The majority of breast cancers (w70

The majority of breast cancers (w70%) express oestrogen receptors and in these cases oestrogen is considered to promote tumor growth. Hence, treat- ments subsequent to surgery, radiotherapy, and/or chemotherapy are directed towards reducing oestro- genic effects within breast tissue (Smith & Chua 2006). The incidence rate of breast cancer continues to increase with age despite the loss of ovarian hormones in postmenopausal women. This apparent paradox has been resolved by the fact that extragonadal sites, including breast, brain, muscle, skin, bone, and adipose tissue can synthesize potent androgens and oestrogens from relatively inactive circulating steroid precursors derived from the adrenal cortex and to a much lesser extent the ovaries (Simpson et al. 2005). Indeed, after the menopause, nearly 100% oestrogens are formed in peripheral tissues (Labrie 2003) and exert their effects locally in a paracrine or intracrine manner.
In breast tissues, enzymes are present to convert inactive circulating precursors, such as androstene- dione, dehydroepiandrostenedione (DHEA) and its sulfated form DHEA-S, and oestrone sulfate (E1S) into biologically active androgens and oestrogens (see Fig. 2).
In fact, postmenopausal breast cancer illustrates the importance of local oestrogen biosynthesis. In post- menopausal women, the concentration of 17b-oestra- diol (E2) present in breast tumors is at least 20-fold higher than that in the circulation , but in premenopausal women with carcinomas, this ratio was only 5