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Peer-reviewed veterinary case report

Genome changes in dog mammary tumors found in blood DNA

By Beck, Julia et al.·Published in PloS one·2013·Chronix Biomedical, Germany·View original on PubMed

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Original publication title: Genome aberrations in canine mammary carcinomas and their detection in cell-free plasma DNA.

Species:
dog

Plain-English summary

A 7-year-old female dog with a mammary tumor was studied to understand the genetic changes associated with this common cancer. Researchers found various genetic abnormalities in the tumor cells, including deletions and fusions of DNA that affect important cancer-related genes. They also discovered that tumor-specific DNA could be detected in the dog's blood, even more than a year after surgery, indicating the potential for metastasis (spread of cancer). This research helps in understanding canine mammary tumors better and may lead to improved methods for monitoring and detecting cancer in dogs.

People also search for: dog mammary tumor symptoms · canine cancer blood test · dog breast cancer treatment

Abstract

Mammary tumors are the most frequent cancers in female dogs exhibiting a variety of histopathological differences. There is lack of knowledge about the genomes of these common dog tumors. Five tumors of three different histological subtypes were evaluated. Massive parallel sequencing (MPS) was performed in comparison to the respective somatic genome of each animal. Copy number and structural aberrations were validated using droplet digital PCR (ddPCR). Using mate-pair sequencing chromosomal aneuploidies were found in two tumors, frequent smaller deletions were found in one, inter-chromosomal fusions in one other, whereas one tumor was almost normal. These aberrations affect several known cancer associated genes such as cMYC, and KIT. One common deletion of the proximal end of CFA27, harboring the tumor suppressor gene PFDN5 was detected in four tumors. Using ddPCR, this deletion was validated and detected in 50% of tumors (N = 20). Breakpoint specific dPCRs were established for four tumors and tumor specific cell-free DNA (cfDNA) was detected in the plasma. In one animal tumor-specific cfDNA was found >1 year after surgery, attributable to a lung metastasis. Paired-end sequencing proved that copy-number imbalances of the tumor are reflected by the cfDNA. This report on chromosomal instability of canine mammary cancers reveals similarities to human breast cancers as well as special canine alterations. This animal model provides a framework for using MPS for screening for individual cancer biomarkers with cost effective confirmation and monitoring using ddPCR. The possibility exists that ddPCR can be expanded to screening for common cancer related variants.

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Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/24098698/