OROMUCOSAL FILM COMPOSITIONS COMPRISING EPINEPHRINE PARTICLES
20230157950 · 2023-05-25
Assignee
Inventors
Cpc classification
B33Y10/00
PERFORMING OPERATIONS; TRANSPORTING
A61K31/167
HUMAN NECESSITIES
A61K45/06
HUMAN NECESSITIES
A61K47/10
HUMAN NECESSITIES
A61K31/5517
HUMAN NECESSITIES
A61K47/32
HUMAN NECESSITIES
A61K31/137
HUMAN NECESSITIES
A61K31/167
HUMAN NECESSITIES
A61K31/569
HUMAN NECESSITIES
A61P1/00
HUMAN NECESSITIES
B33Y80/00
PERFORMING OPERATIONS; TRANSPORTING
A61K2300/00
HUMAN NECESSITIES
A61K2300/00
HUMAN NECESSITIES
A61K31/137
HUMAN NECESSITIES
B33Y70/10
PERFORMING OPERATIONS; TRANSPORTING
A61K9/006
HUMAN NECESSITIES
A61K31/5513
HUMAN NECESSITIES
International classification
A61K9/00
HUMAN NECESSITIES
A61K31/167
HUMAN NECESSITIES
A61K31/137
HUMAN NECESSITIES
A61K47/10
HUMAN NECESSITIES
A61K9/70
HUMAN NECESSITIES
Abstract
The invention provides an oromucosal film composition comprising: a therapeutically effective amount of epinephrine solid particles having a particle size in the range of from about 0.01 um to about 100 um; and a pharmaceutically acceptable polymer
wherein the epinephrine solid particles are dispersed in and/or disposed on a polymeric layer. The film compositions can be used for the treatment of anaphylactic shock, cardiac arrest, asthma, bronchial asthma, bronchitis, emphysema, respiratory infections, and allergic reactions. The film compositions may further contain local anesthetics and used for providing local anesthesia, such as for the treatment or prevention of tooth pain and treatment of mouth ulcers.
Claims
1. An oromucosal film composition comprising: a therapeutically effective amount of epinephrine solid particles having a particle size in the range of from about 0.01 um to about 100 um; and a pharmaceutically acceptable polymer wherein the epinephrine solid particles are dispersed in and/or disposed on a polymeric layer.
2. The composition of claim 1 wherein the polymer is selected from the group consisting of hypromellose, hydroxypropyl cellulose, hydroxyethyl cellulose, carboxymethyl cellulose, carboxymethyl cellulose sodium, carbomer, polycarbophil, povidone, polyvinyl alcohol, polyethylene oxide, polyethylene glycol, sodium alginate, calcium alginate, xanthan gum, pectin, hyaluronic acid, sodium hyaluronate, tragacanth, guar gum, acacia gum, arabic gum, lectin, starch, gelatin, pullulan, carrageenan, chitosan, amino methacrylate copolymers, poloxamer, collagen, poly-amino acids, and mixtures thereof.
3. The composition of claim 1 wherein the epinephrine particle size is in the range of from about 10 um to about 80 um.
4. The composition of claim 1 wherein the composition further comprises one or more pharmaceutically acceptable excipients selected from the group consisting of pH modifiers, absorption enhancers, disintegrants, plasticizers, saliva stimulating agent, taste masking agents, flavoring agents, sweeting agent, coloring agent, antioxidants, stabilizers, anti-foaming and/or defoaming components and mixtures thereof.
5. The composition of claim 4 wherein the pH modifiers are selected from the group consisting of citric acid, acetic acid, succinic acid, tartaric acid, maleic acid, malic acid, ascorbic acid, acetylsalicylic acid, adipic acid, fumaric acid, glutaric acid, glutamic acid itaconic acid, aspartic acid, lactic acid, and salts and mixtures thereof.
6. The composition of claim 4 wherein the absorption enhancers are selected from the group consisting of chelators, non-ionic surfactants, cationic surfactants, anionic surfactants, bile salts and other steroidal detergents, fatty acids, fatty acids salts and esters, sucrose fatty acid esters, non-surfactants, phospholipids, complexing agents, cyclodextrins, alkyl glycosides, polyethylene glycol alkyl ethers, self-emulsifying agents, and mixtures thereof.
7. The composition of claim 4 wherein the absorption enhancers are selected from the group consisting of limonene, menthol, pinene, clove oil, eugenol, caprylocaproyl polyoxyl-8-glycerides, propylene glycol monocaprylate, deoxycholate sodium, taurocholate sodium, glycocholate sodium, diethylene glycol monoethyl ether, dodecylmaltoside, tetradecyl maltoside, and mixtures thereof.
8. The composition of claim 1 wherein the composition is a bi-layered film where a first layer comprises epinephrine solid particles dispersed in and/or disposed on a mucoadhesive polymeric layer, and a second layer which acts as a backing layer.
9. The composition of claim 1 wherein the composition is a tri-layered film comprising: a layer comprising the epinephrine solid particles dispersed in and/or disposed on a polymeric layer; a mucoadhesive layer; and a backing layer, wherein either the mucoadhesive layer or the polymeric layer comprising epinephrine particles is the middle layer.
10. The composition of claim 8 further comprising one or more local anesthetics in the polymeric layer.
11. The composition of claim 10 wherein the local anesthetic is selected from the group consisting of lidocaine, articaine, bupivacaine, prilocaine, mepivacaine and mixtures thereof.
12. A method for preparation of the composition of claim 1 wherein the method comprises solvent casting, hot melt extrusion, electrospinning, 3-dimensional or flexographic printing, spraying, combination of solvent casting and spraying, electrospraying, solution blow spinning, electroblowing, centrifugal spinning, or a combination of electrospinning and electrospraying.
13. The method of claim 12 wherein the method involves using a solvent/dispersant selected from the group consisting of lower alkyl alcohols, acetone, methyl acetate, ethyl acetate, isopropyl acetate, acetonitrile, heptane, tetrahydrofuran, water, alkaline water, aqueous buffer, and mixtures thereof.
14. A method for preparation of the composition of claim 1 wherein the method comprises: providing a suspension of epinephrine solid particles having a particle size in the range of from about 0.01 um to about 100 um in a solvent/dispersant; simultaneously or separately providing a suspension or solution of the polymer in a solvent/dispersant; combining the epinephrine solid particle suspension and the polymer suspension/solution if prepared separately; and removing the solvent/dispersant to obtain the polymeric layer.
15. The method of claim 14 wherein the solvent is selected from the group consisting of lower alkyl alcohols, acetone, methyl acetate, ethyl acetate, isopropyl acetate, acetonitrile, heptane, tetrahydrofuran, water, alkaline water, aqueous buffer, and mixtures thereof.
16. A method of treating anaphylactic shock, cardiac arrest, asthma, bronchial asthma, bronchitis, emphysema, respiratory infections, or allergic reactions in a subject in need thereof comprising administering to the subject a composition according to claim 1.
17. The method of claim 16 wherein the composition is administered sublingually or buccally.
18. A method of providing local anesthesia or treating tooth pain or mouth ulcers in a subject in need thereof comprising administering to the subject a composition according to claim 10.
19. An oromucosal film composition comprising: a therapeutically effective amount of epinephrine solid particles having a particle size in the range of from about 0.01 um to about 100 um; and a pharmaceutically acceptable polymer, wherein the epinephrine solid particles are dispersed in and/or disposed on a polymeric layer, and wherein the composition excludes an anti-crystallization agent elected from the group consisting of sugar alcohols and di-alcohols.
20. An oromucosal film composition consisting essentially of: a therapeutically effective amount of epinephrine solid particles having a particle size in the range of from about 0.01 um to about 100 um; one or more absorption enhancers; one or more pH modifiers; and a pharmaceutically acceptable polymer wherein the epinephrine solid particles are dispersed in and/or disposed on a polymeric layer.
Description
BRIEF DESCRIPTION OF THE DRAWINGS
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DETAILED DESCRIPTION OF THE INVENTION
[0069] The epinephrine particles used in the invention may be in the form of epinephrine free base, epinephrine acid addition salts, or mixtures thereof. Salts of epinephrine include bitartrate, and hydrochloride acid addition salts. Epinephrine base and salts are well known in the art and may be prepared by convention methods or obtained commercially.
[0070] The term “consisting essentially of” means that the composition is limited to the components specified and those additional components that do not materially affect the basic and novel characteristic(s) of the composition.
[0071] The epinephrine solid particles are dispersed in and/or disposed on a polymeric layer which is a consistent homogeneous film or porous layer comprising of one or more polymers. In some embodiments, epinephrine particles are embedded within the polymeric layer, thus forming a composite material of polymers and particles. In some other embodiments, epinephrine particles are attached to, or disposed on the polymeric layer.
[0072] Epinephrine particles may be distributed uniformly throughout the polymeric layer, disposed or embedded on the entire surface of the polymeric layer or only a portion of its surface, as shown in
[0073] In some embodiments, the polymeric layer is a porous layer comprising polymeric nanofibers and/or microfibers. When nano or microfibers are used, epinephrine particles are deposited on the surface of fibers, and/or deposited into a mesh of polymeric nano or microfibers as shown in
[0074] In some embodiments epinephrine solid particles are at least partly included or embedded within the polymeric microfiber and/or nanofiber. In some other embodiments, epinephrine solid particles are dispersed in the polymeric layer but are not part of or included within the polymeric microfibers and/or nanofibers.
[0075] The epinephrine particle-containing polymer layer may be designed to dissolve in about 1 to about 30 minutes in the mouth, including more than 1 minute, more than 5 minutes, more than 10 minutes, more than 20 minutes or less than 30 minutes. In some embodiments, such as when used for local anesthesia, such as dental anesthesia, the polymer layer may dissolve in more than 30 minutes and last up to 12 hours in the mouth.
[0076] For fast dissolving films low molecular weight hydrophilic polymers, such as polymers having a molecular weight between about 1,000 to 9,000 daltons, or polymers having a molecular weight up to 900,000 daltons may be used, optionally in combination with other suitable polymers. For slower dissolving films higher molecular weight polymers, such as those having a molecular weight in millions of daltons may be used, optionally in combination with other suitable polymers. Desired results can be achieved by adjusting the concentration of two or more types of polymers. Concentration of the polymers and the type/nature/solubility of the polymers used in each layer of the composition may be varied to control the amount of time the film composition resides on the mucosa. Disintegrants and plasticizers may be used to adjust erodibility of the film composition. Water soluble pharmaceutically acceptable excipients may be used to achieve desired erodibility/solubility of the film, particularly when insoluble or low solubility polymers are included.
[0077] In certain embodiments, pH modifiers are formulated into the epinephrine particle-containing polymer layer. In certain other embodiments, pH modifiers are formulated into the mucoadhesive and/or backing layer.
[0078] In certain embodiments, absorption enhancers are formulated into the epinephrine particle-containing polymer layer. In certain other embodiments, absorption enhancers are formulated into the mucoadhesive or backing layer.
[0079] In certain embodiments, absorption enhancers, pH modifying agents and epinephrine particles are mixed with the polymer to formulate a polymeric matrix so as to form a composite pharmaceutical film formulation. In certain other embodiments, absorption enhancers, pH modifying agents are formulated into a polymeric matrix comprising nano/microfibers and epinephrine particles are deposited in the polymeric matrix. In certain embodiments, absorption enhancers and pH modifying agents are formulated into a polymeric matrix and epinephrine particles are deposited or deposed on the polymeric matrix.
[0080] In certain embodiments, when polymeric nano/microfibers are used, mucoadhesive polymers are used in forming the fibers.
[0081] The weight ratio of epinephrine to the polymer(s) used in the polymeric layer may be from about 5% to about 50%, from about 10% to about 40%, from about 15% to about 35%, from about 15% to about 30%, or from about 15% to about 25%.
[0082] While epinephrine solid particles dispersed in and/or disposed on the polymeric layer have a particle size in the range of from about 0.01 um to about 100 um, in some embodiments the particle size may be from about 0.1 um to about 50 um, from about 1 um to about 40 um, from about 8 um to about 100 um, from about 8 um to about 80 um, from about 10 um to about 100 um, from about 10 um to about 80 um, from about 20 um to about 80 um, from about 20 um to about 30 um, or from about 0.1 um to 3 um.
[0083] In some embodiments, the polymers used in the polymeric layer may be rapidly or moderately dissolvable in the saliva. In some embodiments, the polymers may be water soluble or swellable. Suitable polymers include water-soluble synthetic polymers and co-polymers, polosynthetic polymers and co-polymers, and natural polymers. Examples of suitable polymers include cellulose derivatives, polyacrylates, poloxamers, polyethylene oxides, polyvinyl alcohols, povidone, poly-amino acids, gums and other natural polymers.
[0084] Polymers that may be used in the polymeric layer include hypromellose, hydroxypropyl cellulose, hydroxyethyl cellulose, carboxymethyl cellulose, carboxymethyl cellulose sodium, croscarmellose sodium, carbomer, polycarbophil, povidone, crospovidone, polyvinyl alcohol, polyethylene oxide, polyethylene glycol, sodium alginate, calcium alginate, xanthan gum, pectin, hyaluronic acid, sodium hyaluronate, tragacanth, guar gum, acacia gum, arabic gum, lectin, starch, gelatin, pullulan, carrageenan, chitosan, amino methacrylate copolymers, poloxamer, collagen, and mixtures thereof.
[0085] In case of a single layered or bi-layered film composition comprising a backing layer, the polymers used in the polymeric layer include one or more mucoadhesive polymers. A suitable mucoadhesive polymer is also used in the mucoadhesive layer of a bi-layered or tri-layered film.
[0086] Mucoadhesive polymers in the polymeric or mucoadhesive layer are used to enhanced retention of the film composition on the oral mucosa. Such polymers include soluble and insoluble, non-biodegradable and biodegradable polymers. These polymers can be hydrogels or thermoplastics, homopolymers, copolymers or blends, natural or synthetic. Examples of suitable polymers include the same polymers as listed above for polymeric layer, provided they have mucoadhesive properties.
[0087] A backing layer is an occlusive layer designed to drive unidirectional release and absorption of epinephrine into the mucosa thereby decreasing amount of active ingredient required. A backing layer can also improve mechanical properties of the film to facilitate handling during production and use.
[0088] Backing layer may be formed using a hydrophobic, hydrophilic, erodible, low solubility or insoluble polymer, such as ethyl cellulose, hydroxyethyl cellulose, hydroxypropyl cellulose, methylcellulose, hypromellose, hypromellose phthalate, cellulose acetate, cellulose acetate phthalate, cellulose acetate butyrate, polyvinyl alcohol, povidone, crospovidone, polyethylene glycol, polyethylene oxide, polyvinyl alcohol-polyethylene glycol graft-copolymers, amino methacrylate copolymers, ethylene oxide, propylene oxide co-polymers, poly(vinyl acetate), poly(ethylene-co-vinyl) acetate, polycaprolactone, pharmaceutical wax, and mixtures thereof.
[0089] The mucoadhesive layer and/or backing layers may fully overlap with the polymeric layer or be larger than the polymeric layer such that they extend beyond and encompass the polymeric layer on all sides to facilitate effective mucoadhesion and/or prevent peripheral loss of epinephrine.
[0090] In some embodiments, the polymeric layer comprising the epinephrine solid particles is printed onto the mucoadhesive and/or backing layer.
[0091] One or more local anesthetics may be included in the polymeric layer and/or the mucoadhesive layer when the film composition is intended for providing local anesthesia, such as for treating tooth pain or mouth ulcers. Suitable local anesthetics include lidocaine, articaine, bupivacaine, prilocaine, mepivacaine, and mixtures thereof.
[0092] The thickness of the film composition may vary, depending on the number of layers and their thickness. The thickness and number of layers may be adjusted in order to vary the release/absorption of epinephrine particles and erosion/residence of the film in the mouth. For example, the thickness may range from about 0.05 μm to about 2 mm, from about 0.1 to about 0.5 mm, from about 0.01 mm to about 1 mm, or greater than 0.1 mm, greater than 0.2 mm, or less than 0.5 mm, less than 0.2 mm, less than 0.1 mm, or less than 1 um. The thickness of each layer may vary from 0.1 to 99.9% of the overall thickness, or 1 to 99% of the overall thickness, or 10 to 90% of the overall thickness of the multi-layered composition. For example, the thickness of each layer may vary from 0.01 mm to 0.9 mm.
Pharmaceutically Acceptable Excipients
[0093] The film composition may further comprise one or more pharmaceutically acceptable excipients, such as pH modifiers, absorption enhancers, binders, disintegrants, plasticizers, saliva stimulating agent, taste masking agents, flavoring agents, sweeting agent, coloring agent, antioxidants, stabilizers, anti-foaming and/or defoaming components and mixtures thereof. In some embodiments, the excipients are exclusively or partly present in the mucoadhesive layer and/or backing layer in case of a multilayered film. These excipients are well known in the art, such as those described in US20170348251A1.
[0094] The excipients may constitute up to about 80%, such as about 0.005% to 50%, or from about 1% to about 30% by weight of the composition. Epinephrine base may comprise
[0095] In some embodiments, pH modifiers are used to enhance the bioavailability of epinephrine. include weak organic acids including amino acids, phosphoric acid, acidic polymers, and salts and mixtures thereof.
[0096] Weak organic acids include citric acid, acetic acid, succinic acid, tartaric acid, maleic acid, malic acid, ascorbic acid, acetylsalicylic acid, adipic acid, fumaric acid, glutaric acid, glutamic acid, itaconic acid, aspartic acid, lactic acid, and salts and mixtures thereof. Salts of acids include inorganic salts, such as alkali metal salt, alkaline earth metal salt, ammonium salt, and salts formed with an organic base, such as lysine, arginine and meglumine.
[0097] In some embodiments, the pH modifiers are acidic polymers which serve the dual role of forming the polymeric layer and pH modification. Suitable acidic polymers include carboxymethylcellulose, cross-linked carboxymethylcellulose, poly(acrylic acid) polymers and copolymers, alginic acid, sodium alginate, calcium alginate, hyaluronic acid, mixtures and salts thereof.
[0098] In some embodiments, absorption enhancers are used to increase the bioavailability of epinephrine. Suitable absorption enhancers include chelators, non-ionic surfactants, cationic surfactants, anionic surfactants, bile salts and other steroidal detergents, fatty acids, fatty acids salts and esters, sucrose fatty acid esters, non-surfactants, phospholipids, complexing agents, cyclodextrins, alkyl glycosides, polyethylene glycol alkyl ethers, self-emulsifying agents, and mixtures thereof. Specific absorption enhancers include limonene, menthol, pinene, clove oil, eugenol, caprylocaproyl polyoxyl-8-glycerides, propylene glycol monocaprylate, deoxycholate sodium, taurocholate sodium, glycocholate sodium, diethylene glycol monoethyl ether (Transcutol® HP), dodecylmaltoside, tetradecyl maltoside, Intravail®, and mixtures thereof.
[0099] Flavoring agents and/or sweeteners include acacia syrup, acesulfame K, alitame, anise, apple, aspartame, banana, berry, black currant, butterscotch, calcium citrate, camphor, caramel, cherry, cherry cream, chocolate, cinnamon, bubble gum, citrus, citrus punch, citrus cream, cotton candy, cocoa, cola, cool cherry, cool citrus, cyclamate, cylamate, dextrose, eucalyptus, eugenol, fructose, fruit punch, ginger, glycyrrhetinate, glycyrrhiza syrup, grape, grapefruit, honey, isomalt, lemon, lime, lemon cream, monoammonium glyrrhizinate, maltol, mannitol, maple, marshmallow, menthol, mint cream, mixed berry, neohesperidine DC, neotame, orange, pear, peach, peppermint, peppermint cream, raspberry, root beer, rum, saccharin, safrole, sorbitol, spearmint, spearmint cream, strawberry, strawberry cream, stevia, sucralose, sucrose, sodium saccharin, saccharin, aspartame, acesulfame potassium, mannitol, talin, sylitol, sucralose, sorbitol, swiss cream, tagatose, tangerine, thaumatin, tutti fruitti, vanilla, walnut, watermelon, wild cherry, wintergreen, xylitol, or mixtures thereof.
[0100] Antioxidants include tocopherols and the esters thereof, sesamol of sesame oil, coniferyl benzoate of benzoin resin, nordihydroguaietic resin and nordihydroguaiaretic acid, gallates, butylated hydroxyanisole, ascorbic acid and salts and esters thereof, such as acorbyl palmitate, erythorbinic acid and salts and esters thereof, monothioglycerol, sodium formaldehyde sulfoxylate, sodium metabisulfite, sodium bisulfate, sodium sulfite, potassium metabisulfite, butylated hydroxy toluene, propionic acid, and combinations thereof.
[0101] Stabilizers include calcium chloride, calcium disodium ethylene diamine tetra-acetate, glucono delta-lactone, sodium gluconate, potassium gluconate, sodium tripolyphosphate, sodium hexametaphosphate, as cyclodextrins, cyclomannins (5 or more α-D-mannopyranose units linked at the 1,4 positions by α linkages), cyclogalactins (5 or more β-D-galactopyranose units linked at the 1,4 positions by β linkages), cycloatrins (5 or more α-D-altropyranose units linked at the 1,4 positions by α linkages), and combinations thereof.
[0102] Suitable coloring agents include azo dyes, organic or inorganic pigments, such as the oxides or iron or titanium, or coloring agents of natural origin. Anti-foaming and/or de-foaming agents include simethicone and similar agents.
[0103] Plasticizers include polyethylene glycols, polypropylene glycols, polyethylene-propylene glycols, glycerol, glycerol monoacetate, diacetate or triacetate, triacetin, polysorbate, cetyl alcohol, propylene glycol, sorbitol, sodium diethylsulfosuccinate, triethyl citrate, tributyl citrate, phytoextracts, fatty acid esters, fatty acids, and mixtures thereof.
[0104] Binders include starches, natural gums, pregelatinized starches, gelatin, polyvinylpyrrolidone, methylcellulose, sodium carboxymethylcellulose, ethyl celluiose, polymerylamides, polyvinyloxoazolidone, polyvinyl alcohols, and mixtures thereof.
[0105] The amount of epinephrine base used in the epinephrine base particle-containing layer may be from about 10% to about 30%, from about 12% to about 25%, from about 15% to about 20%, from about 15% to about 30%, or from about 15% to about 25%.
[0106] The amount of polymer used in the polymeric layer may be from about 5% to about 90%, from about 10% to about 85%, from about 25% to about 85%, from about 50% to about 75%, from about 55% to about 75%, or from about 60% to about 70%. The amount of absorption enhancer used in the polymeric layer may be from about 1% to about 3%, from about 1% to about 20%, from about 2% to about 15%, from about 6% to about 12%, or from about 3% to about 10%. The amount of antioxidant used in the polymeric layer may be from about 0.001% to about 10%, from about 0.005% to about 5%, from about 0.01% to about 3.5%, or from about 0.1% to about 3%. The amount of plasticizer used in the polymeric layer may be from about 2% to about 20%, from about 3% to about 18%, from about 4% to about 17%, from about 5% to about 20%, or from about 12% to about 18%.The amount of pH modifier used in the polymeric layer may be from about 1% to about 25%, from about 2% to about 20%, from about 3% to about 18%, from about 4% to about 17%, or from about 5% to about 15%.
Preparation Methods
[0107] The film compositions of invention may be prepared by conventional methods, such as solvent casting, hot melt extrusion, spinning, electro spinning, 3-dimensional or flexographic printing, spraying, electrospraying, combination of solvent casting and spraying, a combination of electrospinning and electrospraying, or any other permutation or combination of these methods. For example, methods described in Boda et al., J Aerosol Sci. 2018 November; 125: 164-181; Nguyen et al., J. Parm. Sci. 2016; 105: 2601-2620; Soares et al., Mater. Sci. Eng. C 2018 November; 92(1): 969-982; and Janßen et al., Int. J. Pharm. 2013 January; 441(1-2): 818-825 may be used.
[0108] In some embodiments, micronized particles of epinephrine are used.
[0109] The film may be formulated as a dispersion of epinephrine solid particles in a polymeric solution, such as by solvent casting method, or epinephrine particles are deposited into/onto the polymer layer by alternative methods, such as electrospinning, electrospraying, hot-melt extrusion, printing techniques (e.g., flexographic printing) or spraying, combination of solvent casting and spraying, solution blow spinning, electroblowing, centrifugal spinning, a combination of electrospinning and electrospraying, or any other suitable permutation or combination thereof.
[0110] Polymeric micro/nanofibers are produced by electrospinning, or other alternative methods (e.g. solution blowing, spinning method). Epinephrine particles are deposited using alternative spraying methods, such as electrospraying, simultaneously, or consecutively when producing polymeric fibers.
[0111] In case of a multi-layered film compositions, the layers may be manufactured separately and then laminated or layered in succession. Binding solution of polymer(s) may be sprayed between two film layers, such as the polymeric and backing layer to combine the layers. The binding solution can contain excipients, such as mucoadhesive polymer, pH modifier, and/or absorption enhancer, thereby forming the third layer of a three-layered system in situ.
[0112] In some embodiments, in case of a multi-layered film, the polymeric layer comprising the epinephrine solid particles is printed onto the mucoadhesive and/or backing layer, such as by employing a 3-dimensional or flexographic printing method. The mucoadhesive and/or backing layers may also be prepared by 3-dimensional or flexographic printing.
[0113] In some embodiments, the preparation method comprises: [0114] providing a suspension of epinephrine solid particles having a particle size in the range of from about 0.01 um to about 100 um in a solvent/dispersant; [0115] simultaneously or separately providing a suspension or solution of the polymer in a solvent/dispersant; [0116] combining the epinephrine solid particle suspension and the polymer suspension/solution if prepared separately; and [0117] removing the solvent/dispersant to obtain the polymeric layer.
[0118] Solvents/dispersants are used in the manufacturing process of oromucosal films of the invention to dissolve polymers and pharmaceutical excipients including plasticizers, pH modifiers, stabilizers, antioxidants, taste masking agents and absorption enhancers; all or just some of these excipients may be used depending on the requirements of the film formulation. In some embodiments, one or more polymers may remain suspended/dispersed or partially dissolved. In some embodiments, one or more excipients may remain suspended/dispersed or partially dissolved.
[0119] During the manufacturing process, those solvents/dispersants are used when processing epinephrine that do not dissolve epinephrine particles to any appreciable extent. The solvents/dispersant should disperse solid particles of epinephrine base without substantial dissolution to ensure the vast majority of epinephrine base is maintained as particulate in nature without any recrystallization, degradation or oxidization. More specifically, epinephrine particles are insoluble, practically insoluble, very slightly soluble or slightly soluble (as defined in the United States Pharmacopeia) in the solvents/dispersant used.
[0120] Suitable solvent/dispersant used in the preparation methods of the invention include lower alkyl alcohols, acetone, methyl acetate, ethyl acetate, isopropyl acetate, acetonitrile, heptane, tetrahydrofuran, water, alkaline water, aqueous buffer, and mixtures thereof. Suitable lower alkyl alcohols include methanol, ethanol, isopropyl alcohol, 2-propanol, 1-propanol 1-butanol, t-butanol, and mixtures thereof.
[0121] In some embodiments an aqueous dispersion of epinephrine base solid particles is prepared, and the pH of the dispersion is maintained above about 8 using a base or an alkali to prevent dissolution of the particles. For example, the pH of the dispersion may be maintained between about 8.5 to about 9.5.
Use
[0122] The film compositions of the invention may be used for the treatment of anaphylactic shock, cardiac arrest, asthma, bronchial asthma, bronchitis, emphysema, respiratory infections, and allergic reactions. The composition may be administered sublingually, buccally or via any other suitable mucosal surface.
[0123] When a local anesthetic is included, the film compositions of the invention may be used for the providing for local anesthesia, such as for treatment and/or prevention of tooth pain and treatment of mouth ulcers. A lower dose of epinephrine is used in combination with local anesthetics, such as lodicaine, novocaine, articaine, prilocaine, or mepivacaine, in a slower dissolving polymer for local or dental anesthesia. The amount of epinephrine base used in epinephrine base particle-containing layers in such cases may be from about 0.05% to about 5%, from about 0.1% to about 2%, from about 0.25% to about 1%, or from about 0.5% to about 1%. The amount of local anesthetic used in epinephrine base particle-containing layers in such cases may be from about 5% to about 90%, from about 10% to about 85%, or from about 50% to about 80%, or from about 50% to about 60%. The amount of polymer used in the polymeric layer may be from about 5% to about 40%, from about 10% to about 35%, or from about 15% to about 30. The amount of plasticizer used in the polymeric layer may be from about 1% to about 10%, from about 2% to about 8%, from about 2% to about 5%, or from about 2% to about 3. In addition to providing drug delivery, once the film composition adheres to the mucosal surface, it may also provide protection to the treatment site by acting as an erodible bandage.
[0124] When a low dose of epinephrine is used in combination with local anesthetics, and an absorption enhancer selected from the group consisting of diethylene glycol monoethyl ether, eugenol, bile acids, caprylocaproyl polyoxyl-8 glycerides, disodium ethylenediaminetetraacetic acid salt, and mixtures thereof, the epinephrine need not be in solid particulate form for preparing the oromucosal film. The quantity of ingredients used and the manner and design of film composition may be the same as that describes herein when solid particles of epinephrine are used. Epinephrine and one or more of local anesthetics may be present in a single layer or in separate layers. Epinephrine and one or more of local anesthetics may be dispersed or dissolved in and/or disposed on a polymeric layer which may be mucoadhesive.
EXAMPLES
[0125] The examples demonstrate that the epinephrine base particles maintain their structure when formulated into film using methods of the invention and that epinephrine base particles are compatible with absorption enhancers, and other excipients when formulated into film compositions of the invention. The examples also show that epinephrine is released rapidly from the film compositions of the invention and is quickly and effectively absorbed, as demonstrated under both ex-vivo and in-vivo conditions.
Example 1
The Effect of Different Solvents/Dispersants on the Size and Structure of Epinephrine Base Particles
Size Distribution of Epinephrine Particles
[0126] The epinephrine base particles were obtained as active pharmaceutical ingredient from Cambrex. The particles were micronized through microfluidization. The original and modified particles were evaluated for particle size distribution prior to formulation into film compositions. The results of are depicted in
Methods
Size Distribution Determination
[0127] The particle size distribution of starting/original epinephrine base particles (as supplied by Cambrex), and those obtained after micronization were analyzed using pictures taken by scanning electron microscopy (Hitachi SU8020, Japan). The size of particles was expressed as a Feret's diameter measured in a fixed direction.
Micronization
[0128] Epinephrine base particles (Cambrex) were subjected to micronization using Microfluidizer LV-1 (Microfluidics) for one or four cycles. Briefly, epinephrine base particles were suspended in alkaline water or isopropanol (50 mg/ml) and the pressure was set to 1200 PSI. One or four cycles of microfluidization were performed. Sodium metabisulphite was added into the suspension to prevent epinephrine oxidation during the process.
SEM Observation
[0129] The particles were observed using scanning electron microscopy. The samples were prepared by deposition of the sample on a glass surface, evaporation of solvent in the sample, and sputter coating using platinum/palladium electrode.
Results
[0130]
Conclusion
[0131] The original particle size was successfully reduced from about the size of 20 um to about 2 um or less using one or more cycles of microfluidization.
Solubility of Epinephrine Particles
[0132] Solubility experiments were performed to confirm the suitability of solvents/dispersants for manufacturing the film compositions of the invention. Solid particles of epinephrine base were subjected to solubility tests at increasing time intervals and temperatures using selected solvents/dispersants suitable for use in industrial pharmaceutical manufacturing processes. Selected solvents/dispersants dissolve film-forming excipients, plasticizers and eventually other pharmaceutical excipients including pH modifiers, stabilizers, antioxidants, taste masking agents, absorption enhancers but disperse epinephrine particles. The solubility of epinephrine particles may not be higher than 10% weight/volumes in the solvent/dispersant used. Epinephrine particles are very slightly soluble in some of the selected solvents/dispersants and preferably practically insoluble in some of the other selected solvents/dispersants.
[0133] Epinephrine solubility experiments were performed under various experimental conditions corresponding to those occurring during the manufacture of conventional oromucosal films. The effect of time, temperature and the concentration of epinephrine were evaluated using selected solvents/dispersants. Solvents/dispersants were selected from acetone, ethanol, ethyl acetate, 1-butanol, t-butanol, isopropyl alcohol, isopropyl acetate, methanol, 2-propanol, 1-propanol or acetonitrile, heptane, tetrahydrofuran, alkaline water-based solvents (water, buffers of pH 7, 8, 8.5, 9) and mixtures with water-miscible solvents thereof.
Method
[0134] Acetone, ethanol, methanol, isopropyl alcohol and alkaline water-based solvents of pH 7, 8, 8.5 and 9 were chosen as suitable solvents/dispersant candidates for the screening. Their effect on the solubility of epinephrine base particles was observed using scanning electron microscopy. Citric acid solution and water solution acidified using hydrochloric acid (HCl) of pH 2 were used as examples of standards/comparative solvents that dissolve epinephrine particles. The dissolution was followed by crystallization by evaporating the solvent prior to scanning with SEM.
[0135] To confirm the level of epinephrine base solubility at different concentrations, suspensions of epinephrine base particles at concentrations of 0.5 g/L, 5 g/L and 50 g/L were prepared in solvent/dispersants and the mixture gently stirred at 25° C. and 45° C. After this step, the solvent/dispersant was evaporated at 25° C. or 45° C. and the size and structure of the epinephrine particles obtained was evaluated using scanning electron microscopy (SEM, HITACHI SU 8020, Japan). Samples of the mixtures were withdrawn at 60, 180 and 360 minutes and the structure of the epinephrine particles was evaluated.
Results
[0136]
[0137]
[0138]
[0139]
Conclusion
[0140] The size and structure of epinephrine particles is maintained when using acetone, ethanol, methanol, isopropyl alcohol, and alkaline water-based solvents/dispersants at temperatures of 25° C. and 45° C. for at least 6 hours. Small micron-sized nanostructured crystals were observed that existed before and after dispersion with the selected solvents/dispersants; these particles were not formed due to a process of recrystallization. The concentration of epinephrine base particles in the dispersant/solvents had no influence on the physical size and structure of the processed epinephrine base particles.
Example 2
Preparation of the Oromucosal Film Compositions of the Invention
[0141] Various formulations were designed including single, bi and tri-layered oromucosal films to demonstrate the use of epinephrine base particles in alternative formulation designs. Selected solvents/dispersants as listed in Example 1 were used in the formulation of the epinephrine base particle-containing layer.
The Preparation Method
[0142] Each layer was formed separately (in the case of bi- and tri-layered films) and then laminated/combined to form the desired oromucosal film compositions. Alternatively, the layers could be built up in succession using the solvent casting or flexographic printing technique.
[0143] Each tri-layered film consists of 1) a backing layer, 2) a mucoadhesive layer and 3) an epinephrine particle-containing layer. In the first step the upper surface of a prepared mucoadhesive layer was coated with a polymer to form: i) a non-soluble backing layer (ethyl cellulose (Eleftheriadis et al. Fabrication of Mucoadhesive Buccal Films for Local Administration of Ketoprofen and Lidocaine Hydrochloride by Combining Fused Deposition Modeling and Inkjet Printing. J Pharm Sci. 2020 September; 109(9):2757-2766. doi: 10.1016/j.xphs.2020.05.022) or polycaprolactone (Colley et al. Pre-clinical evaluation of novel mucoadhesive bilayer patches for local delivery of clobetasol-17-propionate to the oral mucosa. Biomaterials. 2018 September; 178:134-146. doi: 10.1016/j.biomaterials.2018.06.009, Edmans et al. Mucoadhesive Electrospun Fiber-Based Technologies for Oral Medicine. Pharmaceutics. 2020 Jun. 2; 12(6):504. doi: 10.3390/pharmaceutics12060504); or ii) soluble backing layer (e.g. amino methacrylate copolymer-Eudragit® (Mašek et al. Multi-layered nanofibrous mucoadhesive films for buccal and sublingual administration of drug-delivery and vaccination nanoparticles—important step towards effective mucosal vaccines. J Control Release. 2017 Mar. 10; 249:183-195. doi: 10.1016/j.jconrel.2016.07.036)). In the second step, the bottom side of each mucoadhesive layer was moistened with a vapor stream and the epinephrine base particle-containing layer (third layer) was immediately pressed against this moistened mucoadhesive layer surface to form the tri-layered oromucosal film. Thermal-induced lamination could also be employed to attach the epinephrine containing third layer.
[0144] A variety of polymers, mucoadhesive polymers, and pharmaceutical excipients, including pH modifiers, absorption enhancers and antioxidants could be used in the formulations. In the case of pH modifiers, citric acid was used but other organic weak acids including tartaric, ascorbic and malic acids were also tested and could be used as alternatives to citric acid, e.g., adipic acid, ascorbic acid, citric acid, fumaric acid, glutaric acid, itaconic acid, maleic acid, malic acid, succinic acid, tartaric acid. Many other alternative absorption enhancers, plasticizers or antioxidants etc. could be used.
[0145] The non-adhesive backing layer was formed by i) spraying a 2.5% ethanolic solution of ethyl cellulose (Ethocel™, Colorcon Limited, UK) with 2% dibutyl phthalate (DBP, Merck KGaA, Germany) directly onto the surface of the mucoadhesive layer or the epinephrine base particle-containing layer, or ii) by spraying an ethanolic solution of amino methacrylate copolymer (Eudragit® L100-55, Evonik, Germany) to form an oro-dissolving backing layer. (Mašek et al. Multi-layered nanofibrous mucoadhesive films for buccal and sublingual administration of drug-delivery and vaccination nanoparticles—important step towards effective mucosal vaccines. J Control Release. 2017 Mar. 10; 249:183-195. doi: 10.1016/j.jconrel.2016.07.036). The non-adhesive backing layer was alternatively formed using solvent casting methodology and laminated to the mucoadhesive layer or the epinephrine base particle-containing layer.
[0146] Mucoadhesive layers were prepared by solvent casting. Carbomer (Carbopol® 974P, Lubrizol Advanced Materials, USA) and hypromellose 2208 (hydroxypropyl methylcellulose, viscosity 4000 mPa.Math.s, Methocel™ K4M, Colorcon Limited, UK) were combined in a 2:1 (w/w) ratio in water to form a viscous opaque solution. Glycerol at 15% (w/w) was added as a plasticizer and the combined mixture was then treated by sonication to remove air bubbles. The required volume was then poured into plastic Petri dishes. The excess water was removed by evaporation at a temperature of 37° C. to produce the desired mucoadhesive layers. It is noted that the mucoadhesive layer could contain other excipients, for example to modify pH or enhance absorption. Table I describes composition of the mucoadhesive layers:
TABLE-US-00001 TABLE I Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 72 hrs at 25° C.; solvent evaporation: 48 hrs at 37° C.) using water 0.592 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Carbomer 56.070 4.734 Hypromellose 2208 28.035 2.367 Glycerol 15.896 1.342 Total 100.000 8.443
[0147] Epinephrine base particle-containing layers were prepared using selected solvents/dispersants (see example 1) and polymers:
[0148] Formula I: Hypromellose 2910 (hydroxypropyl methylcellulose, viscosity 6 mPa.Math.s, Pharmacoat® 606, Shin-Etsu Chemical Co. Ltd., Japan) and hydroxypropyl cellulose (viscosity 300-600 mPa.Math.s, Klucel™ EF PHARM, Ashland, USA) in a 2:1 (w/w) ratio were added to the chosen solvent/disperant (ethanol, acetone, alkaline water of pH above 8.5 or mixture of thereof). Polyethylene glycol (PEG 600, Merck KGaA, Germany) at a concentration range of 12-17% (w/w) was added as a plasticizer. Sodium metabisulfite (Merck KGaA, Germany) in the concentration range of 0.007-2.284% was added as an antioxidant to stabilize the solution. Epinephrine base particles (Cambrex Profarmaco Milano S.r.l., Italy) were added at a concentration of 13.7-28.5% (w/w). Citric acid (Merck KGaA, Germany), ascorbic acid (Merck KGaA, Germany) and tartaric acid (Merck KGaA, Germany) was added to the mixture in the concentration range of 1.76-15.14% (w/w). Edetic acid (EDTA, Merck KGaA, Germany), sodium deoxycholate (Merck KGaA, Germany), polyoxyethylene (23) lauryl ether (Brij 35®, Merck KGaA, Germany), caprylocaproyl polyoxyl-8 glycerides NF (Labrasol®, Gattefossé, France) were added as absorption enhancers (2.5-2.9% w/w). The wet mixtures were then treated by sonication to remove air bubbles and the required volumes poured out into Petri dishes. The selected solvent/dispersant was then removed by evaporation at a temperature of 37° C. (ethanol, alkaline water of pH above 8.5) or at room temperature (acetone) to form the desired epinephrine base particle-containing layer. Each epinephrine base particle-containing oromucosal film layer contained 1.42-3.98 mg/cm.sup.2 of epinephrine base.
[0149] The following tables describes examples of the composition of the epinephrine base particle-containing layers:
TABLE-US-00002 TABLE II Epinephrine base particle-containing layer containing 18% of epinephrine base (1.99-3.98 mg/cm.sup.2) prepared by solvent casting method ((polymer swelling/dissolution conditions: 2 hrs at 25° C.; solvent evaporation: 3 hrs at 37° C.) using ethanol or ethanol/alkaline water mixture (80/20% v/v) 0.398 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Epinephrine base 18.019 1.988 Hypromellose 2910 44.446 4.904 Hydroxypropyl Cellulose 22.223 2.452 Sodium Metabisulfite 0.042 0.005 Polyethylene Glycol 15.271 1.685 Total 100.000 11.033 Epinephrine base 17.839 2.982 Hypromellose 2910 43.608 7.290 Hydroxypropyl Cellulose 21.804 3.645 Sodium Metabisulfite 1.070 0.179 Polyethylene Glycol 15.679 2.621 Total 100.000 16.716 Epinephrine base 17.858 3.976 Hypromellose 2910 44.644 9.940 Hydroxypropyl Cellulose 22.322 4.970 Sodium Metabisulfite 0.042 0.009 Polyethylene Glycol 15.134 3.370 Total 100.000 22.266
TABLE-US-00003 TABLE IIIa Examples of the preparation epinephrine base particle-containing layer with concentration of epinephrine base in the range of 13.7-22.6% prepared by solvent casting method (polymer swelling/dissolution conditions: 2 hrs at 25° C.; solvent evaporation 3 hrs at 37° C.) using ethanol 0.398 ml/cm.sup.2 or ethanol/alkaline water mixture (80/20% v/v): Material % of dry composition mg/cm.sup.2 film Epinephrine base 13.705 1.420 Hypromellose 2910 45.683 4.734 Hydroxypropyl Cellulose 22.841 2.367 Sodium Metabisulfite 2.284 0.237 Polyethylene Glycol 15.487 1.605 Total 100.000 10.362 Epinephrine base 22.623 2.982 Hypromellose 2910 40.218 5.302 Hydroxypropyl Cellulose 20.109 2.651 Sodium Metabisulfite 0.007 0.001 Polyethylene Glycol 17.043 2.247 Total 100.000 13.182
TABLE-US-00004 TABLE IIIb Examples of the preparation epinephrine base particle-containing layer with concentration of epinephrine base in range 14- 24.6% prepared by solvent casting method (solvent evaporation 2 hrs at 25° C.) using acetone 0.393 ml/cm.sup.2. Material % of dry composition mg/cm.sup.2 film Epinephrine base 14.025 1.887 Hypromellose 2910 46.751 6.290 Hydroxypropyl Cellulose 23.375 3.145 Sodium Metabisulfite 0.000 0.000 Polyethylene Glycol 15.848 2.132 Total 100.000 13.455 Epinephrine base 24.600 3.774 Hypromellose 2910 41.001 6.290 Hydroxypropyl Cellulose 20.500 3.145 Sodium Metabisulfite 0.000 0.000 Polyethylene Glycol 13.899 2.132 Total 100.000 15.342
TABLE-US-00005 TABLE IIIc Examples of the preparation micron-size epinephrine base particle- containing layer containing 1.66, 1.99, 2.99 mg/cm.sup.2 micronized epinephrine base in the range of 17.9-19.5% prepared by solvent casting method (polymer swelling/dissolution conditions: 2 hrs at 25° C.; solvent evaporation: 3 hrs at 37° C.) using ethanol/alkaline water mixture (80/20% v/v) or ethanol/alkaline water mixture (90/10% v/v) 0.398 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Epinephrine base 19.463 1.657 Hypromellose 2910 42.818 3.645 Hydroxypropyl Cellulose 21.409 1.822 Sodium Metabisulfite 1.051 0.089 Polyethylene Glycol 15.259 1.299 Total 100.000 8.512 Epinephrine base 17.898 1.988 Hypromellose 2910 43.551 4.838 Hydroxypropyl Cellulose 21.775 2.419 Sodium Metabisulfite 1.074 0.119 Polyethylene Glycol 15.702 1.744 Total 100.000 11.108 Epinephrine base 17.864 2.982 Hypromellose 2910 43.668 7.290 Hydroxypropyl Cellulose 21.834 3.645 Sodium Metabisulfite 1.072 0.179 Polyethylene Glycol 15.562 2.598 Total 100.000 16.693
[0150] The following tables describes the composition of the epinephrine base particle-containing layers in combination with other excipients:
TABLE-US-00006 TABLE IVa Examples of preparation of epinephrine base particle- containing layers with pH modifier (citric acid) prepared by solvent casting method (solvent evaporation: 2 hrs at 25° C.) using acetone 0.398 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Epinephrine base: citric acid 1:1 Epinephrine base 15.135 2.982 Hypromellose 2910 37.024 7.290 Hydroxypropyl Cellulose 18.487 3.645 Sodium Metabisulfite 0.914 0.179 Polyethylene Glycol 13.306 2.621 Citric Acid 15.135 2.982 Total 100.000 19.698 Epinephrine base: citric acid 10:1 Epinephrine base 17.519 2.982 Hypromellose 2910 42.857 7.290 Hydroxypropyl Cellulose 21.399 3.645 Sodium Metabisulfite 1.058 0.179 Polyethylene Glycol 15.403 2.621 Citric Acid 1.764 0.298 Total 100.000 17.015
TABLE-US-00007 TABLE IVb Examples of the preparation of epinephrine base particle- containing layers with absorption enhancers (sodium deoxycholate, edetic acid) prepared by solvent casting method (polymer swelling/dissolution conditions: 2 hrs at 25° C.; solvent evaporation: 3 hrs at 37° C.) using ethanol 0.398 ml/cm.sup.2 or ethanol/alkaline water mixture (80/20% v/v): Material % of dry composition mg/cm.sup.2 film Epinephrine base 17.316 2.982 Hypromellose 2910 42.359 7.290 Hydroxypropyl Cellulose 21.150 3.645 Sodium Metabisulfite 1.046 0.179 Polyethylene Glycol 15.224 2.621 Sodium Deoxycholate 2.905 0.497 Total 100.000 17.213 Epinephrine base 17.316 2.982 Hypromellose 2910 42.359 7.290 Hydroxypropyl Cellulose 21.150 3.645 Sodium Metabisulfite 1.046 0.179 Polyethylene Glycol 15.224 2.621 Edetic acid 2.905 0.497 Total 100.000 17.213
TABLE-US-00008 TABLE IVc Examples of the preparation of epinephrine base particle-containing layers with pH modifier (citric acid or tartaric acid or ascorbic acid) and absorption enhancers (sodium deoxycholate, edetic acid, polyoxyethylene lauryl ether - Brij 35 ®, caprylocaproyl polyoxyl-8 glycerides NF - Labrasol ®) prepared by solvent casting method (polymer swelling/dissolution conditions: 2 hrs at 25° C.; solvent evaporation: 3 hrs at 37° C.) using ethanol or acetone 0.398 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Epinephrine base 14.760 2.982 Hypromellose 2910 36.107 7.290 Hydroxypropyl Cellulose 18.029 3.645 Sodium Metabisulfite 0.892 0.179 Polyethylene Glycol 12.977 2.621 Citric Acid 14.760 2.982 Sodium Deoxycholate 2.476 0.497 Total 100.000 20.195 Epinephrine base 14.760 2.982 Hypromellose 2910 36.107 7.290 Hydroxypropyl Cellulose 18.029 3.645 Sodium Metabisulfite 0.892 0.179 Polyethylene Glycol 12.977 2.621 Citric Acid 14.760 2.982 Edetic acid 2.476 0.497 Total 100.000 20.195 Epinephrine base 15.943 2.982 Hypromellose 2910 38.973 7.290 Hydroxypropyl Cellulose 19.486 3.645 Sodium Metabisulfite 0.957 0.179 Polyethylene Glycol 14.012 2.621 Tartaric Acid 7.972 1.491 Polyoxyethylene lauryl ether 2.657 0.497 Total 100.000 18.704 Epinephrine base 16.744 2.982 Hypromellose 2910 40.930 7.290 Hydroxypropyl Cellulose 20.465 3.645 Sodium Metabisulfite 1.005 0.179 Polyethylene Glycol 14.716 2.621 Ascorbic Acid 3.349 0.596 Labrasol 2.791 0.497 Total 100.000 17.810
[0151] Formula II: Epinephrine base particle-containing layer containing only hypromellose 2910 (hydroxypropyl methylcellulose, viscosity 6 mPa s, Pharmacoat® 606, Shin-Etsu Chemical Co. Ltd., Japan) was prepared by solvent casting method.
TABLE-US-00009 TABLE Va Epinephrine base particle-containing layer with 18% of epinephrine base prepared by solvent casting method (polymer swelling/dissolution conditions: 2 hrs at 25° C.; solvent evaporation: 3 hrs at 37° C.) using ethanol or ethanol/alkaline water mixture (80/20% v/v) 0.398 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Epinephrine base 18.080 2.982 Hypromellose 2910 66.292 10.934 Sodium Metabisulfite 2.009 0.331 Polyethylene Glycol 13.620 2.247 Total 100.000 16.494
TABLE-US-00010 TABLE Vb Epinephrine base particle-containing layer with 28% of epinephrine base prepared by solvent casting method (polymer swelling/dissolution conditions: 2 hrs at 25° C.; solvent evaporation: 6 hrs at 37° C.) using ethanol or ethanol/alkaline water mixture (80/20% v/v) 0.469 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Epinephrine base 28.511 3.756 Hypromellose 2910 59.399 7.825 Sodium Metabisulfite 0.009 0.001 Polyethylene Glycol 12.082 1.592 Total 100.000 13.173
[0152] Formula III: Epinephrine base particle-containing layer with hypromellose 2910 (hydroxypropyl methylcellulose, viscosity 6 mPa s, Pharmacoat® 606, Shin-Etsu Chemical Co. Ltd., Japan) and hypromellose 2208 (hydroxypropyl methylcellulose, viscosity 4000 mPa.Math.s, Methocel™ K4M, Colorcon Limited, UK) was prepared by solvent casting method (polymer swelling/dissolution conditions: 2 hrs at 25° C.; solvent evaporation: 6 hrs at 37° C.) using ethanol or ethanol/alkaline water mixture (80/20% v/v) 0.592 ml/cm.sup.2 as described above for Formula I.
TABLE-US-00011 TABLE VI Material % of dry composition mg/cm.sup.2 film Epinephrine base 13.705 1.420 Hypromellose 2910 45.683 4.734 Hypromellose 2208 22.841 2.367 Sodium Metabisulfite 2.284 0.237 Polyethylene Glycol 15.487 1.605 Total 100.000 10.362
[0153] Formula IV: Epinephrine base particle-containing layer with hypromellose 2910 (hydroxypropyl methylcellulose, viscosity 6 mPa s, Pharmacoat® 606, Shin-Etsu Chemical Co. Ltd., Japan) and Povidon (Polyvinylpyrrolidone K 30, Merck KGaA, Germany) was prepared by solvent casting method (polymer swelling/dissolution conditions: 2 hrs at 25° C.; solvent evaporation: 3 hrs at 37°) using ethanol or ethanol/alkaline water mixture (80/20% v/v) 0.592 ml/cm.sup.2.
TABLE-US-00012 TABLE VII Material % of dry composition mg/cm.sup.2 film Epinephrine base 13.705 1.420 Hypromellose 2910 45.683 4.734 Povidon 22.841 2.367 Sodium Metabisulfite 2.284 0.237 Polyethylene Glycol 15.487 1.605 Total 100.000 10.362
Example 3
Dissolution of Epinephrine Base Particles Formulated as an Oromucosal Film/Polymeric Layer of the Invention
[0154] This dissolution study was performed to confirm the effect of pH modifiers and absorption enhancers on the dissolution rate of epinephrine base particles contained in oromucosal films of the invention. Epinephrine base particles formulated in an oromucosal film of the invention dissolve quickly and are released from the oromucosal film within minutes. Rapid release of epinephrine following in-vivo administration in patients suffering from anaphylactic shock is a key requirement for any anaphylaxis treatment.
[0155] The following oromucosal films were studied for dissolution rate and solubility with and without a pH modifier or absorption enhancer: [0156] i) Epinephrine base particles formulated in an oromucosal film. [0157] ii) Epinephrine base particles formulated in an oromucosal film with citric acid as a pH modifier. [0158] iii) Epinephrine base particles formulated in an oromucosal film with sodium deoxycholate as an absorption enhancer.
[0159] The standard USP dissolution test was modified to clearly show the effect of an acidifier (pH modifier) and an absorption enhancer on both the dissolution rate and solubility as follows:
[0160] The dissolution test was performed using either simulated saliva (pH 6.8) or citric acid solution (15 mg/ml) as the dissolution medium with 30 mg/ml sodium metabisulfite as antioxidant maintained at 37±0.5° C. The total volume used in all cases was 20 ml. The solutions were continually mixed using a magnetic stirrer (100 rpm) during the whole experiment. The oromucosal film was cut into a square of 1 cm.sup.2 and adhered to a glass plate held in position with double sided adhesive tape. 0.5 ml samples were withdrawn at time intervals of 0, 1, 2, 3, 4, 5, 10, 15 and 60 minutes with subsequent addition of 5 μl of 10% solution of formic acid into each sample. As each sample was withdrawn, it was replaced with the same volume of fresh medium. The concentration of epinephrine in each of the samples was measured by using liquid chromatography—tandem mass spectrometry (LCMS/MS).
Sample Preparation for LCMS/MS
[0161] 200 μl of dissolution medium was mixed with 100 μl (±)-epinephrine-D6 internal standard (concentration 10 μg/ml) and 1000 μl 2-propanol. The sample was vortexed and left at 6° C. for 30 minutes. The sample was then centrifuged for 30 minutes at 10 000 rpm at 4° C. After centrifugation extracts were dried under a stream of nitrogen, redissolved in 150 μl of 50% methanol with 0.1% formic acid and an aliquot of 5 μl was injected into the HPLC column.
LCMS/MS
[0162] Sample analyses were performed by using liquid chromatography-tandem mass spectrometry. An Agilent 1200 chromatographic system (Agilent Technologies, Germany), consisting of binary pump, vacuum degasser, autosampler and thermostatted column compartment, was used. Separation of epinephrine was carried out using an Ascentis Express C18, 2.1×150 mm, 2.7 μm particle size column (Supelco, Bellefonte, Pa., USA) with a 20-min linear gradient from 50 to 100% of methanol. Mobile phase contained 0.1% of formic acid. The flow rate of the mobile phase was 0.2 ml/min, the column temperature was set at 45° C. A triple quadrupole mass spectrometer Agilent 6410 Triple Quad LCMS (Agilent Technologies, USA) with an electrospray interface (ESI) was used for detection of the analyte. Epinephrine (MRM transition m/z 166−57) and internal standard (172−157) were detected using multi reaction monitoring mode.
[0163] The standard USP dissolution test was modified to simulate the effect of a limited amount of fluid following administration of the film to oral mucosa in vivo; lowering the total volume in the dissolution test better mimics in-vivo conditions. The 20 ml volume of dissolution media was considered as a good compromise between both the standard USP dissolution test and the real in-vivo conditions occurring in the oral mucosa. This volume was also considered appropriate to demonstrate the effect of citric acid as a pH modifier and the effect of deoxycholate sodium as a absorption enhancer.
[0164] The following formulations of epinephrine base particles as oromucosal films were tested: [0165] 1) The composition of the film layer containing epinephrine base particles
TABLE-US-00013 Material % of dry composition mg/cm.sup.2 film Epinephrine base 17.83 2.98 Pharmacoat 606 43.63 7.29 Klucel EF 21.78 3.64 Sodium metabisulfite 1.08 0.18 PEG 600 15.68 2.62 Total 100.00 16.71 [0166] 2) The composition of the oromucosal films containing epinephrine base particles co-formulated with a pH modifier (citric acid)
TABLE-US-00014 Material % of dry composition mg/cm.sup.2 film Epinephrine base 15.13 2.98 Pharmacoat 606 37.02 7.29 Klucel EF 18.49 3.64 Sodium metabisulfite 0.91 0.18 PEG 600 13.31 2.62 Citric acid 15.13 2.98 Total 100.00 19.69 [0167] 3) The composition of the oromucosal film layer containing epinephrine base particles co-formulated with an absorption enhancer (sodium deoxycholate)
TABLE-US-00015 Material % of dry composition mg/cm.sup.2 film Epinephrine base 17.32 2.98 Pharmacoat 606 42.36 7.29 Klucel EF 21.15 3.64 Sodium metabisulfite 1.05 0.18 PEG 600 15.22 2.62 Sodium deoxycholate 2.91 0.5 Total 100.00 17.21
[0168] The most significant difference in dissolution profile is seen when comparing the epinephrine base particle-containing film formulated with citric acid and when the dissolution test was performed in citric acid solution as a dissolution medium. These conditions help in understanding the behavior of epinephrine base particles formulated as an oromucosal film administered to oral mucosa with the presence of limited amounts of fluid. The results show that citric acid solution has a significantly positive effect on the dissolution rate and solubility of epinephrine base particles. The artificial saliva solution (pH 6.8) showed no significant impact on dissolution rate or solubility. To conclude, the presence of pH modifiers (acidifiers), as demonstrated by the example of citric acid here, is beneficial for the dissolution rate and increased local solubility of epinephrine base particles.
[0169]
[0170]
Example 4
Ex-Vivo Absorption of Epinephrine Base Particles Formulated in an Oromucosal Film of the Invention
[0171] The objective of this study was to study the effect of absorption enhancers on the absorption rate of epinephrine base solid particles formulated as an oromucosal film according to the present invention following the application (administration) of the film onto excised sublingual porcine mucosa ex-vivo using a diffusion cell model.
Methods
[0172] Porcine sublingual mucosa was removed immediately after sacrifice. The mucosa was then prepared and mounted to the diffusion cell with the receptor compartment having a volume of 2 mL, containing both citric acid solution (3 mg/ml) and sodium metabisulfite (30 mg/ml). The oromucosal film (1 cm.sup.2, 2.98 mg of epinephrine base) formulation of epinephrine base particles was then applied to the surface of the sublingual mucosa and moistened with 50 ul of artificial saliva solution (buffer, pH 6.8). The rate of absorption was assessed by measuring the increasing concentration of epinephrine in the receptor compartment under constant mixing at 37° C. Samples were taken at 0, 1, 3, 5, 8, 11, 14, 17 and 20 minutes, added 5 μl 10% solution of formic acid, to measure the concentration of epinephrine in the receptor chamber. The concentration level was determined as described in Example 3.
Sample Preparation for LCMS/MS
[0173] 200 μl of fluid from receptor chamber was mixed with 100 μl (±)-epinephrine-D6 internal standard (concentration 10 μg/ml) and 1000 μl 2-propanol. The sample was vortexed and left at 6° C. for 30 minutes. The sample was then centrifuged for 30 minutes at 10000 rpm at 4° C. After centrifugation extracts were dried under a stream of nitrogen, redissolved in 150 μl of 50% methanol with 0.1% formic acid and an aliquot of 5 μl was injected into the HPLC column.
[0174] The following formulations of epinephrine base particles as oromucosal films were tested: [0175] 1) The composition of the oromucosal film layer containing epinephrine base particles
TABLE-US-00016 Material % of dry composition mg/cm.sup.2 film Epinephrine base 17.83 2.98 Pharmacoat 606 43.63 7.29 Klucel EF 21.78 3.64 Sodium metabisulfite 1.08 0.18 PEG 600 15.68 2.62 Total 100.00 16.71 [0176] 2) The composition of the oromucosal film layer containing epinephrine base particles co-formulated with a absorption enhancer (sodium deoxycholate)
TABLE-US-00017 Material % of dry composition mg/cm.sup.2 film Epinephrine base 17.32 2.98 Pharmacoat 606 42.36 7.29 Klucel EF 21.15 3.64 Sodium metabisulfite 1.05 0.18 PEG 600 15.22 2.62 Sodium deoxycholate 2.91 0.5 Total 100.00 17.21 [0177] 3) The composition of the oromucosal film layer containing epinephrine base particles co-formulated with pH modifier (citric acid) and absorption enhancer (edetic acid)
TABLE-US-00018 Material % of dry composition mg/cm.sup.2 film Epinephrine base 14.760 2.982 Hypromellose 2910 36.107 7.290 Hydroxypropyl Cellulose 18.029 3.645 Sodium Metabisulfite 0.892 0.179 Polyethylene Glycol 12.977 2.621 Citric acid 14.760 2.982 Edetic acid 2.476 0.497 Total 100.000 20.195
Results
[0178]
[0179] Surprisingly, the absorption of epinephrine through sublingual mucosa ex-vivo was observed within a minute of the administration of the oromucosal film formulation of the invention comprising epinephrine base particles. The absorption of significant levels of epinephrine occurred within 1-3 minutes following administration of the film. The level of epinephrine was quantifiable after the first minute, with only a very slight lag followed by a linear increase in permeated epinephrine (
Conclusion
[0180] Surprisingly, epinephrine in the form of solid epinephrine base particles formulated in an oromucosal film of the invention is able to permeate within 1-3 minutes from when it is applied to sublingual porcine mucosa ex-vivo. It was also demonstrated that absorption enhancers significantly increase the absorption rate of epinephrine, even though it is formulated as solid particles (in the oromucosal film) and hence needs to dissolve directly at the site of administration.
Example 5
Pharmacokinetic Study of Epinephrine Base Particles Formulated in an Oromucosal Film of the Invention
[0181] The pharmacokinetic profile of epinephrine base particles formulated in an oromucosal film of the invention was compared to an intramuscular injection of epinephrine using a pharmacokinetic model in piglets (Sus scrofa domesticus). Blood plasma concentrations of epinephrine were measured following administration of the formulations to the sublingual mucosa and muscle, respectively. The study compared EpiPen 0.3 mg (Mylan) with an epinephrine oromucosal film (8 mg) containing epinephrine base particles.
[0182] The oromucosal film was formulated as a tri-layered film. The following formulations of epinephrine base particles as oromucosal films were tested:
The composition of the film layer containing epinephrine base particles, for sublingual application two mucoadhesive films were applied simultaneously (2×4 mg of epinephrine base):
TABLE-US-00019 Material % of dry composition mg/cm.sup.2 film Epinephrine base 13.70 1.42 Hypromellose 2910 45.68 4.73 Hydroxypropyl Cellulose 22.84 2.37 Sodium Metabisulfite 2.28 0.24 Polyethylene Glycol 15.49 1.61 Total 100.00 10.36
[0183] The oromucosal film was formulated as described in Example 2. The size of the film layer containing epinephrine base particles used in the experiment: 2.5 cm×1.1 cm.
[0184] Piglets weighing 18-20 Kg (n=3) were utilized. The piglets were anesthetized by intramuscular injection and plasma levels of endogenous epinephrine were monitored prior to epinephrine administration (sublingual or intramuscular). Samples of 200 μl of blood plasma were taken and epinephrine levels were measured using mass spectrometry.
Sample Preparation for LCMS/MS
[0185] 200 μl of plasma was mix with 100 μl (±)-Epinephrine-D6 internal standard (concentration 10 μg/ml) and 1000 μl 2-propanol. The sample was vortexed and left at 6° C. for 30 minutes. The sample was then centrifuged for 30 minutes at 10000 rpm at 4° C. After centrifugation extracts were dried under a stream of nitrogen, redissolved in 150 μl of 50% methanol with 0.1% formic acid and an aliquot of 5 μl was injected into the HPLC column. The concentration level was determined as described in Example 3.
[0186] The epinephrine formulations were administered to the animals only after endogenous levels of epinephrine decreased to less than 10 ng/ml; this took approximately 20 mins following anesthesia of the animals. The initial high levels of endogenous epinephrine probably occurred due to stress caused by the physical manipulation of the animals prior to anesthesia.
[0187]
[0188] The results show increased plasma concentrations of both sublingually administered epinephrine base particles formulated in an oromucosal film (
Example 6
Plasma Levels of Epinephrine Following the Administration of Epinephrine Base Particle-Containing Oromucosal Film of the Invention to Rabbits
[0189] To prove the efficacy of the oromucosal epinephrine base particle-containing film formulation of the invention, plasma concentration of epinephrine following sublingual administration was studied using a rabbit model. The study compares 6 mg epinephrine base particle-containing film and a placebo film.
[0190] The oromucosal film was formulated as a tri-layered film. Composition of the film layer containing epinephrine base particles for sublingual application—two mucoadhesive films were applied simultaneously (2×3 mg of epinephrine base):
TABLE-US-00020 Material % of dry composition mg/cm.sup.2 film Epinephrine base 17.839 2.982 Hypromellose 2910 43.608 7.290 Hydroxypropyl Cellulose 21.804 3.645 Sodium Metabisulfite 1.070 0.179 Polyethylene Glycol 15.679 2.621 Total 100.000 16.716
[0191] The size of the film layer containing epinephrine base particles used in the experiment: 0.8 cm×1.3 cm.
[0192] New Zealand rabbits weighing 5-6 Kg were used in this experiment. The rabbits were anesthetized using an intramuscular injection of Ketamine and Xylazine. Epinephrine/placebo film was administered approximately 30 mins after the animals were anesthetized. The plasma level of epinephrine was determined 10 minutes prior to the sublingual administration of the oromucosal epinephrine base particle-containing film and once every 10 minutes for 60 minutes after administration. 200 μl samples of blood plasma were taken for analysis at each interval. Mass spectrometry and the same analytical protocol as described in Example 5 was utilized to determine plasma levels of epinephrine.
[0193]
Example 7
Design of Mucoadhesive Films with pH Modifier Formulated in the Backing Layer and Effect of pH Modifier on Dissolution of Epinephrine Base Particles after Administration Ex Vivo
[0194] Each tested bi-layered film consists of 1) a backing layer, and 2) an Epinephrine base particle-containing mucoadhesive layer. The backing layer contains a pH modifier. Citric acid was used as an example of a pH modifier. Both layers, the non-adhesive backing layer, and mucoadhesive epinephrine particle-containing layers were prepared using the solvent casting method. [0195] 1) The Composition of the Backing Layer with Citric:
TABLE-US-00021 TABLE VIII The backing layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 4 hrs at 37° C. or 1 hrs at 60° C.) using ethanol and water mixture (80/20% v/v) 0.331 ml/cm2: Material % of dry composition mg/film unit Citric acid 14.7 10.06 Pharmacoat 606 46.8 31.93 Klucel EF 23.4 15.96 PEG 600 15.1 10.28 Total 100.0 — Citric acid 16.5 10.06 Pharmacoat 606 52.5 31.93 Klucel EF 26.3 15.96 Glycerol 99.7% 4.7 2.84 Total 100.0 — Citric acid 22.1 10.06 Pharmacoat 606 48.6 22.09 Klucel EF 24.3 11.04 Glycerol 99.7% 5.0 2.30 Total 100.0 — [0196] 2) The Composition of the Mucoadhesive Film Layers Containing Epinephrine Base Particles:
TABLE-US-00022 TABLE IX The mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 4 hrs at 37° C. or 1 hrs at 60° C.) using ethanol and alkaline water mixture (80/20% v/v) 0.331 ml/cm.sup.2: Material % of dry composition mg/film unit Composition 1A-2 Epinephrine base 20.1 10.06 Pharmacoat 606 41.5 20.78 Klucel EF 14.0 7.00 Sodium Metabisulfite 1.2 0.60 Transcutol HP 9.2 4.59 PEG 600 14.0 7.00 Total 100.0 — Composition 1B-2 Epinephrine base 24.8 10.06 Pharmacoat 606 51.1 20.78 Klucel EF 17.2 7.00 Sodium Metabisulfite 1.5 0.60 Glycerol 99.7% 5.4 2.19 Total 100.0 — Composition 1C-2 Epinephrine base 22.2 10.06 Pharmacoat 606 45.9 20.78 Klucel EF 15.5 7.00 Sodium Metabisulfite 1.3 0.60 Glycerol 99.7% 4.8 2.19 Transcutol HP 10.2 4.59 Total 100.0 — Composition 2A-2 Epinephrine base 16.7 10.06 Pharmacoat 606 45.7 27.55 Klucel EF 15.2 9.18 Sodium Metabisulfite 1.0 0.60 PEG 600 13.8 8.31 Transcutol HP 7.6 4.59 Total 100.0 — Composition 2B-2 Epinephrine base 20.3 10.06 Pharmacoat 606 55.6 27.55 Klucel EF 18.5 9.18 Sodium Metabisulfite 1.2 0.60 Glycerol 99.7% 4.4 2.19 Total 100.0 — Composition 2C-2 Epinephrine base 18.4 10.06 Pharmacoat 606 50.4 27.55 Klucel EF 16.8 9.18 Sodium Metabisulfite 1.2 0.66 Glycerol 99.7% 4.8 2.62 Transcutol HP 8.4 4.59 Total 100.0 — Composition 3A-2 Epinephrine base 13.7 10.06 Pharmacoat 606 43.5 31.93 Klucel EF 21.7 15.96 Sodium Metabisulfite 0.8 0.60 PEG 600 14.0 10.28 Transcutol HP 6.3 4.59 Total 100.0 — [0197] 3) The Lamination of the Film Layers
[0198] The lamination of the mucoadhesive layer and the backing layer was performed using binding solution. Several alternative for lamination layers are shown below:
Binding Solutions for Lamination:
[0199] a) Pure Ethanol 96%, or pure Ethylacetate
[0200] b) Solution of Kollidon VA 64, and PEG 600 in Ethylacetate,
TABLE-US-00023 Component Percentage (%) Kollidon VA 64 3 PEG 600 15 Ethyl acetate 82 Total 100
[0201] c) Solution of Kollidon VA 64, Glycerol in Etanol 96%.
TABLE-US-00024 Component Percentage (%) Kollidon VA 64 3 Glycerol 99.7% 15 Ethanol 96% 82 Total 100
[0202] The binding solution is applied to the surface of the film layer preferably by spraying.
[0203] The design of the bi-layered mucoadhesive orodispersible film including a thin binding layer formed using the binding solution is presented in
[0205] NMR analysis was used to confirm crystalline state of Epinephrine base following lamination of the films.
The Compositions Tested:
A) Mucoadhesive Layer:
Composition 2C-2
[0206]
TABLE-US-00025 Material % of dry composition mg/film unit Epinephrine base 18.4 10.06 Pharmacoat 606 50.4 27.55 Klucel EF 16.8 9.18 Sodium Metabisulfite 1.2 0.66 Glycerol 99.7% 4.8 2.62 Transcutol HP 8.4 4.59 Total 100.0 —
B) Binding Solution: Ethanol 96%
[0207] C) Backing Layer with Citric Acid:
TABLE-US-00026 Material % of dry composition mg/film unit Citric acid 14.7 10.06 Pharmacoat 606 46.8 31.93 Klucel EF 23.4 15.96 PEG 600 15.1 10.28 Total 100.0 —
D) Controls for the NMR Analysis:
[0208] As a placebo film, the same composition of mucoadhesive film layer was used in the experiment, but without Epinephrine base.
[0209] As a film formulation with dissolved Epinephrine base (solid dispersion system), the same composition of mucoadhesive film layer was used, but with addition of citric acid (10 mg/film unit) into the solution of polymers used for manufacturing of the film using solvent casting.
E) Conclusion:
[0210] The NMR analysis of
[0212] Ex vivo application of the film on the oral mucosa was performed to determine the effect of citric acid in the backing layer on the dissolution rate of the Epinephrine base in the mucoadhesive layer. The bi-layered film was applied onto porcine tongue as a model of the oral mucosa. The film was moistened by spraying a small amount of water at intervals of 2 minutes to mimic the environment in the oral cavity. The dissolution of Epinephrine base particles within the film was observable by the eye as the color of the film changed from white to transparent. The following tables describe the composition of films tested, and
TABLE-US-00027 TABLE X The mucoadhesive layer was prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 4 hrs at 37° C.) using ethanol and alkaline water mixture (80/20% v/v) 0.331 ml/cm.sup.2: Material % of dry composition mg/film unit Epinephrine base 13.7 10.06 Pharmacoat 606 43.5 31.93 Klucel EF 21.7 15.96 Sodium Metabisulfite 0.8 0.60 PEG 600 14.0 10.28 Transcutol HP 6.3 4.59 Total 100.0 — [0214] B) The Composition of the Backing Film Layer Containing pH Modifier Citric Acid (10 mg/Film, 5 mg/Film, 1.5 mg/Film):
TABLE-US-00028 TABLE XI The backing layer was prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 4 hrs at 37° C.) using ethanol and water mixture (80/20% v/v) 0.331 ml/cm.sup.2: Material % of dry composition mg/film unit 1. Backing layer with citric acid (10 mg/film) Citric acid 14.7 10.06 Pharmacoat 606 46.8 31.93 Klucel EF 23.4 15.96 PEG 600 15.1 10.28 Total 100.0 — 2. Backing layer with citric acid (5 mg/film) Citric acid 8.0 5.03 Pharmacoat 606 50.5 31.93 Klucel EF 25.2 15.96 PEG 600 16.3 10.28 Total 100.0 — 3. Backing layer with citric acid (1.5 mg/film) Citric acid 2.6 1.53 Pharmacoat 606 53.5 31.93 Klucel EF 26.7 15.96 PEG 600 17.2 10.28 Total 100.0 —
[0216] Crystalline state of Epinephrine base in the film can be easily observed (white color) as shown in the
Example 8
Preparation of Film Compositions with Lidocaine Hydrochloride and/or Prilocaine Hydrochloride, Epinephrine Base and Absorption Enhancers
[0217] Various film formulations were prepared to show compatibility of Lidocaine HCl with Prilocaine HCl, Epinephrine base, and selected absorption enhancers and film-forming excipients in the formulation. Two-layered design of the film was prepared: each of prepared two-layered films consisted of 1) a backing layer and 2) a mucoadhesive active pharmaceutical ingredient (API)-containing layer.
Non-Adhesive Backing Layers were Prepared by:
1) spraying a 2.5% ethanolic solution of Ethylcellulose (Ethocel™, Colorcon Limited, UK) with 2% Dibutyl phthalate (DBP, Merck KgaA, Germany) directly onto the surface of a mucoadhesive layer as an example of the non-soluble layer;
2) using the solvent casting method using ethanol/water solution or water with the combination of Hypromellose 2910 (Pharmacoat® 606, ShinEtsu, Japan) and Hydroxypropyl Cellulose (Klucel™ EF PHARM, Ashland, USA) in a 2:1 or 3:1 (w/w) ratio. Glycerol 99.5% was used at 1.8-6.7% (w/w) as plasticizer as an example of a soluble backing layer. The backing layer was then laminated with the mucoadhesive layer using a binding solution as exemplified in example 7.3) above.
Mucoadhesive API-containing layers were prepared by solvent casting method using ethanolic water or water solution with the combination of Hypromellose 2910 (Pharmacoat® 606, ShinEtsu, Japan) and Hydroxypropyl Cellulose (Klucel™ EF PHARM, Ashland, USA) in a 2:1 or 3:1 (w/w) ratio. Glycerol 99.5% was used at 1.8-6.7% (w/w) as plasticizer. Transcutol® HP, Sodium deoxycholate, Eugenol, Labrasol, Disodium ethylenediaminetetraacetic acid salt or combinations thereof were added as absorption enhancers. The combination mixture was then treated by sonication to remove air bubbles and required volumes were poured out into plastic dishes. Organic solvent/water mixture or water used as solvent were removed by evaporation at temperature 37° C./60° C. leading to the formation of the desired mucoadhesive API-containing layers.
The following table describes examples of the composition layers containing Lidocaine Hydrochloride Prilocaine Hydrochloride, Epinephrine base and absorption enhancers:
TABLE-US-00029 TABLE XIIa Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 24 hrs at 37° C.) using water 0.331 ml/cm.sup.2 Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 31.77 8.28 Prilocaine Hydrochloride 31.77 8.28 Pharmacoat ® 606 18.55 4.84 Klucel ™ EF 9.28 2.42 Epinephrine base 0.95 0.25 Sodium metabisulfite 0.06 0.01 Transcutol HP 5.08 1.33 Glycerol 2.54 0.66 Total 100.00 26.07
TABLE-US-00030 TABLE XIIb Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 24 hrs at 37° C.) using water 0.331 ml/cm.sup.2 Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 30.12 8.28 Prilocaine Hydrochloride 30.12 8.28 Pharmacoat ® 606 17.59 4.84 Klucel ™ EF 8.80 2.42 Epinephrine base 0.90 0.25 Sodium metabisulfite 0.05 0.01 Transcutol HP 10.00 2.75 Glycerol 2.41 0.66 Total 100.00 27.49
TABLE-US-00031 TABLE XIIc Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 24 hrs at 37° C.) using water 0.331 ml/cm.sup.2 Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 32.98 8.28 Prilocaine Hydrochloride 32.98 8.28 Pharmacoat ® 606 19.26 4.84 Klucel ™ EF 9.63 2.42 Epinephrine base 0.99 0.25 Sodium metabisulfite 0.06 0.01 Deoxycholate sodium 1.45 0.37 Glycerol 2.64 0.66 Total 100.00 25.11
TABLE-US-00032 TABLE XIId Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; evaporation: 24 hrs at 37° C.) using water 0.331 ml/cm.sup.2 Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 38.20 14.21 Prilocaine Hydrochloride 38.20 14.21 Pharmacoat ® 606 13.00 4.84 Klucel ™ EF 6.50 2.42 Epinephrine base 0.67 0.25 Sodium metabisulfite 0.04 0.01 Deoxycholate sodium 1.60 0.60 Glycerol 1.78 0.66 Total 100.00 37.20
TABLE-US-00033 TABLE XIIe Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; evaporation: 24 hrs at 37° C.) using water 0.331 ml/cm.sup.2 Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 37.67 14.21 Prilocaine Hydrochloride 37.67 14.21 Pharmacoat ® 606 12.82 4.84 Klucel ™ EF 6.41 2.42 Epinephrine base 0.66 0.25 Sodium metabisulfite 0.04 0.01 Deoxycholate sodium 2.99 1.13 Glycerol 1.76 0.66 Total 100.00 37.73
TABLE-US-00034 TABLE XIIf Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 2 hrs at 60° C.) using ethanol and alkaline water (80/20% v/v) 0.331 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 36.00 5.00 Pharmacoat ® 606 34.80 4.84 Klucel ™ EF 17.40 2.42 Epinephrine base 1.79 0.25 Sodium metabisulfite 0.24 0.03 Transcutol ® HP 5.01 0.7 Glycerol 4.77 0.76 Total 100.00 14.00
TABLE-US-00035 TABLE XIIg Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 2 hrs at 60° C.) using ethanol and alkaline water (80/20% v/v) 0.331 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 33.74 5.00 Pharmacoat ® 606 32.63 4.84 Klucel ™ EF 16.31 2.42 Epinephrine base 1.68 0.25 Sodium metabisulfite 0.22 0.03 Transcutol ® HP 10.28 1.52 Glycerol 5.14 0.76 Total 100.00 14.46
TABLE-US-00036 TABLE XIIh Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 2 hrs at 60° C.) using ethanol and alkaline water (80/20% v/v) 0.331 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 36.52 5.00 Pharmacoat ® 606 35.31 4.84 Klucel ™ EF 17.65 2.42 Epinephrine base 1.81 0.25 Sodium metabisulfite 0.24 0.03 Sodium deoxycholate 3.14 0.43 Glycerol 5.32 0.73 Total 100.00 13.70
TABLE-US-00037 TABLE XIIi Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 2 hrs at 60° C.) using ethanol and alkaline water (80/20% v/v) 0.331 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 36.52 5.00 Pharmacoat ® 606 35.31 4.84 Klucel ™ EF 17.65 2.42 Epinephrine base 1.81 0.25 Sodium metabisulfite 0.24 0.03 Labrasol 3.14 0.43 Glycerol 5.32 0.73 Total 100.00 13.70
TABLE-US-00038 TABLE XIIj Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 2 hrs at 60° C.) using ethanol and alkaline water (80/20% v/v) 0.331 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 35.40 5.00 Pharmacoat ® 606 34.23 4.84 Klucel ™ EF 17.12 2.42 Epinephrine base 1.76 0.25 Sodium metabisulfite 0.23 0.03 Eugenol 6.10 0.86 Glycerol 5.16 0.73 Total 100.00 14.13
TABLE-US-00039 TABLE XIIk Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 2 hrs at 60° C.) using ethanol and alkaline water (80/20% v/v) 0.331 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 24.18 5.00 Prilocaine Hydrochloride 24.18 5.00 Pharmacoat ® 606 23.38 4.84 Klucel ™ EF 11.69 2.42 Epinephrine base 1.20 0.25 Sodium metabisulfite 0.16 0.03 Transcutol HP 10.09 2.09 Glycerol 5.12 1.06 Total 100.00 20.69
TABLE-US-00040 TABLE XIIl Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 2 hrs at 60° C.) using ethanol and alkaline water (80/20% v/v) 0.331 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 31.77 8.28 Prilocaine Hydrochloride 31.77 8.28 Pharmacoat ® 606 18.55 4.84 Klucel ™ EF 9.28 2.42 Epinephrine base 0.95 0.25 Sodium metabisulfite 0.06 0.01 Transcutol HP 5.08 1.33 Glycerol 2.54 0.66 Total 100.00 26.07
TABLE-US-00041 TABLE XIIm Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 2 hrs at 60° C.) using ethanol and alkaline water (80/20% v/v) 0.331 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 30.12 8.28 Prilocaine Hydrochloride 30.12 8.28 Pharmacoat ® 606 17.59 4.84 Klucel ™ EF 8.80 2.42 Epinephrine base 0.90 0.25 Sodium metabisulfite 0.05 0.01 Transcutol HP 10.00 2.75 Glycerol 2.41 0.66 Total 100.00 27.49
TABLE-US-00042 TABLE XIIn Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 2 hrs at 60° C.) using ethanol and alkaline water (80/20% v/v) 0.331 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 32.98 8.28 Prilocaine Hydrochloride 32.98 8.28 Pharmacoat ® 606 19.26 4.84 Klucel ™ EF 9.63 2.42 Epinephrine base 0.99 0.25 Sodium metabisulfite 0.06 0.01 Deoxycholate sodium 1.45 0.37 Glycerol 2.64 0.66 Total 100.00 25.11
TABLE-US-00043 TABLE XIIo Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; evaporation: 2 hrs at 60° C.) using ethanol and alkaline water (80/20% v/v) 0.331 ml/cm.sup.2: Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 38.20 14.21 Prilocaine Hydrochloride 38.20 14.21 Pharmacoat ® 606 13.00 4.84 Klucel ™ EF 6.50 2.42 Epinephrine base 0.67 0.25 Sodium metabisulfite 0.04 0.01 Deoxycholate sodium 1.60 0.60 Glycerol 1.78 0.66 Total 100.00 37.20
TABLE-US-00044 TABLE XIIp Mucoadhesive layer prepared by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; evaporation: 2 hrs at 60° C.) using ethanol and alkaline water (80/20% v/v) 0.331 ml/cm.sup.2 Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 37.67 14.21 Prilocaine Hydrochloride 37.67 14.21 Pharmacoat ® 606 12.82 4.84 Klucel ™ EF 6.41 2.42 Epinephrine base 0.66 0.25 Sodium metabisulfite 0.04 0.01 Deoxycholate sodium 2.99 1.13 Glycerol 1.76 0.66 Total 100.00 37.73
Example 9
Pharmacokinetic Study of Lidocaine Hydrochloride Containing Film of the Invention
[0218] The pharmacokinetic profile of Lidocaine Hydrochloride formulated in mucoadhesive film was determined using a pharmacokinetic model in piglets (Sus scrofa domesticus). Blood plasma concentrations of Lidocaine Hydrochloride were measured following administration of the film formulations to the gum in the area of front teeth (mandibula). The absorption of lidocaine into blood circulation confirms the local absorption into the deeper layers of the tissue. The mucoadhesive film was formulated as a bi-layered film. 1 cm×2 cm size of the film layer containing Lidocaine Hydrochloride was used in the experiment. The composition of the film layer containing Lidocaine Hydrochloride, a mucoadhesive film was applied (46 mg of Lidocaine Hydrochloride with/without 0.5 mg Epinephrine base with/without Transcutol as a absorption enhancer). The thickness of the mucoadhesive film was 160 μm.
The following formulations of Lidocaine Hydrochloride in mucoadhesive films were tested:
Mucoadhesive layer was formulated by solvent casting method (polymer swelling/dissolution conditions: 3 hrs at 25° C.; solvent evaporation: 24 hrs at 37° C.) using water 0.331 ml/cm.sup.2.
Composition of Film Containing Lidocaine HCl
[0219]
TABLE-US-00045 Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 77.85 28.41 Pharmacoat ® 606 13.26 4.84 Klucel ™ EF 6.63 2.42 Epinephrine base 0.00 0.00 Sodium Metabisulfite 0.00 0.00 Transcutol HP 0.00 0.00 Glycerol 2.27 0.83 Total 100.00 36.50
Composition of Film Containing Lidocaine HCl+Epinephrine Base
[0220]
TABLE-US-00046 Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 77.25 28.41 Pharmacoat ® 606 13.15 4.84 Klucel ™ EF 6.58 2.42 Epinephrine base 0.68 0.25 Sodium Metabisulfite 0.09 0.03 Transcutol HP 0.00 0.00 Glycerol 2.25 0.83 Total 100.00 36.78
Composition of Film Containing Lidocaine HCl+Epinephrine Base+Transcutol HP
[0221]
TABLE-US-00047 Material % of dry composition mg/cm.sup.2 film Lidocaine Hydrochloride 75.22 28.41 Pharmacoat ® 606 12.81 4.84 Klucel ™ EF 6.40 2.42 Epinephrine base 0.66 0.25 Sodium Metabisulfite 0.09 0.03 Transcutol HP 2.63 0.99 Glycerol 2.19 0.83 Total 100.00 37.77
Pharmacokinetic profile of Lidocaine following administration of the prepared films is shown in
Conclusion
[0222] Effective absorption of Lidocaine through the oral mucosa of the gum was shown from the tested mucoadhesive film using a porcine animal model. Moreover, the effect of both, Transcutol as a absorption enhancer, and Epinephrine as a peripheral vasoconstrictor was clearly shown. From the data in
[0223] a) Epinephrine base decreases the systemic absorption of Lidocaine from the site of absorption (gum), and
[0224] b) absorption enhancer, Transcutol®, significantly promotes local absorption leading to increase in plasma concentration of Lidocaine.
When absorption enhancer and peripheral vasoconstrictor are combined, the effect on the plasma concentration of lidocaine can be observed as shown in the graph. Therefore, the combination of local anesthetic (e.g. Lidocaine) with absorption enhancer (e.g. Transcutol), and/or peripheral vasoconstrictor (e.g. Epinephrine) can be advantageous in terms of achieving high local concentration of local anesthetic with reduced systemic absorption.