Molecular characterisation of canine osteosarcoma in high risk breeds

Simpson, Siobhan; Dunning, Mark; de Brot, Simone; Alibhai, Aziza; Bailey, Clara; Woodcock, Corinne L.; Mestas, Madeline; Akhtar, Shareen; Jeyapalan, Jennie N.; Lothion-Roy, Jennifer; Emes, Richard D.; Allegrucci, Cinzia; Rizvanov, Albert A.; Mongan, Nigel P.; Rutland, Catrin S.

doi:10.3390/cancers12092405

Molecular characterisation of canine osteosarcoma in high risk breeds

Simpson, Siobhan; Dunning, Mark; de Brot, Simone; Alibhai, Aziza; Bailey, Clara; Woodcock, Corinne L.; Mestas, Madeline; Akhtar, Shareen; Jeyapalan, Jennie N.; Lothion-Roy, Jennifer; Emes, Richard D.; Allegrucci, Cinzia; Rizvanov, Albert A.; Mongan, Nigel P.; Rutland, Catrin S.

Authors

Siobhan Simpson

Professor MARK DUNNING mark.dunning@nottingham.ac.uk
PROFESSOR

Simone de Brot

Aziza Alibhai

Clara Bailey

Corinne L. Woodcock

Madeline Mestas

Shareen Akhtar

Dr JENNIE JEYAPALAN jennie.jeyapalan@nottingham.ac.uk
ASSISTANT PROFESSOR

Jennifer Lothion-Roy

Richard D. Emes

Dr CINZIA ALLEGRUCCI cinzia.allegrucci@nottingham.ac.uk
ASSOCIATE PROFESSOR

Albert A. Rizvanov

Professor Nigel Mongan nigel.mongan@nottingham.ac.uk
ASSOCIATE PRO-VICE CHANCELLORGLOBAL ENGAGEMENT

Professor CATRIN RUTLAND CATRIN.RUTLAND@NOTTINGHAM.AC.UK
PROFESSOR OF MOLECULAR MEDICINE

Abstract

© 2020 by the authors. Licensee MDPI, Basel, Switzerland. Dogs develop osteosarcoma (OSA) and the disease process closely resembles that of human OSA. OSA has a poor prognosis in both species and disease-free intervals and cure rates have not improved in recent years. Gene expression in canine OSAs was compared with non-tumor tissue utilising RNA sequencing, validated by qRT-PCR and immunohistochemistry (n = 16). Polymorphic polyglutamine (polyQ) tracts in the androgen receptor (AR/NR3C4) and nuclear receptor coactivator 3 (NCOA3) genes were investigated in control and OSA patients using polymerase chain reaction (PCR), Sanger sequencing and fragment analysis (n = 1019 Rottweilers, 379 Irish Wolfhounds). Our analysis identified 1281 significantly differentially expressed genes (>2 fold change, p < 0.05), specifically 839 lower and 442 elevated gene expression in osteosarcoma (n = 3) samples relative to non-malignant (n = 4) bone. Enriched pathways and gene ontologies were identified, which provide insight into the molecular pathways implicated in canine OSA. Expression of a subset of these genes (SLC2A1, DKK3, MMP3, POSTN, RBP4, ASPN) was validated by qRTPCR and immunohistochemistry (MMP3, DKK3, SLC2A1) respectively. While little variation was found in the NCOA3 polyQ tract, greater variation was present in both polyQ tracts in the AR, but no significant associations in length were made with OSA. The data provides novel insights into the molecular mechanisms of OSA in high risk breeds. This knowledge may inform development of new prevention strategies and treatments for OSA in dogs and supports utilising spontaneous OSA in dogs to improve understanding of the disease in people.

Citation

Simpson, S., Dunning, M., de Brot, S., Alibhai, A., Bailey, C., Woodcock, C. L., Mestas, M., Akhtar, S., Jeyapalan, J. N., Lothion-Roy, J., Emes, R. D., Allegrucci, C., Rizvanov, A. A., Mongan, N. P., & Rutland, C. S. (2020). Molecular characterisation of canine osteosarcoma in high risk breeds. Cancers, 12(9), Article 2405. https://doi.org/10.3390/cancers12092405

Journal Article Type	Article
Acceptance Date	Aug 14, 2020
Online Publication Date	Aug 25, 2020
Publication Date	Sep 1, 2020
Deposit Date	Aug 21, 2020
Publicly Available Date	Aug 25, 2020
Journal	Cancers
Electronic ISSN	2072-6694
Publisher	MDPI
Peer Reviewed	Peer Reviewed
Volume	12
Issue	9
Article Number	2405
DOI	https://doi.org/10.3390/cancers12092405
Keywords	Androgen; Androgen receptor; Bone; Cancer risk; Canine; KEGG; Wiki
Public URL	https://nottingham-repository.worktribe.com/output/4845775
Publisher URL	https://www.mdpi.com/2072-6694/12/9/2405