Neonatal-Onset Congenital Ectropion Uveae May Be Caused by a Distinct CYP1B1 Pathologic Variant

Sushmita Kaushik; Sandeep Choudhary; Anupriya Kaur; Priyanka Srivastava; Bikrant Pokharel; Madhuri Akella; Surinder Singh Pandav

doi:10.1016/j.ajo.2022.01.014

Neonatal-Onset Congenital Ectropion Uveae May Be Caused by a Distinct CYP1B1 Pathologic Variant

Am J Ophthalmol. 2022 Jul:239:54-65. doi: 10.1016/j.ajo.2022.01.014. Epub 2022 Jan 24.

Authors

Sushmita Kaushik¹, Sandeep Choudhary², Anupriya Kaur², Priyanka Srivastava², Bikrant Pokharel², Madhuri Akella², Surinder Singh Pandav²

Affiliations

¹ From the Advanced Eye Center and Advanced Pediatric Center, Postgraduate Institute of Medical Education and Research, Chandigarh, India. Electronic address: sushmita_kaushik@yahoo.com.
² From the Advanced Eye Center and Advanced Pediatric Center, Postgraduate Institute of Medical Education and Research, Chandigarh, India.

PMID: 35085548
DOI: 10.1016/j.ajo.2022.01.014

Abstract

Purpose: To report underlying genetic variants of recently described distinct phenotype of newborn glaucoma: neonatal-onset congenital ectropion uveae (NO-CEU).

Design: Prospective cohort study.

Methods: Setting: tertiary care teaching institute.

Subjects: Thirteen children with clinical diagnosis of NO-CEU who had completed 1-year follow-up after glaucoma surgery and had undergone clinical exome sequencing (CES) by selective capture and sequencing of the protein-coding regions of the genes including 19 candidate genes for NO-CEU were assessed. The same criteria were applied for evaluating pathogenicity of variants to all the candidate genes.

Outcome measures: primary-genetic variants found on CES keeping in view the clinical indication of congenital glaucoma; secondary-corneal clarity and intraocular pressure (IOP) at baseline and 1-year follow-up, interventions required to control IOP, and postoperative visual acuity. The genetic variants were correlated with the outcome.

Results: All 13 patients diagnosed with NO-CEU had onset of glaucoma at birth and severe bilateral disease. Twelve of 13 (92.3%) patients harbored CYP1B1 variants. Nine of these 12 patients (83.3%) were homozygous for [c.1169G>A(p.Arg390His)] in exon-3 of CYP1B, with 5 common homozygous single-nucleotide polymorphisms flanking the pathogenic variant. They had intractable glaucoma and required multiple surgeries. Six patients had persistent corneal opacities, necessitating optical iridectomies. Three patients were compound heterozygous for CYP1B1 variants, showing [c.1169G>A(p.Arg390His)] along with [c.1103G>A(p.Arg368His)], [c.1103G>A (p.Arg368His)] along with [c.1403_1429dup(p.Arg468_Ser476dup)], and [(c.1063C>T(p.Arg355Ter)] along with [c.1325del(p.Pro442GlnfsTer15)]. These patients had better visual outcomes.

Conclusions: NO-CEU appears to be a phenotypic marker for specific CYP1B1 genotypes, one of which is [c.1169G>A(p.Arg390His)] in our study population. Phenotype recognition is helpful to characterize the underlying genetic variants.

MeSH terms

Cytochrome P-450 CYP1B1 / genetics
DNA Mutational Analysis
Ectropion* / congenital
Ectropion* / genetics
Glaucoma* / diagnosis
Glaucoma* / genetics
Glaucoma* / surgery
Humans
Hydrophthalmos* / diagnosis
Hydrophthalmos* / genetics
Hydrophthalmos* / surgery
Infant, Newborn
Intraocular Pressure
Mutation
Prospective Studies

Substances

CYP1B1 protein, human
Cytochrome P-450 CYP1B1