Exemestane

Exemestane
Systematic (IUPAC) name
6-Methylideneandrosta-1,4-diene-3,17-dione[1]
Clinical data
Trade names Aromasin
AHFS/Drugs.com monograph
MedlinePlus a607006
Pregnancy
category
  • US: D (Evidence of risk)
Routes of
administration
Oral
Legal status
Legal status
Pharmacokinetic data
Bioavailability ~60%
Protein binding 90%
Metabolism Liver (CYP3A4, aldo-keto reductase)
Biological half-life 24 hours
Duration of action 4–5 days
Excretion Urine and feces ~ 1:1 (mainly metabolites)
Identifiers
CAS Number 107868-30-4 YesY
ATC code L02BG06 (WHO)
PubChem CID 60198
IUPHAR/BPS 7073
DrugBank DB00990 YesY
ChemSpider 54278 YesY
UNII NY22HMQ4BX YesY
KEGG D00963 YesY
ChEBI CHEBI:4953 N
ChEMBL CHEMBL1200374 YesY
Synonyms FCE-24304
Chemical data
Formula C20H24O2
Molar mass 296.403 g/mol
 NYesY (what is this?)  (verify)

Exemestane (trade name Aromasin) is a drug used to treat breast cancer. It is a member of the class of drugs known as aromatase inhibitors. Some breast cancers require estrogen to grow. Those cancers have estrogen receptors (ERs), and are called ER-positive. They may also be called estrogen-responsive, hormonally-responsive, or hormone-receptor-positive. Aromatase is an enzyme that synthesizes estrogen. Aromatase inhibitors block the synthesis of estrogen. This lowers the estrogen level, and slows the growth of cancers.

Medical uses

Exemestane is indicated for the adjuvant treatment of postmenopausal women with estrogen-receptor positive early breast cancer who have received two to three years of tamoxifen and are switched to it for completion of a total of five consecutive years of adjuvant hormonal therapy.[2] US FDA approval was in October 2005.[3]

Exemestane is also indicated for the treatment of advanced breast cancer in postmenopausal women whose disease has progressed following tamoxifen therapy.[4]

Contraindications

The drug is contraindicated in premenopausal women, which of course includes pregnant and lactating women.[5]

Adverse effects

The most common side effects (more than 10% of patients) are hot flashes and sweating, which are typical of estrogen deficiency as caused by exemestane, and also insomnia, headache, and joint pain. Nausea and fatigue are mainly observed in patients with advanced breast cancer.[5][6]

Overdose

Single doses of up to at least 32-fold (800 mg), as well as continuous therapy with 24-fold (600 mg) the usual daily dose are well tolerated. No life-threatening overdosing is known in humans, but only in animal studies with 2000- to 4000-fold doses (adjusted to body surface area).[5]

Interactions

Exemestane is metabolized by the liver enzyme CYP3A4. While the CYP3A4 inhibitor ketoconazole had no significant effect on exemestane levels in a clinical trial, the strong CYP3A4 inductor rifampicin significantly cut exemenstane levels about in half (AUC −54%, Cmax −41% for a single dose), potentially compromising its effectiveness. Other 3A4 inductors such as carbamazepine and St John's Wort are expected to have similar effects.[5][6] The clinical relevance of this effect has not been investigated.[7]

Estrogens probably reduce exemestane effectiveness:[6] It would usually be counter-productive to reduce the body's estrogen synthesis with exemestane and then substitute estrogen with pharmaceuticals.

Pharmacology

Mechanism of action

Exemestane is an oral steroidal aromatase inhibitor that is used in ER-positive breast cancer in addition to surgery and/or radiation in post-menopausal women.

The main source of estrogen is the ovaries in premenopausal women, while in post-menopausal women most of the body's estrogen is produced via the conversion of androgens into estrogen by the aromatase enzyme in the peripheral tissues (i.e. adipose tissue like that of the breast) and a number of sites in the brain. Estrogen is produced locally via the actions of the aromatase enzyme in these peripheral tissues where it acts locally. Any circulating estrogen in post-menopausal women as well as men is the result of estrogen escaping local metabolism and entering the circulatory system.[8]

Exemestane is an irreversible, steroidal aromatase inactivator of type I, structurally related to the natural substrate 4-androstenedione. It acts as a false substrate for the aromatase enzyme, and is processed to an intermediate that binds irreversibly to the active site of the enzyme causing its inactivation, an effect also known as "suicide inhibition." By being structurally similar to enzyme targets, exemestane permanently binds to the enzymes, preventing them from converting androgen into estrogen.[5]

Type II aromatase inhibitors such as anastrozole and letrozole, by contrast, are not steroids and work by interfering with the aromatase's heme.[7]

The estrogen suppression rate for exemestane varies from 35% for estradiol (E2) to 70% for estrone (E1).[9]

Pharmacokinetics

Exemestane is quickly absorbed from the gut, but undergoes a strong first-pass effect in the liver. Highest blood plasma concentrations are reached after 1.2 hours in breast cancer patients and after 2.9 hours in healthy subjects. Maximal aromatase inhibition occurs after two to three days.[7] 90% of the absorbed substance are bound to plasma proteins. The liver enzyme CYP3A4 oxidizes the methylidene group in position 6, and the 17-keto group (on the five-membered ring) is reduced by aldo-keto reductases to an alcohol. Of the resulting metabolites, 40% are excreted via the urine and 40% via the feces within a week. The original substance accounts for only 1% of excretion in the urine. The terminal half-life is 24 hours.[5][10]

Physical and chemical properties

4-Androstenedione for comparison

Like the aromatase inhibitors formestane and atamestane, exemestane is a steroid that is structurally similar to 4-androstenedione, the natural substrate of aromatase. It is distinguished from the natural substance only by the methylidene group in position 6 and an additional double bond in position 1.[11]

Pure exemestane is a white to off-white powder that is soluble in DMSO to at least 20 mg/mL. Optical rotation [α]D is +250 to 300° (per g/100 cm³ and decimetre at 589 nm wavelength).[12]

Society and culture

Recreational use

Exemestane has been used in doping to raise luteinizing hormone (LH) and follicle stimulating hormone (FSH) levels, which in turn increases the ratio of male over female sexual hormones and so improves performance. The drug also counteracts gynecomastia as well as fat and water retention following excessive aromatase production due to testosterone doping.[13]

Along with other aromatase inhibitors, exemestane is on the World Anti-Doping Agency's list of prohibited substances.[14]

Research

Oral exemestane 25 mg/day for 2–3 years of adjuvant therapy was generally more effective than 5 years of continuous adjuvant tamoxifen in the treatment of postmenopausal women with early-stage estrogen receptor-positive/unknown receptor status breast in a large well-designed trial. Preliminary data from the open-label TEAM trial comparing exemestane with tamoxifen indicated in 2009 that exemestane 25 mg/day is also effective in the primary adjuvant treatment of early-stage breast cancer in postmenopausal women.[15]

Interim phase III trial results in 2011 showed that adding everolimus to exemestane therapy against advanced breast cancer can significantly improve progression-free survival compared with exemestane therapy alone.[16]

A Phase III trial was reported in 2011, concluding that the use of exemestane in postmenopausal women at an increased risk for breast cancer reduced the incidence of invasive breast cancer. In 4,560 women, after 35 months, the administration of exemestane at a dose of 25 mg/day resulted in a 65% reduction in the risk of breast cancer compared with placebo; annual incidence rates were 0.19% and 0.55%, respectively (hazard ratio: 0.35; 95% CI [0.18-0.70]; p = 0.002).[17]

References

  1. Exemestane at ChEBI
  2. Coombes RC; et al. (2007). "Survival and safety of exemestane versus tamoxifen after 2–3 years' tamoxifen treatment (Intergroup Exemestane Study): a randomised controlled trial". Lancet 369 (9561): 559–70. doi:10.1016/S0140-6736(07)60200-1. PMID 17307102.
  3. "FDA Approval for Exemestane". National Cancer Institute. 5 October 2005.
  4. Aromasin For Advanced Breast Cancer on Aromasin.com
  5. 1 2 3 4 5 6 Jasek, W, ed. (2007). Austria-Codex (in German) (62nd ed.). Vienna: Österreichischer Apothekerverlag. pp. 656–660. ISBN 978-3-85200-181-4.
  6. 1 2 3 Drugs.com: monograph on exemestane.
  7. 1 2 3 Dinnendahl, V, Fricke, U, ed. (2007). Arzneistoff-Profile (in German) 4 (21 ed.). Eschborn, Germany: Govi Pharmazeutischer Verlag. ISBN 978-3-7741-9846-3.
  8. Simpson ER (2003). "Sources of estrogen and their importance". The Journal of Steroid Biochemistry and Molecular Biology 86 (3–5): 225–30. doi:10.1016/S0960-0760(03)00360-1. PMID 14623515.
  9. Mauras, N; Lima, J; Patel, D; Rini, A; Di Salle, E; Kwok, A; Lippe, B (2003). "Pharmacokinetics and Dose Finding of a Potent Aromatase Inhibitor, Aromasin (Exemestane), in Young Males". The Journal of Clinical Endocrinology & Metabolism 88 (12): 5951–6. doi:10.1210/jc.2003-031279. PMID 14671195.
  10. Mutschler, Ernst; Schäfer-Korting, Monika (2001). Arzneimittelwirkungen (in German) (8 ed.). Stuttgart: Wissenschaftliche Verlagsgesellschaft. p. 904. ISBN 3-8047-1763-2.
  11. Steinhilber, D; Schubert-Zsilavecz, M; Roth, HJ (2005). Medizinische Chemie (in German). Stuttgart: Deutscher Apotheker Verlag. pp. 467f. ISBN 3-7692-3483-9.
  12. Sigma-Aldrich Co., Exemestane, ≥ 98 % (HPLC). Retrieved on 12 December 2015.
  13. Das Schwarze Buch – Anabole Steroide (in German). 2007. p. 133. ISBN 978-3-00-020944-4.
  14. Substance Classification Booklet, Canadian Centre for Ethics in Sport, Version 4.0, January 2009.
  15. Deeks ED, Scott LJ. (2009). "Exemestane: A Review of its Use in Postmenopausal Women with Breast Cancer". Drugs 69 (7): 889–918. doi:10.2165/00003495-200969070-00007.
  16. "Positive Trial Data Leads Novartis to Plan Breast Cancer Filing for Afinitor by Year End". 2011.
  17. Goss, Paul E. (June 6, 2011). "Exemestane Offers New Option for Breast Cancer Prevention". American Society of Clinical Oncology. Retrieved June 6, 2011.

External links

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