Microemulsion formulation of clonixic acid: solubility enhancement and pain reduction

Lee, Jung Mi; Park, Kyung-Mi; Lim, Soo-Jeong; Lee, Mi-Kyung; Kim, Chong‐Kook

doi:10.1211/0022357021771904

Cited by 36 publications

(15 citation statements)

References 21 publications

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“…The osmotic pressure of the vehicle was remarkably lower than the commercial formulation. In vivo studies indicated less pain in injection by the microemulsion formulation but the pharmacokinetic parameters were not significantly different 120…”

Section: Biological Studies In Vitro and In Vivomentioning

confidence: 87%

Biocompatible Microemulsions and Their Prospective Uses in Drug Delivery

Gupta

Moulik

2008

Journal of Pharmaceutical Sciences

166

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Section: Biological Studies In Vitro and In Vivomentioning

confidence: 87%

Biocompatible Microemulsions and Their Prospective Uses in Drug Delivery

Gupta

Moulik

2008

Journal of Pharmaceutical Sciences

166

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“…Further medium-chain triacylglycerides are widely used in SMEDDS Type III, due to their higher polarity compared with long-chain triacylglycerides, which facilitates the emulsification process. [37,52,64,66,72,74,75] Other lipid phases that have been employed are ethyl oleate [52] and oleic acid. [74] In conclusion the LFCS does not encompass all the SEDDS and SMEDDS that have recently been used in research and thus would benefit from being updated as suggested in the present review.…”

Section: Sedds and Smedds Recently Used In Researchmentioning

confidence: 99%

New perspectives on lipid and surfactant based drug delivery systems for oral delivery of poorly soluble drugs

Müllertz

Ogbonna

Ren

et al. 2010

Journal of Pharmacy and Pharmacology

260

136

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Objectives The aim of this review is to highlight relevant considerations when implementing a rational strategy for the development of lipid and surfactant based drug delivery system and to discuss shortcomings and challenges to the current classification of these delivery systems. We also aim to offer suggestions for an improved classification system that will accommodate lipid based formulations that are not currently accommodated in the lipid formulation classification system. Key findings When categorising lipid and surfactant based drug delivery systems, the current Lipid Formulations Classifications System is a useful tool. However, it does not apply to all marketed lipid and surfactant systems or those reported in research papers. A more profound understanding of the functionalities of lipids and surfactants and their role in emulsion formation will enable a rational development strategy and will create the basis for a revised classification system encompassing all employed lipid and surfactant drug delivery systems. Summary The ever-increasing number of poorly soluble compounds in drug discovery and development calls for the serious need for effective and affordable drug delivery strategies that will enhance bioavailability and decrease variability. Lipid and surfactant based drug delivery systems offer these advantages; however, the development of these systems requires proper understanding of the physicochemical nature of the compound as well as the lipid excipients and gastrointestinal digestion. One major challenge of lipid excipients and delivery systems is the varying range of compounds they contain. This has contributed to the challenge of proper characterisation and evaluation of these delivery systems, their stability, classification and regulatory issues, which consequently have affected the number of these formulations that eventually reach the market. Suggestions as to proper classification of these delivery systems based on their main lipid component and recommended use are put forward. The prospect of these delivery systems looks promising.

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“…From the work of Lee et al,63 injections made with nanogels are less painful when compared with cosolvent-based formulation. High blood circulation time could be achieved due to the size of the nanogels, which is very important to extend the therapeutic efficacy of the LA.…”

Section: Nanogel Systems As Carriersmentioning

confidence: 99%

Application of nanogel systems in the administration of local anesthetics

Tam¹

2010

LRA

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Nanogels are robust nanoparticles that could be used to deliver active drug compounds in controlled drug delivery applications. This review discusses the design, synthesis, loading, and release of local anesthetics using polymeric nanoparticles produced via various types of polymerization techniques. The strategy of using layer-by-layer approach to control the burst release of procaine hydrochloride (PrHy; a local anesthetic drug of the amino ester group) is described and discussed.

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Microemulsion formulation of clonixic acid: solubility enhancement and pain reduction

Cited by 36 publications

References 21 publications

Biocompatible Microemulsions and Their Prospective Uses in Drug Delivery

Biocompatible Microemulsions and Their Prospective Uses in Drug Delivery

New perspectives on lipid and surfactant based drug delivery systems for oral delivery of poorly soluble drugs

Application of nanogel systems in the administration of local anesthetics

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