Phenotypic similarities and differences in patients with a p.Met112Ile mutation in SOX10.

[hirschsprung disease]

Waardenburg syndrome (WS ) is characterized by an association of pigmentation abnormalities and sensorineural hearing loss . Four types , defined on clinical grounds , have been delineated , but this phenotypic classification correlates imperfectly with known molecular anomalies . SOX 10 mutations have been found in patients with type II and type IV WS (i .e ., with Hirschsprung disease ), more complex syndromes , and partial forms of the disease . The phenotype induced by SOX 10 mutations is highly variable and , except for the neurological forms of the disease , no genotype-phenotype correlation has been characterized to date . There is no mutation hotspot in SOX 10 and most cases are sporadic , making it particularly difficult to correlate the phenotypic and genetic variability . This study reports on three independent families with SOX 10 mutations predicted to result in the same missense mutation at the protein level (p .Met 112 Ile ), offering a rare opportunity to improve our understanding of the mechanisms underlying phenotypic variability . The pigmentation defects of these patients are very similar , and the neurological symptoms showed a somewhat similar evolution over time , indicating a potential partial genotype-phenotype correlation . However , variability in gastrointestinal symptoms suggests that other genetic factors contribute to the expression of these phenotypes . No correlation between the rs 2435357 polymorphism of RET and the expression of Hirschsprung disease was found . In addition , one of the patients has esophageal achalasia , which has rarely been described in WS .