A Mutation in the FAM83G Gene in Dogs with Hereditary Footpad Hyperkeratosis (HFH)

Hereditary footpad hyperkeratosis (hfh) represents a palmoplantar hyperkeratosis,which is inherited as a monogenic autosomal recessive trait in several dog breeds,such as e.g. kromfohrländer and irish terriers. we performed genome-wide association studies (gwas) in both breeds. in kromfohrländer we obtained a single strong association signal on chromosome 5 (praw = 1.0×10-13) using 13 hfh cases and 29 controls. the association signal replicated in an independent cohort of irish terriers with 10 cases and 21 controls (praw = 6.9×10-10). the analysis of shared haplotypes among the combined kromfohrländer and irish terrier cases defined a critical interval of 611 kb with 13 predicted genes. we re-sequenced the genome of one affected kromfohrländer at 23.5× coverage. the comparison of the sequence data with 46 genomes of non-affected dogs from other breeds revealed a single private non-synonymous variant in the critical interval with respect to the reference genome assembly. the variant is a missense variant (c.155g>c) in the fam83g gene encoding a protein with largely unknown function. it is predicted to change an evolutionary conserved arginine into a proline residue (p.r52p). we genotyped this variant in a larger cohort of dogs and found perfect association with the hfh phenotype. we further studied the clinical and histopathological alterations in the epidermis in vivo. affected dogs show a moderate to severe orthokeratotic hyperplasia of the palmoplantar epidermis. thus,our data provide the first evidence that fam83g has an essential role for maintaining the integrity of the palmoplantar epidermis. © 2014 drögemüller et al.