A second cohort of CHD3 patients expands the molecular mechanisms known to cause Snijders Blok-Campeau syndrome

Drivas, Theodore G.; Liu, Dong; Nair, Divya; Alaimo, Joseph T.; Alders, Mariëlle; Altmüller, Janine; Barakat, Tahsin Stefan; Bebin, E. Martina; Bertsch, Nicole L.; Blackburn, Patrick R.; Blesson, Alyssa; Bouman, Arjan; Brockmann, Knut; Brunelle, Perrine; Burmeister, Margit; Cooper, Gregory M.; Denecke, Jonas; Dieux-Coëslier, Anne; Dubbs, Holly; Ferrer, Alejandro; Gal, Danna; Bartik, Lauren; Gunderson, Lauren; Hasadsri, Linda; Jain, Mahim; Karimov, Catherine; Keena, Beth; Klee, Eric W.; Kloth, Katja; Lāce, Baiba; Macchiaiolo, Marina; Marcadier, Julien L.; Milunsky, Jeff M.; Napier, Melanie; Ortiz-González, Xilma R.; Pichurin, Pavel N.; Pinner, Jason; Powis, Zöe; Prasad, Chitra; Radio, Francesca Clementina; Rasmussen, Kristen; Renaud, Deborah L.; Rush, Eric T.; Saunders, Carol J.; Selcen, Duygu; Seman, Ann; Shinde, Deepali N.; Smith, Erica D.; Smol, Thomas; Blok, Lot Snijders; Stoler, Joan M.; Tang, Sha; Tartaglia, Marco; Thompson, Michelle L.; Kamp, Jiddeke M. van de; Wang, Jingmin; Weise, Dagmar; Weiss, Karin; Woitschach, Rixa; Wollnik, Bernd; Yan, Huifang; Zackai, Elaine H.; Zampino, Giuseppe; Campeau, Philippe M.; Bhoj, Elizabeth

doi:10.1038/s41431-020-0654-4

Cited by 26 publications

(57 citation statements)

References 14 publications

(29 reference statements)

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“…In general, this novel SMARCA5 -associated syndrome reported here appears to result in a less severe phenotype when compared to other neurodevelopmental disorders due to pathogenic variants in ARID, SMARC , and CHD gene families, where almost all of the variants occur de novo and parent-child transmission is rarely documented ( 49, 55 ). We present here a three-generation pedigree (for individuals 4-6) segregating a deleterious missense variant.…”

Section: Discussionmentioning

confidence: 66%

“…We identified six missense variants, one splice-altering variant that lead to exon skipping and in-frame deletion, and one recurrent in-frame deletion in eleven individuals from nine unrelated families from around the world. The individuals in our study demonstrated a broad range of clinical features, as is not uncommon in neurodevelopmental disorders associated with pathogenic variants in aforementioned chromatin remodeling complexes (i.e., SWI/SNF, CHD, and ISWI) that vary from isolated autism to syndromic intellectual disability ( 5, 17, 48, 49 ). The most consistent clinical findings in our cohort are postnatal microcephaly and short stature observed in 10/12 individuals, and developmental delay in 8/10 individuals, although again, the severity of these delays varies widely from mild to severe (individual 7).…”

Section: Discussionmentioning

confidence: 69%

“…Varying degrees of developmental delay have been consistently reported in neurodevelopmental disorders associated with pathogenic variants involved in chromatin remodeling complexes. Similarly, varying head size ranging from microcephalic to macrocephalic is also frequently observed, for example, in SMARCB1 and CHD3 ( 49, 50 ). It is widely acknowledged that different variants within different functional domains of a gene can cause different phenotypes.…”

Section: Discussionmentioning

confidence: 92%

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Pathogenic variants inSMARCA5, a chromatin remodeler, cause a range of syndromic neurodevelopmental features

Liu

Wang

Gong

et al. 2020

Preprint

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Intellectual disability (ID) encompasses a wide spectrum of neurodevelopmental disorders, with many linked genetic loci. However, the underlying molecular mechanism for over 50% of the patients remains elusive. We describe mutations in SMARCA5, encoding the ATPase motor of the ISWI chromatin remodeler, as a cause of a novel neurodevelopmental disorder, identifying twelve individuals with de novo or dominantly segregating rare heterozygous variants. Accompanying phenotypes include mild developmental delay, frequent postnatal short stature, and microcephaly, and recurrent dysmorphic features. Loss of function of the SMARCA5 Drosophila ortholog Iswi led to smaller body size, reduced dendrite complexity, and tiling defects in larvae. In adult flies, Iswi neural knockdown caused decreased brain size, aberrant mushroom body morphology and abnormal locomotor function. Iswi loss of function was rescued by wild-type but not mutant SMARCA5. Our results demonstrate that SMARCA5 pathogenic variants cause a neurodevelopmental syndrome with mild facial dysmorphia.

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Section: Discussionmentioning

confidence: 66%

Section: Discussionmentioning

confidence: 69%

Section: Discussionmentioning

confidence: 92%

See 1 more Smart Citation

Pathogenic variants inSMARCA5, a chromatin remodeler, cause a range of syndromic neurodevelopmental features

Liu

Wang

Gong

et al. 2020

Preprint

Self Cite

View full text Add to dashboard Cite

show abstract

“…We identified seven missense variants, one splice-altering variant that led to exon skipping and in-frame deletion, and one recurrent in-frame deletion in 12 individuals from 10 unrelated families from around the world. The individuals in our study demonstrated a broad range of clinical features, as is not uncommon in neurodevelopmental disorders associated with pathogenic variants in aforementioned chromatin remodeling complexes (i.e., SWI/SNF, CHD, and ISWI) that vary from isolated autism to syndromic intellectual disability (5,17,49,50). The most consistent clinical findings in our cohort are postnatal microcephaly and short stature observed in 10 of 12 individuals as well as developmental delay in 8 of 10 individuals, although, again, the severity of these delays varies widely from mild to severe (individual 7).…”

Section: Discussionmentioning

confidence: 71%

Pathogenic variants in SMARCA5 , a chromatin remodeler, cause a range of syndromic neurodevelopmental features

et al. 2021

Self Cite

View full text Add to dashboard Cite

Intellectual disability encompasses a wide spectrum of neurodevelopmental disorders, with many linked genetic loci. However, the underlying molecular mechanism for more than 50% of the patients remains elusive. We describe pathogenic variants in SMARCA5, encoding the ATPase motor of the ISWI chromatin remodeler, as a cause of a previously unidentified neurodevelopmental disorder, identifying 12 individuals with de novo or dominantly segregating rare heterozygous variants. Accompanying phenotypes include mild developmental delay, frequent postnatal short stature and microcephaly, and recurrent dysmorphic features. Loss of function of the SMARCA5 Drosophila ortholog Iswi led to smaller body size, reduced sensory dendrite complexity, and tiling defects in larvae. In adult flies, Iswi neural knockdown caused decreased brain size, aberrant mushroom body morphology, and abnormal locomotor function. Iswi loss of function was rescued by wild-type but not mutant SMARCA5. Our results demonstrate that SMARCA5 pathogenic variants cause a neurodevelopmental syndrome with mild facial dysmorphia.

show abstract

“…2 ) [ 208 ]. Patients with CHD3 mutations are only very recently identified with Snijders Blok–Campeau syndrome, which is characterized by ID (with a wide range of severity), developmental delays, macrocephaly, impaired speech and language skills, and characteristic facial features [ 209 , 210 ].…”

Section: Epigenetic Modulation During Neurodevelopment and Diseasementioning

confidence: 99%

The emerging role of chromatin remodelers in neurodevelopmental disorders: a developmental perspective

Mossink

Negwer

Schubert

et al. 2020

Cell. Mol. Life Sci.

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Neurodevelopmental disorders (NDDs), including intellectual disability (ID) and autism spectrum disorders (ASD), are a large group of disorders in which early insults during brain development result in a wide and heterogeneous spectrum of clinical diagnoses. Mutations in genes coding for chromatin remodelers are overrepresented in NDD cohorts, pointing towards epigenetics as a convergent pathogenic pathway between these disorders. In this review we detail the role of NDD-associated chromatin remodelers during the developmental continuum of progenitor expansion, differentiation, cell-type specification, migration and maturation. We discuss how defects in chromatin remodelling during these early developmental time points compound over time and result in impaired brain circuit establishment. In particular, we focus on their role in the three largest cell populations: glutamatergic neurons, GABAergic neurons, and glia cells. An in-depth understanding of the spatiotemporal role of chromatin remodelers during neurodevelopment can contribute to the identification of molecular targets for treatment strategies.

show abstract

A second cohort of CHD3 patients expands the molecular mechanisms known to cause Snijders Blok-Campeau syndrome

Cited by 26 publications

References 14 publications

Pathogenic variants inSMARCA5, a chromatin remodeler, cause a range of syndromic neurodevelopmental features

Pathogenic variants inSMARCA5, a chromatin remodeler, cause a range of syndromic neurodevelopmental features

Pathogenic variants in SMARCA5 , a chromatin remodeler, cause a range of syndromic neurodevelopmental features

The emerging role of chromatin remodelers in neurodevelopmental disorders: a developmental perspective

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