Nonanthracycline Containing Docetaxel-Based Combinations in Metastatic Breast Cancer

Transcription

1 nanthracycline Containing Docetaxel-Based Combinations in Metastatic Breast Cancer JOHN CROWN St. Vincent s Hospital, Dublin, Ireland Key Words. MBC Docetaxel Cisplatin Carboplatin Vinorelbine Gemcitabine ABSTRACT Many active nonanthracycline-containing regimens are emerging from clinical trials and may offer the option of treating metastatic breast cancer without resorting to doxorubicin or analogues. When used first-line in metastatic breast cancer, both cisplatin and carboplatin are active agents and hence candidates for combination therapy. In a dose-finding study in patients with no prior chemotherapy for metastatic disease, docetaxel administered together with cisplatin produced a promising response rate (RR) of 60% (73% in patients without prior adjuvant chemotherapy). The combination is feasible, although adequate hydration and antiemetic medication must be given. There is also an early indication that it may be possible to dramatically cytoreduce disease in patients with locally advanced breast cancer who are treated with docetaxel plus cisplatin. Given its lower toxicity, carboplatin may also have a role in combination with the taxanes. Of the nonplatinum agents, vinorelbine appears to hold promise; its combination with docetaxel produced an RR of 59% in a group of anthracycline-pretreated patients with progressive disease. Forty-two percent of the patients studied also had prior exposure to a taxane. Weekly gemcitabine plus monthly docetaxel is feasible and active, as is the combination of docetaxel q 3 weeks with daily oral capecitabine. The Oncologist 2001;6(suppl 3):17-21 INTRODUCTION Evidence to date suggests that docetaxel is one of the most active single agents in metastatic breast cancer [1, 2]. Docetaxel has been shown to be superior to doxorubicin in the treatment of patients with prior exposure to an alkylating agent-containing regimen, and it is also superior to mitomycin/vinblastine and methotrexate/5-fluourouracil (5-FU) in patients whose cancer had progressed following anthracycline therapy [3-6]. The latter finding is of particular relevance to designers of combination regimens in that it indicates at least a degree of non-cross-resistance between docetaxel and doxorubicin, and the use of these two drugs in combination thus seems logical. In two Breast Cancer International Research Group studies, docetaxel-doxorubicin combinations were superior to more traditional anthracycline-alkylating agentbased combinations. However, the increasing use of anthracyclines in the adjuvant setting mandates the development of nonanthracycline-containing, docetaxel-based combinations. Candidate drugs for such combinations include: vinorelbine, gemcitabine, cyclophosphamide, 5-FU, methotrexate, and mitomycin C. Another group of agents which is seldom used in routine breast cancer clinical practice but which has been shown to have substantial activity in this disease are the platinum coordination complexes. OVERVIEW OF PLATINUM AGENTS IN BREAST CANCER Although cisplatin and carboplatin are seldom used in the routine treatment of breast cancer in the clinic, a critical look at the data suggests that these agents are among the most active drugs currently available for the initial treatment of metastatic breast cancer [7]. According to the review of Smith and Talbot, cisplatin can be expected to induce responses in around 50% of patients without prior chemotherapy [7], however the activity of these drugs in the salvage setting is much Correspondence: John Crown, M.D., Elm Park, St. Vincent s Hospital, Dublin 4, Ireland. Telephone: ; Fax: ; john.crown@icorg.ie Received February 6, 2001; accepted for publication March 5, AlphaMed Press /2001/$5.00/0 The Oncologist 2001;6(suppl 3):

2 18 nanthracycline-docetaxel Combinations in MBC less prominent. Among 113 previously treated patients who were given cisplatin as second or subsequent treatment, the response rate (RR) was 9% (Table 1). While this appears to suggest a near-unique reduction in activity between first- and second-line use, at least a component of the reduction must be attributed to the fact that breast cancer patients given cisplatin in these trials had typically been exposed to a wide range of active agents including anthracycline. Carboplatin also has activity in the first-line setting (Table 1) [7-16]. Four studies of the drug as initial chemotherapy reveal an overall RR of 31% (27 of 85 patients responded). In the second-line setting, the RR was 7% in four studies that included 60 cases. While these data might suggest that carboplatin is somewhat less active than cisplatin. The increasing understanding of the pharmacokinetics of carboplatin allows for the possibility that earlier studies which used body surface area might have been under-dosing. NONTAXANE, PLATINUM-CONTAINING COMBINATIONS The description of preclinical synergy between the platinum coordination complexes and etoposide has resulted in this combination being extensively tested in the clinic [17]. In a trial conducted by the rth Central Cancer Treatment Group, cisplatin/vp-16 produced responses in 25% of pretreated patients [17]. Cocconi et al. randomized 140 previously untreated patients to receive either cisplatin/vp-16 or CMF [17]. The RR with cisplatin (63%) was statistically significantly superior to CMF (48%). Investigators at the Memorial Sloan-Kettering Cancer Center reported an RR of 42% in 19 patients with no prior cytotoxic exposure who were given carboplatin plus VP-16. However, the RR was only 8% among 12 patients with a history of adjuvant chemotherapy. PLATINUM/DOCETAXEL COMBINATIONS IN BREAST CANCER There has been considerable interest in combining docetaxel with platinum agents in ovarian and lung cancer. Much phase I work had therefore been completed in other disease areas. However, the combination of docetaxel with cisplatin has been studied in a phase I trial conducted in Ireland and France [18]. This study recruited patients with no prior chemotherapy for their metastatic disease. Patients had measurable and/or evaluable lesions, and a World Health Organization performance status of less than 2. A total of 72% of patients recruited to the dose-finding trial had received prior adjuvant therapy, and this had involved an anthracycline in 39% of cases. Many patients had relapsed within a year of adjuvant treatment. Gastrointestinal (GI) toxicity was dose-limiting at amounts higher than 75 mg/m 2 of each drug (Table 2). Table 1. Overview of platinum trials in the treatment of breast cancer Study Prior chemotherapy RR Single-agent Cisplatin Kolaric and Roth [8] Mechi and Sopova [7] 33/66 (50%) Sledge [9] Yap [10] Ostrow [7] Forestiere [7] 10/113 (9%) Martino [11] Bajorin [12] Single-agent Carboplatin Kolaric and Vukes [13] Carmo-Pereira [7] Martin [14] O Brien [15] Booth [7] Martin [16] Carmo-Pereira [7] O Brien [15] Adapted with permission [7]. The combination of docetaxel with cisplatin in these first-line metastatic patients proved active, with an overall RR of 60%. In total, two complete responses (CR) were seen, and 16 partial responses (PR). Ten patients had stable disease, two progressive disease, and nine cases were not evaluable. Importantly, while the overall RR in all 30 evaluable patients was 60%, this rose to 73% in the subgroup of 15 patients with no prior adjuvant therapy. In this study, adequate doses of antiemetics and hydration were both crucial. Nevertheless, the activity of the combination is promising, and it is recommended (given the GI toxicity at higher doses) that further work be undertaken using 75 mg/m 2 of both agents. The combination of taxanes/platinum as chemotherapy for breast cancer has been studied by other investigators (Table 3). Gelmon et al. administered paclitaxel (90 mg/m 2 ) and cisplatin (60 mg/m 2 ) to 27 patients with prior anthracycline exposure, reporting an RR of 85% [19]. Higher dose paclitaxel (220 mg/m 2 ) with cisplatin (75 mg/m 2 ) produced 27/85 (31%) 4/60 (7%) Table 2. Dose-escalation study of docetaxel combined with cisplatin [18] Dose (mg/m 2 ) n of Withdrawal prior to cycle 5 Docetaxel Cisplatin pts for toxicity (evaluable patients) / / / / /4

3 Crown 19 Table 3. Cisplatin-taxane combinations in breast cancer [18-24] Study Setting n of Pts Cisplatin (mg/m 2 ) Taxane (mg/m 2 ) RR Gainford et al. [18] MBC Doc 75 60% Gelmon et al. [19] MBC (anth) biwkly Pac 90 biwkly 85% Wasserheit et al. [20] MBC Pac 220 (G-CSF) 52% Pescia et al. [21] Anth treated Doc 75 52% Spielmann et al. [22] Anth resist Doc 75 56% Antoine et al. [23] Anth resist Doc % Hurley et al. [24] Neoadj Doc 70 96% 20% pcr Abbreviations: Doc = docetaxel; Pac = pacitaxel; anth = anthracycline; MBC = metastatic breast cancer; pcr = partial complete resonse an RR of 52% [20]. The same RR was seen in a study in which 19 previously anthracycline-treated patients received docetaxel 75 mg/m 2 plus cisplatin 75 mg/m 2 [21]. Interestingly, a similar regimen (75 mg/m 2 docetaxel plus 80 mg/m 2 cisplatin) produced a 56% RR in 41 patients with anthracycline-resistant disease [22]. Also in a resistant population, Antoine et al. found a 52% RR in 65 patients given docetaxel 100 mg/m 2 plus cisplatin 100 mg/m 2 [23]. Investigators in Miami have reported striking results with docetaxel/cisplatin in patients with stage III breast cancer [24]. The overall RR was 96% (CR 52%; PR 44%). In a trial involving docetaxel, administered at 75 mg/m 2, carboplatin was given to an area under the concentration time curve of 5 [25]. The RR in 20 second-line patients was 40%. A similar RR (44%) was seen when paclitaxel was combined with carboplatin, again in anthracycline-resistant patients (Table 4) [26]. DOCETAXEL PLUS VINORELBINE In a Southwest Oncology Group phase II study, docetaxel was administered together with vinorelbine (and G- CSF support) to a group of patients with poor-prognosis stage IV breast cancer [27]. Patients entered had progressed while receiving an anthracycline or relapsed within a year of such therapy. Prior paclitaxel treatment was allowed. Docetaxel was administered at 60 mg/m 2 on day 1 and vinorelbine 27.5 mg/m 2 on days 8 and 15, q 3 weeks. G-CSF was administered on days 2-21 of each cycle in all patients. The 13% of patients who were HER-2-positive also received Herceptin. Of the 36 patients entered, 84% had visceral disease. The median number of disease sites was two and median number of prior treatment regimens 1.8. Forty-five percent of patients had already been exposed to a taxane. The overall RR in this group of patients with extensive disease and pretreatment was 59%: 10 patients had a CR and 9 a PR. The median time to progression was 10 months. DOCETAXEL PLUS GEMCITABINE Laufman et al. studied a regimen of weekly gemcitabine plus monthly docetaxel in the therapy of patients with metastatic breast cancer [28]. This phase II study followed previous work showing that weekly gemcitabine could safely be combined with docetaxel and that four of the seven poor-risk patients treated had a response [29]. In the phase II trial, gemcitabine was given at 800 mg/m 2 on days 1, 8, and 15 while docetaxel was administered at 100 mg/m 2 on day 1, q 4 weeks [29]. Response was assessed after the second and fourth cycles, and responding patients had the option to continue treatment. Based on intent-to-treat, the RR was 79% among 39 patients (there were 2 CRs and 29 PRs; three patients each had stable and progressive disease, and two were lost to follow-up). The median response duration among patients who responded to this regimen given as first-line treatment for metastases was more than 26 months. One- and two-year survival rates were 74% and 65%, respectively. Patients for whom the gemcitabine/docetaxel combination was second-line therapy for metastatic disease had a median survival of 10 months and 44% were alive at 1 year. Table 4. Carboplatin-taxane combinations in breast cancer Study Setting Phase n of Pts Carboplatin Taxane (mg/m 2 ) RR Alberti et al. [25] 2nd line II 20 5 mg min/ml Doc 75 40% Fountzilas et al. [26] Anth resist II 37 7 mg min/ml Pac 200 (G-CSF) 44% Abbreviations: Doc = docetaxel; Pac = paclitaxel

4 20 nanthracycline-docetaxel Combinations in MBC DOCETAXEL AND CAPECITABINE In a phase I study, docetaxel 75, 85, or 100 mg/m 2 was administered on day 1 q 3 weeks with capecitabine (given orally bid at doses of 825, 1,000, or 1,250 mg/m 2 on days 1-14) [30]. The 33 patients treated in this dose-escalation trial had solid tumors that had not responded to standard therapy, and a Karnofsky performance score of 70 or greater. The dose-limiting toxicities were grade 2/3 asthenia, grade 3 septicemia, and grade 3 nausea. Two of three patients with breast cancer achieved a PR and activity was also seen in other tumors including colorectal cancer. The regimens of 100 mg/m 2 docetaxel plus 825 mg/m 2 capecitabine and 75 mg/m 2 docetaxel plus 1,250 mg/m 2 capecitabine were both shown to be feasible. There was no evidence of a pharmacokinetic interaction between docetaxel and capecitabine. In a phase III study in which recruitment is now complete, patients with metastatic breast cancer who had failed anthracycline therapy were randomized to receive either docetaxel 100 mg/m 2 q 3 weeks or 75 mg/m 2 docetaxel plus capecitabine 1,250 mg/m 2 administered bid on days 1-14 of each cycle. The primary objective of the study is to demonstrate superior time to progression in the combination arm. Results are awaited. DISCUSSION Platinums are active agents in breast cancer [24]. The demonstrations of substantial activity for the combination of docetaxel and cisplatin are particularly interesting, given the proven synergy between these drugs and trastuzumab. However, the early use in metastatic breast cancer of combinations of highly active drugs raises difficult questions about the sequencing of therapy. Might we be doing patients a disservice by using up too many of our therapeutic options at once? Such issues can only be resolved by carefully designed and conducted randomized trials. Meanwhile, the exceptionally high RR recorded by combination therapy (especially taxane/anthracycline combinations) must be considered encouraging. Furthermore, patients who have had such therapy early in the treatment history of their metastatic disease retain the possibility of having other active regimens, such as those based on weekly docetaxel, vinorelbine/5-fu, and capecitabine, on relapse. REFERENCES 1 Crown J. Docetaxel: overview of an active drug for breast cancer. The Oncologist 2001;6(suppl 3): Nabholtz J-M, Tonkin K, Smylie M et al. Chemotherapy of breast cancer: are the taxanes going to change the natural history of breast cancer? Exp Opin Pharmacother 2000;1: Chan S, Friedrichs K, el D et al. Prospective randomized trial of docetaxel versus doxorubicin in patients with metastatic breast cancer. J Clin Oncol 1999;17: Sjostrom J, Blomqvist C, Mouridsen H et al. Docetaxel compared with sequential methotrexate and 5-fluorouracil in patients with advanced breast cancer after anthracycline failure: a randomized phase III study with crossover on progression by the Scandinavian Breast Group. Eur J Cancer 1999;35: Nabholtz J-M, Senn HJ, Bezwoda WR et al. Prospective randomized trial of docetaxel versus mitomycin C plus vinblastine in patients with metastatic breast cancer progressing despite previous anthracycline-containing chemotherapy. J Clin Oncol 1999;17: Sjöström J, Mouridsen H, Pluzanska A et al. Taxotere (T) versus methotrexate-5-fluorouracil (MF) in patients with advanced anthracycline-resistant breast cancer: preliminary results of a randomized phase III study by Scandanavian Breast Cancer Group. Proc Am Soc Clin Oncol 1998;17:111a. 7 Smith IE, Talbot DC. Cisplatin and its analogues in the treatment of advanced breast cancer: a review. Br J Cancer 1992;65: Kolaric K, Roth A. Phase II clinical trial of cis-dichlorodiammine platinum (cis-ddp) for antitumorigenic activity in previously untreated patients with metastatic breast cancer. Cancer Chemother Pharmacol 1983;11: Sledge GW, Loehrer PJ, Roth BJ et al. Cisplatin as first-line therapy for metastatic breast cancer. J Clin Oncol 1988;6: Yap HY, Salem P, Hortobagyi GN et al. Phase II study of cisdichlorodiammineplatinum(ii) in advanced breast cancer. Cancer Treat Rep 1978;62: Marino S, Samal BA, Singhakowinta A et al. A phase II study of cis-diamminedichloroplatinum II for advanced breast cancer. Two dose schedules. J Cancer Res Clin Oncol 1984;108: Bajorin D. Bosl GF, Fein R. Phase I trial of escalating doses of cisplatin in hypertonic saline. J Clin Oncol 1987;5: Kolaric K, Vukas D. Carboplatin activity in untreated metastatic breast cancer patients results of a phase II study. Cancer Chemother Pharmacol 1991;27: Martin M, Diaz-Rubio E, Casado A et al. Carboplatin: an active drug in metastatic breast cancer. J Clin Oncol 1992;10: O Brien ME, Talbot DC, Smith IE. Carboplatin in the treatment of advanced breast cancer: a phase II study using a pharmacokinetically guided dose schedule. J Clin Oncol 1993;11: Martin M, Diaz-Rubio E, Casado A et al. Phase II study of carboplatin in advanced breast cancer: preliminary results. Semin Oncol 1991;18(suppl 2): Kardinal CG, Cole JT. Chemotherapy of breast cancer. In: Perry MC, ed. The Chemotherapy Source Book (Second Edition). Baltimore:Williams and Willkins, 1997:

5 Crown Gainford C, O Leary M, El-Fiki T et al. Phase I trial of docetaxel (T) and cisplatin (P) as first-line chemotherapy for metastatic breast cancer (MBC). Proc Am Soc Clin Oncol 2000;19:439a. 19 Gelmon KA, O Reilly SE, Tolcher AW et al. Phase I/II trial of biweekly paclitaxel and cisplatin in the treatment of metastatic breast cancer. J Clin Oncol 1996;14: Wasserheit C, Frazein A, Oratz R et al. Phase II trial of paclitaxel and cisplatin in women with advanced breast cancer: an active regimen with limiting neurotoxicity. J Clin Oncol 1996;14: Pescia V, Bordenave HR, Foglia S et al. Taxotere (T) and cisplatin (P) in anthracycline-pretreated advanced breast cancer (ABC): preliminary results. Proc Am Soc Clin Oncol 2000;19:452a. 22 Spielmann M, Llombart A, Zelek L et al. Docetaxel-cisplatin combination (DC) chemotherapy in patients with anthracyclineresistant advanced breast cancer. Ann Oncol 1999;10: Antoine EC, Méric JB, Coeffic D et al. Anthracycline-primary resistant breast cancer (APRBC): confirmatory results of the high level of activity of the docetaxel (D)-cisplatin (C) regimen. Proc Am Soc Clin Oncol 1999;18:491a. 24 Hurley J, Doliny P, Gomez L et al. Neoadjuvant Taxotere/cisplatin in locally advanced breast cancer. Proc Am Soc Clin Oncol 2000;19:127a. 25 Alberti AM. A phase II study of docetaxel (T) and carboplatin (CBP) as second line chemotherapy in metastatic breast cancer. Proc Am Soc Clin Oncol 2000;19:452a. 26 Fountzilas G, Dimopoulos AM, Papadimitriou C et al. Firstline chemotherapy with paclitaxel by three-hour infusion and carboplatin in advanced breast cancer (final report): a phase II study conducted by the Hellenic Cooperative Oncology Group. Ann Oncol 1998;9: Gralow JR, Ellis JK, Williams MA et al. Study of docetaxel plus vinorelbine. Proc Am Soc Clin Oncol 2000;19:106a. 28 Laufman L, Spridonidis CH, Carman L et al. Second-line chemotherapy with weekly gemcitabine (GEM) and monthly docetaxel (DOC) in patients (PTS) with metastatic breast cancer (MBC): a phase II study. Proc Am Soc Clin Oncol 19:408a. 29 Spiridonidis CH, Laufman LR, Jones J et al. Phase I study of docetaxel dose escalation in combination with fixed weekly gemcitabine in patients with advanced malignancies. J Clin Oncol 1998;16: Pronk LC, Vasey P, Sparreboom A et al. A phase I and pharmacokinetic study of the combination of capecitabine and docetaxel in patients with advanced solid tumours. Br J Cancer 2000;83:22-29.