EP2097069A1 - Robuste oxymorphin-formulierungen mit verzögerter freisetzung - Google Patents

Robuste oxymorphin-formulierungen mit verzögerter freisetzung

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Publication number
EP2097069A1
EP2097069A1 EP06816745A EP06816745A EP2097069A1 EP 2097069 A1 EP2097069 A1 EP 2097069A1 EP 06816745 A EP06816745 A EP 06816745A EP 06816745 A EP06816745 A EP 06816745A EP 2097069 A1 EP2097069 A1 EP 2097069A1
Authority
EP
European Patent Office
Prior art keywords
oxymorphone
formulation
sustained release
ethanol
drug
Prior art date
Legal status (The legal status 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 status listed.)
Withdrawn
Application number
EP06816745A
Other languages
English (en)
French (fr)
Inventor
Anand R. Baichwal
Kevin Fitzmaurice
Steve Labudzinski
Michelle Howard-Sparks
William Hein
Allen Rychtman
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Penwest Pharmaceuticals Co
Original Assignee
Penwest Pharmaceuticals Co
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 Penwest Pharmaceuticals Co filed Critical Penwest Pharmaceuticals Co
Publication of EP2097069A1 publication Critical patent/EP2097069A1/de
Withdrawn legal-status Critical Current

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Classifications

    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/2004Excipients; Inactive ingredients
    • A61K9/2022Organic macromolecular compounds
    • A61K9/205Polysaccharides, e.g. alginate, gums; Cyclodextrin
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/14Particulate form, e.g. powders, Processes for size reducing of pure drugs or the resulting products, Pure drug nanoparticles
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/14Particulate form, e.g. powders, Processes for size reducing of pure drugs or the resulting products, Pure drug nanoparticles
    • A61K9/16Agglomerates; Granulates; Microbeadlets ; Microspheres; Pellets; Solid products obtained by spray drying, spray freeze drying, spray congealing,(multiple) emulsion solvent evaporation or extraction
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/2004Excipients; Inactive ingredients
    • A61K9/2022Organic macromolecular compounds
    • A61K9/205Polysaccharides, e.g. alginate, gums; Cyclodextrin
    • A61K9/2054Cellulose; Cellulose derivatives, e.g. hydroxypropyl methylcellulose
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • A61P25/04Centrally acting analgesics, e.g. opioids
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P29/00Non-central analgesic, antipyretic or antiinflammatory agents, e.g. antirheumatic agents; Non-steroidal antiinflammatory drugs [NSAID]

Definitions

  • the invention provides robust sustained release pharmaceutical formulations and methods for making and using same.
  • the formulations of the invention comprise at least one drug and a sustained release delivery system.
  • Sustained release drug formulations often contain higher amounts of drugs than immediate release formulations. Functionality and safety of a sustained release formulation are based on a known controlled rate of drug release from the formulation over an extended period of time after administration, such as 8-24 hours. The drug release profile of a formulation often depends on the chemical environment of the sustained release formulation, for example, on pH, ionic strength and presence of solvents such as ethanol.
  • the relatively high amount of drug that is present in a sustained release formulation can, in some instances, harm a patient if the formulation releases the drug at a rate that is faster than the intended controlled release rate. If the formulation releases the drug at a rate that is slower than the intended controlled release rate, the therapeutic efficacy of the drug can be reduced.
  • sustained release formulation results in a rapid release of the drug into the bloodstream. This rapid release is generally faster than the intended sustained release of the drug from the formulation, and is sometimes referred to as "dose dumping.”
  • Dose dumping can create severe consequences for a patient, including permanent harm and even death.
  • Oral dosage formulations are often taken with a commonly available beverage, such as water, juice, a carbonated beverage or occasionally an ethanol-containing beverage.
  • An ethanol-containing beverage is commonly referred to as an alcoholic beverage, liquor, or simply alcohol.
  • alcohol refers to ethanol, or an ethanol-containing (“alcoholic”) beverage such as beer, wine, and hard liquors such as vodka, rum, or whiskey.
  • Dose dumping in the presence of ethanol creates a safety concern because of the likelihood that a patient will ingest the formulation with an alcoholic beverage. This can be exacerbated where the drug may interact with the alcohol.
  • An additional safety concern is that a patient will consume alcoholic beverages while being treated with the drug in the formulation, even if the patient does not ingest the formulation at the same time as an alcoholic beverage.
  • Patients who desire to abuse a drug may want to intentionally induce dose dumping in order to magnify the euphoric effect of the drug.
  • a person wanting to abuse a drug might already be abusing alcohol, which increases the likelihood of the sustained release formulation of the drug to be ingested or taken concurrently with an alcoholic beverage.
  • AVTNZA® morphine sulfate extended-release capsules
  • AVTNZA 30 mg was mixed with 900 mL of buffer solutions containing ethanol (20% and 40%)
  • the dose of morphine that was released was alcohol concentration-dependent, leading to a more rapid release of morphine, which in vivo could result in the absorption of a potentially fatal dose of morphine.
  • Ligand Pharmaceuticals Inc. revised several sections of the AVINZA® prescribing information to highlight and strengthen the warning that patients should not consume alcohol while taking AVINZA®. Additionally, patients were warned not to use prescription or non-prescription medications containing alcohol while on AVINZA® therapy.
  • FDA has also indicated that for future sustained release products, in vitro testing for alcohol- induced undermining of sustained release characteristics may be advisable as a routine characterization test. Furthermore, FDA's position is that for certain drugs (e.g., drugs with a narrow therapeutic index or dire consequences of high C max or low C m i n ), alcohol sensitive sustained release formulations should not be approved. FDA prefers that formulations be made ethanol-resistant by design, rather than simply a confirmation that dose dumping does not occur through an in vivo study, (c.f. Summary of FDA's position on alcohol-induced dose dumping as presented at the Pharmaceutical Sciences Advisory Committee Meeting Oct. 26, 2005)
  • an in vivo alcohol resistance test is not the preferred approach due to potential harm the test could pose to a human subject.
  • the preferred approach is an in vitro dissolution test in the presence of 40% ethanol. This approach may be preferred because the strength of most common "hard” liquors is about 80 proof, or about 40% ethanol.
  • FDA is proposing classifying formulations into three groups: rugged, vulnerable and uncertain. At the Pharmaceutical Sciences Advisory Committee Meeting of Oct. 26, 2005, OPS (Office of Pharmaceutical Science) at the CDER (Center for Drug Evaluation and Research) personnel presented data showing that in a vulnerable formulation, a higher concentration of ethanol (e.g., 40%) is likely to trigger faster drug release than a lower concentration of ethanol (e.g., 20% or 4%).
  • Oxymorphone HCl 14-hydroxydihydromorphinone hydrochloride
  • Oxymorphone HCl 14-hydroxydihydromorphinone hydrochloride
  • Oxymorphone is currently marketed as an injection (1 mg/ml in 1 ml ampules) for intramuscular, subcutaneous, and intravenous administration. At one time, a 10 mg oral immediate release tablet fo ⁇ nation of oxymorphone HCl was marketed. Oxymorphone HCl is metabolized principally in the liver and undergoes conjugation with glucuronic acid and reduction to 6-alpha and 6-beta hydroxy epimers.
  • An important goal of analgesic therapy is to achieve continuous relief of chronic pain.
  • Regular administration of an analgesic is generally required to ensure that the next dose is given before the effects of the previous dose have worn off.
  • Compliance with opioids increases as the required dosing frequency decreases.
  • Non-compliance results in suboptimal pain control and poor quality of life outcomes.
  • Scheduled rather than "as needed" administration of opioids is currently recommended in guidelines for their use in treating chronic non-malignant pain.
  • Unfortunately evidence from prior clinical trials and clinical experience suggests that the short duration of action of immediate release oxymorphone would necessitate administration every four hours in order to maintain optimal levels of analgesia in patients with chronic pain.
  • immediate release oxymorphone exhibits low oral bioavailability, because oxymorphone is extensively metabolized in the liver. Because many drugs, e.g., opioids such as oxymorphone, can cause serious adverse effects or even death to a patient if the sustained release formulation fails, there is a need in the art for pharmaceutical formulations that are more robust or rugged, and therefore safer, when compared to currently available sustained release formulations.
  • sustained release formulations have been described in U.S. Pat. No. 5,399,358, the disclosure of which is incorporated by reference herein in its entirety. It has now been unexpectedly discovered that the particle size of hydrophilic gums, e.g., xanthan gum, affects the robustness and dissolution properties of sustained release formulations.
  • the invention provides sustained release pharmaceutical formulations and solid dosage forms comprising the sustained release formulations.
  • the invention also provides methods for treating a patient using the sustained release formulations and methods for preventing dose dumping, for example, by providing to patients a therapeutically effective amount of a sustained release drug formulation.
  • the pharmaceutical formulations described herein are less likely to dose dump compared to conventional sustained release formulations, which makes them more rugged, safer, and applicable to a wide variety of drugs.
  • the invention further provides ethanol-resistant pharmaceutical fo ⁇ nulations and methods for increasing drug safety and reducing the potential for drug abuse. This can be achieved by providing, prescribing and/or administering to patients an effective amount of an ethanol-resistant drug formulation.
  • the ethanol-resistant drug formulations are safer and have less potential for abuse when compared to commercially available formulations because their sustained release dissolution profile in an aqueous solution or in an ethanol-containing solution is essentially the same.
  • the drug in the ethanol-resistant formulation comprises an opioid compound or a derivative thereof.
  • the invention also provides ethanol-resistant pharmaceutical formulations and methods for preventing dose dumping. This can be achieved by providing, prescribing and/or administering to patients an effective amount of an ethanol-resistant drug formulation.
  • the ethanol-resistant pharmaceutical formulations described herein do not dose dump in the presence of beverage-strength ethanol.
  • the drug in the ethanol-resistant formulation comprises an opioid compound, a pharmaceutically acceptable salt of an opioid compound, or a derivative thereof.
  • the invention provides a sustained release formulation comprising: a drug; and a sustained release delivery system comprising a hydrophilic gum, a homopolysaccharide gum, and a pharmaceutical diluent, wherein at least about 30% of the hydrophilic gum used to make the sustained release fo ⁇ nulation can pass through a #270 mesh sieve and the sustained release formulation releases less than about 70% of the drug within 2 hours after ingestion with either an ethanol-free or an ethanol-containing beverage.
  • the invention provides a sustained release formulation comprising: a drag; and a sustained release delivery system comprising a hydrophilic gum, a cationic cross-linking compound selected from monovalent cations, multivalent cations and salts, and a pharmaceutical diluent, wherein at least about 30% of the hydrophilic gum used to make the sustained release fonnulation can pass through a #270 mesh sieve and the sustained release fo ⁇ nulation releases less than about 70% of the drug within 2 hours after ingestion with either an ethanol-free or an ethanol-containing beverage.
  • the hydrophilic gum is a heteropolysaccharide gum. In some embodiments, the hydrophilic gum is xanthan gum.
  • the sustained release delivery system further comprises a cationic cross-linking compound selected from monovalent cations, multivalent cations, and salts.
  • the cationic cross-linking agent is a sodium salt.
  • the invention provides a sustained release fonnulation comprising: a drug; and a sustained release delivery system comprising a hydrophilic gum, a homopolysaccharide gum, and a pharmaceutical diluent, wherein at least about 30% of the hydrophilic gum particles used to make the sustained release formulation are smaller than about 53 microns in diameter and the sustained release formulation releases less than 70% of the drag within 2 hours after ingestion with either an ethanol-free or an ethanol-containing beverage.
  • the invention provides a sustained release formulation comprising: a drug; and a sustained release delivery system comprising a hydrophilic gum, a cationic cross-linking compound selected from monovalent cations, multivalent cations and salts, and a pharmaceutical diluent, wherein at least about 30% of the hydrophilic gum particles used to make the sustained release formulation are smaller than about 53 microns in diameter and the sustained release formulation releases less than 70% of the drug within 2 hours after ingestion with either an ethanol-free or an ethanol- containing beverage.
  • the sustained delivery system further comprises a hydrophobic polymer.
  • the sustained release formulation further comprises an outer coating.
  • the outer coating comprises a hydrophobic polymer and/or a plasticizer.
  • the drug is a water-soluble drug.
  • the drug is an anti-depressant, a drug used to treat bipolar disorder, panic disorder, epilepsy, migraine, and/or attention deficit hyperactivity disorder.
  • the drug is selected from the group consisting of alprazolam, lithium carbonate, divalproex sodium, neutral sulfate salts of dextroamphetamine and amphetamine with the dextro isomer of amphetamine saccharate and d,l-amphetamine aspartate monohydrate, tramadol hydrochloride, and other pharmaceutically acceptable salts of the active pharmaceutical ingredient thereof.
  • the drug is an opioid, e.g., alfentanil, allylprodine, alphaprodine, anileridine, benzylmorphine, bezitramide, buprenorphine, butorphanol, clonitazene, codeine, cyclazocine, desomorphine, dextromoramide, dezocine, diampromide, dihydrocodeine, dihydromorphine, dimenoxadol, dimepheptanol, dimethylthiambutene, dioxaphetyl butyrate, dipipanone, eptazocine, ethoheptazine, ethylmethylthiambutene, ethylmorphine, etonitazine, fentanyl, heroin, hydrocodone, hydromorphone, hydroxypethidine, isomethadone, ketobemidone, levallorphan, levorphanol, levophenacylmorphan
  • opioid
  • the invention provides a method for making a sustained release formulation comprising: a drug; and a sustained release delivery system, wherein the sustained release delivery system comprises a hydrophilic gum, a homopolysaccharide gum, and a pharmaceutical diluent, the method comprising: providing the hydrophilic gum with at least a fraction of particles less than about 53 microns in diameter; granulating the hydrophilic gum, the homopolysaccharide gum and the phannaceutical diluent to form granules; mixing the granules with the drug to form a granulated composition; and applying pressure to the granulated composition to make the fo ⁇ nulation.
  • the invention provides a method for making a sustained release formulation comprising: a drug; and a sustained release delivery system, wherein the sustained release delivery system comprises a hydrophilic gum, a cationic cross-linking compound selected from monovalent cations, multivalent cations and salts, and a pharmaceutical diluent, the method comprising: providing the hydrophilic gum with at least a fraction of particles less than about 53 microns in diameter; granulating the hydrophilic gum, the homopolysaccharide gum and the pharmaceutical diluent to form granules; mixing the granules with the drug to form a granulated composition; and applying pressure to the granulated composition to make the formulation.
  • providing comprises receiving, manufacturing, and/or processing the hydrophilic gum.
  • processing comprises measuring the size of at least a fraction of the hydrophilic gum particles and/or passing at least a fraction of the hydrophilic gum through a sieve.
  • the sieve is a #270 mesh sieve.
  • the method for making the sustained release fo ⁇ nulation and a solid dosage fo ⁇ n further comprises applying an outer coating onto at least part of the sustained release formulation.
  • granulating comprises mixing ingredients with a solution comprising water. In other embodiments, granulating comprises mixing ingredients with an alcohol solution, for example a solution comprising ethanol.
  • the invention provides a method for making a sustained release fo ⁇ nulation comprising: a drug; and a sustained release delivery system, wherein the sustained release delivery system comprises a hydrophilic gum, a homopolysaccharide gum, and a pharmaceutical diluent, the method comprising: mixing the hydrophilic gum of average and/or mean particle size larger than about 53 microns in diameter, the homopolysaccharide gum and the pharmaceutical diluent with a solution comprising water to form granules; mixing the granules with drug to form a granulated composition; and applying pressure to the granulated composition to make the fo ⁇ nulation.
  • the invention provides a method for making a sustained release fo ⁇ nulation comprising: a drug; and a sustained release delivery system, wherein the sustained release delivery system comprises a hydrophilic gum, a cationic cross-linking compound selected from monovalent cations, multivalent cations and salts, and pham ⁇ aceutical diluent, the method comprising: mixing the hydrophilic gum of average and/or mean particle size larger than about 53 microns in diameter, the cationic cross- linking compound and the pharmaceutical diluent with a solution comprising water to fonn granules; mixing the granules with the drug to form a granulated composition; and applying pressure to the granulated composition to make the formulation.
  • a method for making a sustained release foraiulation further comprises recording a dissolution profile of the sustained release formulation or a solid dosage form comprising the sustained release fom ⁇ ulation in an ethanol-containing solution.
  • the invention provides a method for relieving pain comprising administering to a patient a therapeutically effective amount of a sustained release fonnulation or a solid dosage fo ⁇ n comprising a sustained release formulation described herein.
  • the invention provides a method for treating a patient having a condition comprising administering to the patient a therapeutically effective amount of a sustained release formulation or a solid dosage form comprising a sustained release formulation described herein.
  • the invention provides a method for reducing dose dumping of a sustained release drug formulation comprising providing a patient a sustained release formulation described herein.
  • the invention provides a solid dosage form comprising a sustained release formulation described herein.
  • the solid dosage form is a powder, a granule, a tablet, or a capsule.
  • the sustained release formulation comprises from about 5 to about 80 mg of oxymorphone hydrochloride and about 80 mg to about 360 mg of a sustained release delivery system; wherein the sustained release delivery system comprises from about 8.3% to about 41.7% by weight locust bean gum from about 8.3% to about 41.7% by weight xanthan gum wherein at least about 30% of the xanthan gum particles can pass through a #270 mesh sieve; from about 20% to about 55% by weight dextrose, from about 5% to about 20% by weight calcium sulfate dihydrate, and from about 2% to about 10% ethyl cellulose, and the sustained release formulation releases less than 70% of the drug within 2 hours after ingestion with either an ethanol-free or an ethanol-containing beverage.
  • the sustained release formulation comprises from about 5 to about 80 mg of oxymorphone hydrochloride and from about 300 mg to about 420 mg of a sustained release delivery system; wherein the sustained release delivery system comprises from about 8.3% to about 41.7% by weight locust bean gum, from about 8.3% to about 41.7% by weight xanthan gum having at least about 30% of particles smaller than about 53 microns in diameter; from about 20% to about 55% by weight dextrose, from about 5% to about 20% by weight calcium sulfate dihydrate, and from about 2% to about 10% ethyl cellulose, and the sustained release formulation releases less than 70% of the drug within 2 hours after ingestion with either an ethanol-free or an ethanol- containing beverage.
  • the sustained release formulation comprises about 20 mg of oxymorphone hydrochloride. In another embodiment, the sustained release formulation comprises about 160 mg of a sustained release delivery system. In yet another embodiment, the sustained release formulation comprises about 360 mg of a sustained release delivery system. In still another embodiment, the sustained release delivery system comprises about 25% locust bean gum, about 25% xanthan gum, about 35% dextrose, about 10% calcium sulfate dihydrate, and about 5% ethyl cellulose.
  • the invention provides a method of preventing dose-dumping of a drug in the presence of ethanol comprising: providing a patient who could consume ethanol while being treated with the drug an effective amount of the drug in the form of an ethanol-resistant sustained release fo ⁇ nulation comprising: the drug; and a sustained release delivery system, the delivery system comprising at least one hydrophilic gum, at least one homopolysaccharide gum and at least one pharmaceutical diluent, wherein at least about 30% of the hydrophilic gum used to make the sustained release fo ⁇ nulation can pass through a #270 mesh sieve and the sustained release formulation releases less than about 70% of the drug within 2 hours after ingestion with either an ethanol-free or an ethanol-containing beverage.
  • the invention provides a method of preventing dose-dumping of a drug in the presence of ethanol comprising: providing a patient who could consume ethanol while being treated with the drug an effective amount of the drug in the form of an ethanol-resistant sustained release formulation comprising: the drug; and a sustained release delivery system, the delivery system comprising at least one hydrophilic gum, at least one cationic cross-linking compound selected from monovalent metal cations, multivalent metal cations and salts, and at least one pharmaceutical diluent, wherein at least about 30% of the hydrophilic gum used to make the sustained release formulation can pass through a #270 mesh sieve and the sustained release formulation releases less than about 70% of the drug within 2 hours after ingestion with either an ethanol-free or an ethanol-containing beverage.
  • the invention provides a method of improving safety of a drug formulation comprising: providing a patient who could consume ethanol while being treated with the drug an effective amount of the drug in the form of an ethanol-resistant sustained release formulation comprising: the drug; and a sustained release delivery system, the sustained release delivery system comprising at least one hydrophilic gum, at least one homopolysaccharide gum and at least one pharmaceutical diluent, wherein the improvement in safety is a result of controlled hydrophilic gum particle size and ethanol- resistant sustained release properties of the formulation.
  • the invention provides a method of improving safety of a drug formulation comprising: providing a patient who could consume ethanol while being treated with the drug an effective amount of the drug in the form of an ethanol-resistant sustained release formulation comprising: the drug; and a sustained release delivery system, the delivery system comprising at least one hydrophilic gum, at least one cationic cross-linking compound selected from monovalent metal cations, multivalent metal cations and salts, and at least one pharmaceutical diluent, wherein the improvement in safety is a result of controlled hydrophilic gum particle size and ethanol-resistant sustained release properties of the formulation.
  • the invention provides a sustained release oxymorphone formulation comprising a sustained release delivery system and from about 5 mg to about 80 mg of oxymorphone, wherein after oral administration of a single dose to a patient with about 200 mL to about 300 mL of about 4% to about 40% ethanol the formulation provides a secondary peak of blood oxymorphone concentration about 12 hours after administration, and the formulation provides analgesia to the patient for at least about 12 hours after administration.
  • the formulation comprises from about 20 mg to about 60 mg of oxymorphone or about 40 mg of oxymorphone.
  • the formulation is a solid dosage, for example, a tablet, a granule, a capsule or a powder.
  • the invention provides a sustained release oxymorphone formulation comprising a sustained release delivery system and from about 5 mg to about 80 mg of oxymorphone, wherein after oral administration of a single dose to a patient the formulation provides a maximum blood concentration of oxymorphone less than about 5 times higher when ingested with about 200 mL to about 300 mL of up to about 40% ethanol compared to when ingested without ethanol, and the fonnulation provides analgesia to the patient for at least about 12 hours after administration.
  • the maximum blood concentration of oxymorphone is less than about 2.5 times higher when ingested with about 200 mL to about 300 mL of up to about 40% ethanol compared to when ingested without ethanol.
  • the formulation comprises from about 20 mg to about 60 mg of oxymorphone or about 40 mg of oxymorphone.
  • the formulation is a solid dosage, for example, a tablet, a granule, a capsule or a powder.
  • the invention provides a sustained release oxymorphone formulation comprising a sustained release delivery system and from about 5 mg to about 80 mg of oxymorphone, wherein after oral administration of a single dose to a patient the formulation provides a ratio of the maximum blood concentration of oxymorphone when ingested with about 200 mL to about 300 mL of about 40% ethanol to the maximum blood concentration of oxymorphone when ingested after a high-fat meal without ethanol from about 0.5 to about 2, and the formulation provides analgesia to the patient for at least about 12 hours after administration.
  • the ratio of the maximum blood concentration of oxymorphone when the formulation is ingested with about 200 mL to about 300 mL of about 40% ethanol to the maximum blood concentration of oxymorphone when the formulation is ingested after a high- fat meal without ethanol is from about 0.8 to about 1.5.
  • the formulation comprises from about 20 mg to about 60 mg of oxymorphone or about 40 mg of oxymorphone.
  • the formulation is a solid dosage, for example, a tablet, a granule, a capsule or a powder.
  • the invention provides a sustained release oxymorphone formulation comprising a sustained release delivery system and from about 5 mg to about 80 mg of oxymorphone, wherein after oral administration of a single dose to a patient with about 200 mL to about 300 mL of about 4% to about 40% ethanol the formulation provides a maximum blood concentration of oxymorphone from about 0.1 ng/mL to about 15 ng/mL, and the formulation provides analgesia to the patient for at least about 12 hours after administration.
  • the formulation provides a maximum blood concentration of oxymorphone from about 0.5 ng/mL to about 7.5 ng/mL or from about 1 ng/mL to about 4 ng/mL.
  • the formulation comprises from about 10 mg to about 20 mg of oxymorphone and the formulation provides a maximum blood concentration of oxymorphone from about 0.3 ng/mL to about 3.2 ng/mL or from about 0.4 ng/mL to about 2.8 ng/mL.
  • the formulation comprises about 10 mg of oxymorphone and the formulation provides a maximum blood concentration of oxymorphone from about 0.3 ng/mL to about 1.8 ng/mL or from about 0.5 ng/mL to about 1.5 ng/mL.
  • the formulation comprises from about 20 mg to about 40 mg of oxymorphone and the formulation provides a maximum blood concentration of oxymorphone from about 0.5 ng/mL to about 7 ng/mL or from about 0.9 ng/mL to about 6 ng/mL. In yet another embodiment, the formulation comprises about 20 mg of oxymorphone and the formulation provides a maximum blood concentration of oxymorphone from about 0.5 ng/mL to about 3.2 ng/mL or from about 0.75 ng/mL to about 2.8 ng/mL.
  • the formulation comprises from about 40 mg to about 80 mg of oxymorphone and the formulation provides a maximum blood concentration of oxymorphone from about 1 ng/mL to about 15 ng/mL or from about 1.9 ng/mL to about
  • the formulation comprises about 40 mg of oxymorphone and the formulation provides a maximum blood concentration of oxymorphone from about 1 ng/mL to about 7 ng/mL or from about 1.4 ng/mL to about 5 ng/mL.
  • the formulation comprises about 80 mg of oxymorphone and the fo ⁇ nulation provides a maximum blood concentration of oxymorphone from about 3.5 ng/mL to about 15 ng/mL or from about 4 ng/mL to about
  • the invention provides a sustained release oxymorphone fo ⁇ nulation comprising a sustained release delivery system and from about 5 mg to about 80 mg of oxymorphone, wherein the formulation provides a minimum blood concentration of oxymorphone of at least about 0.013 ng/mL at about 12 hours after oral administration of a single dose to a patient with about 200 mL to about 300 mL of about 4% to about 40% ethanol, and the formulation provides analgesia to the patient for at least about 12 hours after administration.
  • the formulation comprises about 5 mg of oxymorphone and provides a minimum blood concentration of oxymorphone of at least about 0.07 ng/mL.
  • the formulation comprises about 10 mg of oxymorphone and provides a minimum blood concentration of oxymorphone of at least about 0.15 ng/mL.
  • the formulation comprises about 20 mg of oxymorphone and provides a minimum blood concentration of oxymorphone of at least about 0.3 ng/mL.
  • the formulation comprises about 40 mg of oxymorphone and provides a minimum blood concentration of oxymorphone of at least about 0.6 ng/mL.
  • the formulation comprises about 80 mg of oxymorphone and provides a minimum blood concentration of oxymorphone of at least about 1.2 ng/mL.
  • the formulation is a solid dosage form, for example, a tablet, a capsule, a granule, or a powder.
  • the invention provides a method of relieving pain comprising administering to a patient a sustained release oxymorphone formulation comprising a sustained release delivery system and from about 5 mg to about 80 mg of oxymorphone, wherein after oral administration of a single dose to the patient with about 200 mL to about 300 mL of about 4% to about 40% ethanol the formulation provides a secondary peak of blood oxymorphone concentration about 12 hours after administration, and the formulation provides analgesia to the patient for at least about 12 hours after administration.
  • the formulation comprises from about 20 mg to about 60 mg of oxymorphone or about 40 mg of oxymorphone.
  • the formulation is a solid dosage, for example, a tablet, a granule, a capsule or a powder.
  • the invention provides a method of relieving pain comprising administering to a patient a sustained release oxymorphone formulation comprising a sustained release delivery system and from about 5 mg to about 80 mg of oxymorphone, wherein after oral administration of a single dose to a patient the formulation provides a maximum blood concentration of oxymorphone less than about 5 times higher when ingested with about 200 mL to about 300 mL of up to about 40% ethanol compared to when ingested without ethanol, and the formulation provides analgesia to the patient for at least about 12 hours after administration.
  • the maximum blood concentration of oxymorphone is less than about 2.5 times higher when ingested with about 200 mL to about 300 mL of up to about 40% ethanol compared to when ingested without ethanol.
  • the formulation comprises from about 20 mg to about 60 mg of oxymorphone or about 40 mg of oxymorphone.
  • the fo ⁇ nulation is a solid dosage, for example a tablet, a granule, a capsule or a powder.
  • the invention provides a method of relieving pain comprising administering to a patient a sustained release oxymorphone formulation comprising a sustained release delivery system and from about 5 mg to about 80 mg of oxymorphone, wherein after oral administration of a single dose to a patient the formulation provides a ratio of the maximum blood concentration of oxymorphone when ingested with about 200 mL to about 300 mL of about 40% ethanol to the maximum blood concentration of oxymorphone when ingested after a high-fat meal without ethanol of about 0.5 to about 2, and the fo ⁇ nulation provides analgesia to the patient for at least about 12 hours after administration.
  • the ratio of the maximum blood concentration of oxymorphone when the formulation is ingested with about 200 mL to about 300 mL of about 40% ethanol to the maximum blood concentration of oxymorphone when the formulation is ingested after a high- fat meal without ethanol is from about 0.8 to about 1.5.
  • the formulation comprises from about 20 mg to about 60 mg of oxymorphone or about 40 mg of oxymorphone.
  • the formulation is a solid dosage, for example, a tablet, a granule, a capsule or a powder.
  • the invention provides a method of relieving pain comprising administering to a patient a sustained release oxymorphone formulation comprising a sustained release delivery system and from about 5 mg to about 80 mg of oxymorphone, wherein after oral administration of a single dose to a patient with about 200 mL to about 300 mL of about 4% to about 40% ethanol the formulation provides a maximum blood concentration of oxymorphone from about 0,1 ng/mL to about 15 ng/mL, and the formulation provides analgesia to the patient for at least about 12 hours after administration.
  • the formulation provides a maximum blood concentration of oxymorphone from about 0.5 ng/mL to about 7.5 ng/mL or from about 1 ng/mL to about 4 ng/mL.
  • the formulation comprises from about 10 mg to about 20 mg of oxymorphone and the formulation provides a maximum blood concentration of oxymorphone from about 0.3 ng/mL to about 3.2 ng/mL or from about 0.4 ng/mL to about 2.8 ng/mL.
  • the formulation comprises about 10 mg of oxymorphone and the formulation provides a maximum blood concentration of oxymorphone from about 0.3 ng/mL to about 1.8 ng/mL or from about 0.5 ng/mL to about 1.5 ng/mL.
  • the formulation comprises from about 20 mg to about 40 mg of oxymorphone and the formulation provides a maximum blood concentration of oxymorphone from about 0.5 ng/mL to about 7 ng/mL or from about 0.9 ng/mL to about 6 ng/mL.
  • the formulation comprises about 20 mg of oxymorphone and the formulation provides a maximum blood concentration of oxymorphone from about 0.5 ng/mL to about 3.2 ng/mL or from about 0.75 ng/mL to about 2.8 ng/mL.
  • the fo ⁇ nulation comprises from about 40 mg to about 80 mg of oxymorphone and the formulation provides a maximum blood concentration of oxymorphone from about 1 ng/mL to about 15 ng/mL or from about 1.9 ng/mL to about 12 ng/mL.
  • the formulation comprises about 40 mg of oxymorphone and the formulation provides a maximum blood concentration of oxymorphone from about 1 ng/mL to about 7 ng/mL or from about 1.4 ng/mL to about 5 ng/mL.
  • the formulation comprises about 80 mg of oxymorphone and the fo ⁇ nulation provides a maximum blood concentration of oxymorphone from about 3.5 ng/mL to about 15 ng/mL or from about 4 ng/mL to about 13 ng/mL.
  • the invention provides a method of relieving pain comprising administering to a patient a sustained release oxymorphone formulation comprising a sustained release delivery system and from about 5 mg to about 80 mg of oxymorphone, wherein the formulation provides a minimum blood concentration of oxymorphone of at least about 0.013 ng/mL at about 12 hours after oral administration of a single dose to a patient with about 200 mL to about 300 mL of about 4% to about 40% ethanol, and the formulation provides analgesia to the patient for at least about 12 hours after administration.
  • the fo ⁇ nulation comprises about 5 mg of oxymorphone and provides a minimum blood concentration of oxymorphone of at least about 0.07 ng/mL.
  • the formulation comprises about 10 mg of oxymorphone and provides a minimum blood concentration of oxymorphone of at least about 0.15 ng/mL.
  • the formulation comprises about 20 mg of oxymorphone and provides a minimum blood concentration of oxymorphone of at least about 0.3 ng/mL.
  • the formulation comprises about 40 mg of oxymorphone and provides a minimum blood concentration of oxymorphone of at least about 0.6 ng/mL.
  • the formulation comprises about 80 mg of oxymorphone and provides a minimum blood concentration of oxymorphone of at least about 1.2 ng/mL.
  • Sustained release formulations described herein can be used in therapy.
  • sustained release formulations described herein can be used in the manufacture of a medicament for treatment of a condition.
  • the sustained release formulations described herein can be used for the manufacture of a medicament for relieving pain.
  • the formulation is a solid dosage form, for example, a tablet, a capsule, a granule, or a powder.
  • the conjunction "or” is used in the inclusive sense of “and/or” and not the exclusive sense of "either/or.”
  • the term “robust” refers to a property of a sustained release formulation that makes it less likely to have its dissolution profile substantially modified, injured, or otherwise fail. An example of a failure of a sustained release formulation is dose dumping. "Robust” and “rugged” are meant to be synonyms.
  • fine refers to a particle size of a polymer having a diameter smaller than 53 microns, or alternatively, having particles capable of passing through a #270 mesh sieve.
  • dose dumping refers to a rapid release of a drug or an active ingredient from a sustained release formulation into the bloodstream. This rapid release is generally faster than the sustained release of a drug from the fo ⁇ nulation. Dose dumping also refers to a release having a peak concentration of the drug in the blood plasma higher than the peak concentration of the intended sustained release of the drug.
  • sustained release means that the drug is released from the fo ⁇ nulation at a controlled rate so that therapeutically beneficial blood levels (but below toxic levels) of the drug are maintained over an extended period of time.
  • sustained release means that the drug is released from the formulation in a short period of time, e.g., within about 4 hours after administration of the formulation.
  • AUC refers to the area under the concentration-time curve.
  • C max refers to the maximum observed concentration
  • RSD refers to the relative standard deviation
  • CI refers to the confidence interval
  • high-fat meal refers to a meal wherein approximately 50 percent of total caloric content of the meal is derived from fat.
  • An example of a high- fat meal is two eggs fried in butter, two strips of bacon, two slices of toast with butter, four ounces of hash brown potatoes and eight ounces of whole milk.
  • liquids includes, for example, gastrointestinal fluids, aqueous solutions (such as those used for in vitro dissolution testing), and mucosas (e.g., of the mouth, nose, lungs, esophagus, and the like).
  • ethanol-resistant refers to releasing less than 50% of an active ingredient (e.g., a drug) within one hour in a dissolution profile measurement by USP Procedure Drug Release USP 23 in 0.1N HCl and 40% ethanol solution.
  • drug includes any pharmaceutically active chemical or biological compound, and any pharmaceutically acceptable salt thereof, used for alleviating symptoms, treating or preventing a condition.
  • Drugs suited for the robust sustained release formulations described herein include, but are not limited to, alprazolam (XANAX XR®), lithium carbonate (LITHOBID®), divalproex sodium (DEPAKOTE®), neutral sulfate salts of dextroamphetamine and amphetamine, with the dextro isomer of amphetamine saccharate and d,l-amphetamine aspartate monohydrate (ADDERALL XR®), tramadol hydrochloride (TRAMADOL ER®) and opioids such as morphine (AVTNZA® and KADIAN®) and oxycodone (OXYCONTIN ® ).
  • alprazolam XANAX XR®
  • LITHOBID® lithium carbonate
  • DEPAKOTE® divalproex sodium
  • ADDERALL XR® dextro isomer of amphetamine saccharate and d,l-amphetamine aspartate monohydrate
  • opioid includes stereoisomers thereof, metabolites thereof, salts thereof, ethers thereof, esters thereof and/or derivatives thereof (e.g. , pharmaceutically acceptable salts thereof).
  • the opioids may be mu-antagonists and/or mixed mu-agonists/antagonists.
  • opioids include alfentanil, allylprodine, alphaprodine, anileridine, benzylmorphine, bezitramide, bupreno ⁇ hine, butorphanol, clonitazene, codeine, cyclazocine, desomorphine, dextromoramide, dezocine, diampromide, dihydrocodeine, dihydromorphine, dimenoxadol, dimepheptanol, dimethylthiambutene, dioxaphetyl butyrate, dipipanone, eptazocine, ethoheptazine, ethylmethylthiambutene, ethylmorphine, etonitazine, fentanyl, heroin, hydrocodone, hydromorphone, hydroxypethidine, isomethadone, ketobemidone, levallo ⁇ han, levorphanol, levophenacylmorphan, lofentanil, me
  • the opioid is mo ⁇ hine, codeine, hydromo ⁇ hone, hydrocodone, oxycodone, dihydrocodeine, dihydromo ⁇ hine, oxymo ⁇ hone, 6-hydroxyoxymo ⁇ hone (including 6- ⁇ -hydroxyoxymo ⁇ hone and/or 6- ⁇ - hydroxyoxymo ⁇ hone), or tramadol.
  • oxymo ⁇ hone includes oxymo ⁇ hone, metabolites thereof, and derivatives thereof. Metabolites of oxymo ⁇ hone include, for example, 6- hydroxyoxymo ⁇ hone (e.g., 6- ⁇ -hydroxyoxymo ⁇ hone and/or 6- ⁇ - hydroxyoxymo ⁇ hone) .
  • condition includes any disease or a collection of symptoms that requires treatment with a drug.
  • exemplary conditions include panic disorder (with or without agoraphobia), bipolar disorder (manic depressive illness), acute manic or mixed episodes associated with bipolar disorder, epilepsy, migraine, attention deficit hyperactivity disorder (ADHD), depression and pain.
  • the pain can be minor to moderate, or moderate to severe.
  • the pain can be acute or chronic.
  • the pain can also be persistent and require continuous around-the-clock relief for an extended period of time.
  • the pain can be associated with, for example, cancer, autoimmune diseases, infections, surgical traumas, or accidental traumas.
  • the patient can be an animal, a mammal, or a human.
  • the drug may be in the form of any pharmaceutically acceptable salt known in the art.
  • exemplary pharmaceutically acceptable salts include hydrochloric, sulfuric, nitric, phosphoric, hydrobromic, maleric, malic, ascorbic, citric, tartaric, pamoic, lauric, stearic, palmitic, oleic, myristic, lauryl sulfuric, napthalinesulfonic, linoleic, linolenic acid, and the like.
  • the robust sustained release formulations of drugs are administered in an amount sufficient to alleviate symptoms, treat or prevent a condition for an extended period of time, for example about 8 hours to about 24 hours, or for a period of about 12 hours to about 24 hours.
  • the robust sustained release oral solid dosage fo ⁇ nulations described herein may be administered four times a day, three times a day, twice daily, or only once daily.
  • the sustained release formulations of opioids are administered in an amount sufficient to alleviate pain for an extended period of time, for example about 8 hours to about 24 hours, or for a period of about 12 hours to about 24 hours.
  • the opioid sustained release oral solid dosage formulations described herein may be administered four times a day, three times a day, twice daily, or only once daily.
  • a therapeutically effective amount of a drug is an amount sufficient to eliminate or to alleviate symptoms of a condition (e.g., reduce the pain compared to the pain present prior to administration of the opioid sustained release fo ⁇ nulation).
  • the drug can be present in the composition in an amount of about 0.5 milligrams to about 1000 milligrams, in an amount of about 1 milligram to about 800 milligrams, in an amount of about 1 milligram to about 200 milligrams, or in an amount of about 1 milligram to about 100 milligrams.
  • hydrophilic gums e.g., xanthan gum
  • dissolution properties of the sustained release formulations and solid dosage forms comprising the sustained release formulations thereby affecting their robustness.
  • a drug e.g., an opioid
  • particle size of hydrophilic gums has been found to affect robustness of ethanol/ethylcellulose granulated formulation.
  • ethanol/ethylcellulose granulated formulations comprising xanthan gum as the hydrophilic gum are robust when the fraction of particles smaller than 53 microns in diameter is about 30% or more.
  • this fraction might be smaller or larger, for example between about 20-80%, about 40-60%, or about 50%.
  • hydrophilic gum particles are screened through a different mesh filter, the size distribution of the hydrophilic gum required to produce a robust sustained release formulation can be different. Robustness of the sustained release formulations described herein is likely to be a combination of the choice of hydrophilic gum and particle size distribution.
  • the coarser the hydrophilic gum is the larger the fraction of small particles is required for a robust formulation.
  • the finer the hydrophilic gum is the smaller the fraction of small particles is required for a robust formulation.
  • hydrophilic properties of certain hydrophilic gums contribute to the initial hydration of the sustained release formulations and the solid dosage forms, which in one embodiment comprise a drug, one or more heteropolysaccharide gums and one or more homopolysaccharide gums, and in another embodiment comprise a drug, one or more heteropolysaccharide gums and one or more cross-linking compound selected from monovalent cations, multivalent cations, and salts.
  • Integrity of sustained release formulations and solid dosage forms comprising hydrophilic gums has also been found to be sensitive to the method used for granulation of fo ⁇ nulations comprising xanthan gum particles.
  • the granulation method of choice is wet-granulation with non-aqueous solvents such as alcohols, glycerol, propylene glycol, or other non-aqueous solvents, the particle size of xanthan gum will have a substantial effect on hydration and integrity of the granulated sustained release formulation and the solid dosage form.
  • Rapid hydration of xanthan gum in cold water contributes to the integrity of non- water granulated sustained release formulations and finished solid dosage forms described herein.
  • the rate of hydration of xanthan gum was found to depend on the xanthan gum particle size. Xanthan gum particles of small diameter will, for example, hydrate faster than xanthan gum particles of large diameter. Therefore, non-water granulated sustained release fo ⁇ nulations and solid dosage forms comprising xanthan gum particles of smaller average and/or mean diameter will hydrate faster and be more robust than granulated sustained release formulations and solid dosage forms comprising xanthan gum particles of larger average and/or mean diameter.
  • wet-granulation with non-aqueous solvents includes a dispersion of one or more hydrophobic materials (e.g., an alkylcellulose, a copolymer of acrylic and methacrylic acid esters, waxes, shellac, zein, hydrogenated vegetable oils, and mixtures of any of the foregoing) in an amount effective to slow the hydration of the formulation when exposed to an environmental fluid.
  • hydrophobic materials e.g., an alkylcellulose, a copolymer of acrylic and methacrylic acid esters, waxes, shellac, zein, hydrogenated vegetable oils, and mixtures of any of the foregoing
  • the size of xanthan gum particles affects the hydration properties and integrity of the granulated sustained release formulation and the solid dosage form.
  • the hydration will be effected using the water from the aqueous solution, and the particle size of xanthan gum will have a lesser, negligible, or even nonexistent effect on the hydration of the solid dosage formulation.
  • certain homopolysaccharide gums such as locust bean gum, are not expected to contribute to the initial hydration of the sustained release fo ⁇ nulation and solid dosage form. Therefore, the average and/or mean particle size of these homopolysaccharides gums does not affect the hydration properties and integrity of the sustained release formulation and the solid dosage form.
  • Particle size can be measured using any suitable method used in the art.
  • exemplary methods include optical methods, e.g., laser diffraction measurements, light microscopy, surface area measurements (e.g., mercury porosimetry, nitrogen gas adsorption, krypton gas adsorption). Other physical measurements can also be used to calculate particle size.
  • Robustness and integrity of solid dosage forms, such as tablets, capsules, granules and powders can be measured using several techniques, such as dissolution profile measurements. Exemplary dissolution profile measurements include drug release measurements using a USP Type I, Type II, Type III, or Type IV dissolution apparatus.
  • sustained release formulations described herein retain their sustained release dissolution properties in the presence of ethanol.
  • the physicochemical properties of the hydrophilic compound ⁇ e.g., xanthan gum) cross-linked by a cross-linking agent are such that they together fo ⁇ n a gum or gum-like matrix, which is insoluble or substantially insoluble in ethanol.
  • a cross-linking agent e.g., locust bean gum
  • These solubility properties of the formulation may be attributed to the hydrophilic nature of the sustained release delivery system, which in one embodiment comprises one or more hydrophilic gums and one or more homopolysaccharide gums, and in another embodiment comprises or one or more hydrophilic gums, and one or more monovalent cations, multivalent cations, and/or salts.
  • hydrophobic agents e.g., hydrophobic polymers such as ethylcellulose
  • hydrophobic polymers such as ethylcellulose
  • solubility of the drug in ethanol materials comprising the formulation (e.g., hydrophilic compounds are more resistant to ethanol than hydrophobic compounds), and dosage form of the formulation (e.g., tablets are more resistant to ethanol than capsules).
  • sustained release formulations described herein can, therefore, be used to prevent or substantially reduce any undesired effects of ethanol on the release of the drug from a formulation.
  • exemplary undesired effects include dose dumping and altered sustained release dissolution profiles.
  • Alteration of a sustained release profile can be exhibited, for example, in the bioavailability profile of the drug, such as altered blood plasma concentration time curve after administration of the drug with or without a beverage containing ethanol.
  • Typical parameters measured are the high peak drug concentration (C max ), an increase of which can increase the safety risk of a drug, drug concentration at the end of the therapeutic period (C m i n ), a decrease of which can reduce the efficacy of the drug.
  • the sustained release formulations described herein exhibit mean increases in C max of about 1.7 fold when taken with 40% alcohol compared to 0% alcohol. This is considered acceptable because C max ratios in an individual when a drug is administered to a fed (with a standard high-fat meal) vs.
  • a fasted individual can vary from about 0.7 to about 3.5, with a mean C max ratio of about 1.5. Therefore, taking a drug with 40% ethanol has a comparable effect to taldng the drug after a high-fat meal. Taking the drug with 20% or 4% ethanol has a smaller effect on C max than a high- fat meal, as exhibited by the mean C max ratios of about 1.2 and about 1.1, respectively.
  • a formulation with an altered sustained release profile by ethanol may, for example, release a larger amount of the drug shortly after administration (e.g., within 0-6 hours), resulting in a higher-than-intended C max .
  • a higher-than-intended C max can lead to harmful side effects for the patient, including death.
  • less drug is available for subsequent release, resulting in a lower-than-intended C m i n at the end of the therapeutic period (i.e., just prior to administration of a subsequent dose).
  • a lower-than-intended Cmin can result in reduced efficacy or even ineff ⁇ cacy of the drug, which can result in recurrence of a condition in a patient.
  • a higher-than-intended peak drug concentration C max can be, for example, a concentration more than four times higher than intended C max .
  • a lower-than-intended C m jn concentration can be, for example, a concentration less than one third of the intended
  • the sustained release formulations described herein can, therefore, be used to increase safety of drugs with potentially harmful effects at high concentrations and to reduce abuse of drugs producing a euphoric effect, such as opioids.
  • the formulations described herein can also be used to reduce or prevent harm to a patient in situations where a reduced level of a drug (e.g., lower than the therapeutically beneficial level) can adversely affect the health of the patient.
  • the formulations described herein can be useful for formulation of narrow therapeutic range drugs, sometimes referred to as narrow therapeutic index drugs.
  • a formulation described herein is ingested with an alcoholic beverage, or ingested by a patient prior to or after consumption of an alcoholic beverage, the formulation will essentially retain its sustained release properties and will slowly release the drug from the resulting hydrophilic gel matrix. Because the formulations described herein do not dose dump in the presence of ethanol, they can be used for formulation of drugs that are at risk to be taken with ethanol, such as abuse-potential drugs and drugs prescribed to alcohol and/or drug abusers, or drugs that produce harmful or lethal side effects if over-dosed. Examples of such drugs include opioids.
  • patients being treated for conditions such as panic disorder (with or without agoraphobia), bipolar disorder (manic depressive illness), acute manic or mixed episodes associated with bipolar disorder, epilepsy, migraine, attention deficit hyperactivity disorder (ADHD), depression and/or pain may be more likely to consume alcohol compared to the general population. This could be a result of the patients' desire to experience the euphoric effects from inebriation and/or to eliminate or alleviate the symptoms of their condition, such as pain.
  • the patient e.g., a drug addict
  • conventional formulations e.g., opioid formulations
  • oral inhalation/ingestion or oral ingestion with an alcoholic beverage e.g., a drug addict
  • conventional formulations e.g., opioid formulations
  • the sustained release formulations described herein resist extraction of the drug from the formulation by grounding up the solid dosage forms into powder, pouring over 95% ethanol, diluting the resulting solution with water to beverage-strength ethanol, and removing the undissolved material by filtration through a coffee or other paper filter.
  • Ethanol content of hard liquors is typically in the range of 40-45%.
  • sustained release formulations contain relatively high amounts of the drug.
  • Sustained release formulations containing high amounts of drugs can be more harmful to a patient when they fail compared to immediate release fonnulations, which generally contain smaller amounts of the drug. Therefore, the drug formulations described herein can increase safety of drugs that can be harmful and/or lethal at higher than therapeutically beneficial levels.
  • the sustained release delivery system comprises at least one hydrophilic compound.
  • the hydrophilic compound is a gum, for example a heteropolysaccharide gum, forms a gel matrix that releases the drug at a sustained rate upon exposure to liquids.
  • the rate of release of the drug from the gel matrix depends on the drug's partition coefficient between the components of the gel matrix and the aqueous phase within the gastrointestinal tract.
  • the weight ratio of drug to hydrophilic compound is generally in the range of about 1 :0.5 to about 1 :25, or in the range of about 1 :0.5 to about 1:20.
  • the sustained release delivery system generally comprises the hydrophilic compound in an amount of about 20% to about 80% by weight, in an amount of about 20% to about 60% by weight, in an amount of about 40% to about 60% by weight, or in an amount of about 50% by weight.
  • the hydrophilic compound can be any known in the art.
  • Exemplary hydrophilic compounds include gums, cellulose ethers, acrylic resins, polyvinyl pyrrolidone, protein- derived compounds, and mixtures thereof.
  • Exemplary gums include heteropolysaccharide gums and homopolysaccharide gums, such as xanthan, tragacanth, pectins, acacia, karaya, alginates, agar, guar, hydroxypropyl guar, carrageenan, locust bean gums, and gellan gums.
  • Exemplary cellulose ethers include hydroxyalkyl celluloses and carboxyalkyl celluloses, such as hydroxyethyl celluloses, hydroxypropyl celluloses, hydroxypropylmethyl-celluloses, carboxy methylcelluloses, and mixtures thereof.
  • Exemplary acrylic resins include polymers and copolymers of acrylic acid, methacrylic acid, methyl acrylate and methyl methacrylate.
  • the hydrophilic compound is a gum, for example a heteropolysaccharide gum, such as a xanthan gum or derivative thereof.
  • the sustained release delivery system further comprises at least one cross-linking agent.
  • the cross-linking agent can be a compound that is capable of cross-linking the hydrophilic compound to form a gel matrix in the presence of liquids.
  • the sustained release delivery system generally comprises the cross-linking agent in an amount of about 0.5% to about 80% by weight, in an amount of about 2% to about 54% by weight, in an amount of about 20% to about 30% by weight, or in an amount of about
  • Exemplary cross-linking agents include homopolysaccharides.
  • Exemplary homopolysaccharides include galactomannan gums, such as guar gum, hydroxypropyl guar gum, and locust bean gum.
  • the cross-linking agent is a locust bean gum, a guar gum, or a derivative thereof.
  • the cross-linking agent is an alginic acid derivative or a hydrocolloid.
  • the ratio of hydrophilic compound to cross-linking agent is generally from about 1:9 to about 9:1, or from about 1 :3 to about 3:1.
  • the sustained release delivery system comprises one or more cationic cross-linking compounds.
  • the cationic cross-linking compound can be used instead of or in addition to the cross-linking agent.
  • the cationic cross-linking compound can be used in an amount sufficient to cross-link the hydrophilic compound to form a gel matrix in the presence of liquids.
  • the cationic cross-linking compound is present in the sustained release delivery system in an amount of about 0.5% to about 30% by weight, or from about 5% to about 20% by weight.
  • Exemplary cationic cross-linking compounds include monovalent metal cations, multivalent metal cations, and inorganic salts, including alkali metal and/or alkaline earth metal sulfates, chlorides, borates, bromides, citrates, acetates, lactates, and mixtures thereof.
  • the cationic cross-linking compound can be one or more of calcium sulfate, sodium chloride, potassium sulfate, sodium carbonate, lithium chloride, tripotassium phosphate, sodium borate, potassium bromide, potassium fluoride, sodium bicarbonate, calcium chloride, magnesium chloride, sodium citrate, sodium acetate, calcium lactate, magnesium sulfate, sodium fluoride, or mixtures thereof.
  • the ratio of the hydrophilic compound to the cationic cross-linking compound is generally from about 1 :9 to about 9: 1, or from about 1 :3 to about 3:1.
  • Two properties of compounds e.g., the at least one hydrophilic compound and the at least one cross-linking agent; or the at least one hydrophilic compound and the at least one cationic cross-linking compound) that form a gel matrix upon exposure to liquids are fast hydration of the compounds/agents and a gel matrix having a high gel strength. These two properties, which are needed to achieve a slow release gel matrix, are maximized by the particular combination of compounds (e.g., the at least one hydrophilic compound and the at least one cross-linking agent; or the at least one hydrophilic compound and the at least one cationic cross-linking compound).
  • hydrophilic compounds e.g., xanthan gum
  • hydrophilic compounds have excellent water- wicking properties that provide fast hydration
  • materials that are capable of cross-linking the rigid helical ordered structure of the hydrophilic compound e.g., cross-linking agents and/or cationic cross-linking compounds
  • the sustained release delivery system further comprises one or more pharmaceutical diluents known in the art.
  • pharmaceutical diluents include monosaccharides, disaccharides, polyhydric alcohols and mixtures thereof, such as starch, lactose, dextrose, sucrose, microcrystalline cellulose, sorbitol, xylitol, fructose, and mixtures thereof.
  • the pharmaceutical diluent is water-soluble, such as lactose, dextrose, sucrose, or mixtures thereof.
  • the ratio of pharmaceutical diluent to hydrophilic compound is generally from about 1:8 to about 8:1, or from about 1 :3 to about 3:1.
  • the sustained release delivery system generally comprises one or more pharmaceutical diluents in an amount of about 20% to about 80% by weight, for example about 35% by weight. In other embodiments, the sustained release delivery system comprises one or more pharmaceutical diluents in an amount of about 40% to about 80% by weight.
  • the sustained release delivery system further comprises one or more hydrophobic polymers.
  • the hydrophobic polymers can be used in an amount sufficient to slow the hydration of the hydrophilic compound without disrupting it.
  • the hydrophobic polymer may be present in the sustained release delivery system in an amount of about 0.5% to about 20% by weight, in an amount of about 2% to about 10% by weight, in an amount of about 3% to about 7% by weight, or in an amount of about 5% by weight.
  • hydrophobic polymers include alkyl celluloses (e.g., Ci -6 alkyl celluloses, carboxymethylcellulose), other hydrophobic cellulosic materials or compounds (e.g., cellulose acetate phthalate, hydroxypropylmethylcellulose phthalate), polyvinyl acetate polymers (e.g., polyvinyl acetate phthalate), polymers or copolymers derived from acrylic and/or methacrylic acid esters, zein, waxes, shellac, hydrogenated vegetable oils, and mixtures thereof.
  • the hydrophobic polymer can be, for example, methyl cellulose, ethyl cellulose, or propyl cellulose.
  • compositions described herein may be further admixed with one or more wetting agents (such as polyethoxylated castor oil, polyethoxylated hydrogenated castor oil, polyethoxylated fatty acid from castor oil, polyethoxylated fatty acid from hydrogenated castor oil), one or more lubricants (such as magnesium stearate), one or more buffering agents, one or more colorants, and/or other conventional ingredients.
  • wetting agents such as polyethoxylated castor oil, polyethoxylated hydrogenated castor oil, polyethoxylated fatty acid from castor oil, polyethoxylated fatty acid from hydrogenated castor oil
  • lubricants such as magnesium stearate
  • buffering agents such as magnesium stearate
  • the robust sustained release formulations comprising a drug are solid dosage formulations, such as orally administrable solid dosage formulations, for example, tablets, capsules comprising a plurality of granules, sublingual tablets, powders, or granules.
  • the orally administrable solid dosage fonnulations are tablets.
  • the tablets optionally comprise an enteric coating or a hydrophobic coating.
  • the robust sustained release fonnulations described herein comprise an analgesically effective amount of oxymorphone or a pharmaceutically acceptable salt thereof.
  • oxymorphone is frequently hindered by the very low bioavailability of the oral immediate release fonnulations of oxymorphone, which require a 4 hourly dosing frequency.
  • the bioavailability of the robust sustained release formulations described herein is sufficiently high that the robust sustained release fonnulations can be used to treat patients suffering from pain with only once or twice daily dosing.
  • the robust sustained release fonnulations of oxymorphone are administered in an amount sufficient to alleviate pain for an extended period of time, for example, for a period of about 8 hours to about 24 hours, or for a period of about 12 hours to about 24 hours.
  • the oxymorphone sustained release oral solid dosage formulations described herein can be administered four times a day, three times a day, twice daily, or once daily.
  • the robust sustained release formulation upon oral ingestion of the robust sustained release formulation comprising oxymorphone and contact of this formulation with gastrointestinal fluids, the robust sustained release formulation swells and gels to form a hydrophilic gel matrix from which the oxymorphone is released.
  • the swelling of the gel matrix causes a reduction in the bulk density of the formulation and provides the buoyancy necessary to allow the gel matrix to float on the stomach contents to provide a slow delivery of the oxymorphone.
  • the hydrophilic matrix the size of which is dependent upon the size of the original formulation, can swell considerably and become obstructed near the opening of the pylorus.
  • oxymorphone is dispersed throughout the formulation (and consequently throughout the gel matrix), a constant amount of oxymorphone is released per unit time in vivo by dispersion or erosion of the outer portions of the hydrophilic gel matrix. The process continues, with the gel matrix remaining buoyant in the stomach, until substantially all of the oxymorphone is released.
  • the chemistry of certain of the components of the formulation is such that the components are considered to be self-buffering agents which are substantially insensitive to the solubility of the oxymorphone and the pH changes along the length of the gastrointestinal tract.
  • the chemistry of the components is believed to be similar to certain known muco-adhesive substances, such as polycarbophil. Muco- adhesive properties are desirable for buccal delivery systems.
  • the robust sustained release fo ⁇ nulation can loosely interact with the mucin in the gastrointestinal tract and thereby provide another mode by which a constant rate of delivery of the oxymorphone is achieved.
  • the robust sustained release formulations described herein when measured by USP Procedure Di-Ug Release USP 23 (incorporated by reference herein in its entirety), exhibit an in vitro dissolution rate of about 15% to about 50% by weight oxymorphone after 1 hour, about 45% to about 80% by weight oxymorphone after 4 hours, and at least about 80% by weight oxymorphone after 10 hours.
  • the in vitro and in vivo release characteristics of the robust sustained release formulations described herein can be modified using mixtures of one or more different water insoluble and/or water soluble compounds, using different plasticizers, varying the thickness of the sustained release film, including providing release-modifying compounds in the coating, and/or by providing passageways through the coating.
  • Some embodiments provide robust sustained release solid dosage formulations comprising from about 1 mg to about 200 mg of oxymorphone hydrochloride, or from about 5 mg to about 80 mg of oxymorphone hydrochloride; and from about 80 mg to about 200 mg of a sustained release delivery system, or from about 120 mg to about 200 mg of a sustained release delivery system, or about 160 mg of a sustained release delivery system; where the sustained release delivery system comprises about 8.3 to about 41.7% locust bean gum, or about 25% locust bean gum; from about 8.3 to about 41.7% xanthan gum having at least about 30% of particles smaller than about 53 microns in diameter, or about 25% xanthan gum with at least about 30% of particles smaller than about 53 microns in diameter; from about 20 to about 55% dextrose, or about 35% dextrose; from about 5 to about 20% calcium sulfate dihydrate, or about 10% calcium sulfate dihydrate; and from about 2 to 10% ethyl cellulose, or about 5% ethyl
  • sustained release solid dosage formulations comprising from about 1 mg to about 200 mg of oxymorphone hydrochloride, or from about 5 mg to about 80 mg of oxymorphone hydrochloride; and from about 80 mg to about 200 mg of a sustained release delivery system, or from about 120 mg to about 200 mg of a sustained release delivery system, or about 160 mg of a sustained release delivery system; where the sustained release delivery system comprises from about 8.3 to about 41.7% locust bean gum, or about 25% locust bean gum; from about 8.3 to about 41.7% xanthan gum wherein at least about 30% of the xanthan gum particles can pass through a #270 mesh sieve, or about 25% xanthan gum of which at least about 30% of the particles can pass through a #270 mesh sieve; from about 20 to about 55% dextrose, or about 35% dextrose; from about 5 to about 20% calcium sulfate dihydrate, or about 10% calcium sulfate dihydrate; and from about 2 to about 10% ethyl
  • Some embodiments provide robust sustained release solid dosage formulations comprising from about 1 mg to about 200 mg of oxymorphone hydrochloride, or from about 5 mg to about 80 mg of oxymorphone hydrochloride; and from about 200 mg to about 420 mg of a sustained release delivery system, or from about 300 mg to about 420 mg of a sustained release delivery system, or about 360 mg of a sustained release delivery system; where the sustained release delivery system comprises from about 8.3 to about 41.7% locust bean gum, or about 25% locust bean gum; from about 8.3 to about 41.7% xanthan gum having at least about 30% of particles smaller than about 53 microns in diameter, or about 25% xanthan gum with at least about 30% of particles smaller than about 53 microns in diameter; from about 20 to about 55% dextrose, or about 35% dextrose; from about 5 to about 20% calcium sulfate dihydrate, or about 10% calcium sulfate dihydrate; and from about 2 to 10% ethyl cellulose, or about 5% eth
  • sustained release solid dosage formulations comprising from about 1 mg to about 200 mg of oxymorphone hydrochloride, or from about 5 mg to about 80 mg of oxymorphone hydrochloride; and from about 200 mg to about 420 mg of a sustained release delivery system, or from about 300 mg to about 420 mg of a sustained release delivery system, or about 360 mg of a sustained release delivery system; where the sustained release delivery system comprises from about 8.3 to about 41.7% locust bean gum, or about 25% locust bean gum; from about 8.3 to about 41.7% xanthan gum wherein at least about 30% of the xanthan gum particles can pass through a #270 mesh sieve, or about 25% xanthan gum of which at least about 30% of the particles can pass through a #270 mesh sieve; from about 20 to about 55% dextrose, or about 35% dextrose; from about 5 to about 20% calcium sulfate dihydrate, or about 10% calcium sulfate dihydrate; and from about 2 to 10% ethyl
  • the robust sustained release formulations described herein exhibit the following in vivo characteristics: (a) a peak plasma level of oxymorphone occurs within about 2 to about 6 hours after administration; (b) the duration of the oxymorphone analgesic effect is about 8 to about 24 hours; and (c) the relative oxymorphone bioavailability is about 0.5 to about 1.5 compared to an orally administered aqueous solution of oxymorphone.
  • the oxymorphone compositions described herein can be administered as the sole active pharmaceutical compound in the methods described herein, they can also be used in combination with one or more compounds which are known to be therapeutically effective against pain.
  • pharmaceutical kits comprising one or more containers filled with one or more of robust sustained release oxymorphone formulations described herein are provided. The kits can further comprise other pharmaceutical compounds known in the art to be therapeutically effective against pain, and instructions for use.
  • the robust sustained release formulations described herein can be prepared by wet granulation methods.
  • the solid dosage forms described herein can be prepared by direct compression or by wet granulation of the fonnulations.
  • the sustained release formulations are manufactured by a wet granulation technique.
  • the components e.g., hydrophilic compounds such a xanthan gum, cross-linking agents, pharmaceutical diluents, cationic cross-linking compounds, hydrophobic polymers, etc.
  • one or more liquids e.g., water, propylene glycol, glycerol, alcohol
  • the dried mass is then milled with conventional equipment into granules of the sustained release delivery system.
  • the sustained release delivery system is mixed in the desired amounts with the drug and, optionally, one or more wetting agents, one or more lubricants, one or more buffering agents, one or more coloring agents, or other conventional ingredients, to produce a granulated composition.
  • the sustained release delivery system and the drug can be blended with, for example, a high shear mixer.
  • the drug can be finely and homogeneously dispersed in the sustained release delivery system.
  • the granulated composition in an amount sufficient to make a uniform batch of tablets, is subjected to tableting in a conventional production scale tableting machine at normal compression pressures, i.e., about 2,000-16,000 psi. The mixture should not be compressed to a point where there is subsequent difficulty with hydration upon exposure to liquids.
  • the particle size of the hydrophilic compound affects the robustness and integrity of the formulation and solid dosage forms when the sustained release delivery system is wet-granulated with a non-aqueous solution, such as an ethanol/ethylcellose suspension.
  • the fraction of small particles (e.g., smaller than 53 microns in diameter) of the hydrophilic compound (e.g., xanthan gum) affects the robustness and integrity of the sustained release fo ⁇ nulations and solid dosage forms prepared by wet- granulation with a non-aqueous solvent.
  • the xanthan gum used to make the formulation contains less than a certain fraction (e.g., about 30%) of small xanthan gum particles, the sustained release formulation is prone to failure.
  • the fraction of small xanthan gum particles used to make the formulation meets or exceeds certain threshold value, the formulations are robust and not prone to failure. For example, once a threshold fraction of about 30% of xanthan gum particles smaller than 53 microns in diameter is met or exceeded, no change in robustness and integrity of the formulation and solid dosage form is observed (see Table 4).
  • xanthan gum particle sizes and threshold fractions may also be used to manufacture robust sustained release fonnulations described herein.
  • a formulation comprising xanthan gum particles smaller than 45, 38, 32, 25, or 20 microns in diameter may be robust when the threshold fraction is less than about 30%, for example between about 5-25%, or between about 10-20%.
  • a formulation comprising xanthan gum particles smaller than 63, 75, 90, 106, 125, or 150 microns in diameter may be robust when the threshold fraction is more than about 30%, for example between about 30-100%, or between about 50-90%.
  • Robustness and integrity of sustained release formulations and solid dosage fonns granulated with a non-aqueous solution can be improved by controlling the particle size distribution of the hydrophilic compound (e.g., xanthan gum).
  • Control of the particle size distribution of the hydrophilic compound can be achieved, for example, by screening the hydrophilic compound (e.g., xanthan gum) particles through a sieve, (e.g., a #270 mesh sieve) which allows particles smaller than a certain size (e.g., 53 microns in diameter) to pass through. Batches, lots, and combinations thereof having a desired fraction of particles of a desired size can then be used for combination with other components to make a robust sustained release formulation.
  • a sieve e.g., a #270 mesh sieve
  • the hydrophilic compound e.g., xanthan gum
  • the hydrophilic compound having a desired particle size distribution can be received from an external source, for example, a commercial manufacturer or a distributor.
  • the sustained release delivery system is wet-granulated with water or any other aqueous solution, the particle size of the hydrophilic compound (e.g., xanthan gum) does not appear to affect the robustness and integrity of the sustained release formulation and the solid dosage form (see Table 5).
  • the average particle size of the pharmaceutical formulations before tableting is from about 50 microns to about 400 microns, or from about 185 microns to about 265 microns.
  • the average density of the pharmaceutical formulations is from about 0.3 g/ml to about 0.8 g/ml, or from about 0.5 g/ml to about 0.7 g/ml.
  • the tablets formed from the pharmaceutical formulations are generally from about 6 to about 8 kg hardness.
  • the particle size of the hydrophilic compound e.g., xanthan gum
  • the particle size of the hydrophilic compound does not affect the robustness and dissolution properties of the solid dosage form.
  • the sustained release coatings over an inner core comprise at least one drug.
  • the inner core comprising the drug can be coated with a sustained release film, which, upon exposure to liquids, releases the drug from the core at a sustained rate.
  • the sustained release coating comprises at least one water insoluble compound.
  • the water insoluble compound can be a hydrophobic polymer.
  • the hydrophobic polymer can be the same as or different from the hydrophobic polymer used in the sustained release delivery system.
  • Exemplary hydrophobic polymers include alkyl celluloses (e.g., Cj -6 alkyl celluloses, carboxymethylcellulose), other hydrophobic cellulosic materials or compounds (e.g., cellulose acetate phthalate, hydroxypropylmethylcellulose phthalate), polyvinyl acetate polymers (e.g., polyvinyl acetate phthalate), polymers or copolymers derived from acrylic and/or methacrylic acid esters, zein, waxes (alone or in admixture with fatty alcohols), shellac, hydrogenated vegetable oils, and mixtures thereof.
  • the hydrophobic polymer can be, for example, methyl cellulose, ethyl cellulose, or propyl cellulose.
  • the robust sustained release fo ⁇ nulations can be coated with a water insoluble compound to a weight gain from about 1 to about 20% by weight.
  • the sustained release coating can further comprise at least one plasticizer such as tri ethyl citrate, dibutyl phthalate, propylene glycol, polyethylene glycol, or mixtures thereof.
  • plasticizer such as tri ethyl citrate, dibutyl phthalate, propylene glycol, polyethylene glycol, or mixtures thereof.
  • the sustained release coating can also contain at least one water soluble compound, such as polyvinylpyrrolidones, hydroxypropylmethylcelluloses, or mixtures thereof.
  • the sustained release coating can comprise at least one water soluble compound in an amount from about 1% to about 6% by weight, for example, in an amount of about 3% by weight.
  • the sustained release coating can be applied to the drug core by spraying an aqueous dispersion of the water insoluble compound onto the drug core.
  • the drug core can be a granulated composition made, for example, by dry or wet granulation of mixed powders of drug and at least one binding agent; by coating an inert bead with an drug and at least one binding agent; or by spheronizing mixed powders of an drug and at least one spheronizing agent.
  • Exemplary binding agents include hydroxypropylmethylcelluloses.
  • Exemplary spheronizing agents include microcrystalline celluloses.
  • the inner core can be a tablet made by compressing the granules or by compressing a powder comprising a drug.
  • compositions comprising at least one drug and a sustained release delivery system, as described herein are coated with a sustained release coating, as described herein.
  • the compositions comprising at least one drug and a sustained release delivery system, as described herein are coated with a hydrophobic polymer, as described herein.
  • the compositions comprising at least one drug and a sustained release delivery system, as described herein are coated with an enteric coating, such as cellulose acetate phthalate, hydroxypropylmethylcellulose phthalate, polyvinylacetate phthalate, methacrylic acid copolymer, shellac, hydroxypropylmethylcellulose succinate, cellulose acetate trimelliate, or mixtures thereof.
  • compositions comprising at least one drug and a sustained release delivery system, as described herein are coated with a hydrophobic polymer, as described herein, and further coated with an enteric coating, as described herein.
  • the compositions comprising the drug and a sustained release delivery system, as described herein can optionally be coated with a hydrophilic coating which may be applied above or beneath the sustained release film, above or beneath the hydrophobic coating, and/or above or beneath the enteric coating.
  • Exemplary hydrophilic coatings comprise hydroxypropylmethylcellulose.
  • the sustained release formulation upon oral ingestion of the drug sustained release fo ⁇ nulation and contact of the formulation with gastrointestinal fluids, the sustained release formulation swells and gels to form a hydrophilic gel matrix from which the drug is released.
  • the swelling of the gel matrix causes a reduction in the bulk density of the formulation and provides the buoyancy necessary to allow the gel matrix to float on the stomach contents to provide a slow delivery of the drug.
  • the hydrophilic matrix the size of which is dependent upon the size of the original formulation, can swell considerably and become obstructed near the opening of the pylorus.
  • the chemistry of certain of the components of the formulation is such that the components are considered to be self-buffering agents which are substantially insensitive to the solubility of the drugs and the pH changes along the length of the gastrointestinal tract.
  • the chemistry of the components is believed to be similar to certain known muco-adhesive substances, such as polycarbopb.il. Muco-adhesive properties are desirable for buccal delivery systems.
  • the sustained release formulation could potentially loosely interact with the mucin in the gastrointestinal tract and thereby provide another mode by which a constant rate of delivery of the drug is achieved.
  • the robust sustained release formulations and solid dosage forms described herein are useful for formulation of drugs that pose a risk to the patient in case of a formulation failure.
  • the formulations and solid dosage forms comprising the formulations described herein are useful for providing (e.g., prescribing, administering) drugs that pose a risk to the patient in case of a formulation failure.
  • examples of such drugs include, for example, opioids such as oxymorphone.
  • the robust sustained release formulations and solid dosage fo ⁇ ns described herein are useful for treating a condition (e.g., pain), by prescribing and/or administering a therapeutically effective amount of the robust sustained release formulations of the drug (e.g., an opioid such as oxymorphone) to a patient who could consume ethanol while being treated with the drug.
  • a therapeutically effective amount is an amount sufficient to eliminate the condition or to alleviate the condition (i.e., reduce the symptoms compared to the symptoms present prior to administration of the robust sustained release formulation).
  • the formulations and solid dosage forms described herein can be administered as the sole active pharmaceutical composition in the methods described herein, they can also be used in combination with one or more compounds and/or compositions that are known to be therapeutically effective against the condition.
  • kits comprising one or more of the drug formulations described herein are provided.
  • Pharmaceutical kits can, for example, comprise one or more containers filled with one or more of the robust sustained release formulations and/or solid dosage forms described herein.
  • the kits can further comprise other pharmaceutical compounds known in the art to be therapeutically effective against a condition, and instructions for use.
  • albuterol sulfate which has dosage, solubility and other physicochemical properties similar to opioids, such as oxymorphone and oxycodone.
  • xanthan gum (Jungbunzlauer, Perhoven, Austria or CP Kelco, Chicago, IL) were particle-size tested using a series of mesh sieves. These sieves included a #270 mesh sieve, which allowed particles smaller than 53 microns in diameter to pass through (fine particles). The weight fraction of xanthan gum particles passing through the sieves (i.e., fraction of fine xanthan gum) was determined. Batches with known fractions of fine xanthan gum particles were then prepared. TIMERx-N® was prepared by dry blending the requisite amounts of xanthan gum, locust bean gum, calcium sulfate, and dextrose in a high speed mixer/granulator for 3 minutes.
  • a slurry of hydrophobic polymer (ethylcellulose) was prepared by dissolving ethyl cellulose in ethyl alcohol. The slurry was added to the dry blended mixture and the material was subsequently granulated for 4 minutes while running the choppers/impeller. The granulation was then dried in a fluid bed dryer to a LOD (loss on drying) of less than 9% by weight (e.g., typical LOD was ⁇ 3- 5%). The granulation was then milled using a 1.0 mm (0.040") screen.
  • the ingredients of the sustained release excipient are set forth in Table 1 :
  • Xanthan gum batches with known fractions of fine particles were prepared according to Example 1.
  • TIMERx-M50A® was prepared by dry blending the requisite amounts of xanthan gum, locust bean gum, calcium sulfate, and mannitol in a high speed mixer/granulator for 3 minutes. While running choppers/impellers, water was added to the dry blended mixture, and the mixture was granulated for another 3 minutes. The granulation was then dried in a fluid bed dryer to a loss on drying (LOD) of less than about 6% by weight. Typical LOD was between -3-5%. The granulation was then milled using a 0.065" screen.
  • LOD loss on drying
  • a sustained release formulation was prepared by screening albuterol sulfate, ProSolv SMCC® 90 (Silicified Microcrystalline Cellulose, JRS Pharma LP, Patterson, New York) and TIMERx-N® or TIMERx-M50A® separately through a #20 mesh sieve.
  • the blended granulation was compressed to 224.0 mg and ⁇ 11 Kp hardness on a tablet press using 5/16" round standard concave beveled edge tooling.
  • the final tablet composition is listed in the Table 3.
  • Albuterol sulfate tablets with TIMERx-N® and TIMERx-M50A® sustained release delivery systems were prepared as described in Example 3. Dissolution profiles of tablets were evaluated using a USP Apparatus 2 dissolution tester in 900 mL of 50 mM potassium phosphate buffer (pH 4.5). The solution was stirred at 50 r.p.m. A series of samples of about 1.5 mL were withdrawn at predetermined intervals for a period of up to 14 hours. Drug release for all tablets was monitored by RP-HPLC using a Waters
  • Symmetry® Cl 8 column (4.6 x 250 mm) (or equivalent) preceded by a Phenomenex® SecurityGuardTM Cl 8 (4 x 3.0 mm) guard column. Monitoring wavelength was set to 226 nm.
  • the mobile phase consisted of buffer: acetonitrile:methanol in 85:10:5 v/v ratios.
  • the buffer consisted of 1 mL triethylamine and 1 mL trifluoroacetic acid in 1 L of H 2 O.
  • the column temperature was 3O 0 C and the flow rate was set to 1.5 mL/min. To determine the percentage of drug released at each timepoint, the concentration of the sample taken at that timepoint was compared to the concentration of a standard solution.
  • the standard solution was prepared by dissolving 45 mg of albuterol sulfate in 100 mL of 50 mM potassium phosphate buffer (pH 4.5) and then taking 5 mL of this solution and diluting it to 50 mL with more of 50 mM potassium phosphate buffer (pH 4.5).
  • Tablets comprising 13.7% and 27.9% of fine xanthan gum in the ethanol/ethylcelluose-granulated TIMERx-N® released nearly the entire quantity of drug almost immediately. This is an example of undesired dose dumping. Tablets with 31.6% or more of fine xanthan gum dissolved in the expected sustained release manner.
  • Table 4 indicate that there appears to be no substantial difference in dissolution profiles of fo ⁇ nulations containing between about 31.6% and about 88.8% of fine xanthan gum particles.
  • Tablets made by direct compression of water-granulated TIMERx-M50A® formulations comprising xanthan gum are not sensitive to xanthan gum particle size.
  • the data in Table 5 indicate that there appears to be no substantial difference between the dissolution profiles of tablets made with xanthan gum having particle size of less than 180 microns and less than 75 microns when xanthan gum is granulated with water in the process of making the formulation.
  • Table 6 shows dissolution profiles of tablets made by direct compression and granulation of ethanol/ethylcellulose-granulated sustained release formulations with different fractions of #270 (fine) mesh xanthan gum particles.
  • Direct compression of ethanol/ethylcellulose-granulated formulations produced tablets with desired dissolution profiles when the fraction of fine xanthan gum was more than about 30%.
  • Tablets of TIMERx-N® formulations of albuterol sulfate were prepared as described in Example 3. Dissolution profiles of each formulation were measured as described in Example 4. A medium of 40% ethanol and 60% 0.1 M HCl was used as a model of dissolution in the presence of alcohol. 0. IM HCl was chosen to mimic the biological environment of upper GI tract/stomach area, where the sustained release formulation first begins to release the drug.
  • Dissolution experiments were perfo ⁇ ned using a USP II Type dissolution apparatus according to methods described above. Results of dissolution experiments with tablets made with alcohol/ethylcellulose-granulated TIMERx-N® comprising xanthan gum with different particle size distributions are shown in Table 7.
  • Tablets comprising 28% of fine xanthan gum in the ethanol/ethylcelluose- granulated TIMERx-N® released nearly the entire quantity of drug almost immediately. This is an example of undesired dose dumping. Tablets with 35% or more of fine xanthan gum dissolve in the expected sustained release manner.
  • Table 7 indicate that there appears to be no substantial difference in dissolution profiles of formulations containing between about 35% and about 86% of fine xanthan gum particles, although the formulation containing about 86% of fine xanthan gum particles dissolved slightly slower in 40% ethanol solution than in a standard buffer. Therefore, formulations comprising about 30% or more of fine xanthan gum, exhibit robust dissolution properties, and dissolve in a sustained release manner in the presence and absence of beverage-strength ethanol.
  • a controlled release delivery system was prepared by dry blending xanthan gum, locust bean gum, calcium sulfate dihydrate, and dextrose in a high speed mixed/granulator for a few minutes.
  • a slurry was prepared by mixing ethyl cellulose with alcohol. While running choppers/impellers, the slurry was added to the dry blended mixture, and granulated for a few minutes. The granulation was then dried to a LOD
  • Tablets comprising 40 mg of oxymorphone hydrochloride were prepared using the controlled release delivery system shown in Table 8 A. The quantities of ingredients per tablet are listed in Table 8B.
  • Tablets of TIMERx-N® sustained release formulations with 40 mg of oxymorphone were tested for abuse potential in an intravenous route of administration.
  • a person, such as a drug addict, trying to abuse the formulation, may attempt to extract the opioid from the tablets and inject themselves with the resulting solution.
  • Tablets of TIMERx-N® sustained release formulations with 40 mg of oxymorphone were prepared according to procedures in Example 6 and ground into powder.
  • the resulting powder was dispersed into 30 mL of water and stirred for 5 seconds.
  • the resulting powder was dispersed into 15 mL of 95% ethanol, stirred for 5 seconds, and then diluted with an additional 15 mL of water.
  • the resulting powder was dispersed into 30 mL of 95% ethanol and stirred for 5 seconds.
  • the resulting solution was allowed to set for 15 minutes before being filtered through a paper filter.
  • Oxymorphone recovery from the filtered solutions was measured using HPLC at 4O 0 C, using a Zorbax® XDB-C 18 column and a UV detector set at 230 nm. Recovery of oxymorphone from each test is shown in Table 9.
  • sustained release tablets comprising 40 mg of oxymorphone, formulated with TIMERx-N® made with xanthan gum in which at least 30% of particles can pass through a #270 mesh sieve, were powdered and extracted with water, approximately 3- 4% of oxymorphone was released into water after 15 minutes.
  • powdered tablets were first suspended in 95% ethanol for 5 seconds, followed by dilution with water to provide a 47.5% ethanol solution. In this experiment, approximately 11- 15% of oxymorphone was released into the water/ethanol solution after 15 minutes.
  • Healthy volunteers were used in a study to assess the pharmacokinetics of oxymorphone 40 mg sustained release tablets when co-administered with 240 mL of 40%, 20%, 4%, and 0% (water) ethanol.
  • the study design was a randomized, open-label, single-dose, four-period crossover in 28 subjects.
  • naltrexone HCl 50 mg was administered approximately 12 and 2 hours prior to each oxymorphone administration, and again at 12 hours after administration.
  • Subjects were fasted overnight for at least 8 hours prior to dosing. Water was allowed ad lib except from 1 hour before dosing until 1 hour after dosing.
  • a standardized meal was served 4 hours and 10 hours after dosing.
  • Oxymorphone 40 mg sustained release tablets were administered on four separate occasions with 240 mL of: A) 40% ethanol, B) 20% ethanol, C) 4% ethanol, or D) 0% ethanol.
  • Serial blood samples were obtained from 0 to 48 hours after dosing. Plasma samples were assayed for oxymorphone.
  • Pharmacokinetic parameters for oxymorphone were dete ⁇ nined using non-compartmental methods for data evaluation. Point estimates and 90% confidence intervals (CIs) for natural logarithmic transfo ⁇ ned C max , AUCo-t, and AUCo-inf were calculated using Least Squares Means (LSMeans). Any treatment in which a subject vomited during the dosing interval (0-12 hours) was excluded from the primary pharmacokinetic analysis.
  • LSMeans Least Squares Means
  • GMR Geometric mean ratios
  • the mean plasma concentration-time data in Table 11 show that the 40% and 20% ethanol treatments produce higher plasma concentrations during the first 4 to 6 hours compared to the 0% ethanol treatment.
  • the 4% ethanol treatment mean plasma concentrations were similar to those for the 0% ethanol treatment. All data were comparable from 16 to 48 hours after dosing. Secondary peaks were observed at 5 hours for the 4% and 0% ethanol treatments and 12 hours for all four treatments.
  • the 40% ethanol treatment mean plasma concentration was higher than 0%, 4%, or 20% from 0.5 to 6 hours, the concentration then declined and was lower than the other three treatments at 8 to 12 hours.
  • C max was the only pharmacokinetic parameter that appeared to be directly related to the ethanol treatment (Table 12).
  • GMR data shown in Table 16 indicate that increases in C max were 62%, 15%, and 8% for the 40% ethanol, 20% ethanol and 4% ethanol treatments, respectively, as compared to the 0% ethanol treatment.
  • Changes in AUC 0 - t and AUCo -inf ranged from - 10% to 7% for the ethanol treatments as compared to 0% ethanol (Table 16).
  • the 40% and 20% C max , AUC 0-t and AUC 0-inf increases were lower when subjects who vomited were included.
  • naltrexone HCl 50 mg was administered approximately 12 hours prior to each oxymorphone administration. Subjects were fasted overnight for at least 8 hours prior to dosing. For the fed treatment subjects were served a high-fat breakfast and were dosed 10 minutes after completion of the breakfast.
  • Each dose was administered with 240 mL of water. Subjects were not permitted any other food until 4 hours after dosing. Serial blood samples were obtained from 0 to 72 hours after dosing. Plasma samples were assayed for oxymorphone. Pharmacokinetic parameters for oxymorphone were determined using non-compartmental methods. Point estimates and 90% CIs for natural logarithmic transformed C max , AUC 0-t , and AUC 0 .j n f were calculated using LSMeans. Twenty-five subjects completed the study. The mean plasma concentration-time data for the fasted and fed treatments for the sustained release tablet are shown in Table 17.
  • the fed treatment produced higher plasma oxymorphone concentrations during the first 8 hours compared to the fasted treatment.
  • the mean plasma concentrations for both treatments were similar from 10 to 48 hours after dosing. Secondary peaks were observed at 5 hours for the fasted treatment and at 12 hours both treatments.
  • the mean plasma oxymorphone concentration-time data or the fasted and fed treatments for the immediate release tablets are shown in Table 18.
  • the fed treatment produced higher plasma concentrations during the first 10 hours compared to the fasted treatment.
  • the mean plasma concentrations for both treatments were similar from 12 to 48 hours after dosing. Secondary peaks were seen at 12 hours for the fasted and fed treatments.
  • the fed treatment with 4 x 10 mg immediate release oxymorphone tablets produced higher plasma oxymorphone concentrations during the first 10 hours compared to the fasted treatment.
  • the mean plasma oxymorphone concentrations for both treatments were similar from 12 to 48 hours after dosing. Secondary peaks were observed at 12 hours for the fasted treatment and fed treatments.
  • C max was increased in the presence of food for both the sustained release and the immediate release tablets and AUC was increased by food for the immediate release tablets (Table 19). From the GMR data (Table 20) it can be seen that food increased C max by 51% and 38% for the sustained release and immediate release tablets, respectively, when compared to administration under fasted conditions.
  • Example 8 The in vitro study (Example 8) showed that 40% ethanol did not increase the dissolution rate of the oxymorphone sustained release 40 mg tablet. These data indicate that the formulation drug release matrix is not compromised by beverage-strength ethanol concentrations and the premature release of oxymorphone in vivo when exposed to ethanol at concentrations up to 40% does not occur. However, the data from the human ethanol study demonstrated that co-administration of 240 mL of 40% ethanol, and to a lesser extent 20% ethanol, increased the C max of oxymorphone from the 40 mg sustained release tablet while having no demonstrable effect on the AUC (Tables 12 and 13).
  • the increases in C max observed are not believed to be caused by early release of oxymorphone owing to disintegration of the sustained release delivery system (i.e., dose dumping), but instead by an apparent increased rate of absorption, which is independent of the formulation.
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IL198169A0 (en) 2009-12-24
MX2009003772A (es) 2009-07-22
KR20090076946A (ko) 2009-07-13
BRPI0621952A2 (pt) 2011-10-18
WO2008045046A1 (en) 2008-04-17
CN101578095A (zh) 2009-11-11
AU2006349471A1 (en) 2008-04-17
JP2010505947A (ja) 2010-02-25
CA2652980A1 (en) 2008-04-17

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