Division of Hematology/Oncology and Jonsson Comprehensive Cancer Center, University of California, Los Angeles, CA, USA
Received 18 June 2001; revised 26 September 2001; accepted 16 October 2001.
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Abstract |
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5-Fluorouracil (5-FU)-based regimens have not been shown to prolong survival or provide clinical benefit in patients with advanced pancreatic cancer. The purpose of this study was to determine the tolerability of protracted venous infusion (PVI) of 5-FU, modulated by a low dose of the synthetic antifolate trimetrexate, in patients with advanced pancreatic cancer.
Patients and methods
Twenty-three chemotherapy-naïve patients were evaluated. Patients were enrolled in four consecutive cohorts in which the weekly dose of trimetrexate was escalated in 10 mg/m2 increments, from 20 to 50 mg/m2. PVI 5-FU was administered at a fixed dose of 225 mg/m2/day. Treatment was administered for 6 successive weeks, every 8 weeks.
Results
Twenty-two patients were assessable. The maximum tolerated dose of trimetrexate was 40 mg/m2. The most common grade 3 and 4 toxicity was diarrhea. There were no treatment-related deaths. Preliminary analysis of activity revealed a response rate of 9%, with 41% of the patients having stable disease for a median duration of 3.8 months. The median survival for the entire group was 6.9 months (range 129 months). A clinical benefit response was experienced by 27.2% of patients.
Conclusions
Low-dose trimetrexate can be safely administered in combination with PVI 5-FU. This treatment is well tolerated and is associated with palliative activity in advanced pancreatic cancer.
Key words: antifolates, 5-fluorouracil, 5-FU modulation, infusional 5-FU, pancreatic cancer, trimetrexate
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Introduction |
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Trimetrexate is a synthetic folate analog, which potently inhibits dihydrofolate reductase (DHFR) [1719]. As a result of inhibition of purine synthesis, trimetrexate increases intracellular levels of phosphoribosyl pyrophosphate (PRPP), a cofactor for the enzyme orotate phosphoribosyltransferase, which is required for the intracellular conversion of 5-FU to active fluorinated nucleotides. These fluoronucleotides are incorporated into RNA, thus potentiating 5-FU cytotoxicity [20, 21]. Trimetrexate has been reported to enhance the cytotoxicity of 5-FU and folinic acid in vitro [22] in a schedule-dependent manner [20, 23, 24]. Based on these preclinical results, sequential administration of trimetrexate has been studied in patients with colorectal cancer using schedules that employ bolus 5-FU [21, 25].
It is unknown whether trimetrexate-mediated 5-FU modulation occurs using PVI 5-FU. As indicated, increased levels of PRPP mediate RNA and protein synthesis inhibition. However, the putative primary mechanism of action of PVI 5-FU is inhibition of thymidylate synthase (TS), rather than RNA synthesis [2628]. Several lines of evidence lend support to the possibility of synergy between trimetrexate and PVI 5-FU, based on potentiation of TS inhibition in the absence of folinic acid. First, elevation of intracellular PRPP results in increased levels of 5-fluorodeoxyuridine monophosphate (FdUMP), the 5-FU nucleotide involved in TS inhibition. Secondly, inhibition of DHFR by methotrexate is associated with an increase in intracellular levels of dihydrofolate polyglutamates [29]. These metabolites, like folinic acid [30], can complex with TS and FdUMP to enhance TS inhibition [31].
Based on the activity and favorable toxicity profile of PVI 5-FU in phase II studies, which suggests synergy between trimetrexate and 5-FU, and on the above rationale for a potential modulatory effect on PVI 5-FU by trimetrexate, we conducted this dose escalation trial in previously untreated patients with advanced pancreatic cancer. The main objectives of this study were to assess toxicity and to determine maximum tolerated dose. Secondary objectives were response rate, time to treatment failure, survival and clinical benefit.
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Patients and methods |
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Treatment
All patients were treated on an outpatient basis. Patients underwent placement of a central venous catheter for PVI 5-FU infusion. Patients were entered into one of four cohorts to receive trimetrexate glucuronate at 20, 30, 40 or 50 mg/m2 weekly. As folinic acid can exacerbate the toxicity associated with PVI 5-FU, we used lower doses of trimetrexate than those previously employed [21, 25] to avoid the need for folinic acid rescue. We performed dose escalation after treatment of five patients in a prior cohort had been completed without excessive toxicity. In the event that three patients in any given cohort experienced grade 3 or 4 toxicity, dose escalation was terminated and all remaining patients were to be enrolled at the preceding dose level. All patients remained in their cohort of entry until discontinuation from the study. A treatment cycle was defined as 8 weeks and included 6 weeks of chemotherapy followed by a 2-week rest period. Treatment cycles were repeated until either disease progression or unacceptable toxicity supervened.
Trimetrexate glucuronate was supplied by MedImmune Oncology (Gaithersburg, MD, USA) in lyophilized powder (25 mg/vial). The drug was reconstituted and diluted, with 5% Dextrose Water for Injection USP, to obtain concentrations of 0.25 mg/ml to 2 mg/ml. Patients received 2050 mg/m2 of trimetrexate i.v. over 60 min on days 1, 8, 15, 22, 29 and 36 of every 8-week cycle. Patients were to receive folinic acid rescue in the event of grade 4 hematological toxicity. After completion of trimetrexate infusion on day 1, patients received treatment with 5-FU at a dose of 225 mg/m2/day administered as a continuous i.v. infusion during the first 6 weeks of every 8-week cycle.
Dose modifications
All toxicities were graded using the NCI Common Toxicity Criteria version 1. Patients were evaluated weekly for toxicity. In the event of a grade 2 hematological toxicity, the dose of trimetrexate was reduced by 25%. For grade 3 or 4 hematological toxicity, both trimetrexate and 5-FU were withheld until blood counts returned to ANC >2000/mm3 and platelets >100 000/mm3, then the dose of trimetrexate was reduced by 25% for grade 3 and 50% for grade 4, and 5-FU was resumed at a dose of 225 mg/m2. For grade 2, or greater, mucosal ulceration or diarrhea, 5-FU and trimetrexate were discontinued until symptom resolution, and then the doses were resumed as follows: unmodified for grade 2; reduced by 10% for 5-FU and 25% for trimetrexate in the event of grade 3; and by 20 and 50%, respectively, in the event of grade 4. For handfoot syndrome (including pain, erythema, swelling and tenderness in hands and/or feet), both agents were discontinued and treatment was resumed after resolution of symptoms with full dose trimetrexate, 90% dose-reduced 5-FU for grade 3 and 80% for grade 4. The duration of the cycles was not prolonged to compensate for toxicity-related treatment interruptions. Patients whose doses were withheld for 3 consecutive weeks because of any toxicity were terminated from the study.
Assessment of efficacy
Standard radiographic criteria for response were used. Survival and time to treatment failure were assessed prospectively. Clinical benefit analysis was performed using a modified version of methods previously described [4], in which weight was considered a primary measure along with pain and functional status, measured using the KPS scale. Data on these parameters were collected weekly. The pain parameter was a composite of information obtained on pain score and analgesic consumption. Information on pain score was obtained weekly from a brief pain inventory. Records of analgesic consumption were normalized to milligrams of oral morphine sulfate over a 1-week period. KPS was assessed by two observers. Patients were classified as positive, stable or negative for each of the three parameters. To be considered as positive or negative in any parameter, improvements or deteriorations had to be sustained for at least 28 days. Pain was scored as positive if it improved 50% from baseline (assuming an initial minimum pain score of
2 on a 010 scale), as negative if it worsened over baseline and as stable for all other results. Analgesic consumption was scored as positive if it decreased
50% from baseline (assuming an initial minimum of
5 mg of morphine), as negative if it increased from baseline and as stable if any other result. If both pain score and analgesic consumption were positive, or if one was positive and the other remained stable, the patient was classified as positive for clinical pain score. If either or both were negative, the patient was classified as a non-responder and if both remained unchanged the patient was classified as stable. Weight parameter was scored as positive if dry weight increased by
7% from baseline, as negative if it decreased by
4% and stable for all other results. KPS score was considered as positive if it increased by
20%, as negative if it decreased by
20% and as stable for all other results. Patients were classified as positive for overall clinical benefit if at least one of the parameters improved without deterioration of the others and as non-responder if all three parameters remained stable or if any deteriorated.
Statistical methods
Patient survival and time to disease progression were measured in days from study entry and data were summarized by KaplanMeier survivor function estimates and associated confidence intervals. Cox proportional hazards regression was used to assess the effects of trimetrexate dose, treatment time and baseline patient characteristics, on survival and time to progressive disease. Differential incidence of toxicity events across dose levels was analyzed by the 2 test of equivalent incidence, and asso-ciations between trimetrexate dose and toxicity grade were analyzed by the
2 test of association.
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Results |
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Toxicity
Seven patients required dose modifications because of toxicity; in four of them toxicity was grade 3 or 4. One patient (a radiographic and clinical benefit responder) had to be withdrawn from the study because of repeated dose reductions and treatment discontinuations for grade 2 mucositis and handfoot syndrome. This patient was enrolled on the trimetrexate cohort receiving 20 mg/m2. No other toxicity-related study discontinuations occurred. Out of 230 administered doses of trimetrexate and 5-FU in this study, 6% of the doses were withheld because of toxicity, and dose modifications were implemented in 7.3% of the trimetrexate doses and 3.5% of the 5-FU doses. Dose reductions or discontinuations occurred in 21% of patients in cohorts receiving 2040 mg/m2 trimetrexate, and 50% of patients in the 50 mg/m2 cohort.
There were no treatment-related deaths. Grade 3 and 4 toxicity is shown in Table 2. The most common toxicity event leading to drug modification or discontinuation was diarrhea. Diarrhea was also the most common grade 3 and 4 toxicity overall (23% of all patients). Three patients, or 50% of the cohort treated at the 50 mg/m2 dose, experienced grade 4 diarrhea. Therefore, diarrhea was considered the dose-limiting toxicity. One patient in the 50 mg/m2 group experienced a non-neutropenic septic episode that resolved with antibiotic treatment. There were no catheter-related thrombotic episodes, grades 3 or 4, stomatitis, handfoot syndrome or hypersensitivity reactions. The most common grade 1 and 2 non-hematological toxicities were nausea and vomiting (55%), cutaneous (50%), stomatitis (45%), diarrhea (32%) and handfoot syndrome (27%). With regard to hematological toxicity, grades 1 and 2 neutropenia, anemia and thrombocytopenia occurred in 9, 27 and 27% of patients, respectively, across all four cohorts. There were no grade 4 hematological toxicity events. One patient in the 40 mg/m2 cohort experienced grade 3 anemia and neutropenia.
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Activity
Twenty-two patients were assessable for radiographic response. Two patients experienced a partial response (response rate 9%) and nine patients (41%) had stable disease for at least 8 weeks. The two responses lasted 3 and 3.9 months, occurring in one patient with metastatic disease and in another with locally advanced disease, in the 20 mg/m2 and 40 mg/m2 cohorts, respectively. The median duration of stable disease was 3.8 months. The median time to disease progression for the entire group was 2 months (Figure 1). The median survival for the entire group was 6.9 months (range 129 months) and the 1-year survival was 27% (Figure 2). For patients with stage IV disease, median and 1-year survivals were 6.7 months and 26%, respectively. No correlation was observed between baseline patient characteristics or trimetrexate dose, and time to treatment failure or survival. At the time of this analysis, the two responders remain alive at 32 and 25 months from initiation of therapy.
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Discussion |
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In the present study, response seemed to correlate with survival; the two patients that experienced a radiographic response (one with metastatic and one with locally advanced disease) remain alive at 32 and 25 months from initiation of therapy. As a secondary objective of this study, we sought to obtain preliminary evidence of clinical improvement, because symptom control is an important endpoint in the treatment of advanced pancreatic cancer. Our analysis showed a clinical benefit response rate of 27%. However, because the main endpoint of this study was dose finding, with patients treated across a range of trimetrexate doses, these efficacy results should be considered preliminary. It should also be noted that, although the study was opened to community oncologists, reducing the possibility of selection bias, extrapolating these toxicity and activity results to routine clinical practice should take into account that most patients had well-preserved performance status, a relatively uncommon situation in patients presenting with advanced pancreatic cancer.
It is not known whether trimetrexate-mediated 5-FU modulation resulted in enhanced activity over that obtained with unmodulated PVI 5-FU. A randomized study would be required to establish the role of trimetrexate in this treatment schedule. Any benefit of the combination of trimetrexate and 5-FU is unlikely to be derived from a direct cytotoxic action of trimetrexate, as previous studies indicate that trimetrexate, as a single agent, is inactive against pancreatic cancer [34, 35]. Given that 5-FU and gemcitabine do not exhibit cross-resistance in this disease [36], it is conceivable that the regimen described here combined with gemcitabine may result in additive or synergistic activity. The reproducible activity of regimens containing un-modulated PVI 5-FU [1215, 37] and the results reported herein, support further exploration of PVI 5-FU combinations in pancreatic cancer.
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Acknowledgements |
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Footnotes |
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