Does heterogeneity matter in the estimation of tumour budding and tumour stroma ratio in colon cancer?

Ann C. Eriksen; Johnnie B. Andersen; Jan Lindebjerg; René dePont Christensen; Torben F. Hansen; Sanne Kjær-Frifeldt; Flemming B. Sørensen

doi:10.1186/s13000-018-0697-9

Diagnostic Pathology (Mar 2018)

Does heterogeneity matter in the estimation of tumour budding and tumour stroma ratio in colon cancer?

Ann C. Eriksen,
Johnnie B. Andersen,
Jan Lindebjerg,
René dePont Christensen,
Torben F. Hansen,
Sanne Kjær-Frifeldt,
Flemming B. Sørensen

Affiliations

Ann C. Eriksen: Institute of Regional Health Research, University of Southern Denmark
Johnnie B. Andersen: Department of Clinical Medicine, Stereological Research Laboratory and University Institute of Pathology, Aarhus University
Jan Lindebjerg: Institute of Regional Health Research, University of Southern Denmark
René dePont Christensen: Research Unit of General Practice, University of Southern Denmark
Torben F. Hansen: Institute of Regional Health Research, University of Southern Denmark
Sanne Kjær-Frifeldt: Department of Pathology, Danish Colorectal Cancer Center South, Vejle Hospital
Flemming B. Sørensen: Institute of Regional Health Research, University of Southern Denmark

DOI: https://doi.org/10.1186/s13000-018-0697-9
Journal volume & issue: Vol. 13, no. 1
pp. 1 – 9

Abstract

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Abstract Background Tumour budding (TB) and Tumour Stroma Ratio (TSR) may be rewarding in the treatment stratification of patients with stage II colon cancer. However, lack of standardization may exclude these parameters from being used in a clinical setting. The purpose of this methodologic study was to compare stereology with semi-quantitative estimations of TSR, to investigate the intra-tumoural heterogeneity of TB and TSR, and to assess the intra- and inter-observer agreement. Methods Three paraffin embedded tumour blocks, one of them representing the deepest invasive front, were selected from each of 43 patients treated for stage II colon cancer. TSR was estimated in H&E sections semi-quantitatively using conventional microscopy, and stereologically on scanned slides, using the newCAST stereology platform. TB was scored across 10 high power fields at the invasive front in cytokeratin AE1/AE3 stained sections. Results Subjective, semi-quantitative estimates of TSR significantly correlated to the stereological estimates, with the best correlation found for sections with the deepest invasive tumour penetration (σ = 0.621, p < 0.001). Inter-observer agreement was moderate to substantial for both TB (Κappa = 0.46–0.73) and TSR (Κappa = 0.70–0.75). The Intraclass correlation coefficient (ICC) for TSR varied from 0.322 based on stereological hotspot estimation to 0.648 for the semi-quantitative evaluation. For TB, ICC varied from 0.646 based on continuous data to 0.698 based on categorical data (cut-off: 10 buds). Thus, the intra-tumoural heterogeneity for both TB and the semi-quantitative estimation of TSR was low. Conclusion We recommend using only one tissue section representing the deepest invasive tumour area for estimation of TSR. For TB we recommend using one tissue section; however due to low representation of high-budding tumours, results must be considered with caution.

Published in Diagnostic Pathology

ISSN: 1746-1596 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Pathology
Website: https://diagnosticpathology.biomedcentral.com/

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