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Gamma linolenic acid with tamoxifen as primary therapy in breast cancer

  1. Frances S. Kenny1,
  2. Sarah E. Pinder2,
  3. Ian O. Ellis2,
  4. Julia M.W. Gee3,
  5. Robert I. Nicholson3,
  6. Richard P. Bryce4,
  7. John F.R. Robertson1,*

Article first published online: 2 MAR 2000

DOI: 10.1002/(SICI)1097-0215(20000301)85:5<643::AID-IJC8>3.0.CO;2-Z

Issue

International Journal of Cancer

International Journal of Cancer

Volume 85, Issue 5, pages 643–648, 1 March 2000

Additional Information

How to Cite

Kenny, F. S., Pinder, S. E., Ellis, I. O., Gee, J. M.W., Nicholson, R. I., Bryce, R. P. and Robertson, J. F.R. (2000), Gamma linolenic acid with tamoxifen as primary therapy in breast cancer. Int. J. Cancer, 85: 643–648. doi: 10.1002/(SICI)1097-0215(20000301)85:5<643::AID-IJC8>3.0.CO;2-Z

Author Information

  1. 1

    Professorial Unit of Surgery, City Hospital, Nottingham, UK

  2. 2

    Department of Histopathology, City Hospital, Nottingham, UK

  3. 3

    Tenovus Cancer Research Centre, University of Wales College of Medicine, Cardiff, UK

  4. 4

    Scotia Pharmaceuticals, Stirling, UK

*City Hospital, Hucknall Road, Nottingham, NG5 1PB, UK. Fax: +44 (0) 115 8402 618

Publication History

  1. Issue published online: 2 MAR 2000
  2. Article first published online: 2 MAR 2000
  3. Manuscript Revised: 21 SEP 1999
  4. Manuscript Received: 26 JUL 1999

Funded by

  • Scotia Pharmaceuticals and Departments of Surgery and Histopathology. Grant Number: Nottingham City Hospital

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Abstract

Gamma linolenic acid (GLA) has been proposed as a valuable new cancer therapy having selective anti-tumour properties with negligible systemic toxicity. Proposed mechanisms of action include modulation of steroid hormone receptors. We have investigated the effects of GLA with primary hormone therapy in an endocrine-sensitive cancer. Thirty-eight breast cancer patients (20 elderly Stage I-II, 14 locally advanced, 4 metastatic) took 8 capsules of oral GLA/day (total = 2.8 g) in addition to tamoxifen 20 mg od (T+GLA). Quality and duration of response were compared with matched controls receiving tamoxifen 20 mg od alone (n = 47). Serial tumour biopsies were taken to assess changes in oestrogen receptor (ER) and bcl-2 expression during treatment. GLA was well tolerated with no major side effects. T+GLA cases achieved a significantly faster clinical response (objective response vs. static disease) than tamoxifen controls, evident by 6 weeks on treatment (p = 0.010). There was significant reduction in ER expression in both treatment arms with T+GLA objective responders sustaining greater ER fall than tamoxifen counterparts (6-week biopsy p = 0.026; 6-month biopsy p = 0.019). We propose GLA as a useful adjunct to primary tamoxifen in endocrine-sensitive breast cancer. The effects of GLA on ER function and the apparent enhancement of tamoxifen-induced ER down-regulation by GLA require further investigation. Int. J. Cancer 85:643–648, 2000. © 2000 Wiley-Liss, Inc.

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