WO2008079295A1 - Stable anti-nausea oral spray formulations and methods - Google Patents

Stable anti-nausea oral spray formulations and methods Download PDF

Info

Publication number
WO2008079295A1
WO2008079295A1 PCT/US2007/026070 US2007026070W WO2008079295A1 WO 2008079295 A1 WO2008079295 A1 WO 2008079295A1 US 2007026070 W US2007026070 W US 2007026070W WO 2008079295 A1 WO2008079295 A1 WO 2008079295A1
Authority
WO
WIPO (PCT)
Prior art keywords
ondansetron
oral spray
spray
formulation
concentration
Prior art date
Application number
PCT/US2007/026070
Other languages
French (fr)
Inventor
Frank E. Blondino
Carrie Chen
Original Assignee
Novadel Pharma Inc.
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by Novadel Pharma Inc. filed Critical Novadel Pharma Inc.
Priority to JP2009542925A priority Critical patent/JP2010513525A/en
Priority to EP07863183A priority patent/EP2124897A4/en
Priority to CA2673049A priority patent/CA2673049C/en
Publication of WO2008079295A1 publication Critical patent/WO2008079295A1/en

Links

Classifications

    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/0012Galenical forms characterised by the site of application
    • A61K9/0053Mouth and digestive tract, i.e. intraoral and peroral administration
    • A61K9/006Oral mucosa, e.g. mucoadhesive forms, sublingual droplets; Buccal patches or films; Buccal sprays
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/06Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite
    • A61K47/08Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite containing oxygen, e.g. ethers, acetals, ketones, quinones, aldehydes, peroxides
    • A61K47/10Alcohols; Phenols; Salts thereof, e.g. glycerol; Polyethylene glycols [PEG]; Poloxamers; PEG/POE alkyl ethers
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/06Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite
    • A61K47/26Carbohydrates, e.g. sugar alcohols, amino sugars, nucleic acids, mono-, di- or oligo-saccharides; Derivatives thereof, e.g. polysorbates, sorbitan fatty acid esters or glycyrrhizin
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P1/00Drugs for disorders of the alimentary tract or the digestive system
    • A61P1/08Drugs for disorders of the alimentary tract or the digestive system for nausea, cinetosis or vertigo; Antiemetics

Definitions

  • the field of this invention is anti-nausea oral spray pharmaceutical formulations, methods of manufacturing such formulations, and their use in treating and preventing nausea and other conditions in human and non-human mammals.
  • Preferred embodiments of the invention provide stable formulations of ondansetron hydrochloride and pharmaceutically acceptable salts thereof suitable for oral administration, and related methods of preparation and administration of ondansetron hydrochloride formulations.
  • the invention provides stable, oral spray formulations in a simple, elegant format for fast onset of the active ingredient via absorption to the systemic circulatory system through the oral mucosa.
  • ondansetron hydrochloride is formulated in a non-aqueous or primarily non-aqueous, oral, propellant-free spray formulation at a concentration of about 0.1 to 7% w/w, more preferably 1 to 6% w/w, and most preferably about 5% w/w.
  • Preferred, primarily non-aqueous, ondansetron hydrochloride formulations comprise, for example, (1) ondansetron hydrochloride (e.g., 0.1 - 7% w/w), acesulfame potassium salt (e.g., 0 - 0.5% w/w), propylene glycol (e.g., 30 - 70%), glycyrrhizic acid (e.g., 0 - 15%), bitter mask (e.g., 0 - 10% w/w), peppermint oil (e.g., 0 - 1% w/w), dehydrated ethanol (e.g., 15 - 50% w/w), and purified water (e.g., 0 - 10% w/w); or (2) ondansetron hydrochloride, acesulfame potassium salt, neotame (e.g., 0 — 1% w/w), propylene glycol, glycy
  • the ondansetron oral spray formulation contains propylene glycol, ethanol, and water.
  • ondansetron HCl is present at about 4-6%, preferably 4.5-5.5%, and most preferably 5.1-5.2% w/w;
  • propylene glycol is present at about 55-65%, preferably 57-62%, and most preferably 60.1-60.3% w/w;
  • ethanol is present at about 25-30%, more preferably 26-29%, and most preferably 27.1-27.3% w/w; and water is present at about 4-6%, preferably 4.5-5.8%, and most preferably 5.3-5.4% w/w.
  • a pharmaceutically effective amount of ondansetron hydrochloride is delivered to the systemic circulatory system of a mammal via actuation of a spray pump adapted for administration of the formulations to the oral mucosal surfaces to spray a unit dose volume of about 10 to 500 ⁇ l of the formulation, wherein the spray preferably has a median particle size of about 30 um to 150 ⁇ m and an ovality ratio of less than abut 2.0.
  • sugar-free ondansetron hydrochloride spray formulations are provided. Further embodiments of the invention provide preservative-free, non-aqueous or primarily non-aqueous ondansetron hydrochloride formulations and methods for their preparation.
  • FIG. 1 illustrates the concentration of Impurity D in preferred formulations of the invention over time under two stability testing conditions (40°C/75%RH and 25°C/60%RH);
  • FIG. 2 is an HPLC chromatogram of a resolution solution of ondansetron (18.526) and Impurity A (15.985) at 306 nm depicting peaks for Impurities C (5.569) and D (6.886);
  • FIG. 3 is an HPLC chromatogram of a resolution solution of ondansetron and Impurities C and D at 328 nm depicting a peak for Impurity A;
  • FIG. 4 is an HPLC chromatogram of a sample solution of Sunett® Formulation C for the analysis of ondansetron at 306 nm; toon]
  • FIG. 5 is an HPLC chromatogram of a sample solution of Sunett® Formulation C for the analysis of ondansetron at 328 nm; and
  • FIG. 6 depicts the residence time of an exemplary formulation in the oral cavity at various dosing volumes.
  • Preferred embodiments of the present invention provide stable, preservative-free pharmaceutical compositions which are primarily non-aqueous solutions comprising a therapeutically effective amount of ondansetron hydrochloride.
  • the preferred compositions do not resort to use of a preservative, but instead achieve inhibition of microbial growth by including an alcohol, preferably at least about 20% w/w ethanol, in the formulation.
  • Ondansetron as the free base or hydrochloride salt, is indicated to prevent nausea and vomiting associated with initial and repeat courses of emetogenic cancer chemotherapy, including high-dose cisplatin, and to prevent postoperative nausea and/or vomiting.
  • Ondansetron is a selective 5-HT 3 receptor antagonist inhibiting the serotonin stimulation of the 5-HT 3 receptor, which initiates the vomiting reflex.
  • Ondansetron can be supplied and employed in formulations according to the invention as a hydrochloride salt and as a free base.
  • the hydrochloride salt is used, for example, in the injectable solution (2 mg/mL), oral tablets (4, 8, and 24 mg), and oral solution (0.8 mg/mL).
  • the free base is used, for example, in the orally disintegrating tablets (4 and 8 mg).
  • the hydrochloride salt is referred to as ( ⁇ ) 1,2,3, 9-tetrahydro-9- methyl-3-[(2-methyl-lH-imidazol-l-yl)methyl]-4H-carbazol-4-one, monohydrochloride, dihydrate.
  • the empirical formula of the hydrochloride salt is Ci 8 Hi 9 N 3 O HCl ⁇ H 2 O; representing a molecular weight of 365.9.
  • the free base is referred to as ( ⁇ )1, 2,3,9- tetrahydro-9-methyl-3-[(2-methyl-lH-imidazol-l-yl)methyl]-4H-carbazol-4-one.
  • the empirical formula of the free base is Ci 8 Hi 9 N 3 O representing a molecular weight of 293.4. Both the free base and HCl salt forms are white to off-white powders and sensitive to light.
  • the formulations according to the invention may also contain additional active pharmaceutical ingredients, such as, for example, including other serotonin antagonists (e.g., dolasetron (Anzemet®), granisetron (Kytril®), and palonosetron (Aloxi®), dopamine antagonists (e.g., chlorpromazine (Thorazine®), droperidol (Inapsine®), metoclopramide (Reglan®), prochlorperazine (Compazine®), promethazine (Phenergan®), trimethobenzamide (Tigan®)), anticholinergic agents such as scopolamine (Transderm Scop®), and antihistamines (e.g., buclizine (Bucladin-S®), cyclizine (Marezine®), dimenhydrinate (Dramamine®), diphenhydramine (Benadryl®), and meclizine (Antivert®)) including salts thereof.
  • Other drugs suitable for combination therapy include droperidol,
  • the storage stable compositions of the present invention show remarkable maintenance of the initial concentration of ondansetron hydrochloride and reduced levels of impurities.
  • preferred formulations of the invention maintain ondansetron content between a concentration of 3.9 mg/spray pump actuation and 4.2 mg/spray actuation over a 15 month period at 25°C and 60% RH, while the average impurity concentration was less than 0.1% for the 15 month period.
  • storage stable means liquid pharmaceutical formulations which include ondansetron as an active ingredient, and in which the concentration of the active ingredient is substantially maintained during storage stability testing, and degradation products and/or impurities which are typically observed in storage stability testing of such formulations are absent or significantly reduced during storage stability testing.
  • storage stability is determined at a temperature range from about 5°C to about 80°C, about 20°C to about 70°C, or about 25°C to about 60°C.
  • storage stability is determined at a relative humidity (“RH") range from about 30% RH to about 90% RH, about 50% RH to about 65% RH, or about 65% RH to about 75% RH.
  • RH relative humidity
  • Preferred time intervals for measuring storage stability range, for example, from about 1 week to 5 years, from about 2 weeks to about 4 months, or at intervals of 2 weeks, 4 weeks, 8 weeks, 12 weeks, 16 weeks, 7 months, and 12 months.
  • non-aqueous refers to spray formulations which include ondansetron and are free or substantially-free of water.
  • non-aqueous formulations may include a minimal quantity of aqueous solvent.
  • water is present only to the degree necessary to dissolve acesulfame potassium salt.
  • Other preferred formulations such as those which do not contain acesulfame potassium salt, for example the sucralose containing formulation, may be entirely free of water, i.e., non-aqueous.
  • Preferred formulations of the invention contain ethanol and/or propylene glycol.
  • propylene glycol and ethanol inhibits microbial growth in the formulation and leads to increased stability of the formulation.
  • Other alcohols such as benzyl alcohol, the parabens (for example, butylparaben, methylparaben), glycerol, propylene glycol, chlorobutanol, phenol, phenoxyethanol, and phenylethyl alcohol, at appropriate concentrations, may be used in place of ethanol for this purpose.
  • Preferred formulations of the invention are primarily non-aqueous permitting inclusion of a higher concentration of the active ingredient (e.g., ondansetron). It is believed that the non-aqueous nature of the preferred formulations of the invention contribute to their self-preserving qualities.
  • various antimicrobials which are suitable for use in foods and other ingestible substances can be used in the present invention.
  • examples include the parabens (butylparaben, methylparaben, and propylparaben), propyl-p- hydroxybenzoates, sodium benzoate, and sorbic acid including salts thereof.
  • a preferred antimicrobial agent is benzoic acid or salts thereof, e.g., sodium benzoate.
  • Preferred embodiments of the invention are directed to buccal spray formulations for fast onset of the active ingredient via absorption to the systemic circulatory system through the oral mucosa. Therefore, preferred spray formulations of the invention maximize absorption to the systemic circulatory system and minimize or avoid absorption by other body systems (e.g., lungs, digestive system).
  • the size of the spray particles contributes to whether the particles are absorbed into body systems other than the oral mucosa/circulatory system (e.g., lungs). For example, smaller sized particles are more likely to be inhaled.
  • uccal herein we mean of, or pertaining to, the mouth and oral cavity, including but not limited to the oral mucosal surfaces of the tongue, cheeks, gums and/or sublingual surfaces.
  • the percentage of the particles (droplets) of the spray formulation (e.g., after actuation of a spray pump) having a diameter of less than ten microns is less than about 2%, more preferably less than about 1.5%.
  • the median diameter of the spray particles is from about 30 microns to about 150 microns, more preferably from about 60 microns to about 120 microns (e.g., Table 1).
  • the ellipticity or ovality ratio of the spray pattern indicates whether the spray is symmetrical.
  • the ovality is defined as the ratio of D max and D min .
  • D max is defined as the largest chord, in mm, that can be drawn within the spray pattern that crosses the COMw (i.e., center of mass of the spray pattern) in base units.
  • D m ⁇ n is described as the smallest chord, in mm, that can be drawn within the spray pattern that crosses the COMw in base units.
  • COMw is defined as the center of mass of the detected spray pattern, where each pixel's intensity is taken into account.
  • the ovality ratio of the spray pattern indicates whether the spray is symmetrical.
  • the ovality ratio of the pattern is less than about 2.0, more preferably less than about 1.5 (Table 1). In another embodiment, increasing the viscosity of the formulation decreases the ovality of the spray pattern.
  • the active ondansetron hydrochloride component may be incorporated into an aqueous solution.
  • ethanol and/or propylene glycol are used as solvents in the formulations of the invention.
  • water is optional and may be included, for example, in a minimal amount to serve as a solvent for taste masking components (e.g., acesulfame potassium salt, FCC).
  • other solvents may be used which aid in solubilizing ondansetron hydrochloride and/or other components of the preferred spray formulations. These may include, for example, aliphatic alcohols, benzyl alcohol, glycerin, glycofurol, and polyethylene glycol.
  • the formulations can contain a propellant for delivery as an aerosol spray or can be propellant-free and delivered by a metered valve spray pump.
  • Suitable propellants include, but are not limited to, hydrocarbons (butane, propane, etc.), chlorofluorocarbons (CFC-1 1, CFC-12, etc.), hydrofluorocarbons (HFA-134a, HFA-227ea, etc.), and ethers (dimethylether, diethylether, etc.).
  • ondansetron hydrochloride formulations which do not contain sweetening, taste masking, or flavoring agents.
  • sweetening, taste masking, or flavoring agents such as Splenda® (sucralose), sorbitol, sucrose, neotame, bitter mask, peppermint oil, strawberry flavor, glycyrrhizic, or Sunett® (acesulfamate K) can be added if desired.
  • Various flavors or flavoring agents may be included to impart a pleasant taste. A pleasant taste is particularly important when the formulation is intended for administration to children or animals. Numerous flavors that are commonly used in pharmaceuticals, foods, candies and beverages are also suitable for use in the present invention. Examples include fruit, peppermint, licorice, bubble gum, and other flavors.
  • the formulations of the present invention can be prepared by various methods.
  • a manufacturing method for Formula A is as follows.
  • Sunett ® e.g., acesulfame potassium salt, FCC
  • FCC acesulfame potassium salt
  • USP purified water
  • This "Sunett ® Solution” is then added later in the manufacturing process.
  • ondansetron HCl, USP is dissolved in propylene glycol, USP. It is preferred that the ondansetron is completely dissolved in propylene glycol, USP before adding any other excipients.
  • the ingredients are preferably added in the following order with constant stirring and thorough mixing between each addition: Magnasweet ® (glycyrrhizic acid, FCC); Bitter Mask, water, Sunett ® Solution, peppermint oil, NF, and dehydrated ethanol, USP.
  • Magnasweet ® glycyrrhizic acid, FCC
  • Bitter Mask water
  • Sunett ® Solution aquenett ® Solution
  • peppermint oil NF
  • dehydrated ethanol USP.
  • dehydrated ethanol, USP is added last and after complete dissolution and mixing of previous ingredients.
  • the final solution is preferably mixed well.
  • containers are pharmaceutically acceptable glass, PET, and HDPE bottles with a capacity of
  • amber glass between 1 and 100 mL. To ensure long-term photostability amber glass can be utilized.
  • the bottle may be opaque to ensure long-term
  • formulations are preferably dispensed using a metered pump device capable
  • the pump and actuator may be any suitable for use with these formulations.
  • the pump and actuator may be any suitable for use with these formulations.
  • the pump and actuator may be any suitable for use with these formulations.
  • the pump and actuator may be any suitable for use with these formulations.
  • the pump and actuator may be any suitable for use with these formulations.
  • the pump and actuator may be any suitable for use with these formulations.
  • the pump and actuator may be any suitable for use with these formulations.
  • the pump and actuator may be any suitable for use with these formulations.
  • the actuator may include an extension, if desired, to
  • the present invention also provides methods of treating various conditions in a
  • the methods include administering to a subject in need of treatment a storage stable pharmaceutical composition according to the invention.
  • the subject is a human; in another embodiment the subject is a non-human mammal, preferably selected from the group of dogs, cats, horses, cattle, sheep, and swine.
  • the storage stable pharmaceutical composition can be administered to a patient in a dosage range of, for example, 0.1 mg to about 260 mg per day, preferably about 1 mg to about 64 mg per day, and more preferably 2 to 48 mg per day.
  • a physical stability study was conducted by placing 60/40 PG/ H 2 O and PG/EtOH solutions containing 5% API (e.g., ondansetron HCl) in a 5 0 C refrigerator.
  • the solution with a PG/H 2 O solvent system crystallized after 2 days.
  • the solution with a PG/EtOH solvent system remained in solution for more than 30 days.
  • Formulation B was preferred over formulation C due to the higher concentration of sweetener, which results in a better taste profile.
  • Tables 4 and 5 provide stability data for
  • Ondansetron concentrations were normalized based on their spray weight. These normalized values may represent a more accurate representation of the stability of the formulations. Ondansetron concentration and label claim per actuation incorporates the variability of inconsistent spray weights, which can contribute to the wider data range fluctuation (see e.g., Table 4, 12 weeks 40°C/75%RH of formulation B). The Ondansetron concentration/actuation was 3.57mg, which was 89.2% label claim, but the concentration/ 1 OO ⁇ l (the theoretical spray volume) was 3.95 mg, which comes out to be 98.8% label claim (FIG. 1).
  • a cycling study was conducted.
  • a set of bulk samples of Formulations B and C (Tables 4 and 5, respectively) and their placebos were stored in clear scintillation vials, wrapped in aluminum foil to protect them from light, and cycled between 5°C in a refrigerator and the 40°C/75%RH stability chamber daily.
  • After 29 days a small white particle was observed in one of the three formulation B samples, and a small amount of white precipitation was observed in all of the formulation C samples, including the placebos. This observation was made immediately after 16 hours of refrigeration. After 8 hours of warming in the 40°C/75%RH stability chamber, the precipitate was still present. The presence of the precipitate in the placebo suggested that it was related to the excipient rather than the API.
  • Formulations 5 and 6 from the above table precipitated out after one night of refrigeration.
  • Formulation 3 precipitated out after two days.
  • Formulations 1 , 2, and 4 remained in solution for 35 days of daily cycling.
  • the remaining solutions all contained Magnasweet®. It was concluded that a component of Magnasweet®, possibly the glycerol vehicle, was likely responsible for maintaining the solution system.
  • HPLC analysis revealed the relative retention time and relative response factor for five impurities and ondansetron as shown below.
  • Figures 2 - 5 are an HPLC chromatogram of a resolution solution of Ondansetron and Impurity A at 306 nm depicting peaks for Impurities C and D; an HPLC chromatogram of a resolution solution of Ondansetron and Impurities C and D at 328 nm depicting a peak for Impurity A; an HPLC chromatogram of a sample solution of Sunett® Formulation C for the analysis of Ondansetron at 306 nm; and, an HPLC chromatogram of a sample solution of Sunett® Formulation C for the analysis of Ondansetron at 328 nm.
  • the exemplary formulations use 55% propylene glycol ("PG"). Saccharin Sodium was prepared as a 2% aqueous solution for ease of solubilization. The percentage of water in the primary solvent system was 60%/40% PG/H 2 O or PG/Ethanol ("EtOH").
  • Formulations 2 and 4 were filled to volume with ethanol (EtOH), with formulation 4 containing an extra 2% of oleic acid and formulations 3 and 5 were filled to volume with H 2 O, with formulation 5 containing an extra 0.1% of benzalkonium chloride. During preparation of formulation 4 the oleic acid was not soluble with the rest of the solution, and this formulation was eliminated as a candidate.
  • Formulations 2, 3, and 5 were placed in three different storage conditions: 5°C refrigerator; 25°C/60% RH; and 40°C/75% RH stability chambers. After one day, all three formulations were placed in the refrigerator and the 25°C/60%RH stability chamber. Formulation 2 showed very little precipitation compared to Formulations 3 and 5 (Tables 12).
  • formulations stored in the 40°C/75% RH stability chamber remained in solution. However, after 45 days, formulation 2 stored in the 40°C/75% RH stability chamber did not show significant precipitation. The formulations had an average spray content of 97.3% label claim and 0.02% impurity D at day 45 in the 40°C/75% RH stability chamber.
  • Formulation 2 was prepared 3 ways: without API, without saccharin solution (replaced by water), and without both API and saccharin. These samples remained in solution after incubation in the refrigerator overnight. Next, the samples were scratched and cycled between the refrigerator and the 40°C/75%RH stability chamber daily for 3 days and subsequently stored in the refrigerator for 3 months. The solutions remained clear. It is believed that the precipitation of ondansetron was caused by the coexistence of ondansetron HCl and saccharin in one solution.
  • Flavors for use in these exemplary formulations include strawberry, mint, fruit punch, strawberry banana, and combinations thereof.

Abstract

Stable formulations of selective 5-hydroxytryptamine receptor antagonists for oral spray administration for absorption by the oral mucosa and related methods of preparation and administration are provided. A preferred embodiment includes ondansetron in a concentration of about 5.1 to about 5.2% w/w; propylene glycol in a concentration of about 60.1 to about 60.3% w/w; water in a concentration of about 5.3 to about 5.4% w/w; and ethanol in a concentration of about 27.1 to about 27.3% w/w. Additional preferred embodiments are preservative free and/or non-aqueous or primarily non-aqueous.

Description

STABLE ANTI-NAUSEA ORAL SPRAY FORMULATIONS AND METHODS
[0001] This application claims priority to U.S. Provisional Patent Application Number 60/876,484, filed on December 22, 2006, the disclosure of which is incorporated by reference herein in its entirety.
FIELD OF THE INVENTION
[0002] The field of this invention is anti-nausea oral spray pharmaceutical formulations, methods of manufacturing such formulations, and their use in treating and preventing nausea and other conditions in human and non-human mammals.
SUMMARY OF THE INVENTION
[0003] Preferred embodiments of the invention provide stable formulations of ondansetron hydrochloride and pharmaceutically acceptable salts thereof suitable for oral administration, and related methods of preparation and administration of ondansetron hydrochloride formulations. The invention provides stable, oral spray formulations in a simple, elegant format for fast onset of the active ingredient via absorption to the systemic circulatory system through the oral mucosa. In one embodiment, ondansetron hydrochloride is formulated in a non-aqueous or primarily non-aqueous, oral, propellant-free spray formulation at a concentration of about 0.1 to 7% w/w, more preferably 1 to 6% w/w, and most preferably about 5% w/w. Preferred, primarily non-aqueous, ondansetron hydrochloride formulations comprise, for example, (1) ondansetron hydrochloride (e.g., 0.1 - 7% w/w), acesulfame potassium salt (e.g., 0 - 0.5% w/w), propylene glycol (e.g., 30 - 70%), glycyrrhizic acid (e.g., 0 - 15%), bitter mask (e.g., 0 - 10% w/w), peppermint oil (e.g., 0 - 1% w/w), dehydrated ethanol (e.g., 15 - 50% w/w), and purified water (e.g., 0 - 10% w/w); or (2) ondansetron hydrochloride, acesulfame potassium salt, neotame (e.g., 0 — 1% w/w), propylene glycol, glycyrrhizic acid, bitter mask, peppermint oil, dehydrated ethanol, and purified water; or (3) ondansetron hydrochloride, sucralose (e.g., 0 - 2% w/w), propylene glycol, glycyrrhizic acid, bitter mask, peppermint oil, strawberry flavor (e.g. 0-1% w/w), purified water, and dehydrated ethanol.
[0QQ4] In one embodiment, the ondansetron oral spray formulation contains propylene glycol, ethanol, and water. In this embodiment, ondansetron HCl is present at about 4-6%, preferably 4.5-5.5%, and most preferably 5.1-5.2% w/w; propylene glycol is present at about 55-65%, preferably 57-62%, and most preferably 60.1-60.3% w/w; ethanol is present at about 25-30%, more preferably 26-29%, and most preferably 27.1-27.3% w/w; and water is present at about 4-6%, preferably 4.5-5.8%, and most preferably 5.3-5.4% w/w.
[00Q5] In another embodiment of the invention, a pharmaceutically effective amount of ondansetron hydrochloride is delivered to the systemic circulatory system of a mammal via actuation of a spray pump adapted for administration of the formulations to the oral mucosal surfaces to spray a unit dose volume of about 10 to 500 μl of the formulation, wherein the spray preferably has a median particle size of about 30 um to 150 μm and an ovality ratio of less than abut 2.0. In yet another embodiment of the invention, sugar-free ondansetron hydrochloride spray formulations are provided. Further embodiments of the invention provide preservative-free, non-aqueous or primarily non-aqueous ondansetron hydrochloride formulations and methods for their preparation.
[0006] Additional features and advantages of the invention will be set forth in the description which follows and will be apparent from the description or may be learned by practice of the invention.
BRIEF DESCRIPTION OF THE DRAWINGS
[0007] FIG. 1 illustrates the concentration of Impurity D in preferred formulations of the invention over time under two stability testing conditions (40°C/75%RH and 25°C/60%RH);
[0008] FIG. 2 is an HPLC chromatogram of a resolution solution of ondansetron (18.526) and Impurity A (15.985) at 306 nm depicting peaks for Impurities C (5.569) and D (6.886);
[0009] FIG. 3 is an HPLC chromatogram of a resolution solution of ondansetron and Impurities C and D at 328 nm depicting a peak for Impurity A; [0010] FIG. 4 is an HPLC chromatogram of a sample solution of Sunett® Formulation C for the analysis of ondansetron at 306 nm; toon] FIG. 5 is an HPLC chromatogram of a sample solution of Sunett® Formulation C for the analysis of ondansetron at 328 nm; and
[0012] FIG. 6 depicts the residence time of an exemplary formulation in the oral cavity at various dosing volumes.
DETAILED DESCRIPTION OF THE INVENTION
[0013] Reference will now be made in detail to the presently preferred embodiments of the invention, which, together with the following examples, serve to explain the principles of the invention. It is to be understood that the application of the teachings of the present invention to a specific problem or environment will be within the capabilities of one having ordinary skill in the art in light of the teachings contained herein. Illustrative embodiments of the products of the present invention and processes for their preparation and use appear in the following examples.
[0014] Preferred embodiments of the present invention provide stable, preservative-free pharmaceutical compositions which are primarily non-aqueous solutions comprising a therapeutically effective amount of ondansetron hydrochloride. In one embodiment, the preferred compositions do not resort to use of a preservative, but instead achieve inhibition of microbial growth by including an alcohol, preferably at least about 20% w/w ethanol, in the formulation.
[0015] Ondansetron, as the free base or hydrochloride salt, is indicated to prevent nausea and vomiting associated with initial and repeat courses of emetogenic cancer chemotherapy, including high-dose cisplatin, and to prevent postoperative nausea and/or vomiting.
[0016] Ondansetron is a selective 5-HT3 receptor antagonist inhibiting the serotonin stimulation of the 5-HT3 receptor, which initiates the vomiting reflex.
[0017] Ondansetron can be supplied and employed in formulations according to the invention as a hydrochloride salt and as a free base. The hydrochloride salt is used, for example, in the injectable solution (2 mg/mL), oral tablets (4, 8, and 24 mg), and oral solution (0.8 mg/mL). The free base is used, for example, in the orally disintegrating tablets (4 and 8 mg). Chemically, the hydrochloride salt is referred to as (±) 1,2,3, 9-tetrahydro-9- methyl-3-[(2-methyl-lH-imidazol-l-yl)methyl]-4H-carbazol-4-one, monohydrochloride, dihydrate. The empirical formula of the hydrochloride salt is Ci8Hi9N3O HCl^H2O; representing a molecular weight of 365.9. The free base is referred to as (±)1, 2,3,9- tetrahydro-9-methyl-3-[(2-methyl-lH-imidazol-l-yl)methyl]-4H-carbazol-4-one. The empirical formula of the free base is Ci8Hi9N3O representing a molecular weight of 293.4. Both the free base and HCl salt forms are white to off-white powders and sensitive to light. The term "ondansetron," as used herein, refers to both the free base and all pharmaceutically acceptable salt forms unless otherwise noted.
[0018] The formulations according to the invention may also contain additional active pharmaceutical ingredients, such as, for example, including other serotonin antagonists (e.g., dolasetron (Anzemet®), granisetron (Kytril®), and palonosetron (Aloxi®), dopamine antagonists (e.g., chlorpromazine (Thorazine®), droperidol (Inapsine®), metoclopramide (Reglan®), prochlorperazine (Compazine®), promethazine (Phenergan®), trimethobenzamide (Tigan®)), anticholinergic agents such as scopolamine (Transderm Scop®), and antihistamines (e.g., buclizine (Bucladin-S®), cyclizine (Marezine®), dimenhydrinate (Dramamine®), diphenhydramine (Benadryl®), and meclizine (Antivert®)) including salts thereof. Other drugs suitable for combination therapy include droperidol, dexamethasone, methylprednisolone (Medrol®), and metoclopramide including salts thereof.
[0019] Under stability analyses, the storage stable compositions of the present invention show remarkable maintenance of the initial concentration of ondansetron hydrochloride and reduced levels of impurities. For example, preferred formulations of the invention maintain ondansetron content between a concentration of 3.9 mg/spray pump actuation and 4.2 mg/spray actuation over a 15 month period at 25°C and 60% RH, while the average impurity concentration was less than 0.1% for the 15 month period. [0020] As used herein, "storage stable" means liquid pharmaceutical formulations which include ondansetron as an active ingredient, and in which the concentration of the active ingredient is substantially maintained during storage stability testing, and degradation products and/or impurities which are typically observed in storage stability testing of such formulations are absent or significantly reduced during storage stability testing. In one embodiment, storage stability is determined at a temperature range from about 5°C to about 80°C, about 20°C to about 70°C, or about 25°C to about 60°C. In another embodiment, storage stability is determined at a relative humidity ("RH") range from about 30% RH to about 90% RH, about 50% RH to about 65% RH, or about 65% RH to about 75% RH. Preferred time intervals for measuring storage stability range, for example, from about 1 week to 5 years, from about 2 weeks to about 4 months, or at intervals of 2 weeks, 4 weeks, 8 weeks, 12 weeks, 16 weeks, 7 months, and 12 months.
[0021] As used herein, the term "primarily non-aqueous" refers to spray formulations which include ondansetron and are free or substantially-free of water. Primarily non-aqueous formulations may include a minimal quantity of aqueous solvent. For example, in preferred primarily non-aqueous formulations of the invention, water is present only to the degree necessary to dissolve acesulfame potassium salt. Other preferred formulations such as those which do not contain acesulfame potassium salt, for example the sucralose containing formulation, may be entirely free of water, i.e., non-aqueous. [0022] Preferred formulations of the invention contain ethanol and/or propylene glycol. Without being bound by theory, it is believed that the inclusion of propylene glycol and ethanol inhibits microbial growth in the formulation and leads to increased stability of the formulation. Other alcohols such as benzyl alcohol, the parabens (for example, butylparaben, methylparaben), glycerol, propylene glycol, chlorobutanol, phenol, phenoxyethanol, and phenylethyl alcohol, at appropriate concentrations, may be used in place of ethanol for this purpose. Thus, in accordance with one embodiment of the invention, it is not necessary to include an antimicrobial component or agent to ensure safe storage without the proliferation of pathogenic molds, yeasts, or bacteria. Preferred formulations of the invention are primarily non-aqueous permitting inclusion of a higher concentration of the active ingredient (e.g., ondansetron). It is believed that the non-aqueous nature of the preferred formulations of the invention contribute to their self-preserving qualities.
[0023] In another embodiment of the invention, various antimicrobials which are suitable for use in foods and other ingestible substances can be used in the present invention. Examples include the parabens (butylparaben, methylparaben, and propylparaben), propyl-p- hydroxybenzoates, sodium benzoate, and sorbic acid including salts thereof. A preferred antimicrobial agent is benzoic acid or salts thereof, e.g., sodium benzoate.
[0024] Preferred embodiments of the invention are directed to buccal spray formulations for fast onset of the active ingredient via absorption to the systemic circulatory system through the oral mucosa. Therefore, preferred spray formulations of the invention maximize absorption to the systemic circulatory system and minimize or avoid absorption by other body systems (e.g., lungs, digestive system). The size of the spray particles contributes to whether the particles are absorbed into body systems other than the oral mucosa/circulatory system (e.g., lungs). For example, smaller sized particles are more likely to be inhaled. By "buccal" herein we mean of, or pertaining to, the mouth and oral cavity, including but not limited to the oral mucosal surfaces of the tongue, cheeks, gums and/or sublingual surfaces.
[0025] In one embodiment, the percentage of the particles (droplets) of the spray formulation (e.g., after actuation of a spray pump) having a diameter of less than ten microns is less than about 2%, more preferably less than about 1.5%. In another embodiment, the median diameter of the spray particles is from about 30 microns to about 150 microns, more preferably from about 60 microns to about 120 microns (e.g., Table 1).
[0026] The ellipticity or ovality ratio of the spray pattern indicates whether the spray is symmetrical. The ovality is defined as the ratio of Dmax and Dmin. Dmax is defined as the largest chord, in mm, that can be drawn within the spray pattern that crosses the COMw (i.e., center of mass of the spray pattern) in base units. Dmιn is described as the smallest chord, in mm, that can be drawn within the spray pattern that crosses the COMw in base units. COMw is defined as the center of mass of the detected spray pattern, where each pixel's intensity is taken into account. The ovality ratio of the spray pattern indicates whether the spray is symmetrical. It is believed that the more symmetrical the oval shape of the pattern of spray particles, the more likely the particles will evenly cover the oral mucosa. In accordance with a preferred embodiment of the invention, the ovality ratio of the pattern is less than about 2.0, more preferably less than about 1.5 (Table 1). In another embodiment, increasing the viscosity of the formulation decreases the ovality of the spray pattern.
Figure imgf000012_0001
ι
[0027] In preparing the formulations of the present invention, the active ondansetron hydrochloride component may be incorporated into an aqueous solution. Preferably, ethanol and/or propylene glycol are used as solvents in the formulations of the invention. In one embodiment, water is optional and may be included, for example, in a minimal amount to serve as a solvent for taste masking components (e.g., acesulfame potassium salt, FCC). However, other solvents may be used which aid in solubilizing ondansetron hydrochloride and/or other components of the preferred spray formulations. These may include, for example, aliphatic alcohols, benzyl alcohol, glycerin, glycofurol, and polyethylene glycol.
[0028] The formulations can contain a propellant for delivery as an aerosol spray or can be propellant-free and delivered by a metered valve spray pump. Suitable propellants include, but are not limited to, hydrocarbons (butane, propane, etc.), chlorofluorocarbons (CFC-1 1, CFC-12, etc.), hydrofluorocarbons (HFA-134a, HFA-227ea, etc.), and ethers (dimethylether, diethylether, etc.).
[0029] In one embodiment of the invention, ondansetron hydrochloride formulations are provided which do not contain sweetening, taste masking, or flavoring agents. However, sweetening, taste masking, or flavoring agents such as Splenda® (sucralose), sorbitol, sucrose, neotame, bitter mask, peppermint oil, strawberry flavor, glycyrrhizic, or Sunett® (acesulfamate K) can be added if desired. [QQ30] Various flavors or flavoring agents may be included to impart a pleasant taste. A pleasant taste is particularly important when the formulation is intended for administration to children or animals. Numerous flavors that are commonly used in pharmaceuticals, foods, candies and beverages are also suitable for use in the present invention. Examples include fruit, peppermint, licorice, bubble gum, and other flavors.
[0031] The formulations of the present invention can be prepared by various methods. One embodiment of a manufacturing method for Formula A is as follows. Preferably, Sunett® (e.g., acesulfame potassium salt, FCC) is dissolved in purified water, USP. This "Sunett® Solution" is then added later in the manufacturing process. Next, ondansetron HCl, USP is dissolved in propylene glycol, USP. It is preferred that the ondansetron is completely dissolved in propylene glycol, USP before adding any other excipients. Following dissolution, the ingredients are preferably added in the following order with constant stirring and thorough mixing between each addition: Magnasweet® (glycyrrhizic acid, FCC); Bitter Mask, water, Sunett® Solution, peppermint oil, NF, and dehydrated ethanol, USP. Preferably, dehydrated ethanol, USP is added last and after complete dissolution and mixing of previous ingredients. The final solution is preferably mixed well. Formula A:
Item# mg/g
1 Sunett® (Acesulfame potassium salt, FCC) 2.6
2 Purified Water, USP 48.6
3 Ondansetron HCl, USP 51.2
4 Propylene Glycol, USP 562.9
5 MagnaSweet®, FCC (Glycyrrhizic acid) 51.2
6 Bitter Mask 25.6
7 Peppermint Oil, NF 5.1
8 Dehydrated Ethanol, USP 252.8
[0032] The solution can then be packaged into any suitable containers. Preferred
containers are pharmaceutically acceptable glass, PET, and HDPE bottles with a capacity of
between 1 and 100 mL. To ensure long-term photostability amber glass can be utilized.
Additionally, if PET or HDPE is chosen, the bottle may be opaque to ensure long-term
photostability.
[0033] The formulations are preferably dispensed using a metered pump device capable
of delivering between 10 and 500 mcL. Pumps commonly used for dispensing nasal sprays
are suitable for use with these formulations. In one embodiment, the pump and actuator may
be modified such that the spray is dispensed horizontally to the bottle. This will allow easy
dispensing to the mouth of the patient. The actuator may include an extension, if desired, to
facilitate delivery to the buccal area of humans or animals.
[0034] The present invention also provides methods of treating various conditions in a
subject (e.g., prevention of nausea and vomiting, chemotherapy-induced emesis, and post- operative nausea and vomiting). The methods include administering to a subject in need of treatment a storage stable pharmaceutical composition according to the invention. In one embodiment, the subject is a human; in another embodiment the subject is a non-human mammal, preferably selected from the group of dogs, cats, horses, cattle, sheep, and swine. The storage stable pharmaceutical composition can be administered to a patient in a dosage range of, for example, 0.1 mg to about 260 mg per day, preferably about 1 mg to about 64 mg per day, and more preferably 2 to 48 mg per day.
[0035] It is to be understood that application of the teachings of the present invention to a specific problem or environment will be within the capability of one having ordinary skill in the art in light of the teachings contained herein. The present invention is more fully illustrated by the following non-limiting examples.
EXAMPLE 1
[0036] A physical stability study was conducted by placing 60/40 PG/ H2O and PG/EtOH solutions containing 5% API (e.g., ondansetron HCl) in a 50C refrigerator. The solution with a PG/H2O solvent system crystallized after 2 days. The solution with a PG/EtOH solvent system remained in solution for more than 30 days.
[0037] Stability studies for formulations B and C (Tables 2 and 3) were conducted by preparing a 250 mL batch for each formulation, along with corresponding placebos. An aqueous solution of 20% Sunett® (w/v) was prepared and used to allow for more rapid mixing. To limit the total amount of water in the formulation at 5%, the amount of water added was reduced according to the amount of the Sunett® solution added.
Table 2: Sunett Formulation B
Figure imgf000017_0001
[0038] Formulation B was preferred over formulation C due to the higher concentration of sweetener, which results in a better taste profile. Tables 4 and 5 provide stability data for
Formulations B and C respectively. Table 4: Stabilit data of Sunett® Formulation B
Figure imgf000018_0001
Average Ond. HCl Concentration =Average of 3 data points from analyst printout
Calculation for Ondansetron content (mg/actuation) = Average Ond. HCl Concentration /365.86*293.37*0.1
Calculation for Normalized Ond. Concentration (mg/100μl)= Ondansetron (mg/actuation)/(Spray wt./97.69)
Calculation for L.C./actuation = Ondansetron (mg/actuation)/4.00 i
Calculation for Normalized L.C./IOOul = Normalized Ond. Concentration (mg/100μl)/4.00 ~
Specifications: ~
Spray weight: 83.0mg - 112.3mg; %L.C: 85% -115%; Impurity D: no more than 0.10% (see Example 2)
Table 5: Stability data tor Formulation C
Figure imgf000019_0001
Calculations same as in Table 4. i - -
[0039] Ondansetron concentrations were normalized based on their spray weight. These normalized values may represent a more accurate representation of the stability of the formulations. Ondansetron concentration and label claim per actuation incorporates the variability of inconsistent spray weights, which can contribute to the wider data range fluctuation (see e.g., Table 4, 12 weeks 40°C/75%RH of formulation B). The Ondansetron concentration/actuation was 3.57mg, which was 89.2% label claim, but the concentration/ 1 OOμl (the theoretical spray volume) was 3.95 mg, which comes out to be 98.8% label claim (FIG. 1).
[0040] The plot of concentration versus time for the formation of Impurity D indicates a zero order reaction. This is not what is typically observed in chemical degradation profiles. Typical profiles exhibit first order kinetics. However, Waterman and Adam have shown that under certain circumstances the degradation of a parent molecule, and thus the subsequent appearance of the degradation product, appear to exhibit zero order kinetics. K.C. Waterman and R.C. Adami "Accelerated aging: Prediction of chemical stability of pharmaceuticals", Int J Pharm 23(1 -2): 101-125 (2005). The data indicate the current formulation is stable, i.e. Impurity D present at less than or equal to 0.1%, for 243 weeks at 25°C/60%RH. This exceeds the 104 weeks necessary for a 2 year shelf-life based upon the appearance of Impurity D.
EXAMPLE 2
[0041] A cycling study was conducted. A set of bulk samples of Formulations B and C (Tables 4 and 5, respectively) and their placebos were stored in clear scintillation vials, wrapped in aluminum foil to protect them from light, and cycled between 5°C in a refrigerator and the 40°C/75%RH stability chamber daily. After 29 days, a small white particle was observed in one of the three formulation B samples, and a small amount of white precipitation was observed in all of the formulation C samples, including the placebos. This observation was made immediately after 16 hours of refrigeration. After 8 hours of warming in the 40°C/75%RH stability chamber, the precipitate was still present. The presence of the precipitate in the placebo suggested that it was related to the excipient rather than the API.
[0042] To further investigate the cause of precipitation, six formulations were prepared and cycled between 5°C refrigerator and 40°C/75%RH daily. The formulations were:
Figure imgf000021_0001
[0043] Formulations 5 and 6 from the above table precipitated out after one night of refrigeration. Formulation 3 precipitated out after two days. Formulations 1 , 2, and 4 remained in solution for 35 days of daily cycling. The remaining solutions all contained Magnasweet®. It was concluded that a component of Magnasweet®, possibly the glycerol vehicle, was likely responsible for maintaining the solution system.
[0044] Another attempt to prevent precipitation was the addition of 0.9% benzyl alcohol. A comparative study of Formulation B with 5% water, with and without benzyl alcohol was conducted by preparing triplicate samples of both formulations and cycling them daily. All samples were free of precipitation at 40 days, after which the samples were left in the 5°C refrigerator. They remained in solution for more than 6 months. EXAMPLE 3
[0045] To further investigate formulations with reduced precipitation, two alternative systems were investigated (Tables 7 and 8). The alternative neotame/Sunett® Formulation contains approximately the same amount of water as Sunett® Formulations B and C above. However, the amount of Sunett® is reduced. The alternative Splenda® Formulation does not contain any added water. Both formulations were stored for significant periods of time without any precipitation. Physical observations and chemical analysis were performed on the neotame/Sunett® and Splenda® formulations after 11 and 15 months, respectively (Tables 9 and 10). After 11 and 15 months of refrigeration, neither Formulation exhibited precipitation. Thus, Sunett® may have some effect on the physical stability of the product. In addition, removing Sunett® and water completely, as in the Splenda® Formulation, resulted in similar acceptable physical stability. These exemplary formulations would be suitably stable after 2 years of storage at room temperature.
Table 7. Alternative Neotame/Sunett® Formulation
Figure imgf000023_0001
Table 8. Alternative Splenda® Formulation
Figure imgf000023_0002
Table 9. Stability Data For Alternative Neotame/Sunett® Formulation
Figure imgf000024_0001
Table 10. Stability Data for Alternative Splenda® Formulation
Figure imgf000024_0002
EXAMPLE 4
[0046] HPLC analysis revealed the relative retention time and relative response factor for five impurities and ondansetron as shown below. Figures 2 - 5 are an HPLC chromatogram of a resolution solution of Ondansetron and Impurity A at 306 nm depicting peaks for Impurities C and D; an HPLC chromatogram of a resolution solution of Ondansetron and Impurities C and D at 328 nm depicting a peak for Impurity A; an HPLC chromatogram of a sample solution of Sunett® Formulation C for the analysis of Ondansetron at 306 nm; and, an HPLC chromatogram of a sample solution of Sunett® Formulation C for the analysis of Ondansetron at 328 nm.
Table 1 1 : Relative retention time and response factor of im urities
Figure imgf000025_0001
Note: Except Impurity D, all other impurities are calculated based on the sample solutions prepared for ondansetron.
EXAMPLE 5
[0047] Stability studies were conducted for formulations utilizing saccharin sodium
to determine the long term compatibilities of saccharin sodium and bitter mask with the drug solution.
[0048] The exemplary formulations use 55% propylene glycol ("PG"). Saccharin Sodium was prepared as a 2% aqueous solution for ease of solubilization. The percentage of water in the primary solvent system was 60%/40% PG/H2O or PG/Ethanol ("EtOH").
Table 12: Saccharin Sodium Formulation 2
Figure imgf000026_0001
[0049] Formulations 2 and 4 were filled to volume with ethanol (EtOH), with formulation 4 containing an extra 2% of oleic acid and formulations 3 and 5 were filled to volume with H2O, with formulation 5 containing an extra 0.1% of benzalkonium chloride. During preparation of formulation 4 the oleic acid was not soluble with the rest of the solution, and this formulation was eliminated as a candidate. Formulations 2, 3, and 5 were placed in three different storage conditions: 5°C refrigerator; 25°C/60% RH; and 40°C/75% RH stability chambers. After one day, all three formulations were placed in the refrigerator and the 25°C/60%RH stability chamber. Formulation 2 showed very little precipitation compared to Formulations 3 and 5 (Tables 12). All three formulations stored in the 40°C/75% RH stability chamber remained in solution. However, after 45 days, formulation 2 stored in the 40°C/75% RH stability chamber did not show significant precipitation. The formulations had an average spray content of 97.3% label claim and 0.02% impurity D at day 45 in the 40°C/75% RH stability chamber.
[0050] The cause of precipitation of ondansetron in formulations 2, 3, and 5 in the refrigerator and in room temperature was investigated to evaluate the effect of saccharin: Formulation 2 was prepared 3 ways: without API, without saccharin solution (replaced by water), and without both API and saccharin. These samples remained in solution after incubation in the refrigerator overnight. Next, the samples were scratched and cycled between the refrigerator and the 40°C/75%RH stability chamber daily for 3 days and subsequently stored in the refrigerator for 3 months. The solutions remained clear. It is believed that the precipitation of ondansetron was caused by the coexistence of ondansetron HCl and saccharin in one solution. The study was continued by preparing formulations 2 and 3 based on the original formulations and using the same formulations where the saccharin solution was replaced with water. These four formulations were prepared in triplicate. After one night of refrigeration, the ondansetron in the samples containing saccharin sodium precipitated out. The ondansetron in two out of three samples of formulation 3 without saccharin sodium precipitated out as well. However, the ondansetron in the formulation 2 without saccharin sodium stayed in solution for 3 months.
Docket No.: N9810.0060
Table 16: Effect of saccharin solution and water on formulations 2 and 3
Figure imgf000029_0001
Kt
[0051] To investigate the cause of precipitation in formulation 3 without saccharin, three additional samples were made which included 5%, 10%, and 15% EtOH. Following incubation in the 5°C refrigerator, the samples were analyzed. The ondansetron in the sample containing 5% EtOH stayed in solution for more than a week, the ondansetron in the sample containing 10% EtOH precipitated out in one day, and the ondansetron in the sample containing 15% EtOH stayed in solution for more than a day and less than a week. This indicated that an optimal EtOH concentration was preferred to maintain a homogeneous solution when using this combination of excipients. Three samples of formulation 5 were made by replacing the 2% saccharin sodium solution with water and replacing 17% water (QS part) with EtOH; and adding only 0.1%, 0.15%, and 0.2% saccharin sodium to each sample. The ondansetron in these three formulations precipitated overnight as well. It was suspected that water contributed to the instability. Three samples of formulation 2 were made without saccharin and without water, along with another three samples made without saccharin and with only 5% water. These six samples were placed in the 50C refrigerator. The ondansetron in one out of three samples with 5% water precipitated after 2 1/2 weeks, and the ondansetron in the other two samples precipitated after 6 weeks. The ondansetron in the 3 samples with no water remained in solution for 12 weeks. These experiments led to the conclusion that saccharin sodium was not soluble in the formulation solution, and large amounts of water will cause physical instability of the formulation as well. EXAMPLE 6
[0052] Studies were conducted to determine the residence time in the oral cavity. Briefly, a placebo formulation was radiolabeled with Technetium 99m-DTPA. Various volumes of the radiolabeled formulation were delivered to 8 human subjects after receiving necessary IRB clearance and consent. After the defined volume was delivered, deposition was imaged using gamma scintigraphy through the entire gastrointestinal tract (oral cavity through large intestine). Oral cavity imaging was conducted for the first 3 minutes at 15 second intervals, followed by imaging at 5, 10, 15, 20, 30, 45, 60, 90, 120, 150, 180, 210, and 240 minutes post dosing. After the 3 minute interval, lower gastrointestinal tract images were taken at the time points above. From this data, it was determined that it was beneficial to minimize the dosing volume (Figure 6). From Figure 6, it was observed that the lowest dosing volume, 50mcL, resulted in the longest residence time of the label in the mouth. At 5 minutes, there was still approximately 20% of the label still present in the oral cavity. There is approximately half as much residing in the oral cavity at the same time point for 400mcL. In addition, there was little difference between lOOmcL and 200mcL, although the percent remaining in the mouth at 5 minutes was slightly less than that of the 50mcL dose but more than that observed after a 400mcL dose. Longer residence times in the oral cavity will increase oral mucosal absorption. This longer residence time effectively increases the exposure of the oral mucosa to the compound and increases transport across the mucosal membrane. EXAMPLE 7
[0053] As described above, it is advantageous to give embodiments a pleasant taste for administration to children or non-human animals. An embodiment including a flavoring ingredient is formulated as shown in Tables 17 and 18. The ranges given in Tables 17 and 18 are illustrative of one embodiment using MagnaSweet and Sucralose in combination with one or more flavoring ingredients.
Table 17: Flavored Sucralose Formulation
Figure imgf000032_0001
Table 18: Flavored Sucralose Formulation
Figure imgf000032_0002
[0054] Flavors for use in these exemplary formulations include strawberry, mint, fruit punch, strawberry banana, and combinations thereof.
[0055] The above description and examples are only illustrative of preferred embodiments which achieve the objects, features, and advantages of the present invention, and it is not intended that the present invention be limited thereto.

Claims

CLAIMS What is claimed as new and desired to be protected by Letters Patent is:
1. A pharmaceutical oral spray product comprising a selective 5- hydroxytryptamine receptor antagonist formulation in a spray pump container, wherein the formulation is primarily non-aqueous and when a unit dosage volume of about 10 to about 500 μL of the formulation is sprayed, the spray has a median particle diameter of about 30 μm to about 150 μm and an ovality ratio of less than about 2.0.
2. The oral spray of claim 1, wherein the spray has a median particle diameter of about 60 μm to about 120 μm.
3. The oral spray of claim 1, wherein the spray has an ovality ratio of less than about 1.5.
4. The oral spray of claim 1, wherein the formulation further comprises a flavoring ingredient.
5. The oral spray of claim 4, wherein the flavoring ingredient is sucralose.
6. The oral spray of claim 4, wherein the flavoring ingredient is selected from the group consisting of peppermint oil, strawberry flavor, neotame, bitter mask, glycyrrhizic, acesulfamate potassium, sucrose, and sorbitol.
7. The oral spray of claim 1, wherein the formulation further comprises a propellant.
8. The oral spray of claim 7, wherein the propellant is selected from the group consisting of hydrocarbons, chlorofluorocarbons, hydrofluorocarbons, and ethers.
9. The oral spray of claim 1, wherein the formulation further comprises a solvent.
10. The oral spray of claim 9, wherein the solvent is an alcohol.
1 1. The oral spray of claim 9, wherein the solvent is selected from the group consisting of H2O, ethanol, propylene glycol.
12. The oral spray of claim 1, wherein the formulation is storage stable.
13. The oral spray of claim 1, wherein the selective 5- hydroxytryptamine receptor antagonist is ondansetron.
14. The oral spray of claim 13, wherein ondansetron is present in about 0.1 to about 7% w/w.
15. The oral spray of claim 14, wherein ondansetron is present in about 5.0 to about 5.2% w/v.
16. The oral spray of claim 13, wherein the formulation comprises about 15 to about 50% w/w ethanol.
17. The oral spray of claim 16, wherein the ethanol is present in about 20 to about 29.2% w/v.
18. The oral spray of claim 1, wherein the formulation is nonaqueous.
19. The oral spray of claim 1, wherein the formulation is preservative-free.
20. The oral spray of claim 1, wherein the formulation is nonaqueous and preservative free.
21. An oral spray composition, comprising: ondansetron in a concentration of about 4 to about 6% w/w; propylene glycol in a concentration of about 55 to about 65% w/w; water in a concentration of about 4 to about 6% w/w; and ethanol in a concentration of about 25 to about 30% w/w.
22. The oral spray of claim 21, comprising ondansetron in a concentration of about 4.5 to about 5.5% w/w; propylene glycol in a concentration of abut 57 to about 62% w/w; water in a concentration of about 4.5 to about 5.8% w/w; and ethanol in a concentration of about 26 to about 29 %.
23. The oral spray of claim 21 , comprising ondansetron in a concentration of about 5.1 to about 5.2% w/w;
propylene glycol in a concentration of about 60.1 to about 60.3% w/w; water in a concentration of about 5.3 to about 5.4% w/w; and ethanol in a concentration of about 27.1 to about 27.3% w/w.
24. The oral spray of claim 21, further comprising one or more of a sweetening agent, a taste masking agent or a flavoring agent.
25. A method of treating a condition in a human or non-human animal comprising spraying a unit dose volume of about 10 to about 500 μL of a pharmaceutical composition on the oral mucosa of the animal, wherein the composition is primarily non-aqueous and the spray has a median particle size diameter of about 30 to 150 μm and an ovality ratio of less than about 2.0, wherein the composition comprises ondansetron and a solvent, and the ondansetron is absorbed through the oral mucosa to alleviate said condition.
26. The method of claim 25, wherein ondansetron is present in the composition at about 0.1 to about 7% w/w.
27. The method of claim 25, wherein ondansetron is present in the composition at about 5.0 to about 5.2% w/w.
28. The method of claim 25, wherein the ondansetron is administered in a dose from about 0.1 mg to about 260 mg per day.
29. The method of claim 28, wherein the ondansetron is administered in a dose from about 1 mg to about 64 mg per day.
30. The method of claim 29, wherein the ondansetron is administered in a dose from about 2 mg to about 48 mg per day.
31. The method of claim 25, wherein the solvent is selected from the group consisting of ethanol, water, propylene glycol, benzyl alcohol, aliphatic alcohol, glycerin, glycofurol, and polyethylene glycol.
32. The method of claim 25, wherein the condition is selected from the group consisting of nausea, vomiting, and emesis.
PCT/US2007/026070 2006-12-22 2007-12-21 Stable anti-nausea oral spray formulations and methods WO2008079295A1 (en)

Priority Applications (3)

Application Number Priority Date Filing Date Title
JP2009542925A JP2010513525A (en) 2006-12-22 2007-12-21 Stable anti-emetic oral spray formulations and methods
EP07863183A EP2124897A4 (en) 2006-12-22 2007-12-21 Stable anti-nausea oral spray formulations and methods
CA2673049A CA2673049C (en) 2006-12-22 2007-12-21 Stable anti-nausea oral spray formulations and methods

Applications Claiming Priority (2)

Application Number Priority Date Filing Date Title
US87648406P 2006-12-22 2006-12-22
US60/876,484 2006-12-22

Publications (1)

Publication Number Publication Date
WO2008079295A1 true WO2008079295A1 (en) 2008-07-03

Family

ID=39562843

Family Applications (1)

Application Number Title Priority Date Filing Date
PCT/US2007/026070 WO2008079295A1 (en) 2006-12-22 2007-12-21 Stable anti-nausea oral spray formulations and methods

Country Status (5)

Country Link
US (2) US20080171089A1 (en)
EP (1) EP2124897A4 (en)
JP (1) JP2010513525A (en)
CA (1) CA2673049C (en)
WO (1) WO2008079295A1 (en)

Cited By (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2010070236A1 (en) 2008-12-19 2010-06-24 Philippe Perovitch Formulation for the buccal transmucosal administration of setrons
FR2940116A1 (en) * 2008-12-22 2010-06-25 Philippe Perovitch FORMULATION FOR THE ADMINISTRATION OF HYPOALIMENTS BY ORAL TRANSMUCOSAL PATHWAY
FR2940911A1 (en) * 2009-01-13 2010-07-16 Philippe Perovitch FORMULATION FOR ORAL TRANSMUCOSAL ADMINISTRATION OF ANTALGIC AND / OR ANTI-SPASMODIC MOLECULES
EP3068376A4 (en) * 2013-11-14 2017-06-07 Insys Pharma, Inc. Ondansetron sublingual spray formulation

Families Citing this family (6)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US20110288115A1 (en) * 2010-05-24 2011-11-24 Avmedis Llc Treatment of vagally-mediated spectrum disorders
US20120003162A1 (en) 2010-06-30 2012-01-05 Mcneil-Ppc, Inc. Methods of Preparing Non-Alcohol Bioactive Esential Oil Mouth Rinses
US9084902B2 (en) 2010-06-30 2015-07-21 Mcneil-Ppc, Inc. Non-alchohol bioactive essential oil mouth rinses
WO2015093923A1 (en) * 2013-12-19 2015-06-25 Castro Aldrete Jorge Isaac Veterinary compositions comprising an active substance and a pharmaceutically acceptable vehicle for the administration thereof via mucous membranes
US9855234B2 (en) * 2014-07-08 2018-01-02 Insys Development Company, Inc. Diclofenac sublingual spray
US10172833B2 (en) 2015-08-11 2019-01-08 Insys Development Company, Inc. Sublingual ondansetron spray

Citations (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US5178855A (en) * 1989-01-30 1993-01-12 Schering Corporation Treatment of luekocyte dysfunction with GM-CSF
US20060239928A1 (en) * 2005-02-17 2006-10-26 Heit Mark C Transmucosal administration of drug compositions for treating and preventing disorders in animals

Family Cites Families (76)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
BE632504A (en) * 1962-05-24
US3304230A (en) * 1963-02-18 1967-02-14 Revlon Liquid aerosol propellant solutions of fatty acid salts of physiologically active amines
SU432703A3 (en) * 1971-08-24 1974-06-15 Фридрих Боссерт, Вульф Фатер, Курт Бауер
SE7812207L (en) * 1977-12-01 1979-06-02 Welsh Nat School Med APPARATUS, PROCEDURE AND MANUFACTURED PRODUCTS FOR USE IN THE ADMINISTRATION OF ANTIHISTAMINES
US4495168A (en) * 1983-08-22 1985-01-22 Basf Wyandotte Corporation Aerosol gel
GB8501015D0 (en) * 1985-01-16 1985-02-20 Riker Laboratories Inc Drug
DE3522550A1 (en) * 1985-06-24 1987-01-02 Klinge Co Chem Pharm Fab SPRAYABLE PHARMACEUTICAL PREPARATION FOR TOPICAL APPLICATION
GB8522453D0 (en) * 1985-09-11 1985-10-16 Lilly Industries Ltd Chewable capsules
DE3544692A1 (en) * 1985-12-18 1987-06-19 Bayer Ag DIHYDROPYRIDINE SPRAY, METHOD FOR THE PRODUCTION THEREOF AND ITS PHARMACEUTICAL USE
US4689233A (en) * 1986-01-06 1987-08-25 Siegfried Aktiengesellschaft Coronary therapeutic agent in the form of soft gelatin capsules
EP0259383B1 (en) * 1986-03-10 1991-01-23 Kurt Dr. Burghart Pharmaceutical preparation and process for preparing the same
US4863970A (en) * 1986-11-14 1989-09-05 Theratech, Inc. Penetration enhancement with binary system of oleic acid, oleins, and oleyl alcohol with lower alcohols
JPH0645538B2 (en) * 1987-09-30 1994-06-15 日本化薬株式会社 Nitroglycerin spray
US5719197A (en) * 1988-03-04 1998-02-17 Noven Pharmaceuticals, Inc. Compositions and methods for topical administration of pharmaceutically active agents
GB8816187D0 (en) * 1988-07-07 1988-08-10 Glaxo Group Ltd Medicaments
HU199678B (en) * 1988-07-08 1990-03-28 Egyt Gyogyszervegyeszeti Gyar Process for producing aerosols containing nitroglicerol
US5128132A (en) * 1988-11-22 1992-07-07 Parnell Pharmaceuticals, Inc. Eriodictyon compositions and methods for treating internal mucous membranes
US5225183A (en) * 1988-12-06 1993-07-06 Riker Laboratories, Inc. Medicinal aerosol formulations
US5766573A (en) * 1988-12-06 1998-06-16 Riker Laboratories, Inc. Medicinal aerosol formulations
US4935243A (en) * 1988-12-19 1990-06-19 Pharmacaps, Inc. Chewable, edible soft gelatin capsule
US5011678A (en) * 1989-02-01 1991-04-30 California Biotechnology Inc. Composition and method for administration of pharmaceutically active substances
DE4007705C1 (en) * 1990-03-10 1991-09-26 G. Pohl-Boskamp Gmbh & Co. Chemisch-Pharmazeutische Fabrik, 2214 Hohenlockstedt, De
DE69122464T2 (en) * 1990-03-30 1997-02-20 Yasunori Morimoto TRANSDERMAL ABSORBABLE AGENT WITH MORPHINE HYDROCHLORIDE
AU7880991A (en) * 1990-05-10 1991-11-27 Novo Nordisk A/S A pharmaceutical preparation containing n-glycofurols and n-ethylene glycols
US5143731A (en) * 1990-08-07 1992-09-01 Mediventures Incorporated Body cavity drug delivery with thermo-irreversible polyoxyalkylene and ionic polysaccharide gels
US5135753A (en) * 1991-03-12 1992-08-04 Pharmetrix Corporation Method and therapeutic system for smoking cessation
ES2181673T3 (en) * 1991-05-01 2003-03-01 Jackson H M Found Military Med PROCESS OF TREATMENT OF INFECTIOUS RESPIRATORY DISEASES.
US5457100A (en) * 1991-12-02 1995-10-10 Daniel; David G. Method for treatment of recurrent paroxysmal neuropsychiatric
US5824307A (en) * 1991-12-23 1998-10-20 Medimmune, Inc. Human-murine chimeric antibodies against respiratory syncytial virus
PT679088E (en) * 1992-09-29 2002-12-31 Inhale Therapeutic Syst PULMONARY ADMINISTRATION OF ACTIVE FRAGMENTS OF PARTIROID HORMONE
ES2122261T3 (en) * 1993-03-17 1998-12-16 Minnesota Mining & Mfg AEROSOL FORMULATION CONTAINING A DISPERSION ADJUVANT DERIVED FROM AN ESTER, AMIDA OR MERCAPTOESTER.
US5362496A (en) * 1993-08-04 1994-11-08 Pharmetrix Corporation Method and therapeutic system for smoking cessation
GB9401891D0 (en) * 1994-02-01 1994-03-30 Boots Co Plc Therapeutic agents
US5502076A (en) * 1994-03-08 1996-03-26 Hoffmann-La Roche Inc. Dispersing agents for use with hydrofluoroalkane propellants
GB9405304D0 (en) * 1994-03-16 1994-04-27 Scherer Ltd R P Delivery systems for hydrophobic drugs
US5519059A (en) * 1994-08-17 1996-05-21 Sawaya; Assad S. Antifungal formulation
US5456677A (en) * 1994-08-22 1995-10-10 Spector; John E. Method for oral spray administration of caffeine
AUPM769394A0 (en) * 1994-08-25 1994-09-15 Commonwealth Scientific And Industrial Research Organisation Assay for the detection of proteases
US5563177A (en) * 1995-01-30 1996-10-08 American Home Products Corporation Taste masking guaifenesin containing liquids
US5908611A (en) * 1995-05-05 1999-06-01 The Scripps Research Institute Treatment of viscous mucous-associated diseases
US5635161A (en) * 1995-06-07 1997-06-03 Abbott Laboratories Aerosol drug formulations containing vegetable oils
US6258032B1 (en) * 1997-01-29 2001-07-10 William M. Hammesfahr Method of diagnosis and treatment and related compositions and apparatus
AUPN814496A0 (en) * 1996-02-19 1996-03-14 Monash University Dermal penetration enhancer
US5955098A (en) * 1996-04-12 1999-09-21 Flemington Pharmaceutical Corp. Buccal non polar spray or capsule
AU2190697A (en) * 1996-04-12 1997-11-07 Flemington Pharmaceutical Corporation Buccal polar spray or capsule
US5869082A (en) * 1996-04-12 1999-02-09 Flemington Pharmaceutical Corp. Buccal, non-polar spray for nitroglycerin
US6271240B1 (en) * 1996-05-06 2001-08-07 David Lew Simon Methods for improved regulation of endogenous dopamine in prolonged treatment of opioid addicted individuals
US5891465A (en) * 1996-05-14 1999-04-06 Biozone Laboratories, Inc. Delivery of biologically active material in a liposomal formulation for administration into the mouth
US5795909A (en) * 1996-05-22 1998-08-18 Neuromedica, Inc. DHA-pharmaceutical agent conjugates of taxanes
US6071539A (en) * 1996-09-20 2000-06-06 Ethypharm, Sa Effervescent granules and methods for their preparation
US5906811A (en) * 1997-06-27 1999-05-25 Thione International, Inc. Intra-oral antioxidant preparations
US20050163719A1 (en) * 1997-10-01 2005-07-28 Dugger Harry A.Iii Buccal, polar and non-polar spray containing diazepam
US20030077227A1 (en) * 1997-10-01 2003-04-24 Dugger Harry A. Buccal, polar and non-polar spray or capsule containing drugs for treating disorders of the central nervous system
US20040141923A1 (en) * 1997-10-01 2004-07-22 Dugger Harry A. Buccal, polar and non-polar spray containing alprazolam
US20030077228A1 (en) * 1997-10-01 2003-04-24 Dugger Harry A. Buccal, polar and non-polar spray or capsule containing drugs for treating endocrine disorders
US7632517B2 (en) * 1997-10-01 2009-12-15 Novadel Pharma Inc. Buccal, polar and non-polar spray containing zolpidem
US20040136914A1 (en) * 1997-10-01 2004-07-15 Dugger Harry A. Buccal, polar and non-polar spray containing ondansetron
US20040136915A1 (en) * 1997-10-01 2004-07-15 Dugger Harry A. Buccal, polar and non-polar spray containing atropine
US20050180923A1 (en) * 1997-10-01 2005-08-18 Dugger Harry A.Iii Buccal, polar and non-polar spray containing testosterone
US20030095927A1 (en) * 1997-10-01 2003-05-22 Dugger Harry A. Buccal, polar and non-polar spray or capsule containing drugs for treating muscular and skeletal disorders
US20030082107A1 (en) * 1997-10-01 2003-05-01 Dugger Harry A. Buccal, polar and non-polar spray or capsule containing drugs for treating an infectious disease or cancer
US20030095926A1 (en) * 1997-10-01 2003-05-22 Dugger Harry A. Buccal, polar and non-polar spray or capsule containing drugs for treating disorders of the gastrointestinal tract or urinary tract
US20030095925A1 (en) * 1997-10-01 2003-05-22 Dugger Harry A. Buccal, polar and non-polar spray or capsule containing drugs for treating metabolic disorders
EP1029536B1 (en) * 1997-10-01 2007-11-28 Novadel Pharma Inc. Buccal non-polar spray
US20030185761A1 (en) * 1997-10-01 2003-10-02 Dugger Harry A. Buccal, polar and non-polar spray or capsule containing drugs for treating pain
US20030077229A1 (en) * 1997-10-01 2003-04-24 Dugger Harry A. Buccal, polar and non-polar spray or capsule containing cardiovascular or renal drugs
US20050002867A1 (en) * 1997-10-01 2005-01-06 Novadel Pharma Inc. Buccal, polar and non-polar sprays containing propofol
US20030190286A1 (en) * 1997-10-01 2003-10-09 Dugger Harry A. Buccal, polar and non-polar spray or capsule containing drugs for treating allergies or asthma
US20040136913A1 (en) * 1997-10-01 2004-07-15 Dugger Harry A. Buccal, polar and non-polar spray containing sumatriptan
US6212227B1 (en) * 1997-12-02 2001-04-03 Conexant Systems, Inc. Constant envelope modulation for splitterless DSL transmission
US6375975B1 (en) * 1998-12-21 2002-04-23 Generex Pharmaceuticals Incorporated Pharmaceutical compositions for buccal and pulmonary application
CO5271697A1 (en) * 2000-01-12 2003-04-30 Pfizer Prod Inc COMPOSITIONS AND PROCEDURES FOR THE TREATMENT OF AFFECTIONS THAT RESPOND TO AN INCREASE OF TESTOSTERONE
CZ303537B6 (en) * 2000-03-09 2012-11-21 Gw Pharma Limited Use of cannabis for preparing pharmaceutical formulation and pump spray device
AU4866001A (en) * 2000-03-28 2001-10-08 Farmarc Nederland Bv Alprazolam inclusion complexes and pharmaceutical compositions thereof
EP1343521A2 (en) * 2000-12-01 2003-09-17 Battelle Memorial Institute Method for the stabilizing biomolecules (e.g. insulin) in liquid formulations
CA2649895C (en) * 2006-04-19 2013-03-26 Novadel Pharma Inc. Stable hydroalcoholic oral spray formulations and methods

Patent Citations (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US5178855A (en) * 1989-01-30 1993-01-12 Schering Corporation Treatment of luekocyte dysfunction with GM-CSF
US20060239928A1 (en) * 2005-02-17 2006-10-26 Heit Mark C Transmucosal administration of drug compositions for treating and preventing disorders in animals

Non-Patent Citations (1)

* Cited by examiner, † Cited by third party
Title
See also references of EP2124897A4 *

Cited By (11)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2010070236A1 (en) 2008-12-19 2010-06-24 Philippe Perovitch Formulation for the buccal transmucosal administration of setrons
FR2940120A1 (en) * 2008-12-19 2010-06-25 Philippe Perovitch FORMULATION FOR TRANSMUCOSAL DELIVERY OF SETRONS
FR2940116A1 (en) * 2008-12-22 2010-06-25 Philippe Perovitch FORMULATION FOR THE ADMINISTRATION OF HYPOALIMENTS BY ORAL TRANSMUCOSAL PATHWAY
WO2010072950A1 (en) * 2008-12-22 2010-07-01 Philippe Perovitch Formulation for delivering lipid-lowering drugs by oral transmucosal administration
RU2528897C2 (en) * 2008-12-22 2014-09-20 Филипп ПЕРОВИЧ Formulation for oral transmucosal use of lipid-lowering agents
US8889663B2 (en) 2008-12-22 2014-11-18 Philippe Perovitch Formulation for oral transmucosal administration of lipid-lowering drugs
FR2940911A1 (en) * 2009-01-13 2010-07-16 Philippe Perovitch FORMULATION FOR ORAL TRANSMUCOSAL ADMINISTRATION OF ANTALGIC AND / OR ANTI-SPASMODIC MOLECULES
WO2010081984A1 (en) * 2009-01-13 2010-07-22 Philippe Perovitch Formulation for oral transmucosal administration of analgesic and/or antispasmodic molecules
CN102245167A (en) * 2009-01-13 2011-11-16 菲利普·佩罗维奇 Formulation for oral transmucosal administration of analgesic and/or antispasmodic molecules
US9532947B2 (en) 2009-01-13 2017-01-03 Philippe Perovitch Formulation for oral transmucosal administration of analgesic and/or antispasmodic molecules
EP3068376A4 (en) * 2013-11-14 2017-06-07 Insys Pharma, Inc. Ondansetron sublingual spray formulation

Also Published As

Publication number Publication date
US20110171273A1 (en) 2011-07-14
CA2673049A1 (en) 2008-07-03
EP2124897A1 (en) 2009-12-02
CA2673049C (en) 2016-02-23
JP2010513525A (en) 2010-04-30
EP2124897A4 (en) 2012-05-09
US20080171089A1 (en) 2008-07-17

Similar Documents

Publication Publication Date Title
CA2673049C (en) Stable anti-nausea oral spray formulations and methods
EP2015632B1 (en) Stable hydroalcoholic oral spray formulations and methods
US20080031959A1 (en) Anti-migraine oral spray formulations and methods
EP2152247A1 (en) Anti-insomnia compositions and methods
CA2666581A1 (en) Buprenorphine-containing non-pressurised spray composition for transmucosal administration
EP3277283B1 (en) Sildenafil sublingual spray formulations
US20140275151A1 (en) Dye free liquid therapeutic solution
US20170105970A1 (en) Ondansetron sublingual spray formulation
US20210251886A1 (en) Oral mucosal delivery systems comprising monophasic concentrate of teriparatide
EP2338473B9 (en) Pharmaceutical dosage forms of tizanidine and administration route thereof
CN114828829A (en) Liquid composition comprising ibuprofen and phenylephrine
WO2021044357A1 (en) Apomorphine formulation
JP2017523231A (en) Afatinib drug kit for cancer treatment
CA3159285A1 (en) Liquid pharmaceutical composition comprising cytisine
EP3863604A1 (en) Oromucosal solutions of zolpidem or pharmaceutically acceptable salts thereof
ES2475942A1 (en) Pharmaceutical composition of sildenafil citrate in the form of an aqueous solution (Machine-translation by Google Translate, not legally binding)
PL241743B1 (en) Liquid pharmaceutical composition containing cytisine
US20140187629A1 (en) Use of Bethanechol for Treatment of Xerostomia

Legal Events

Date Code Title Description
121 Ep: the epo has been informed by wipo that ep was designated in this application

Ref document number: 07863183

Country of ref document: EP

Kind code of ref document: A1

WWE Wipo information: entry into national phase

Ref document number: 2673049

Country of ref document: CA

ENP Entry into the national phase

Ref document number: 2009542925

Country of ref document: JP

Kind code of ref document: A

NENP Non-entry into the national phase

Ref country code: DE

WWE Wipo information: entry into national phase

Ref document number: 2007863183

Country of ref document: EP