The therapeutic pharmacological properties of zopiclone include
hypnotic,
anxiolytic,
anticonvulsant, and
myorelaxant properties. Zopiclone and benzodiazepines bind to the same sites on GABAA receptors, causing an enhancement of the actions of
GABA to produce the therapeutic and adverse effects of zopiclone. The metabolite of zopiclone
desmethylzopiclone is also pharmacologically active, although it has predominately anxiolytic properties. One study found some slight selectivity for zopiclone on α1 and α5 subunits, although it is regarded as being unselective in its binding to GABAA receptors containing α1, α2, α3, and α5 subunits. Desmethylzopiclone has been found to have
partial agonist properties, unlike the parent drug zopiclone, which is a full agonist. The
mechanism of action of zopiclone is similar to benzodiazepines, with similar effects on
locomotor activity and on
dopamine and
serotonin turnover. A
meta-analysis of randomised controlled
clinical trials that compared benzodiazepines to zopiclone or other Z drugs such as zolpidem and zaleplon has found few clear and consistent differences between zopiclone and the benzodiazepines in
sleep onset latency, total sleep duration, number of awakenings, quality of sleep, adverse events, tolerance, rebound insomnia, and daytime alertness. Zopiclone is in the
cyclopyrrolone family of drugs. Other cyclopyrrolone drugs include
suriclone. Zopiclone, although molecularly different from benzodiazepines, shares an almost identical pharmacological profile as benzodiazepines, including anxiolytic properties. Its mechanism of action is by binding to the benzodiazepine site and acting as a
full agonist, which in turn positively modulates benzodiazepine-sensitive GABAA receptors and enhances GABA binding at the GABAA receptors to produce zopiclone's pharmacological properties. In addition to zopiclone's benzodiazepine pharmacological properties, it also has some
barbiturate-like properties.
Pharmacokinetics After oral administration, zopiclone is rapidly absorbed, with a
bioavailability around 75–80%. Time to peak plasma concentration is 1–2 hours. A high-fat meal preceding zopiclone administration does not change absorption (as measured by
AUC), but reduces peak plasma levels and delays its occurrence, thus may delay the onset of therapeutic effects. The plasma protein-binding of zopiclone has been reported to be weak, between 45 and 80% (mean 52–59%). It is rapidly and widely distributed to body tissues, including the brain, and is excreted in urine, saliva, and
breast milk. Zopiclone is partly extensively metabolized in the liver to form an active
N-demethylated derivative (
N-desmethylzopiclone) and an inactive zopiclone-
N-oxide. Hepatic enzymes playing the most significant role in zopiclone metabolism are
CYP3A4 and
CYP2E1. In addition, about 50% of the administered dose is decarboxylated and excreted via the lungs. In urine, the
N-demethyl and
N-oxide metabolites account for 30% of the initial dose. Between 7 and 10% of zopiclone is recovered from the urine, indicating extensive metabolism of the drug before excretion. The terminal elimination half-life of zopiclone ranges from 3.5 to 6.5 hours (5 hours on average). In severe chronic
kidney failure, the area under the curve value for zopiclone was larger and the half-life associated with the elimination rate constant longer, but these changes were not considered to be clinically significant. Sex and race have not been found to interact with pharmacokinetics of zopiclone. ==Chemistry==