NL2028709B1 - Process for preparing particles comprising an encapsulated lipid - Google Patents

Process for preparing particles comprising an encapsulated lipid Download PDF

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Publication number
NL2028709B1
NL2028709B1 NL2028709A NL2028709A NL2028709B1 NL 2028709 B1 NL2028709 B1 NL 2028709B1 NL 2028709 A NL2028709 A NL 2028709A NL 2028709 A NL2028709 A NL 2028709A NL 2028709 B1 NL2028709 B1 NL 2028709B1
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Prior art keywords
particle
shell
lipids
lipid
range
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NL2028709A
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Dutch (nl)
Inventor
De Bruijn Robin
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Stabican B V
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Priority to NL2028709A priority Critical patent/NL2028709B1/en
Priority to PCT/NL2022/050404 priority patent/WO2023287283A1/en
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Publication of NL2028709B1 publication Critical patent/NL2028709B1/en

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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/50Microcapsules having a gas, liquid or semi-solid filling; Solid microparticles or pellets surrounded by a distinct coating layer, e.g. coated microspheres, coated drug crystals
    • A61K9/5005Wall or coating material
    • A61K9/5015Organic compounds, e.g. fats, sugars
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/50Microcapsules having a gas, liquid or semi-solid filling; Solid microparticles or pellets surrounded by a distinct coating layer, e.g. coated microspheres, coated drug crystals
    • A61K9/5089Processes
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P21/00Drugs for disorders of the muscular or neuromuscular system
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P21/00Drugs for disorders of the muscular or neuromuscular system
    • A61P21/04Drugs for disorders of the muscular or neuromuscular system for myasthenia gravis
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • A61P25/06Antimigraine agents
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • A61P25/08Antiepileptics; Anticonvulsants
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • A61P25/26Psychostimulants, e.g. nicotine, cocaine

Abstract

The invention relates to a process for preparing particles comprising an encapsulated lipid, wherein first a solution is provided wherein the solvent has a water solubility in the range of 2—100 g/L at 25 °C and wherein the solution comprises 1) a lipid component comprising one or more lipids; and 2) a shellforming component comprising one or more compounds selected from the group of 010—030 fatty alcohols, 010—030 fatty acids and esters of 010—030 fatty alcohols and 010—030 fatty acids. Then, droplets of the solution are generated in an aqueous medium and the solvent is allowed to migrate from the droplets to the aqueous medium to thereby form solid particles wherein a shell of shellforming component encapsulates the lipid component.

Description

Process for preparing particles comprising an encapsulated lipid
FIELD OF THE INVENTION The present invention relates to a process for preparing particles comprising an encapsulated lipid, to a particle obtainable by such method and to a particle comprising an encapsulated lipid.
BACKGROUND Many pharmaceuticals, food supplements and other chemical compounds need to be provided in a form wherein they do not degrade until their consumption, and in a form that makes their, handling, dosing and administration convenient to e.g. a producer, a supplier and a consumer.
One method of doing so is to mix the substance with a filler material, to thereby provide a dosage composition with a particular amount of substance in it. In some cases, the substance is merely diluted in such filler so that there is substantial but no complete shielding from the atmosphere. In other cases, the substance is truly encapsulated by a protective shell. Present dosage compositions however still have some shortcomings.
For example, it is difficult to prepare dosage compositons in a reproducible way, in particular to include the same amounts of substance in each dosage composition. Especially for medical purposes, this is very important.
Another shortcoming is that many conventional dosage compositions as such are difficult to handle, for example because they cannot be obtained as a dry and easy to dose powder whilst also meeting the requirement of providing sufficient protection to the enclosed substance.
Yet another shortcoming is that the stability of conventional dosage forms is often insufficient. This is in particular encountered when it is desired to use the composition as a medicine, since this requires long shelf lives.
A difficulty that is often observed with terpenes is that they are volatile and therefore easily evaporate during processing and storage. For example, compositions comprising such volatile terpenes may release the terpenes over time. This results in a decreased terpene content of such compositions, which is undesired.
it can generally be stated that at present, dosage compositions of many substances are not available in a satisfactory form, e.g. a form that is convenient to handle and/or has a long shelf-life. In particular, there is a need for a standardized formulation comprising the substance, preferably in a powder form, as a way to enable consumers and patients to accurately and repeatably take the same dose of a pharmaceutical or food supplement to address their (medical) needs. At the same time, it is desired that the manufacturing of such formulation can be performed in a way that is easy, reliable and/or reproducible.
SUMMARY OF THE INVENTION It is therefore an object of the present invention to provide a formulation comprising a lipid that does not suffer from one or more of the abovementioned shortcomings.
It has now been found that a particular encapsulation method may overcome these shortcomings.
Accordingly, the invention relates to a process for preparing particles comprising an encapsulated lipid, the process comprising - providing a solution wherein the following components are dissolved in a solvent that has a water solubility in the range of 2-100 g/L at 25 °C: o a shell-forming component comprising one or more compounds selected from the group of C10-C30 fatty alcohols, C10-C30 fatty acids and esters of C10-C30 fatty alcohols and C10-C30 fatty acids; o a lipid component comprising one or more lipids that have the property that they do not form a single phase with the one or more compounds of the shell-forming component when they are mixed with the one or more compounds of the shell-forming component in a mass ratio of 50:50 at the temperature at which the process is carried out;
- generating droplets of the solution in an aqueous medium and allowing the solvent to migrate from the droplets to the aqueous medium to thereby form solid particles wherein a shell of shell-forming component encapsulates the lipid component. The invention also relates to a particle comprising an encapsulated lipid obtainable by such process. The invention also relates to a particle comprising an encapsulated lipid wherein - one or more lipids are encapsulated by a shell of one or more compounds selected from the group of C10-C30 fatty alcohols, C10-C30 fatty acids and esters of C10-C30 fatty alcohols and C10-C30 fatty acids; - the one or more lipids has the property that it does not form a single phase with the one or more compounds of the shell when it is mixed with the one or more compounds of the shell in a mass ratio of 1:1; - the content of the one or more lipids in the particle is in the range of 25-95 wt. % The invention also relates to a pharmaceutical composition comprising such a particle and a pharmaceutically acceptable excipient.
DETAILED DESCRIPTION OF THE INVENTION The invention relates to a process for preparing particles comprising an encapsulated lipid, the process comprising - providing a solution wherein the following components are dissolved in a solvent that has a water solubility in the range of 2-100 g/L at 25 °C: o a shell-forming component comprising one or more compounds selected from the group of C10-C30 fatty alcohols, C10-C30 fatty acids and esters of C10-C30 fatty alcohols and C10-C30 fatty acids; o a lipid component comprising one or more lipids; - generating droplets of the solution in an aqueous medium and allowing the solvent to migrate from the droplets to the aqueous medium to thereby form solid particles wherein a shell of shell-forming component encapsulates the lipid component.
Usually, the one or more lipids has the property that it does not form a single phase with the one or more compounds of the shell-forming component when it is mixed with the one or more compounds of the shell forming component in a mass ratio of 50:50 at the temperature at which the process is carried out.
The solvent has a solubility in water that is in the range of 2-100 g/L at 25 °C. This range on the one hand ensures that the solution of the lipid component and the shell-forming component in the solvent is capable of existing as droplets in a water phase; and on the other hand that the solvent migrates from the droplet to the water phase. For example, a solvent with a solubility higher than 100 g/L (including infinite solubility), will not form droplets, or only droplets with insufficient stability, so that the two water- insoluble components do not phase separate and solid particles are not formed. Also, a solvent with a solubility lower than 2 g/L (including complete insolubility) will nevertheless form droplets, but its migration from the droplets to the water phase, if any, cannot be accomplished under satisfying conditions.
The solubility of the solvent in water may also be in the range of 6-90 g/L at 25 °C, in the range of 8-80 g/L at 25 °C, in the range of 10-70 g/L at 25 °C, in the range of 12-60 g/L at 25 °C, or in the range of 15-50 g/L at 25 °C. It may also be in the range of 5-75 g/L at 25 °C, in the range of 8-50 g/L at °C or in the range of 10-40 g/L at 25 °C.
The solvent may be selected from the group of benzyl alcohol, 1-butanol, n-butyl acetate, gamma-butyrolacton, chloroform, 1,2- 25 dichloroethane, diethylene glycol, diethyl ether, diethoxyethane, di- isopropylether, ethyl acetate, methyl butyl ether, methylene chloride, N-methyl-2-pyrrolidinone, nitromethane, 1-pentanol, 2-pentanol, 3-pentanol, 3-pentanone, benzaldehyde, prenol, o-cresol, m-cresol, and p-cresol. The solvent may also be a terpenoid with a water solubility in the range of 2-100 g/L at 25 °C. In particular, the solvent is benzyl alcohol or methylene chloride.
The solvent usually has a molar mass of less than 200 g/mol. It is in particular less than 150 g/mol. It may also be less than 140 g/mol, less than 125 g/mol or less than 100 g/mol.
The solution in a process of the invention comprises a mixture of the two components that in the end make up the particles that comprise an encapsulated lipid. This means that both components are dissolved in the solvent. The migration of the solvent from the droplet to the aqueous medium 5 has the effect that both components come separately out of solution and gain their natural appearance, i.e. the appearance they normally have as a neat substance; the C10-C30 fatty acids, alcohols and ester are solid (or at least waxy), while the lipid is typically a solid or a liquid (such as an oil). Importantly, the solvent migration also results in the separation of both components, wherein the lipid component constitutes the inner part of the particles and the shell-forming component constitutes a shell that completely surrounds the lipid component. Usually, the solution consists of these two components and the solvent, i.e. no other dissolved or undissolved substances are present in the solution. It is however possible that certain additives are contained in the solution (preferably dissolved therein), which either end up in the produced particle or migrate together with the solvent. For example, an additional active pharmaceutical ingredient may be present. It is also possible that a co-solvent is present in the solution, which migrates together with the solvent (i.e. the primary solvent) out of the droplet (or particle) into the aqueous medium. For example, such co-solvent is a solvent selected from the group of the (primary) solvents mentioned above. In the solution, the weight ratio of lipid component to shell-forming component is usually in the range of 0.05 : 0.95 to 0.95 : 0.05. The ratio may also be in the range of 0.25 : 0.75 to 0.95 : 0.05, in particular in the range of
0.50 : 0.50 to 0.90 : 0.10. It may also be in the range of 0.40 : 0.60 to 0.80 :
0.20, or in the range of 0.60 : 0.40 to 0.95 : 0.05. With the method of the invention, it is possible to prepare particles in suspension (in particular a suspension in water) that are dry and not tacky. This is an important advantage of the method of the invention, since the dry form of the product makes the handling of the product convenient. Another advantage is that the lipids that are contained in the particles are surprisingly stable.
The lipid component comprises one or more lipids. It in particular consists of one or more lipids. The one or more lipids is preferably selected from the group of alkaloids, fat-soluble vitamins and terpenes.
In case the one or more lipids comprises an alkaloid, then the alkaloid is typically an alkaloid having a molecular structure comprising an N- heterocycle, i.e. a molecular structure wherein a nitrogen atom forms part of a heterocycle. By an N-heterocycle is meant a ring or ring structure that has one or more nitrogen atoms as members of the ring or ring structure. An alkaloid in a process of the invention for example comprises one or more N-heterocycles selected from the group of a pyrrolidine-based heterocycle, a tropane-based heterocycle, a pyrrolizidine-based heterocycle, a piperidine- based heterocycle, a quinolizidine-based heterocycle, an indolizidine-based heterocycle, a prydine-based heterocycle, an isoquinoline-based heterocycle, an oxazole-based heterocycle, an isoxazole-based heterocycle, a thiazole- based heterocycle, a quinazoline-based heterocycle, an acridine-based heterocycle, a quinoline-based heterocycle, an indole-based heterocycle, an imidazole-based heterocycle and a purine-based heterocycle.
The one or more lipids is in particular selected from the group of atropine, nicotine, morphine, psilocybine, psilocine, N,N-dialkyltryptamines such as N,N-dimethyltryptamine, bufotenin, baeocystin, aeruginascin, ergolines such as lysergic acid diethylamide (LSD) and lysergic acid amide (LSA), phenethylamines such as alpha-methyl-phenethylamines (amphetamines), and benzoxazines such as efavirenz. In case the one or more lipids comprises a fat-soluble vitamin, then the fat-soluble vitamin is typically selected from the group of vitamin A, vitamin D, vitamin E and vitamin K.
Vitamin A is known as a group of unsaturated nutritional organic compounds that includes retinol, retinal and several provitamin A carotenoids such as alpha-carotene, beta-carotene and beta-cryptoxanthin.
Vitamin D includes vitamin D2 (ergocalciferol) and vitamin Ds (cholecalciferol), Vitamin E is known as a group of eight nutritional organic compounds that include four tocopherols (alpha-tocopherol, beta-tocopherol, gamma-
tocopherol and delta-tocopherol) and four tocotrienols (alpha-tocotrienol, beta-tocotrienol, gamma-tocotrienol and delta-tocotrienol). Also derivatives of vitamin E may be applied in the present invention, for example acetates of vitamin E (alpha-tocoferylacetate, beta-tocoferylacetate, gamma-tocoferylacetate and delta-tocoferylacetate).
Vitamin K is the collective term for compounds that share a 2-methyl- 1,4-naphthoquinone ring, but differ in the side-chain at the 3-position. The main classes of vitamin K concern vitamin Ks (phylloquinone) and vitamin Kz (menaquinone). Vitamin Kz comprises a number of related chemical subtypes, such as menaquinone-4 (MK-4) and menaquinone-7 (MK-7). Another main vitamin K class concerns vitamin Ks (menadione), a synthetic form of vitamin K.
In case the one or more lipids comprises a terpene, then the terpene is typically selected from the group of alpha-bulnessene, beta-bulnessene, caryophyllene, farnesene, alpha-humulene, geraniol, alpha-guaiene, beta- guaiene, delta-guaiene, guaiol, limonene, linalool, myrcene, terpinolene, patchoulol, norpatchoulenol, alpha-patchoulene, beta-patchoulene, gamma-patchoulene, delta-patchoulene, alpha-pinene, beta-pinene, pogostol, seychellene, cycloseychellene, santalene, santalol and valencene.
A process according to the invention may be a process as claimed in claim 1, with the proviso that the one or more lipids does not comprise a cannabinoid. In this respect, a cannabinoid is understood to be a compound that naturally occurs in Cannabis plants such as Cannabis sativa, Cannabis indica or Cannabis ruderalis. Examples of a cannabinoid are delta-9- tetrahydrocannabinol, cannabidiol, cannabinol cannabigerol, tetrahydrocannabivarin, cannabidivarin, cannabichromene, delta-9- tetrahydrocannabinolic acid and cannabidiolic acid.
In a process of the invention, the one or more lipids to be encapsulated in principle has the property that, at the temperature at which the process of the invention is carried out, it does not form a single phase when it is mixed with the one or more compounds of the shell-forming component (i.e. with the one or more compounds selected from the group of C10-C30 fatty alcohols, C10-C30 fatty acids and esters of C10-C30 fatty alcohols and C10-C30 fatty acids) in a mass ratio of 50:50, e.g. when equal masses of both are mixed.
In particular, the one or more lipids to be encapsulated has the property that it does not form a single phase with the one or more compounds when it is mixed with the one or more compounds in a mass ratio in the range of 60:40 to 40:60, in a mass ratio in the range of 70:30 to 30:70, in a mass ratio in the range of 80:20 to 20:80, in a mass ratio in the range of 90:10 to 10:90 or in a mass ratio in the range of 95:5 to 5:95. The term ‘not forming a single phase’ includes the formation of two phases on the basis of non-miscibility (one phase does not dissolve in the other) as well as the formation of two phases on the basis of a different state of matter (e.g. a solid phase and a liquid phase). Further, the defintition that a particular first substance ‘does not form a single phase with a particular second substance at a particular temperature’ is to be viewed as a property of matter of the particular first substance as the neat substance (e.g. in pure form and not dissolved in any solvent), which property may be known from handbooks or which can be determined unambiguously by a person skilled in the art performing conventional procedures.
The shell-forming component contains the material from which the shell is formed.
The shell-forming component is mostly formed by the one or more compounds selected from the group of C10-C30 fatty alcohols, C10- C30 fatty acids and esters of C10-C30 fatty alcohols and C10-C30 fatty acids.
Usually, the one or more compounds makes 100% of the weight of the shell-forming component, i.e. the shell-forming component consists of the one or more compounds.
Optionally, the shell-forming component comprises one or more other compounds that also end up in the shell.
For example, any such other compound(s) makes up 10 wi% of the shell-forming component or less than that.
It may also make up 7 wit% or less, 5 wt.% or less, 3 wt.% or less, 2 wt.% or less, 1 wi.% or less or 0.5 wt.% or less.
So, the one or more compounds of the shell-forming component makes up at least 90 wt.%, at least 93 wi.%, at least 95 wt.%, at least 97 wt.%, at least 98 wt.%, at least 99 wt.% or at least 99.5 wt.% of the shell-forming component.
The C10-C30 fatty alcohol may be an alcohol selected from the group of capric alcohol, lauryl alcohol, myristyl alcohol, cetyl alcohol, palmitoleyl alcohol, stearyl alcohol, isosteary! alcohol, oleyl alcohol, elaidy! alcohol, petroselinyl alcohol, elaeosteary! alcohol, arachyl alcohol, gadoleyl alcohol, behenyl alcohol, erucyl alcohol and brassidyl alcohol.
The C10-C30 fatty acid may be an acid selected from the group of capric acid, lauric acid, palmitic acid, palmitoleic acid, stearic acid, isostearic acid, oleic acid, elaidic acid, petroselic acid, elaeostearic acid, arachic acid, gadoleic acid, behenic acid and erucic acid.
It may also be any of the abovementioned fatty acids with a branched chain, as long as the total number of carbons does not exceed 30.
The esters of C10-C30 fatty alcohols and C10-C30 fatty acids may also be composed of branched C10-C30 fatty alcohols and/or branched C10-C30 fatty acids.
In particular, the shell-forming component in the solvent comprises cetyl alcohol and/or cetyl palmitate.
In the process of the invention, droplets of the solution are generated in an aqueous medium. During the solvent migration, the droplets become the solid particles as the product of the process. The droplets are usually prepared by conventional methods, in particular by stirring. Vigorous stirring is typically applied to attain droplets that in the form particles with dimensions in the micrometer domain, in particular in the range of 2-500 um. A person skilled in the art can reach the appropriate conditions for this by routine experimentation and without exerting any inventive effort.
The temperature at which the process is performed (i.e. the operating temperature) may in principle be any temperature above the freezing point of water and below the boiling point of the solvent. For example, the temperature may be in the range 0-60 °C, in the range of 5-50 °C or in the range of 10-35 °C. Usually, however, the temperature is in the range of 15- 30 °C. In particular, it is in the range of 20-25 °C.
The invention further relates to a particle comprising an encapsulated lipid obtainable by the process described above.
A particle comprising an encapsulated lipid that is obtained by a process of the invention has a core of one or more lipids and a shell encapsulating this core. The shell compartimentalizes the one or more lipids and so protects them against influences from the outer environment such as micro-organisms or reactive compounds such as oxygen.
Accordingly, the invention further relates to a particle comprising an encapsulated lipid, wherein - One or more lipids are encapsulated by a shell of one or more compounds selected from the group of C10-C30 fatty alcohols, C10-C30 fatty acids and esters of C10-C30 fatty alcohols and C10-C30 fatty acids; - the content of the one or more lipids in the particle is in the range of 5-95 wt. %, in particular in the range of 25-85 wt.%. For the particle of the invention, the same considerations apply as those mentioned hereabove for the process of the invention, when the following is concerned: 1) the presence of the types of C10-C30 fatty alcohols; 2) the presence of the types of C10-C30 fatty acids; 3) the presence of the types of esters of C10-C30 fatty alcohols and C10-C30 fatty acids; 4) the presence of the types of terpenes.
Usually, the one or more lipids has the property that it does not form a single phase with the one or more compounds of the shell when it is mixed with the one or more compounds of the shell in a mass ratio of 1:1 at 25 °C, in particular a temperature in the range of 15-30 °C, more in particular a temperature in the range of 0-50 °C.
In particular, the one or more lipids has the property that it does not form a single phase with the one or more compounds when it is mixed with the one or more compounds in a mass ratio in the range of 60:40 to 40:60, in a mass ratio in the range of 70:30 to 30:70, in a mass ratio in the range of 80:20 to 20:80, in a mass ratio in the range of 90:10 to 10:90 or in a mass ratio in the range of 95:5 to 5:95.
Usually, the content of lipid in a particle of the invention is in the range of 20-80 wt. %, preferably it is in the range of 25-75 wt.%, more preferably it is in the range of 30-70 wt.% (the weight percentages are based on the total weight of the particle). Assuming no other constituents are present (in particular not encapsulated), it then follows that the shell constitutes 5-95 wt.% of the particle, in particular 15-75 wt.%. Usually, it is 20-80 wt.%, preferably 25-75 wt.%, more preferably 30-70 wt. %.
In similar disclosures of particles that comprise an encapsulated lipid, a wax is present as a filler material that forms an interpenetrating network between the lipd(s). In particles with such composition, a plurality of lipid domains is present. The wax then remains tacky due to such morphology. In contrast, a particle of the invention in principle comprises one domain, namely the core of the particle.
It has been demonstrated that the lipid in a particle of the invention is stable during a periode of at least 13 months, which is (beside the non- tackyness) also an effect of the excellent shielding that is provided by the process of the invention.
In a particle of the invention, the one or more lipids in particular comprises an alkaloid. In an embodiment, the one or more lipids is selected from the group of atropine, nicotine, morphine, psilocybine, psilocine, N,N- dialkyltryptamines such as N,N-dimethyltryptamine, bufotenin, baeocystin, aeruginascin, ergolines such as lysergic acid diethylamide (LSD) and lysergic acid amide (LSA), phenethylamines such as alpha-methyl-phenethylamines (amphetamines), and benzoxazines such as efavirenz.
In a particle of the invention, the one or more lipids may also or alternatively comprise a terpene, for example a terpene is typically selected from the group of alpha-bulnessene, beta-buinessene, caryophyllene, farnesene, alpha-humulene, geraniol, alpha-guaiene, beta-guaiene, delta- guaiene, guaiol, limonene, linalool, myrcene, terpinolene, patchoulol, norpatchoulenol, alpha-patchoulene, beta-patchoulene, gamma-patchoulene, delta-patchoulene, alpha-pinene, beta-pinene, pogostol, seychellene, cycloseychellene, santalene, santalol and valencene.
In a particle of the invention, the one or more lipids may also or alternatively comprise a fat-soluble vitamin, for example a fat-soluble vitamin typically selected from the group of vitamin A, vitamin D, vitamin E and vitamin K.
In a particle of the invention, the weight ratio of lipid to shell is typically in the range of 0.25 : 0.75 to 0.95 : 0.05. It may also be 0.50 : 0.50 to
0.90 : 0.10, in the range of 0.40 : 0.60 to 0.80 : 0.20, or in the range of 0.60 :
0.40 to 0.95 : 0.05. This ratio is reflected by the ratio of lipid component to shell-forming component in the solution that is used for preparing the particle. A particle of the invention is usually globular. This shape is governed by the shape of the initial droplet in the process of the invention, which is usually globular. The diameter of a particle of the invention is usually in the range of 100 nm-500 um, in particular in the range of 250 nm—400 um, more in particular in the range of 1-250 um, even more in particular in the range of 3- 100 um or yet even more in particular in the range of 5-50 um. For example, it is 200 nm or more, 300 nm or more, 400 nm or more, 500 nm or more, 750 nm or more, 1 um or more, 2 um or more, 3 um or more, 4 um or more, 5 um or more, 6 um or more, 7 um or more, 8 um or more, 9 um or more, 10 um or more, 12 um or more, 14 um or more, 20 um or more, 30 um or more, 40 um or more, 50 um or more, 75 um or more, 100 um or more, 200 um or more, 300 um or more, or 400 um or more. It may also be 500 um or less, 400 um or less, 300 um or less, 200 um or less, 100 um or less, 75 um or less, 70 um or less, 25 um or less, 20 um or less, 15 um or less, 10 um or less, 8 um or less, 7 um or less, 6 um or less, 5 um or less, 4 um or less, 3 um or less, 2 um or less, 1 um or less, 800 nm or less, 600 nm or less, 400 nm or less or 200 nm or less. The shell of a particle of the invention is mostly composed of the one or more compounds selected from the group of C10-C30 fatty alcohols, C10- C30 fatty acids and esters of C10-C30 fatty alcohols and C10-C30 fatty acids. In a preferred embodiment, the one or more compounds makes up 100% of the weight of the shell, i.e. the shell then consists of the one or more compounds. Optionally, the shell comprises one or more other compounds. For example, any such other compound(s) makes up 10 wi% of the shell or less than that. It may also make up 7 wt% or less, 5 wt.% or less, 3 wt.% or less, 2 wt.% or less, 1 wt.% or less or 0.5 wi.% or less. So, the one or more compounds of the shell makes up at least 90 wt.%, at least 93 wt.%, at least
95 wt.%, at least 97 wt.%, at least 98 wt.%, at least 99 wt.% or at least 99.5 wt.% of the shell.
The invention further relates to a pharmaceutical composition comprising a particle comprising an encapsulated lipid as described above and an excipient.
The term excipient as used herein refers to any substance, generally pharmaceutically inert, used to formulate active pharmaceutical ingredients (API) into pharmaceutical formulations. For example, an excipient is selected from the group of diluents, binders, glidants, lubricants, colouring agents and disintegrants. The excipient material itself may be composed of one or more materials selected from the group of sugar alcohols, polyols (e.g. sorbitol, mannitol, xylitol), crystalline sugars, monosaccharides (e.g. glucose, arabinose), disaccharides (e.g. maltose, saccharose, dextrose, lactose), oligosaccharides (e.g. dextrins, cyclodextrins), polysaccharides (e.g. cellulose starch and derivatives thereof), inorganic salts (e.g. sodium chloride, calcium carbonate, magnesium carbonate, talc), and organic salts (e.g. sodium lactate, magnesium stearate).
The invention further relates to a particle comprising an encapsulated lipid as described above or a pharmaceutical composition as described above for use as a medicament.
The invention further relates to a particle comprising an encapsulated lipid as described above or a pharmaceutical composition as described above, wherein the one or more lipids comprises an alkaloid, in particular an alkaloid selected from the group of atropine, nicotine, morphine, psilocybine, psilocine, N‚N-dialkyltryptamines such as N‚N-dimethyltryptamine, bufotenin, baeocystin, aeruginascin, ergolines such as lysergic acid diethylamide (LSD) and lysergic acid amide (LSA), and benzoxazines such as efavirenz, for use in the treatment of a neurological disorder.
Such neurological disorder is in particular a neurological disorder selected from the group of acute spinal cord injury, Alzheimer's disease, amyotrophic lateral sclerosis (ALS), ataxia, bell's palsy, brain tumors, cerebral aneurysm, epilepsy and, seizures, Guillain-Barré syndrome, headache, head injury, hydrocephalus, lumbar disk disease (herniated disk), meningitis,
multiple sclerosis, muscular dystrophy, neurocutaneous syndromes, Parkinson's disease, stroke (brain attack), cluster headaches, tension headaches, migraine headaches, encephalitis, septicemia, types of muscular dystrophy and neuromuscular diseases, and myasthenia gravis.
For a particular medical use or treatment, such as any of the treatments mentioned above, the particle is a delayed release composition for the release of one or more lipids in for example the small intestine or the large intestine. In the context of the present invention, delayed release means that the composition releases the one or more encapsulated lipids after passing through the stomach. In particular, a delayed release composition of the invention releases the one or more encapsulated lipids in the distal small intestine. Preferably, no dissolution of the composition occurs in the stomach The invention further relates to a method for treating a medical condition of a human or an animal, comprising administering to the human or animal an effective amount of a particle comprising an encapsulated lipid or of a pharmaceutical composition as described above.
As used herein, the term "effective amount” means that amount of a drug or pharmaceutical agent that will elicit the biological or medical response of an animal or human that is being sought, for instance, by a researcher or clinician.
The invention further relates to the use of a particle comprising an encapsulated lipid or a pharmaceutical composition as described above for treating a human or an animal.
The invention further relates to the use of a particle comprising an encapsulated lipid or a pharmaceutical composition as described above for the manufacture of a medicament for the treatment of a medical condition.
The term medical condition as used herein is a broad term that includes all diseases, lesions, disorders, or nonpathologic condition that normally receives medical treatment, such as pregnancy or childbirth.

Claims (24)

CONCLUSIESCONCLUSIONS 1. Werkwijze voor het bereiden van deeltjes omvattende een omhuld lipide, omvattende - het verschaffen van een oplossing waarbij de volgende componenten zijn opgelost in een oplosmiddel met een wateroplosbaarheid in het bereik van 2-100 g/L bij 25 °C: o een schilvormende component omvattende een of meer verbindingen gekozen uit de groep van C10-C30 vetalcoholen, C10-C30 vetzuren en esters van C10-C30 vetalcoholen en C10-C30 vetzuren; o een lipidecomponent omvattende een of meer lipiden die de eigenschap hebben dat ze niet een enkele fase vormen met de een of meer verbindingen van de schilvormende component wanneer ze gemengd worden met de een of meer verbindingen van de schilvormende component in een massaverhouding van 1:1 bij de temperatuur waarop de werkwijze wordt uitgevoerd; - het genereren van druppels van de oplossing in een waterig medium en het oplosmiddel laten migreren van de druppels naar het waterig medium om daardoor vaste deeltjes te vormen waarbij een schil van de schilvormende component de lipidecomponent omhult.Method for preparing particles comprising an enveloped lipid, comprising - providing a solution wherein the following components are dissolved in a solvent with a water solubility in the range of 2-100 g/L at 25°C: o a shell-forming component comprising one or more compounds selected from the group of C10-C30 fatty alcohols, C10-C30 fatty acids and esters of C10-C30 fatty alcohols and C10-C30 fatty acids; o a lipid component comprising one or more lipids which have the property of not forming a single phase with the one or more compounds of the shell-forming component when mixed with the one or more compounds of the shell-forming component in a mass ratio of 1:1 at the temperature at which the process is carried out; - generating droplets of the solution in an aqueous medium and allowing the solvent to migrate from the droplets to the aqueous medium thereby forming solid particles wherein a shell of the shell-forming component encapsulates the lipid component. 2. Werkwijze volgens conclusie 1, waarbij de een of meer lipiden is geselecteerd uit de groep van alkaloïden, vetoplosbare vitamines en terpenen.The method according to claim 1, wherein the one or more lipids is selected from the group of alkaloids, fat-soluble vitamins and terpenes. 3. Werkwijze volgens conclusie 2, waarbij de een of meer lipiden een alkaloïde omvat met een moleculaire structuur die een N-heteroring omvat.The method of claim 2, wherein the one or more lipids comprises an alkaloid having a molecular structure comprising an N-heterocycle. 4. Werkwijze volgens conclusie 1, waarbij de een of meer lipiden is geselecteerd uit de groep van atropine, nicotine, morfine, psilocybine, psilocine, N‚N- dialkyltryptamines zoals N,N-dimethyltryptamine, bufotenine, baeocystine, aeruginascine, ergolines zoals lyserginezuur diethylamide (LSD) en lyserginezuur amide (LSA), fenethylamines zoals alfa-methyl-fenethylamines (amfetamines), en benzoxazines zoals efavirenz.4. The method of claim 1, wherein the one or more lipids is selected from the group of atropine, nicotine, morphine, psilocybin, psilocine, N,N-dialkyltryptamines such as N,N-dimethyltryptamine, bufotenine, baeocystin, aeruginascine, ergolines such as lysergic acid diethylamide (LSD) and lysergic acid amide (LSA), phenethylamines such as alpha-methyl-phenethylamines (amphetamines), and benzoxazines such as efavirenz. 5. Werkwijze volgens conclusie 2, waarbij de een of meer lipiden een vetoplosbaar vitamine omvat gekozen uit de groep van vitamine A, vitamine D, vitamine E en vitamine K.The method of claim 2, wherein the one or more lipids comprises a fat-soluble vitamin selected from the group consisting of vitamin A, vitamin D, vitamin E and vitamin K. 6. Werkwijze volgens conclusie 2, waarbij de een of meer lipiden een terpeen omvat gekozen uit de groep van alfa-buinesseen, beta-buinesseen, caryophylieen, farneseen, alfa-humuleen, geraniol, alfa-guaieen, beta- guaieen, delta-guaieen, guaiol, limoneen, linalool, myrceen, terpinoleen, patchoulol, norpatchoulenol, alfa-patchouleen, beta-patchouleen, gamma-patchouleen, delta-patchouleen, alfa-pineen, beta-pineen, pogostol, seychelleen, cycloseychelleen, santaleen, santalol en valenceen.The method of claim 2, wherein the one or more lipids comprises a terpene selected from the group of alpha-buinessene, beta-buinessene, caryophyllene, farnesene, alpha-humulene, geraniol, alpha-guaiene, beta-guaiene, delta-guaiene , guaiol, limonene, linalool, myrcene, terpinolene, patchoulol, norpatchoulenol, alpha-patchoulene, beta-patchoulene, gamma-patchoulene, delta-patchoulene, alpha-pinene, beta-pinene, pogostol, seychellene, cycloseychellene, santalene, santalol, and valencene . 7. Werkwijze volgens een der conclusies 1-6, met dien verstande dat de een of meer lipiden niet een cannabinoïde omvat.The method according to any one of claims 1-6, provided that the one or more lipids does not comprise a cannabinoid. 8. Werkwijze volgens een der conclusies 1-7, waarbij het oplosmiddel is geselecteerd uit de groep van 1-butanol, n-butyl acetaat, gamma-butyrolacton, chloroform, 1,2-dichloorethaan, diethyleenglycol, diethylether, diethoxyethaan, di-isopropylether, dimethyisulfoxide, ethylacetaat, methyl-f-butylether, N-methyl-2-pyrrolidinon, nitromethaan, 1-pentanol, 2-pentanol, 3-pentanol, 3-pentanon, benzaldehyde, prenol, o-cresol, m-cresol, en p-cresol.A method according to any one of claims 1-7, wherein the solvent is selected from the group consisting of 1-butanol, n-butyl acetate, gamma-butyrolactone, chloroform, 1,2-dichloroethane, diethylene glycol, diethyl ether, diethoxyethane, di-isopropyl ether , dimethyl sulfoxide, ethyl acetate, methyl f-butyl ether, N-methyl-2-pyrrolidinone, nitromethane, 1-pentanol, 2-pentanol, 3-pentanol, 3-pentanone, benzaldehyde, prenol, o-cresol, m-cresol, and p-cresol. 9. Werkwijze volgens een der conclusies 1-8, waarbij het oplosmiddel benzylaicohol of methyleenchloride is.A method according to any one of claims 1 to 8, wherein the solvent is benzyl alcohol or methylene chloride. 10. Werkwijze volgens een der conclusies 1-9, waarbij het oplosmiddel een wateroplosbaarheid heeft in het bereik van 8-80 g/L bij 25 °C, in het bijzonder in het bereik van 10-40 g/L bij 25 °C.A method according to any one of claims 1-9, wherein the solvent has a water solubility in the range of 8-80 g/L at 25°C, in particular in the range of 10-40 g/L at 25°C. 11. Werkwijze volgens een der conclusies 1-10, waarbij de schilvormende component cetylalcohol en/of cetylpalmitaat omvat.A method according to any one of claims 1-10, wherein the shell-forming component comprises cetyl alcohol and/or cetyl palmitate. 12. Werkwijze volgens een der conclusies 1-11, waarbij de gewichtsverhouding van lipidecomponent tot schilvormende component in de oplossing in het bereik ligt van 0.25 : 0.75 tot en met 0.95 : 0.05, in het bijzonder in het bereik van 0.55 : 0.45 tot en met 0.75 : 0.25.A method according to any one of claims 1-11, wherein the weight ratio of lipid component to shell-forming component in the solution is in the range from 0.25 : 0.75 to 0.95 : 0.05, in particular in the range from 0.55 : 0.45 to 0.75 : 0.25. 13. Deeltje omvattende een omhuld lipide verkrijgbaar met een werkwijze volgens een der conclusies 1-12.A particle comprising an encapsulated lipid obtainable by a method according to any one of claims 1-12. 14. Deeltje omvattende een omhuld lipide, waarbij - een of meer lipiden omhuld zijn door een schil van een of meer verbindingen gekozen uit de groep van C10-C30 vetalcoholen, C10-C30 vetzuren en esters van C10-C30 vetalcoholen en C10-C30 vetzuren; - de een of meer lipiden de eigenschap heeft dat het niet een enkele fase vormt met de een of meer verbindingen van de schil wanneer het gemengd wordt met de een of meer verbindingen van de schil in een massaverhouding van 1:1; - het gehalte van de een of meer lipiden in het deeltje in het bereik ligt van 25-95 gew.%.14. Particle comprising an enveloped lipid, wherein - one or more lipids are enveloped by a shell of one or more compounds selected from the group of C10-C30 fatty alcohols, C10-C30 fatty acids and esters of C10-C30 fatty alcohols and C10-C30 fatty acids ; - the lipid(s) has the property that it does not form a single phase with the shell compound(s) when mixed with the shell compound(s) in a mass ratio of 1:1; - the content of the one or more lipids in the particle is in the range of 25-95% by weight. 15. Deeltje omvattende een omhuld lipide volgens conclusie 13 of 14, waarbij de schil in hoofdzaak vrij is van de een of meer lipiden, in het bijzonder vrij van alkaloïden, vetoplosbare vitamines en terpenen.A particle comprising an enveloped lipid according to claim 13 or 14, wherein the shell is substantially free of the one or more lipids, in particular free of alkaloids, fat-soluble vitamins and terpenes. 16. Deeltje omvattende een omhuld lipide volgens een der conclusies 13-15, waarbij de gewichtsverhouding van de een of meer lipiden tot schil in het bereik ligt van 0.50 : 0.50 tot en met 0.90 : 0.10 of in het bereik van 0.60 : 0.40 tot en met 0.95 : 0.05.A particle comprising an enveloped lipid according to any one of claims 13-15, wherein the weight ratio of the lipid(s) to shell is in the range of 0.50 : 0.50 to 0.90 : 0.10 or in the range of 0.60 : 0.40 to with 0.95 : 0.05. 17. Deeltje omvattende een omhuld lipide volgens een der conclusies 13-16, waarbij het deeltje een diameter heeft in het bereik van 100 nm-500 um, in het bijzonder in het bereik van 1-50 um.A particle comprising an enveloped lipid according to any one of claims 13-16, wherein the particle has a diameter in the range of 100 nm-500 µm, in particular in the range of 1-50 µm. 18. Deeltje omvattende een omhuld lipide volgens een der conclusies 13-17, met dien verstande dat de een of meer lipiden niet een cannabinoïde omvat.A particle comprising an enveloped lipid according to any one of claims 13-17, provided that the one or more lipids does not comprise a cannabinoid. 19. Farmaceutische samenstelling omvattende een deeltje omvattende een omhuld lipide volgens een der conclusies 13-18 en een excipiéns.A pharmaceutical composition comprising a particle comprising an encapsulated lipid according to any one of claims 13-18 and an excipient. 20. Deeltje omvattende een omhuld lipide volgens een der conclusies 13-18 of een farmaceutische samenstelling volgens conclusie 19 voor gebruik als een medicament.A particle comprising an encapsulated lipid according to any one of claims 13-18 or a pharmaceutical composition according to claim 19 for use as a medicament. 21. Deelije volgens een der conclusies 13-18 of een farmaceutische samenstelling volgens conclusie 19, waarbij de een of meer lipiden is geselecteerd uit de groep van atropine, nicotine, morfine, psilocybine, psilocine, N‚N-dialkyliryptamines zoals N‚N-dimethyltryptamine, bufotenine, baeocystine, aeruginascine, ergolines zoals lyserginezuur diethylamide (LSD) en lyserginezuur amide (LSA), fenethylamines zoals alfa-methyl- fenethylamines (amfetamines), en benzoxazines zoals efavirenz, voor gebruik in de behandeling van neurologische stoornissen.21. Part according to any one of claims 13-18 or a pharmaceutical composition according to claim 19, wherein the one or more lipids is selected from the group of atropine, nicotine, morphine, psilocybin, psilocin, N,N-dialkyliryptamines such as N,N- dimethyltryptamine, bufotenine, baeocystin, aeruginascine, ergolines such as lysergic acid diethylamide (LSD) and lysergic acid amide (LSA), phenethylamines such as alpha-methylphenethylamines (amphetamines), and benzoxazines such as efavirenz, for use in the treatment of neurological disorders. 22. Deeltje of farmaceutische samenstelling voor gebruik volgens conclusie 21, waarbij de neurologische stoornis een neurologische stoornis is geselecteerd uit de groep van acute dwarslaesie, ziekte van Alzheimer, amyotrofische laterale sclerose (ALS), ataxie, aangezichtsverlamming van Bell, hersentumoren, cerebraal aneurysma, epilepsie en toevallen, Guillain-Barré- syndroom, hoofdpijn, hoofdletsel, hydrocephalus, lumbale schijfziekte (hernia), meningitis, multiple sclerose, spierdystrofie, neurocutane syndromen, ziekte van Parkinson, beroerte (hersenaanval), clusterhoofdpijnen, spanningshoofdpijnen, migrainehoofdpijnen, encefalitis, bloedvergiftiging, soorten spierdystrofie en neuromusculaire ziekten, en myasthenia gravis.The particle or pharmaceutical composition for use according to claim 21, wherein the neurological disorder is a neurological disorder selected from the group of acute spinal cord injury, Alzheimer's disease, amyotrophic lateral sclerosis (ALS), ataxia, Bell's facial palsy, brain tumors, cerebral aneurysm, epilepsy and seizures, Guillain-Barré syndrome, headache, head injury, hydrocephalus, lumbar disc disease (herniated disc), meningitis, multiple sclerosis, muscular dystrophy, neurocutaneous syndromes, Parkinson's disease, stroke (brain attack), cluster headaches, tension headaches, migraine headaches, encephalitis, septicemia , types of muscular dystrophy and neuromuscular diseases, and myasthenia gravis. 23. Deeltje of farmaceutische samenstelling voor gebruik volgens conclusie 22, waarbij het deeltje of de samenstelling, respectievelijk, een vertraagde afgifte samenstelling is voor de afgifte van een of meer lipiden in de dunne darm en/of de dikke darm.A particle or pharmaceutical composition for use according to claim 22, wherein the particle or composition, respectively, is a sustained release composition for the release of one or more lipids in the small intestine and/or the large intestine. 24. Werkwijze voor het behandelen van een medische toestand van een mens of een dier, omvattende het toedienen aan het mens of dier van een effectieve hoeveelheid van een deeltje omvattende een omhuld lipide volgens één der conclusies 13-18 of een farmaceutische samenstelling volgens conclusie 19.A method of treating a medical condition of a human or an animal comprising administering to the human or animal an effective amount of a particle comprising an encapsulated lipid according to any one of claims 13-18 or a pharmaceutical composition according to claim 19 .
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US20190000763A1 (en) * 2015-08-06 2019-01-03 Pratibha Pilgaonkar Particulate delivery systems

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* Cited by examiner, † Cited by third party
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US20190000763A1 (en) * 2015-08-06 2019-01-03 Pratibha Pilgaonkar Particulate delivery systems

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Title
BANERJEE SUROJIT ET AL: "Lipids for Taste masking and Taste assessment in pharmaceutical formulations", CHEMISTRY AND PHYSICS OF LIPIDS, LIMERICK, IR, vol. 235, 19 December 2020 (2020-12-19), XP086504604, ISSN: 0009-3084, [retrieved on 20201219], DOI: 10.1016/J.CHEMPHYSLIP.2020.105031 *

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