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Combination chemotherapy with carboplatin and paclitaxel (CP) has been the standard of care for patients with platinum-sensitive recurrent ovarian cancer. Treatment with CP is associated with longer progression-free survival (PFS) and overall survival than conventional platinum-based chemotherapy (Parmar et al, 2003; Pfisterer et al, 2006). More recently, the CALYPSO study has demonstrated that carboplatin and liposomal doxorubicin (CPLD) is associated with less toxicity and improved PFS compared with CP using standard doses (Pujade-Lauraine et al, 2010).

However, more than half of these patients relapse within a year. In addition to finding novel therapies, further research is required to identify factors associated with benefit using available chemotherapeutic agents, which may allow individualisation of treatment and improve efficacy.

Leukopenia and sensory neuropathy are common toxicities of paclitaxel (Rowinsky et al, 1993a,1993b). These toxicities may reflect both the level of exposure and tissue susceptibility to this chemotherapy. Several studies have demonstrated that myelosuppression is associated with improved clinical outcomes in a number of cancers treated with various chemotherapeutic agents (Saarto et al, 1997; Poikonen et al, 1999; Di Maio et al, 2005; Yamanaka et al, 2007; Koutras et al, 2008; Pallis et al, 2008; Rocconi et al, 2008; Shitara et al, 2009, 2010b). An association between sensory neuropathy and clinical outcome has not yet been established.

We hypothesised that in patients with platinum-sensitive ovarian cancer treated with CP, leukopenia and sensory neuropathy would be associated with superior PFS and used data from the CALYPSO trial to test this hypothesis. We also investigated whether these particular toxicities predicted clinical efficacy in patients treated with CP compared with those treated with CPLD.

Materials and methods

Patient population

The CALYPSO study has been reported (Pujade-Lauraine et al, 2010). The primary objective of this non-inferiority phase III trial was to evaluate the safety and efficacy of the CPLD administered at 4-weekly intervals compared with CP at 3-weekly intervals on PFS. Eligible patients were enrolled between April 2005 and September 2007. Patients were evaluated for tumour response or progression every 3 months while on chemotherapy. In both arms, six cycles of treatment in the absence of progressive disease or unacceptable toxicity were planned; continuation beyond six cycles was at the discretion of the treating clinicians.

Chemotherapy dosing and use of granulocyte-colony stimulating factor

In the first cycle, patients randomised to CPLD received PLD at 30 mg m2 intravenously on day 1 and carboplatin at area under the time-concentration curve (AUC) 5, based on the Calvert formula, using the glomerular filtration rate (GFR) calculated from serum creatinine values according to the method of Cockroft and Gault, and administered intravenously on day 1 at 4-week intervals. Patients randomised to the CP arm received paclitaxel at 175 mg m2 intravenously on day 1 and carboplatin at AUC 5 intravenously on day 1 at 3-week intervals. Dose escalation of carboplatin to AUC 6 in the absence of significant toxicity was allowed. Dose reduction due to excessive toxicity was allowed but dose re-escalation in the subsequent cycles was prohibited.

Prophylactic treatment with granulocyte-colony stimulating factor (G-CSF) was allowed and optional. Supportive treatment with G-CSF was allowed if patients developed neutropenia (absolute neutrophil count nadir <0.5 × 109 per litre lasting for >5 days), febrile neutropenia or sepsis in any cycle of chemotherapy.

Leukopenia and sensory neuropathy evaluation

Blood tests were performed within 2 weeks of study enrolment, at mid-cycle of chemotherapy and up to 3 days before the next cycle of chemotherapy. The study protocol, however, did not require mandatory evaluation of nadir blood count.

Baseline evaluations for sensory neuropathy were performed within 2 weeks of study enrolment. Clinical re-evaluations for sensory neuropathy were performed up to 3 days prior each new cycle of chemotherapy.

Leukopenia and sensory neuropathy definitions

Patients were classified as leukopenic, based on nadir count of first chemotherapy cycle, with white blood cells (WBCs) <4.0 × 109 per litre (NCI-CTCAE grade 1). Patients were also classified as leukopenic, regardless of the nadir count of the first chemotherapy cycle, if they developed febrile neutropenia or severe infection (NCI-CTCAE grade 3) after the first cycle of chemotherapy. Patients who were treated with G-CSF starting from the second cycle, regardless of the nadir count of first chemotherapy cycle, were also classified as leukopenic. Patients were excluded if G-CSF was used prophylactically as part of the first cycle, or if they progressed or died within the first month of treatment.

Sensory neuropathy was defined as new onset of neuropathy (NCI-CTCAE grade 1) or worsening of pre-existing neuropathy graded according to NCI-CTCAE criteria during treatment. Patients were excluded if there was no assessment of neuropathy at baseline and were required to have at least one assessment during treatment.

Statistical methods

Baseline patient demographic and disease characteristics were compared by using t-tests for continuous variables and χ2-tests for categorical variables. We performed landmark analysis using a cutoff time of 30 days after randomisation and restrict the analyses to patients who were still alive and not progressed during these 30 days. The PFSL is defined as time from landmark to documented evidence of disease progression by RECIST criteria, the occurrence of new disease or death from any cause. In patients who received study treatment without a progression date or death, PFSL will be censored on the date of last clinical assessment. The PFSL was estimated with the Kaplan–Meier method, and compared by leukopenic status, overall and by assigned treatment, using the log-rank tests. Proportional-hazards models were constructed to report hazard ratios (HRs) for PFSL adjusting for baseline prognostic factors (treatment-free interval, presence of measurable disease, baseline CA-125 and baseline white cell count). A test of interaction between leukopenic status and treatment effect was also used to assess whether leukopenia predicted treatment effect.

In multivariable analyses, we modelled sensory neuropathy as a time-varying covariate over the entire course of treatment to examine whether it was prognostic of PFS. The PFS is defined as time from randomisation to documented evidence of disease progression by RECIST criteria, the occurrence of new disease or death from any cause. A test of interaction between neuropathy status and treatment effect was also used to assess whether neuropathy predicted treatment effect.

Exploratory analysis was also performed to test for an association between grade of leukopenia and PFS. Logistic regression models were constructed to characterise the relationship between leukopenia and neuropathy.

Results

Of 975 trial patients, 608 (62%) (299 from the CP group and 309 from the CPLD group) received chemotherapy, did not progress or die during the first month of chemotherapy, did not receive prophylactic G-CSF and had a nadir blood count during cycle 1 of chemotherapy. Of these, 72% of patients (CP 70%, CPLD 73%) were classified as leukopenic. Table 1 summarises the patients’ baseline demographic and disease characteristics. Apart from baseline WBC levels, patients with and without leukopenia were similar.

Table 1 Baseline characteristics of CALYPSO trial patients

Prognostic and predictive value of leukopenia

In the overall population, the median PFSL was 11.0 months for patients with leukopenia and 10.2 months for those without (HR=0.76; 95% CI=0.61–0.94; P=0.01). When examined according to treatment groups, leukopenia predicted better PFSL in patients treated with CP (HR=0.61; 95% CI=0.45–0.82; P=0.001) but not with CPLD (HR=0.95; 95% CI=0.70–1.29; P=0.73; Figure 1). After adjustment for baseline prognostic factors, leukopenia remained significant in patients treated with CP (adjusted HR (aHR)=0.66; 95% CI=0.49–0.90; P=0.01) but not in CPLD.

Figure 1
figure 1

Kaplan–Meier survival in patients with and without leukopenia in the carboplatin–paclitaxel (CP) treatment group and the carboplatin–liposomal doxorubicin (CPLD) group. For the effect of leukopenia on PFS, in the CP arm, log-rank P=0.0009; in the CPLD arm, log-rank P=0.73; overall log-rank P=0.002.

Severity of leukopenia and PFS outcome

Among those with leukopenia, grades 1, 2, 3 and 4 leukopenia were detected in 49, 41, 10 and <1%, respectively. The PFSL benefit increased with increasing severity of leukopenia (Figure 2; Ptrend=0.04).

Figure 2
figure 2

Prognostic value of leukopenia, by grade, for progression-free survival (PFS).

Treatment effect and leukopenia

The treatment benefit of CPLD over CP was greater in patients without leukopenia (aHR=0.51; 95% CI=0.35–0.75; P=0.001), but this difference was not observed in those with leukopenia (aHR=0.93; 95% CI=0.73–1.18; P=0.54). The test of interaction between leukopenic status and the relative treatment effect of CPLD vs CP was significant (P=0.008; Figure 3).

Figure 3
figure 3

Effects of treatment on progression-free survival (PFS), after adjustment for baseline prognostic factors, for patients with and without leukopenia. CP, carboplatin–paclitaxel treatment group; CPLD, carboplatin–liposomal doxorubicin treatment group. *Total patients with evaluable white cell count. #Total patients with evaluable actual neutrophil count.

Less data were available on neutropenia (absolute neutrophil counts 2.0 × 109 per litre), but similar effect was observed as leukopenia when the above analyses were repeated (Figure 3).

Incidence of sensory neuropathy

Of the 975 patients, 949 (494 from the CP group and 455 from the CPLD group), received chemotherapy, had an assessment of neuropathy at baseline, and had at least one assessment of neuropathy during treatment. The mean number of neuropathy evaluations for patients across the entire study period was 5.6 (range 1–12) and 5.9 (range 1–14) in the CP and CPLD groups, respectively. One month after randomisation, development or worsening of sensory neuropathy was reported for 305 patients (61.7%) from the CP group and 125 (27.5%) from the CPLD group.

Prognostic and predictive value of sensory neuropathy

There was significant difference in PFS between patients with and without neuropathy in the CP group (median PFS=11.5 vs 10.1 months; HR=0.77; 95% CI=0.62–0.95; P=0.02; Figure 4). Adjustment of baseline prognostic factors did not change this result (aHR=0.77; 95% CI=0.62–0.95; P=0.02).

Figure 4
figure 4

Kaplan–Meier survival in patients with and without sensory neuropathy in the carboplatin–paclitaxel (CP) treatment group and the carboplatin–liposomal doxorubicin (CPLD) group. For the effect of neuropathy, in the CP arm, log-rank P=0.02; in the CPLD arm, log-rank P=0.97; overall log-rank P=0.003.

In the CPLD group, there was no significant difference in PFS between patients with and without neuropathy (median PFS=12.1 vs 11.9 months; HR=1.01; 95% CI=0.72–1.40; P=0.97).

Treatment effect and sensory neuropathy

The benefit of CPLD over CP appeared to be greater among patients without neuropathy (HR=0.70; 95% CI=0.58–0.84; P<0.0001), but this difference was not observed in those with neuropathy (HR=0.96; 95% CI=0.67–1.36; P=0.81). However, the test of interaction between neuropathy status and the relative treatment effect of CPLD vs CP was not significant (P=0.15).

Relationship between leukopenia and sensory neuropathy

There was no relationship between leukopenia at landmark and development or worsening of sensory neuropathy from landmark (odds ratio (OR) (neuropathy vs no neuropathy)=0.91; 95% CI=0.64–1.29; P=0.59). However, for patients treated with CP who had NCI-CTCAE grade 2 leukopenia (WBC <3.0 × 109 per litre) at landmark, there was a non-statistically significant trend in development of neuropathy during the course of treatment (OR=1.53; 95% CI=0.94–2.49; P=0.08).

Discussion

In this analysis, chemotherapy-induced leukopenia and sensory neuropathy were associated with improved prognosis in patients with platinum-sensitive recurrent ovarian cancer treated with CP. Women developing leukopenia during cycle 1 of CP had a 34% reduction in the risk of disease progression compared with those without leukopenia, with increasing severity of leukopenia associated with longer PFS. Likewise, development or worsening of sensory neuropathy on CP was associated with a 24% reduction in the risk of disease progression. Chemotherapy-induced leukopenia and sensory neuropathy were not prognostic for patients treated with CPLD. The CALYPSO trial reported superiority in PFS and better therapeutic index for CPLD over CP (Pujade-Lauraine et al, 2010). In this analysis, the treatment benefit was similar in patients treated with CPLD or CP only when CP induced leukopenia or sensory neuropathy, although a statistically significant interaction was only observed for leukopenia only (interaction P=0.008).

Our findings are consistent with a growing number of studies that report an association between chemotherapy-induced myelotoxicity and patient outcomes in a number of malignancies (Saarto et al, 1997; Poikonen et al, 1999; Di Maio et al, 2005; Yamanaka et al, 2007; Koutras et al, 2008; Pallis et al, 2008; Rocconi et al, 2008; Shitara et al, 2009, 2010b). A meta-analysis of 13 trials of various cancers (n=9528) reported a 31% reduction in risk of death for patients who developed grades 3 and 4 neutropenia or leukopenia compared with those experiencing lower grade or no cytopenia (Shitara et al, 2010a). In ovarian cancer, Rocconi et al (2008) reported improvement in PFS in patients who developed myelosuppression from platinum- and taxane-based chemotherapy. In another retrospective cohort study, Kim et al (2010) reported a non-significant increase in PFS and overall survival for patients with grades 3 and 4 neutropenia from treatment with CP compared with those with lower grade or no neutropenia. However, the multivariate analysis indicated that stage of disease, clear histology type and amount of residual disease were significant predictors of survival, but not neutropenia. In addition to the significant limitation of the smaller sample size to detect a true effect (n=130), several differences between the patient population and analytic techniques used in this study and the present analysis may have contributed to these conflicting results.

Lack of treatment-induced toxicity as surrogate for poorer patient outcome in the CP arm may be due to one of the several explanations. The first is that patients with less toxicity may have insufficient drug exposure and thus less cytotoxicity. Joerger et al (2007) demonstrated that using body surface area (BSA)-derived dose of paclitaxel led to a significant interpatient variation in drug exposure of >35%. This finding and others suggest that standard dose calculation methods may result in a significant proportion of patients being exposed to suboptimal drug concentration (Gurney, 2005). This may relate to variations in hepatic metabolism where polymorphism of P450 influences paclitaxel metabolism (Sonnichsen et al, 1995), whereas PLD is protected from hepatic metabolism (Hilmer et al, 2004). However, in our study, chemotherapy-induced leukopenia was prognostic of PFS only in patients treated with CP, indicating that myelotoxicity may be more reflective of adequate drug exposure in CP but not in CPLD. Leukopenia was a dose-limiting toxicity for paclitaxel in phase 1 trials (Rowinsky et al, 1993b). Unlike doxorubicin, PLD causes minimal myelosuppression due to a slower clearance rate and a longer elimination half-life (Hilmer et al, 2004). Instead, hand–foot syndrome and stomatitis are the dose-limiting side-effects of PLD (Uziely et al, 1995; Gordon et al, 2001). We did not observe a statistically significant association between hand–foot syndrome or stomatitis and PFS in patients assigned to CPLD in the CALYPSO trial (data not shown), suggesting that they may not be correlated with cytotoxicity in ovarian cancers. Alternatively, this lack of correlation may possibly be due to the limitations in the current grading system used to score toxicities.

The second explanation of the association between treatment-induced toxicity and anticancer effect observed in the CP arm may relate to genetic similarity between normal and malignant cells, resulting in both having similar susceptibility to the cytotoxic effects of the chemotherapy with adequate drug exposure. A number of genes have been proposed to be involved with drug resistance in ovarian cancer including the P-glycoprotein efflux transporter (PGP), anti-apoptotic proteins and other survival pathways (Richardson and Kaye, 2005). It is possible that, in any patient, the normal and malignant cells may share the same resistance mechanisms. For example, PGP, encoded for by ABCB1 (also known as multidrug resistance gene 1), is affected by gene polymorphisms in tumour and non-malignant tissue. With taxane-based chemotherapy, the 2677G>T/A polymorphism of ABCB1 is associated with leukopenia (Sissung et al, 2006; Tran et al, 2006), greater tumour response(Green et al, 2006), longer PFS (Johnatty et al, 2008) but higher drug clearance(Gréen et al, 2009). The 3435C>T polymorphism is associated with leukopenia (Tran et al, 2006) and neuropathy (Sissung et al, 2006) but not response (Green et al, 2006) or survival (Johnatty et al, 2008). However, these associations have not yet been validated, with small studies with different population of racial distribution reporting conflicting results. These studies have also not separated the clinical outcomes according to the polymorphisms occurring in the tumour (affecting resistance) or in normal tissue (affecting drug elimination) or both (Marsh et al, 2006, 2007). Such studies are required to determine whether these associations are due to issues related to drug exposure or shared drug resistance mechanisms between normal and tumour cells.

The findings of this study support further research into toxicity-adjusted dosing as a strategy to personalise treatment with recurrent ovarian cancer (Gurney, 1996). In general, this involves assigning an arbitrary toxicity target to infer that an adequate dose of chemotherapy has been given. Such research has been conducted in various cancers with variable results. In a large randomised phase III study of adjuvant chemotherapy for high-risk breast cancer patients, dose escalation based on lack of haematological toxicity resulted in 9% improvement in 3-year relapse-free survival (Bergh et al, 2000). In that study, the toxicity-adjusted dose led to a 3- to 4-fold range in doses of epirubicin and cyclophosphamide which is similar to the known interpatient variation in clearance of these drugs, as opposed to the <2-fold dose range achieved with BSA dose. However, the SCOTROC4 study of single agent carboplatin in advanced ovarian cancer failed to show a PFS benefit for patients who had dose escalation based on lack of neutropenia (Kaye et al, 2009). Carboplatin dose was derived using GFR which gives a narrow interpatient variation in drug exposure and leads to relatively less inadvertent under-dosing compared with BSA-derived dose. This is reflected in the relatively small difference in the dose of carboplatin received between the standard and the toxicity-adjusted arms (AUC 6.0 vs 6.8). As this study is yet unpublished, it will be important to review the range of doses received between the two arms (rather than just the median) with a particular focus on any overlap in the low-dose range.

A major strength of this study is the availability of high-quality large sample trial data from CALYPSO to investigate the study hypothesis. The assessment of toxicity and disease progression events was specified in the trial protocol according to standard definitions. Our analysis plan was designed to overcome the challenges for measuring the association between toxicity and disease progression. First, we have applied a landmark strategy by restricting the analysis to patients who had completed one cycle of chemotherapy and who were alive at 4 weeks after randomisation to minimise the potential for confounding by number of cycles of chemotherapy received as an explanation for the association observed between leukopenia and improved prognosis. A higher incidence of leukopenia would be expected as the number of cycles of chemotherapy increased due to cumulative bone marrow suppression, and patients with longer PFS would have receive additional cycles. Second, due to the cumulative effect of chemotherapy on development or worsening of sensory neuropathy, we performed a separate analysis where this toxicity is modelled as a time-varying covariate. This approach used all clinical assessments of neuropathy throughout the trial to provide a greater power to detect its prognostic value.

This study has a number of limitations. Approximately one third of the randomised patients did not have nadir blood count recorded during the first cycle of chemotherapy and were excluded from analysis. As compared with patients in this analysis, these patients without nadir blood count were different in terms of some of the baseline characteristics and other toxicities experienced during cycle 1 of chemotherapy (Table 1). However, there was no statistically significant difference in treatment effect (no nadir count, HR (CP vs CPLD)=0.79; 95% CI=0.60–1.04 and nadir count, HR (CP vs CPLD)=0.87; 95% CI=0.72–1.06; interaction P=0.46) or PFS in those with or without nadir blood count (10.9 vs 9.8 months, P=0.15). We have also adjusted for these baseline characteristics in our multivariate models.

In summary, first-cycle leukopenia and sensory neuropathy were associated with better prognosis in patients treated with CP, but not with CPLD in the CALYPSO trial. Efficacy of CP treatment was similar to CPLD in patients who developed leukopenia. These findings are hypothesis generating and should be interpreted with appropriate caution. However, these findings support further research to understand the mechanisms of treatment-related toxicity. Individualisation of chemotherapy dose based on toxicity should be explored in future trials.