1 Department of Internal Medicine, Kangnam St Mary's Hospital; 2 Department of Internal Medicine, The Catholic University of Korea, 505 Ban-po dong, Seo Cho Gu; 3 Department of Internal Medicine and 4 Department of Surgery, Yong-Dong Severance Hospital, Yonsei University College of Medicine, Do-gok dong, Kang Nam Gu, Seoul, Korea
* Correspondence to: Dr Jae Yong Cho, Yong-Dong Severance Hospital, Yonsei University Medical College, Do-gok Dong, Kang-nam Gu, Seoul, Korea. Tel: +82-2-3497-3310; Fax: +82-2-3463-3882; Email: chojy{at}yumc.yonsei.ac.kr
![]() |
Abstract |
---|
![]() ![]() ![]() ![]() ![]() ![]() ![]() |
---|
Patients and methods: Forty-four patients received capecitabine 1250 mg/m2 twice daily (2500 mg/m2/day) for 14 days followed by 7 days of rest, for up to six cycles.
Results: Capecitabine produced an objective response rate of 34% (all partial responses) and stable disease in 14 patients (30%). The median time to disease progression (TTP) was 3.2 months [95% confidence interval (CI) 2.76.4 months] and median overall survival was 9.5 months (95% CI 6.913.2 months). Hand-foot syndrome (HFS), nausea, anorexia, diarrhea and vomiting were the most common adverse events. While HFS was the most frequent grade 3/4 toxicity (National Cancer Institute Common Toxicity Criteria), only 9% of patients experienced grade 3 HFS. Severe myelosuppression was not reported during the study.
Conclusions: Capecitabine monotherapy is active and well tolerated as first-line therapy in patients with advanced/metastatic gastric cancer. Larger comparative trials investigating capecitabine-based combination regimens in patients with advanced gastric cancer are warranted.
Key words: capecitabine, gastric cancer, metastatic, untreated
![]() |
Introduction |
---|
![]() ![]() ![]() ![]() ![]() ![]() ![]() |
---|
In a Japanese clinical trial of 60 patients with previously untreated advanced and metastatic gastric cancer, intermittent capecitabine (828 mg/m2 twice daily for 3 weeks followed by 1 week of rest) led to a response rate of 25.5% and a median survival of 8.8 months [6]. A similar response rate (24%) has been observed following administration of capecitabine in combination with epirubicin and cisplatin in 29 patients with inoperable esophago-gastric adenocarcinoma [7
]. In both studies, capecitabine-based therapy was well tolerated. To investigate further the potential of capecitabine in this setting, we evaluated the efficacy and safety of the global standard 3-weekly intermittent capecitabine regimen in an open-label, multicenter, non-comparative, phase II study of previously untreated patients with advanced and/or metastatic gastric cancer.
![]() |
Patients and methods |
---|
![]() ![]() ![]() ![]() ![]() ![]() ![]() |
---|
A detailed medical history, physical and neurologic examinations, chest X-ray, spiral computed tomographic (CT) scan of the abdomen, electrocardiogram, and pregnancy test for women were performed within the 2 weeks before study commencement. Run-in procedures, including vital signs and clinical laboratory tests were performed within 7 days before the start of chemotherapy.
Patients received oral capecitabine 1250 mg/m2 approximately every 12 h for 2 weeks, followed by 1 week of rest, every 3 weeks. Capecitabine was supplied as film-coated tablets in two dose strengths (150 and 500 mg tablets), which patients were instructed not to split. Patients with complete remission (CR), partial remission (PR) or stable disease (SD), and who were tolerating treatment well, were treated for up to six cycles. Those with clearly documented progressive disease (PD) were taken off treatment at the time of progression. Responding patients (CR or PR) or those with SD after 18 weeks were followed until PD, and were able to continue on capecitabine at the discretion of the investigator. Treatment doses were not interrupted or reduced because of toxicities considered by the investigator to be unlikely to become serious or life-threatening. The dosage was adjusted or interrupted for treatment-related adverse events of grade 2 based on a defined algorithm [8
].
Tumor assessments, according to WHO criteria [9] were performed at 6-week intervals by the investigators and an Independent Review Committee (IRC). Tumor lesions were assessed by CT scan, X-rays or magnetic resonance imaging (MRI), and objective tumor response was based on the dimensions of measurable marker lesions, measured by the same radiologist throughout the study. TTP was calculated as the time from the first treatment to the time the patient was first recorded as having PD, or the date of death if the patient died before PD was demonstrated. Survival was monitored every 3 months after the patient completed treatment.
Safety was monitored throughout the study and for 28 days after the last study treatment. Adverse events were graded according to the National Cancer Institute of Common Toxicity Criteria. Hand-foot syndrome (HFS) was graded as in previous capecitabine studies [10]. Patients were educated to recognize grade
2 toxicity and to interrupt capecitabine until further instructed by their physician.
The response rate was expected to be 25% based on data from a previous Japanese phase II trial [6
]. A sample size of 38 was calculated by Fleming's single-stage design [11
] to ensure at least 80% power for proving lack of efficacy if the true response rate was <25%. Estimating a drop-out rate of 15%, a total of 44 patients were recruited to ensure that at least 38 patients were evaluable. TTP and survival were analyzed by the KaplanMeier product limit method. Patients who received at least one dose of study medication were included in the intention-to-treat (ITT) analysis. Those who did not receive at least one dose of study medication or for whom no follow-up safety information was available were excluded from the safety analysis.
![]() |
Results |
---|
![]() ![]() ![]() ![]() ![]() ![]() ![]() |
---|
|
|
|
Safety
The most common treatment-related clinical adverse events were HFS (68%), nausea (27%), diarrhea (27%) and anorexia (21%). Most events were mild to moderate in severity and did not exceed grade 2 (Figure 2). The predominant grade 3 toxicities were HFS, diarrhea and anorexia. One patient experienced a grade 4 genital rash, although no other grade 4 toxicity or toxicity-related deaths were reported. The most common events leading to treatment modification were HFS, nausea, vomiting, diarrhea, leukopenia and pyrexia.
|
There were 23 deaths reported during the study, the majority of which occurred >28 days after the end of the planned treatment schedule. All of the deaths were related to PD.
![]() |
Discussion |
---|
![]() ![]() ![]() ![]() ![]() ![]() ![]() |
---|
The median treatment duration was 61 days (range 7196 days) and the mean relative dose intensity was 91%, which is higher than that reported in previous studies in colon cancer [15] and gastric cancer [6
, 7
]. The higher dose intensity in the current study might be one of the possible explanations for our higher response rate compared with the previous Japanese trial reported by Kondo, in which patients received a lower dose 4-weekly regimen [6
]. It is also important to acknowledge that 10 patients (23%) had undergone one or more surgical intervention for gastric cancer, which could impact on the absorption of orally administered drugs. While there are no pharmacokinetic data on the use of capecitabine in patients following gastric surgery [16
], neither our findings nor those from previous studies of capecitabine suggest that previous surgery impacts on the efficacy of capecitabine in this setting.
The safety profile of capecitabine in this trial is similar to that observed with a 4-weekly capecitabine regimen in patients with advanced/metastatic gastric cancer [6], capecitabine plus epirubicin, and cisplatin in patients with inoperable esophago-gastric adenocarcinoma [7
], and compares favorably with that of 5-FU-based regimens in similar patient populations [13
, 14
]. Importantly, very few patients (5%) experienced grade 3 diarrhea, and capecitabine was minimally myelosuppressive and did not cause significant hair loss. The predominant treatment-related grade 3 adverse event was HFS (9%), which is a well known adverse event related to chronic fluoropyrimidine exposure, and is one of the most commonly reported adverse events following treatment with capecitabine [17
]. HFS is manageable with therapy interruption and, if necessary, dose reduction, and is never life threatening.
These efficacy and safety findings, together with the striking 9:1 patient preference for oral rather than i.v. chemotherapy as treatment for late-stage disease [1820
], indicate that capecitabine is unique among currently available treatments for gastric cancer in that it is compatible with oral, patient-oriented, home-based therapy. Larger, randomized trials of capecitabine, either as a single agent or in combination with other highly active drugs, possibly incorporating pharmacoeconomic and quality of life end points, are clearly warranted in the first-line setting. Ongoing phase III trials include a Korean study of capecitabine/cisplatin versus 5-FU/cisplatin in patients with previously untreated advanced/metastatic gastric cancer, and a UK, four-arm trial evaluating capecitabine plus 5-FU and oxaliplatin plus cisplatin in patients with advanced esophago-gastric cancer [21
].
![]() |
Acknowledgements |
---|
Received for publication October 6, 2003. Revision received April 20, 2004. Accepted for publication April 26, 2004.
![]() |
References |
---|
![]() ![]() ![]() ![]() ![]() ![]() ![]() |
---|
2. Cao S, Lu K, Ishitsuka H et al. Antitumor efficacy of capecitabine against fluorouracil-sensitive and resistant tumors. Proc Am Soc Clin Oncol 1997; 16: 226a (Abstr 795).
3. Miwa M, Ura M, Nishida M et al. Design of a novel oral fluoropyrimidine carbamate, capecitabine, which generates 5-fluorouracil selectively in tumours by enzymes concentrated in human liver and cancer tissue. Eur J Cancer 1998; 34: 12741281.[CrossRef][ISI][Medline]
4. Budman DR, Meropol NJ, Reigner B et al. Preliminary studies of a novel oral fluoropyrimidine carbamate: capecitabine. J Clin Oncol 1998; 16: 17951802.[Abstract]
5. Mackean MJ, Planting AS, Twelves C et al. Phase I and pharmacological study of intermittent twice-daily oral therapy with capecitabine in patients with advanced and/or metastatic cancer. J Clin Oncol 1998; 16: 29772985.[Abstract]
6. Kondo K, Chin K, Sakamoto J et al. A multicenter phase II trial using 4-week cycles of capecitabine in advanced/metastatic gastric cancer (AGC). Proc Am Soc Clin Oncol 2003; 22: 321 (Abstr 1289).
7. Evans TR, Pentheroudakis G, Paul J et al. A phase I and pharmacokinetic study of capecitabine in combination with epirubicin and cisplatin in patients with inoperable oesophago-gastric adenocarcinoma. Ann Oncol 2002; 13: 14691478.
8. Blum JL, Jones SE, Buzdar AU et al. Multicenter phase II study of capecitabine in paclitaxel-refractory metastatic breast cancer. J Clin Oncol 1999; 17: 485493.
9. World Health Organization (WHO). Handbook for Reporting Results of Cancer Treatment. Publication No. 48. Geneva: WHO; 1979.
10. Van Cutsem E, Hoff PM, Harper P et al. Oral capecitabine vs intravenous 5-fluorouracil and leucovorin: integrated efficacy data and novel analyses from two large, randomized, phase III trials. Br J Cancer 2004; 90: 11901197.[CrossRef][ISI][Medline]
11. Fleming TR. One-sample multiple testing procedure for phase II clinical trials. Biometrics 1982; 38: 143151.[ISI][Medline]
12. Karpeh MS, Kelsen DP, Tepper JE. Cancers of the gastrointestinal tract: cancer of the stomach. In De Vita VT, Hellman S, Rosenberg SA (eds): Cancer: Principles and Practice of Oncology, 6th edition. Philadelphia, PA: Lippincott Williams and Wilkins; 2001.
13. Constenla M, Garcia-Arroyo R, Lorenzo I et al. Docetaxel, 5-fluorouracil and leucovorin as treatment for advanced gastric cancer: results of a phase II study. Gastr Cancer 2002; 5: 142147.[CrossRef]
14. Cascinu S, Baldelli AM, Catalano V et al. Infusional 5-fluorouracil, cisplatin and mitomycin C in advanced gastric cancer: a low cost effective regimen. Br J Cancer 2002; 86: 213217.[CrossRef][ISI][Medline]
15. Van Cutsem E, Findlay M, Osterwalder B et al. Capecitabine, an oral fluoropyrimidine carbamate with substantial activity in advanced colorectal cancer: results of a randomized phase II study. J Clin Oncol 2000; 18: 13371345.
16. Reigner B, Blesch K, Weidekamm E. Clinical pharmacokinetics of capecitabine. Clin Pharmacokinet 2001; 40: 85104.[ISI][Medline]
17. Cassidy J, Twelves C, Van Cutsem E et al. Capecitabine Colorectal Cancer Study Group. First-line oral capecitabine therapy in metastatic colorectal cancer: a favorable safety profile compared with intravenous 5-fluorouracil/leucovorin. Ann Oncol 2002; 13: 566575.
18. Payne SA. A study of quality of life in cancer patients receiving palliative chemotherapy. Soc Sci Med 1992; 35: 15051509.[CrossRef][ISI][Medline]
19. Liu G, Franssen E, Fitch MI et al. Patient preference for oral versus intravenous palliative chemotherapy. J Clin Oncol 1997; 15: 110115.[Abstract]
20. Borner MM, Schoffski P, de Wit R et al. Patient preference and pharmacokinetics of oral modulated UFT versus intravenous fluorouracil and leucovorin: a randomised crossover trial in advanced colorectal cancer. Eur J Cancer 2002; 38: 349358.[CrossRef][ISI][Medline]
21. Tebbutt N, Norman A, Cunningham D et al. Randomised, multicentre phase III study comparing capecitabine with fluorouracil and oxaliplatin with cisplatin in patients with advanced esophago-gastric cancer; interim analysis. Proc Am Soc Clin Oncol 2002; 21: 131a (Abstract 523).