Long term follow‐up in a patient with a de novo microdeletion of 14q11.2 involving <i>CHD8</i>

Drabova, Jana; Seemanová, E; Hančárová, Miroslava; Pourová, Radka Kremlíková; Horacek, Martin; Jancuskova, Tereza; Pekova, Sona; Novotna, Drahuse; Sedláček, Zdeněk

doi:10.1002/ajmg.a.36957

Cited by 10 publications

(1 citation statement)

References 10 publications

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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%

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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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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The CHD8 overgrowth syndrome: A detailed evaluation of an emerging overgrowth phenotype in 27 patients

Ostrowski

Zachariou

Loveday

et al. 2019

American J of Med Genetics Pt C

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CHD8 has been reported as an autism susceptibility/intellectual disability gene but emerging evidence suggests that it additionally causes an overgrowth phenotype. This study reports 27 unrelated patients with pathogenic or likely pathogenic CHD8 variants (25 null variants, two missense variants) and a male:female ratio of 21:6 (3.5:1, p < .01). All patients presented with intellectual disability, with 85% in the mild or moderate range, and 85% had a height and/or head circumference ≥2 standard deviations above the mean, meeting our clinical criteria for overgrowth. Behavioral problems were reported in the majority of patients (78%), with over half (56%) either formally diagnosed with an autistic spectrum disorder or described as having autistic traits. Additional clinical features included neonatal hypotonia (33%), and less frequently seizures, pes planus, scoliosis, fifth finger clinodactyly, umbilical hernia, and glabellar hemangioma (≤15% each). These results suggest that, in addition to its established link with autism and intellectual disability, CHD8 causes an overgrowth phenotype, and should be considered in the differential diagnosis of patients presenting with increased height and/or head circumference in association with intellectual disability.

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A CNV Catalogue

Wyandt

Wilson

Tonk

2017

Human Chromosome Variation: Heteromorphism, Polymorphism and Pathogenesis

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Long term follow‐up in a patient with a de novo microdeletion of 14q11.2 involving CHD8

Cited by 10 publications

References 10 publications

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

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

The CHD8 overgrowth syndrome: A detailed evaluation of an emerging overgrowth phenotype in 27 patients

A CNV Catalogue

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