A novel classification system to predict the pathogenic effects of CHD7 missense variants in CHARGE syndrome

Bergman, Jorieke E. H.; Janssen, Nicole; Sloot, Almer M. van der; Walle, Hermien E. K. de; Schoots, Jeroen; Rendtorff, Nanna Dahl; Tranebjærg, Lisbeth; Hoefsloot, Lies H.; Ravenswaaij-Arts, Conny M. A. van; Hofstra, Robert

doi:10.1002/humu.22106

Cited by 65 publications

(51 citation statements)

References 69 publications

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“…Although we only have detailed information on the variant in CHD7 for 23 patients, the fact that all reported variants lead to a premature stop in CHD7 is interesting, because truncating CHD7 variants are in general associated with a more severe phenotype. 12 Are certain phenotypic features more common in our collected cohort?…”

Section: Immunological Abnormalities Reported In Charge Syndromementioning

confidence: 99%

“…There is no clear genotype-phenotype correlation, but variants leading to a premature stop codon are, in general, associated with a more severe phenotype than variants with a non-truncating effect, that is, missense variants. 12 Since the genetic cause of CHARGE syndrome was identified, its phenotype has been further explored. In addition to the above symptoms, other common clinical features of CHARGE syndrome are: absent or hypoplastic semicircular canals, cranial nerve dysfunction (including facial nerve palsy), cleft lip and/or palate, anosmia, feeding difficulties and skeletal abnormalities.…”

Section: Introductionmentioning

confidence: 99%

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CHARGE syndrome: a review of the immunological aspects

et al. 2015

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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.

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Section: Immunological Abnormalities Reported In Charge Syndromementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

CHARGE syndrome: a review of the immunological aspects

et al. 2015

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“…Some variants may be erroneously interpreted as disease-causing. An interpretation algorithm for missense variants has been published by Bergman et al 6 2.3 Clinical sensitivity (proportion of positive tests if the disease is present)…”

Section: Analytical Specificity (Proportion Of Negative Tests If the mentioning

confidence: 99%

“…The clinical specificity of these criteria is~85%, as 14-17% of the patients with a CHD7 disease-causing variant do not completely fulfill these criteria. 4 Bergman et al 6 defined criteria for CHD7 testing and showed that if these criteria were used the risk of not offering the test to a patient with a CHD7 disease-causing variant was extremely low. 4 But, it should be taken into account that the mild end of the phenotypic spectrum is still expanding.…”

Section: Analytical Specificity (Proportion Of Negative Tests If the mentioning

confidence: 99%

Clinical utility gene card for: CHARGE syndrome - update 2015

et al. 2015

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“…On the basis of the prediction programs (score +2) and de novo occurrence (score +3), this missense variant probably affects function according to the scoring classification published by Bergman. 15 In Patient 3, CHD7 sequencing revealed an intronic variant predicted to disrupt the exon 6 donor splice site (c.2442+5G4C; NM_017780.3; g.127819G4C; NG_007009.1). The same variant was present in his affected older brother 9 and their mildly affected father.…”

Section: Methodsmentioning

confidence: 98%

Prominent scapulae mimicking an inherited myopathy expands the phenotype of CHD7-related disease

O’Grady

Sival

et al. 2016

Eur J Hum Genet

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CHD7 variants are a well-established cause of CHARGE syndrome, a disabling multi-system malformation disorder that is often associated with deafness, visual impairment and intellectual disability. Less severe forms of CHD7-related disease are known to exist, but the full spectrum of phenotypes remains uncertain. We identified a de novo missense variant in CHD7 in a family presenting with musculoskeletal abnormalities as the main manifestation of CHD7-related disease, representing a new phenotype. The proband presented with prominent scapulae, mild shoulder girdle weakness and only subtle dysmorphic features. Investigation revealed hypoplasia of the trapezius and sternocleidomastoid muscles and semicircular canal defects, but he did not fulfill diagnostic criteria for CHARGE syndrome. Although the shoulders are often sloping and anteverted in CHARGE syndrome, the underlying neuromuscular cause has never been investigated. This report expands the phenotypes associated with CHD7 mutations to include a musculoskeletal presentation, with hypoplasia of the shoulder and neck muscles. CHD7 should be considered in patients presenting in childhood with stable scapular winging, particularly if accompanied by dysmorphic features and balance difficulties.

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A novel classification system to predict the pathogenic effects of CHD7 missense variants in CHARGE syndrome

Cited by 65 publications

References 69 publications

CHARGE syndrome: a review of the immunological aspects

CHARGE syndrome: a review of the immunological aspects

Clinical utility gene card for: CHARGE syndrome - update 2015

Prominent scapulae mimicking an inherited myopathy expands the phenotype of CHD7-related disease

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