Nottingham Prognostic Index Plus: Validation of a clinical decision making tool in breast cancer in an independent series

Andrew R Green; Daniele Soria; Jacqueline Stephen; Desmond G Powe; Christopher C Nolan; Ian Kunkler; Jeremy Thomas; Gillian R Kerr; Wilma Jack; David Cameron; Tammy Piper; Graham R Ball; Jonathan M Garibaldi; Emad A Rakha; John Ms Bartlett; Ian O Ellis

doi:10.1002/cjp2.32

Nottingham Prognostic Index Plus: Validation of a clinical decision making tool in breast cancer in an independent series

J Pathol Clin Res. 2016 Jan 15;2(1):32-40. doi: 10.1002/cjp2.32. eCollection 2016 Jan.

Authors

Affiliations

¹ Division of Cancer and Stem Cells Breast Cancer Pathology Research Group, School of Medicine, University of Nottingham, Nottingham City Hospital Hucknall Road Nottingham NG5 1PB.
² Intelligent Modelling & Analysis Research GroupSchool of Computer ScienceUniversity of Nottingham, Jubilee CampusWollaton RoadNottinghamNG8 1BB; Advanced Data Analysis Centre, University of Nottingham, University ParkNottinghamNG7 2RD.
³ School of Molecular, Genetic and Population Health Sciences Centre for Population Health Sciences, Medical School, University of Edinburgh Teviot Place Edinburgh EH8 9AG.
⁴ Cellular Pathology, Nottingham University Hospitals NHS Trust Hucknall Road Nottingham NG5 1PB.
⁵ The Institute of Genetics and Molecular Medicine Edinburgh Cancer Research Centre, University of Edinburgh, Western General Hospital Crewe Road South Edinburgh EH4 2XR.
⁶ Edinburgh Breast Unit, Western General Hospital Crewe Road South Edinburgh EH4 2XU.
⁷ John van Geest Cancer Research Centre, School of Science and Technology, Nottingham Trent University Nottingham NG11 8NS.
⁸ Division of Cancer and Stem CellsBreast Cancer Pathology Research Group, School of Medicine, University of Nottingham, Nottingham City HospitalHucknall RoadNottinghamNG5 1PB; Cellular Pathology, Nottingham University Hospitals NHS TrustHucknall RoadNottinghamNG5 1PB.
⁹ The Institute of Genetics and Molecular MedicineEdinburgh Cancer Research Centre, University of Edinburgh, Western General HospitalCrewe Road SouthEdinburghEH4 2XR; Transformative PathologyOntario Institute for Cancer Research, MaRS Centre661 University Avenue, Suite 510TorontoCanadaM5G 0A3.

PMID: 27499914
PMCID: PMC4858129
DOI: 10.1002/cjp2.32

Abstract

The Nottingham Prognostic Index Plus (NPI+) is a clinical decision making tool in breast cancer (BC) that aims to provide improved patient outcome stratification superior to the traditional NPI. This study aimed to validate the NPI+ in an independent series of BC. Eight hundred and eighty five primary early stage BC cases from Edinburgh were semi-quantitatively assessed for 10 biomarkers [Estrogen Receptor (ER), Progesterone Receptor (PgR), cytokeratin (CK) 5/6, CK7/8, epidermal growth factor receptor (EGFR), HER2, HER3, HER4, p53, and Mucin 1] using immunohistochemistry and classified into biological classes by fuzzy logic-derived algorithms previously developed in the Nottingham series. Subsequently, NPI+ Prognostic Groups (PGs) were assigned for each class using bespoke NPI-like formulae, previously developed in each NPI+ biological class of the Nottingham series, utilising clinicopathological parameters: number of positive nodes, pathological tumour size, stage, tubule formation, nuclear pleomorphism and mitotic counts. Biological classes and PGs were compared between the Edinburgh and Nottingham series using Cramer's V and their role in patient outcome prediction using Kaplan-Meier curves and tested using Log Rank. The NPI+ biomarker panel classified the Edinburgh series into seven biological classes similar to the Nottingham series (p > 0.01). The biological classes were significantly associated with patient outcome (p < 0.001). PGs were comparable in predicting patient outcome between series in Luminal A, Basal p53 altered, HER2+/ER+ tumours (p > 0.01). The good PGs were similarly validated in Luminal B, Basal p53 normal, HER2+/ER- tumours and the poor PG in the Luminal N class (p > 0.01). Due to small patient numbers assigned to the remaining PGs, Luminal N, Luminal B, Basal p53 normal and HER2+/ER- classes could not be validated. This study demonstrates the reproducibility of NPI+ and confirmed its prognostic value in an independent cohort of primary BC. Further validation in large randomised controlled trial material is warranted.

Keywords: breast cancer; classification; clinical; molecular; outcome; prognostic index.

Abstract

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