# Oculocutaneous albinism in a patient with an OCA2 variant: molecular and clinical insights

**Authors:** Mostafa Neissi, Sahar Kareem Al-Mozani, Ayoob Radhi Al-Zaalan, Samaneh Sanavi Shiri, Motahareh Sheikh-Hosseini, Adnan Issa Al-Badran, Elaheh Nekouei

PMC · DOI: 10.2478/abm-2025-0019 · 2025-06-30

## TL;DR

A new OCA2 gene variant causing albinism is identified in an Iranian family, providing insights into its molecular and clinical effects.

## Contribution

A novel homozygous missense variant in the OCA2 gene is identified and analyzed for its role in oculocutaneous albinism.

## Key findings

- A novel OCA2 variant, c.1274T>G (p.Met425Arg), was identified as the cause of albinism in a consanguineous Iranian family.
- The variant is predicted to be pathogenic based on bioinformatics and structural modeling analyses.
- The study confirms autosomal recessive inheritance with both parents as heterozygous carriers.

## Abstract

Albinism is a rare genetic condition characterized by hypopigmentation of the skin, hair, and eyes, as well as visual impairments. Oculocutaneous albinism type 2 (OCA2) is commonly associated with variants in the OCA2 gene, which encodes a protein critical for melanosomal pH regulation and melanin biosynthesis. Exome sequencing, validated by Sanger sequencing, was employed to investigate the genetic basis of albinism in a consanguineous Iranian family. Bioinformatics analyses and structural modeling were conducted to assess the pathogenicity and impact of the detected variant.

A 27-year-old male from a consanguineous Iranian family presented with features of oculocutaneous albinism, including white hair, blue eyes, strabismus, sun-sensitive skin, reduced visual acuity, and significant photophobia, resulting in functional limitations in bright environments. Genetic analysis identified a novel homozygous missense variant in the OCA2 gene, NM_000275.3:c.1274T>G (p.Met425Arg), located in exon 13. The genomic coordinates of the variant are chr15:g.27985154A>C (GRCh38/hg38). In silico tools classified the variant as likely pathogenic based on its evolutionary conservation, absence in population databases, and structural modeling predictions. Segregation analysis confirmed autosomal recessive inheritance, with both parents being heterozygous carriers.

The identified OCA2 variant, c.1274T>G; p.Met425Arg, disrupts protein function, impairing melanosomal activity and melanin biosynthesis. This study underscores the importance of genetic analysis in characterizing OCA2 variants and highlights the need for further exploration of molecular mechanisms and phenotypic variability in OCA2-related albinism to improve diagnosis and counseling.

## Linked entities

- **Genes:** OCA2 (OCA2 melanosomal transmembrane protein) [NCBI Gene 4948]
- **Diseases:** oculocutaneous albinism (MONDO:0018910), albinism (MONDO:0043209)

## Full-text entities

- **Genes:** LGR5 (leucine rich repeat containing G protein-coupled receptor 5) [NCBI Gene 8549] {aka FEX, GPR49, GPR67, GRP49, HG38}, SLC45A2 (solute carrier family 45 member 2) [NCBI Gene 51151] {aka 1A1, AIM1, MATP, OCA4, SHEP5}, OCA2 (OCA2 melanosomal transmembrane protein) [NCBI Gene 4948] {aka BEY, BEY1, BEY2, BOCA, D15S12, EYCL}, SLC24A2 (solute carrier family 24 member 2) [NCBI Gene 25769] {aka NCKX2}, GLDC (glycine decarboxylase) [NCBI Gene 2731] {aka GCE, GCE1, GCSP, HYGN1}, MITF (melanocyte inducing transcription factor) [NCBI Gene 4286] {aka CMM8, COMMAD, MI, MITF-A, WS2, WS2A}, MC1R (melanocortin 1 receptor) [NCBI Gene 4157] {aka CMM5, MSH-R, SHEP2}, MYBPH (myosin binding protein H) [NCBI Gene 4608], ACP1 (acid phosphatase 1) [NCBI Gene 52] {aka HAAP, LMW-PTP, LMWPTP}, SLC24A5 (solute carrier family 24 member 5) [NCBI Gene 283652] {aka JSX, NCKX5, OCA6, SHEP4}, TYRP1 (tyrosinase related protein 1) [NCBI Gene 7306] {aka CAS2, CATB, GP75, OCA3, TRP, TRP1}, GCSH (glycine cleavage system protein H) [NCBI Gene 2653] {aka GCE, MMDS7, NKH}, TYR (tyrosinase) [NCBI Gene 7299] {aka ATN, CMM8, OCA1, OCA1A, OCAIA, SHEP3}
- **Diseases:** reduced visual acuity (MESH:D014786), related (MESH:D019973), OCA type 2 (MESH:C537730), OCA (MESH:D016115), deviation of the right eye (MESH:D010262), nystagmus (MESH:D009759), blue (MESH:D018329), foveal hypoplasia (MESH:C537858), photophobia (MESH:D020795), strabismus (MESH:D013285), Albinism (MESH:D000417), OA (MESH:D016117), coagulation (MESH:D001778), malignancies (MESH:D009369), pigmentation (MESH:D010859), sunburn (MESH:D013471), skin damage (MESH:D012871), hypopigmentation (MESH:D017496), autosomal recessive disorders (MESH:D030342)
- **Chemicals:** Methionine (MESH:D008715), EDTA (MESH:D004492), melanin (MESH:D008543), eumelanin (MESH:C041877), agarose (MESH:D012685), pheomelanin (MESH:C018362)
- **Species:** Homo sapiens (human, species) [taxon 9606]
- **Mutations:** g.27985154 A>C, c.2020C>G, g.27985154A>C, methionine with arginine, c.1762C>T, S192Y, c.593C>T, p.Ser820Pro, c.1274T>G, p.Met425Arg, p.Gly780Ser, c.1274T>G, c.1045-15T>G, thymine (T) to guanine (G) at position 1274, c.408_409delAA, p.Val443Ile, p.L374F, methionine (Met) to arginine (Arg) at position 425, p.Asn476Asp, T>G, c.2458T>C, p.R151C, p.R160W, Arg425, Met425, R402Q
- **Cell lines:** FATHMM-XF — Homo sapiens (Human), Transformed cell line (CVCL_2631)

## Figures

4 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12303592/full.md

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Source: https://tomesphere.com/paper/PMC12303592