An Individualized Prediction Model for Early-Stage Classic Hodgkin's Lymphoma

Angie Mae Rodday; Andrew M Evens; Matthew J Maurer; Jenica N Upshaw; Nicholas Counsell; Sara Rossetti; Cheryl Chang; Zhu Cui; Qingyan Xiang; Raphael Mwangi; Ranjana Advani; Marc Andre; Andrea Gallamini; Annette E Hay; David C Hodgson; Richard T Hoppe; Martin Hutchings; Peter Johnson; Eric Mou; Stephen Opat; John Raemaekers; Kerry J Savage; Susan K Parsons; John Radford

doi:10.1056/EVIDoa2500115

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An Individualized Prediction Model for Early-Stage Classic Hodgkin's Lymphoma

Journal article

Peer reviewed

An Individualized Prediction Model for Early-Stage Classic Hodgkin's Lymphoma

Angie Mae Rodday, Andrew M Evens, Matthew J Maurer, Jenica N Upshaw, Nicholas Counsell, Sara Rossetti, Cheryl Chang, Zhu Cui, Qingyan Xiang, Raphael Mwangi, …

NEJM evidence, Vol.4(9)

09/2025

DOI: 10.1056/EVIDoa2500115

PMCID: PMC12498259

PMID: 40536772

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https://www.ncbi.nlm.nih.gov/pmc/articles/12498259View

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Abstract

A predictive model for early-stage classic Hodgkin's lymphoma (cHL) does not exist. Leveraging patient-level data from large clinical trials and registries, we developed and validated a model that we term the Early-Stage cHL International Prognostication Index (E-HIPI) to predict 2-year progression-free survival (PFS). We developed the model using the Transparent Reporting of a Multivariable Prediction Model for Individual Prognosis or Diagnosis (TRIPOD) guidelines in 3000 adults with newly diagnosed early-stage cHL from four international phase III clinical trials conducted from 1994 to 2011. External validation was performed in two cohorts, totaling 2360 treated patients from five international cHL registries (1996 to 2019). Two-year PFS was estimated using a Cox model with pretreatment variables selected using backward elimination. Internal validation corrected for overfitting. External validation assessed discrimination and calibration. The final model was also compared against European Organisation for Research and Treatment of Cancer (EORTC) favorable or unfavorable status. The median age in the development cohort was 31.2 years; 77.4% had stage II disease. The estimated 2-year PFS was 93.7%. Final variables retained in the model were sex and continuous values of maximum tumor diameter (MTD), and levels of hemoglobin and albumin. The optimism-corrected C statistic in the development cohort was 0.63 (95% confidence interval, 0.60 to 0.69). Two-year PFS was lower in the validation cohorts 1 (90.3%) and 2 (91.6%). In validation cohort 1, the C statistic was 0.63 and the calibration slope was near 1, but overall calibration indicated underprediction, which improved on updating the intercept. The performance was similar in validation cohort 2. In addition, higher-risk E-HIPI scores were associated with worse outcomes in both the EORTC unfavorable and favorable subgroups. When included altogether in one Cox model, the E-HIPI was associated with PFS, whereas EORTC favorable or unfavorable status was not. Online risk calculators were developed (https://rtools.mayo.edu/holistic_ehipi/). Utilizing objective, continuous, and readily available variables, we developed and validated a new prediction model for early-stage cHL. Male sex, lower hemoglobin or albumin levels, and higher MTDs were associated with worse PFS. (Funded by the National Cancer Institute; grant number, NCI R01 CA 262265-04.).

Details

Title: Subtitle: An Individualized Prediction Model for Early-Stage Classic Hodgkin's Lymphoma
Creators: Angie Mae Rodday - Tufts Medical Center
Andrew M Evens - Rutgers, The State University of New Jersey
Matthew J Maurer - Mayo Clinic
Jenica N Upshaw - Tufts Medical Center
Nicholas Counsell - University College London
Sara Rossetti - Rigshospitalet
Cheryl Chang - Stanford University
Zhu Cui - Tufts Medical Center
Qingyan Xiang - Tufts Medical Center
Raphael Mwangi - Mayo Clinic
Ranjana Advani - Stanford University
Marc Andre - CHU Dinant Godinne UCL Namur
Andrea Gallamini - Centre Antoine Lacassagne
Annette E Hay - Queen's University
David C Hodgson - Princess Margaret Cancer Centre
Richard T Hoppe - Stanford University
Martin Hutchings - Copenhagen University Hospital
Peter Johnson - University of Southampton
Eric Mou - University of Iowa
Stephen Opat - Monash University
John Raemaekers - European Organisation for Research and Treatment of Cancer
Kerry J Savage - University of British Columbia
Susan K Parsons - Tufts Medical Center
John Radford - NIHR Manchester Biomedical Research Centre
Resource Type: Journal article
Publication Details: NEJM evidence, Vol.4(9)
DOI: 10.1056/EVIDoa2500115
PMID: 40536772
PMCID: PMC12498259
NLM abbreviation: NEJM Evid
ISSN: 2766-5526
eISSN: 2766-5526
Publisher: MASSACHUSETTS MEDICAL SOC
Grant note: National Cancer Institute: R01 CA 262265-04
Drs. Parsons and Evens (multi-principal investigator) were supported by a grant from the National Cancer Institute; grant number, R01 CA 262265-04 (Modeling Multi-Source Data in Hodgkin Lymphoma).
Language: English
Electronic publication date: 06/19/2025
Date published: 09/2025
Academic Unit: Hematology, Oncology, and Blood & Marrow Transplantation; Internal Medicine
Record Identifier: 9984832086802771

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