Release kinetics of liposome-encapsulated ganciclovir after intravitreal injection in rabbits

Bourlaist, C. Le; Chevanne, François; Ropert, P.; Bretagne, G.; Acar, L.; Zia, Hossein; Sado, P. A.; Needham, Thomas E.; Leverge, R.

doi:10.3109/02652049609026032

Cited by 24 publications

(9 citation statements)

References 16 publications

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“…Different liposomal administration routes to deliver drugs (oral [40], intranasal [41], ocular [42][43][44], topical instillation [45][46][47], intravitreal and subconjunctival [48,49], topical [50], aerosol [51], epidural) have been extensively investigated to provide more effective therapy through direct targeting to the site of action, extending level of drug, prolonging drug activity at the targeted site.…”

Section: Liposomesmentioning

confidence: 99%

Liposome-Nanogel Structures for Future Pharmaceutical Applications

Казаков¹,

Levón²

2006

CPD

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Nanoparticles have been extensively studied as drug delivery systems. In this review, we focus on a relatively new type of nanoparticles--lipobeads--a liposome-hydrogel assembly as a novel drug delivery system. An appropriate assemblage of spherical hydrogel particles and liposomes combines the properties of both classes of materials and may find a variety of biomedical applications. The bi-compartmental structure of lipobeads is a natural configuration. Thus, the technology of their preparation can be a key step of designing more stable and effective vaccines. Biocompatibility and stability, ability to deliver a broad range of bioactive molecules, environmental responsiveness of both inner nanogel core and external lipid bilayer, and individual specificity of both compartments make the liposome-nanogel design a versatile drug delivery system relevant for all known drug administration routes and suitable for different diseases with possibility of efficient targeting to different organs. New findings on reversible and irreversible aggregation of lipobeads can lead to novel combined drug delivery systems regarding lipobeads as multipurpose containers. The research on hydrogel-liposome submicrometer structures has just begun and fundamental studies on interactions between hydrogels and liposomes are in demand.

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Section: Liposomesmentioning

confidence: 99%

Liposome-Nanogel Structures for Future Pharmaceutical Applications

Казаков¹,

Levón²

2006

CPD

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“…The elimination rate constant from the vitreous for the liposome-encapsulated fluconazole was approximately 7 times slower than the plain fluconazole injection. The delayed elimination of drag from the vitreous was also documented in liposomeentrapped ganciclovir (14). Drag transport within the vitreous space of the normal phakic eyes should be slow because of collagenous matrix present in the vitreous cavity.…”

Section: Discussionmentioning

confidence: 90%

Intravitreal Pharmacokinetics of Plain and Liposome-Entrapped Fluconazole in Rabbit Eyes

Gupta¹,

Velpandian²,

Dhingra³

et al. 2000

Journal of Ocular Pharmacology and Therapeutics

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The objective of our experiment was to study the pharmacokinetics of plain and liposome-encapsulated fluconazole after an intravitreal injection (100 microg/0.1 ml) in rabbit eyes. Equal concentrations of plain and liposome-entrapped fluconazole were injected intravitreally into albino rabbits through the pars plana after intravenous pentobarbitone anesthesia. The rabbits were sacrificed at various time intervals, and the concentration of fluconazole in vitreous, retina-choroid, aqueous humor and cornea was estimated using High Performance Liquid Chromatography (HPLC). Plain fluconazole showed a rapid vitreal clearance and a short half-life (3.08 hr), whereas liposome-entrapped fluconazole showed a longer half-life (23.40 hr). The terminal elimination constant (Ke) of the liposome-loaded drug from the vitreous was seven times less than the plain drug. In the plain fluconazole group, at 1 hr, a high concentration of the drug was found in the retina. To conclude, the elimination of fluconazole was primarily transretinal and was very rapid. Liposome encapsulation significantly increased the half-life of fluconazole in the vitreous cavity.

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“…In order to overcome these drawbacks and to improve patient comfort by reducing the frequency of dosing, many drug delivery systems able to provide therapeutic ganciclovir concentrations for prolonged periods of time have been proposed, including implantable devices [32,33], liposomes [34] and microparticles [35]. Ganciclovir intravitreal implants continuously release drug for 6 to 8 months into the vitreous at levels substantially higher than those achieved with intravenous therapy [36,37].…”

Section: Ganciclovir (Gcv)mentioning

confidence: 99%

“…These new pharmaceutical dosage forms appear to preserve the visual acuity and quality of life of patients; although it has been described that an intravitreal injection of particulate or vesicle dispersions requires submicronic size ranges to avoid interference with vision [39]. On the one hand, liposomal formulations can provide effective intravitreal concentrations of ganciclovir for 30 days with no sign of ocular toxicity [34]. On the other hand, microparticles containing ganciclovir did not show any retinal or adjacent tissue toxicity following either electroretinography or histological studies [35].…”

Section: Ganciclovir (Gcv)mentioning

confidence: 99%

Albumin Nanoparticles for the Intravitreal Delivery of Anticytomegaloviral Drugs

Irache¹,

Merodio²,

Arnedo³

et al. 2005

MRMC

113

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Albumin nanoparticles (NP) were proved to be effective and safe carriers for delivering anticytomegaloviral compounds in the vitreous. NP improved the antiviral activity of both ganciclovir and the phosphodiester oligonucleotide analog to formivirsen. NP appeared to be fusogenic carriers able to target the nucleus of cells. In addition, these drug carriers were well tolerated when administered by the intravitreal route and did not induce autoimmune reactions.

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Release kinetics of liposome-encapsulated ganciclovir after intravitreal injection in rabbits

Cited by 24 publications

References 16 publications

Liposome-Nanogel Structures for Future Pharmaceutical Applications

Liposome-Nanogel Structures for Future Pharmaceutical Applications

Intravitreal Pharmacokinetics of Plain and Liposome-Entrapped Fluconazole in Rabbit Eyes

Albumin Nanoparticles for the Intravitreal Delivery of Anticytomegaloviral Drugs

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