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Clinical Therapy Trials—Drug |
University of California, San Francisco (M.D.P., K.L., S.C., M.K.N.), San Francisco, CA 94143; University of Texas M.D. Anderson Cancer Center, Houston, TX 77030 (W.K.A.Y., K.J., K.H.); University of Wisconsin Medical Center, Madison, WI 53792 (H.I.R., M.M.); National Institutes of Health, Bethesda, MD 20892 (H.F.); Dana-Farber/Brigham and Women's Cancer Center, Boston, MA 02115 (P.Y.W.); University of California, Los Angeles, Los Angeles, CA 90095 (T.C.); University of Virginia Health Science Center, Charlottesville, VA 22908 (D.S.); University of Michigan Medical Center, Ann Arbor, MI 48109 (H.G., L.J.); University of Texas Southwestern Medical Center, Dallas, TX 75390 (K.F.); and University of Texas Health Sciences Center, San Antonio, TX 78229 (J.K.); USA
2 Address correspondence to Michael Prados, University of California, San Francisco, 400 Parnassus Avenue, Room A808, San Francisco, California 94143-0372 (pradosm{at}neurosurg.ucsf.edu).
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Abstract |
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 Top Abstract IntroductionPatients and MethodsResultsDiscussionReferences |
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Key Words: clinical trial • irinotecan • phase 2 • recurrent malignant glioma
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Introduction |
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TopAbstractIntroductionPatients and MethodsResultsDiscussionReferences |
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Based on the aforementioned background, the North American Brain Tumor Consortium (NABTC) completed a phase 1 study of CPT-11 in patients on EIAED to determine the optimal phase 2 dose when given every three weeks, and to compare the pharmacokinetics with those in patients not on EIAED who are treated at the recommended phase 2 dose for other cancers (Prados et al., 2004). The recommended phase 2 dose was 750 mg/m2 given every three weeks to patients on EIAED. A phase 2 study was then conducted based on the results of the phase 1 trial. Patients not on EIAED were treated at a dose of 350 mg/m2. This report details the results of the phase 2 study.
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Patients and Methods |
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60, and acceptable hematologic, liver, and renal function. The latter required an absolute neutrophil count of 1500/mm3 and platelet count of 100,000/mm3, serum creatinine level <1.5 mg/dl, serum bilirubin level <1.5 mg/dl, and aspartate aminotransferase level less than three times the institutional upper normal limits. Patients in this study had undergone no more than one prior chemotherapy regimen, including either one prior adjuvant therapy or one prior regimen for recurrent tumor. Patients not on EIAED (group A) received a dose of 350 mg/m2, and patients on EIAED (group B) were treated at a dose of 750 mg/m2. In both groups, the interval from prior irradiation or chemotherapy had to be at least four weeks, and six weeks if prior nitrosourea therapy had been used. All patients had a retrospective central neuropathology review. Patients previously treated with CPT-11, topotecan, or other topoisomerase 1 inhibitors were excluded. All patients were provided with and had to sign a written informed consent approved by the local Institutional Review Board at each institution before treatment, informing them of the investigational nature of this study.
Treatment
Patients who met eligibility requirements received an intravenous infusion of CPT-11 over a 90-min period every three weeks. Patients continued to receive this dose throughout treatment until tumor progression, unacceptable toxicity, or completion of 12 treatment cycles. A treatment cycle was considered one infusion and a three-week evaluation period. No dose escalation was allowed. Dose reduction was allowed if during the prior infusion there had been evidence of toxicity as defined by the NCI Common Toxicity Criteria version 2.0 scale.
Patient Monitoring and Toxicity Assessment
Complete physical and neurological examinations, including KPS, were performed every other cycle. Weekly complete blood counts with differential and platelets were obtained throughout treatment. Levels of creatinine, blood urea nitrogen, total bilirubin, aspartate aminotransferase, and serum electrolytes were measured before each cycle. Magnetic resonance imaging of the brain was done every other cycle to assess response. Patients with stable or responding disease received the same dose at the next cycle or a reduced dose if adverse events were observed in the current cycle. If a patient experienced grade 3 or greater nonhematologic toxicity or grade 4 hematologic toxicity, the dose of the subsequent cycle was reduced by one level (50 mg/m2). If the toxicity was thought to be directly related to CPT-11, subsequent doses were not reescalated, even if there was minimal or no toxicity at the reduced dose. A new course of treatment could begin if the absolute neutrophil count was 1500/mm2, the platelet count was 100,000/mm3, and any other treatment-related toxicities were 
grade 1. If, after a one-week delay, toxicities were grade 1, treatment resumed. If the toxicity did not resolve in one week, a second one-week delay was allowed, but retreatment required a reduction of one dose level. If retreatment had to be held off for more than two weeks, or if the administered dose would be 200 mg/m2, the patient was removed from the study.
Patients were removed from study if tumor progression was determined by MRI. The definition of progression was a 25% increase in the sum of the products of all measurable disease over the smallest sum observed, a clear worsening of any evaluable disease, or the appearance of any new lesion. Failure to return for evaluation due to death or deteriorating condition was considered to represent disease progression. Although this was not an imaging response study, claimed responses by the individual investigator were recorded as either partial response (decrease in cross-sectional area by 50% with stable or improving steroids) or stable disease (less than a partial response, but not qualified as progression). There was no central review of claimed partial responses.
Statistical Considerations
The goal of this study was to determine whether CPT-11 could significantly delay progression in patients with recurrent malignant glioma. The primary end point was progression-free survival at six months (PFS-6). The trial cohort includes both GBM and AG patients who were entered at an anticipated 2:1 ratio. The trial was sized to be able to discriminate between a 20% and 40% rate of PFS-6 for the entire cohort and a 15% and 35% rate for the GBM group alone. The GBM comparison is the one of primary concern. With accrual of 32 GBM patients, the trial would be considered a success if at least eight GBM patients showed PFS-6. This would give a 0.92 probability of detecting a 35% rate of PFS-6, with 0.9 probability of rejecting the agent if the PFS-6 were only 15%. Assuming an accrual of approximately 16 AG patients, there would be a reasonable power to discriminate between a 20% and 40% rate of PFS-6 for the entire group. For the group as a whole, CPT-11 would be considered effective if there was at least 30% PFS-6. This would give at least a 0.9 probability of detecting a 40% rate of PFS-6, with at least a 0.9 probability of rejecting the drug if the PFS-6 was only 20%. Because central neuropathology review was done retrospectively, a small increase in patient numbers (five additional patients) was allowed in order to have a sufficient number of eligible patients with GBM, the cohort of primary concern. As noted below, the final result of GBM enrollment was higher than anticipated.
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Results |
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Toxicity
Only four patients discontinued treatment because of toxicity; the remainder continued treatment until tumor progression or the completion of planned therapy. The majority of recorded toxicities were grade 1 and grade 2. Grade 3 and 4 toxicities were more frequent in patients not on EIAEDs (group A), including a higher rate of grades 3 and 4 granulocytopenia. Patients on EIAEDs (group B) had no grade 4 toxicities, and patients in group A had 10 grade 4 events (all hematologic).
Efficacy
The primary end point was the number of patients who were progression free at six months. Overall, the PFS-6 for the entire group was 17.6% (9 of 51 patients). Of the 13 AG patients, three were known to have time to progression longer than six months (95% confidence interval [CI], 0.07-0.52, response rate). Of the 38 grade 4 patients, six were known to have time to progression of longer than six months (95% CI, 0.07-0.31, response rate). Thus, even with a slight increase in eligible patients with GBM, only six of 38 met the PFS-6 target rather than the eight of 32 anticipated for calling this a successful regimen, and the upper bound of the 95% CI was less than 35%. For the entire group of 51 patients, the best claimed radiographic response was immediate disease progression in 30, stable disease in 17, and partial responses (PRs) in three (5.8% PR rate). One patient was not evaluable for response because the patient was treated with only one cycle of CPT-11 and was removed because of toxicity prior to MRI.
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Discussion |
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TopAbstractIntroductionPatients and MethodsResultsDiscussionReferences |
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A number of clinical trials have now been reported using CPT-11 in various schedules and doses. Friedman et al. (1999) reported 60 patients (48 GBM patients) treated at a dose of 125 mg/m2 once weekly for four weeks with a two-week break. Of these, nine (15%) had a PR and 33 (55%) had stable disease. Median time to tumor progression was 18 weeks in the GBM group, but ranged from 6 to 68+ weeks at the time of the report. The PFS-6 was not described. Friedman et al. concluded that CPT-11 was active and likely to have more activity with strategies to increase drug exposure. Chamberlain (2002) reported a phase 2 study of 40 patients with recurrent GBM, treated with a starting dose of 400 mg/m2, which was increased to 500 mg/m2 every three weeks. Fifteen patients were not receiving EIAEDs. In this study, the disease of all patients progressed within six weeks, and the author concluded the drug was ineffective in this patient population. Cloughesy et al. (2003) reported on two studies using a three-week schedule. In the first group, 14 patients were treated at a starting dose of 300 mg/m2, which was escalated ultimately to 350 mg/m2. There were two PRs and two patients with stable disease, with median time to tumor progression of six weeks. The second group of 35 patients (26 with GBM) was treated with intrapatient dose escalation, increasing the dose by 100 mg/m2 increments (based on toxicity of the prior infusion) every three weeks. Dose-limiting toxicity ranged from 400 to 1700 mg/m2, with three cases of PR and 15 with stable disease. Median time to tumor progression was 2.7 months, and the estimated PFS-6 was 26% (confidence intervals not given). The authors concluded that the drug was active and that a higher level of efficacy might be possible if an MTD could be established for each patient. Raymond et al. (2003) reported a phase 2 study using a dose of 350 mg/m2 every three weeks, with the preferred anticonvulsant being valproic acid. Twenty-five patients were treated prior to radiation, and the remaining patients were treated following disease progression after radiotherapy. All patients were chemotherapy naive. The overall response rate was 2.2%, estimated PFS-6 was 46%, and median time to tumor progression was 14.4 weeks in the patients whose disease recurred after radiotherapy. The authors concluded that CPT-11 has limited clinical activity as a single agent. Buckner et al. (2003) summarized the results of two sequential phase 2 studies conducted by the North Central Cancer Treatment Group. The first trial treated patients with a dose of either 125 mg/m2 or 100 mg/m2 weekly for four weeks with a two-week break, using the lower dose if prior nitrosourea therapy had been given. The second trial used a dose of 300 mg/m2 or 250 mg/m2 given once every three weeks, using the lower dose in cases of prior nitrosourea treatment. A total of 64 patients were enrolled in both studies. The response rate was 10%, but the duration of the response was not reported.
None of the aforementioned studies systematically investigated the efficacy of CPT-11 based on an MTD pharmacologically derived in patients on or not on EIAEDs. However, Batchelor et al. (2004) reported on a multicenter, two-stage, phase 2 study of weekly administration of CPT-11, using a dose based on the prior phase 1 study conducted by the New Approaches to Brain Tumor Treatment (NABTT) consortium. Patients on EIAEDs were treated with a dose of 411 mg/m2 weekly for four weeks, and those not on EIAEDs were treated with a dose of 117 mg/m2 weekly for four weeks, followed by a two-week break. The estimated PFS-6 was 56% (95% CI, 31%-79%). The response rate was 6% of the 18 patients (12 with GBM) treated in the first stage of this study. Because of the low response rate, the study was terminated after the first stage. The authors concluded that CPT-11 has minimal efficacy in this patient setting.
The current study, similar to the NABTT trials, sought to evaluate the clinical efficacy of CPT-11 based on the pharmacokinetics of this agent, and as in the former study, little benefit was found in use of the drug. It appears that either dose schedule (weekly for four weeks or every three weeks) is ineffective in patients with recurrent malignant glioma, both in terms of objective response rates or duration of response. However, given the observation that some patients had objective responses, the drug may be of some use in other treatment settings, such as in combination with other agents or radiotherapy. We would conclude this drug as a single agent has little efficacy and should not be used in patients with recurrent malignant glioma.
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Acknowledgments |
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Footnotes |
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3 Karen Fink is currently with baylor University Medical center in Dallas. M. Kelly Nicholas is currently with the University of chicago brain tumor center.
4 Abbreviations used are as follows: AG, anaplastic glioma; AUc, area under the concentration-time curve; cI, confidence interval; cPt-11, irinotecan; eIAeD, enzyme-inducing antiepileptic drug; GbM, glioblastoma multiforme; Gcrc; General clinical research center; MtD, maximum tolerated dose; NAbtc, North American brain tumor consortium; NAbtt, New Approaches to brain tumor treatment consortium; PFS-6, six-month progression-free survival; Pr, partial response.
Received for publication September 26, 2005. Accepted for publication December 20, 2005.
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References |
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Batchelor, T.T., Gilbert, M.R., Supko, J.G., Carson, K.A., Nabors, L.B., Grossman, S.A., Lesser, G.J., Mikkelsen, T., and Phuphanich, S. (2004) Phase 2 study of weekly irinotecan in adults with recurrent malignant glioma: Final report of NABTT 97-11. Neuro-Oncology 6, 21-27.[Abstract]
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