Acute toxicity and skin irritation of pyrrolidone derivatives as transdermal penetration enhancer

We investigated preliminary acute toxicity and primary skin irritation of nine pyrrolidone derivatives which had been previously developed as transdermal penetration enhancers. The acute toxicity was observed at a dose of 500 mg/kg after intraperitoneal administration in mice. Their primary skin irritations were examined with rabbit dorsal skin. 1-Lauryl-2-pyrrolidone induced the most severe irritation among the derivatives. Pyrrolidone derivatives having methyl group and methyloxycarbonyl group caused little irritation. The primary irritation indices of pyrrolidone derivatives were not relative to their accumulations in the skin but to their enhancing effects. In conclusion, 1-hexyl-4-methyloxycarbonyl- and 1-lauryl-4-methyloxycarbonyl-2-pyrrolidone are suggested to be adequate enhancers, judging from the balance of their enhancing activity and irritation.     

Confinement of DNA in water-in-oil microemulsions

The study of systems that allow DNA condensation in confined environments is an important task in producing cell-mimicking microreactors capable of biochemical activities. The water droplets formed in water-in-oil emulsions are potentially good candidates for such microcompartments. The anionic surfactant AOT was used here to stabilize the droplets. We have studied in detail the DNA distribution and the structural modifications of these microemulsion drops by varying the concentration and molecular weight of DNA and using various techniques such as light, X-ray, and neutron scattering, electrical conductivity, and surface tension. DNA induces the formation of large drops into which it is internalized. The size of these drops depends on the amount of DNA dissolved in water as well as on its molecular weight. The local DNA concentration is very high (>100 mg/mL). The large drops coexist with small empty drops (not containing DNA), similar to those found in the DNA-free microemulsion.     

Preparation and characterization of water-in-oil decane/AOT microemulsions containing silver and gold nanoparticles and large amounts of water

Stable microemulsions with water contents as high as 10 vol % have been obtained, including those additionally containing silver and gold nanoparticles. Especial attention has been focused on the influence of water and stabilizer contents on the structure of adsorption layers on nanoparticles. The properties of nanoparticles obtained via the traditional microemulsion synthesis have been compared with the properties of nanoparticles that have preliminarily been concentrated with the help of electrophoresis and dried. The electrophoretic concentration and drying of nanoparticles have been shown to improve the stability of their microemulsions. Microemulsions with the highest content of water have been studied to determine the occurrence of percolation and the influence of nanoparticles on their percolation temperature and electrical conductivity.     

Growth of silica nanoparticles in methylmethacrylate-based water-in-oil microemulsions

The mechanism of silica particle formation in monomer microemulsions is studied using dynamic light scattering (DLS), atomic force microscopy, small-angle X-ray scattering (SAXS), and conductivity measurements. The hydrolysis of tetraethylorthosilicate (TEOS) in methylmethacrylate (MMA) microemulsions (MMA = methylmethacrylate) is compared with the formation of SiO₂ particles in heptane microemulsions. Stable microemulsions without cosurfactant were found for MMA, the nonionic surfactant Marlophen NP10, and aqueous ammonia (0.75 wt%). In the one-phase region of the ternary phase diagram, the water/surfactant ratio (R _w) could be varied from 6 to 18. The DLS and SAXS measurements show that reverse micelles form in these water-in-oil (w/o) microemulsions. The minimum water-to-surfactant molar ratio required for micelle formation was determined. Particle formation is achieved from the base-catalyzed hydrolysis of TEOS. According to atomic force microscopy measurements of particles isolated from the emulsion, the particle size can be effectively tailored in between 20 and 60 nm by varying R _w from 2–6 in heptane w/o microemulsions. For MMA-based microemulsions, the particle diameter ranges from 25 to 50 nm, but the polydispersity is higher. Tailoring of the particle size is not achieved with R _w, but adjusting the particle growth period produces particles between 10 and 70 nm.     

Preparation of Cu-Ni alloy nanocrystallites in water-in-oil microemulsions

The well-mixed copper-nickel nanoparticles were prepared when the molar ratio of Cu2+ to Ni2+ was 1:1 by simultaneous reduction of CuSO4 and NiCl2 with hydrazine in the microemulsion of SDS/n-butanol/n-heptane/water at 70 degrees C, and was characterized by TEM, ED, TGA, EDS, and XRD. ED analysis and XRD patterns suggest the formation of the homogeneous alloy structure in the bimetallic nanoparticles. Average size of the sample calculated from the full width at medium height of peak 111 in the XRD patterns using Scherrer formula is 5.53 nm. TEM photographs show a narrow distribution of Cu-Ni nanoparticles that essentially are monodispersed and the mean diameter is 12 nm. The results indicate that the composition and size of alloy nanoparticles depend on the mole ratio of H2O to SDS, the method of addition of Cu2+ and Ni2+, and the mole ratio of Cu2+ and Ni2+ in the initial precursor solution.     

Preparation of organic nanoparticles using microemulsions: their potential use in transdermal delivery

Organic nanoparticles of cholesterol and retinol have been synthesized in various AOT (Aerosol OT; sodium bis(2-ethylhexyl) sulfosuccinate)/heptane/water microemulsions by direct precipitation of the active principle in the aqueous cores. The nanoparticles are observed by transmission electron microscopy (TEM) using the adsorption of a contrasting agent, such as iodine vapor. The size of the nanoparticles can be influenced, in principle, by the concentration of the organic molecules and the diameter of the water cores, which is related to the ratio R=[H2O]/[surfactant]. The particles remain stable for several months. The average diameter of the cholesterol nanoparticles varies between 3.0 and 7.0 nm, while that of retinol varies between 4.0 and 10 nm. The average size of the cholesterol nanoparticles does not change much either as a function of the ratio R or as a function of the concentration of cholesterol. The constant size of the nanoparticles can be explained by the thermodynamic stabilization of a preferential size of the particles. Chloroform is used to carry the active principle into the aqueous cores. Retinol molecules form J-complexes composed of two or three molecules, as detected by UV-visible spectroscopy.     

Numerical study of a drug release profile in the transdermal drug delivery system

Drug release by diffusion from an unstressed thin polymer film with a dissolved crystallizable component was simulated using a kinetic Monte Carlo model. This model was used previously to study Ostwald ripening in a high crystallizable component regime and was shown to correctly simulate solvation, diffusion, and precipitation. In this study, the same model with modifications was applied to the drug transportation and release in the low concentration regime of interest to the transdermal drug delivery system (TDS) community. We demonstrate the model's utility by simulating diffusion, crystal precipitation, growth and shrinkage during storage, and drug release from the thin TDS to a surface under different conditions. The simulation results provide a first approximation for the drug release profile occurring from TDS to skin. It has been reported that growth of drug crystals in TDS occurs mainly in the middle third of the polymer layer at relatively higher temperatures. The results from the simulations showed that the release rate and concentration profile of a TDS depend on the dissolution process of the crystal. At low storage temperature, the drug precipitates to form small evenly distributed crystals throughout the thickness of the TDS patch. The release rate of these small, evenly distributed crystals most closely matched that of a completely dissolved drug.     

Tailoring of horseradish peroxidase activity in cationic water-in-oil microemulsions

Horseradish peroxidase (HRP) in cationic water-in-oil (W/O) microemulsions has always been ignored in reverse micellar enzymology, mainly because cationic surfactants are inhibitors of enzyme peroxidase. In the present study, for the first time, we have successfully introduced the cationic W/O microemulsion as an attractive host for efficient HRP activity. To this notion, much improved activity of HRP was observed in the W/O microemulsion of cetyltrimethylammonium bromide (CTAB) with an increase in n-hexanol concentration and W0 ([water]/[surfactant]), presumably due to the increased interfacial area of the microemulsions. In support of our above observation, six surfactants were synthesized with an increased headgroup size where the methyl groups of CTAB were subsequently replaced by the n-propyl and 2-hydroxyethyl groups, respectively, to prepare mono-, di-, and tripropylated/hydroxyethylated n-hexadecylammonium bromide. The peroxidase activity enhanced with headgroup size and also followed an overall trend similar to that found in the case of CTAB. Possibly, the reduced positive charge density at the augmented interfacial area by means of increase, either in headgroup size, cosurfactant concentration, and/or W0, is not capable of inactivating HRP. Also, the larger space at the interface may facilitate easier solubilization of the enzyme and increase the local concentration of enzyme and substrate, leading to the higher activity of HRP. The best activity was obtained with surfactant N-hexadecyl-N,N,N-tripropylammonium bromide, the highest ever found in any cationic W/O microemulsions, being almost 3 times higher than that found in water. Strikingly, this observed highest activity is comparable with that observed in an anionic bis(2-ethylhexyl)sulfosuccinate sodium salt (AOT)-based system, the best W/O microemulsions used for HRP.     

Structure of microemulsions of AOT and water in dodecane

The dielectric properties of the system water/AOT/dodecane are studied as a function of volume fraction of the dispersed phase and molar ration (water/surfactant). Data shows that the spherical model is valid only at lown values or low values. At high concentrations of dispersed phase, one has to consider micellar aggregation or deformation.     

Investigation of AOT reverse microemulsions in supercritical carbon dioxide

Bis(2-ethylhexyl) sodium sulphosuccinate (AOT) was successfully solubilised in supercritical carbon dioxide (scCO₂), with ethanol or pentanol as co-solvent. Three molecular spectroscopic probes: methyl orange (MO), 8-hydroxy-1,3,6-pyrenetrisulphonic acid trisodium salt (HPTS), and riboflavin (RF) were used to examine the solubilisation characteristics of the water/scCO₂ microemulsions formed with AOT. MO was extracted at various operating conditions, although the wavelength of its solvatochromic absorption maximum was not indicative of bulk water properties. Instead, the spectral results imply that MO may be located at the surfactant/water interface. The highly water-soluble dye HPTS was unable to be extracted into scCO₂/AOT/water systems, suggesting that the water in the reverse micelle core was not as polar under supercritical conditions as those at ambient conditions. Finally, RF was extracted into the supercritical phase (40°C, 175 bar) with pentanol co-solvent, with an apparent enhanced uptake compared with the value at 40°C and ambient pressure in bulk water. This appears to be due to the presence of microcrystals dispersed in the supercritical phase.     

Iontophoretic transdermal drug delivery system using a conducting polymeric membrane

This work investigated the application of a porous polyaniline (PANi) membrane as a conducting polymeric membrane as well as an electrode in an iontophoretic transdermal drug delivery (TDD) system. Model drugs studied were: caffeine (MW: 194.2), lidocaine HCl (MW: 270.8) and doxycycline HCl (MW: 480.1). The PANi membrane was first tested as a simple membrane between the donor and receptor solutions; it provided satisfactory permeation profiles; the observed flux values were well described by a simplified mass transport model. A mouse skin was then mounted beneath the PANi film; such a composite system also presented satisfactory permeation profiles. Iontophoretic TDD experiments were next performed using both Ag|AgCl electrodes and PANi|AgCl electrodes for comparison; a PANi anode replaced the Ag anode in the last set. For doxycycline HCl, the flux and the 24-h accumulation from the PANi|AgCl set were 94.4 ± 81.2 μg/cm² h and 2760 ± 3980 μg/cm², respectively; those from the Ag|AgCl set were zero. For lidocaine HCl, the flux and 10-h accumulation from the PANi|AgCl set were, respectively, 43 ± 15 μg/cm² h and 392 ± 130 μg/cm²; the corresponding values from the Ag|AgCl set were 48 ± 20 μg/cm² h and 348 ± 78 μg/cm². Porous polyaniline membrane appears to be capable of replacing the Ag part of Ag|AgCl electrode system; further such a membrane can exercise additional control over agent transport rate. Aqueous-organic partitioning system through the porous membrane of PANi was tested with this novel technique as well. Because of the rather low porosity of the synthesized PANi film, such a system did not yield a high permeation rate.     

Effect of AOT on enzymatic activity of the organic solvent resistant tyrosinase from Streptomyces sp. REN-21 in aqueous solutions and water-in-oil microemulsions

The effect of AOT (sodium-bis(2-ethylhexyl sulfosuccinate)) on enzymatic activity of the organic solvent resistant tyrosinase (OSRT) in aqueous phosphate buffer solutions and in water-in-oil microemulsions of the water/AOT/isooctane system has been investigated. In contrast to mushroom tyrosinase, AOT does not activate OSRT in aqueous solutions, altering its activity very little at concentrations lower than 2 mM. Increasing contents of AOT in isooctane reduce the observed initial reaction rates of oxidation of t-butylcatechol (tBC) and 4-methylcatechol (4-MC). Similarly to mushroom tyrosinase, the effect has been described using an equation based on preferential binding of the substrates by surfactant interface layers. The apparent Michaelis-Menten substrate binding constants increase linearly with AOT concentration (with slopes of 0.12+/-0.02 and 0.051+/-0.006 for tBC and 4-MC, respectively), and the effective enzyme turnover number in the microemulsions remains practically constant.     

The use of novel water-in-oil microemulsions in microemulsion electrokinetic chromatography

We describe the novel use of water-in-oil (W/O) microemulsions to achieve unique separations in microemulsion electrokinetic chromatography (MEEKC). The choice and concentration of the buffer type, surfactant and co-surfactant were all examined and optimized. Separations of a range of neutral and acidic analytes was shown to be markedly different to that obtained by (oil-in-water) O/W MEEKC. Neutral solutes are separated by virtue of their solubility (log P) values in O/W MEEKC with the more water-insoluble solutes migrating last. This separation process does not occur in W/O, as neutral solutes are not separated in order of log P.     

Temperature-controlled change of charge transport mechanisms in nonionic water-in-oil microemulsions

 The temperature-controlled transition from the Stokes charge transport of aqueous nanodroplets to the intrinsic conduction of nanodroplet clusters in nonionic microemulsions was studied. Two different charge transport processes apparent from a minimum value of the conductance have been simulated based on straightforward physical models. Their predictions compare favourably with the observations. Received: 4 September 2001 Accepted: 20 September 2001     

Spectrometric study of AOT-hydrolysis reaction in water/AOT/isooctane microemulsions using phenolphthalein as a chemical probe

The kinetics of the alkaline hydrolysis of sodium bis(2-ethylhexyl)sulfosuccinate (AOT) in water/AOT/isooctane microemulsions has been studied by monitoring the absorbance change of the phenolphthalein in the system with time. The apparent first-order rate constant k(obs) has been obtained and found to be dependent on both the molar ratio of water to AOT ω and the temperature. The dependences of k(obs) on ω have been analyzed by a pseudophase model which gives the true rate constants k(i) of the AOT-hydrolysis reaction on the interface and the partition coefficients K(wi) for the distribution of OH(-) between aqueous and interface pseudophases at various temperatures; the latter is almost independent of the temperature and ω. The temperature dependences of the reaction rate constants k(obs) and k(i) have been analyzed to obtain enthalpy ΔH(≠), entropy ΔS(≠), and energy E(a) of activation, which indicate that the distribution of OH(-) between aqueous and interface pseudophases increases ΔS(≠) but makes no contribution to E(a) and ΔH(≠). The influence of the overall concentration of AOT in the system on the rate constant has been examined and found to be negligible. It contradicts with what was reported by García-Río et al. (1) but confirms that the first-order reaction of the AOT-hydrolysis takes place on the surfactant interface. The study of the influence of AOT-hydrolysis on the kinetics of the alkaline fading of crystal violet or phenolphthalein in the water/AOT/isooctane microemulsions suggests that corrections for the AOT-hydrolysis in these reactions are required.     

Influence of polyethylene glycols on percolative phenomena in AOT microemulsions

The influence of different polyethylene glycol (PEG) on the percolation of the ternary system composed by sodium bis(2-ethylhexyl) sulfosuccinate (AOT) + isooctane + water has been studied. The additives used were chosen on the basis of its chain length (the number of polymeric units). In all cases, we observed a decrease in the percolation threshold on increasing the amount of PEG added to the AOT microemulsions. We observed a correlation between the effect exerted by the additive upon the percolation temperature and its chain length. Moreover, a relationship between the percolation temperature and the additive partition coefficient between 1-octanol and water (logP) was found. Both of them proved the importance of the inclusion of the additives into the microemulsion interface to explain their influence upon the percolative phenomenon. Such inclusion modified the properties of the AOT film, facilitating the exchange of matter between droplets.     

Proteolytic activity in various water-in-oil microemulsions as related to the polarity of the reaction medium

The catalytic behaviors of α-chymotrypsin and of trypsin were studied in anionic AOT-isooctane-water and cationic CTAB-ROH-isooctane-water microemulsion systems. The effects of various parameters, such as the pH and the water content expressed in terms of the molar ratio w_o = [H₂O]/[Surfactant], on the enzyme activity, were examined. The kinetic constants were calculated and it was found that in the case of trypsin the enzyme exhibited a remarkable “superactivityrd, when studied in the CTAB microemulsion systems. The effect of the alcohol cosurfactant used in these cationic systems was investigated in relation to the polarity of the reaction medium. By using the hydrophilic probe 1-methyl-8-oxyquinolinium betaine the micropolarity of the water core was determined and related to the kinetic results.     

Colloidochemical aspects of transdermal drug delivery (review)

This review generalizes scientific information on factors that determine the efficacy of transdermal drug delivery, including the barrier functions of skin, the properties of drugs and enhancers of skin permeability, and the type of a transdermal therapeutic system, i.e., plaster. Colloidochemical aspects of transdermal drug delivery are considered in relation to the amphiphilic structure of drugs and action mechanisms of enhancers, among which nonionic surfactants prevail. Advantages of microreservoir-type transdermal therapeutic systems are shown, information on which is very scarce; the prospects of their development on the basis of oil-in-water and water-in-oil emulsions containing nonionic surfactants and polymer adhesives are outlined.