Subcutaneous mast cell tumours: A prospective multi‐institutional clinicopathological and prognostic study of 43 dogs

Background Canine subcutaneous mast cell tumours (ScMCTs) reportedly have a good prognosis. However, biomarkers that can be used to predict outcome are currently limited. Methods A multicentre prospective study was conducted to identify new prognostic markers. Dogs with a first occurrence of ScMCT w...

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Bibliographic Details
Published in:Veterinary record 2023-07, Vol.193 (1), p.no-no
Main Authors: Marconato, Laura, Stefanello, Damiano, Solari Basano, Fabrizio, Faroni, Eugenio, Dacasto, Mauro, Giantin, Mery, Bettini, Giuliano, Aresu, Luca, Bonfanti, Ugo, Bertazzolo, Walter, Annoni, Maurizio, Lecchi, Cristina, Sabattini, Silvia
Format: Article
Language:English
Subjects:
Animals
canine
cytograding
Dog Diseases - diagnosis
Dog Diseases - genetics
Dog Diseases - therapy
Dogs
lymph node metastasis
Lymph Nodes - pathology
Mast Cells - metabolism
Mast Cells - pathology
mastocytoma
Medical prognosis
Metastasis
Prognosis
Prospective Studies
Tumors
Veterinary medicine
Vinblastine
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Summary:Background Canine subcutaneous mast cell tumours (ScMCTs) reportedly have a good prognosis. However, biomarkers that can be used to predict outcome are currently limited. Methods A multicentre prospective study was conducted to identify new prognostic markers. Dogs with a first occurrence of ScMCT were enrolled upon primary tumour removal and regional lymphadenectomy. In the absence of metastasis, dogs were monitored, while dogs with overtly metastatic lymph nodes (histological node 3, HN3) received adjuvant vinblastine. Results Forty‐three dogs were enrolled: 15 (34.9%) had at least one HN3 lymph node and received vinblastine, and 28 (65.1%) were monitored. Three tumours harboured exon 8 and 9 c‐kit mutations. Eight (18.6%) dogs experienced tumour progression, and five (11.6%) died of MCT‐related causes. The 1‐ and 2‐year survival rates were 90% and 77%, respectively. Variables significantly associated with an increased risk of progression included high cytograde, a mitotic count (MC) greater than 4/10 high‐power fields (hpf) and Ki67‐index greater than 23. An MC greater than 4/10 hpf was also associated with an increased risk of tumour‐related death. Limitations Regional rather than sentinel lymphadenectomy was performed in these dogs. Dogs were enrolled in oncology referral centres, constituting a different population compared to previous studies. Conclusions ScMCTs have a good prognosis. However, the metastatic rate at admission was higher in this study than previously reported, and a subset of tumours were associated with a fatal outcome despite multimodal treatment. Proliferative activity and cytograding may predict more aggressive behaviour in ScMCTs.
ISSN:0042-4900
2042-7670
DOI:10.1002/vetr.2991