This was a retrospective comparative multicenter study, including patients with histologically confirmed epithelial ovarian carcinoma from the Gynecological Oncology departments at two university hospitals (Örebro and Gothenburg) in Sweden. All patients were in FIGO stage IIB–IV and underwent primary cytoreductive surgery. The period of recruitment was from May 2003 to December 2008. In all, 167 patients were included in the study and 108 patients received weekly docetaxel (Örebro) and 59 received docetaxel every three weeks (Gothenburg) together with carboplatin given every three weeks in both regimens. Of these patients, 147 (88%) completed 3 or more courses of chemotherapy. Clinical and biochemical response rates were based on patients with measurable disease and/or elevated CA-125 levels at the start of chemotherapy. The results from a phase II study of weekly treatment have been published previously (17). Toxicity, which is the main topic of this study, was recorded in all 167 patients (≥1 course of chemotherapy). Patient and tumor characteristics are shown in Table I.

A chemotherapy regimen of weekly docetaxel 30 mg/m² and carboplatin [area under the curve (AUC) 5] was given every 3 weeks to 108 patients (17). Six cycles were administered during 18 weeks. Of these patients, 71 (66%) completed 6 cycles of chemotherapy. The mean dose intensity of docetaxel was 29.8 mg/m²/week (95% CI, 29.6–29.9) and of carboplatin 105.7 mg/m²/week (95% CI, 102.0–109.5).

A chemotherapy regimen of docetaxel 75 mg/m² and carboplatin (AUC 5) was given every 3 weeks to 59 patients (9). Six cycles were administered during 18 weeks. Of these patients, 41 (70%) completed 6 cycles of chemotherapy. The mean dose intensity of docetaxel was 25.1 mg/m²/week (95% CI, 24.9–25.3) and of carboplatin 109.4 mg/m²/week (95% CI, 105.5–113.3).

Eligible patients had adequate bone marrow, renal and hepatic function, and an absolute neutrophil count (ANC) ≥1.5×10⁹/l, a platelet count ≥100×10⁹/l, serum-creatinine ≤1.25 times the normal level, serum ASAT/ALAT ≤1.5 times the normal level, no previous history of chemotherapy or radiotherapy, and an Eastern Cooperative Oncology Group (ECOG) performance status ≤2. Exclusion criteria included severe infection, hypertension and myocardial infarction within the previous 6 months, congestive heart failure, prior serious allergic reactions and previous malignancy within 5 years. The study was approved by the Ethics Committees of the participating University Hospitals (Dnr 03-258). Informed consent was obtained from all patients.

Patients were treated with intravenous docetaxel (30 mg/m²) and carboplatin (AUC 5) on day 1. Docetaxel was repeated on days 8 and 15 and was administered via a ½-hour infusion. Carboplatin was administered in accordance with the Calvert formula (19) for 30 min on day 1. In the group with standard chemotherapy, intravenous docetaxel (75 mg/m²) and carboplatin (AUC 5) were both given on day 1. The second course started on day 22. Before docetaxel infusion, patients were premedicated with intravenous dexamethasone, diphenhydramine and a histamine H₂-receptor antagonist, such as cimetidine. The creatinine clearance was calculated by the method of Cockcroft and Gault (20).

Clinical response was assessed at the completion of 6 chemotherapy cycles (or after at least 3 completed cycles) via clinical, radiographic and serologic means in accordance with the WHO response criteria (21) and the Rustin criteria (22). Patients with residual disease at the start of chemotherapy and who completed at least 3 cycles of chemotherapy (n=85) were evaluable for clinical response evaluation. Efficacy data of weekly therapy have been presented in an earlier report (17). In the present study efficacy data were not further analyzed.

Toxicity was graded according to the Common Terminology Criteria for Adverse Events (CTCAE v3.0, 2003) (23). Patients were required to have an ANC ≥1.5×10⁹/l and a platelet count ≥100×10⁹/l on day 1 to receive chemotherapy. Complete blood cell values were obtained weekly until the conclusion of cycle 6 and then subsequently, every 3 weeks. Adequate renal function was defined as serum creatinine <1.25 times the upper normal limit, and liver function of bilirubin < upper normal limit, AST/ALT <1.5 times the upper normal limit, and ALP <3 times the upper normal limit. Symptomatic peripheral neuropathy ≥ CTCAE grade 2 was an exclusion criterion. All subjects who completed at least 1 cycle of chemotherapy were included in the toxicity analysis.

A quality-of-life measurement questionnaire (EORTC QOL-C30, version 3) was used in the evaluation of the symptoms recorded during the six courses of treatment (24). The compliance rate was high and 93–99% of the patients had evaluable data. The results from the weekly schedule were analyzed and presented in a prior publication (18).

The median follow-up time of all patients alive was 33 months (range, 1–60 months).

According to the inclusion and exclusion criteria, 108 patients were included in the one-week group and 59 in the three-week group. Originally the patients were recruited into two separate phase II studies during the same period of time. T-test, Pearson’s Chi-square test and Fisher’s exact test were used to compare continuous and non-continuous data. ANOVA (repeated measurements) was used to compare symptom scores during the whole period of treatment (cycles 1–6). A P-value <0.05 was considered to indicate a statistically significant result. STATISTICA software (StatSoft, Inc., Tulsa, OK, USA) version 10.0 was used for all statistical analyses in this study.

In the weekly schedule, 38 patients demonstrated a clinical complete response (44.7%), and 29 patients exhibited a partial response (34.1%), resulting in a total clinical response rate of 78.8% (95% CI, 70.1–87.5%). Data from the three-week schedule showed a clinical response rate of 88.7% (95% CI, 80.2–97.2%).

In the weekly schedule the median overall survival time was 35.3 months and the progression-free survival time was 12.0 months. The corresponding figures in the three-week schedule were 54.1 and 20.0 months, respectively.

Since this was not a randomized study, response and survival data could not be compared compared between the weekly and the three-week schedule due to differences in the study populations; this was not the purpose of the study.

Grade 3-4 neutropenia was recorded in 8 patients (11.3%) in the one-week group and in 32 patients (78.1%) in the three-week group after six completed courses of chemotherapy. This was a highly significant difference (Table II). Grade 1–2 neutropenia was recorded in 29 patients (40.9%) and 6 patients (14.6%) in the two groups, respectively.

During all six courses of chemotherapy the mean neutrophil count was significantly lower in the three-week group compared with the one-week group (ANOVA; p<0.0001). A time-dependent effect was also observed in the one-week group with successively decreasing mean values from cycle 1 to cycle 5. This time-dependent pattern was not observed in the three-week group, with low but stable mean values from cycles 1–6 (Fig. 1).

Febrile neutropenia and septicemia were also more frequent in the three-week group (Table III).

Grade 3–4 thrombocytopenia was recorded in one patient in the one-week group and in no patients in the three-week group. However, grade 1–2 thrombocytopenia was more frequent in the one-week group (50.7%) than in the three-week group (14.6%). The thrombocytic toxicity was more pronounced in the one-week-group and significantly increased with every chemotherapy cycle administered. In the three-week group this pattern was not observed.

None of the patients exhibited grade 3–4 anemia. Grade 1–2 anemia was more frequent in the one-week group (95.8%) than in the three-week group (73.2%). The degree of anemia increased with every successive course of chemotherapy and in a similar manner for both treatment groups. All of these differences were statistically significant (Table II). Despite the different pattern of hematological toxicity, the compliance rate with the chemotherapy regimens was similar in the two groups, and 65.5 and 69.5% of the patients, respectively, completed the planned 6 cycles.

Fatigue was the most frequently recorded non-hematological side-effect associated with the one-week regimen and was significantly more frequent than with the three-week regimen (ANOVA; p<0.0001). This difference was noted for every individual cycle of the weekly schedule and the time-effect was also present with increasing fatigue during the treatment period (Table IV).

The second most common adverse event was watery eyes and tearing (epiphora), affecting 55 patients (50.9%) in the one-week group but only one patient (1.7%) in the three-week group. Thus, this side-effect was very specific for the weekly regimen and the frequency increased for every consecutive treatment cycle (Fig. 3).

Nail changes were relatively common with the weekly schedule and were reported in 30 cases (27.8%) compared with 9 cases (15.3%) with the three-week schedule (Fisher’s exact test; p= 0.049). Analyzed with ANOVA repeated test, significant differences (p<0.005) were shown after 3 courses of chemotherapy and until 6 completed courses as well as for the complete treatment (course 1–6). A significant time-dependent effect was noted after 3 cycles in the one-week group and after 5 cycles in the three-week group (p<0.0001).

With regard to peripheral neurotoxicity, no significant differences (ANOVA; p=0.125) were reported between the two treatment schedules, but a very pronounced time-effect was observed in both groups (ANOVA; p<0.0001; Table IV). After 6 completed courses of chemotherapy, 28 patients (39.4%) had grade 1–2 neurotoxicity in the weekly group and 13 patients (24.5%) in the three-week group. No patients exhibited grade 3 or higher sensory neuropathy (Table III).

Oral mucositis was significantly more common with the three-week schedule (ANOVA; p<0.0001) and increased in frequency from cycle 1 to cycle 3 and then reached a plateau and slightly decreased up to cycle 6. In the one-week group this was a less common problem but showed a slight increase with every consecutive cycle of treatment.

Taste disturbances were significantly more common after weekly treatment (ANOVA; p<0.0001) and showed a clear cut increase in frequency from the first to the fourth docetaxel cycle and then reached a plateau. In the three-week group this was a minor problem with a different time pattern (Table IV).

Myalgia following treatment was more pronounced with the three-week schedule than with weekly administration of docetaxel. The difference was highly significant (ANOVA; p<0.0001) during the complete period of treatment. There was no significant change in myalgia with time and this was true for both treatment groups (ANOVA; p=0.626).

Cardiac toxicity was extremely rare in the two groups. No significant differences were noted during the treatment period of six administered cycles of docetaxel-carboplatin (ANOVA; p=0.809). No significant time-dependent effect was noted in either group (ANOVA; p=0.210).

The mean score of nausea and vomiting was 14–15 on the scale of 1–100 in both groups after the first course of chemotherapy and then significantly decreased to ∼6 after five courses of therapy (ANOVA; p<0.0001). There were no significant differences between the two chemotherapy regimens (ANOVA; p= 0.277). Dyspnea and diarrhea were slightly more common after weekly administration of docetaxel but of limited clinical significance.

Fever and clinical infections were significantly more frequent after three-week administration of docetaxel than after weekly administration (ANOVA; p<0.0001; Fig. 2). This was possibly associated with neutropenia for the three-week schedule.