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Aromatase inhibitors better than tamoxifen at reducing the risk of breast cancer recurrence in women

Hina ZahidWritten by Hina Zahid Published On 2022-02-10T09:00:16+05:30  |  Updated On 2022-02-10T09:00:33+05:30
Aromatase inhibitors better than tamoxifen at reducing the risk of breast cancer recurrence in women
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A new study has shown that giving aromatase inhibitors instead of tamoxifen to premenopausal women with oestrogen receptor positive (hormone-sensitive) breast cancer significantly reduces the risk of breast cancer recurrence. The results have been published today in The Lancet Oncology.For women with hormone-sensitive, operable breast cancer, giving tamoxifen treatment after surgery reduces...

A new study has shown that giving aromatase inhibitors instead of tamoxifen to premenopausal women with oestrogen receptor positive (hormone-sensitive) breast cancer significantly reduces the risk of breast cancer recurrence. The results have been published today in The Lancet Oncology.

For women with hormone-sensitive, operable breast cancer, giving tamoxifen treatment after surgery reduces the risk of dying from breast cancer within 15 years by about one third. Aromatase inhibitors, drugs which block oestrogen production, are even more effective than tamoxifen in postmenopausal women, reducing this risk by a further 30%.

For premenopausal women, however, aromatase inhibitors are ineffective, since the ovaries respond by increasing oestrogen production. However, this problem may be overcome by using treatments that suppress ovarian function, such as drug therapies or surgery. But until now, it was unclear whether aromatase inhibitors or tamoxifen were the most effective treatment for premenopausal women in reducing breast cancer recurrence.

Researchers from the Early Breast Cancer Trialists' Collaborative Group (EBCTCG), based at Oxford Population Health (University of Oxford) and primarily funded by Cancer Research UK, combined all the available evidence to answer this question, since data from individual trials had been inconclusive. They combined data from four large-scale randomised controlled trials, which involved a total of over 7,000 women with early stage breast cancer, from countries across the world.

Each woman had received an ovarian suppressing treatment. In addition, they were randomly allocated to take an aromatase inhibitor or tamoxifen for three or five years. Over a median follow-up period of eight years, the researchers looked for differences between the two groups in breast cancer recurrence, and deaths from breast cancer or any cause.

In women receiving ovarian suppression therapy

  • Breast cancer recurrence was significantly reduced in the group who had received aromatase inhibitors instead of tamoxifen. Overall, the risk was reduced by an average of a fifth (21%).
  • The main benefit was seen in the first five years, when the treatments differed, where the risk of recurrence was a third (32%) lower in the aromatase inhibitor group. The absolute reduction in the risk of recurrence was 3.2%: 6.9% in the aromatase inhibitor group versus 10.1% in the tamoxifen group.
  • There was no further benefit, or loss of benefit, between five to ten years.
  • Aromatase inhibitors were just as effective in women aged under 35, who have a higher risk of recurrence than older women.
  • There was no apparent difference in the number of deaths from breast cancer or any cause; however survival benefits from aromatase inhibitors may become apparent after a longer period of follow-up.

Known side effects of aromatase inhibitors include an increased risk of osteoporosis, which can cause bone fractures. In the analysis, a slightly higher proportion of women in the aromatase inhibitor group had a bone fracture over the follow-up period, compared with the tamoxifen group: 6.4% vs 5.1%. However, the frequency of bone fractures was low overall, and this can be mitigated through treatment with drugs that help to strengthen bones (bisphosphonates).

Tamoxifen can increase the risk of endometrial abnormalities, including uterine polyps and endometrial cancers. In this analysis, the five-year incidence of endometrial cancer was higher in the tamoxifen group (0.3%) compared with the aromatase inhibitor group (0.2%), but still rare overall.

Lead author, Rosie Bradley from Oxford Population Health said: 'Our aim was to find out whether premenopausal women treated with ovarian suppression could benefit more from aromatase inhibitors than tamoxifen, and these findings conclusively show this is the case for preventing breast cancer recurrence.'

'However, we need to follow patients for longer to find out whether breast cancer deaths are also reduced. Effects on quality of life need to be considered as well, and it is important that clinicians discuss with patients the potential benefits and risks for each treatment approach.'

Caroline Geraghty, specialist cancer information nurse at Cancer Research UK, said: 'This finding has the potential to make a difference in the lives of thousands of women. Most breast cancers are hormone sensitive and treated with hormone therapy. Though there is potential for some side effects, aromatase inhibitors could increase the chance of these women remaining disease free – allowing them to return to normal life.'

'Breast cancer recurrence is especially problematic in younger women, so it's great news to see that the use of aromatase inhibitors is just as effective in women under the age of 35. We look forward to seeing the results of longer-term follow ups to see if aromatase inhibitors save lives.'

https://www.thelancet.com/journals/lanonc/article/PIIS1470-2045(21)00758-0/fulltext

the lancet oncology aromatase inhibitors tamoxifen 
Hina Zahid
Hina Zahid

    Hina Zahid Joined Medical Dialogue in 2017 with a passion to work as a Reporter. She coordinates with various national and international journals and association and covers all the stories related to Medical guidelines, Medical Journals, rare medical surgeries as well as all the updates in the medical field. Email: editorial@medicaldialogues.in. Contact no. 011-43720751

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