This review highlights the importance of controlling the digestion process of orally administered lipid-based delivery systems (LBDS) and their performance. Oral LBDS are prone to digestion via pancreatic lipase in the small intestine. Rapid or uncontrolled digestion may cause the loss of delivery system integrity, its structural changes, reduced solubilization capacity and physical stability issues. All these events can lead to uncontrolled drug release from the digested LBDS into the gastrointestinal environment, exposing the incorporated drug to precipitation or degradation by luminal proteases. To prevent this, the digestion rate of orally administered LBDS can be estimated by appropriate choice of the formulation type, excipient combinations and their ratios. In addition, in vitro digestion models like pH-stat are useful tools to evaluate the formulation digestion rate. Controlling digestion can be achieved by conventional lipase inhibitors like orlistat, sterically hindering of lipase adsorption on the delivery system surface with polyethylene glycol (PEG) chains, lipase desorption or saturation of the interface with surfactants as well as formulating LBDS with ester-free excipients. Recent in vivo studies demonstrated that digestion inhibition lead to altered pharmacokinetic profiles, where Cmax and Tmax were reduced in spite of same AUC compared to control or even improved oral bioavailability.
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Univ Claude Bernard Lyon 1, Univ Lyon, LAGEP, CNRS,UMR 5007, 43 Blvd 11 Novembre 1918, F-69100 Villeurbanne, France
Univ Claude Bernard Lyon 1, Univ Lyon, Fac Pharm Lyon, ISPB, F-69008 Lyon, FranceGattefosse SAS, 36 Chemin Genas, F-69804 St Priest, France
Bourgeois, Sandrine
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Fessi, Hatem
Jannin, Vincent
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Gattefosse SAS, 36 Chemin Genas, F-69804 St Priest, FranceGattefosse SAS, 36 Chemin Genas, F-69804 St Priest, France
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Northeastern Univ, Ctr Pharmaceut Biotechnol & Nanomed, Boston, MA 02115 USA
Jiangxi Univ Chinese Med, State Key Lab Innovat Drug & Efficient Energy Sav, Nanchang 330006, Jiangxi, Peoples R ChinaNortheastern Univ, Ctr Pharmaceut Biotechnol & Nanomed, Boston, MA 02115 USA
Li, Xiang
Khan, Muhammad Muzamil
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Islamia Univ Bahawalpur, Fac Pharm, Dept Pharmaceut, Punjab 63100, PakistanNortheastern Univ, Ctr Pharmaceut Biotechnol & Nanomed, Boston, MA 02115 USA
Khan, Muhammad Muzamil
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Parveen, Farzana
Torchilin, Vladimir
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Northeastern Univ, Ctr Pharmaceut Biotechnol & Nanomed, Boston, MA 02115 USA
IM Sechenov First Moscow State Med Univ, Dept Oncol Radiotherapy & Plast Surg, Moscow 119991, RussiaNortheastern Univ, Ctr Pharmaceut Biotechnol & Nanomed, Boston, MA 02115 USA