Literature DB >> 36239105

Whole-exome sequencing analysis in a case of primary congenital glaucoma due to the partial uniparental isodisomy.

Parisima Ghaffarian Zavarzadeh1, Morteza Bonyadi1, Zahra Abedi2.   

Abstract

We described a clinical, laboratory, and genetic presentation of a pathogenic variant of the CYP1B1 gene through a report of a case of primary congenital glaucoma and a trio analysis of this candidate variant in the family with the sanger sequencing method and eventually completed our study with the secondary/incidental findings. This study reports a rare case of primary congenital glaucoma, an 8-year-old female child with a negative family history of glaucoma and uncontrolled intraocular pressure. This case's whole-exome sequencing data analysis presents a homozygous pathogenic single nucleotide variant in the CYP1B1 gene (NM 000104:exon3:c.G1103A:p.R368H). At the same time, this pathogenic variant was obtained as a heterozygous state in her unaffected father but not her mother. The diagnosis was made based on molecular findings of whole-exome sequencing data analysis. Therefore, the clinical reports and bioinformatics findings supported the relation between the candidate pathogenic variant and the disease. However, it should not be forgotten that primary congenital glaucoma is not peculiar to the CYP1B1 gene. Since the chance of developing autosomal recessive disorders with low allele frequency and unrelated parents is extraordinary in offspring. However, further data analysis of whole-exome sequencing and sanger sequencing method were applied to obtain the type of mutation and how it was carried to the offspring.

Entities:  

Keywords:  CYP1B1; glaucoma; primary congenital; sequence analysis; whole-exome sequencing

Year:  2022        PMID: 36239105      PMCID: PMC9576475          DOI: 10.5808/gi.21044

Source DB:  PubMed          Journal:  Genomics Inform        ISSN: 1598-866X


  24 in total

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