Waardenburg syndrome type 4: report of two new cases caused by SOX10 mutations in Spain.

[hirschsprung disease]

Shah-Waardenburg syndrome or Waardenburg syndrome type 4 (WS 4 ) is a neurocristopathy characterized by the association of deafness , depigmentation and Hirschsprung disease . Three disease-causing genes have been identified so far for WS 4 : EDNRB , EDN 3 , and SOX 10 . SOX 10 mutations , found in 45 -55 % of WS 4 patients , are inherited in autosomal dominant way . In addition , mutations in SOX 10 are also responsible for an extended syndrome involving peripheral and central neurological phenotypes , referred to as PCWH (peripheral demyelinating neuropathy , central dysmyelinating leucodystrophy , Waardenburg syndrome , Hirschsprung disease ). Such mutations are mostly private , and a high intra- and inter-familial variability exists . In this report , we present a patient with WS 4 and a second with PCWH due to SOX 10 mutations supporting again the genetic and phenotypic heterogeneity of these syndromes . Interestingly , the WS 4 family carries an insertion of 19 nucleotides in exon 5 of SOX 10 , which results in distinct phenotypes along three different generations : hypopigmentation in the maternal grandmother , hearing loss in the mother , and WS 4 in the proband . Since mosaicism can not explain the three different related-WS features observed in this family , we propose as the most plausible explanation the existence of additional molecular events , acting in an additive or multiplicative fashion , in genes or regulatory regions unidentified so far . On the other hand , the PCWH case was due to a de novo deletion in exon 5 of the gene . Efforts should be devoted to unravel the mechanisms underlying the intrafamilial phenotypic variability observed in the families affected , and to identify new genes responsible for the still unsolved WS 4 cases .