Randomized, dose-finding phase III study of lithium gamolenate in patients with advanced pancreatic adenocarcinoma

Author:

Johnson C D1,Puntis M2,Davidson N3,Todd S4,Bryce R5

Affiliation:

1. University Surgical Unit, Southampton General Hospital, Southampton, UK

2. Department of Surgery, University Hospital of Wales, Cardiff, UK

3. Department of Radiotherapy and Oncology, North Middlesex Hospital, London, UK

4. Medical and Pharmaceutical Statistics Research Unit, University of Reading, Reading, UK

5. Scotia Pharmaceuticals Ltd, Stirling, UK

Abstract

Abstract Background Chemotherapy for pancreatic cancer offers small survival benefits and considerable side-effects. Unsaturated fatty acids have an antitumour effect in experimental studies; in phase II studies few side-effects were seen. Methods In this group-sequential, open-label, randomized study, 278 patients with a diagnosis of inoperable pancreatic cancer were treated with either oral (700 mg daily for 15 days), low-dose (0·28 g/kg) or high-dose (0·84 g/kg) intravenous lithium gamolenate (LiGLA). The primary endpoint was survival time from randomization using Kaplan–Meier estimates. Results Median survival after oral and low-dose intravenous treatment was 129 and 121 days respectively. Median survival after high-dose intravenous treatment was 94 days. A good Karnofsky score and the absence of metastases were associated with increased survival. Haemolysis, a marker of rapid infusion, was associated with a median survival time of 249 days in the low-dose intravenous group. Conclusion Oral or low-dose intravenous LiGLA led to survival times similar to those of other treatments for pancreatic cancer although one subgroup (low-dose intravenous LiGLA with haemolysis) had longer survival. High-dose intravenous treatment appeared to have an adverse effect. Systemic treatment with LiGLA cannot be recommended for the treatment of pancreatic cancer.

Publisher

Oxford University Press (OUP)

Subject

Surgery

Reference20 articles.

1. Pancreatic carcinoma;Rosewicz;Lancet,1997

2. Essential fatty acids: molecular and cellular basis of their anti-cancer action and clinical implications;Jiang;Crit Rev Oncol Hematol,1998

3. Growth inhibitory effect of lithium gammalinolenate on pancreatic cancer cell lines: the influence of albumin and iron;Ravichandran;Eur J Cancer,1998

4. An open-label phase I/II dose escalation study of the treatment of pancreatic cancer using lithium gammalinolenate;Fearon;Anticancer Res,1996

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