| Literature DB >> 27250922 |
Magalie S Leduc1, Zhiyv Niu1, Weimin Bi1,2, Wenmiao Zhu2, Irene Miloslavskaya2, Theodore Chiang3, Haley Streff1, John R Seavitt1, Stephen A Murray4, Christine Eng1,2, Audrey Chan5, Yaping Yang1,2, Seema R Lalani1.
Abstract
Mutations in CRIPT encoding cysteine-rich PDZ domain-binding protein are rare, and to date have been reported in only two patients with autosomal recessive primordial dwarfism and distinctive facies. Here, we describe a female with biallelic mutations in CRIPT presenting with postnatal growth retardation, global developmental delay, and dysmorphic features including frontal bossing, high forehead, and sparse hair and eyebrows. Additional clinical features included high myopia, admixed hyper- and hypopigmented macules primarily on the face, arms, and legs, and syndactyly of 4-5 toes bilaterally. Using whole exome sequencing (WES) and chromosomal microarray analysis (CMA), we detected a c.8G>A (p.C3Y) missense variant in exon 1 of the CRIPT gene inherited from the mother and a 1,331 bp deletion encompassing exon 1, inherited from the father. The c.8G>A (p.C3Y) missense variant in CRIPT was apparently homozygous in the proband due to the exon 1 deletion. Our findings illustrate the clinical utility of combining WES with copy number variant (CNV) analysis to provide a molecular diagnosis to patients with rare Mendelian disorders. Our findings also illustrate the clinical spectrum of CRIPT related mutations.Entities:
Keywords: CRIPT mutation; genome wide microarray; microcephaly; postnatal growth retardation; whole exome sequencing
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Year: 2016 PMID: 27250922 PMCID: PMC5725961 DOI: 10.1002/ajmg.a.37780
Source DB: PubMed Journal: Am J Med Genet A ISSN: 1552-4825 Impact factor: 2.802