Abstract
Synpolydactyly type 1 (SPD1, OMIM 186000) is inherited as autosomal dominant and is caused by HOXD13 mutations. The condition is rare and is known for its phenotypic heterogeneity. In the homozygous state, the phenotype is generally more severe and is characterized by three main features: a more severe degree of syndactyly, a more severe degree of brachydactyly, and the frequent loss of the normal tubular shape of the metacarpals/metatarsals. Due to the phenotypic heterogeneity and the phenotypic overlap with other types of syndactyly, no pathognomonic feature has been described for the homozygous phenotype of SPD1. In the current communication, the author reviews the literature on the phenotypes of SPD1 in homozygous patients. The review documents that not all homozygous patients show a severe hand phenotype. The review also defines the “relatively long and medially deviated big toe with/without cupping of the forefoot” as a pathognomonic feature in the phenotype. Illustration of this feature is done through a demonstrative clinical report in a multigeneration family with SPD1 and HOXD13 polyalanine repeat expansion. Finally, the pathogenesis of the clinical features is reviewed.
Highlights
Type 1 (SPD1) is inherited as autosomal dominant and is caused by HOXD13 mutations
Malik and Grzeschik [2] stressed on the extreme phenotypic heterogeneity in Synpolydactyly type 1 (SPD1) and classified the clinical variants into three categories according to the degree of severity of the phenotype: heterozygous patients showing a very mild phenotype, patients with classic SPD1 features, and homozygous patients with severe phenotypes
Al-Qattan [3] stressed on the three main features of the homozygous phenotype: syndactyly frequently involves the postaxial three or four digits, a more severe degree of concurrent brachydactyly, and the frequent loss of the normal tubular shapes of the metacarpals/metatarsals
Summary
Due to the phenotypic heterogeneity and the phenotypic overlap with other types of syndactyly, no pathognomonic feature has been described for the homozygous phenotype of SPD1. The author reviews the literature on the phenotypes of SPD1 in homozygous patients. The review documents that not all homozygous patients show a severe hand phenotype. The review defines the “relatively long and medially deviated big toe with/without cupping of the forefoot” as a pathognomonic feature in the phenotype. Illustration of this feature is done through a demonstrative clinical report in a multigeneration family with SPD1 and HOXD13 polyalanine repeat expansion.
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