A novel compound heterozygous BEST1 gene mutation in two siblings causing autosomal recessive bestrophinopathy

Obaid Imtiyazul Haque; Anbukayalvizhi Chandrasekaran; Faisal Nabi; Owais Ahmad; João Pedro Marques; Tanweer Ahmad

doi:10.1186/s12886-022-02703-5

A novel compound heterozygous BEST1 gene mutation in two siblings causing autosomal recessive bestrophinopathy

BMC Ophthalmol. 2022 Dec 16;22(1):493. doi: 10.1186/s12886-022-02703-5.

Authors

Obaid Imtiyazul Haque¹, Anbukayalvizhi Chandrasekaran², Faisal Nabi³, Owais Ahmad⁴, João Pedro Marques⁵, Tanweer Ahmad⁶

Affiliations

¹ Massachusetts General Hospital, Harvard Medical School, Boston, USA. oihaque@myamu.ac.in.
² MedGenome Labs Limited, Bengaluru, India.
³ Interdisciplinary Biotechnology Unit, Aligarh Muslim University, Aligarh, India.
⁴ Department of Microbiology and Cell Biology, Indian Institute of Science, Bangalore, India.
⁵ Ophthalmology Unit, Centro Hospitalar E Universitário de Coimbra (CHUC), Coimbra, Portugal.
⁶ Northampton General Hospital, Northampton, UK.

Abstract

Purpose: To describe the clinical features, imaging characteristics, and genetic test results associated with a novel compound heterozygous mutation of the BEST1 gene in two siblings with autosomal recessive bestrophinopathy.

Methods: Two siblings underwent a complete ophthalmic examination, including dilated fundus examination, fundus photography, fundus autofluorescence imaging, spectral-domain optical coherence tomography, fluorescein angiography, electroretinography, and electrooculography. A clinical diagnosis of autosomal recessive bestrophinopathy was established based on ocular examination and multimodal retinal imaging. Subsequently, clinical exome sequencing consisting of a panel of 6670 genes was carried out to confirm the diagnosis and assess genetic alterations in the protein-coding region of the genome of the patients. The identified mutations were tested in the two affected siblings and one of their parents.

Results: Two siblings (a 17-year-old female and a 15-year-old male) presented with reduced visual acuity and bilaterally symmetrical subretinal deposits of hyperautofluorescent materials in the posterior pole, which showed staining in the late phase of fluorescein angiogram. Spectral-domain optical coherence tomography demonstrated hyperreflective subretinal deposits and subretinal fluid accumulation. Both patients shared two mutations in the protein-coding region of the BEST1 gene, c.103G > A, p.(Glu35Lys) and c.313C > A, p.(Arg105Ser) (a novel disease-causing mutation). Sanger sequencing confirmed that the unaffected mother of the proband was carrying p.(Glu35Lys) variant in a heterozygous state.

Conclusions: We have identified and described the phenotype of a novel disease-causing mutation NM_004183.4:c.313C > A, p.(Arg105Ser) in a heterozygous state along with a previously reported mutation NM_004183.4:c.103G > A, p.(Glu35Lys) of the BEST1 gene in two related patients with autosomal recessive bestrophinopathy.

Keywords: Autosomal recessive bestrophinopathy; BEST1; Bestrophin-1; Genetics; Inherited retinal dystrophy.

Publication types

Case Reports

MeSH terms

Bestrophins / genetics
Chloride Channels / genetics
DNA Mutational Analysis
Electroretinography
Eye Proteins / genetics
Female
Fluorescein Angiography
Humans
Male
Mutation
Pedigree
Retinal Diseases* / diagnosis
Retinal Diseases* / genetics
Retinal Dystrophies*
Siblings
Tomography, Optical Coherence

Substances

Bestrophins
Eye Proteins
Chloride Channels
BEST1 protein, human

Supplementary concepts

Bestrophinopathy