Pharmacodynamics Anastrozole works by
reversibly binding to the
aromatase enzyme, and through
competitive inhibition blocks the conversion of
androgens to
estrogens in peripheral (extragonadal)
tissues. The medication has been found to achieve 96.7% to 97.3% inhibition of aromatase at a dosage of 1 mg/day and 98.1% inhibition of aromatase at a dosage of 10 mg/day in humans. As such, 1 mg/day is considered to be the minimal dosage required to achieve maximal suppression of aromatase with anastrozole. As such, anastrozole may have
peripheral selectivity in humans, although this has yet to be confirmed. In any case, estradiol is synthesized peripherally and readily crosses the blood–brain barrier, so anastrozole would still expected to reduce estradiol levels in the central nervous system to a certain degree. The
plasma protein binding of anastrozole is 40%. The
metabolism of anastrozole is by
N-dealkylation,
hydroxylation, and
glucuronidation. Inhibition of aromatase is due to anastrozole itself rather than to
metabolites, with the major circulating metabolite being inactive. The
elimination half-life of anastrozole is 40 to 50 hours (1.7 to 2.1 days). This allows for convenient once-daily administration. The medication is
eliminated predominantly by metabolism in the
liver (83 to 85%) but also by residual
excretion by the
kidneys, unchanged (11%). Anastrozole is excreted primarily in
urine but also to a lesser extent in
feces. ==Chemistry==