Claims for Patent: 11,077,073
✉ Email this page to a colleague
Summary for Patent: 11,077,073
| Title: | Methods of using amantadine compositions |
| Abstract: | Provided herein are oral pharmaceutical compositions comprising amantadine, or a pharmaceutically acceptable salt thereof, and a pharmaceutically acceptable excipient, and which have a low level of organic solvent. Provided are also methods of orally administrating a composition comprising amantadine, or a pharmaceutically acceptable salt thereof, to a subject, which has reduced gastrointestinal side effects or sleep disturbances. Further provided are extended release oral compositions comprising amantadine, or a pharmaceutically acceptable salt thereof, that are suitable for once daily administration. |
| Inventor(s): | Went; Gregory T. (San Francisco, CA), Fultz; Timothy J. (Big Canoe, GA), Ghosh; Sangita (Foster City, CA), McClure; Natalie (Portola Valley, CA) |
| Assignee: | Adamas Pharma, LLC (Emeryville, CA) |
| Application Number: | 16/409,554 |
| Patent Claims: |
1. A method of reducing levodopa-induced dyskinesia (LID) in a subject with Parkinson's disease in need thereof, comprising orally administering once daily to the subject an
oral pharmaceutical composition comprising: a drug, wherein the drug is amantadine or a pharmaceutically acceptable salt thereof, and wherein said oral pharmaceutical composition comprises from 50 mg to 500 mg of the amantadine or an equivalent amount of
the pharmaceutically acceptable salt thereof, and at least one excipient that modifies the release of at least a portion of said drug; wherein said oral pharmaceutical composition has a dissolution profile of said drug which shows: (i) 0% to 10% in 2
hours, (ii) 3% to 14% in 4 hours, (iii) 23% to 40% in 6 hours, and (iv) not less than 80% in 12 hours; wherein the dissolution profile is determined with a USP Type 2 apparatus (paddles) at 50 rpm at 37.0.+-.0.5.degree. C. with 500 ml water as the
dissolution medium; and wherein said oral pharmaceutical composition provides (i) a Tmax for amantadine of 11 to 19 hours, and (ii) an AUC.sub.0-inf for amantadine of 44 to 72 ng*hr/ml per mg of said drug and (iii) a pAUC.sub.0-8 for amantadine of 1.0
to 2.0 ng*hr/ml per mg of said drug, when said oral pharmaceutical composition is dosed in healthy subjects of a single dose, human pharmacokinetic study, wherein the subjects are dosed in the morning after an overnight fast; wherein said oral
pharmaceutical composition comprises less than 2000 ppm of organic solvent; and wherein LID is reduced in the subject.
2. A method of increasing ON time without troublesome dyskinesia in a subject with Parkinson's disease in need thereof, wherein the subject has levodopa-induced dyskinesia (LID), the method comprising orally administering once daily to the subject an oral pharmaceutical composition comprising: a drug, wherein the drug is amantadine or a pharmaceutically acceptable salt thereof, and wherein said oral pharmaceutical composition comprises from 50 mg to 500 mg of the amantadine or an equivalent amount of the pharmaceutically acceptable salt thereof; and at least one excipient that modifies the release of at least a portion of said drug; wherein said oral pharmaceutical composition has a dissolution profile of said drug which shows: (i) not more than 9% dissolution at 2 hours, (ii) 3% to 14% dissolution at 4 hours, (iii) 20% to 43% dissolution at 6 hours, and (iv) at least 82% dissolution at 12 hours; wherein the dissolution profile is determined with a USP Type 2 apparatus (paddles) at 50 rpm at 37.0.+-.0.5.degree. C. with 500 ml water as the dissolution medium; wherein said oral pharmaceutical composition provides (i) a Tmax for amantadine of 11 to 19 hours, and (ii) an AUC.sub.0-inf for amantadine of 44 to 72 ng*hr/ml per mg of said drug and (iii) a pAUC.sub.0-8 for amantadine of 1.0 to 2.0 ng*hr/ml per mg of said drug, when said oral pharmaceutical composition is dosed in healthy subjects of a single dose, human pharmacokinetic study, wherein the subjects are dosed in the morning after an overnight fast; and wherein said oral pharmaceutical composition comprises less than 2000 ppm of organic solvent. 3. A method of reducing OFF time in a subject with Parkinson's disease in need thereof, wherein the subject has levodopa-induced dyskinesia (LID), the method comprising orally administering once daily to the subject an oral pharmaceutical composition comprising: a drug, wherein the drug is amantadine or a pharmaceutically acceptable salt thereof, and wherein said oral pharmaceutical composition comprises from 50 mg to 500 mg of the amantadine or an equivalent amount of the pharmaceutically acceptable salt thereof; and at least one excipient that modifies the release of at least a portion of said drug; wherein said oral pharmaceutical composition has a dissolution profile of said drug which shows: (i) not more than 9% dissolution at 2 hours, (ii) 3% to 14% dissolution at 4 hours, (iii) 20% to 43% dissolution at 6 hours, and (iv) at least 82% dissolution at 12 hours; wherein the dissolution profile is determined with a USP Type 2 apparatus (paddles) at 50 rpm at 37.0.+-.0.5.degree. C. with 500 ml water as the dissolution medium; and wherein said oral pharmaceutical composition provides (i) a Tmax for amantadine of 11 to 19 hours, and (ii) an AUC.sub.0-inf for amantadine of 44 to 72 ng*hr/ml per mg of said drug and (iii) a pAUC.sub.0-8 for amantadine of 1.0 to 2.0 ng*hr/ml per mg of said drug, when said oral pharmaceutical composition is dosed in healthy subjects of a single dose, human pharmacokinetic study, wherein the subjects are dosed in the morning after an overnight fast; wherein said oral pharmaceutical composition comprises less than 2000 ppm of organic solvent; and wherein OFF time is reduced in the subject. 4. A method of reducing levodopa-induced dyskinesia (LID) in a subject with Parkinson's disease in need thereof, comprising orally administering once daily to the subject an oral pharmaceutical composition comprising: a drug, wherein the drug is amantadine or a pharmaceutically acceptable salt thereof, and wherein said oral pharmaceutical composition comprises from 50 mg to 500 mg of the amantadine or an equivalent amount of the pharmaceutically acceptable salt thereof; and at least one excipient that modifies the release of at least a portion of said drug; wherein said oral pharmaceutical composition has a dissolution profile of said drug which shows: (i) not more than 10% dissolution at 2 hours; (ii) 5% to 13% dissolution at 4 hours; (iii) 20% to 43% dissolution at 6 hours; and (iv) at least 80% dissolution at 12 hours; wherein the dissolution profile is determined with a USP Type 2 apparatus (paddles) at 50 rpm at 37.0.+-.0.5.degree. C. with 500 ml water as the dissolution medium; and wherein said oral pharmaceutical composition provides (i) a Tmax for amantadine of 11 to 19 hours, and (ii) an AUC.sub.0-inf for amantadine of 44 to 72 ng*hr/ml per mg of said drug and (iii) a pAUC.sub.0-8 for amantadine of 1.0 to 2.0 ng*hr/ml per mg of said drug, when said oral pharmaceutical composition is dosed in healthy subjects of a single dose, human pharmacokinetic study, wherein the subjects are dosed in the morning after an overnight fast; wherein said oral pharmaceutical composition comprises less than 2000 ppm of organic solvent; and wherein LID is reduced in the subject. 5. A method of reducing levodopa-induced dyskinesia (LID) in a subject with Parkinson's disease in need thereof, comprising orally administering once daily to the subject an oral pharmaceutical composition comprising: a drug, wherein the drug is amantadine or a pharmaceutically acceptable salt thereof, and wherein said oral pharmaceutical composition comprises from 50 mg to 500 mg of the amantadine or an equivalent amount of the pharmaceutically acceptable salt thereof; and at least one excipient that modifies the release of at least a portion of said drug; wherein said oral pharmaceutical composition has a dissolution profile of said drug which shows: (i) not more than 9% dissolution at 2 hours, (ii) 3% to 14% dissolution at 4 hours, (iii) 20% to 43% dissolution at 6 hours, and (iv) at least 82% dissolution at 12 hours; wherein the dissolution profile is determined with a USP Type 2 apparatus (paddles) at 50 rpm at 37.0.+-.0.5.degree. C. with 500 ml water as the dissolution medium; and wherein said oral pharmaceutical composition provides (i) a Tmax for amantadine of 11 to 19 hours, and (ii) an AUC.sub.0-inf for amantadine of 44 to 72 ng*hr/ml per mg of said drug and (iii) a pAUC.sub.0-8 for amantadine of 1.0 to 2.0 ng*hr/ml per mg of said drug, when said oral pharmaceutical composition is dosed in healthy subjects of a single dose, human pharmacokinetic study, wherein the subjects are dosed in the morning after an overnight fast; wherein said oral pharmaceutical composition comprises less than 2000 ppm of organic solvent; and wherein LID is reduced in the subject. 6. The method of claim 1, wherein the oral pharmaceutical composition comprises from 100 mg to 450 mg of amantadine, or an equivalent amount of a pharmaceutically acceptable salt thereof. 7. The method of claim 1, wherein the oral pharmaceutical composition comprises one, two, three, or four unit dosage forms. 8. The method of claim 1, wherein the oral pharmaceutical composition comprises one or two unit dosage forms. 9. The method of claim 1, wherein the drug is a pharmaceutically acceptable salt of amantadine. 10. The method of claim 1, wherein the drug is amantadine hydrochloride. 11. The method of claim 1, wherein the oral pharmaceutical composition comprises: a plurality of coated pellets, wherein each coated pellet comprises amantadine or a pharmaceutically acceptable salt thereof; and a capsule shell. |
Make Better Decisions: Try a trial or see plans & pricing
Drugs may be covered by multiple patents or regulatory protections. All trademarks and applicant names are the property of their respective owners or licensors. Although great care is taken in the proper and correct provision of this service, thinkBiotech LLC does not accept any responsibility for possible consequences of errors or omissions in the provided data. The data presented herein is for information purposes only. There is no warranty that the data contained herein is error free. thinkBiotech performs no independent verification of facts as provided by public sources nor are attempts made to provide legal or investing advice. Any reliance on data provided herein is done solely at the discretion of the user. Users of this service are advised to seek professional advice and independent confirmation before considering acting on any of the provided information. thinkBiotech LLC reserves the right to amend, extend or withdraw any part or all of the offered service without notice.
© Copyright 2002-2024 thinkBiotech LLC
ISSN: 2162-2639
Privacy and Cookies
Terms & Conditions
Site Map
DrugPatentWatch Alternatives
LOE / Major Patent Expirations 2024 - 2025
NCE-1 Patent Challenge Dates 2024 - 2025
Trigger-based marketing for the life sciences
Get DrugPatentWatch Business Intelligence Reports at Amazon.com
DrugChatter - AI-based answers to questions about drugs
RxJam - HIPAA-ready chat for life sciences
ISSN: 2162-2639
Privacy and Cookies
Terms & Conditions
Site Map
DrugPatentWatch Alternatives
LOE / Major Patent Expirations 2024 - 2025
NCE-1 Patent Challenge Dates 2024 - 2025
Trigger-based marketing for the life sciences
Get DrugPatentWatch Business Intelligence Reports at Amazon.com
DrugChatter - AI-based answers to questions about drugs
RxJam - HIPAA-ready chat for life sciences
Preferred Citation:
Friedman, Yali. "DrugPatentWatch" DrugPatentWatch, thinkBiotech, 2024, www.DrugPatentWatch.com.
See Primary Research Papers Citing DrugPatentWatch
Links
Follow DrugPatentWatch:
