Peer-reviewed veterinary case report
Gene changes found in dog mouth melanomas and healthy tissue
By Stell, Anneliese J et al.·Published in American journal of veterinary research·2009·Royal Veterinary College, United Kingdom·View original on PubMed →
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Original publication title: Evaluation of variants of melanoma-associated antigen genes and mRNA transcripts in melanomas of dogs.
- Species:
- dog
Plain-English summary
A group of 18 dogs with malignant melanoma, a type of skin cancer, was studied to understand the genetic changes associated with their tumors. Researchers found specific gene variants in the melanoma tissues that could help in developing targeted treatments. Notably, a unique variant of the tyrosinase gene was only present in the melanoma samples, suggesting it might be a good target for future immunotherapy. One Great Dane in the study had a mutation linked to its coat color, but the genetic changes did not seem to affect the pigmentation of the tumors.
People also search for: dog melanoma treatment · Great Dane skin cancer · melanoma gene variants in dogs · immunotherapy for dog cancer · dog skin problems melanoma
Abstract
OBJECTIVE-To characterize variability in melanoma-associated antigen (MAA) genes and gene expression in melanomas of dogs. ANIMALS-18 dogs with malignant melanomas and 8 healthy control dogs. PROCEDURES-cDNA was prepared from malignant melanoma biopsy specimens and from pigmented oral mucocutaneous tissues of healthy control dogs. Genomic DNA was extracted from poorly pigmented melanomas. A PCR assay was performed by use of Melan-A, SILV, or tyrosinase-specific primers. RESULTS-Splice variants of Melan-A and SILV were identified in malignant melanomas and also in healthy pigmented tissues, whereas a tyrosinase splice variant was detected in melanoma tissues only. A short interspersed nuclear element (SINE) insertion mutation was identified in the SILV gene in 1 of 10 poorly pigmented melanomas. Six novel exonic single nucleotide polymorphisms (SNPs; 3 synonymous and 3 nonsynonymous) were detected in the tyrosinase gene, and 1 nonsynonymous exonic SNP was detected in the SILV gene. CONCLUSIONS AND CLINICAL RELEVANCE-Variants of MAA mRNA were detected in malignant melanoma tissues of dogs. The importance of MAA alternative transcripts expressed in melanomas and normal pigmented tissues was unclear, but they may have represented a means of regulating melanin synthesis. The tyrosinase splice variant was detected only in melanomas and could potentially be a tumor-specific target for immunotherapy. A SILV SINE insertion mutation was identified in a melanoma from a Great Dane, a breed known to carry this mutation (associated with merle coat color). The nonsynonymous SNPs detected in tyrosinase and SILV transcripts did not appear to affect tumor pigmentation.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/19951123/