Novel genomic prognostic biomarkers for dogs with cancer

Author:

Chon Esther1ORCID,Sakthikumar Sharadha1,Tang Min2,Hamilton Matthew J.3,Vaughan Andrew4,Smith Ashley5,Sommer Breann6,Robat Cecilia7,Manley Christina8,Mullin Christine9,Ohashi Emi10,Manor Emily11,Custis James12,Intile Joanne13,Shiu Kai Biu7ORCID,Parshley Lisa14,Bergman Noelle5,Sheppard‐Olivares Sabina15,Hafeman Scott16,Wright Zachary12,Haworth David1,Hendricks William1,Wang Guannan1ORCID

Affiliation:

1. Vidium Animal Health A Subsidiary of The Translational Genomics Research Institute (TGen) Scottsdale Arizona USA

2. STATBEYOND Consulting LLC Irvine California USA

3. Private Veterinary Specialties Lebanon New Jersey USA

4. Las Vegas Veterinary Specialty Center Las Vegas Nevada USA

5. Department of Clinical Sciences Auburn University College of Veterinary Medicine Auburn Alabama USA

6. Wisconsin Veterinary Referral Center by Ethos Waukesha Wisconsin USA

7. VCA Veterinary Emergency Service & Veterinary Specialty Center Middleton Wisconsin USA

8. The Oncology Service – Leesburg Leesburg Virginia USA

9. BluePearl Malvern Malvern Pennsylvania USA

10. VCA Animal Specialty Group Los Angeles California USA

11. VCA Advanced Veterinary Care Center Fishers Indiana USA

12. VCA Animal Diagnostic Clinic Dallas Texas USA

13. North Carolina State University Raleigh North Carolina USA

14. Olympia Veterinary Specialists – The Cancer Center Olympia Washington USA

15. Pet Specialists of Austin Austin Texas USA

16. VCA Highlands Ranch Animal Specialty and Emergency Center Highlands Ranch Colorado USA

Abstract

AbstractBackgroundGrowing evidence from dogs and humans supports the abundance of mutation‐based biomarkers in tumors of dogs. Increasing the use of clinical genomic diagnostic testing now provides another powerful data source for biomarker discovery.HypothesisAnalyzed clinical outcomes in dogs with cancer profiled using SearchLight DNA, a cancer gene panel for dogs, to identify mutations with prognostic value.AnimalsA total of 127 cases of cancer in dogs were analyzed using SearchLight DNA and for which clinical outcome information was available.MethodsClinical data points were collected by medical record review. Variables including mutated genes, mutations, signalment, and treatment were fitted using Cox proportional hazard models to identify factors associated with progression‐free survival (PFS). The log‐rank test was used to compare PFS between patients receiving and not receiving targeted treatment before first progression.ResultsCombined genomic and outcomes analysis identified 336 unique mutations in 89 genes across 26 cancer types. Mutations in 6 genes (CCND1, CCND3, SMARCB1, FANCG, CDKN2A/B, and MSH6) were significantly associated with shorter PFS. Dogs that received targeted treatment before first progression (n = 45) experienced significantly longer PFS compared with those that did not (n = 82, P = .01). This significance held true for 29 dogs that received genomically informed targeted treatment compared with those that did not (P = .05).Conclusion and Clinical ImportanceWe identified novel mutations with prognostic value and demonstrate the benefit of targeted treatment across multiple cancer types. These results provide clinical evidence of the potential for genomics and precision medicine in dogs with cancer.

Publisher

Wiley

Subject

General Veterinary

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