RU2599007C1 - Method of producing nanocapsules of ciprofloxacin hydrochloride in sodium alginate - Google Patents

Abstract

FIELD: medicine.

SUBSTANCE: invention relates to nanotechnology and medicine. Method of producing nanocapsules of ciprofloxacin hydrochloride in sodium alginate envelope is described. According to the method of invention ciprofloxacin hydrochloride powder is added to sodium alginate suspension in benzene, containing 0.01 g of preparation E472c as surfactant. Then butyl chloride is added. Obtained suspension of nanocapsules is filtered and dried. Process is performed at 25 ^oC during 15 minutes.

EFFECT: method provides simple and fast process of producing nanocapsules and increases mass output.

1 cl, 1 dwg, 5 ex

Description

The invention relates to the field of nanotechnology, medicine, pharmacology and veterinary medicine.

Previously known methods for producing microcapsules of drugs. So, in US Pat. 2092155 IPC A61K 047/02, A61K 009/16, published on 10/10/1997, Russian Federation, a method for microencapsulation of drugs based on the use of special equipment using ultraviolet radiation was proposed.

The disadvantages of this method are the duration of the process and the use of ultraviolet radiation, which can affect the process of formation of microcapsules.

In US Pat. 2095055 IPC A61K 9/52, A61K 9/16, A61K 9/10, Russian Federation, published November 10, 1997, a method for producing solid non-porous microspheres, including melting a pharmaceutically inactive carrier substance, dispersing the pharmaceutically active substance in a melt in an inert atmosphere, spraying the resulting dispersion in the form of fog in a freezing chamber under pressure in an inert atmosphere at a temperature of from -15 to -50 ° C and separating the resulting microspheres into fractions by size. A suspension intended for administration by parenteral injection contains an effective amount of said microspheres distributed in a pharmaceutically acceptable liquid vector, the pharmaceutically active substance of the microsphere being insoluble in said liquid medium.

The disadvantages of the proposed method: the complexity and duration of the process, the use of special equipment.

In US Pat. 2076765 IPC B01D 9/02, Russian Federation, published on 04/10/1997, a method for producing dispersed particles of soluble compounds in microcapsules by crystallization from a solution is proposed, characterized in that the solution is dispersed in an inert matrix, cooled, and dispersed particles are obtained by changing the temperature.

The disadvantage of this method is the difficulty of execution: obtaining microcapsules by dispersion with subsequent change in temperature, which slows down the process.

In US Pat. 2101010 IPC A61K 9/52, A61K 9/50, A61K 9/22, A61K 9/20, A61K 31/19, Russian Federation, published January 10, 1998, a chewing form of the drug with a taste mask is proposed, which has the properties of a controlled release of the drug contains microcapsules with a size of 100-800 microns in diameter and consists of a pharmaceutical core with crystalline ibuprofen and a polymer coating comprising a plasticizer flexible enough to withstand chewing. The polymer coating is a methacrylic acid based copolymer.

The disadvantages of the invention: the use of a copolymer based on methacrylic acid, as these polymer coatings can cause cancerous tumors; obtaining microcapsules by suspension polymerization; complexity of execution; the duration of the process.

In US Pat. 2139046 IPC A61K 9/50, A61K 49/00, A61K 51/00, Russian Federation, published on 10/10/1999, a method for producing microcapsules as follows. An oil-in-water emulsion is prepared from an organic solution containing dissolved mono-, di-, triglyceride, preferably tripalmitin or tristearin, and possibly a therapeutically active substance, and an aqueous solution containing a surfactant, possibly a portion of the solvent is evaporated, a redispersing agent is added the agent and the mixture are freeze dried. The freeze-dried mixture is then redispersed in an aqueous carrier to separate the microcapsules from organic residues, and the hemispherical or spherical microcapsules are dried.

The disadvantages of the proposed method are the complexity and duration of the process, the use of freeze-drying, which takes a lot of time and slows down the process of obtaining microcapsules.

In US Pat. 2159037 IPC A01N 25/28, A01N 25/30, Russian Federation, published November 20, 2000, a method for producing microcapsules by a polymerization reaction at the phase boundary, containing solid agrochemical material 0.1-55 wt. % suspended in a water-miscible organic liquid, 0.01-10 wt. % non-ionic dispersant active at the phase boundary and not acting as an emulsifier.

The disadvantages of the proposed method: complexity, duration, the use of high shear mixer.

In the article “Development of microencapsulated and gel-like products and materials for various industries”, Russian Chemical Journal, 2001, vol. XLV, No. 5-6, p. 125-135 describes a method for producing microcapsules of drugs by gas-phase polymerization, since the authors of the article consider the method of chemical coacervation from aqueous media to be microencapsulated as unsuitable because most of them are water-soluble. The microencapsulation process using the gas phase polymerization method using n-xylylene includes the following main stages: evaporation of the n-xylylene dimer (170 ° C), its thermal decomposition in a pyrolysis furnace (650 ° C at a residual pressure of 0.5 mm Hg), transfer of reaction products to the “cold” polymerization chamber (20 ° C, residual pressure 0.1 mm Hg), precipitation and polymerization on the surface of the protected object. The polymerization chamber is made in the form of a rotating drum, the optimum speed for coating the powder is 30 rpm. The thickness of the shell is regulated by the time of coating. This method is suitable for encapsulation of any solids (with the exception of prone to intense sublimation). The resulting poly-n-xylylene highly crystalline polymer, characterized by high orientation and tight packaging, provides a conformal coating.

The disadvantages of the proposed method are the complexity and duration of the process, the use of gas phase polymerization, which makes the method inapplicable for producing microcapsules of drugs in polymers of protein nature due to denaturation of proteins at high temperatures.

In US Pat. WO / 2010/076360 ES IPC B01J 13/00; A61K 9/14; A61K 9/10; A61K 9/12, published July 8, 2010, proposes a new method for producing solid micro- and nanoparticles with a homogeneous structure with a particle size of less than 10 μm, where the treated solid compounds have a natural crystalline, amorphous, polymorphic and other states associated with the starting compound. The method allows to obtain solid micro- and nanoparticles with substantially spheroidal morphology.

The disadvantage of the proposed method is the complexity and duration of the process.

In US Pat. WO / 2010/119041 EP IPC A23L 1/00, published October 21, 2010, a method for producing microspheres containing an active component encapsulated in a gel matrix of whey protein including denatured protein, serum and active components is proposed. The invention relates to a method for producing beads that contain components such as probiotic bacteria. A method for producing microspheres includes the stage of production of microspheres in accordance with the method of the invention and the subsequent curing of the microspheres in a solution of an anionic polysaccharide with a pH of 4.6 or lower for at least 10, 30, 60, 90, 120, 180 minutes. Examples of suitable anionic polysaccharides: pectins, alginates, carrageenans. Ideally, whey protein is heat-denaturing, although other denaturation methods are also applicable, such as pressure-induced denaturation. In a preferred embodiment, the whey protein is denatured at a temperature of from 75 ° C to 80 ° C, appropriately for from 30 minutes to 50 minutes. As a rule, whey protein is mixed with heat denaturation. Accordingly, the concentration of whey protein is from 5 to 15%, preferably from 7 to 12%, and ideally from 9 to 11% (weight / volume). Typically, the product is subject to filtration, which is carried out through many filters with a gradual reduction in pore size. Ideally, a fine filter has submicron pore sizes, for example from 0.1 to 0.9 microns. A preferred method for producing beads is a method using vibratory encapsulators (Inotech, Switzerland) and machines manufactured by Nisco Engineering AG ,. As a rule, nozzles have openings of 100 and 600 microns, and ideally about 150 microns.

The disadvantage of this method is the use of special equipment (vibration encapsulators (Inotech, Switzerland)), the production of microcapsules by protein denaturation, the difficulty of isolating the microcapsules obtained by this method is filtration using multiple filters, which makes the process long.

In US Pat. WO / 2011/003805 EP IPC B01J 13/18; B65D 83/14; C08G 18/00, published January 13, 2011, describes a method for producing microcapsules that are suitable for use in compositions forming sealants, foams, coatings or adhesives.

The disadvantage of the proposed method is the use of centrifugation to separate from the process fluid, the duration of the process, as well as the use of this method not in the pharmaceutical industry.

In US Pat. 20110223314 IPC B05D 7/00 20060101 B05D 007/00, B05C 3/02 20060101 B05C 003/02; B05C 11/00 20060101 B05C 011/00; B05D 1/18 20060101 B05D 001/18; B05D 3/02 20060101 B05D 003/02; B05D 3/06 20060101 B05D 003/06 dated 03/10/2011 US describes a method for producing microcapsules by suspension polymerization, which belongs to the group of chemical methods using a new device and ultraviolet radiation.

The disadvantage of this method is the complexity and duration of the process, the use of special equipment, the use of ultraviolet radiation.

In US Pat. WO / 2011/150138 US IPC C11D 3/37; B01J 3/08; C11D 17/00, published 01.12.2011, describes a method for producing microcapsules of solid water-soluble agents by polymerization.

The disadvantages of this method are the complexity of execution and the duration of the process.

In US Pat. WO / 2011/104526 GB IPC B01J 3/00; B01J 13/14; С09В 67/00; C09D 11/02, published 01.09.2011, a method for producing a dispersion of encapsulated solid particles in a liquid medium is proposed, comprising: a) grinding a composition comprising solid, liquid media and polyurethane dispersants with an acid number from 0.55 to 3.5 mmol per gram dispersant, said composition comprises from 5 to 40 parts of a polyurethane dispersant per 100 parts of solid products, by weight; and b) crosslinking the polyurethane dispersant in the presence of a solid and liquid medium, as for the encapsulation of solid particles, which polyurethane dispersant contains less than 10% by weight of repeating elements from polymer alcohols.

The disadvantages of the proposed method are the complexity and duration of the process for producing microcapsules, as well as the fact that the encapsulated particles of the proposed method are useful as dyes in ink, especially inkjet inks, for the pharmaceutical industry this technique is not applicable.

In US Pat. WO / 2011/056935 US IPC C11D 17/00; A61K 8/11; B01J 13/02; C11D 3/50, published May 12, 2011, describes a method for producing microcapsules with a size of 15 microns or more. Polymers of the group consisting of polyethylene, polyamides, polystyrenes, polyisoprenes, polycarbonates, polyesters, polyacrylates, polyureas, polyurethanes, polyolefins, polysaccharides, epoxies, vinyl polymers and mixtures thereof are proposed as a shell material. The proposed polymer shells are sufficiently impervious to core material and materials in the environment in which the agents are encapsulated, the benefit will be used to provide the benefits that will be obtained. The core of encapsulated agents may include perfumes, silicone oils, waxes, hydrocarbons, higher fatty acids, essential oils, lipids, skin cooling fluids, vitamins, sunscreens, antioxidants, glycerin, catalysts, bleaching particles, particles of silicon dioxide, etc.

The disadvantages of the proposed method are the complexity, duration of the process, the use as shells of microcapsules of polymers of synthetic origin and their mixtures.

In US Pat. WO / 2011/160733 EP IPC B01J 13/16, published December 29, 2011, describes a method for producing microcapsules that contain shells and cores of water-insoluble materials. An aqueous solution of a protective colloid and a solution of a mixture of at least two structurally different bifunctional diisocyanates (A) and (B) insoluble in water are collected together until an emulsion is formed, then added to a mixture of bifunctional amines and heated to a temperature of at least 60 ° C until microcapsules are formed.

The disadvantages of the proposed method are the complexity, duration of the process, the use as shells of microcapsules of polymers of synthetic origin and their mixtures.

The closest method is the method proposed in US Pat. 2134967 IPC A01N 53/00, A01N 25/28, published 08/27/1999, Russian Federation (1999). A solution of a mixture of natural lipids and a pyrethroid insecticide in a weight ratio of 2-4: 1 in an organic solvent is dispersed in water, which simplifies the microencapsulation method.

The disadvantage of this method is dispersion in an aqueous medium, which makes the proposed method inapplicable for producing microcapsules of water-soluble preparations in water-soluble polymers.

The technical task is to simplify and accelerate the process of obtaining nanocapsules of ciprofloxacin hydrochloride in sodium alginate, reduce losses in the production of nanocapsules (increase in yield by mass).

The solution of the technical problem is achieved by the method of producing nanocapsules of ciprofloxacin hydrochloride, characterized in that sodium alginate is used as the shell of the nanocapsules, as well as the preparation of nanocapsules by the physicochemical precipitation method with a non-solvent using a precipitator - butyl chloride.

A distinctive feature of the proposed method is the use of sodium alginate antibiotics as a shell of nanocapsules, as well as the preparation of nanocapsules by the physicochemical method of precipitation with a non-solvent using a precipitator, butyl chloride.

The result of the proposed method is the preparation of ciprofloxacin hydrochloride nanocapsules in sodium alginate at 25 ° C for 15 minutes. The yield of nanocapsules is 100%.

EXAMPLE 1

 Obtaining nanocapsules of ciprofloxacin hydrochloride in sodium alginate, ratio of core: shell 1: 3

In a suspension of 1.5 g of sodium alginate in benzene and 0.01 g of the preparation E472c (glycerol ester with one or two molecules of food fatty acids and one or two molecules of citric acid, moreover, citric acid, as a tribasic, can be esterified with other glycerides and like oxoacid, other fatty acids. Free acid groups can be neutralized with sodium) as a surfactant, in small portions add 0.5 g of ciprofloxacin hydrochloride powder. Then 5 ml of butyl chloride are added dropwise. The resulting suspension of nanocapsules is filtered and dried.

Received 2 g of a white powder. The yield was 100%.

EXAMPLE 2

Obtaining nanocapsules of ciprofloxacin hydrochloride in sodium alginate, ratio of core: shell 1: 1

0.5 g of ciprofloxacin hydrochloride powder is added to a suspension of 0.5 g of sodium alginate in benzene and 0.01 g of the preparation as a surfactant. Then 5 ml of butyl chloride are added dropwise. The resulting suspension of nanocapsules is filtered and dried.

Received 1 g of a white powder. The yield was 100%.

EXAMPLE 3

Obtaining nanocapsules of ciprofloxacin hydrochloride in sodium alginate, ratio of core: shell 1: 5

To a suspension of 1.5 g of sodium alginate in benzene and 0.01 g of the preparation E472c as a surfactant, 0.3 g of ciprofloxacin hydrochloride powder is added. Then 5 ml of butyl chloride are added dropwise. The resulting suspension of nanocapsules is filtered and dried.

Received 1.8 g of a white powder. The yield was 100%.

EXAMPLE 4

Obtaining nanocapsules of ciprofloxacin hydrochloride in sodium alginate, ratio of core: shell 5: 1

To a suspension of 0.5 g of sodium alginate in benzene and 0.01 g of the preparation E472c as a surfactant, add 2.5 g of ciprofloxacin hydrochloride powder. Then 5 ml of butyl chloride are added dropwise. The resulting suspension of nanocapsules is filtered and dried.

Received 3 g of a white powder. The yield was 100%.

EXAMPLE 5

Sizing nanocapsules by NTA.

The measurements were carried out on a Nanosight LM0 multiparameter nanoparticle analyzer manufactured by Nanosight Ltd (Great Britain) in the HS-BF configuration (Andor Luca high-sensitivity video camera, 405 nm semiconductor laser with a power of 45 mW). The device is based on the Nanoparticle Tracking Analysis (NTA) method described in ASTM E2834.

The optimal dilution for dilution was 1: 100. For measurement, the device parameters were selected: Camera Level = 16, Detection Threshold = 10 (multi), Min Track Length: Auto, Min Expected Size: Auto, duration of a single measurement 215s, use of a syringe pump.

Claims (1)

A method of producing nanocapsules of ciprofloxacin hydrochloride in sodium alginate, characterized in that sodium alginate is used as the shell of the nanocapsules, and ciprofloxacin hydrochloride is used as the core, while ciprofloxacin hydrochloride powder is added to a suspension of sodium alginate in benzene containing 0.01 g of the preparation E472c in as a surfactant, butyl chloride is then added, the resulting suspension of nanocapsules is filtered and dried, the process is carried out at 25 ° C for 15 minutes.

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