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Efficacy of vincristine and etoposide with escalating cyclophosphamide in poor-prognosis pediatric brain tumors¹

Centre for Children's Cancer and Blood Disorders, Sydney Children's Hospital, Randwick, New South Wales 2031 (D.S.Z., R.J.C., C.O., L.W.); School of Women's and Children's Health, University of New South Wales, Kensington, New South Wales (D.S.Z., R.J.C., L.W.); Oncology Unit, Children's Hospital at Westmead, Westmead, New South Wales (G.M.); Haematology and Oncology Department, John Hunter Hospital, New South Wales (F.A.); and Amgen Australia, Pty. Ltd., Melbourne, Victoria 3122 (R.M.); Australia

² Address correspondence to Richard J. Cohn, Centre for Children's Cancer and Blood Disorders, Sydney Children's Hospital, High St., Randwick, NSW 2031, Australia (r.cohn{at}unsw.edu.au).

The objective of this study was to assess the efficacy of the VETOPEC regimen, a regimen of vincristine and etoposide with escalating doses of cyclophosphamide (CPA), in pediatric patients with high-risk brain tumors. Three consecutive studies by the Australia and New Zealand Children's Cancer Study Group—VETOPEC I, Baby Brain 91, and VETOPEC II—have used a specific chemotherapy regimen of vincristine (VCR), etoposide (VP-16) and escalating CPA in patients with relapsed, refractory, or high-risk solid tumors. Patients in the VETOPEC II cohort were treated with very high dose CPA with peripheral blood stem cell (PBSC) rescue. We analyzed the subset of patients with high-risk brain tumors treated with these intensive VETOPEC-based protocols to assess the response, toxicity, and survival. We also assessed whether the use of very high dose chemotherapy with stem cell rescue improved the response rate or affected toxicity. Seventy-one brain tumor patients were treated with VETOPEC-based protocols. Of the 54 patients evaluable for tumor response, 17 had a complete response (CR) and 20 a partial response (PR) to treatment, which yielded an overall response rate of 69%. The CR + PR was 83% (19/23) for medulloblastomas, 56% (5/9) for primitive neuroectodermal tumors, 55% (6/11) for grade 3 and 4 astrocytomas, and 80% (6/8) for ependymomas. At a median follow-up of 36 months, overall survival for the entire cohort of 71 patients was 32%, with event-free survival of 13%. There were no toxic deaths within the PBSC-supported VETOPEC II cohort, despite higher CPA doses, compared with 7% among the non-PBSC patients. This regimen produces high response rates in a variety of very poor prognosis pediatric brain tumors. The maximum tolerated dose of CPA was not reached. Higher escalation in doses of CPA did not deliver a further improvement in response. With PBSC rescue in the VETOPEC II study, hematologic toxicity was no longer a limiting factor. The response rates observed support further development of this chemotherapy regimen.

Key Words: brain tumor • childhood • cyclophosphamide • high-dose chemotherapy • stem cell transplant