An enhanced prognostic score for overall survival of patients with cancer derived from a large real-world cohort

T Becker; J Weberpals; A M Jegg; W V So; A Fischer; M Weisser; F Schmich; D Rüttinger; A Bauer-Mehren

doi:10.1016/j.annonc.2020.07.013

An enhanced prognostic score for overall survival of patients with cancer derived from a large real-world cohort

Ann Oncol. 2020 Nov;31(11):1561-1568. doi: 10.1016/j.annonc.2020.07.013. Epub 2020 Jul 31.

Authors

T Becker¹, J Weberpals¹, A M Jegg², W V So³, A Fischer¹, M Weisser², F Schmich¹, D Rüttinger², A Bauer-Mehren⁴

Affiliations

¹ Data Science, Pharma Research and Development, Roche Innovation Center Munich, Munich, Germany.
² Early Clinical Development Oncology, Pharma Research and Development, Roche Innovation Center Munich, Munich, Germany.
³ Data Science, Pharma Research and Development, Roche Innovation Center New York, New York, USA.
⁴ Data Science, Pharma Research and Development, Roche Innovation Center Munich, Munich, Germany. Electronic address: anna.bauer-mehren@roche.com.

PMID: 32739409
DOI: 10.1016/j.annonc.2020.07.013

Abstract

Background: By understanding prognostic biomarkers, we gain insights into disease biology and may improve design, conduct, and data analysis of clinical trials and real-world data. In this context, we used the Flatiron Health Electronic Health Record-derived deidentified database that provides treatment outcome and biomarker data from >280 oncology centers in the USA, organized into 17 cohorts defined by cancer type.

Patients and methods: In 122 694 patients, we analyzed demographic, clinical, routine hematology, and blood chemistry parameters within a Cox proportional hazard framework to derive a multivariable prognostic risk model for overall survival (OS), the 'Real wOrld PROgnostic score (ROPRO)'. We validated ROPRO in two independent phase I and III clinical studies.

Results: A total of 27 variables contributed independently and homogeneously across cancer indications to OS. In the largest cohort (advanced non-small-cell lung cancer), for example, patients with elevated ROPRO scores (upper 10%) had a 7.91-fold (95% confidence interval 7.45-8.39) increased death hazard compared with patients with low scores (lower 10%). Median survival was 23.9 months (23.3-24.5) in the lowest ROPRO quartile Q1, 14.8 months (14.4-15.2) in Q2, 9.4 months (9.1-9.7) in Q3, and 4.7 months (4.6-4.8) in Q4. The ROPRO model performance indicators [C-index = 0.747 (standard error 0.001), 3-month area under the curve (AUC) = 0.822 (0.819-0.825)] strongly outperformed those of the Royal Marsden Hospital Score [C-index = 0.54 (standard error 0.0005), 3-month AUC = 0.579 (0.577-0.581)]. We confirmed the high prognostic relevance of ROPRO in clinical Phase 1 and III trials.

Conclusions: The ROPRO provides improved prognostic power for OS. In oncology clinical development, it has great potential for applications in patient stratification, patient enrichment strategies, data interpretation, and early decision-making in clinical studies.

Keywords: Cox regression; Flatiron Health; overall survival; prognostic score (ROPRO); real world data (RWD).

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Carcinoma, Non-Small-Cell Lung*
Cohort Studies
Humans
Lung Neoplasms*
Prognosis
Retrospective Studies