2016
DOI: 10.3109/10717544.2015.1132797
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Novel non-ionic surfactant proniosomes for transdermal delivery of lacidipine: optimization using 23factorial design andin vivoevaluation in rabbits

Abstract: Context: Proniosomes offer a versatile vesicle drug delivery concept with potential for delivery of drugs via transdermal route. Objectives: To develop proniosomal gel using cremophor RH 40 as non-ionic surfactant containing the antihypertensive drug lacidipine for transdermal delivery so as to avoid its extensive first pass metabolism and to improve its permeation through the skin. Materials and methods: Proniosomes containing 1% lacidipine were prepared by the coacervation phase separation method, characteri… Show more

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Cited by 45 publications
(26 citation statements)
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“…The mean vesicle size of diluted proniosomes ranged from 161.55 ± 1.06 nm to 250.60 ± 1.27 nm with a low polydispersity index ( Table 1). The smaller vesicle size would allow for lowered skin irritation and enhanced skin penetration [34].…”
Section: Resultsmentioning
confidence: 99%
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“…The mean vesicle size of diluted proniosomes ranged from 161.55 ± 1.06 nm to 250.60 ± 1.27 nm with a low polydispersity index ( Table 1). The smaller vesicle size would allow for lowered skin irritation and enhanced skin penetration [34].…”
Section: Resultsmentioning
confidence: 99%
“…The observed permeation improvement of curcumin proniosomes could be attributed to the penetration enhancing capabilities of the included surfactants in the fabrication of proniosomes, which are known by their ability to increase fluidity, solubilize, and extract lipid component of the stratum corneum. Keratin interactions are considered as an additional mechanism through which the surfactants can exert penetration enhancing effects [34]. In addition, the formed niosomes also can enhance the permeability of drugs through structure modification of stratum corneum [64].…”
Section: Discussionmentioning
confidence: 99%
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“…Another study manifested that proniosomes are flexible drug delivery carrier system having potential to deliver drugs effectively through transdermal route. Anti-hypersensitive drug lacidipine loaded transdermal proniosomes were produced by using cremophor RH as nonionic surfactant (Soliman et al, 2016). Rajabalaya et al (2016) successfully encapsulated oxybutynin chloride in proniosomes for its transdermal delivery in overactive bladder therapy.…”
Section: Dermal and Transdermal Deliverymentioning
confidence: 99%
“…The enhancement ratio (Er) attributed to ethosome encapsulation was calculated by the following equation [27]: The data obtained from the permeation studies were kinetically analyzed and the order of drug permeation from the ethosomal gel was determined. Zero-and first-order kinetics as well as the Higuchi diffusion model was employed and the correlation coefficient values (R 2 ) were determined.…”
Section: Preparation and Characterization Of Phcl Ethosomalbuccal Gelmentioning
confidence: 99%