The clinical presentation caused by truncating <i>CHD8</i> variants

Douzgou, Sofia; Liang, Hui; Metcalfe, Kay; Somarathi, Suresh; Tischkowitz, Marc; Wafik, Mohamed; Kini, Usha; McKee, Shane; Yates, Laura; Bértoli, Marta; Lynch, Sally Ann; Holder, Susan; Banka, Siddharth

doi:10.1111/cge.13554

Cited by 37 publications

(42 citation statements)

References 38 publications

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“…In the current study, we report a new model created using a gene trap after Exon 31 of Chd8 that is predicted to result in a truncated protein product. This mutation is clinically relevant because multiple different truncating mutations in this region have been reported in the literature [Douzgou et al, 2019]. The current study adds to the growing resource of Chd8 mouse models.…”

Section: Introductionmentioning

confidence: 84%

A Novel Chd8 Mutant Mouse Displays Altered Ultrasonic Vocalizations and Enhanced Motor Coordination

et al. 2020

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Mutations in CHD8 are among the most common autism-causing genetic defects identified in human genomics studies. Therefore, many labs have attempted to model this disorder by generating mice with mutations in Chd8. Using a gene trap inserted after Exon 31, we created a novel Chd8 mutant mouse (Chd8 +/E31T) and characterized its behavior on several different assays thought to have face validity for the human condition, attempting to model both the core symptoms (repetitive behaviors and social communication impairments) and common comorbidities (motor deficits, anxiety, and intellectual disability). We found that Chd8 +/E31T mice showed no difference compared to wild-type mice in amount of self-grooming, reproducing the negative finding most other studies have reported. Unlike some of the other published lines, Chd8 +/E31T mice did not show deficits in the three-chamber test for social novelty preference. A few studies have examined ultrasonic vocalizations in Chd8 mutant mice, but we are the first to report an increase in call length for adult mice. Additionally, we found that in contrast to previous published lines, Chd8 +/E31T mice displayed no anxiety-like behaviors or learning impairments but showed paradoxically significant improvement in motor function. The inconsistencies in behavioral phenotypes in the Chd8 mutant mice generated by different laboratories poses a challenge for modeling autism spectrum disorder and preclinical studies in mice going forward and warrants further investigation into the molecular consequences of the different mutations in Chd8 and the functional impact on behavior.

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Section: Introductionmentioning

confidence: 84%

A Novel Chd8 Mutant Mouse Displays Altered Ultrasonic Vocalizations and Enhanced Motor Coordination

et al. 2020

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“…Myasthenia has to date not been reported in association with CHD8 mutations. The clinical phenotype of patients with CHD8 mutations does vary, but macrosomia, macrocephalus, ASD [14,23,24] and gastrointestinal problems [25][26][27][28][29][30][31][32][33][34][35][36][37] appear to be constant features [29,38]. Some reports mention muscle hypotonia, however, in cases of microdeletions it often remains unclear, whether a certain symptom might be caused by CHD8 deficiency per se or by derangement of neighbouring genes [25].…”

Section: Discussionmentioning

confidence: 99%

“…Some reports mention muscle hypotonia, however, in cases of microdeletions it often remains unclear, whether a certain symptom might be caused by CHD8 deficiency per se or by derangement of neighbouring genes [25]. The majority of disease-associated variants are de novo microdeletions [25,33,38] and frameshift mutations [29,35,38]. So far, only one other missense mutation (p.R1797Q) and two deletions of one amino acid (p.K2287del; p.H2498del) have been published along with phenotype descriptions [29].…”

Section: Discussionmentioning

confidence: 99%

A spontaneous missense mutation in the chromodomain helicase DNA‐binding protein 8 (CHD8) gene: a novel association with congenital myasthenic syndrome

Lee

Petkova

Morales‐Gonzalez

et al. 2020

Neuropathology Appl Neurobio

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A spontaneous missense mutation in the chromodomain helicase DNA-binding protein 8 (CHD8) gene: a novel association with congenital myasthenic syndrome Aims: Congenital myasthenic syndromes (CMS) are characterized by muscle weakness, ptosis and episodic apnoea. Mutations affect integral protein components of the neuromuscular junction (NMJ). Here we searched for the genetic basis of CMS in female monozygotic twins. Methods: We employed whole-exome sequencing for mutation detection and Sanger sequencing for segregation analysis. Immunohistology was done with antibodies against CHD8, rapsyn, b-catenin (bCAT) and golgin on fibroblasts, human and mouse muscle. We recorded superresolution images of the NMJ using 3D-structured illumination microscopy. Results: We discovered a spontaneous missense mutation in CHD8 [chr14: g.21,884,051G>A, GRCh37.p11 | c.1732C>T, NM_0011 7062 | p.(R578C)], the gene encoding chromodomain helicase DNA-binding protein 8. This is the first missense mutation affecting Duplin, the short 110 kDa isoform of CHD8. It is known that CHD8/Duplin negatively regulates bCAT signalling in the WNT pathway and plays a role in chromatin remodelling. Inactivating CHD8 mutations are associated with autism spectrum disorder and intellectual disability in combination with facial dysmorphism, overgrowth and macrocephalus. No musclespecific phenotype has been reported to date. Co-immunostaining with rapsyn on human and mouse muscle revealed a strong presence of CHD8 at the NMJ being located towards the sarcoplasmic side of the rapsyn cluster, where it co-localizes with bCAT. Conclusion: We hypothesize CHD8 to have a role in the maintenance of the structural integrity and function of the NMJ. Both patients benefited from treatment with 3,4-diaminopyridine, a reversible blocker of voltage-gated potassium channels at the nerve terminal that prolongs the action potential and increases acetylcholine release.

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“…Detailed phenotyping studies of individuals with pathogenic variants in specific genes are another source of data for evaluating ASD specificity. For example, the gene CHD8 is frequently discussed as a model "ASD gene" because mutations in this gene are associated with a high rate of ASD (Bernier et al, 2014 24 Twenty-one of the 25 (84%) had a diagnosis of ASD (Douzgou et al, 2019). 24 However, ascertainment bias is also a concern with clinical cohorts such as these, since individuals with mild phenotypes are less likely to be identified.…”

Section: Genotype-based Cohortsmentioning

confidence: 99%

“…For example, the gene CHD8 is frequently discussed as a model "ASD gene" because mutations in this gene are associated with a high rate of ASD (Bernier et al, 2014 24 Twenty-one of the 25 (84%) had a diagnosis of ASD (Douzgou et al, 2019). 24 However, ascertainment bias is also a concern with clinical cohorts such as these, since individuals with mild phenotypes are less likely to be identified. For example, Guo et al (2018) assessed three families in which likely gene disrupting CHD8 mutations were transmitted from parents with full-scale IQ scores between 80 and 87 (verbal IQ 88-95, nonverbal IQ 75-79), establishing the possibility of relative sparing of cognition.…”

Section: Genotype-based Cohortsmentioning

confidence: 99%

Insufficient Evidence for “Autism-Specific” Genes

Myers¹,

Challman²,

Bernier³

et al. 2020

Preprint

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Despite the evidence that deleterious variants in the same genes are implicated across multiple neurodevelopmental disorders, there has been considerable interest in identifying genes that, when mutated, confer risk that is largely specific for autism spectrum disorder (ASD). Here, we review recent efforts to identify “autism-specific” genes, which focus on rare variants of large effect size that are thought to account for the observed phenotype in participants, present a divergent interpretation of the published evidence, and provide additional contradictory data. There is currently insufficient evidence to establish ASD-specificity of any genes based on large-effect rare variant data.

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The clinical presentation caused by truncating CHD8 variants

Cited by 37 publications

References 38 publications

A Novel Chd8 Mutant Mouse Displays Altered Ultrasonic Vocalizations and Enhanced Motor Coordination

A Novel Chd8 Mutant Mouse Displays Altered Ultrasonic Vocalizations and Enhanced Motor Coordination

A spontaneous missense mutation in the chromodomain helicase DNA‐binding protein 8 (CHD8) gene: a novel association with congenital myasthenic syndrome

Insufficient Evidence for “Autism-Specific” Genes

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