Feline intestinal mast cell tumours: clinicopathological characterisation and KIT mutation analysis

Silvia Sabattini; Mery Giantin; Adele Barbanera; Lara Zorro Shahidian; Mauro Dacasto; Vanessa Zancanella; Daniela Prata; Eleonora Trivigno; Giuliano Bettini

doi:10.1177/1098612X15581205

Feline intestinal mast cell tumours: clinicopathological characterisation and KIT mutation analysis

J Feline Med Surg. 2016 Apr;18(4):280-9. doi: 10.1177/1098612X15581205. Epub 2015 Apr 27.

Authors

Silvia Sabattini¹, Mery Giantin², Adele Barbanera¹, Lara Zorro Shahidian², Mauro Dacasto², Vanessa Zancanella², Daniela Prata³, Eleonora Trivigno⁴, Giuliano Bettini⁵

Affiliations

¹ Department of Veterinary Medical Sciences, University of Bologna, Bologna, Italy.
² Department of Comparative Biomedicine and Food Science, University of Padua, Padua, Italy.
³ IDEXX Laboratory Alfort, Alfortville, France.
⁴ l'Ourcq Veterinary Clinic, Mitry Mory, France.
⁵ Department of Veterinary Medical Sciences, University of Bologna, Bologna, Italy giuliano.bettini@unibo.it.

PMID: 25916685
DOI: 10.1177/1098612X15581205

Abstract

Objectives: Feline intestinal mast cell tumours (FIMCTs) are rare and reportedly characterised by poor differentiation, aggressive biological behaviour and lack of reliable therapeutic aids. KIT proto-oncogene-activating mutations have never been investigated in these tumours. This study describes the main clinicopathological and microscopic features observed in 17 FIMCTs.

Methods: Tumour degree of differentiation, proliferative activity, Kit protein expression and KIT mutations were evaluated and correlated with survival to assess their prognostic relevance.

Results: Ten tumours were located in the small intestine, two in the ileocaecocolic junction, and five in the large intestine. Survival times ranged from 3-538 days. Fifteen tumours were evaluated histologically, and there were six well-differentiated, six moderately differentiated and three poorly differentiated FIMCTs. The last showed a medium-to-large deposition of collagen tissue (P <0.001), and significantly higher mitotic and Ki67 indexes compared with more differentiated tumours (P = 0.011). On survival analysis, tumour degree of differentiation (P <0.001) and a mitotic index >2 (P = 0.022) were significantly associated with decreased survival times. Twelve cases showed Kit protein immunoexpression. The Kit pattern was membranous in five cases (33.3%), focal paranuclear in five (33.3%) and diffuse cytoplasmic in two (13.3%). Cytoplasmic Kit patterns were associated with a lesser differentiation (P = 0.015). Mutation analysis was successfully performed on 12 primary tumours and four lymph node metastases; however, no encoding mutation was detected.

Conclusions and relevance: Contrary to reports in the literature, FIMCTs seem to have an extremely variable biological behaviour. We propose a classification based on tumour degree of differentiation and proliferative activity. These findings need to be confirmed in larger series, and exploration of further genomic regions of KIT is warranted to clarify its role in the development and progression of these neoplasms.

MeSH terms

Animals
Cat Diseases / enzymology*
Cat Diseases / pathology*
Cats
Cell Differentiation
DNA Mutational Analysis
Intestinal Neoplasms / enzymology
Intestinal Neoplasms / pathology
Intestinal Neoplasms / veterinary*
Intestine, Small / enzymology*
Mast Cells
Mutation
Prognosis
Proto-Oncogene Proteins c-kit*
Survival Analysis

Substances

Proto-Oncogene Proteins c-kit