Feasibility of oral administration of S-1 as adjuvant chemotherapy in gastric cancer: 4-week S‑1 administration followed by 2-week rest vs. 2-week administration followed by 1-week rest
- Authors:
- Published online on: February 2, 2015 https://doi.org/10.3892/mco.2015.500
- Pages: 527-532
Abstract
Introduction
S-1, is an oral fluoropyrimidine anticancer agent that was developed in Japan and was approved as an effective drug for gastric cancer in 1999. This agent combines tegafur, a prodrug of 5-Fluorouracil (5-FU), with gimeracil, a reversible antagonist of the rate-limiting enzyme in the 5-FU degradation pathway and oteracil potassium, a reversible inhibitor of the phosphoenzyme of 5-FU that reduces gastric toxicity, in order to increase the concentration of 5-FU in the blood, thereby enhancing antitumor efficacy but reducing gastric toxicity that typically occurs with increased concentrations (1). The response rates for single-agent S-1 in advanced recurrent gastric cancer were 53.6% (15/28) and 44.6% (45/101) in an early phase II and late phase II trial, respectively. S-1 has been widely used as first-line treatment for gastric cancer and has the highest response rate among anticancer drugs indicated for gastric cancer (2–5).
In 2006, the results of an interim analysis of a clinical trial in patients undergoing resection for gastric cancer, namely the Adjuvant Chemotherapy Trial of S-1 for Gastric Cancer (ACTS-GC), were presented in order to report the benefits of S-1-based adjuvant chemotherapy following surgery in gastric cancer (6). This study was conducted using a 4-week administration schedule for S-1 followed by a 2-week rest period in patients with stage II (excluding T1), IIIA or IIIB gastric cancer who underwent curative R0 or R1 resection with no residual tumor by standard gastric cancer surgery (D2 lymph node dissection). In the group where the treatment regimen was administration of S-1 for 4 weeks followed by 2 weeks of rest, which was continued for 1 year, the risk of death was reduced by 32% and The survival rates at 3 years POST-surgery were 70.1 and 80.5% in the surgery-alone and S-1 groups, respectively, demonstrating a survival benefit with S-1 treatment. With the most frequent ≥Grade 3 adverse event being anorexia at 5.7%, postoperative adjuvant chemotherapy with S-1 has become the standard treatment for patients with stage II or III gastric cancer undergoing curative resection. However, compliance to the S-1 treatment is far from ideal, with 87.4% of the patients compliant at 3 months, 77.9% at 6 months, 70.8% at 9 months and 65.8% at 12 months. Studies investigating alternative dosing regimens to fully exploit the efficacy of S-1 while reducing adverse reactions are required.
A feasibility study of S-1 as postoperative adjuvant chemotherapy using a 2-week administration regimen followed by a 1-week rest period was previously conducted in locally advanced squamous cell carcinoma of the head and neck (SCCHN) in order to increase the compliance to the S-1 therapy. In that study, treatment of scchn with S-1 was continued for 6 months as a 2-week administration/1-week rest (2-week/1-week) regimen or a 4-week administration/2-week rest (4-week/2-week) regimen. The treatment completion rate was reported to be 40 and 29.4%, the ratio of S-1 relative cumulative dose 54.9 and 34.3% and the frequency of ≥Grade 3 adverse events 8 and 17.6% for the 2-week/1-week and 4-week/2-week regimens, respectively (7). These results suggested that the reduction of adverse events by using the 2-week/1-week regimen exerted a significant positive effect on the completion rate of S-1 treatment. However, no distinct evidence associated with the efficacy of the 2-week/1-week regimen as postoperative adjuvant chemotherapy in gastric cancer has been reported.
We conducted a multicenter, randomized clinical trial to investigate the completion rate of treatment using the 4-week/2-week regimen and the 2-week/1-week regimen as postoperative adjuvant chemotherapy with S-1 in order to establish a safer postoperative adjuvant chemotherapy regimen while achieving higher treatment compliance in gastric cancer patients.
Patients and methods
Patients
Among The patients who underwent R0 or R1 surgical resection for stage II (excluding T1), IIIA or IIIB gastric cancer between May, 2008 and February, 2010, 47 patients were enrolled in this study.
Treatment schedule
The patients were randomly assigned to arm A (4-week/2-week treatment regimen arm; N=25); and arm B (2-week/1-week treatment regimen arm; N=22), with the goal of administering S-1 for 1 year. In arm A (4-week/2-week arm), S-1 was orally administered twice a day (after breakfast and dinner) for 28 consecutive days, followed by a 14-day rest period, as a 6-week (42 days) course for a total of 1 year. In arm B (2-week/1-week arm), S-1 was orally administered twice a day (after breakfast and dinner) for 14 consecutive days, followed by a 7-day rest period as a 3-week (21 days) course for a total of 1 year (Fig. 1). The initial dose of S-1 was determined based on The estimated creatinine clearance calculated using the Cockcroft-Gault formula and using age, body weight and serum creatinine at baseline and body surface area. Patients with a body surface area of <1.25 m2 received 80 mg daily; those with a body surface area of 1.25 m2 to <1.5 m2 received 100 mg daily; and those with a body surface area of ≥1.5 m2 received 120 mg daily.
Toxicity
In the event of toxicity [National Cancer Institute Common Toxicity Criteria (NCI-CTC) version 3.0], the following treatment delays and dose reductions were planned: S-1 administration on day 1 in subsequent cycles was delayed when there was a leukocyte count <2,000/mm3; neutrophil count <1,000/mm3; platelet count <75,000/mm3; aspartate aminotransferase (AST) and alanine aminotransferase (ALT) levels >150 IU/l; and serum creatinine >1.5 mg/dl. If these toxicities exhibited a causal relationship with S-1, or in cases with creatinine clearance ≥50 to <80 ml/min prior to the initiation of a new course, the daily dose of S-1 was reduced from 120–100 mg, from 100–80 mg or from 80–50 mg twice daily, but the minimal daily dose was maintained at 40 mg twice daily. Treatment was continued until disease progression, unacceptable toxicity, patient refusal or physician decision.
Inclusion criteria
The eligibility criteria for patient enrollment were as follows: i) Patients who had pathologically confirmed gastric cancer; ii) patients who underwent R0 or R1 surgical resection with D2 or more extended lymph node dissection; iii) patients with stage II (excluding T1), IIIA or IIIB gastric cancer based on comprehensive findings; iv) patients aged 20–75 years at enrollment; v) patients who had not undergone pretreatment other than surgical treatment (radiological, chemical and/or hormonal therapy); vi) patients who were able to tolerate oral administration within 6 weeks after surgery; vii) patients who had no severe postoperative complications and met the following criteria for postoperative laboratory parameters: white blood cell count ≥4,000/mm3 and <12,000/mm3; neutrophil count ≥2,000/mm3; platelet count ≥10×104/mm3; hemoglobin ≥9.0 g/dl; total bilirubin ≤1.5 mg/dl; AST (SGOT) and ALT (SGPT) <100 IU/l; serum creatinine ≤upper limit of the institutional standard; creatinine clearance based on the Cockcroft-Gault formula ≥50 ml/min; and viii) patients who provided written informed consent.
Exclusion criteria
The exclusion criteria were as follows: i) Patients with simultaneous or metachronous double/multiple cancers; ii) patients with contraindications to S-1 treatment; iii) patients requiring use of flucytosine, phenytoin and warfarin potassium; iv) patients with a history of ≥Grade 3 drug allergy; v) patients with severe complication(s), such as intestinal paresis, ileus, interstitial pneumonia or pulmonary fibrosis, uncontrolled diabetes, heart, renal and/or hepatic failure; vi) patients with diarrhea; vii) pregnant women, lactating women and women intending to become pregnant; viii) men who intend to reproduce; ix) human immunodeficiency virus-positive patients; and x) patients who were considered by the investigator or subinvestigator to be unsuitable for this study.
The classification of pathological stage for resected tumors was based on the Japanese classification of gastric carcinoma (8).
Approval for implementing this study was obtained from The Institutional Review Boards of Okayama University and Kawasaki Medical School. Written informed consent was provided from all the participating subjects.
Statistical methods
The primary endpoint was the treatment completion rate in stage II and III gastric cancer treated with the 4-week/2-week or 2-week/1-week regimen of S-1 as adjuvant chemotherapy. The sample size was estimated to be 57 to correctly select a better treatment with probability (P=0.95) based on the expectation that a 15% difference would be observed in the treatment completion rate between the two arms. Taking ineligible patients into account, the sample size was set at 60 for each arm. Safety (NCI-CTC version 3.0), relapse-free survival and overall survival were observed as secondary endpoints. Completion rate was calculated by dividing the number of patients who continued treatment by the total number of patients. The relapse-free survival was defined as the time from the date of registration to the date of confirmed recurrence or death from any cause, rather than the date of treatment discontinuation. The overall survival was defined as the time interval from the date of registration to the date of death from any cause. Survival curves were estimated using the Kaplan-Meier method and differences were analyzed using the stratified log-rank test.
Results
Patient characteristics
Enrollment in this study was completed at the end of February, 2010. The baseline characteristics of the patients are summarized in Table I. There was no significant difference in any characteristic between the two arms. Subsequently, an analysis of data was initiated to evaluate the completion rates of treatment.
Treatment continuation rates
The treatment continuation rates for S-1 were 88 and 100% at 3 months, 83 and 100% at 6 months and 49 and 89% at 12 months after the initiation of S-1 treatment for the 4-week/2-week and the 2-week/1-week arms, respectively, with the 2-week/1-week arm being superior to the 4-week/2-week arm (P=0.0046) (Fig. 2, Table II).
Adverse events
Adverse events were analyzed for all The patients. The frequency of adverse events was 92 and 77.3% for the 4-week/2-week and 2-week/1-week arms, respectively. Grade 3 adverse events included anorexia (8.0 and 0%), nausea (4.0 and 0%), vomiting (4.0 and 0%), fatigue (8.0 and 0%), pigmentation (0 and 4.8%), diarrhea (4.0 and 0%), decreased hemoglobin concentration (4.0 and 4.8%), hand-foot syndrome (4.0 and 0%) and hypoalbuminemia (4.0 and 0%), with a tendency toward lower rates observed in the 2-week/1-week arm. No ≥grade 4 adverse events were observed in either arm (Table III).
Discussion
For the treatment of gastric cancer, which has a high incidence among Japanese individuals, curative surgery is the optimal therapeutic approach. Although a wide variety of postoperative adjuvant chemotherapy options for gastric cancer have been investigated in order to improve The outcome of surgery, S-1 has become the standard adjuvant chemotherapy following gastric cancer surgery in Japan, based on the results of the ACTS-GC study. However, compliance to S-1 treatment was not satisfactory in the ACTS-GC study and an improvement in compliance remains an issue that must be addressed.
The 4-week administration of S-1 followed by a 2-week rest regimen has been established as the standard regimen for S-1 therapy. Results from a post-marketing survey on 4,177 patients with advanced recurrent gastric cancer demonstrated that the rate of toxicity for the 4-week/2-week regimen was 74.3% and the rate of ≥Grade 3 adverse events was 25%. In addition, in 3,801 patients assessed for the efficacy analysis, benefits with the 4-week/2-week regimen were observed, with a median survival time of 8.3 months and a 1-year survival rate of 33.3% (95% confidence interval: 31.8–34.9) (9). However, since the 2-week/1-week regimen is considered to be acceptable in terms of relative dose intensity over a treatment period similar to the usual treatment schedule (4-week/2-week) and since there are reports that antitumor efficacy, adverse reactions and prolongation of the treatment period are not superior compared to the conventional S-1 treatment schedule (4-week/2-week) in advanced recurrent gastric cancer, this regimen does not have a solid reputation (10,11).
The 2-week/1-week regimen investigated in this study exhibited better feasibility and a higher treatment completion rate compared to the standard 4-week/2-week regimen. If the 2-week/1-week regimen is associated with a better relapse-free survival and overall survival, this treatment may be a safe treatment option, with a higher completion rate.
The association between the dosing interval of fluoropyrimidine anticancer drugs and antitumor efficacy and adverse reactions has been extensively investigated. Originally, the known cell cycle of tumor cells is longer (5–7 days) compared to that of normal cells, such as bone marrow and gastrointestinal mucosal cells (~0.5–2 days) (12,13). Shirasaka et al (14) reported that normal cells may be rescued by interrupting the administration of fluoropyrimidine anticancer drugs every 24 h, exploiting the difference in cell cycles between normal and tumor cells. In an alternate-day treatment regimen based on the abovementioned theory, normal cells may have a rest every other day, while tumor cells have no rest due to their longer doubling time, suggesting that The cytotoxic effect on tumor cells is equal to or more potent than on normal cells. Arai et al (15) conducted an alternate-day treatment schedule with S-1 in 36 gastric cancer patients and reported that these patients exhibited adequate blood 5-FU concentrations at 2 h after administration and experienced a reduced frequency of adverse events, with adequate clinical efficacy.
Recently, the benefits of combination treatments with S-1/cisplatin or S-1/docetaxel as adjuvant chemotherapy following surgery in stage III gastric cancer were reported. Takahari et al (16) investigated the benefits of postoperative adjuvant chemotherapy using the S-1/cisplatin combination in stage III gastric cancer and reported excellent outcomes with relapse-free and overall survival rates at 74.1 and 84.5%, respectively, at 3 years. In addition, Fujitani et al (17) investigated postoperative adjuvant chemotherapy with the S-1/docetaxel combination in stage III gastric cancer and reported results that relapse-free and overall survival rates were 66.2 and 78.4%, respectively, at 3 years. However, these aggressive postoperative adjuvant chemotherapies may be associated with low tolerability, as the completion rates for the treatment courses were 72% for 3 courses of S-1/cisplatin and 79.2% for 4 courses of S-1/docetaxel. The development of safer adjuvant chemotherapy regimens of satisfactory efficacy and tolerability are expected in future studies.
In conclusion, the completion of treatment using the 4-week administration followed by a 2-week rest or the 2-week administration followed by a 1-week rest regimen of S-1 as postoperative adjuvant chemotherapy was investigated in a multicenter, randomized clinical trial in order to establish a safe postoperative adjuvant chemotherapy regimen for gastric cancer, with a higher treatment completion rate. The 2-week/1-week regimen was associated with a higher completion rate compared to the 4-week/2-week regimen, with an acceptable frequency of adverse events. If future analyses reveal acceptable relapse-free survival and overall survival rates for the 2-week/1-week regimen, this is expected to be a safer treatment option with a higher completion rate.
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