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Glatiramer acetate

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Glatiramer acetate
Clinical data
Trade namesCopaxone,[1]Glatopa,[2]Brabio
AHFS/Drugs.comMonograph
MedlinePlusa603016
License data
Pregnancy
category
  • AU:B1
Routes of
administration		Subcutaneous injection
ATC code
Legal status
Legal status
Identifiers
CAS Number
PubChemCID
DrugBank
ChemSpider
  • none
UNII
ChEMBL
CompTox Dashboard(EPA)
ECHA InfoCard100.248.824Edit this at Wikidata
Chemical and physical data
FormulaC25H45N5O13
Molar mass623.657g·mol−1
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Glatiramer acetate(also known asCopolymer 1,Cop-1), sold under the brand nameCopaxoneamong others, is animmunomodulatormedication used to treatmultiple sclerosis.[1][2]Glatiramer acetate is approved in the United States to reduce the frequency of relapses, but not for reducing the progression of disability.Observational studies,but not randomized controlled trials, suggest that it may reduce progression of disability. While a conclusivediagnosis of multiple sclerosisrequires a history of two or more episodes of symptoms and signs, glatiramer acetate is approved to treat a first episode anticipating a diagnosis. It is also used to treat relapsing-remitting multiple sclerosis. It is administered bysubcutaneous injection.[1][2]

It is a mixture of random-sized peptides that are composed of the fouramino acidsfound inmyelin basic protein,namelyglutamic acid,lysine,alanine,andtyrosine.Myelin basic protein is theantigenin themyelin sheathsof the neurons that stimulates anautoimmunereaction in people with MS, so the peptide may work as a decoy for the attacking immune cells.

It is on theWorld Health Organization's List of Essential Medicines.[6]

History[edit]

Glatiramer acetate was originally discovered at theWeizmann Institute of Science.Three main clinical trials followed to demonstrate safety and efficacy: The first trial was performed in a single center, double-blind,placebo controlled trialand included 50 patients.[7] The second trial was a two-year, multi-center, randomized, double-blind, placebo controlled trial and involved 251 patients.[8]The third trial was a double-blindMRIstudy involving participation of 239 patients.[9]

Medical uses[edit]

Glatiramer acetate isindicatedfor the treatment of relapsing forms of multiple sclerosis (MS), to include clinically isolated syndrome, relapsing-remitting disease, and active secondary progressive disease, in adults.[1]

A 2010Cochranereview concluded that glatiramer acetate had partial efficacy in "relapse-related clinical outcomes" but no effect on progression of the disease.[10]As a result, it is approved by the FDA for reducing the frequency of relapses, but not for reducing the progression of disability.[1][2]

A 15-year followup of the original trial compared patients who continued with glatiramer to patients who dropped out of the trial. Patients with glatiramer had reduced relapse rates, and decreased disability progression and transition to secondary progressive MS, compared to patients who did not continue glatiramer. However, the two groups were not necessarily comparable, as it was no longer a randomized trial. There were no long-term safety issues.[11]

Adverse effects[edit]

An injection site reaction on the upper left arm

Side effects may include a lump at the injection site (injection site reaction) in approximately 30% of users, and aches, fever, chills (flu-like symptoms) in approximately 10% of users.[12]Side effect symptoms are generally mild in nature. A reaction that involves flushing, shortness of breath, anxiety and rapid heartbeat has been reported soon after injection in up to 5% of patients (usually after inadvertently injecting directly into a vein). These side effects subside within thirty minutes. Over time, a visible dent at a repeat-injection site can occur due to the local destruction of fat tissue, known aslipoatrophy,that may develop.

More serious side effects have been reported for glatiramer acetate, according to the FDA's prescribing label, these include serious side effects to the cardiovascular, digestive (including the liver), hematopoietic, lymphatic, musculoskeletal, nervous, respiratory, and urogenital systems as well as special senses (in particular the eyes). Metabolic and nutritional disorders have also been reported; however a link between glatiramer acetate and these adverse effects has not been established.[1][2]

It may also causeJessner lymphocytic infiltrate.[13]

Mechanism of action[edit]

Glatiramer acetate is a random polymer (average molecular mass 6.4kD) composed of fouramino acidsfound inmyelin basic protein.The mechanism of action for glatiramer acetate is not fully elucidated. It is thought to act by modifying immune processes that are believed to be responsible for the pathogenesis of MS. Administration of glatiramer acetate shifts the population of T cells from proinflammatoryTh1 T-cellsto regulatoryTh2 T-cellsthat suppress the inflammatory response.[14]This is done by the inhibition of secretion of proinflammatory cytokines (IL-1, IL-12, TNF, INFγ) by Th1 T-cells, thereby inducing Th2 T-cells to cross the blood–brain barrier and produce anti-inflammatory cytokines (IL-4, IL-5, IL-13, IL-10, TGF-β).[15]Given its resemblance to myelin basic protein, glatiramer acetate may act as a decoy, diverting an autoimmune response against myelin. This hypothesis is supported by findings of studies that have been carried out to explore the pathogenesis ofexperimental autoimmune encephalomyelitis(EAE), a condition induced in several animal species through immunization against central nervous system derived material containing myelin and often used as an experimental animal model of MS. Studies in animals and in vitro systems suggest that upon its administration, glatiramer acetate-specificregulatory T cells(Tregs) are induced and activated in the periphery, inhibiting the inflammatory reaction to myelin basic protein.[1][2]

The integrity of theblood–brain barrier,however, is not appreciably affected by glatiramer acetate, at least not in the early stages of treatment. Glatiramer acetate has been shown in clinical trials to reduce the number and severity of multiple sclerosis exacerbations.[16]

Society and culture[edit]

Marketing[edit]

Glatiramer acetate has been approved for marketing in numerous countries worldwide, including theUnited States,Israel,Canadaand 24European Unioncountries.[17][18]Approval in the U.S. was obtained in 1997.[19]Glatiramer acetate was approved for marketing in theU.K.in August 2000, and launched in December.[20]This first approval in a major European market led to approval across theEuropean Unionunder themutual recognition procedure. Iran is proceeding with domestic manufacture of glatiramer acetate.[21][22]

Patent status[edit]

Novartissubsidiary Sandoz has marketed Glatopa since 2015, a generic version of the original Teva 20 mg formulation that requires daily injection.[23]

Teva developed a long-acting 40 mg formulation, marketed since 2015, which reduced required injections to three per week.[24]In October 2017, the FDA approved a generic version, which is manufactured in India byNatco Pharma,and imported and sold by Dutch firmMylan.[25][26]In February 2018, Sandoz received FDA approval for their generic version.[27]In parallel with the development and approval processes, the generic competitors have disputed Teva's newer patents, any of which if upheld, would prevent marketing of long-acting generics.[28]

While thepatenton the chemical drug expired in 2015,[29]Teva obtained new US patents covering pharmaceutical formulations for long-acting delivery.[30]Litigation from industry competitors in 2016-2017 resulted in the new patents being judged invalid.[31][32]In October 2018, theU.S. Court of Appealsfor theFederal Circuitupheld the patent invalidation forobviousness.[33][34]The case reflects the larger controversy overevergreeningof generic drugs.

References[edit]

  1. ^abcdefgh"Copaxone- glatiramer acetate injection, solution".DailyMed.23 July 2020.Retrieved11 November2020.
  2. ^abcdefg"Glatopa- glatiramer acetate injection, solution".DailyMed.31 July 2020.Retrieved11 November2020.
  3. ^"Neurological therapies".Health Canada.9 May 2018.Retrieved13 April2024.
  4. ^"Brabio 20 mg/mL Solution for Injection, Pre-filled Syringe - Summary of Product Characteristics (SmPC)".(emc).Retrieved11 November2020.
  5. ^"Copaxone 20 mg/ml solution for injection in pre-filled syringe - Summary of Product Characteristics (SmPC)".(emc).29 September 2020.Retrieved11 November2020.
  6. ^World Health Organization(2023).The selection and use of essential medicines 2023: web annex A: World Health Organization model list of essential medicines: 23rd list (2023).Geneva: World Health Organization.hdl:10665/371090.WHO/MHP/HPS/EML/2023.02.
  7. ^Bornstein MB, Miller A, Slagle S, Weitzman M, Crystal H, Drexler E, Keilson M, Merriam A, Wassertheil-Smoller S, Spada V (August 1987). "A pilot trial of Cop 1 in exacerbating-remitting multiple sclerosis".The New England Journal of Medicine.317(7): 408–14.doi:10.1056/NEJM198708133170703.PMID3302705.
  8. ^Johnson KP, Brooks BR, Cohen JA, Ford CC, Goldstein J, Lisak RP, Myers LW, Panitch HS, Rose JW, Schiffer RB (July 1995). "Copolymer 1 reduces relapse rate and improves disability in relapsing-remitting multiple sclerosis: results of a phase III multicenter, double-blind placebo-controlled trial. The Copolymer 1 Multiple Sclerosis Study Group".Neurology.45(7): 1268–76.doi:10.1212/WNL.45.7.1268.PMID7617181.S2CID28895177.
  9. ^Comi G, Filippi M, Wolinsky JS (March 2001). "European/Canadian multicenter, double-blind, randomized, placebo-controlled study of the effects of glatiramer acetate on magnetic resonance imaging--measured disease activity and burden in patients with relapsing multiple sclerosis. European/Canadian Glatiramer Acetate Study Group".Annals of Neurology.49(3): 290–7.doi:10.1002/ana.64.PMID11261502.S2CID35614752.
  10. ^La Mantia L, Munari LM, Lovati R (May 2010). "Glatiramer acetate for multiple sclerosis".The Cochrane Database of Systematic Reviews.5(5): CD004678.doi:10.1002/14651858.CD004678.pub2.PMID20464733.
  11. ^Ford C, Goodman AD, Johnson K, Kachuck N, Lindsey JW, Lisak R, et al. (March 2010)."Continuous long-term immunomodulatory therapy in relapsing multiple sclerosis: results from the 15-year analysis of the US prospective open-label study of glatiramer acetate".Multiple Sclerosis.16(3): 342–50.doi:10.1177/1352458509358088.PMC2850588.PMID20106943.
  12. ^"Copaxone".MediGuard.
  13. ^Krafchik BR (2011)."Reaction Patterns".In Schachner LA, Hansen RC (eds.).Pediatric Dermatology.Elsevier Health Sciences. p. 1022.ISBN978-0-7234-3665-2.
  14. ^Arnon R, Sela M (1999)."The chemistry of the Copaxone drug"(PDF).Chem. Israel.1:12–17. Archived fromthe original(PDF)on 2003-09-07.
  15. ^https://go.drugbank.com/drugs/DB05259;Glatiramer Mechanism of Action
  16. ^"Copaxone".All About Multiple Sclerosis.
  17. ^McKeage K (May 2015). "Glatiramer Acetate 40 mg/mL in Relapsing-Remitting Multiple Sclerosis: A Review".CNS Drugs.29(5): 425–32.doi:10.1007/s40263-015-0245-z.PMID25906331.S2CID30186027.
  18. ^Comi G, Amato MP, Bertolotto A, Centonze D, De Stefano N, Farina C, et al. (2016)."The heritage of glatiramer acetate and its use in multiple sclerosis".Multiple Sclerosis and Demyelinating Disorders.1(1).doi:10.1186/s40893-016-0010-2.
  19. ^"Copaxone".CenterWatch.
  20. ^"Teva's Copaxone approved in UK".The Pharma Letter.
  21. ^"Glatiramer Acetate".Tofigh Daru Research and Engineering Company. Archived fromthe originalon 2018-10-21.Retrieved2017-02-01.
  22. ^Isayev S, Jafarov T (1 May 2012)."Iran to manufacture multiple sclerosis cure".Trend News Agency.
  23. ^"Sandoz announces US launch of Glatopa".Novartis. 2015. Archived fromthe originalon 2018-02-03.Retrieved2017-02-21.
  24. ^Silva P (9 October 2015)."New 3-Times-Per-Week Regimen For Teva's Copaxone".Multiple Sclerosis News Today.
  25. ^Erman M, Grover D (3 October 2017)."Mylan surges, Teva slumps after FDA okays Copaxone copy".Reuters.Retrieved4 October2017.
  26. ^"NATCO's marketing partner Mylan receives final approval of generic glatiramer acetate, for both 20 mg/mL and 40 mg/mL versions".NATCO Pharma (India).3 October 2017. Archived fromthe originalon 10 January 2019.Retrieved4 October2017.>
  27. ^"Sandoz announces US FDA approval and launch of Glatopa 40 mg/mL".Novartis International AG.February 13, 2018.RetrievedMay 10,2018.
  28. ^"Teva's Copaxone still growing despite patent risks".BioPharmaDive.
  29. ^Helfand C."Copaxone".FiercePharma.
  30. ^Decker S (1 September 2016)."Teva loses decision on validity of 302 copaxone patent".Bloomberg Markets.
  31. ^Decker S, Flanagan C, Benmeleh Y (30 January 2017)."Teva loses ruling invalidating patents on copaxone drug".Bloomberg Markets.
  32. ^"Teva loses patent ruling".Briefcase.The Philadelphia Inquirer.Bloomberg News. September 2, 2017. p. A12.RetrievedJune 23,2018– via Newspapers.com (Publisher Extra).
  33. ^"U.S. appeals court upholds ruling that canceled Teva Copaxone patents".Reuters.October 12, 2018.RetrievedOctober 12,2018.
  34. ^"In Re: Copaxone Consolidated Cases"(PDF).United States Court of Appeals for the Federal Circuit.October 12, 2018.RetrievedOctober 12,2018.
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