Gastric Pre-Processing Is an Important Determinant of the Ability of Medium-Chain Lipid Solution Formulations to Enhance Oral Bioavailability in Rats

“…The report concluded that rapid transfer of medium chain formulation to intestinal mixed micelles possibly was achieved by efficient dispersion and partial digestion in stomach. Also absorption in the upper intestine prior to drug precipitation was preferred [ 48 ].…”

Section: Drug Delivery Systemsmentioning

confidence: 99%

Recent Advances in Delivery Systems and Therapeutics of Cinnarizine: A Poorly Water Soluble Drug with Absorption Window in Stomach

Raghuvanshi

Pathak

2014

Journal of Drug Delivery

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Low solubility causing low dissolution in gastrointestinal tract is the major problem for drugs meant for systemic action after oral administration, like cinnarizine. Pharmaceutical products of cinnarizine are commercialized globally as immediate release preparations presenting low absorption with low and erratic bioavailability. Approaches to enhance bioavailability are widely cited in the literature. An attempt has been made to review the bioavailability complications and clinical therapeutics of poorly water soluble drug: cinnarizine. The interest of writing this paper is to summarize the pharmacokinetic limitations of drug with special focus on strategies to improvise bioavailability along with effectiveness of novel dosage forms to circumvent the obstacle. The paper provides insight to the approaches to overcome low and erratic bioavailability of cinnarizine by cyclodextrin complexes and novel dosage forms: self-nanoemulsifying systems and buoyant microparticulates. Nanoformulations need to systematically explored in future, for their new clinical role in prophylaxis of migraine attacks in children. Clinical reports have affirmed the role of cinnarizine in migraine prophylaxis. Research needs to be dedicated to develop dosage forms for efficacious bioavailability and drug directly to brain.

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“…15) to suggest that the digestion of the SEDDSs plays a leading role in bioavailability enhancement, as is now well established for conventional lipid delivery systems (17,18). A recent study focused on the evaluation of the impact of gastric digestion on the bioavailability of the model drug cinnarizine from lipid-based formulations composed of medium-and long-chain lipids (19). The results showed that the bioavailability of the poorly water-soluble drug administered orally to rats was higher than that of the same formulation administered intraduodenally, suggesting a pivotal role played by gastric processing.…”

Section: Introductionmentioning

confidence: 97%

“…There is compelling evidence that the behaviour of SEDDSs is highly species-dependent, this being ascribed to the amount of fluid within the gastrointestinal tract having an effect on the extent of self-emulsification (19,20). In humans, gastric digestion of either coarse (>20 μm) or fine (1 μm) emulsions has been shown to result in droplets between 15 and 20 μm, irrespective of the initial size, as a product of the enzymatic digestion and shear forces in the stomach (21,22).…”

Section: Introductionmentioning

confidence: 99%

The Effect of Composition and Gastric Conditions on the Self-Emulsification Process of Ibuprofen-Loaded Self-Emulsifying Drug Delivery Systems: A Microscopic and Dynamic Gastric Model Study

et al. 2011

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Gastric Pre-Processing Is an Important Determinant of the Ability of Medium-Chain Lipid Solution Formulations to Enhance Oral Bioavailability in Rats

Cited by 13 publications

References 38 publications

The dynamic gastric environment and its impact on drug and formulation behaviour

The dynamic gastric environment and its impact on drug and formulation behaviour

Recent Advances in Delivery Systems and Therapeutics of Cinnarizine: A Poorly Water Soluble Drug with Absorption Window in Stomach

The Effect of Composition and Gastric Conditions on the Self-Emulsification Process of Ibuprofen-Loaded Self-Emulsifying Drug Delivery Systems: A Microscopic and Dynamic Gastric Model Study

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