Expanding the phenotype for the recurrent p.Ala391Glu variant in FGFR3: Beyond crouzon syndrome and acanthosis nigricans

Expanding the phenotype for the recurrent p.Ala391Glu variant in FGFR3: Beyond crouzon syndrome and acanthosis nigricans

Background Craniosynostosis, or premature fusion of the skull sutures, is a group of disorders that can present in isolation (nonsyndromic) or be associated with other anomalies (syndromic). Delineation of syndromic craniosynostosis is confounded due to phenotypic overlap, variable expression as wel...

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Bibliographic Details
Published in:Molecular genetics & genomic medicine Vol. 7; no. 6; pp. e656 - n/a
Main Authors: Rymer, Karen, Shiang, Rita, Hsiung, Anting, Pandya, Arti, Bigdeli, Tim, Webb, Bradley T., Rhodes, Jennifer
Format: Journal Article
Language:English
Published: United States John Wiley & Sons, Inc 01-06-2019
John Wiley and Sons Inc
Wiley
Subjects:
Acanthosis nigricans
Acanthosis Nigricans - genetics
Adult
Amino acids
Anomalies
Brain
Child
Cranial sutures
Craniofacial Dysostosis - genetics
Craniosynostoses - genetics
Craniosynostosis
Crouzon
Crouzon syndrome
Diagnosis
DNA sequencing
Dysostosis
Ears & hearing
Female
FGFR3
Fibroblast growth factor receptors
Fingers & toes
Genomics
Genotype & phenotype
Hearing loss
Heterogeneity
Humans
Hypoplasia
Infant
Intellectual disabilities
Magnetic resonance imaging
Male
Nose
Original
Palate
Parents
Pfeiffer
Phenotype
Phenotypes
Point Mutation
Polymorphism, Single Nucleotide
Receptor, Fibroblast Growth Factor, Type 3 - genetics
Receptor, Fibroblast Growth Factor, Type 3 - metabolism
Skin
Stenosis
Crouzon
craniosynostosis
FGFR3
Pfeiffer
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Summary:Background Craniosynostosis, or premature fusion of the skull sutures, is a group of disorders that can present in isolation (nonsyndromic) or be associated with other anomalies (syndromic). Delineation of syndromic craniosynostosis is confounded due to phenotypic overlap, variable expression as well as molecular heterogeneity. We report on an infant who presented at birth with multisuture synostosis, turribrachycephaly, midface hypoplasia, beaked nose, low set ears, a high palate and short squat appearing thumbs, and great toes without deviation. The additional MRI findings of choanal stenosis and a Chiari I malformation suggested a diagnosis of Pfeiffer syndrome. First tier molecular testing did not reveal a pathogenic variant. Methods Whole exome sequencing on DNA samples from the proband and her unaffected parents was utilized to delineate the variant causative for the Pfeiffer syndrome diagnosis. Results On whole exome sequencing, a de novo NM_000142.4:c.1428C>A missense variant causing a p.Ala391Glu amino acid change in FGFR3 has been identified. The p.Ala391Glu change has been predominantly identified in patients with Crouzon syndrome with acanthosis nigricans. Conclusions This finding illustrates the first reported case of a child with an overlap with Pfeiffer syndrome to have the p.Ala391Glu variant. Delineation of syndromic craniosynostosis is confounded due to phenotypic overlap, variable expression as well as molecular heterogeneity. On whole exome sequencing, a de novo NM_000142.4:1428C>A missense variant causing a p.Ala391Glu amino acid change in FGFR3 has been identified. This finding illustrates the first reported case of a child with an overlap with Pfeiffer syndrome to have the p.Ala391Glu variant.
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ISSN:2324-9269
2324-9269
DOI:10.1002/mgg3.656