WO2017168426A1 - Compositions and methods for selective gi tract delivery - Google Patents
Compositions and methods for selective gi tract delivery Download PDFInfo
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- WO2017168426A1 WO2017168426A1 PCT/IL2017/050394 IL2017050394W WO2017168426A1 WO 2017168426 A1 WO2017168426 A1 WO 2017168426A1 IL 2017050394 W IL2017050394 W IL 2017050394W WO 2017168426 A1 WO2017168426 A1 WO 2017168426A1
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Definitions
- the present invention relates, in some embodiments thereof, to compositions and methods of using same for selective delivery of active ingredients in the gastrointestinal (GI) tract.
- Controlled release systems for a delivery of active agents are often designed to administer drugs and other active agents to specific areas of the body.
- the agent In the gastrointestinal tract, it is important that the agent will not be eliminated or become materially not bioactive during its passage in the different digestive conditions of the GI tract, and maintain sufficient bioavailability before it can exert a localized effect or to pass into the bloodstream.
- Enteric coated formulations e.g. formulations with non or minimal release of an active ingredient prior to encountering the digestive conditions of the distal small intestines
- enteric coated formulations have been widely used for many years to protect drugs or other biologically active agents administered orally, as well as to delay release.
- microsphere formulations have been proposed as a means for oral drug delivery. These enteric coated formulations are primarily in the form of dry formulations (e.g. delivered in the form of tablets, capsules, etc.).
- WO 2006/039022 discloses a composite formulation being developed for selective, high efficacy delivery to specific regions of the mouth and gastrointestinal tract.
- the formulation in WO 2006/039022 is typically in the form of a tablet or capsule (e.g. maintained in a dry form until consumption), which may include microparticles or beads, where the drug is absorbed in enhanced amounts in the small intestines relative to a formulation absent of the bioadhesive and/or controlled release elements.
- active agent e.g., drug, active or dietary supplement
- the present invention relates, inter alia, to a composition which can be used to selectively deliver active agent(s) (e.g., pharmaceutical and natural APIs and other active ingredients) in the gastro-intestinal (GI) tract.
- active agent(s) e.g., pharmaceutical and natural APIs and other active ingredients
- a composition as described herein targets a specific location and/or region within the GI tract.
- composition comprising at least one microparticle, wherein the microparticle is in the form of a core- shell, and wherein: the core comprises:
- the shell comprises one or more water-insoluble and enzymatically-degradable ingredients, wherein the weight ratio of the active agent and the sum of (b) ranges from 1:1,000 to 10: 1.
- the shell further comprises (i) at least one pH-triggered ingredient or (ii) at least one enteric ingredient.
- the active agent is water-soluble.
- the active agent is water-insoluble.
- the active agent is selected from the group consisting of: pharmaceutical APIs, active ingredients, nutraceuticals, food supplements, food additives, herbals, plant extracts, medicaments, homeopathic agents, and any combination thereof.
- the shell comprises two or more layers, wherein each layer comprises a different composition. In some embodiments, the shell further comprises one or more active agents.
- the composition comprises pH-triggered ingredient or an enteric ingredient, and the enzymatically-degradable ingredient.
- a weight ratio of the at least one active agent and the shell ranges from 100: 1 to 1: 100.
- the composition comprises a plurality of microparticles.
- each microparticle is characterized by different core and shell properties.
- the composition further comprises a liquid.
- the liquid is selected from the group consisting of: water, alcohol, and any combination thereof.
- the alcohol is selected from ethanol and methanol or a mixture thereof.
- the active agents are encapsulated and selected from the group consisting of Sugar, Fructose, Glucose, Carbohydrates, Betaine, Choline, Bi vitamins, Vitamin C, Vitamin D, Vitamin E, Coenzyme A, Cysteine/N-Acetyl-L- cysteine, Carnitine, Kudzu (Puerarin), Huperzia (Huperzine), Guarana (Caffeine, Theophylline), Alpha lipoic acid, Curcuma Longa (Curcumin), Piper Longum (Piperine), Astaxanthin, Quercetin, Resveratrol, Ginkgo Biloba (Bilobalide and Ginkgolides), Ginseng (Ginsenosides), Bacopa Monnieri (Bacosides), Ginger (Gingerols, Shogalos), Butterbur (Petasins), Feverfew (Parthenolides), White Willow Bark (Salicin/S
- the composition comprises one or more non-encapsulated active agents.
- the non-encapsulated active agents are selected from Sugar, Fructose, Glucose, Carbohydrates, Betaine, Choline, Bi vitamins, Vitamin C, Vitamin D, Vitamin E, Coenzyme A, Cysteine/N-Acetyl-L-cysteine, Carnitine, Kudzu (Puerarin), Huperzia (Huperzine), Guarana (Caffeine, Theophylline), Alpha lipoic acid, Curcuma Longa (Curcumin), Piper Longum (Piperin), Astaxanthin, Quercetin, Resveratrol, Ginkgo Biloba (Bilobalide and Ginkgolides), Ginseng (Ginsenosides), Bacopa Monnieri (Bacosides), Ginger (Gingerols, Shogalos), Butterbur (Petasins), Feverfew (Parthenolides), White Willow Bark (Salicin/Salicylic acid
- the liquid further comprises a surfactant.
- the microparticles are dispersed in the liquid.
- the liquid further comprises one or more non- encapsulated supplementary ingredients such as flavoring agents.
- the composition is characterized by pH below 7. In some embodiments, the pH is below 4.
- the enteric ingredients comprise a water soluble or water insoluble polymeric material selected from the group consisting of: hydroxypropylmethyl cellulose phthalate, hydroxypropylmethyl cellulose acetate succinate, methacrylic acid-methyl methacrylate copolymer, ethyl methacrylate-methyl methacrylate-chloro-trimethylammonium ethyl methacrylate copolymer, cellulose acetate phthalate, cellulose propionate phthalate, cellulose acetate maleate, polyvinyl acetate phthalate, polyvinyl alcohol phthalate, styrene-acrylic acid copolymer, methyl acrylate-methacrylic acid copolymer, or a water-soluble ingredient consisting of acetyl cellulose, methyl cellulose, hydroxypropyl cellulose, hydroxypropylmethyl cellulose, carboxymethyl cellulose, hydroxypropyl methylcellulose (HPMC), HPMPC, Car
- the shell comprises one or more materials selected from: HPMC, HPMPC, Carbomers, PEGs, Prolamin proteins (Zein, Gluten, Kafirin, etc.), Shellacs, fats (Coconut oil, Palm oil, Carnauba wax, Stearic acid, Sunflower oil), Gelatin, Soy proteins, Pea proteins (Globulin), Vegetable proteins, Starches, Dextran, Maltodextrin, Cyclodextrin, Whey, Casein, Guar gum, gum Arabic, Pectin, Amylose, Chitosans, Alginates, Hydrogels, HMPC, HPMPC, PVA, PEGs, Carbomers, Polymethacrylate, Ethyl Cellulose and Methyl Cellulose.
- HPMC HPMPC
- Carbomers Polymethacrylate, Ethyl Cellulose and Methyl Cellulose.
- a dimension of the microparticle is characterized by a diameter of 1 to 300 microns. In some embodiments, the dimension of the microparticle is characterized by a diameter of 10 to 100 microns. In some embodiments, the dimension of the microparticle is characterized by a diameter of 25 to75 microns.
- the composition is formulated for at least one dissolution trigger and/or one selective release profile in a GI tract.
- the selective release is within a time limit, temperature threshold, pH threshold, ionic strength, or enzymatic activity, or any combination thereof.
- the composition is in the form of: powder, a beverage, shake, foam, capsule, a tablet, a bar or a gel.
- the composition is characterized by a sigmoidal pattern of controlled release of at least one active agent within a gastrointestinal (GI) tract.
- GI gastrointestinal
- At least two microparticles from a plurality of the microparticles are characterized by having a different dissolution trigger and/or a different sigmoidal pattern of controlled release of the active agent in the GI tract.
- kits for oral administration comprising:
- GI gastrointestinal
- the disclosed composition is for oral administration.
- a method for treating an acute, transient or chronic disorder comprising administrating the disclosed composition to an individual.
- the disclosed composition is specifically formulated for controlled release of the at least one active agent in a specific region of the gastrointestinal (GI) tract of a subject.
- GI gastrointestinal
- the process comprises:
- the one or more enzymatically-degradable and/or water- insoluble ingredients are in amount that ranges from 1% to 99%, by total weight of the core solution.
- the organic solvent is selected from the group consisting of pharma-grade solvents and food-grade solvents, including, but not limited to: ethanol, methanol, acetone, and any combination thereof.
- FIGs 1 A-C illustrates typical dissolution graphs of gastric target release showing the release profile of Vitamin B5 ( Figure 1A), Calcium Pyruvate ( Figure IB), and of Kudzu ( Figure 1C).
- FIG 2 is a graph showing typical enteric release profiles of the active agent (Kudzu).
- FIG 3 is a graph showing the release profile of the active agent (Kudzu) when Zein protein, an encapsulation ingredient subject to enzymatic triggering and disintegration, was used to prevent the release of the active agent disclosed in the microparticle when reconstructed into an acidic liquid formula which is absent of enzymatic triggering conditions.
- FIG 4 is a graph showing the release profile of the active agent (Kudzu) when the microparticles have the core (Kudzu/Shellac 1% + Zein 4%) with no shell protection.
- FIG 5 is a graph showing the release profile of the active agent (Kudzu) when the microparticles have a core component with the enteric ingredient (Kudzu/Shellac 1% + Ethocel 10%) without incorporating an enzymatic -degradable ingredient.
- FIG 6 is a graph showing the release profile of the active agent (Kudzu) when the formulation was produced in an open-loop system spray dryer with a reverse coating approach.
- the present invention relates, inter alia, to a composition which can be used to selectively deliver active agent(s) (e.g., APIs and other active ingredients) in the gastrointestinal (GI) tract.
- active agent(s) e.g., APIs and other active ingredients
- a composition as described herein is selectively targeted to or targets a specific location and/or region within the GI tract.
- a composition as described herein selectively targets multiple or specific locations, regions and/or triggers within the GI tract, as described hereinbelow.
- Non-limiting exemplary locations and/or regions within the GI tract are selected from mouth, stomach, duodenum, jejunum, ileum, cecum, colon and any combination thereof.
- the disclosed composition may be manufactured via spray drying with a three fluid or four fluid or five fluid injectors, or via a combination of spray drying followed by fluidized bed, or via a fluidized bed.
- Injectors with multiple fluid and gas channels may incorporate more than a single fluid nozzle and are capable of generating, in a single step, a core component containing the active ingredient or a matrix containing the active ingredient surrounded by at least one layer of a coating shell made from, for example and without limitation, cellulose derivatives, proteins, methacrylates, phthalates and any other coating materials known in the food and/or pharmaceutical industry.
- the final microencapsulated product may be in the form of a powder that is dispersed into a non-dry delivery composition/environment, e.g., an acidic liquid beverage, shake, a gel or any other forms of non-dry vehicles known in the art.
- a non-dry delivery composition/environment e.g., an acidic liquid beverage, shake, a gel or any other forms of non-dry vehicles known in the art.
- the microencapsulated powder may be water-insoluble and may include a high dose of active ingredients where at least one of the active ingredients is poorly water-soluble, parameters that optimize particles dispersion, active agent loading within the particle, and minimize of a negative mouth sensation (organoleptic) of the microencapsulated powder are selected.
- microcapsules with different coatings which isolate (in contrast to e.g., mask) the odors and the flavors of active ingredients with unpleasant tastes and odors.
- Such microcapsules also enable loading of an effective amount of active ingredients when dispersed in a liquid unit of e.g., from several milliliters to several hundreds of milliliters, in a drink, beverage, shake, a gel or in other non-dry delivery forms e.g., as described herein.
- microencapsulation at the selected particle size/diameter may also be selected so as to minimize or negate the gritty oral sensation often accompanied with consumption of suspended or dispersed powders in no-dry delivery systems.
- gritty oral sensation of a dispersed powder in a drink, beverage, a shake or a gel is a major obstacle for obtaining a satisfactory positive consumption experience by the user.
- the present invention's microencapsulation approaches were designed for the purpose of selectively releasing different active ingredients (e.g., APIs, other actives and/or dietary supplements) throughout the GI tract (as described in the Examples section which follows).
- active ingredients e.g., APIs, other actives and/or dietary supplements
- composition comprising at least one microparticle, wherein the at least one microparticle is in the form of a heterostructure.
- the heterostructure is in the form of a matrix, core-shell or core-shell structure (also referred to as "encapsulated particles").
- the microparticle can be generally shaped as a sphere, a rod, a cylinder, a ribbon, a sponge, and any other shape, or can be in the form of a cluster or an aggregate of any of these shapes, or can comprise a mixture of one or more shapes.
- the core comprises at least one active agent and at least one from (i), (ii) and (iii):
- the composition comprises (i).
- the composition comprises (ii).
- the composition comprises (iii).
- the composition comprises (i) and (ii). In some embodiments, the composition comprises (ii) and (iii). In some embodiments, the composition comprises (i) and (iii). In some embodiments, the composition comprises (i), (ii), and (iii). In some embodiments, the composition comprises two of (i) to (iii).
- the shell comprises one or more ingredients being characterized as enzymatically-degradable, enteric and/or as water-insoluble ingredients. [080] In some embodiments, the shell further comprises one or more active agents described hereinthroughout.
- the shell comprises one or more ingredients being enteric ingredients.
- the enteric ingredients are also enzymatically-degradable ingredients.
- the enteric ingredients are not enzymatically-degradable ingredients.
- core-shell structure generally refers to a solid material, wherein the solid material is a particulate material, and wherein individual particle(s) is characterized by containing at least two different types of materials which may be distinguished from one another by their shape, by their diameter, by their composition, by their structure and/or by their placement within the particle, wherein one or more materials of a certain type are contained in the interior portion of the particles.
- the interior portion is designated by the term “core” or “matrix” or “inner matrix”.
- One or more materials of a certain type which may be distinguished from the one or more materials contained in the interior portion are contained in the outer portion of the particles.
- the outer portion comprising the surface is designated by the terms “shell” or “coating layer” or "encapsulation layer”.
- the core-shell structure is a closed structure.
- closed is a relative term with respect to the size, the shape and the particle or composition of two entities, namely an entity that defines an enclosure (the enclosing entity) and the entity that is being at least partially enclosed therein.
- the term “closed” refers to a morphological state of an object which has a discrete inner (e.g., the core) and outer surfaces which are substantially disconnected, wherein the inner surface constitutes the boundary of the enclosed area.
- the enclosed area may be at least partially secluded from the exterior area of space.
- the shell and/or the core is designed to prevent the release of foul-tasting and/or water insoluble and/or water soluble ingredients (e.g., active agents) into the non-dry delivery composition/environment (e.g., a liquid, drink, beverage, shake, gel, or other non-dry delivery system) for a sufficient time period for a common individual or consumer to completely consume e.g., a 1 - 10 ml, 10 - 100 ml, or 300 - 500 ml or 500 - 1,000 ml serving.
- the non-dry delivery composition/environment e.g., a liquid, drink, beverage, shake, gel, or other non-dry delivery system
- sufficient time period it is meant to refer to at least e.g., 1 min, 5 min, 10 min, 15 min, 20 min, 30 min, 40 min, 50 min 60 min, 90 min, 120 min, 180 min, 240 min, 300 min, 360 min, 420 min, 480 min or 600 min, 720 min, 1 day, 7 days, 14 days, 30 days, 60 days, 90 days, 180 days or 365 days, including any value therebetween.
- liquid may refer to any liquid suitable for human consumption, including, without being limited thereto, water, juice, milk, tea, and alcohol.
- microparticle describes a particle featuring a size of at least one dimension thereof (e.g., diameter, length) that ranges from about 1 micrometer to 1,000 micrometers (microns). In some embodiments, the particle's size ranges from 1 to 300 microns. In some embodiments, the particle's size ranges from 10 to 200 microns. In some embodiments, the particle's size ranges from 30 to 100 microns, e.g., 30 ⁇ , 40 ⁇ , 50 ⁇ , 60 ⁇ , 70 ⁇ , 80 ⁇ , 90 ⁇ , 100 ⁇ , including any value and range therebetween.
- composition comprising at least one microparticle, wherein the microparticle is in the form of a matrix, as demonstrated e.g., in Figure 4, and wherein: the matrix comprises:
- the active agent in the matrix is water-soluble.
- the active agent in the matrix is water-insoluble.
- the active agent in the matrix is selected from pharmaceutical APIs, active ingredients, nutraceuticals, food supplements, food additives, herbals, plant extracts, medicaments, homeopathic agents, and any combination thereof.
- the composition comprises pH-triggered ingredient or an enteric ingredient, and the enzymatically-degradable ingredient.
- the advantages of the disclosed technological approach is that in given optimal parameters (e.g., very small particles) the size / diameter of the particles are below the sensory threshold in an oral cavity.
- sensor threshold it is meant to refer to the weakest stimulus that an organism can detect. That is, if the stimulus falls below the threshold, the subject does not experience it.
- an existence of a plurality of the disclosed microsized particles dispersed in a non-dry delivery system/environment is below the sensory threshold of the tongue (dictated by e.g., bumps on the tongue called fungiform papillae) and all other locations in the oral cavity and the pharynx capable of sensing a particle, and is therefore not sensed by a subject as particles.
- a non-dry delivery system/environment e.g., a liquid, a drink, a beverage, a shake, a gel or any other non-dry delivery system
- the bulk density (gr/ml) of the microparticles is from 0.1 to 0.9, including any value therebetween. In some embodiments, the bulk density of the microparticles is from 0.2 to 0.8. In some embodiments, the bulk density of the microparticles is from 0.3 to 0.7, including any density value therebetween. In some embodiments, the bulk density of the microparticles is from 0.4 to 0.6 including any density value therebetween.
- the size of the particle described herein represents an average or a median size of a plurality of microparticles.
- the average or median size ranges from about 1 micrometer to 500 micrometers. In some embodiments, the average or median size ranges from about 1 micrometer to about 300 micrometers. In some embodiments, the average or median size ranges from about 1 micrometer to about 200 micrometers. In some embodiments, the average or median size ranges from about 1 micrometer to about 100 micrometers.
- the average or median size is about 1 ⁇ , about 2 ⁇ , about 3 ⁇ , about 4 ⁇ , about 5 ⁇ , about 6 ⁇ , about 7 ⁇ , about 8 ⁇ , about 9 ⁇ , about 10 ⁇ , about 11 ⁇ , about 12 ⁇ , about 13 ⁇ , about 14 ⁇ , about 15 ⁇ , about 16 ⁇ , about 17 ⁇ , about 18 ⁇ , about 19 ⁇ , about 20 ⁇ , about 21 ⁇ , about 22 ⁇ , about 23 ⁇ , about 24 ⁇ , about 25 ⁇ , about 26 ⁇ , about 27 ⁇ , about 28 ⁇ , about 29 ⁇ , about 30 ⁇ , about 31 ⁇ , about 32 ⁇ , about 33 ⁇ , about 34 ⁇ , about 35 ⁇ , about 36 ⁇ , about 37 ⁇ , about 38 ⁇ , about 40 ⁇ , about 42 ⁇ , about 44 ⁇ , about 46 ⁇ , about 48 ⁇ , 50 ⁇ , about 60 ⁇ , about 70 ⁇ , about 80 ⁇ , about 90 ⁇ , about 100
- the matrix or shell comprises one or more ingredients which are insoluble in liquid without the presence of enzymes and/or specific pH conditions.
- the matrix or shell comprises one or a combination of ingredients being characterized as e.g., enzymatically-degradable and/or pH- degradable.
- the enzymatically-degradable ingredients are selected from the group consisting of polyethylene glycol, enzymatically degradable peptides and enzymatically degradable proteins, and, synthetic polymers.
- the polymers are selected from poly(ethylene oxide) (PEO), poly (ethylene glycol) (PEG) and copolymers with poly(propylene oxide) (PEG- co-PPG), polyvinyl alcohol) (PVA), poly(vinylpyrrolidone) (PVP), poly(ethyloxazoline) (PEOX), polyaminoacids, and pseudopoly amino acids, and copolymers of these polymers.
- the one or more ingredients are not soluble in water (also referred to as: "water-insoluble”).
- water-insoluble it is meant that the K sp of the ingredient (or agent) in water is below 10 "10 , or in another embodiment below 10 “9 , or in another embodiment below 10 s , at least 10 "7 , or in another embodiment below 10 "6 , or in another embodiment below 10-5, or in another embodiment below 10 "4 , or in another embodiment below 10 "3 , or in another embodiment below 10 "2 , or in another embodiment below 10 "1 .
- each microparticle can include more than one coating/encapsulation layer.
- the shell comprises two or more layers, (e.g., 2, 3, 4, or 5 layers).
- each layer comprises a different ingredient or at least one different ingredient.
- the term "different" refers to different dis solvability profile of each ingredient so as to allow e.g., obtaining stepwise release profiles of the active agent(s).
- the term "enzymatically-degradable” is intended to mean that the stated ingredient is capable of being cleaved or digested, either partially or extensively, by enzymes present in different sections of the GI tract.
- enzymes present in different sections of the GI tract.
- polyamino-acids, lipids, fats, proteins, polysaccharides, carbohydrates and nucleotides are usually enzymatically degradable.
- an enzymatically-degradable ingredient in the core, matrix or in the shell is degradable by only a specific enzyme present in a specific GI location (e.g., mouth, stomach, duodenum, jejunum, ilium, secum or the colon).
- a specific GI location e.g., mouth, stomach, duodenum, jejunum, ilium, secum or the colon.
- an enzymatically-degradable ingredient in the core, matrix and/or in the shell is degradable by a specific enzyme present in more than one specific GI location.
- an enzymatically-degradable ingredient in the core, matrix and/or the shell is degradable by a more than one enzyme presents in more than one specific GI location.
- the core, matrix and/or the shell incorporate at least one ingredient that is both water-insoluble and enzymatically-degradable.
- a weight ratio of the active agents and a total of (i), (ii) and (iii) as defined hereinabove is within the range of from 1 : 1 ,000 to 50: 1 , for example, 1:1,000, 1:900, 1:800, 1:700, 1:600, 1:500, 1:400, 1:300, 1:200, 1: 100, 1:50, 1:40, 1:30, 1:20, 1: 10, 1: 1, 2: 1, 3: 1, 4: 1 5: 1, 10:1, 20: 1 30: 1, 40: 1 or 50: 1 including any value or range therebetween.
- the core, matrix and/or the shell further comprise one or more enteric ingredients.
- the shell comprises one or more enteric ingredients, which are absent in the core.
- the term "enteric ingredient” refers to a barrier (e.g., a polymeric barrier) applied to any orally-delivered medication or other active or dietary supplement, that prevents its dissolution or disintegration in the oral and/or in one or more proximal sites / regions in the gastric environment (e.g. the mouth, the esophagus, the stomach and the proximal part of the small intestines).
- a barrier e.g., a polymeric barrier
- any orally-delivered medication or other active or dietary supplement that prevents its dissolution or disintegration in the oral and/or in one or more proximal sites / regions in the gastric environment (e.g. the mouth, the esophagus, the stomach and the proximal part of the small intestines).
- the enteric material is a polymer, e.g., cellulose or a derivative thereof (e.g., ethyl cellulose, hydroxypropylcellulose (HPC)).
- the enteric ingredient is characterized by pH (between pH 4.5 - pH 7.6) dependent solubility. In some embodiments, the enteric ingredient is characterized by non-pH dependent solubility. In some embodiments, the enteric ingredient is not susceptible to enzymatic degradation. In some embodiments, the enteric ingredient is characterized by water/liquid swellability.
- enteric ingredient further encompasses a reversed enteric material, e.g., a material characterized by increased solubility at low (e.g., acidic) pH than at higher pH.
- a reversed enteric material e.g., Zein protein.
- Non-limiting examples of enteric ingredients or materials are one or more polymeric materials selected from the group consisting of: hydroxypropylmethyl cellulose phthalate, hydroxypropylmethyl cellulose acetate succinate, methacrylic acid- methyl methacrylate copolymer, ethyl methacrylate-methyl methacrylate-chloro- trimethylammonium ethyl methacrylate copolymer, cellulose acetate phthalate, cellulose propionate phthalate, cellulose acetate maleate, polyvinyl acetate phthalate, polyvinyl alcohol phthalate, styrene-acrylic acid copolymer, methyl acrylate- methacrylic acid copolymer, or a water-soluble ingredient consisting of cellulose or a derivative thereof, acetyl cellulose, methyl cellulose, hydroxypropyl cellulose, hydroxypropylmethyl cellulose, carboxymethyl cellulose, (Hydroxypropyl)methyl cellulose (
- an active agent is administered, for example, to treat a temporary, transient or acute disease state or physiological condition, such as a disorder, an imbalance or a nutritional deficiency.
- active agent is understood to include chemical, biological, dietary, nutritional or pharmaceutical entities including any natural or synthetic chemical or biological substance.
- Typical active entities include, but are not limited to, active pharmaceutical ingredients, antibodies, antigens, biological materials, chemical materials, chromatogenic compounds, contrasting agents, drugs, enzymes, fluorescent probes, immunogenes, indicators, ligands, nucleic acids, nutrients, peptides, physiological media, proteins, fats, lipids, oils, carbohydrates, amino acids, selective toxins, and toxins.
- the active agent is selected from, but is not limited to, the group consisting of nutraceuticals, food supplements, food additives, plant extracts, medicaments, herbals, homeopathic agents, and any combination thereof.
- the active agent is a dietary supplement or a specific active molecule within a dietary supplement.
- dietary supplement refers to a product taken orally that contains an ingredient that is intended to supplement an individual's diet and is not considered food (i.e. are not typically an energy source).
- a dietary supplement may be a vitamin, a mineral, herb or other botanical or extract thereof, one or more amino acids, one or more proteins, one or more lipids, or any other non-food substance capable of supplementing a diet.
- the active agent is encapsulated as discussed hereinabove (e.g., is a part of the core of the disclosed microparticle).
- Non-limiting exemplary encapsulated active agents are selected from, without being limited thereto, Cysteine/N-Acetyl-L-cysteine, Kudzu (Puerarin), Huperzia (Huperzine), Guarana (Caffeine, Theophylline), Alpha lipoic acid, Curcuma Longa (Curcumin), Piper Longum (Piperin), Quercetin, Resveratrol and Ginseng (Ginsenosides), Bacopa Monnieri (Bacosides), Ginger (Gingerols, Shogalos), White Willow Bark (Salicin/Salicylic acid), Cannabidiol and Grape seed (Proanthocyanidins) or any combination thereof.
- the composition further comprises one or more active agents which are not encapsulated.
- Non-limiting exemplary non-encapsulated active agents are dietary supplements, such as Vitamin B, Vitamin C, Magnesium salt, Zinc salt, Carnitine/Acetyl-L-carnitine, Pyruvate salt, Cysteine, N-Acetyl-L-cysteine, Kudzu (Puerarin), Huperzia (Huperzine) and Guarana (Caffeine, Theophylline), or any combination thereof.
- Non-limiting exemplary dietary supplements which, in some embodiments, may be encapsulated, include, but are not limited to, Alpha Lipoic Acid, Folic acid, Vitamin B l, Vitamin B2, Vitamin B3, Vitamin B5, Vitamin B6, Vitamin B7, Vitamin B9, Vitamin B 12, Vitamin D, Vitamin E, Glutathione, Carnitine/ Acetyl-L-Carnitine, Cysteine/N-Acetyl-L-Cysteine, Copper salt, Selenium salt, Magnesium salt, Zinc salt, Pyruvate salt, Co-enzyme A, Curcumin, Piperin, Quercetin, Resveratrol, Sesamin, Sulforaphane, Astaxanthin, Lemon (Limonene), Grape seed (Proanthocyanidins), Huperzia (Huperzine), Hovenia Dulcis (Dihydromyricetin), Pueraria Lobata (Puerarin), Ginseng (Ginsenosides), Ginkgo
- exemplary dietary supplements which, in some embodiments, are partially encapsulated and partially not encapsulated include, but are not limited to, Fructose, Glucose, Betaine (TMG), Choline salt, Lemon powder, Citric acid, Sucralose, Caramel, Thickener (e.g., 7HOF), Gum Arabic, Silicon dioxide, Betaine (TMG), SAMe, Choline salt, Creatine, Fructose, Glucose, Vitamin D, Vitamin E, Glutathione, Copper salt, Selenium salt, Co-enzyme A, Sesamin, Sulforaphane, Astaxanthin, Lemon (Limonene), Ginkgo Biloba (Bilobalide, Bacopa Monnieri (Bacosides), Amentoflavone, Ginkgolides), Feverfew (Parthenolides) and Mango (Mangiferin).
- vitamin B it is meant to refer to vitamin B 1, vitamin B2, vitamin B3, vitamin B5, vitamin B6, vitamin B7, vitamin B9, vitamin B 12, or any combination thereof. In some embodiments, by “vitamin B” it is meant to refer to vitamin B complex.
- non- encapsulated active agents may be encapsulated, in some embodiments.
- the active agent is water-soluble.
- water-soluble describes a substance which is capable of forming a homogeneous mixture in water.
- the homogeneous mixture may be a solution, in which the substance dissolves in water.
- the active agent is highly soluble in water.
- the active agent when the active agent is highly soluble in water (for example, vitamin B6), it "leaks" into the non-dry (e.g., liquid) medium (e.g., beverage, shake, gel, etc.).
- the non-dry (e.g., liquid) medium e.g., beverage, shake, gel, etc.
- a shell incorporating more than one encapsulation agent/layer may be desired.
- the active agent is partially soluble in water.
- the active agent is non-soluble in water.
- water-soluble refers to a substance which is materially not water-insoluble, as defined herein above.
- water- solubility is characterized by at least 5 weight percent, at least 10 weight percent, at least 20 weight percent or at least 25 weight percent.
- water-solubility refers to the maximal concentration of a substance in water, at which the substance is water-soluble.
- the at least one active agent and the shell are in a weight ratio that ranges from 1 :20 to 20: 1.
- the weight ratio is 1 :20, 1: 15, 1:10, 1:5, 1:3, 1:2, 1: 1, including any value and range therebetween.
- the composition comprises a plurality of the disclosed microparticle (also referred to as "microparticles", for simplicity).
- microparticles are generally shaped as spheres.
- microparticles have an average size that varies within +20 %.
- At least 10 %, 20 %, 30 %, 40 %, 50 %, 60 %, 70 %, 80 %, 90 %, 95 %, 98 %, 99%, 99.9 %, or all of the microparticles have an average size that varies within +30 %.
- At least 10 %, 20 %, 30 %, 40 %, 50 %, 60 %, 70 %, 80 %, 90 %, 95 %, 98 %, 99%, 99.9 %, or all of the microparticles have an average size that varies within +40 %.
- the present composition can include more than one type of a microparticle in e.g., a single powdered product.
- Different types of microparticles can include different matrices (e.g., different active ingredient in a core without a shell/coating), different cores (i.e. different active ingredient in a matrix with at least one additional ingredient) and/or a different type of shells/coatings (facilitating selective release of more than one active ingredient).
- the disclosed microparticle may comprise different active agents each being characterized by a different solubility profile in water, fluid, digestive fluid or any other liquid.
- the active agent desired to be delivered to the lower gastrointestinal tract region has a selective trigger and/or release profile in the lower gastrointestinal tract.
- the active agent is desired to be delivered to upper gastrointestinal tract has a selective trigger and/or release profile in the upper gastrointestinal tract.
- the selective release is triggered by an environmental trigger, as described hereinbelow under Bioactivity of the Composition.
- a single powdered unit dose may include:
- Each microparticle may have minimal release of the active agent in a liquid.
- Each microparticle may have a core with at least one active ingredient.
- unit dose may refer to a physically discrete unit containing a predetermined quantity of an active material calculated to individually or collectively produce a desired effect.
- a single unit dose or a plurality of unit doses can be used to provide the desired effect, such as recovery effect and/or therapeutic effect.
- the active agent of the core may be mononuclear, multi-nuclear or incorporated in a slow-release or controlled release or sustained release matrix.
- the core may also incorporate intestinal permeability enhancing agents.
- the plurality of microparticle comprises microparticles which have the same or different active agent, e.g., at least 1%, 5%, 10%, 20%, 30%, 40%, 50 %, 60 %, 70 %, 80 %, 90 %, 95 %, 98 %, 99%, 99.9 %, or all of the microparticles have the same active agent.
- the composition is the solid form.
- the composition is in the form of a powder. In some embodiments, the composition is in the form of a capsule. In some embodiments, the composition is in the form of a tablet. In some embodiments, the composition is in the form of a health / sports bar.
- Non-dry Composition Form
- the disclosed composition has a non-dry form, i.e. comprises a liquid (e.g., 1% or more, by weight).
- the composition is in the semi-solid form.
- solid may refer to a material that is a mixture of liquid and solid phases, for example, such as particle suspension, colloidal suspension, emulsion, dispersion, gel, or micelle.
- the disclosed composition comprises e.g., at least 0.1%, 0.5%, 1%, 2%, 5%, 10%, 20%, 30%, 40%, 50%, 60%, 70%, 80%, 90%, 95%, or 99% by weight or by volume, of liquid, including any value therebetween.
- the microparticles in the liquid are in the range of from 0.01% to 99% (w/w or v/v). In some embodiments, the microparticles in the liquid are in the range of from 0.25% to 50% (w/w or v/v). In some embodiments, the microparticles in the liquid are in the range of from 0.50% to 33% (w/w or v/v). In some embodiments, the microparticles in the liquid are in the range of from 1% to 20% (w/w or v/v).
- the microparticles in the liquid are 1% , 2%, 3%, 4%, 5%, 6%, 7%, 8%, 9%, 10%, 11%, 12%, 13%, 14%, 15%, 16%, 17%, 18%, 19% or 20% (w/w or v/v), including any value or range therebetween.
- the microparticles are dispersed in the liquid.
- the liquid further comprises one or more supplementary ingredients.
- the supplementary ingredients comprise one or more non- encapsulated active agents, flavor ingredients, or any combination thereof.
- Non-limiting exemplary supplementary ingredients include sweeteners such as aspartame, sodium saccharin, saccharin, stevia, glycyrrhizin, potassium acesulfame; acidulants such as citric acid, tartaric acid and malic acid; flavoring such as menthol, peppermint oil, peppermint, orange, lemon-lime, lemon and strawberry; and colorants such as caramel, annatto extract pigment, ⁇ -carotene and beet red.
- the composition is in the form of a gel.
- beverage refers to a substantially aqueous drinkable composition suitable for human or other mammal consumption.
- the beverage comprises at least 85% water by weight of the beverage, or at least 90% or from 95% to 99.9% water, by weight.
- gel as used herein is well accepted in the art, describes a semisolid composition for oral consumption. This term further encompasses compositions including a solid network that encages a liquid phase therewithin.
- the shell layer further comprises one or more flavor ingredients.
- one or more flavor ingredients and the non-encapsulated active agents are dispersed and/or dissolved in the liquid
- the disclosed encapsulated microparticles are inert or materially inert in terms of flavor and/or odor as a dispersed suspension in the liquid, (e.g., drink, beverage, gel, or foam) and pass through the mouth and esophagus without substantially releasing its contents.
- the liquid e.g., drink, beverage, gel, or foam
- substantially releasing it is intended to mean releasing of e.g., no more than 33%, no more than 25%, no more than 20%, no more than 15%, no more than 10%, no more than 5% or no more than 1%, including any value in between.
- the liquid is water. In some embodiments, the liquid is alcohol. In some embodiments, the liquid comprises water and ethanol. In some embodiments, the liquid is any liquid approved for human consumption other than water or alcohol.
- the composition is in the form of a non-dry formulation.
- the composition is in the form of a beverage. In some embodiments, the composition is in the form of a shake. In some embodiments, the beverage is a gel. In some embodiments, the beverage is foam. In some embodiments, the beverage is a ready-to-consume drink. In some embodiments, in order to provide a reasonable shelf-life for the ready-to-consume drink version, more than a single encapsulation coating in the shell layer is required, as described hereinabove.
- the liquid is substantially devoid of liquid other than water. In some embodiments, the liquid is substantially devoid of a liquid other than water or alcohol.
- the liquid further comprises one or more ingredients selected from, but are not limited to, colorants, thickeners, flavoring agents, stabilizers and the like.
- the liquid comprising water and ethanol comprises e.g., 1%, 10%, 20%, 30%, 40%, 50%, 60%, 70%, 80%, or 90% alcohol, including any value or range therebetween.
- the alcohol is ethanol. In some embodiments, the alcohol is methanol.
- the microparticles are dispersed in the liquid medium. In some embodiments, the microparticles are suspended in the liquid medium.
- the microparticles when the encapsulated microparticles are reconstructed into a liquid-based or liquid-containing composition, the microparticles are suspended in the liquid and are homogenously distributed therein (e.g., not materially floating at the surface of the liquid and not materially settling at the bottom of the container).
- the disclosed microparticles are capable of maintaining their capacity to disperse and re-disperse in the liquid-containing medium.
- the terms "disperse”, “dispersive” or any grammatical derivative thereof refer to the tendency of a particulate matter not to become or stay as agglomerates, clumps or chunks of mass, but rather become and/or regain a state of discrete, non-aggregated free particles.
- "dispersing” further refers to the act of crumbling, breaking apart or otherwise separating the microparticles which have formed clumps, soft agglomerates and soft aggregates back into the un-clumped particle.
- the term "suspension”, or any grammatical derivative thereof, as used herein, refers to a heterogeneous mixture of a solid in fine solute-like microparticles dispersed in a liquid or solvent-like phase.
- a suspension will have a tendency to settle, namely the fine particles of the solid matter may have the tendency to precipitate after a period of time. This period of time may depend on many factors, such as the substances of the microparticles and the liquid, the temperature and other physical parameters like stirring and shaking, and the presence of other substances, such as dispersing agents, emulsifiers, surface-active agents, thickeners and the likes.
- the term "suspension” as used herein is similar to the term dispersion, with the proviso that the media is a condense medium, typically a liquid.
- a suspension may be a collection of discrete and separated particles dispersed in a liquid-based medium.
- the capacity to re-disperse is applicable also in a liquid-based media, namely the capacity to re-suspend, or go from a precipitant to a suspension reversibly and reproducibly.
- the composition is in the form of dispersion, or as suspension of the disclosed microparticles in liquid or liquid-containing medium.
- the liquid-based medium further comprises one or more surface-active agents, also referred to as "surfactant”.
- the term "surfactant”, as used herein, refers to an acceptable material which imparts emulsifiability, stability, spreading, wetting, dispersibility or other surface-modifying properties.
- the surfactant is selected from, but is not limited to, cationic surfactants, anionic surfactants, non-ionic surfactants, amphoteric surfactants, and zwitterionic surfactants.
- Non-limiting exemplary surfactants are Sodium dodecyl sulfate (SDS) and Polyvinylpyrrolidone (PVP), fatty substances (e.g., lecithin), a cholic acid or a derivative thereof, and bioavailability enhancers (e.g., D -a- Tocopherol polyethylene glycol succinate, TPGS).
- SDS Sodium dodecyl sulfate
- PVP Polyvinylpyrrolidone
- fatty substances e.g., lecithin
- a cholic acid or a derivative thereof e.g., a cholic acid or a derivative thereof
- bioavailability enhancers e.g., D -a- Tocopherol polyethylene glycol succinate, TPGS.
- the disclosed composition in the form of dispersion or suspension (e.g., a beverage, a drink, a shake, a gel, a foam or any other non-dry delivery media) is characterized by a defined pH, where such defined pH prevents or materially prevents premature dissolution and release of the microencapsulated actives into the non-dry media.
- pH refers to the quantitative measure of the acidity or alkalinity (basicity) of liquid solutions or dispersions.
- the pH of the non-dry composition is below 7. In some embodiments, the pH of the non-dry composition is below 5. In some embodiments, the pH of the non-dry composition is 2, 3, 4, 5, 6, or 7, including any value or range therebetween.
- the pH refers to the pH of the non-dry composition. In some embodiments, the pH refers to mouth pH. In some embodiments, the pH refers to esophagus pH. In some embodiments, the pH refers to stomach pH. In some embodiments, the pH refers to duodenum pH. In some embodiments, the pH refers to jejunum pH. In some embodiments, the pH refers to ilium pH. In some embodiments, the pH refers to colon pH.
- the desired value of pH is set by an addition of an acid (e.g., HC1) or a base (e.g., NaOH), or a salt thereof, to the liquid, or to a powder comprising the microparticles.
- an acid e.g., HC1
- a base e.g., NaOH
- the composition begins to release its active ingredients (in a selective and controlled manner) in the stomach and/or in a selected region of the small intestines and/or in the colon, depending on the properties of the core or matrix, the properties of the coating layer or layers, the ratio between the core or matrix and the coating layer or layers (w/w or v/v) and the (w/w or v/v) ratio between the shell material and active agents.
- the disclosed composition is formulated for a subject.
- the term "subject" refers to any member of the mammal.
- the term "subject” is to be read to include “human”, “individual”, “consumer”, “animal”, “patient” or “mammal” where context permits.
- the term "subject" defines any subject, particularly a mammalian subject, for whom treatment is indicated.
- Mammalian subjects include, but are not limited to, humans, domestic animals, farm animals, zoo animals, sport animals, pet animals such as dogs, cats, guinea pigs, rabbits, rats, mice, horses, cattle, cows; primates such as apes, monkeys, orangutans, and chimpanzees; canids such as dogs and wolves; felids such as cats, lions, and tigers; equids such as horses, donkeys, and zebras; food animals such as cows, pigs, and sheep; ungulates such as deer and giraffes; rodents such as mice, rats, hamsters, guinea pigs, and so on.
- a release of the active agent into the subject is a result of an environmental trigger and specific ingredients in the shell and/or the core.
- the term "environmental trigger” refers to a change in one or more environmental conditions (e.g., physiological condition(s)) sufficient to initiate degradation in the encapsulating materials of the shell and/or the core and/or the matrix, the change leading to a pre-defined release profile of the bioactive agent(s) encapsulated therein.
- the environmental trigger is time, or in another embodiment temperature, or in another embodiment moisture content, or in another embodiment pressure, or in another embodiment pH, or in another embodiment ionic strength, or in another embodiment enzymatic activity, or in another embodiment mechanical conditions (e.g., grinding by GI motility), or in another embodiment any combination thereof.
- an ingredient or combination of ingredients in the shell dictates targeted release of the active agent e.g., in the stomach, duodenum, jejunum, ilium, secum or the colon and the controlled release profile during a specified period of time (e.g., 5 minutes to 8 hours).
- the environmental condition change may be by a change of +2.5% in the reference environmental condition, or in another embodiment a change of +5% in the reference environmental condition, or in another embodiment a change of +10% in the reference environmental condition, or in another embodiment a change of +15% in the reference environmental condition, or in another embodiment a change of +20% in the reference environmental condition, or in another embodiment a change of +25% in the reference environmental condition, or in another embodiment a change of +30% in the reference environmental condition, or in another embodiment a change of +35% in the reference environmental condition, or in another embodiment a change of +40% in the reference environmental condition, or in another embodiment a change of +45% in the reference environmental condition, or in another embodiment a change of +50% in the reference environmental condition, or in another embodiment by a change of more than +50% in the reference environmental condition.
- the reference environmental condition is time, or in another embodiment temperature, or in another embodiment moisture content, or in another embodiment pressure, or in another embodiment pH, or in another embodiment ionic strength, or in another embodiment enzymatic activity, or in another embodiment any combination thereof.
- the shell surrounding the core or matrix incorporating an active compound (agent) is specifically designed to degrade, or in another embodiment, undergo controlled release, as a response to exposure to the change in environmental condition, which is in one embodiment time, or in another embodiment temperature, or in another embodiment moisture content, or in another embodiment pressure, or in another embodiment pH, or in another embodiment ionic strength, or in another embodiment enzymatic activity, or in another embodiment any combination thereof.
- the shell is a protecting layer which provides protection to the encapsulated active agent, so that the active agent shall maintain or materially maintain its bioactive properties in hostile pre-consumption or post-consumption conditions.
- the at least one core, matrix or outer protection layer is dissolved, disintegrated or swelled, or in another embodiment outer protection layers are dissolved, disintegrated or swelled and the "dormant" active agent will be released and become physiologically active.
- selective release can be affected using different types of matrix or coating layer (e.g., that are pH independent), and their disintegration is triggered in the presence of enzymes, and augmented mechanical GI tract forces.
- matrix or coating layer e.g., that are pH independent
- different enzymes may be present in the stomach, duodenum, jejunum, ilium and colon, each enabling a specific and different triggering event.
- core, matrix or a coating layer that are insoluble in non-enzymatic acidic conditions can be fabricated from coating compositions based on Prolamin proteins (Zein, Gluten, Kafirin, etc.), Shellac, fats (Coconut oil, Palm oil, etc.), and any combination thereof.
- Such core, matrix or a coating layer can be used to selectively release the active agent from the core.
- a first (and inner) encapsulation coating layer in the shell can control the release of the active agent as described above and at least one additional encapsulation layer can be used to further seal the core and the first encapsulation layer from the non-dry composition (e.g., in the gel or the ready-to-drink (RTD) product).
- at least one additional outer encapsulation coating layer, or shell may be designed for maximum sealing.
- the shell is breached under the enzymatic and/or mechanical grinding conditions of the stomach, the small intestines or the colon, thereby exposing the inner encapsulation layer and its selective dissolution profile thereof.
- the outer (second) encapsulation coating layer can include materials which are insoluble in acidic, non-enzymatic conditions, but are rapidly dissolved/disintegrated under the enzymatic and/or mechanical grinding conditions of the stomach, the small intestines or the colon.
- materials are described hereinthroughout, and include, but are not limited to, Prolamin proteins (Zein, Gluten, Kafirin, etc.) and fats (Coconut oil, Palm oil) and any combinations thereof.
- the coating/shell is dissolved in the presence of specific digestive enzymes, for example, and without limitation, glycoside hydrolase (e.g., chitinases and chitosanases), pepsin, trypsin, amylase, lipase and liver enzymes.
- specific digestive enzymes for example, and without limitation, glycoside hydrolase (e.g., chitinases and chitosanases), pepsin, trypsin, amylase, lipase and liver enzymes.
- a coating dissolved in the presence of specific digestive enzymes can be based on Prolamin proteins (e.g. Zein, Gluten, Kafirin), Gelatin, Soy proteins, Pea proteins (Globulin), Vegetable proteins, fats, Starches, Dextran, Maltodextrin, Cyclodextrin, Whey and Casein, and any combination thereof.
- a coating dissolved or disintegrated in the presence of a specific digestive enzyme of the small intestines include, but are not limited to: Guar gum, gum Arabic, Pectin and Amylose, and any combination thereof. Such coatings can be used to release the active agent of core of the microparticle in the small intestine.
- a coating dissolved or disintegrated in the presence of a specific enzyme of the colon include, but not limited to, Starches, Guar gum, Pectins, Chitosans, Alginates, Hydrogels, and any combination thereof. Such coatings can be used to release the active agent of the core of the microparticle in the colon.
- a coating dissolved or disintegrated under low pH conditions include, but are not limited to, Polymethacrylates. Such coatings can be used to release the active agent of core of the microparticle in the stomach.
- coatings that facilitate slow-release / controlled release / sustained release, independent of enzymatic and pH conditions include, but are not limited to, Ethyl Cellulose and other cellulose derivatives. Such coatings can be used for controlled release of an active agent throughout the GI tract.
- the shell of the microparticles can be non-uniform e.g., to allow selective dissolution of the microparticles and prolonged selective release of the active ingredient.
- the active agent is designed in a way whereby the release of the active agent occurs before entering a gastrointestinal tract GI system of the subject (e.g., human or animal) consuming the formulation.
- the release may be while in contact with specific part(s) of the gastrointestinal tract.
- the term "protect”, or any grammatical derivative thereof, is meant to refer to the encapsulation of the shell protecting the active agent, at least partially, during its passage through the stomach, such that sufficient amounts of the active agent are still bioactive and are capable of promoting the required positive health promotion or the required benefits, whether e.g., acute, prophylactic or chronic.
- the term "protect” and any grammatical derivative thereof further refers to the encapsulation of the shell protecting the active agent, thereby eliminating or significantly minimizing unpleasant odor and/or taste of the active agent.
- the shell surrounding an active agent is specifically designed to degrade or disintegrate or swell, or in another embodiment, undergoes controlled release, as a response to exposure to the change in environmental condition or a combination of environmental conditions.
- controlled release means control of the rate of dissolution of the active agent in a body fluid (e.g., in the gastrointestinal tract) such that it is slower than the intrinsic dissolution rate of the active agent (e.g., pharmaceutical API, an active agent or a dietary supplement) in such a medium. It may otherwise or additionally mean a delayed release of the active agent. This effect results in the active agent being released into the solution over a longer period than would be achieved if the active agent were administered without control of its release pattern and/or after an initial delay.
- a body fluid e.g., in the gastrointestinal tract
- the active agent e.g., pharmaceutical API, an active agent or a dietary supplement
- the pattern of controlled release achieved by the present composition is known as sigmoidal.
- sigmoidal pattern refers to a release profile exhibiting (a) an optional lag time from administration during which no specific active agent or very little amount of a specific active agent (e.g., less than 33%, 25%, 20%, 15%, 10%, 5%, 2% or 1%, by weight) is released, followed by (b) a phase where the rate of the active agent release increases, followed by (c) a phase where the rate of the specific active agent release decreases towards zero as the amount of the active agent in the composition is exhausted or materially exhausted.
- a specific active agent e.g., less than 33%, 25%, 20%, 15%, 10%, 5%, 2% or 1%, by weight
- the changeover from phase (b) to phase (c) occurs when at least 50% by weight of the active agent has been released.
- composition may incorporate e.g., one two several dozens of active agents, each specific active agent may be present in the composition in one or more core, matrix & core-shell and/or shell encapsulation combination, each combination having a different dissolution trigger or different dissolutions triggers and featuring a different release profile.
- the disclosed composition may include a particle with multiple active agents which share an identical core, matrix, core-shell and/or shell providing a specific trigger event and a specific release profile.
- the disclosed composition may include particles, where active agents, based on its water solubility (e.g., all water-soluble active agents, all partially water soluble active agents and all water insoluble actives) are grouped into several particles, each particle type having its own trigger and release profile.
- active agents based on its water solubility (e.g., all water-soluble active agents, all partially water soluble active agents and all water insoluble actives) are grouped into several particles, each particle type having its own trigger and release profile.
- the composition comprises at least two (e.g., 3, 4, 5, 6, 7, 8, 9,10, 11, 12, 13, 14, 15, 16, 17, 18, 19, 20, 21, 22, 23, 24, 25, 26, 27, 28, 29 or 30) different microparticles in a plurality of the microparticle, wherein each microparticle comprises an identical, similar or different active agent being characterized by a different sigmoidal pattern of controlled release or sustained release of the active agent in a GI tract of a subject.
- each microparticle comprises an identical, similar or different active agent being characterized by a different sigmoidal pattern of controlled release or sustained release of the active agent in a GI tract of a subject.
- At least one microparticle comprises at least two (e.g., 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, 12, 13, 14, 15, 16, 17, 18, 19, 20, 21, 22, 23, 24, 25, 26, 27, 28, 29, 30, 32, 34, 36, 38, 40, 42, 44, 46, 48 or 50, including any value therebetween) active agents, wherein each active agent is characterized by a different sigmoidal pattern of controlled release or sustained release thereof in a GI tract of a subject.
- each active agent is characterized by a different sigmoidal pattern of controlled release or sustained release thereof in a GI tract of a subject.
- there is provided a use of the disclosed composition for providing an effective dose of the at least one active agent to one or more target sites of GI tract of a subject.
- the use is for oral administration.
- kits comprising the disclosed composition.
- the kit is for oral administration.
- the kit further comprises instructions for preparation and use.
- the composition in the kit is in the solid form.
- the kit further comprises at least one diluting solution.
- the components of the kit are maintained and/or stored in the form of solutions.
- the composition may be maintained in a dry or solid form and the composition requires reconstruction and/or dissolution under particular condition(s), e.g., gentle blending or vigorous shaking.
- storage it is meant to refer to appropriate condition(s) for storing each one of the components of the kit in a single container, or dual chamber container (e.g. the composition and reconstituting liquid are isolated one from the other until reconstruction and consumption), or in separate containers.
- Container may be any container made of inert materials that do not interact with the content of each component and that are stable under the storage conditions.
- suitable containers for storing each components of the kit include a sachet, a bag, a can, a bottle, a vial, a large volume parenteral, a small volume parenteral, or a cassette.
- Storage conditions may include sterile or aseptic conditions, i.e. each component is preferably maintained sterile or aseptic. Alternatively, the content of each container may be readily sterilized.
- a method for treating a disorder comprising administrating to an individual the disclosed composition.
- the method of treating a health or medical condition associated with any temporary, transient, acute or chronic disease, medical condition, disorder, or nutritional deficiency in a subject in need thereof comprises administering to the subject a therapeutically or nutritionally effective amount of the disclosed composition.
- the subject is a human. In another embodiment, the subject is a human suffering from a temporary, transient or chronic disease, disorder, health condition, or a nutritional deficiency. [243] In some embodiments, the composition is specifically formulated for controlled release of the at least one active agent in a gastrointestinal (GI) tract of a subject.
- GI gastrointestinal
- encapsulation approaches can be used to encapsulate the active agent (e.g., pharmaceutical API, natural active or dietary supplements) of the disclosed composition.
- active agent e.g., pharmaceutical API, natural active or dietary supplements
- Non-limiting examples of such approaches include encapsulating active agent(s) (e.g., pharmaceutical API, active ingredient, natural active or dietary supplement raw materials which are frequently characterized by a foul taste odor; or low water solubility) with enteric and/or other encapsulating materials in a fluidized bed; spray-drying a mixture of a dietary supplement and enteric/encapsulant ingredients; and/or; freeze-drying a mixture spray-drying a mixture of a dietary supplement and enteric/encapsulant ingredients, and then grinding it to the desired final particle size/diameter.
- active agent(s) e.g., pharmaceutical API, active ingredient, natural active or dietary supplement raw materials which are frequently characterized by a foul taste odor; or low water solubility
- a multi-layer encapsulation can be achieved.
- a multi-layer encapsulation can be achieved in a single step e.g., using a 2-fluid, 3 -fluid, 4-fluid or 5 -fluid nozzle in a spray dryer; or a combination of spray drying and fluid bed coating
- the two-step process allows to generate the core in either a spray dryer or by grinding the active agent or a matrix incorporating the active agent to a pre-desired size (e.g., diameter), and then to use a fluidized bed to generate the at least one coating layer.
- the core or matrix may be generated in any of a variety of methods known in the art, and then a single additional step of multiple steps in a fluidized bed of similar equipment (like a mixer with injected solution) is used to create the at least one shell / encapsulating layer.
- the process comprises:
- the mixing of the active agent and the at least one encapsulating ingredients i.e. water-insoluble, enzymatically-degradable coating, liquid-swellable coating, pH-dependent coating, enteric coating or any combination thereto, is performed in a liquid or non-dry solution, thereby forming a core solution.
- encapsulating ingredients i.e. water-insoluble, enzymatically-degradable coating, liquid-swellable coating, pH-dependent coating, enteric coating or any combination thereto
- liquid may refer to a solvent or a mixture of solvents.
- the solvent is or comprise one or more organic (pharma grade or food grade) solvents and/or water.
- the pharma grade or food grade solvent is selected from, but is not limited to, methanol, ethanol, acetone and ethyl acetate, or other appropriate solvents e.g., approved by the regulatory agency (e.g., FDA) for pharmaceutical and/or food grade compositions, or their mixtures or combination thereof.
- the ratio (w/w or v/v) of the active agent (s) and the shell is 20: 1, 15: 1, 10: 1, 9: 1, 8: 1, 75: 6: 1, 5: 1, 4: 1, 3: 1, 2: 1, 1: 1, 1:2, 1:3, 1:4, 1:5, 1:6, 1:7, 1:8, 1:9, 1: 10, 1: 15, 1:20, 1:30, 1:40 or 1:50, including any value therebetween.
- the ratio may relate to the percentage of the raw material incorporating the active(s), or in some embodiments, to the percentage of the active agent per se.
- the active agent (s) are in the range 5% - 66% and the shell is in the range of 10% - 30%, by weight of the total particle.
- the active agent(s) or the raw material incorporating the active(s) are in the range of 1% - 45% and the shell is about 10% - 50%, by total weight of the particle.
- the active agent(s), or the raw material incorporating the active(s) are in the range of 5% to 60% and the shell is in the range of 10% - 25%, by total weight of the particle.
- the total of water- insoluble enzymatically- degradable coating, water- sellable coating, pH-dependent coating and enteric coating ingredients, and the total of active agent (s) are in ratio of about 3: 1:0.5, by weight.
- “about” may refer to with + 10%, + 20%, or + 30% or + 40% variation of any ratio thereof.
- the one or more enzymatically-degradable water- insoluble ingredients are in amount that ranges from 1% to 35%, by total dry weight of the core solution. In some embodiments, the one or more enzymatically-degradable water- insoluble ingredients are in amount that ranges from 1% to 15%, by total dry weight of the core solution. In some embodiments, the one or more enzymatically- degradable water-insoluble ingredients are in amount that ranges from 8% to 12%, by total dry weight of the core solution.
- the shell solution comprises water-insoluble ingredients such as slow release polymers.
- the shell solution further comprises a pH dependent material, for example, and without limitation, phthalate, cellulose, and any derivative thereof.
- the shell solution comprises enteric coating ingredient(s) (e.g., in an amount that ranges from 1% to 33% solids) which are dissolved in an organic solvent solution or water or any combination thereto.
- enteric coating ingredient(s) e.g., in an amount that ranges from 1% to 33% solids
- water may include water- based emulsions.
- the shell solution and the core solution are sprayed, each in a separate fluid channel in a closed-loop or in an open loop (for example, by a Buchi B-290 equipped with a 3-fluid nozzle: a gas channel: nitrogen or air, a fluid channel for the core solution and a fluid channel for the shell solution), optionally without the aid of a humidifier.
- the combination of the core composition and the shell composition incorporating aggregate alcohol content under 25% and preferably under 20%, may be used.
- the core comprises a small amount of an organic solvent (such as, but not limited to alcohol) with or without water.
- the shell comprises a small amount of organic solvent (alcohol), with or without water.
- small amount it is meant to refer to an amount that ranges from 0% to 60%, by weight, for example, 0%, 5%, 10%, 15%, 20%, 25%, 30%, 35%, 40%, 45%, 50%, 55%, or 60%, including any value and range therebetween.
- small amount refers to at most 25%.
- the shell solution and/or the core solution comprise at least 95% of organic solvent(s).
- the organic solvent(s) may necessitate, in some embodiments, the use of a closed-loop spray dryer (e.g., a spray dryer with nitrogen atmosphere and an integral humidifier unit for the cooling and collection of sprayed alcohol) and/or a fluid bed.
- a closed-loop spray dryer e.g., a spray dryer with nitrogen atmosphere and an integral humidifier unit for the cooling and collection of sprayed alcohol
- the process comprises:
- composition blending the active agent and at least one from (i) and (ii) (as defined above under "The composition") in a solution comprising organic solvent (e.g., alcohol) and/or water, thereby forming a core solution;
- organic solvent e.g., alcohol
- compositions, methods or structure may include additional ingredients, steps and/or parts, but only if the additional ingredients, steps and/or parts do not materially alter the basic and novel characteristics of the claimed composition, method or structure.
- method refers to manners, means, techniques and procedures for accomplishing a given task including, but not limited to, those manners, means, techniques and procedures either known to, or readily developed from known manners, means, techniques and procedures by practitioners of the chemical, pharmacological, biological, biochemical and medical arts.
- treating includes abrogating, substantially inhibiting, slowing or reversing the progression of a condition, substantially ameliorating clinical aesthetical, or nutritional symptoms of a condition or substantially preventing the appearance of clinical, nutritional or aesthetical symptoms of a condition.
- a core solution was prepared.
- the core (or matrix) solution contained at least two main components of an enzymatic -degradable coating, active agent and optionally contained enteric coating components in a ratio of 3: 1:0.5, respectively.
- the solution was an alcohol solution or a water based emulsion.
- the coating (shell) solution comprised a slow release polymer, optionally in combination with other ingredients that are pH dependent like phthalates.
- the dissolved enteric coating was in an amount of 10- 20% solids in the coating (shell) solution.
- the core and shell solutions were sprayed in a Buchi B-290 equipped with a 3 -fluid nozzle in a closed-loop (e.g. with Nitrogen atmosphere) or an open loop depending on the specific formulations and the amount of organic solvents (e.g., alcohols) in the solution.
- a closed-loop e.g. with Nitrogen atmosphere
- organic solvents e.g., alcohols
- the ratio in the formulation was: active agent: core matrix: shell coating 1:3: 1.5-5, respectively.
- Second variation (also referred to as: "reverse coated particle”):
- the shell solution contained a water based emulsion of a slow release polymer and an enteric coating ingredient.
- the core solution was also a water based emulsion comprising the active material.
- the core and the shell solutions combined contained low amount of alcohol, minimum as possible from 0% to 25% combined
- the spraying rate was set.
- the coating solution contained the enzymatic - degradable coating components in a water and alcohol solution of max 60% alcohol (depends on the solubility of the coating ingredients).
- the spray ratio of the two solutions was fixed to obtain a max 25% alcohol in both sprayed solutions.
- Increasing of the particle size enables to reduce the amount of the coating and by that reducing the aggregate alcohol levels in the combination of core and shell formulation being sprayed concurrently.
- the total solids content was 4.5% for the core solution and 10% solids for the coating solution.
- the core matrix solution and the coating solution were concurrently spray dried in a 2: 1 ratio using a 3- fluid nozzle fitted to a Buchi-290 Mini spray drier (Flawil, Switzerland) operating in a close loop.
- the inlet temperature was 130 degrees C and the aspirator was set tol00%.
- the outlet temperature was 95-100 degrees C.
- test fluid was 600 ml solution of water in pH 2.5 obtained by using HC1 solution.
- the acidic water solution did not incorporate any enzymes.
- the desired release profile could not be achieved.
- an immediate release of the active agent e.g., Kudzu
- the active agent e.g., Kudzu
- Figure 6 presents the release profile of the active agent (Kudzu) when the formulation was produced by in an open-loop system spray dryer with a reverse coating approach.
- the particle comprises Kudzu, ethyl cellulose and Zein.
- microparticles containing various amounts of active agents were prepared as shown in Table 3.
- the microparticles were further mixed with additional non-encapsulated active agents, as further summarized in one specific example in Table 3. Table 3
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Abstract
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Priority Applications (6)
Application Number | Priority Date | Filing Date | Title |
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CN201780033253.0A CN109562070A (en) | 2016-03-30 | 2017-03-30 | Composition and method for the delivering of selective gastrointestinal tract |
KR1020187031376A KR20190026648A (en) | 2016-03-30 | 2017-03-30 | Compositions and methods for selective gastrointestinal tract delivery |
CA3019745A CA3019745A1 (en) | 2016-03-30 | 2017-03-30 | Compositions and methods for selective gi tract delivery |
US16/088,168 US20190192444A1 (en) | 2016-03-30 | 2017-03-30 | Compositions and methods for selective gi tract delivery |
JP2018551300A JP2019513146A (en) | 2016-03-30 | 2017-03-30 | Compositions and methods for selective GI tract delivery |
EP17773444.9A EP3435983A4 (en) | 2016-03-30 | 2017-03-30 | Compositions and methods for selective gi tract delivery |
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US201662315060P | 2016-03-30 | 2016-03-30 | |
US62/315,060 | 2016-03-30 |
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PCT/IL2017/050394 WO2017168426A1 (en) | 2016-03-30 | 2017-03-30 | Compositions and methods for selective gi tract delivery |
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EP (1) | EP3435983A4 (en) |
JP (1) | JP2019513146A (en) |
KR (1) | KR20190026648A (en) |
CN (1) | CN109562070A (en) |
CA (1) | CA3019745A1 (en) |
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Cited By (2)
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EP3610862A1 (en) * | 2018-08-14 | 2020-02-19 | Apillet APS | Novel oral composition |
WO2022263505A1 (en) * | 2021-06-16 | 2022-12-22 | Société des Produits Nestlé S.A. | Methods of solid phase wax coating of an active ingredient |
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WO2019050969A1 (en) * | 2017-09-06 | 2019-03-14 | Prud'homme, Robert, K. | Dihydromyricetin nanoparticle formulations |
WO2019055539A1 (en) | 2017-09-12 | 2019-03-21 | Prudhomme Robert K | Cellulosic polymer nanoparticles and methods of forming them |
GB2584341B (en) | 2019-05-31 | 2023-03-01 | Gw Res Ltd | Cannabinoid formulations |
CN111317135A (en) * | 2020-02-17 | 2020-06-23 | 天津科技大学 | Method for embedding slow-release curcumin by polyphenol-modified zein nanoparticles |
CN111317824B (en) * | 2020-02-29 | 2022-04-12 | 复旦大学 | Oral nano preparation carrying polypeptide medicine and preparation method thereof |
AU2021232165A1 (en) * | 2020-03-02 | 2022-09-29 | Nuversys Ltd. | A stable food-grade microcapsule for the delivery of unstable and food-incompatible active ingredients to food products |
US20240216479A1 (en) * | 2021-05-05 | 2024-07-04 | Bing Biotech Limited | Encapsulation of dual-enzyme composition for preventing, treating and/or alleviating veisalgia and symptoms associated therewith |
US11878280B2 (en) | 2022-04-19 | 2024-01-23 | Trucapsol Llc | Microcapsules comprising natural materials |
CN115844811B (en) * | 2022-09-10 | 2024-02-09 | 中南民族大学 | PVA-GG-based double-layer heterogeneous microgel delivery system and application thereof in preparation of colonitis treatment drugs |
US11969491B1 (en) * | 2023-02-22 | 2024-04-30 | Trucapsol Llc | pH triggered release particle |
KR102563745B1 (en) * | 2023-03-17 | 2023-08-07 | 원영국 | Pharmaceutical composition for preventing or treating obesity having garcinia cambogia extract and health functional food having the same |
CN118177279B (en) * | 2024-05-14 | 2024-09-03 | 中国农业科学院农产品加工研究所 | High-stability corn endogenous component emulsion capable of resisting gastric environmental stress, and preparation method and application thereof |
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- 2017-03-30 US US16/088,168 patent/US20190192444A1/en not_active Abandoned
- 2017-03-30 CN CN201780033253.0A patent/CN109562070A/en active Pending
- 2017-03-30 WO PCT/IL2017/050394 patent/WO2017168426A1/en active Application Filing
- 2017-03-30 KR KR1020187031376A patent/KR20190026648A/en not_active Application Discontinuation
- 2017-03-30 CA CA3019745A patent/CA3019745A1/en not_active Abandoned
- 2017-03-30 EP EP17773444.9A patent/EP3435983A4/en not_active Withdrawn
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EP3610862A1 (en) * | 2018-08-14 | 2020-02-19 | Apillet APS | Novel oral composition |
WO2020035475A1 (en) * | 2018-08-14 | 2020-02-20 | Apillet Aps | Novel oral composition |
CN112533592A (en) * | 2018-08-14 | 2021-03-19 | 阿匹莱特公司 | Novel oral compositions |
KR20210044225A (en) | 2018-08-14 | 2021-04-22 | 에이필렛 에이피에스 | New oral composition |
WO2022263505A1 (en) * | 2021-06-16 | 2022-12-22 | Société des Produits Nestlé S.A. | Methods of solid phase wax coating of an active ingredient |
Also Published As
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EP3435983A1 (en) | 2019-02-06 |
JP2019513146A (en) | 2019-05-23 |
CA3019745A1 (en) | 2017-10-05 |
US20190192444A1 (en) | 2019-06-27 |
CN109562070A (en) | 2019-04-02 |
KR20190026648A (en) | 2019-03-13 |
EP3435983A4 (en) | 2019-12-18 |
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