Spectrum of CHD7 Mutations in 110 Individuals with CHARGE Syndrome and Genotype-Phenotype Correlation

Lalani, Seema R.; Safiullah, Arsalan M.; Fernbach, Susan; Harutyunyan, Karine C.; Thaller, Christina; Peterson, Leif E.; Mcpherson, John Douglas; Gibbs, Richard A.; White, Lisa D.; Hefner, Margaret A.; Davenport, Sandra L.H.; Graham, John M.; Bacino, Carlos A.; Glass, Nancy L.; Towbin, Jeffrey A.; Craigen, William J.; Neish, Steven R.; Lin, Angela E.; Belmont, John W.

doi:10.1086/500273

Cited by 355 publications

(383 citation statements)

References 33 publications

Supporting

Mentioning

357

Contrasting

Unclassified

Order By: Relevance

“…CHARGE syndrome is characterized by a non‐random clustering of a complex array of congenital malformations (Jongmans et al, 2006; Lalani et al, 2006; Pagon, Zonana, & Yong, 1981). The discovery of loss‐of‐function mutations in the CHD7 gene in patients with CHARGE syndrome (Janssen et al, 2012; Vissers et al, 2004), has led to significant progress in elucidating the developmental and molecular genetic mechanisms underlying specific phenotypes associated with CHARGE syndrome (Layman, Hurd, & Martin, 2010).…”

Section: Introductionmentioning

confidence: 99%

Distinct cerebellar foliation anomalies in a CHD7 haploinsufficient mouse model of CHARGE syndrome

Whittaker

Kasah

Donovan

et al. 2017

American J of Med Genetics Pt C

View full text Add to dashboard Cite

Mutations in the gene encoding the ATP dependent chromatin‐remodeling factor, CHD7 are the major cause of CHARGE (Coloboma, Heart defects, Atresia of the choanae, Retarded growth and development, Genital‐urinary anomalies, and Ear defects) syndrome. Neurodevelopmental defects and a range of neurological signs have been identified in individuals with CHARGE syndrome, including developmental delay, lack of coordination, intellectual disability, and autistic traits. We previously identified cerebellar vermis hypoplasia and abnormal cerebellar foliation in individuals with CHARGE syndrome. Here, we report mild cerebellar hypoplasia and distinct cerebellar foliation anomalies in a Chd7 haploinsufficient mouse model. We describe specific alterations in the precise spatio‐temporal sequence of fissure formation during perinatal cerebellar development responsible for these foliation anomalies. The altered cerebellar foliation pattern in Chd7 haploinsufficient mice show some similarities to those reported in mice with altered Engrailed, Fgf8 or Zic1 gene expression and we propose that mutations or polymorphisms in these genes may modify the cerebellar phenotype in CHARGE syndrome. Our findings in a mouse model of CHARGE syndrome indicate that a careful analysis of cerebellar foliation may be warranted in patients with CHARGE syndrome, particularly in patients with cerebellar hypoplasia and developmental delay.

show abstract

Section: Introductionmentioning

confidence: 99%

Distinct cerebellar foliation anomalies in a CHD7 haploinsufficient mouse model of CHARGE syndrome

Whittaker

Kasah

Donovan

et al. 2017

American J of Med Genetics Pt C

View full text Add to dashboard Cite

show abstract

“…A variant in CHD7 can be found in over 90% of all children who fulfil the clinical diagnostic criteria. 6,[9][10][11] The CHD7 gene encodes a member of the chromodomain helicase DNA-binding protein family that regulates the transcription of genes during embryonic development. Haploinsufficiency of CHD7 affects multiple organ systems, including the heart, the inner ear and the eye.…”

Section: Introductionmentioning

confidence: 99%

CHARGE syndrome: a review of the immunological aspects

et al. 2015

View full text Add to dashboard Cite

CHARGE syndrome is caused by a dominant variant in the CHD7 gene. Multiple organ systems can be affected because of haploinsufficiency of CHD7 during embryonic development. CHARGE syndrome shares many clinical features with the 22q11.2 deletion syndrome. Immunological abnormalities have been described, but are generally given little attention in studies on CHARGE syndrome. However, structured information on immunological abnormalities in CHARGE patients is necessary to develop optimal guidelines for diagnosis, treatment and follow-up in these patients. Here, we provide an overview of the current literature on immunological abnormalities in CHARGE syndrome. We also explore immunological abnormalities in comparable multiple congenital anomaly syndromes to identify common immunological phenotypes and genetic pathways that might regulate the immune system. Finally, we aim to identify gaps in our knowledge on the immunological aspects in CHARGE syndrome that need further study.

show abstract

“…In most cases, de novo truncating mutations in the gene encoding the chromodomain helicase DNA binding protein 7 (CHD7), located on chromosome 8q12, cause the syndrome 2 . Mutations in the CHD7 gene have been demonstrated in 42-64% of cases 3 . The clinical diagnosis is made either if four major features are present, i.e.…”

Section: Charge Syndrome In a Fetus With A Large Paraesophageal Hernimentioning

confidence: 99%

CHARGE syndrome in a fetus with a large paraesophageal hernia presenting prenatally as esophageal atresia

Tempfer-Bentz

Troebs

Sonntag

et al. 2014

Ultrasound in Obstet & Gyne

View full text Add to dashboard Cite

Spectrum of CHD7 Mutations in 110 Individuals with CHARGE Syndrome and Genotype-Phenotype Correlation

Cited by 355 publications

References 33 publications

Distinct cerebellar foliation anomalies in a CHD7 haploinsufficient mouse model of CHARGE syndrome

Distinct cerebellar foliation anomalies in a CHD7 haploinsufficient mouse model of CHARGE syndrome

CHARGE syndrome: a review of the immunological aspects

CHARGE syndrome in a fetus with a large paraesophageal hernia presenting prenatally as esophageal atresia

Contact Info

Product

Resources

About