17b-Oestradiol treatment modulates nitric oxide synthase activity in MDA231 tumour with implications on growth and radiation response

17b-Oestradiol treatment modulates nitric oxide synthase activity in MDA231 tumour with implications on growth and radiation response

The putative oestrogen receptor negative human breast cancer cell line MDA231, when grown as tumours in mice continually receiving 17b-oestradiol, showed substantially increased growth rate when compared to control animals. Further, we observed that 17b-oestradiol treatment could both increase the g...

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Bibliographic Details
Published in:British journal of cancer Vol. 86; no. 1; pp. 136 - 142
Main Authors: Chinje, E C, Williams, K J, Telfer, B A, Wood, P J, van der Kogel, A J, Stratford, I J
Format: Journal Article
Language:English
Published: 07-01-2002
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Summary:The putative oestrogen receptor negative human breast cancer cell line MDA231, when grown as tumours in mice continually receiving 17b-oestradiol, showed substantially increased growth rate when compared to control animals. Further, we observed that 17b-oestradiol treatment could both increase the growth rate of established MDA231 tumours as well as decreasing the time taken for initiating tumour growth. We have also demonstrated that this increase in growth rate is accompanied by a four-fold increase in nitric oxide synthase activity, which was predominantly the inducible form. Inducible-nitric oxide synthase expression in these tumours was confirmed by immunohistochemical analysis and appeared localized primarily in areas between viable and necrotic regions of the tumour (an area that is presumably hypoxic). Prophylactic treatment with the nitric oxide synthase inhibitor nitro-L-arginine methyl ester resulted in significant reduction in this apparent 17b-oestradiol-mediated growth promoting effect. Tumours derived from mice receiving 17b-oestradiol-treatment were characterized by a significantly lower fraction of perfused blood vessels and an indication of an increased hypoxic fraction. Consistent with these observations, 17b-oestradiol-treated tumours were less radio-responsive compared to control tumours when treated with a single radiation dose of 15Gy. Our data suggests that long-term treatment with oestrogen could significantly alter the tumour oxygenation status during breast tumour progression, thus affecting response to radiotherapy.BRITISH JOURNAL OF CANCER: (2002) 86, 136-142. DOI: 10.1038/sj/bjc/6600032 www.bjcancer.com[copy 2002 The Cancer Research Campaign
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ISSN:0007-0920
DOI:10.1038/sj.bjc.6600032