Novel Approaches to Inhibition of Gastric Acid Secretion Journal Articles

abstract

• The gastric H,K-adenosine triphosphatase (ATPase) is the primary target for treatment of acid-related diseases. Proton pump inhibitors (PPIs) are weak bases composed of two moieties, a substituted pyridine with a primary pK(a) of about 4.0 that allows selective accumulation in the secretory canaliculus of the parietal cell, and a benzimidazole with a second pK(a) of about 1.0. Protonation of this benzimidazole activates these prodrugs, converting them to sulfenic acids and/or sulfenamides that react covalently with one or more cysteines accessible from the luminal surface of the ATPase. The maximal pharmacodynamic effect of PPIs as a group relies on cyclic adenosine monophosphate-driven H,K-ATPase translocation from the cytoplasm to the canalicular membrane of the parietal cell. At present, this effect can only be achieved with protein meal stimulation. Because of covalent binding, inhibitory effects last much longer than their plasma half-life. However, the short dwell-time of the drug in the blood and the requirement for acid activation impair their efficacy in acid suppression, particularly at night. All PPIs give excellent healing of peptic ulcer and produce good, but less than satisfactory, results in reflux esophagitis. PPIs combined with antibiotics eradicate Helicobacter pylori, but success has fallen to less than 80%. Longer dwell-time PPIs promise to improve acid suppression and hence clinical outcome. Potassium-competitive acid blockers (P-CABs) are another class of ATPase inhibitors, and at least one is in development. The P-CAB under development has a long duration of action even though its binding is not covalent. PPIs with a longer dwell time or P-CABs with long duration promise to address unmet clinical needs arising from an inability to inhibit nighttime acid secretion, with continued symptoms, delayed healing, and growth suppression of H. pylori reducing susceptibility to clarithromycin and amoxicillin. Thus, novel and more effective suppression of acid secretion would benefit those who suffer from acid-related morbidity, continuing esophageal damage and pain, nonsteroidal anti-inflammatory drug-induced ulcers, and nonresponders to H. pylori eradication.

authors

• Sachs, George
• Shin, Jai Moo
• Hunt, Richard H

status

• published 

publication date

• December 2010

has subject area

• 1103 Clinical Sciences (FoR)
• 2-Pyridinylmethylsulfinylbenzimidazoles (MeSH)
• Enzyme Inhibitors (MeSH)
• Gastric Acid (MeSH)
• Gastroenterology & Hepatology (Science Metrix)
• Gastroesophageal Reflux (MeSH)
• Histamine Antagonists (MeSH)
• Histamine H2 Antagonists (MeSH)
• Humans (MeSH)
• Hydrogen-Ion Concentration (MeSH)
• Lansoprazole (MeSH)
• Omeprazole (MeSH)
• Pantoprazole (MeSH)
• Proton Pump Inhibitors (MeSH)
• Ranitidine (MeSH)

published in

• Current Gastroenterology Reports  Journal

keywords

• 2-Pyridinylmethylsulfinylbenzimidazoles
• Enzyme Inhibitors
• Gastric Acid
• Gastroesophageal Reflux
• Histamine Antagonists
• Histamine H2 Antagonists
• Humans
• Hydrogen-Ion Concentration
• Lansoprazole
• Omeprazole
• Pantoprazole
• Proton Pump Inhibitors
• Ranitidine

Digital Object Identifier (DOI)

• 10.1007/s11894-010-0149-5

start page

• 437

end page

• 447

volume

• 12

issue

• 6