Interface-Mediated Mechanism of Action - The Root of the Cytoprotective Effect of Immediate-Release Omeprazole

Journal
Journal of medicinal chemistry  
Volume
64
Issue
8
Start Page
5171
End Page
5184
Citation
Journal of Medicinal Chemistry 64 (8): 5171-5184 (2021-04-22)
Publisher DOI
10.1021/acs.jmedchem.1c00251
Scopus ID
2-s2.0-85105096781
PubMed ID
33847502
Omeprazole is usually administered under an enteric coating. However, there is a Food and Drug Administration-approved strategy that enables its release in the stomach. When locally absorbed, omeprazole shows a higher efficacy and a cytoprotective effect, whose mechanism was still unknown. Therefore, we aimed to assess the effect of the absorption route on the gastric mucosa. 2D and 3D models of dipalmitoylphosphatidylcholine (DPPC) at different pH values (5.0 and 7.4) were used to mimic different absorption conditions. Several experimental techniques, namely, fluorescence studies, X-ray scattering methodologies, and Langmuir monolayers coupled with microscopy, X-ray diffraction, and infrared spectroscopy techniques, were combined with molecular dynamics simulations. The results showed that electrostatic and hydrophobic interactions between omeprazole and DPPC rearranged the conformational state of DPPC. Omeprazole intercalates among DPPC molecules, promoting domain formation with untilted phospholipids. Hence, the local release of omeprazole enables its action as a phospholipid-like drug, which can reinforce and protect the gastric mucosa.