Aromatase inhibitors

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A 57-year-old woman comes to the emergency department for evaluation of back pain that began 12 hours ago. The patient was picking up a bag of groceries when her symptoms started. She was recently diagnosed with estrogen receptor-positive breast cancer. Her medications include abemaciclib and anastrozole. Her temperature is 37.8°C (100.0°F), pulse is 76/min, and blood pressure is 155/78 mmHg. Physical exam reveals focal tenderness over the lumbar spine. The pain is exacerbated with flexion and extension of the spine. No neurologic deficits are noted in the lower extremities. Imaging is ordered and shown below. Her most recent lab results showed a leukocyte count of 3,600/mm3. Administration of which medications would have most likely prevented this patient’s condition?
  Image reproduced from Radiopedia

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First Aid

2024

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Anastrozole p. 674

reproductive hormones and p. 673

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Aromatase inhibitors, or AIs, are a type of medication used to treat breast cancer in postmenopausal people. However, they should only be used if the breast cancer is positive for estrogen receptors.

Breast cancer, or breast carcinoma, is an uncontrolled growth of epithelial cells within the breast. It’s the most common cancer in female individuals, and the second leading cause of cancer deaths after lung cancer.

Breasts are made up of 15 to 20 lobules, and inside each of these lie a bunch of grape-like structures called the alveoli. Zooming in on the alveoli, there’s a layer of alveolar cells that secrete breast milk into the lumen, which is the space in the center of the gland. These alveolar cells have receptors for certain hormones like, estrogen and progesterone, which are released by the ovaries, and prolactin which is released by the pituitary gland. These hormones stimulate the alveolar cells to divide and increase in number, which makes the lobule enlarge.

Just like healthy alveolar cells, some breast cancer cells have hormone receptors that allow them to grow in the presence of the hormones. When breast cancer cells have estrogen receptors, the cancer is called an ER-positive carcinoma. In this case, hormonal therapy is useful for adjuvant treatment, and includes medications which block the formation or effects of estrogen.

Aromatase inhibitors block the formation of estrogen by inhibiting the aromatase enzyme that converts androgen to estrogen. Now, before menopause, estrogen is mainly synthesized by the ovaries, where there’s a lot of androgen waiting to be converted. And the amount of aromatase enzyme in the ovary depends on the stimulation by gonadotropin. So, even if we gave this medication to premenopausal people with breast cancer, gonadotropin would induce synthesis of more aromatase, which would synthesize more estrogen. However, in postmenopausal people, estrogen is synthesized by other tissues, like the adrenal glands and fat tissue. Here, aromatase levels don’t depend on gonadotropin, so AIs can decrease aromatase and lower estrogen levels in postmenopausal people.

Now, there are two main types of aromatase inhibitors. Type I aromatase inhibitors are classified as steroidal competitive inhibitors because they are structurally similar to natural substrates of these enzymes - androgens. In other words, type I aromatase inhibitors work as fake substrates that bind the active site of the enzyme, and cause irreversible inhibition, also known as “suicide inhibition”. The most important medication in this group is exemestane.

Sources

  1. "Katzung & Trevor's Pharmacology Examination and Board Review,12th Edition" McGraw-Hill Education / Medical (2018)
  2. "Rang and Dale's Pharmacology" Elsevier (2019)
  3. "Goodman and Gilman's The Pharmacological Basis of Therapeutics, 13th Edition" McGraw-Hill Education / Medical (2017)
  4. "Extending Aromatase-Inhibitor Adjuvant Therapy to 10 Years" New England Journal of Medicine (2016)
  5. "Tailoring Adjuvant Endocrine Therapy for Premenopausal Breast Cancer" New England Journal of Medicine (2018)
  6. "Aromatase inhibitors versus tamoxifen in early breast cancer: patient-level meta-analysis of the randomised trials" The Lancet (2015)