# Genetics of Waardenburg Syndrome in Africa: A Systematic Review

**Authors:** Elvis Twumasi Aboagye, Ramses Peigou Wonkam, Carmen de Kock, Collet Dandara, Ambroise Wonkam

PMC · DOI: 10.3390/ijms27010127 · International Journal of Molecular Sciences · 2025-12-22

## TL;DR

This study reviews the genetics and clinical features of Waardenburg Syndrome in Africa, finding that WS2 is the most common type, with PAX3 and SOX10 being the main genetic causes.

## Contribution

The first systematic review of Waardenburg Syndrome in Africa, highlighting the genetic and clinical landscape specific to the region.

## Key findings

- WS type 2 is the most common subtype in Africa, with no dystopia canthorum.
- PAX3 and SOX10 are the most frequently mutated genes in African WS cases.
- South Africa and Tunisia report the highest number of WS cases in Africa.

## Abstract

Waardenburg syndrome (WS) represents a group of genetic conditions characterized by auditory and pigmentation defects. Pathogenic variants in PAX3, MITF, SOX10, EDN3, EDNRB, SNAI2, and KITLG genes have been associated with WS across multiple populations; a comprehensive study of WS in Africa has not yet been reported. We conducted a systematic review of clinical expressions and genetics of WS across Africa. The Preferred Reporting Items for Systematic Reviews and Meta-Analysis (PRISMA) guidelines were followed, and the study protocol was registered on PROSPERO, the International Prospective Register of Systematic Reviews (2025 CRD420250655744). A literature search was performed on Google Scholar, PubMed, Scopus, Directory of Open Access Journals (DOAJ), Global Index Medicus, African-Wide Information, ScienceDirect, Connecting Repositories (CORE), and the Web of Science databases. We reviewed a total of 15 articles describing 84 WS cases, which showed no gender bias and a mean age at reporting of 17.5 years. Congenital, sensorineural, and profound hearing loss was described in most cases (66.7%; n = 56/84). WS type 2 (WS2), with characteristically no dystopia canthorum, is the predominant subtype (36.9%; n = 31/84). Pathogenic variants in four WS known genes, i.e., PAX3 (13 families), SOX10 (7 families), EDNRB (4 families), and EDN3 (1 family), were reported in Morocco, Tunisia, and South Africa. One candidate gene (PAX8) was described in one family in Ghana. Two non-syndromic hearing loss (NSHL) genes (BDP1 and MYO6) were reported in two separate families in South Africa, suggesting a possible phenotypic expansion. The highest number of WS cases was described in South Africa (38.1%; n = 32/84) and Tunisia (26.2%; n = 22/84). Gene variants were missense (27/43), deletion (7/43), splicing (5/43), nonsense (2/43), indel (1/43), and duplication (1/43), chiefly segregating in an autosomal dominant inheritance mode. There was no functional data to support the pathogenicity of putative causative variants. This review showed that WS2 is the most common in Africa. Variants in PAX3 and SOX10 were the predominant genetic causes. This study emphasizes the need to further investigate in-depth clinical characterization, molecular landscape, and the pathobiology of WS in Africa.

## Linked entities

- **Genes:** PAX3 (paired box 3) [NCBI Gene 5077], MITF (melanocyte inducing transcription factor) [NCBI Gene 4286], SOX10 (SRY-box transcription factor 10) [NCBI Gene 6663], EDN3 (endothelin 3) [NCBI Gene 1908], EDNRB (endothelin receptor type B) [NCBI Gene 1910], SNAI2 (snail family transcriptional repressor 2) [NCBI Gene 6591], KITLG (KIT ligand) [NCBI Gene 4254], PAX8 (paired box 8) [NCBI Gene 7849], BDP1 (BDP1 general transcription factor IIIB subunit) [NCBI Gene 55814], MYO6 (myosin VI) [NCBI Gene 4646]
- **Diseases:** Waardenburg Syndrome (MONDO:0018094), non-syndromic hearing loss (MONDO:0019497)

## Full-text entities

- **Genes:** PAX3 (paired box 3) [NCBI Gene 5077] {aka CDHS, HUP2, PAX-3, WS1, WS3}, EDNRB (endothelin receptor type B) [NCBI Gene 1910] {aka ABCDS, ET-B, ET-BR, ETB, ETB1, ETBR}, MYO6 (myosin VI) [NCBI Gene 4646] {aka DFNA22, DFNB37}, PAX8 (paired box 8) [NCBI Gene 7849] {aka PAX-8}, SNAI2 (snail family transcriptional repressor 2) [NCBI Gene 6591] {aka SLUG, SLUGH, SLUGH1, SNAIL2, WS2D}, SOX10 (SRY-box transcription factor 10) [NCBI Gene 6663] {aka DOM, PCWH, SOX-10, WS2E, WS4, WS4C}, EDN3 (endothelin 3) [NCBI Gene 1908] {aka ET-3, ET3, HSCR4, PPET3, WS4B}, BDP1 (BDP1 general transcription factor IIIB subunit) [NCBI Gene 55814] {aka DFNB112, HSA238520, TAF3B1, TFC5, TFIIIB'', TFIIIB150}, MITF (melanocyte inducing transcription factor) [NCBI Gene 4286] {aka CMM8, COMMAD, MI, MITF-A, WS2, WS2A}, KITLG (KIT ligand) [NCBI Gene 4254] {aka DCUA, DFNA69, FPH2, FPHH, KL-1, Kitl}
- **Diseases:** auditory and pigmentation defects (MESH:D010859), WS (MESH:D014849), Congenital, sensorineural, and profound hearing loss (MESH:D006319), WS type 2 (MESH:C536463), NSHL (MESH:C537845)

## Full text

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## Figures

4 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12785251/full.md

## References

62 references — full list in the complete paper: https://tomesphere.com/paper/PMC12785251/full.md

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Source: https://tomesphere.com/paper/PMC12785251