Indirect exclusion of four candidate genes for generalized progressive retinal atrophy in several breeds of dogs

Author:

Lippmann Tanja,Pasternack Sandra M,Kraczyk Britta,Dudek Sabine E,Dekomien Gabriele

Abstract

Abstract Background Generalized progressive retinal atrophy (gPRA) is a hereditary ocular disorder with progressive photoreceptor degeneration in dogs. Four retina-specific genes, ATP binding cassette transporter retina (ABCA 4), connexin 36 (CX 36), c-mer tyrosin kinase receptor (MERTK) and photoreceptor cell retinol dehydrogenase (RDH 12) were investigated in order to identify mutations leading to autosomal recessive (ar) gPRA in 29 breeds of dogs. Results Mutation screening was performed initially by PCR and single strand conformation polymorphism (SSCP) analysis, representing a simple method with comparatively high reliability for identification of sequence variations in many samples. Conspicuous banding patterns were analyzed via sequence analyses in order to detect the underlying nucleotide variations. No pathogenetically relevant mutations were detected in the genes ABCA 4, CX 36, MERTK and RDH 12 in 71 affected dogs of 29 breeds. Yet 30 new sequence variations were identified, both, in the coding regions and intronic sequences. Many of the sequence variations were in heterozygous state in affected dogs. Conclusion Based on the ar transmittance of gPRA in the breeds investigated, informative sequence variations provide evidence allowing indirect exclusion of pathogenetic mutations in the genes ABCA 4 (for 9 breeds), CX 36 (for 12 breeds), MERTK (for all 29 breeds) and RDH 12 (for 9 breeds).

Publisher

Springer Science and Business Media LLC

Subject

General Pharmacology, Toxicology and Pharmaceutics,General Biochemistry, Genetics and Molecular Biology,General Medicine

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