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Clinical Trial
. 2022 Jan;9(1):e49-e57.
doi: 10.1016/S2352-3026(21)00349-5.

Survival by age in paediatric and adolescent patients with Hodgkin lymphoma: a retrospective pooled analysis of children's oncology group trials

Justine M Kahn  1 Qinglin Pei  2 Debra L Friedman  3 Joel Kaplan  4 Frank G Keller  5 David Hodgson  6 Yue Wu  2 Burton E Appel  7 Smita Bhatia  8 Tara O Henderson  9 Cindy L Schwartz  10 Kara M Kelly  11 Sharon M Castellino  5
Affiliations
Clinical Trial

Survival by age in paediatric and adolescent patients with Hodgkin lymphoma: a retrospective pooled analysis of children's oncology group trials

Justine M Kahn et al. Lancet Haematol. 2022 Jan.

Abstract

Background: Adolescents with Hodgkin lymphoma have worse disease outcomes than children. Whether these differences persist within clinical trials is unknown. We examined survival, by age, in patients receiving response-adapted therapy for Hodgkin lymphoma on Children's Oncology Group (COG) trials.

Methods: Patients (aged 1-21 years) diagnosed with classical Hodgkin lymphoma and enrolled between Sept 23, 2002, and Jan 19, 2012, on one of three phase 3 COG trials in the USA and Canada were eligible for inclusion. The three COG trials were defined by risk group according to Ann Arbor stage, B-symptoms, and bulk (AHOD0431 [low risk; NCT00302003], AHOD0031 [intermediate risk; NCT00025259], or AHOD0831 [high risk; NCT01026220]). The outcomes of this study were event-free survival (death, relapse, or subsequent neoplasm) and overall survival. Cox proportional hazards models estimated survival, adjusting for disease and treatment factors both overall and in patients with mixed cellularity or non-mixed cellularity (nodular sclerosing and not-otherwise-specified) disease.

Findings: Of 2155 patients enrolled on the three trials, 1907 (88·4%; 968 [50·8%] male and 939 [49·2%] female; 1227 [64·3%] non-Hispanic White) were included in this analysis. After a median follow-up of 7·4 years (IQR 4·3-10·2), older patients (aged ≥15 years) had worse unadjusted 5-year event-free survival (80% [95% CI 78-83]) than did younger patients (aged <15 years; 86% [83-88]; HR 1·38 [1·11-1·71]; p=0·0038). Older patients also had worse unadjusted 5-year overall survival than did younger patients (96% [95% CI 95-97] vs 99% [98-99]; HR 2·50 [1·41-4·45]; p=0·0012). In patients with non-mixed cellularity histology, older patients had a significantly increased risk of having an event than did younger patients with the same histology (HR 1·32 [1·03-1·68]; p=0·027). Older patients with mixed cellularity had significantly worse 5-year event-free survival than did younger patients in unadjusted (77% [95% CI 65-86] for older patients vs 94% [88-97] for younger patients; HR 2·93 [1·37-6·29]; p=0·0039) and multivariable models (HR 3·72 [1·56-8·91]; p=0·0032). Overall, older patients were more likely to die than younger patients (HR 3·08 [1·49-6·39]; p=0·0025).

Interpretation: Adolescents (≥15 years) treated on COG Hodgkin lymphoma trials had worse event-free survival and increased risk of death compared with children (<15 years). Our findings highlight the need for prospective studies to examine tumour and host biology, and to test novel therapies across the age spectrum.

Funding: National Institutes of Health, St Baldrick's Foundation, and Lymphoma Research Foundation.

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Conflict of interest statement

Declaration of interests We declare no competing interests.

Figures

Figure 1:
Figure 1:
Cohort selection
Figure 2
Figure 2
(A and B): EFS by age ≥15 years vs. <15 years and histologic subgroups in 1,907 patients (<1 – 21 years) enrolled on phase 3 Children’s Oncology Group trials for newly diagnosed Hodgkin lymphoma (HL) (2002 – 2012). The mixed cellularity (MC) group included 196 (10%) of the cohort of 1,907 patients. The non-MC group included 1,711 (90%) of 1,907 patients and was comprised of 1,547 (90%) of 1,711 patients with nodular sclerosing (NS) histology, 108 (6.5%) of 1,711 with classical HL, not-otherwise-specified, and 56 (3.5%) of 1,711 with histology unknown.
See this image and copyright information in PMC

References

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