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Ki67 expression in invasive breast cancer: the use of tissue microarrays compared with whole tissue sections
Authors:Abir A. Muftah  Mohammed A. Aleskandarany  Methaq M. Al-kaabi  Sultan N. Sonbul  Maria Diez-Rodriguez  Chris C. Nolan  Carlos Caldas  Ian O. Ellis  Emad A. Rakha  Andrew R. Green
Affiliation:1.Department of Histopathology, Division of Cancer and Stem Cells, School of Medicine,Nottingham City Hospital, The University of Nottingham and Nottingham University Hospitals NHS Trust,Nottingham,UK;2.Department of Pathology, Faculty of Medicine,University of Benghazi,Benghazi,Libya;3.Department of Pathology, College of Medicine,Al Mustansiriyah University,Baghdad,Iraq;4.Cancer Research UK Cambridge Institute, Li Ka Shing Centre,University of Cambridge,Cambridge,UK
Abstract:

Background

Although the prognostic value of Ki67 in breast cancer is well documented, using optimal cut-points for patient stratification, reproducibility of the scoring and interpretation of the results remains a matter of debate particularly when using tissue microarrays (TMAs). This study aims to assess Ki67 expression assessed on TMAs and their matched whole tissue sections (WTS). Moreover, whether the cut-off used for WTS is reproducible on TMA in BC molecular classes and the association between Ki67 expression cut-off, assessed on TMAs and WTS, and clinicopathological parameters and patient outcome were tested.

Method

A large series (n = 707) of primary invasive breast tumours were immunostained for Ki67 using both TMA and WTS and assessed as percentage staining and correlated with each other, clinicopathological parameters and patient outcome. In addition, MKI67 mRNA expression was correlated with Ki67 protein levels on WTS and TMAs in a subset of cases included in the METABRIC study.

Results

There was moderate concordance in Ki67 expression between WTS and TMA when analysed as a continuous variable (Intraclass correlation coefficient = 0.61) and low concordance when dichotomised (kappa value = 0.3). TMA showed low levels of Ki67 with mean percentage of expression of 35 and 22% on WTS and TMA, respectively. MKI67 mRNA expression was significantly correlated with protein expression determined on WTS (Spearman Correlation, r = 0.52) and to a lesser extent on TMA (r = 0.34) (p < 0.001). Regarding prediction of patient outcome, statistically significant differences were detected upon stratification of patients with tumours expressing Ki67 at 10, 15, 20, 25 or 30% in TMA. Using TMA, ≥20% Ki67 provided the best prognostic cut-off particularly in triple-negative and HER2-positive classes.

Conclusion

Ki67 expression in breast cancer can be evaluated using TMA although different cut-points are required to emulate results from WTS. A cut-off of ≥20% for Ki67 expression in BC provides the best prognostic correlations when TMAs are used.
Keywords:
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