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Reduced and Compressed Cisplatin-Based Chemotherapy in Children and Adolescents With Intermediate-Risk Extracranial Malignant Germ Cell Tumors: A Report From the Children's Oncology Group

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Last modified
  • 03/14/2025
Type of Material
Authors
    Furqan Shaikh, University of TorontoJohn W. Cullen, Rocky Mountain Hospital for Children-Presbyterian Saint Luke’s Medical CenterThomas Olson, Emory UniversityFarzana Pashankar, Yale UniversityMarcio H. Malogolowkin, University of California DavisJames F. Amatruda, University of Texas Southwestern Medical CenterDoojduen Villaluna, Children’s Oncology GroupMark Krailo, Children’s Oncology GroupDeborah F. Billmire, Riley Hospital for ChildrenFrederick J. Rescorla, Riley Hospital for ChildrenRachel A. Egler, Rainbow Babies and Children’s HospitalBryan J. Dicken, Stollery Children’s HospitalJonathan H. Ross, Rainbow Babies and Children’s HospitalMarc Schlatter, Spectrum HealthCarlos Rodriguez-Galindo, St Jude Children’s Research HospitalA. Lindsay Frazier, Dana-Farber Cancer Institute
Language
  • English
Date
  • 2017-04-10
Publisher
  • American Society of Clinical Oncology
Publication Version
Copyright Statement
  • © 2017 by American Society of Clinical Oncology.
Final Published Version (URL)
Title of Journal or Parent Work
ISSN
  • 0732-183X
Volume
  • 35
Issue
  • 11
Start Page
  • 1203
End Page
  • 1210
Grant/Funding Information
  • Supported by Group Chair’s Grant no. U10CA180886, and by Group Statistician’s Grant no. U10CA180899 (M.K. and D.V.).
Abstract
  • Purpose To investigate whether event-free survival (EFS) can be maintained among children and adolescents with intermediate-risk (IR) malignant germ cell tumors (MGCT) if the administration of cisplatin, etoposide, and bleomycin (PEb) is reduced from four to three cycles and compressed from 5 to 3 days per cycle. Patients and Methods In a phase 3, single-arm trial, patients with IR MGCT (stage II-IV testicular, II-III ovarian, I-II extragonadal, or stage I gonadal tumors with subsequent recurrence) received three cycles of PEb. A parametric comparator model specified that the observed EFS rate should not be significantly < 92%. As recommended for trials that test a reduction of therapy, a one-sided P value ≤ .10 was used to indicate statistical significance. In a post hoc analysis, we also compared results to the EFS rate of comparable patients treated with four cycles of PEb in two prior studies. Results Among 210 eligible patients enrolled from 2003 to 2011, 4-year EFS (EFS 4 ) rate was 89% (95% confidence interval, 83% to 92%), which was significantly lower than the 92% threshold of the comparison model (P = .08). Among 181 newly diagnosed patients, the EFS 4 rate was 87%, compared with 92% for 92 comparable children in the historical cohort (P = .15). The EFS 4 rate was significantly associated with stage (stage I, 100%; stage II, 92%; stage III, 85%; and stage IV, 54%; P < .001). Conclusion The EFS rate for children with IR MGCT observed after three cycles of PEb was less than that of a prespecified parametric model, particularly for patients with higher-stage tumors. These data do not support a reduction in the number of cycles of PEb from four to three. However, further investigation of a reduction in the number of cycles for patients with lower-stage tumors is warranted.
Author Notes
  • Corresponding author: Furqan Shaikh, Division of Hematology/Oncology, The Hospital for Sick Children, 555 University Avenue, Toronto, Ontario, M5S 1X8, Canada; e-mail: furqan.shaikh@sickkids. ca.
Keywords
Research Categories
  • Health Sciences, Oncology
  • Health Sciences, General

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