Raltitrexed–eloxatin salvage chemotherapy in gemcitabine-resistant metastatic pancreatic cancer

被引:1
|
作者
M Reni
L Pasetto
G Aprile
S Cordio
E Bonetto
S Dell'oro
P Passoni
L Piemonti
C Fugazza
G Luppi
C Milandri
R Nicoletti
A Zerbi
G Balzano
V Di Carlo
A A Brandes
机构
[1] S. Raffaele Hsc. Scientific Inst.,Department of Oncology
[2] via Olgettina 60,Department of Oncology
[3] Azienda Ospedaliera and University,Department of Oncology
[4] Policlinico Universitario,Department of Oncology
[5] Garibaldi-Nesima H. Catania,Department of Radiology
[6] S. Raffaele Hsc. Scientific Inst.,Department of Diabetes and Transplant Immunology
[7] Laboratory of Experimental Surgery,Department of Medical Oncology
[8] S. Raffaele Hsc. Scientific Inst.,Department of Oncology
[9] Azienda Ospedaliera-Policlinico,Department of Surgery
[10] Pierantoni H. Forlì,undefined
[11] S. Raffaele Hsc. Scientific Inst.,undefined
来源
British Journal of Cancer | 2006年 / 94卷
关键词
chemotherapy; metastatic disease; oxaliplatin; pancreatic cancer; raltitrexed; salvage therapy;
D O I
暂无
中图分类号
学科分类号
摘要
Limited information on salvage treatment in patients affected by pancreatic cancer is available. At failure, about half of the patients present good performance status (PS) and are candidate for further treatment. Patients >18 years, PS ⩾50, with metastatic pancreatic adenocarcinoma previously treated with gemcitabine-containing chemotherapy, and progression-free survival (PFS) <12 months received a combination of raltitrexed (3 mg m−2) and oxaliplatin (130 mg m−2) every 3 weeks until progression, toxicity, or a maximum of six cycles. A total of 41 patients received 137 cycles of chemotherapy. Dose intensity for both drugs was 92% of the intended dose. Main grade >2 toxicity was: neutropenia in five patients (12%), thrombocytopenia, liver and vomiting in three (7%), fatigue in two (5%). In total, 10 patients (24%) yielded a partial response, 11 a stable disease. Progression-free survival at 6 months was 14.6%. Median survival was 5.2 months. Survival was significantly longer in patients with previous PFS >6 months and in patients without pancreatic localisation. A clinically relevant improvement of quality of life was observed in numerous domains. Raltitrexed–oxaliplatin regimen may constitute a treatment opportunity in gemcitabine-resistant metastatic pancreatic cancer. Previous PFS interval may allow the identification of patients who are more likely to benefit from salvage treatment.
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页码:785 / 791
页数:6
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