Omeprazole irreversibly blocks the enzyme system on parietal cells that is needed for the secretion of gastric acid. It is a specific H/KATPase inhibitor. This is the enzyme needed for the final step in the secretion of gastric acid.
Pharmacokinetics The absorption of omeprazole takes place in the small intestine and is usually completed within three to six hours. The systemic
bioavailability of omeprazole after repeated doses is about 60%. Omeprazole has a volume of distribution of 0.4 L/kg. It has high plasma protein binding of 95%.
Bioactivation As with all structurally-similar benzimidazole
proton pump inhibitors, omeprazole is a
prodrug. A basic molecule, it accumulates in the acidic
canaliculi of
parietal cells in a protonated form where the S=O group becomes S-OH, which in turn is interconvertible with an achiral, reactive
sulfenamide form. The sulfenamide form is able to attach onto the
cysteine residue on the H+/K+-ATPase, thereby irreversibly inhibiting it. :
Chirality The two different chiralities of omeprazole are both metabolized into inactive products by
cytochrome P450 enzymes, but each chirality is differently inactivated by specific isozymes. Compared to the (
R)-enantiomer, the (
S)-enantiomer is relatively more resistant to metabolism, especially metabolism by
CYP2C19 (if it's processed by CYP2C19 at all). As a result, among people with a more active version of CYP2C19 ("extensive metabolizers"), the (
R) half of a dose of omeprazole is likely to perform more poorly. Conversely, among those with a less active version of CYP2C19 ("poor metabolizers"), more the (
R) half is expected to survive metabolism and end up useful. The proportion of the poor metabolizer
phenotype varies widely between populations, from 2.0 to 2.5% in African Americans and white Americans to >20% in Asians. Several
pharmacogenomics studies have suggested that PPI treatment should be
tailored according to CYP2C19 metabolism status.
AstraZeneca also
developed esomeprazole (Nexium) which is a
eutomer, purely the (
S)-enantiomer, rather than a racemate like omeprazole.
Mechanism of action Omeprazole is a selective and irreversible proton pump inhibitor. It suppresses stomach acid secretion by specific inhibition of the H+/K+-ATPase system found at the secretory surface of gastric
parietal cells. Because this enzyme system is regarded as the acid (proton, or H+) pump within the
gastric mucosa, omeprazole inhibits the final step of acid production. The inhibitory effect of omeprazole occurs within one hour after oral administration. The maximum effect occurs within two hours. The duration of inhibition is up to 72 hours. When omeprazole is stopped, baseline stomach acid secretory activity returns after three to five days. The inhibitory effect of omeprazole on acid secretion will plateau after four days of repeated daily dosing. Omeprazole is only effective on active H+/K+-ATPase pumps. These pumps are stimulated in the presence of food to aid in digestion. ==Chemistry==