressor Protein p53 - genetics
2021
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Distinct, dosage-sensitive requirements for the autism-associated factor CHD8 during cortical development
by
Scattoni, Maria Luisa
, Brock, Olivier
, Delogu, Alessio
, Michetti, Caterina
, Evans, Romy
, Hurley, Shaun
, Rudari, Fabrizio
, Caruso, Angela
, Lerch, Jason P.
, Mohan, Conor
, Ellegood, Jacob
, Fernandes, Cathy
, Ellingford, Robert
, Riegman, Kimberley L. H.
, Suetterlin, Philipp
, Basson, M. Albert
in
Animals
/ Animals, Newborn
/ Antibodies
/ Apoptosis
/ Autism
/ Autistic Disorder - genetics
/ Behavior, Animal
/ Brain
/ Brain - diagnostic imaging
/ Brain - embryology
/ Brain - growth & development
/ Brain research
/ Cell Proliferation
/ Cerebral cortex
/ CHD8
/ Chromatin
/ Cortex
/ Deoxyribonucleic acid
/ Development and progression
/ Disease Models, Animal
/ DNA
/ DNA-Binding Proteins - deficiency
/ DNA-Binding Proteins - genetics
/ Embryonic development
/ Female
/ Gene expression
/ Gene Expression Regulation, Developmental
/ Gene mutations
/ Genetic aspects
/ Genetic transcription
/ Health aspects
/ Human Genetics
/ Hypomorph
/ Laboratories
/ Medicine
/ Medicine & Public Health
/ Mice, Transgenic
/ Molecular weight
/ Mutation
/ Neurology
/ Neuropsychology
/ Neurosciences
/ Pediatrics
/ Phenotype
/ Pregnancy
/ Proteins
/ Psychiatry
/ Risk factors
/ Stem Cells
/ TBR2
/ Tumor Suppressor Protein p53 - genetics
2021
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Distinct, dosage-sensitive requirements for the autism-associated factor CHD8 during cortical development
Journal Article
Distinct, dosage-sensitive requirements for the autism-associated factor CHD8 during cortical development
2021
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Overview
Background
CHD8
haploinsufficiency causes autism and macrocephaly with high penetrance in the human population.
Chd8
heterozygous mice exhibit relatively subtle brain overgrowth and little gene expression changes in the embryonic neocortex. The purpose of this study was to generate new, sub-haploinsufficient
Chd8
mouse models to allow us to identify and study the functions of CHD8 during embryonic cortical development.
Methods
To examine the possibility that certain phenotypes may only appear at sub-heterozygous
Chd8
levels in the mouse, we created an allelic series of
Chd8
-deficient mice to reduce CHD8 protein levels to approximately 35% (mild hypomorph), 10% (severe hypomorph) and 0% (neural-specific conditional knockout) of wildtype levels. We used RNA sequencing to compare transcriptional dysregulation, structural MRI and brain weight to investigate effects on brain size, and cell proliferation, differentiation and apoptosis markers in immunostaining assays to quantify changes in neural progenitor fate.
Results
Mild
Chd8
hypomorphs displayed significant postnatal lethality, with surviving animals exhibiting more pronounced brain hyperplasia than heterozygotes. Over 2000 genes were dysregulated in mild hypomorphs, including autism-associated neurodevelopmental and cell cycle genes. We identify increased proliferation of non-ventricular zone TBR2+ intermediate progenitors as one potential cause of brain hyperplasia in these mutants. Severe
Chd8
hypomorphs displayed even greater transcriptional dysregulation, including evidence for p53 pathway upregulation. In contrast to mild hypomorphs, these mice displayed reduced brain size and increased apoptosis in the embryonic neocortex. Homozygous, conditional deletion of
Chd8
in early neuronal progenitors resulted in pronounced brain hypoplasia, partly caused by p53 target gene derepression and apoptosis in the embryonic neocortex.
Limitations
Our findings identify an important role for the autism-associated factor CHD8 in controlling the proliferation of intermediate progenitors in the mouse neocortex. We propose that CHD8 has a similar function in human brain development, but studies on human cells are required to confirm this. Because many of our mouse mutants with reduced CHD8 function die shortly after birth, it is not possible to fully determine to what extent reduced CHD8 function results in autism-associated behaviours in mice.
Conclusions
Together, these findings identify important, dosage-sensitive functions for CHD8 in p53 pathway repression, neurodevelopmental gene expression and neural progenitor fate in the embryonic neocortex. We conclude that brain development is acutely sensitive to reduced CHD8 expression and that the varying sensitivities of different progenitor populations and cellular processes to CHD8 dosage result in non-linear effects on gene transcription and brain growth.
Shaun Hurley, Conor Mohan and Philipp Suetterlin have contributed equally to this work.
Publisher
BioMed Central,BioMed Central Ltd,Springer Nature B.V,BMC
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