Abstract
Purpose/Objective(s)After taxane and anthracycline failure, no standard chemotherapy regimen is established in metastatic breast cancer (MBC). Capecitabine and cisplatin (XP) combination shows promising results in gastrointestinal cancer, but there are relatively scarce data in MBC. We reviewed the clinical outcome of XP regimen in anthracycline and taxane resistant, heavily pretreated MBC patients.Materials/MethodsBetween Jan. 2010 to Feb. 2016, 48 HER2 negative MBC patients who failed anthracycline and taxane based chemotherapy were enrolled. In 43.8% of patients, more than 4 regimens were administrated before XP. Thirty-four patients (70.8%) were hormone receptor (HR) positive MBC. Patients were treated with XP (capecitabine [2000mg/m2 per oral; day 1–14] plus cisplatin [60mg/m2 IV; day 1], every 3 weeks) regimen.ResultsMedian progression-free survival (PFS) in total population was 4.33 months (range 1.1~33.57 months). HR positive patients showed trends for superior PFS compared to triple negative breast cancer (TNBC), without statistical significance (6.53 vs. 3.83 months, P = 0.168). In HR positive group, patients receiving 3 or less lines of chemotherapy showed superior PFS compared to others (10.1 vs. 3.0 months, P = 0.039). In multivariate analysis, HR positive patients receiving 3 or less lines of regimens still showed superior PFS (HR = 2.624, 95% CI; 1.071~6.43, P = 0.032). Most common toxicity was grade 3–4 neutropenia, without treatment-related deaths.ConclusionsXP combination regimen showed clinical benefit with tolerable toxicity in heavily pretreated patients, including HR positive patients. After anthracycline and taxane failure, early administration of XP regimen in selected patients may have improve clinical outcome in breast cancer.
Highlights
Breast cancer is most common cancer in women worldwide [1], and second most common after thyroid cancer in Korea [2]
hormone receptor (HR) positive patients showed trends for superior progression-free survival (PFS) compared to triple negative breast cancer (TNBC), without statistical significance (6.53 vs. 3.83 months, P = 0.168)
In HR positive group, patients receiving 3 or less lines of chemotherapy showed superior PFS compared to others (10.1 vs. 3.0 months, P = 0.039)
Summary
Breast cancer is most common cancer in women worldwide [1], and second most common after thyroid cancer in Korea [2]. In advanced breast cancer (ABC) or MBC, anthracycline or taxane-based regimens are initially used for systemic treatment [4]. No standard therapeutic regimen is established after anthracycline and taxane failure in ABC or MBC [5,6]. Capecitabine is an oral fluropyrimidine agent used as single agent in breast and gastrointestinal cancer patients. Combination of cisplatin with 5-FU has shown synergistic effect in prior study [7], but the clinical effect of cisplatin is not clearly analyzed in breast cancer compared to gastrointestinal cancer. Previous studies have shown the clinical efficacy of capecitabine and cisplatin (XP) combination regimen in unselected MBC patients, but with different patient population and different dosage, schedule of chemotherapeutic agents [8,9,10]. Considering the toxicity of cisplatin in heavily pretreated patients [9], there are relatively scarce reports about combining cisplatin to capecitabine
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