Reproducibility of Histologic Prognostic Parameters for Mantle Cell Lymphoma: Cytology, Ki67, P53 and SOX11

Overview

Journal Virchows Arch

Specialties Cell Biology
Molecular Biology
Pathology

Date 2020 Jan 25

PMID 31975037

Citations 10

Authors

Giorgio A Croci

Eva Hoster

Silvia Bea

Guillem Clot

Anna Enjuanes

David W Scott

Jose Cabecadas

Luis Veloza

Elias Campo

Erik Clasen-Linde

Rashmi S Goswami

Lars Helgeland

Stefano Pileri

Grzegorz Rymkiewicz

Sarah Reinke

Martin Dreyling

Wolfram Klapper

Affiliations

Soon will be listed here.

Abstract

Mantle cell lymphoma (MCL) shows a clinical aggressiveness that varies from patient to patient. Despite major advances in outcomes with current immunochemotherapy, the future development of therapies requires risk stratification to tailor therapy intensity. Within the group of reference pathologists for the ongoing trials of the European MCL Network, we performed a round robin test on a tissue microarray to evaluate the reproducibility in assessing the biomarkers of outcome in MCL. Cytological subtype, Ki67-index and expression of p53 and SOX11 were evaluated on 20 diagnostic tumour samples by eight participating labs independently. We demonstrate that the assessment of the proliferation index by counting the Ki67 positive cells as well as assessment of SOX11 and p53 expression status is reproducible between labs. For the most established prognostic biomarker, Ki67, the intra-class correlation coefficient was very good when assessed as a continuous parameter (0.87). The agreement was lower when the values were analysed in a dichotomized way applying the commonly used cutoff of 30% (kappa = 0.65, complete concordance of all labs in 13/20 (65%)). Cases with discrepant results between labs in the dichotomized analysis showed mean values close to the cutoff of 30%. Centralised scoring and digital image analysis revealed results in line with the scores from individual labs. All cases in our cohort were additionally assessed for gene expression signatures and of TP53 gene alterations. Given the good reproducibility when guidelines of assessment are applied, the biomarker studied in this inter-laboratory test presents potential candidates to be enhanced for risk-stratification in the future clinical trials.

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