Posts Tagged ‘aromatase inhibitors’

Taking an aromatase inhibitor for early breast cancer? Check your vitamin D…

Monday, July 5th, 2010

MaturitasA paper just published in the journal Maturitas (the journal of the European Menopause and Andropause Society) is a reminder the importance of vitamin D in breast cancer treatment. As the authors observe:

Aromatase inhibitors (AI) treatment leads to an increased risk of bone loss and fractures.

The authors examined a group of women with early breast cancer (EBC) and baseline Vitamin D deficiency (<30 ng/ml) who were treated with aromatase inhibitors. They followed serum levels of Vitamin D, bone mineral density (BMD), calcium intake, and the increase of serum 25(OH)D from 3 months of Vitamin D supplementation. What did their data show?

“At baseline [the beginning of AI therapy], 88.1% had 25(OH)D levels <30 ng/ml, 21.2% had severe deficiency (<10 ng/ml), and 25% of the participants had osteoporosis…We found a significant association between 25(OH)D levels and BMD…Plasma 25(OH)D levels improved significantly at 3 months follow-up in those treated with high dose Vitamin D supplements.”

This is only one aspect of the crucial role of Vitamin D in breast cancer prevention and treatment. The authors’ conclusion should be borne in mind by all those caring for or dealing with breast cancer:

“Our study suggests a high prevalence of commonly unrecognized Vitamin D deficiency in women with EBC treated with AI, a known osteopenic agent. Our results support the need for a routine assessment of 25(OH)D levels and, when necessary, supplementation in these patients.

For a discussion of aromatase inhibitors versus tamoxifen see this recent post.

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Tamoxifen versus aromatase inhibitors for breast cancer prevention and treatment

Friday, July 2nd, 2010

Cancer InvestigationA paper recently published in the journal Cancer Investigation summarizes the evidence in favor of aromatase inhibitors (that block the synthesis of estrogen) over tamoxifen (which antagonizes the estrogen receptors). As you probably already know, tamoxifen’s side-effects are potentially very serious. It has come to my attention that clinicians assisting women in the prevention and treatment of breast cancer may not be aware of the evidence advanced by the authors:

Aromatase inhibitors (AIs) have largely replaced tamoxifen as adjuvant hormonal therapy for postmenopausal women with early breast cancer. While tamoxifen is effective in reducing breast cancer recurrence and mortality, recent data indicate two peaks of early, mostly distant metastatic recurrences in patients receiving tamoxifen, and AIs have proven more effective in reducing recurrence. As distant recurrence has been associated with poorer survival and death, reduction in this type of early recurrence event may lead to improved survival over the long term. Recent data from major clinical trials are beginning to bear out this contention.”

European Journal of Surgical OncologyThis is not the first time that evidence establishing the superiority of aromatase inhibition over tamoxifen has been presented. Consider this paper published earlier in the European Journal of Surgical Oncology in which the authors observe:

“The aromatase inhibitors (AI)…have demonstrated superior disease-free survival (DFS) over tamoxifen in several trials. As the choice of adjuvant endocrine treatment for early breast cancer (EBC) is evolving from tamoxifen to the AIs, this review compares the AIs with tamoxifen to help surgeons choose a treatment plan that provides the greatest reduction of recurrence risk for their patients.”

The authors note the weight of already accumulated data:

Trials of the AIs versus tamoxifen have established that patients benefit from longer DFS (disease-free survival), and in some cases distant DFS, after the use of an AI as initial adjuvant therapy, as switch therapy following 2–3 years of tamoxifen, or as extended adjuvant therapy following 5 years of tamoxifen.”

Their conclusion carries additional significance considering that we have natural aromatase inhibitors that are equally useful in preventing excessive conversion of testosterone to estrogen in men (a common problem).

“The advantage in DFS associated with AIs over tamoxifen use should prompt physicians and patients to consider the use of an AI as the initial adjuvant endocrine therapy or, alternatively, switching patients who currently take tamoxifen to an AI for the remainder of adjuvant endocrine therapy.”

Bear in mind that is but one point in the constellation of factors, including proportional steroid hormone production, metabolism, elimination and receptor function, that need to be measured with the appropriate tests to evaluate and correct the hormonal milieu for estrogen receptor stimulation.

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