NL8102794A - Prodn. of aq. dispersions of lipid spherules - by forming lamellar phase from lipid and aq. phase for encapsulation then shaking with dispersing liq. - Google Patents

Abstract

Process for forming a dispersion of spherules comprising organised molecular layers contg. an encapsulated aqueous phase comprises (a) mixing (i) a water-dispersible, liq. lipid having a nonionic or ionic hydrophilic portion and a lipophilic portion adn of HLB value such that it swells in the encapsulated aqs. phase, ith (ii) the aqueous phase to be encapsulated; (b) stirring to form a lamellar phase; and (c) addig a dispersing liq. in amt. greater than that of the lamellar phase and vigorously shaking for 15 min. to 3 hrs. Process is esp. used for encapsulation of cosmetic agents such as artificial tanning agents, sunscreen agents, antiperspirants, deodorants, depilatories, antiserborrhoeics etc., or a foodstuff or pharmaceutical agent such as vitamins, hormones, enzymes, vaccines, antiinflammatories, e.g. hydrocortisone, antibiotics and bactericides.

Description

* N.0. 30242!

Division of patent application no. 7607210 dd. June 30, 1976

A method of preparing a dispersion of small spherical particles.

The invention relates to a method for preparing a dispersion of small spherical particles consisting of molecular layers, which enclose an aqueous phase and which are formed by at least one liquid water-dispersible lipid of the formula XY, wherein X is a hydrophilic group and Y represent a lipophilic group.

Such a method is known from French patent 2,221,122, articles by Sessa and Weissmann in 3. Lipid Res. 9 (1968), 310 and 3. of Biological Chemistry, 243 (1970), 3295-3301, one article by Magee and Miller in Nature, 235 (1972), 339-340 and an article 10 by Kinsky et al in Biochimica et Biophysics Acta 152 (1968), 174-185. Thereby, one or more lipids are added to an aqueous phase, after which the resulting mixture is heated slightly, then energized with shock and finally treated with ultrasonic vibrations to reduce the diameter of the small spherical particles formed to a value below 100 nm. It is also possible to evaporate this solvent from a solution of the lipid in a solvent in the presence of a wall, so that thin layers of the lipid are formed on that wall. These layers are then brought into contact with a continuous aqueous phase with energetic movement. The system thus obtained is then treated with ultrasonic vibrations. The spherical particles thus obtained are called liposomes. They consist of a closed system of concentric mono-, bi- and multilayers of lipids, between which the aqueous phase is enclosed, which phase can contain active substances, such as medicines, proteins, enzymes, hormones and vitamins.

This aqueous phase also serves as a dispersing liquid for the liposomes.

All of this known method of preparing liposomes utilized lipids, which may be represented by the formula X-Y, wherein X is an ionic hypophilic group and Y is a lipophilic; group. When nonionic lipids, such as the so-called Triton X * 100, an oxethylation product of p-diisobutylphenol with 9-10 oxyethylene units per molecule, were added, the structure of the 81 02 7 9 4 2 of the liposomes disintegrated and release the trapped hydrous phase (Sessa and Weissmann lc and Kinsky cslc) ·

However, it has been found that a dispersion of small spherical particles with an enclosed aqueous phase can also be obtained when, according to the invention, dispersions known per se for the preparation of analogous dispersions are prepared using lipids of the formula XY. wherein X represents a nonionic hydrophilic group.

The spherical particles formed in the dispersion according to the invention, which are called niosomes, are much more stable than the known liposomes. In both liposomes and niosomes, furthermore, when the particle size is reduced by ultrasonic vibrations, there is always an increase in the permeability for the enclosed aqueous phase. However, this permeability increase is much smaller for the niosomes than for the liposomes. Furthermore, the niosomes can enclose a greater amount of aqueous phase than the liposomes. Finally, when using niosomes, the formation of spherical particles with an electrically charged outer surface can be avoided.

The particle size of the niosomes ranges from 10-5000 nm.

In the water-containing phase to be enclosed, all kinds of active substances may be present, in particular substances which are of importance in the pharmaceutical or food field, or substances with a cosmetic activity.

The cosmetic active agents are, for example, products for the maintenance of the skin and hair, for example wetting agents, such as glycerol, sorbitol, pentaerythritol, inositol, pyrrolidone carboxylic acid and salts thereof, artificial "sun" tanning agents, such as dihydroxy-acetone, erythrulose, glyceraldehyde, -dialdehydes, such as tartar aldehyde (which products may optionally be used in combination with dyes), water-soluble antisolar agents, antiperspirants, deodorants, astringents, refreshing, tonic, wound healing, keratolytic and depilatories, perfumed aqueous liquids animal or vegetable tissue extracts, such as proteins, polysaccharides and amniotic fluid, water-soluble dyes, formation of dander, anti-pimple agents, anti-pimple agents, oxidizing agents (decolorizers) such as hydrogen peroxide, reducing agents such as thioglycolic acid and at that. As active pharmaceutical substances can be mentioned: vitamins, hormones, enzymes (eg 8102794 "3 dismutase peroxide), vaccines, anti-inflammatory agents (eg hydrocortisone), antibiotics and bactericides.

Depending on the active substance present in the aqueous phase to be encapsulated, one selects the lipids with which the water-containing phase can be stably contained. If the lipids are to provide stable spherical particles, it is necessary that there is sufficient lateral interaction between the chains of the lipids, which form side by side the layers or bilayers of the spherical particles, that is, the Van der Waals forces between the chains provide sufficient cohesion of the layers. The lipids which can be used in the method according to the invention belong to the group of emulsifiers of the water-in-oil type.

In the method according to the invention one can use a single lipid or a mixture of lipids. In the lipids, group Y preferably has one or two saturated or unsaturated, branched or straight lipophilic chains of 12-30 carbon atoms, such as a lauryl, tetradecyl, hexadecyl, isostearyl, oleyl, lanolyl, or alkylphenyl chain. The hydrophilic group X of the lipid is preferably derived from polyethylene glycol, polyglycerol and / or polyethylated or unoxylated polyol ester, for example an oxyethylated sorbitol ester.

As lipids, linear or branched polyglycerol ethers of formulas 1 and / or 2 are preferably used, in which n denotes an integer with a value of 1-6 and R denotes a saturated or unsaturated straight chain or branched aliphatic chain with 12 to 30 carbon atoms or hydrocarbon residues of lanolin alcohols or 2-hydroxyalkyl groups of long-chain α-diols, oxyethylated fatty alcohols, whether or not oxyethylated polyol esters, especially oxyethylated sorbitol esters, or glycolipids of natural or synthetic origin, eg cerobrosides.

Various additives can be combined with the non-ionic lipids to modify the permeability and / or surface charge of the spherical particles. Such additives are, for example, long-chain alcohols and diols, sterols, for example, cholesterol, long-chain amines and quaternary ammonium derivatives thereof, dihydroxyalkylamines, oxyethylated fatty amines, long chain amino alcohol esters and quaternary ammonium derivatives thereof, phosphoric acid esters of fatty alcohols for example, the sodium salt 81 02 7 9 4 4 of phosphoric acid dicetyl ester, alkyl sulfates, for example sodium acetyl sulfate, polypeptides and proteins.

Preferably, the aqueous phase to be encapsulated is a solution of an active substance in water and the continuous phase of the dispersion 5 is also an aqueous phase. The weight ratio of the small spherical particles to the continuous phase of the dispersion is preferably between 0.01: 1 and 0.5: 1, while the continuous phase of the dispersion is preferably iso-osmotic to the entrapped aqueous phase .

For example, the niosomes are prepared in the manner described in the above references at room temperature or at elevated temperature, if the lipid is solid at room temperature. If it is desired to prepare spherical particles with a diameter below 100 nm, the dispersion obtained can be subjected to an ultrasonic treatment.

Furthermore, various products can be added to the dispersions of the niosomes according to the invention, the object of which is to change the appearance or the organoleptic character, such as opaque agents, gelling agents, aromas, perfumes and / or dyes.

The dispersions of the niosomes make it possible to absorb hydrophilic substances in a substantially lipophilic medium. They are present in a masked state under these conditions, thereby providing a protective effect over various substances which allow changes, such as oxidizing agents, digestive juices and generally substances which are reactive with the contained active substances. . The penetration and / or fixation of active substances can be modulated by changing the size of the spherical I-shaped particles and their electrical charge. Its action can also be delayed (delayed effect). Moreover, the fact that they are masked makes it possible to suppress or significantly alter their organoleptic character, in particular the taste. Finally, the lipids used in these preparations have a beneficial effect as such, for example a softening, lubricating and / or glossy effect.

The invention is illustrated by the following examples. When the examples refer to an x-molar (NaCl.KCl) solution, this equates to an equimolar solution of 81 02 7 9 4 5

NaCl or KCl in water with a total molarity of x.

Example I,

In a 50 ml round bottom flask placed in a water bath at a temperature of 55 ° C, 500 mg of a product of the formula II, wherein R represents the hexadecyl group and n denotes number 2, were contacted charged with 10 ml of a 0.3 molar methionine aqueous solution, after which the mixture was homogenized at a temperature of 55 ° C,

The flask was placed on a shaker and vigorously stirred at a temperature of 55 ° C for 3 hours.

The dispersion obtained was clear, while the diameter of the spherical particles was 1 / um. A white jelly was obtained by cooling to room temperature.

Example II.

In a 50 ml round bottom flask, 500 mg of a product of the formula 2, wherein R represents the alkyl radical of isostearyl alcohol and n denotes a statistical mean value of 2, were contacted with 5 ml of water, after which the mixture was homogenized. : The procedure was performed at room temperature.

The shaker was placed and agitated vigorously for 4 hours.

The dispersion obtained was milky, while the diameter of the spherical particles was 51-111.

The dispersion was ultrasonicated to significantly reduce the size of the spherical particles.

Example III.

In a 50 ml round bottom flask, 83.2 mg (200 ywol) of a product of the formula 2, wherein R represents the alkyl residue of oleyl alcohol and n denotes the number 2, were dissolved in 2 ml of a mixture of chloroform and ethanol in a mixing ratio of 2: 1. The solvent was evaporated on a rotary evaporator, after which the last trace amounts of solvent were removed by treatment with a rotary vane pump for one hour.

10 ml of a 0.3 molar glucose solution in water were contacted with the lipid. The flask was placed on a shaker and agitated vigorously for b hours. The procedure was performed at room temperature.

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The dispersion was ultrasonicated for 20 minutes to reduce the diameter of the spherical particles to a value of less than 0.5 / 4m. The dispersion was then filtered through a "Sephadex G 50 coarse" gel column, which had been swelled in 0.14-5 molar (NaCl.KCl) solution. The resulting solution was slightly bluish.

Example IV.

In a 50 ml round bottom flask, 58 mg of a product of the formula 2, wherein R represents the alkyl group of isostearyl-10 alcohol and n denotes an average statistical value of 2, were intimately mixed with a product of the formula 2, wherein R represents the alkyl group of isostearyl alcohol and n indicates an average statistical value of 6, after which the resulting mixture is contacted with 10 ml of a 1 molar glucose solution in water. The method was carried out at room temperature. The flask was placed on a shaker and agitated vigorously for 4 hours.

The dispersion obtained was very fine, while the spherical particles had a diameter of. If the dispersion was further exposed to ultrasonic vibrations for 30 minutes, the size of the spherical particles was reduced to a value of less than ^, πι.

The dispersions, containing either spherical particles with a diameter of more than IftiM or spherical particles with a diameter of less than 0.5 µm, were filtered through a gel column of "Sephadex G 50 coarse", which had a 0, 4-75 molar (NaCl.KCl) solution was swelled.

Example V.

In a 50 ml flask, 80 mg of a product of the formula 2, wherein R represents the hexadecyl group and n denotes the number 2, 10 mg of cholesterol and 10 mg of dicetylphosphate were dissolved in 2 ml of a mixture of chloroform and methanol in a mixing ratio of 2: 1.

The solvent was evaporated on a rotary evaporator, after which the last trace amounts of the solvent were removed by treatment with a rotary vane pump for one hour.

Then, 10 ml of 0.15 molar solution of the sodium salt of pyroglutamic acid in water was contacted with the lipids. The flask was placed on a shaker and vigorously stirred in a water bath at 55 ° C for 2 hours, then gradually cooled to room temperature.

The dispersion was subjected to ultrasonication at room temperature for one hour. The dispersion was then filtered through a "Sephadex G 50 coarse" gel column which had been swelled with distilled water. The dispersion 10 obtained, after being subjected to ultrasonic vibrations, was smooth and clear, while the diameter of the spherical particles was less than / tm.

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Claims (4)

A process for preparing a dispersion of small spherical particles consisting of molecular layers, which enclose an aqueous phase and are formed by at least one liquid, water-dispersible lipid of the formula XY, wherein X is a hydrophilic group and Y is a lipophilic group, characterized in that dispersions are prepared in a manner known per se for the preparation of analogous dispersions using lipids of the formula XY, wherein X represents a nonionic hydrophilic group. A method according to claim 1, characterized in that the group X of the lipid is derived from polyethylene glycol, polyglycerol or whether or not oxyethylated polyol ester. 3. Process according to claims 1 and 2, characterized in that the lipophilic group Y contains one or two chains with 12-30 carbon atoms. 4 ·. Process according to claims 1-3, characterized in that one or more linear and / or branched polyglycerol ethers of the formulas 1 and / or 2, wherein n is an integer with a value of 1 to 6, are used as lipids and R represents a saturated or unsaturated linear or branched aliphatic chain of 12 to 30 carbon atoms, hydrocarbon residues of lanolin alcohols and / or 2-hydroxyalkyl residues of long chain oC-diols, oxethylated fatty alcohols, oxethylated sorbitol esters and / or glycolipids of natural 25 or synthetic origin used. 81 02 7 9 4