<i>In vitro</i> and <i>in vivo</i> investigation for optimization of niosomal ability for sustainment and bioavailability enhancement of diltiazem after nasal administration

Ammar, H. O.; Haider, Mohamed; Ibrahim, M.M.; Hoffy, Nada M. El

doi:10.1080/10717544.2016.1259371

Cited by 49 publications

(22 citation statements)

References 57 publications

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“…Niosomes have larger PS so they show lower PDI. On the other hand, spanlastics which have smaller PS show larger PDI that may be due to the difference in composition between both types of vesicular structures [33].…”

Section: The Effect Of Independent Formulation Variables On the Polydmentioning

confidence: 99%

“…While the spanlastics showed lower EE than niosomes this may refer to the presence of span 60 and absence of cholesterol. Span 60 has a low HLB value (5.3), long carbon chain (C16) and it has a high phase transition temperature which decreases the leakage and the fluidity of the bilayer that leads to lower EE [33,37].…”

Section: The Effect Of Independent Formulation Variables On Entrapmenmentioning

confidence: 99%

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Carbamazepine Loaded Vesicular Structures for Enhanced Brain Targeting via Intranasal Route: Optimization, in Vitro Evaluation, and in Vivo Study

2019

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Objective: Carbamazepine (CBZ) is used as a first line in the treatment of grand mal and partial seizures, but it suffers from many side effects on different systems of the body. The objective of the present study was optimization of CBZ vesicular structures using 23 multifactorial design for the most efficient targeting of CBZ to the brain via the intranasal route. Methods: The concentration of CBZ (10 and 20%), type of vesicles (niosomes and spanlastics) and speed of rotation (200 and 300 rpm) were considered as the independent variables XA, XB and XC respectively, while the dependent variables were particle size PS (Y1), polydispersity index PDI (Y2), zeta potential ZP (Y3) and entrapment efficiency EE (Y4). The study of the effect of different formulation variables was carried out using Design-Expert ® software. CBZ-loaded spanlastics and noisome were prepared by the ethanol injection method and thin film hydration method, respectively. The optimized formulation was subjected to viscosity measurement, in vitro drug release and physical stability studies. In vivo evaluations in rats for the optimized formulation in comparison to oral CBZ suspension was carried out using behavioral assessment by elevated plus maze test, determination of endothelial nitric oxide synthase (e-NOS), reduced glutathione (GSH) and ELISA estimation of TNFα. Results: The selected optimized formulation (F0) containing 20% CBZ and spanlastic vesicular structure showed PS, PDI, ZP, and the EE % of 350.09 nm, 0.830, 16.124mV and 82.777%, respectively. In vitro release study of F0 demonstrated the ability of the F0 to increase drug release in the range time from 10-60 min (p<0.05) when compared with CBZ suspension. The viscosity of F0 was nearly uniform (65 cps). The photomicrograph taken by the transmission electron microscopy (TEM) reveals the spherical shape of F0. Good physical stability for six months of storage at 25˚ C was found for F0. The optimized spanlastic formulation F0 showed a decrease in latency time in behavior assessment test using elevated plus Maze test, a decrease in serum eNOS and TNF-α and increase in GSH when compared with the oral CBZ suspension, in addition to the histopathological study that revealed the more CBZ uptake by the brain. Conclusion: The optimized spanlastic formulation F0 achieved better results when compared with the oral CBZ suspension for targeting the CBZ spanlastics vesicular structure to the brain via the nasal route.

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Section: The Effect Of Independent Formulation Variables On the Polydmentioning

confidence: 99%

Section: The Effect Of Independent Formulation Variables On Entrapmenmentioning

confidence: 99%

Carbamazepine Loaded Vesicular Structures for Enhanced Brain Targeting via Intranasal Route: Optimization, in Vitro Evaluation, and in Vivo Study

2019

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“…Intranasal folic acid niosomes intended for brain targeting have shown controlled ex vivo perfusion [147]. Regarding the systemic effects of intranasal niosomes, diltiazem-loaded niosomes have shown high half-life (T1/2 ) and enhanced AUC 0-∞ with a reduced elimination rate; such prolonged action for diltiazem is of great value compared to its low oral bioavailability due to extensive first-pass metabolism [148]. The study of using intranasal niosomes for vaccination with glycoprotein B of herpes simplex virus type 1 has shown in vitro controlled release and in vivo elicited plasma glycoprotein antibodies (IgG) and systemic T helper cells [149].…”

Section: Niosomesmentioning

confidence: 99%

Intranasal Nanoparticulate Systems as Alternative Route of Drug Delivery

Alshweiat

Ambrus

Csóka

2019

CMC

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There is always a need for alternative and efficient methods of drug delivery. The nasal cavity can be considered as a non-invasive and efficient route of administration. It has been used for local, systemic, brain targeting, and vaccination delivery. Although many intranasal products are currently available on the market, the majority is used for local delivery with fewer products available for the other targets. As nanotechnology utilization in drug delivery has rapidly spread out, the nasal delivery has become attractive as a promising approach. Nanoparticulate systems facilitate drug transportation across the mucosal barrier, protect the drug from nasal enzyme degradation, enhance the delivery of vaccines to the lymphoid tissue of the nasal cavity with an adjuvant activity, and offer a way for peptide delivery into the brain and the systemic circulation, in addition to their potential for brain tumor treatment. This review article aims at discussing the potential benefit of the intranasal nanoparticulate systems, including nanosuspensions, lipid and surfactant, and polymer-based nanoparticles as regards productive intranasal delivery. The aim of this review is to focus on the topicalities of nanotechnology applications for intranasal delivery of local, systemic, brain, and vaccination purposes during the last decade, referring to the factors affecting delivery, regulatory aspects, and patient expectations. This review further identifies the benefits of applying the Quality by Design approaches (QbD) in product development. According to the reported studies on nanotechnology-based intranasal delivery, potential attention has been focused on brain targeting and vaccine delivery with promising outcomes. Despite the significant research effort in this field, nanoparticle-based products for intranasal delivery are not available. Thus, further efforts are required to promote the introduction of intranasal nanoparticulate products that can meet the requirements of regulatory affairs with high patient acceptance.

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“…Studies showed that zidovudine (BCS Class III) niosomes prepared with Tween 80 as surfactant and DCP as stabilizer (-ve charge-inducer) effectively entrapped high amounts of drug and released 88.72% of drug over 12 h [13]. Ammar HO et al investigated that Diltiazem (BCS Class I) niosomes prepared with span 60 and Cholesterol (1:1 molar ratio) showed maximum entrapment efficiency and drug release on in-vitro investigation and in-vivo study exhibited an increase in MRT, t1/2 and AUC with a decrease in Ke [14].…”

Section: Choice Of Surfactant and Stabilizermentioning

confidence: 99%

Niosomes as an Emerging Formulation Tool for Drug Delivery-a Review

2019

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Nonionic surfactant based vesicles which are uni/multilamellar in structures are called niosomes. These vesicles contains an aqueous interior surrounded by one or more amphiphilic bilayer membrane forming surfactant which separates them from the bulk solution, and are also called as supramolecular aggregates. Niosomes, being an efficient drug delivery system, investigations are carried out to utilize this system to treat various disorders, to promote improved patient compliance, lesser side effects, reduction in dose, lesser dosage frequency, and higher amount of the drug at the particular site so as to lessen an excessive contact with the whole body. The Pharmacokinetic and Pharmacodynamic profile of Niosomal drug delivery system vary for various entrapped drugs. Drugs that are successful in the mitigation or treatment of CNS disorders should cross the BBB to reach the brain, as BBB seems to be an obstacle for a large number of drugs, including CNS active drugs. This article compiles recent techniques for the preparation and characterization of niosomes, the effect of formulation variables on its physicochemical properties and discussed about its effective applications in drug delivery.Critical packing parameter can be determined by the self-assembly of surfactants to vesicles. CPP=V/IcaHydrophobic tail volume (V), Hydrocarbon tail area (Ic), and Hydrophilic head group area (a) is also shown in fig. 2. I In nt te er rn na at ti io on na al l J Jo ou ur rn na al l o of f A Ap pp pl li ie ed d P Ph ha ar rm ma ac ce eu ut ti ic cs s

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In vitro and in vivo investigation for optimization of niosomal ability for sustainment and bioavailability enhancement of diltiazem after nasal administration

Cited by 49 publications

References 57 publications

Carbamazepine Loaded Vesicular Structures for Enhanced Brain Targeting via Intranasal Route: Optimization, in Vitro Evaluation, and in Vivo Study

Carbamazepine Loaded Vesicular Structures for Enhanced Brain Targeting via Intranasal Route: Optimization, in Vitro Evaluation, and in Vivo Study

Intranasal Nanoparticulate Systems as Alternative Route of Drug Delivery

Niosomes as an Emerging Formulation Tool for Drug Delivery-a Review

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