Niosome-Encapsulated Gentamicin for Ophthalmic Controlled Delivery

Abdelbary, Ghada A.; El-Gendy, Nashwa

doi:10.1208/s12249-008-9105-1

Cited by 278 publications

(183 citation statements)

References 35 publications

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“…In this study, a comparison has been made between spans-and Tweens-loading GNA, the results of the DLS study are shown in Table 1. The studies with the sizes gave us a qualitative idea of the niosomal delivery systems prepared using Spans smaller in the size than that of Tweens, the similar results were reported for Gentamicin niosomes (Abdelbary & El-gendy, 2008). This finding may be due to Spans with shorter alkyl chains and lower HLB values than Tweens, therefore causing a reduction of the repulsion forces between the hydroxyl groups of Spans and the carboxyl groups of the anticancer drug, thus it should be able to produce smaller size PEGylated niosomes.…”

Section: Characteristics Of P-gna-nisvssupporting

confidence: 63%

PEGylated non-ionic surfactant vesicles as drug delivery systems for Gambogenic acid

et al. 2013

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Gambogenic acid (GNA), a popular Chinese traditional medicine, has its limitations of coming into use due to its low aqueous solubility and poor bioavailability. In this study, therefore, the PEGylated non-ionic surfactant vesicles drug delivery systems were prepared from biocompatible non-ionic surfactant of Span60, cholesterol and dicetyl phosphate (DCP) by the improved ethanol injection method, and were modified with a polyethylene glycol monostearate15 (PEG15-SA). PEG15-SA, as a biocompatible, non-toxic and non-immunogenic hydrophilic segment, was grafted onto the surface of colloidal niosomes carries to reduce the uptake by the reticuloendothelial system (RES), prolonging the circulation time and attaining higher entrapment efficiency. To our knowledge, this work is the first to report that PEG15-SA was applied to coating of niosomes for encapsulation of GNA. The optimized PEG-GNA-NISVs (P-GNA-NISVs) were characterized in terms of mean vesicles size, polydispersity index (PDI), Zeta potential and entrapment efficiency of the P-GNA-NISVs. The results showed that the mean diameter, PDI, Zeta potential, and the entrapment efficiency of the P-GNA-NISVs were 70.1 nm, 0.166, À44.3 mV and 87.74%, respectively. Furthermore, the release studies of GNA from PEGylated niosomes in vitro and the pharmacokinetics in vivo exhibited a prolonged release profile as studied over 24 h. In conclusion, the result suggests that P-GNA-NISVs prepared in this way not only have higher encapsulation capacity, more colloidal stability but also offer an approach that the PEGylated niosomes is a promising carrier for anticancer GNA.

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Section: Characteristics Of P-gna-nisvssupporting

confidence: 63%

PEGylated non-ionic surfactant vesicles as drug delivery systems for Gambogenic acid

et al. 2013

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“…Also, as compared to normal drug solution, niosomes of drug show slow release. 57) Niosomal formulation containing timolol meleate (0.25%) prepared by chitosan coating exhibited more effect on intra ocular tension with fewer side effects as compared to the marketed formulation. …”

Section: In Ophthalamic Drug Deliverymentioning

confidence: 94%

Niosomes: A Controlled and Novel Drug Delivery System

Rajera

Nagpal

Singh

et al. 2011

Biological & Pharmaceutical Bulletin

283

162

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During the past decade formulation of vesicles as a tool to improve drug delivery, has created a lot of interest amongst the scientist working in the area of drug delivery systems. Vesicular system such as liposomes, niosomes, transferosomes, pharmacosomes and ethosomes provide an alternative to improve the drug delivery. Niosomes play an important role owing to their nonionic properties, in such drug delivery system. Design and development of novel drug delivery system (NDDS) has two prerequisites. First, it should deliver the drug in accordance with a predetermined rate and second it should release therapeutically effective amount of drug at the site of action. Conventional dosage forms are unable to meet these requisites. Niosomes are essentially non-ionic surfactant based multilamellar or unilamellar vesicles in which an aqueous solution of solute is entirely enclosed by a membrane resulting from the organization of surfactant macromolecules as bilayer. Niosomes are formed on hydration of non-ionic surfactant film which eventually hydrates imbibing or encapsulating the hydrating aqueous solution. The main aim of development of niosomes is to control the release of drug in a sustained way, modification of distribution profile of drug and for targeting the drug to the specific body site. This paper deals with composition, characterization/evaluation, merits, demerits and applications of niosomes.

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“…Niosomes have been used to deliver drugs like gentamicin to the eye (Abdelbary & El-gendy, 2008). Niosomes are formed from the self-assembling of nonionic amphiphiles in aqueous medium which are able to accommodate hydrophilic and hydrophobic drugs (Carafa et al, 1998;Uchegbu & Vyas, 1998;Abdelbary & El-gendy, 2008).…”

Section: • Metabolism By Enzymesmentioning

confidence: 99%

“…Niosomes are formed from the self-assembling of nonionic amphiphiles in aqueous medium which are able to accommodate hydrophilic and hydrophobic drugs (Carafa et al, 1998;Uchegbu & Vyas, 1998;Abdelbary & El-gendy, 2008). Niosomal ocular drug delivery concept aims to enhance periocular retention, corneal penetration, and provide controlled release in a similae manner to SLNs and liposomes.…”

Section: • Metabolism By Enzymesmentioning

confidence: 99%