Genomic analysis across 53 canine cancer types reveals novel mutations and high clinical actionability potential

Author:

Sakthikumar Sharadha1ORCID,Warrier Manisha1,Whitley Derick1,Facista Salvatore1,Adkins Jonathan1,Aman Sara1,Tsinajinnie Darwin1,Duran Natalie1,Siravegna Giulia1,Ahmed Zeeshan1,Day Kenneth1,Jenkins Brooklyn1,Patel Nidhi1,Ryden Kirk1ORCID,Nadai Joe1,Banovich Kathryn1,Powers Barbara1,Edwards Jeffrey1,Steinberg Jennifer2,Fielder Susan1,Wong Shukmei3,Byron Sara A.3,Izatt Tyler3,Zismann Victoria3,Boateng Martin4,Zhu Zhanyang5,Chuang Han‐Yu6,Trent Jeffrey M.3,Haworth David1,Chon Esther1ORCID,Hendricks William1,Wang Guannan1

Affiliation:

1. Vidium Animal Health Phoenix Arizona USA

2. Center for Cancer Research at the National Cancer Institute National Cancer Institute Bethesda Maryland USA

3. Translational Genomics Research Institute Phoenix Arizona USA

4. Self‐employed Phoenix Arizona USA

5. Sampled Piscataway New Jersey USA

6. Guardant Health San Diego California USA

Abstract

AbstractA genomic understanding of the oncogenic processes and individual variability of human cancer has steadily fueled improvement in patient outcomes over the past 20 years. Mutations within tumour tissues are routinely assessed through clinical genomic diagnostic assays by academic and commercial laboratories to facilitate diagnosis, prognosis and effective treatment stratification. The application of genomics has unveiled a wealth of mutation‐based biomarkers in canine cancers, suggesting that the transformative principles that have revolutionized human cancer medicine can be brought to bear in veterinary oncology. To advance clinical genomics and genomics‐guided medicine in canine oncology, we have developed and validated a canine cancer next‐generation sequencing gene panel for the identification of multiple mutation types in clinical specimens. With this panel, we examined the genomic landscapes of 828 tumours from 813 dogs, spanning 53 cancer types. We identified 7856 alterations, encompassing copy number variants, single nucleotide variants, indels and internal tandem duplications. Additionally, we evaluated the clinical utility of these alterations by incorporating a biomarker framework from comprehensive curation of primary canine literature and inferences from human cancer genomic biomarker literature and clinical diagnostics. Remarkably, nearly 90% of the cases exhibited mutations with diagnostic, prognostic or therapeutic implications. Our work represents a thorough assessment of genomic landscapes in a large cohort of canine cancers, the first of its kind for its comprehensive inclusion of multiple mutation types and structured annotation of biomarkers, demonstrating the clinical potential of leveraging mutation‐based biomarkers in veterinary oncology.

Publisher

Wiley

Subject

General Veterinary

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