Phase I Trial of Carmustine Plus O6-Benzylguanine for Patients With Recurrent or Progressive Malignant Glioma

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Journal of Clinical Oncology, Vol 18, Issue 20 (October), 2000: 3522-3528
© 2000 American Society for Clinical Oncology

Phase I Trial of Carmustine Plus O6-Benzylguanine for Patients With Recurrent or Progressive Malignant Glioma

By Henry S. Friedman, James Pluda, Jennifer A. Quinn, Reginald B. Ewesuedo, Lina Long, Allan H. Friedman, Ilkcan Cokgor, O. Michael Colvin, Michael M. Haglund, David M. Ashley, Jeremy N. Rich, John Sampson, Anthony E. Pegg, Robert C. Moschel, Roger E. McLendon, James M. Provenzale, Elizabeth S. Stewart, Sandra Tourt-Uhlig, Ana M. Garcia-Turner, James E. Herndon, II, Darell D. Bigner, M. Eileen Dolan

From the Departments of Surgery, Medicine, Pathology, Radiology, and Community and Family Medicine, Duke University Medical Center, Durham, NC; Departments of Medicine and Pediatrics, University of Chicago, Chicago, IL; Department of Cellular and Molecular Physiology and Pharmacology, Pennsylvania State University School of Medicine, Milton S. Hershey Medical Center, Hershey, PA; Chemistry of Carcinogenesis, Laboratory, Advanced Bioscience Laboratories, National Cancer Institute, Frederick Cancer Research and Development Center, Frederick; Investigational Drug Branch, National Cancer Institute, National Institutes of Health, Bethesda, MD; and Pediatric Hematology-Oncology, Royal Children’s Hospital, Melbourne, Australia.

Address reprint requests to Henry S. Friedman, MD, DUMC-3624, Duke University Medical Center, Durham, NC 27710; email fried003{at}nc.duke.edu

PURPOSE: The major mechanism of resistance to alkylnitrosoureatherapy involves the DNA repair protein O⁶-alkylguanine-DNAalkyltransferase (AGT), which removes chloroethylation or methylationdamage from the O⁶ position of guanine. O⁶-benzylguanine (O⁶-BG)is an AGT substrate that inhibits AGT by suicide inactivation.We conducted a phase I trial of carmustine (BCNU) plus O⁶-BGto define the toxicity and maximum-tolerated dose (MTD) of BCNUin conjunction with the preadministration of O⁶-BG with recurrentor progressive malignant glioma.

PATIENTS AND METHODS: Patients were treated with O⁶-BG at adose of 100 mg/m² followed 1 hour later by BCNU. Cohorts ofthree to six patients were treated with escalating doses ofBCNU, and patients were observed for at least 6 weeks beforebeing considered assessable for toxicity. Plasma samples werecollected and analyzed for O⁶-BG, 8-oxo-O⁶-BG, and 8-oxoguanineconcentration.

RESULTS: Twenty-three patients were treated (22 with glioblastomamultiforme and one with anaplastic astrocytoma). Four dose levelsof BCNU (13.5, 27, 40, and 55 mg/m²) were evaluated, with thehighest dose level being complicated by grade 3 or 4 thrombocytopeniaand neutropenia. O⁶-BG rapidly disappeared from plasma (eliminationhalf-life = 0.54 ± 0.14 hours) and was converted to alonger-lived metabolite, 8-oxo-O⁶-BG (elimination half-life= 5.6 ± 2.7 hours) and further to 8-oxoguanine. Therewas no detectable O⁶-BG 5 hours after the start of the O⁶-BGinfusion; however, 8-oxo-O⁶-BG and 8-oxoguanine concentrationswere detected 25 hours after O⁶-BG infusion. The mean area underthe concentration-time curve (AUC) of 8-oxo-O⁶-BG was 17.5 timesgreater than the mean AUC for O⁶-BG.

CONCLUSION: These results indicate that the MTD of BCNU whengiven in combination with O⁶-BG at a dose of 100 mg/m² is 40mg/m² administered at 6-week intervals. This study providesthe foundation for a phase II trial of O⁶-BG plus BCNU in nitrosourea-resistantmalignant glioma.

Drs Dolan, Pegg, and Moschel have a financial relationship withProcept, the company that is presently licensing O⁶-benzylguanine.Partial support for the trial was provided by Procept.

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