Classifications

• • A—HUMAN NECESSITIES
  • A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
  • A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
  • A61K38/00—Medicinal preparations containing peptides
  • A61K38/02—Peptides of undefined number of amino acids; Derivatives thereof
• • A—HUMAN NECESSITIES
  • A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
  • A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
  • A61K47/00—Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
  • A61K47/30—Macromolecular organic or inorganic compounds, e.g. inorganic polyphosphates
  • A61K47/32—Macromolecular compounds obtained by reactions only involving carbon-to-carbon unsaturated bonds, e.g. carbomers, poly(meth)acrylates, or polyvinyl pyrrolidone
• • A—HUMAN NECESSITIES
  • A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
  • A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
  • A61K47/00—Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
  • A61K47/30—Macromolecular organic or inorganic compounds, e.g. inorganic polyphosphates
  • A61K47/36—Polysaccharides; Derivatives thereof, e.g. gums, starch, alginate, dextrin, hyaluronic acid, chitosan, inulin, agar or pectin
• • A—HUMAN NECESSITIES
  • A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
  • A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
  • A61K47/00—Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
  • A61K47/50—Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates
  • A61K47/51—Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates the non-active ingredient being a modifying agent
  • A61K47/56—Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates the non-active ingredient being a modifying agent the modifying agent being an organic macromolecular compound, e.g. an oligomeric, polymeric or dendrimeric molecule
  • A61K47/59—Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates the non-active ingredient being a modifying agent the modifying agent being an organic macromolecular compound, e.g. an oligomeric, polymeric or dendrimeric molecule obtained otherwise than by reactions only involving carbon-to-carbon unsaturated bonds, e.g. polyureas or polyurethanes
  • A61K47/593—Polyesters, e.g. PLGA or polylactide-co-glycolide
• • A—HUMAN NECESSITIES
  • A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
  • A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
  • A61K9/00—Medicinal preparations characterised by special physical form
  • A61K9/0012—Galenical forms characterised by the site of application
  • A61K9/0019—Injectable compositions; Intramuscular, intravenous, arterial, subcutaneous administration; Compositions to be administered through the skin in an invasive manner
  • A61K9/0024—Solid, semi-solid or solidifying implants, which are implanted or injected in body tissue
• • A—HUMAN NECESSITIES
  • A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
  • A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
  • A61P25/00—Drugs for disorders of the nervous system
  • A61P25/28—Drugs for disorders of the nervous system for treating neurodegenerative disorders of the central nervous system, e.g. nootropic agents, cognition enhancers, drugs for treating Alzheimer's disease or other forms of dementia

Definitions

• the present invention relates to a long acting dosage form of glatiramer acetate and other pharmacologically acceptable salts of glatiramer. Particularly, the present invention relates to depot formulations and other implantable systems for prolonged release of glatiramer acetate.
• MS Multiple Sclerosis
• CNS central nervous system
• MS disease activity can be monitored by magnetic resonance imaging (MRI) of the brain, accumulation of disability, as well as rate and severity of relapses.
• MRI magnetic resonance imaging
• RRMS Relapsing-Remitting Multiple Sclerosis
• Patients suffering from RRMS experience sporadic exacerbations or relapses, as well as periods of remission.
• MS multiple sclerosis
• COPAXONE® glatiramer acetate
• TYSABRI® natalizumab
• PLEGRIDY® peginterferon beta-la
• ZINBRYTA® daclizumab
• Glatiramer acetate Copolymer- 1 also known as glatiramer acetate (GA), marketed under the tradename COPAXONE®, comprises the acetate salts of a mixture of synthetic polypeptides containing L- glutamic acid, L-alanine, L-tyrosine and L-lysine.
• the average molar fractions of the amino acids are 0.141, 0.427, 0.095 and 0.338, respectively, and the average molecular weight of copolymer-1 is between 5,000 and 9,000 Daltons.
• glatiramer acetate is designated L-glutamic acid polymer with L-alanine, L-lysine and L-tyrosine, acetate (salt). Its structural formula is: (Glu, Ala, Lys, Tyr) x « xCH3COOH;
• COPAXONE® is a clear, colorless to slightly yellow, sterile, non-pyrogenic solution for subcutaneous injection. Each milliliter contains 20 mg or 40 mg of glatiramer acetate and 40 mg of mannitol. The pH range of the solution is approximately 5.5 to 7.0 (COPAXONE®, Full Prescribing Information,
• COPAXONE® is indicated for reduction of the frequency of relapses in patients with RRMS, including patients who have experienced a first clinical episode and have MRI features consistent with multiple sclerosis (COPAXONE ® , glatiramer acetate injection, Full Prescribing Information, 2016).
• copolymer- 1 shifts the population of T cells from pro-inflammatory Thl cells to regulatory Th2 cells that suppress the inflammatory response (FDA Copaxone ® label). Given its resemblance to myelin basic protein, copolymer- 1 may also act as a decoy, diverting an autoimmune response against myelin. The integrity of the blood-brain barrier, however, is not appreciably affected by copolymer- 1, at least not in the early stages of treatment.
• Copolymer- 1 is a non-autoantigen which has been demonstrated to suppress experimental allergic encephalomyelitis (EAE) induced by various encephalitogenic agents including mouse spinal cord homogenate (MSCH) which includes all myelin antigens, such as myelin basic protein (MBP) (Sela et al., Bull Inst. Pasteur (1990) 88 303-314), proteolipid protein (PLP) (Teitelbaum et al., J. Neuroimmunol. (1996) 64 209-217) and myelin oligodendrocyte glycoprotein (MOG) (Ben-Nun et al., J. Neurol. (1996) 243 (Suppl. 1) S 14-S22) in a variety of species. EAE is an accepted model for multiple sclerosis.
• MSCH mouse spinal cord homogenate
• MSCH mouse spinal cord homogenate
• myelin antigens such as myelin basic protein (MBP) (S
• Copolymer- 1 therapy is currently limited to daily or thrice weekly subcutaneous administration. Treatment with copolymer- 1 by ingestion or inhalation is disclosed in US 6,214,791, but these routes of administration have not been shown to attain clinical efficacy in human patients. Approved doses
• COPAXONE ® has been approved since 1996 for treating relapsing -remitting multiple sclerosis (RRMS) in a dose of 20 mg administered by daily subcutaneous injections. Since 2014, COPAXONE ® has also been approved in a dose of 40 mg administered by three injections per week, performed at least 48 hours apart. Compared to daily administration of COPAXONE ® in the 20 mg dose, the latter dose and regime reduce the yearly number of injections by about 200, while maintaining the same efficacy. Side effects
• IV intravenous
• IM intramuscular
• SC subcutaneous
• Microparticles, implants and gels are the most common forms of biodegradable polymeric devices used in practice for prolonging the release of drugs in the body. Microparticles are suspended in an aqueous media right before injection and one can load as much as 40% solids in suspensions. Implant/rod formulations are delivered to SC/IM tissue with the aid of special needles in the dry state without the need for an aqueous media. This feature of rods/implants allows for higher masses of formulation, as well as drug content to be delivered. Further, in the rods/implants, the initial burst problems are minimized due to much smaller area in implants compared to the microparticles. Besides biodegradable systems, there are non-biodegradable implants and infusion pumps that can be worn outside the body.
• Non-biodegradable implants require a doctor not only for implanting the device into the SC/IM tissue but also to remove them after the drug release period.
• Injectable compositions containing microparticle preparations are particularly susceptible to problems.
• Microparticle suspensions may contain as much as 40% solids as compared with 0.5- 5% solids in other types of injectable suspensions.
• microparticles used in injectable depot products range in size up to about 250 ⁇ (average, 60-100 ⁇ ), as compared with a particle size of less than 5 ⁇ recommended for IM or SC administration.
• the higher concentrations of solids, as well as the larger solid particle size require larger size of needle (around 18-21 gauge) for injection.
• patients still prefer the considerably less frequently administered dosage forms over everyday drug injections with a smaller needle.
• Biodegradable polyesters of poly(lactic acid) (PLA) and copolymers of lactide and glycolide referred to as poly(lactic-co-glycolic acid) or poly(lactide-co-glycolide) (PLGA) are the most common polymers used in biodegradable dosage forms.
• PLA is hydrophobic molecule and PLGA degrades faster than PLA because of the presence of more hydrophilic glycolide groups.
• These biocompatible polymers undergo random, non-enzymatic, hydrolytic cleavage of the ester linkages to form lactic acid and glycolic acid, which are normal metabolic compounds in the body. Resorbable sutures, clips and implants are the earliest applications of these polymers.
• the biodegradable polymer is selected from PLGA, PLA, PGA and any combination thereof. Each possibility represents a separate embodiment of the invention.
• PLGA polymers are commercially available from multiple suppliers. Besides PLGA and PLA, natural cellulosic polymers such as starch, starch derivatives, dextran and non-PLGA synthetic polymers are also being explored as biodegradable polymers in such systems.
• WO 2011/080733 to some of the inventors describes long-acting parenteral pharmaceutical compositions comprising glatiramer. Khan et al, (Ann. Neurol. 2013, Vol. 73, pages 705-713) describes a study to assess the efficacy and safety of 40 mg glatiramer acetate administered 3 times weekly in patients with relapsing-remitting multiple sclerosis (RRMS).
• RRMS relapsing-remitting multiple sclerosis
• the present invention provides compositions and methods for treating relapsing remitting multiple sclerosis, comprising a single parenteral administration or implantation of a composition in the form of a depot formulation providing a monthly dose of 40 mg of pharmaceutically acceptable salts of glatiramer, in particular glatiramer acetate (GA).
• glatiramer in particular glatiramer acetate (GA).
• the long acting pharmaceutical compositions and depot formulations according to the principles of the present invention provide equal or superior therapeutic efficacy to the commercially available daily or thrice weekly injectable dosage forms, i.e. COPAXONE ® . It has further been surprisingly found that a single administration of a depot of 40 mg glatiramer acetate according to the principles of the present invention every 4 weeks is at least as therapeutically effective as daily injections of 20 mg glatiramer acetate or thrice weekly administration of 40 mg glatiramer acetate, thus lowering the need for GA administrations (injections) by a factor of 28 and 12, respectively.
• the therapeutic efficiency is comparable despite the fact that the total administered dosage of GA is decreased by a factor of 14 and 12, respectively. Treating MS patients by methods disclosed in the present invention requires fewer injections with lower dosages of GA, compared to previously available therapies with glatiramer acetate.
• the present invention provides, in one aspect, a method of alleviating at least one symptom of relapsing-remitting multiple sclerosis (RRMS) in a human patient suffering from RRMS or a human patient who has experienced a first clinical episode and is determined to be at high risk of developing clinically definite multiple sclerosis, comprising administering to the patient a therapeutically effective regimen of a single intramuscular injection of a depot formulation comprising 40 mg dose of glatiramer acetate (GA) every 2 to 6 weeks, the regimen being sufficient to alleviate the at least one symptom of the patient, wherein the symptom is selected from the group consisting of the frequency of relapses, the number of enhancing lesions or the number of new lesions images of brain MRI, and the Expanded Disability Status Scale (EDSS) score of the patient.
• RRMS relapsing-remitting multiple sclerosis
• the depot formulation is administered once every 3 to 5 weeks. In certain embodiments, the depot formulation is administered once every 3 weeks. In certain embodiments, the depot formulation is administered once every 4 weeks. In certain embodiments, the depot formulation is administered once every 5 weeks.
• alleviating a symptom comprises reducing the frequency of relapses.
• alleviating a symptom comprises reducing the number or volume of enhancing lesions or the number of new lesions in the brain. In certain embodiments, alleviating a symptom comprises reducing brain atrophy, reducing the number or volume of Gd-enhancing lesions, reducing the number or volume of Ti-weighted enhancing lesions, or reducing the number of new T2-weighted lesions, in the patient. In certain embodiments, alleviating a symptom comprises reducing the mean cumulative number of Gd-enhancing lesions, reducing the mean number of new T2 lesions, reducing the total volume of T2 lesions, or reducing the cumulative number of enhancing lesions on Tl-weighted images in the brain of the patient. In certain embodiments, alleviating a symptom comprises reducing the number of new hypo- intense lesions on enhanced Tl scans in the patient or reducing the total volume of hypo -intense lesions on enhanced Tl scans in the patient.
• alleviating a symptom comprises reducing the EDSS score of the patient. In certain embodiments, alleviating a symptom comprises reducing the EDSS score of the patient by at least 0.5 score. In certain embodiments, alleviating a symptom comprises reducing a level of disability, as measured by the work productivity and activities impairment-General Health (WPAI-GH) questionnaire, or by EuroQoL (EQ-5D) questionnaire, in the patient. In certain embodiments, alleviating a symptom comprises reducing a change in Ambulation Index in the patient. In certain embodiments of the methods described above, the method alleviates the symptom at least as effectively as daily subcutaneous administrations of 20 mg GA or thrice weekly subcutaneous injections of 40 mg GA.
• WPAI-GH work productivity and activities impairment-General Health
• EQ-5D EuroQoL
• alleviating a symptom comprises reducing a change in Ambulation Index in the patient. In certain embodiments of the methods described above, the method alleviates the symptom at least as effectively as daily subcutaneous administrations of
• the depot formulation is administered intramuscularly by the patient. In certain embodiments, the depot formulation is injected into the deltoid muscle. In certain embodiments, the patient has not received GA therapy prior to initiation of the regimen. In certain embodiments, the patient has received GA therapy prior to initiation of the regimen. In certain embodiments, the patient has at least 1 cerebral lesion detectable by an MRI scan and wherein the lesion is associated with brain tissue inflammation, myelin sheath damage or axonal damage. In certain embodiments, the lesion is a demyelinating white matter lesion visible on brain MRI and wherein the white matter lesion is at least 3 mm in diameter.
• the patient has experienced a first clinical episode and wherein the first clinical episode includes a clinical episode of optic neuritis, blurring of vision, diplopia, involuntary rapid eye movement, blindness, loss of balance, tremors, ataxia, vertigo, clumsiness of a limb, lack of coordination, weakness of one or more extremity, altered muscle tone, muscle stiffness, spasms, tingling, paraesthesia, burning sensations, muscle pains, facial pain, trigeminal neuralgia, stabbing sharp pains, burning tingling pain, slowing of speech, slurring of words, changes in rhythm of speech, dysphagia, fatigue, bladder problems (including urgency, frequency, incomplete emptying and incontinence), bowel problems (including constipation and loss of bowel control), impotence, diminished sexual arousal, loss of sensation, sensitivity to heat, loss of short term memory, loss of concentration, or loss of judgment or reasoning.
• the first clinical episode includes a clinical episode of optic neuritis, blurring of
• the frequency of an immediate post injection reaction, the severity of an immediate post injection reaction or the frequency of an injection site reaction is reduced relative to daily subcutaneous administration of 20 mg GA or a thrice weekly subcutaneous injection of 40 mg GA.
• the depot formulation further comprises a pharmaceutically acceptable biodegradable carrier selected from the group consisting of poly(lactic-co-glycolic acid) (PLGA), poly(lactic acid) (PLA), poly(glycolic acid) (PGA), and any combination thereof.
• the biodegradable carrier is PLGA.
• the depot formulation is in the form of microparticles comprising an internal aqueous phase comprising the GA, a water immiscible polymeric phase comprising a biodegradable or non-biodegradable polymer, and an external aqueous phase.
• the depot formulation is in the form of microparticles prepared by a water-in oil -in water (w/o/w) double emulsification process.
• the internal aqueous phase comprises the GA.
• the water immiscible polymeric phase comprises PLGA.
• the external water phase comprises a surfactant selected from poly(vinyl alcohol) (PVA), polysorbate, polyethylene oxide -polypropylene oxide block copolymers and cellulose esters.
• the surfactant is PVA.
• the depot formulation is administered in 2 mL of water for injection (WFI). In certain embodiments, the depot formulation comprises 10% to 40% solids. In certain embodiments, the depot formulation comprises 20% to 30% solids. In certain embodiments, the depot formulation comprises 25% solids.
• the weight ratio between the GA and the pharmaceutically acceptable biodegradable carrier is between 1 : 1 to 1 : 100. In certain embodiments, the weight ratio between the GA and the pharmaceutically acceptable biodegradable carrier is between 1 :5 to 1 :25.
• the depot formulation provides prolonged release or prolonged action of glatiramer in a subject as compared to a substantially similar dose of an immediate release formulation of glatiramer. In certain embodiments, about 80% of the glatiramer is released from the depot formulation within 22 days in PBS at 37°C under continuous agitation. In certain embodiments, about 20% of the glatiramer is released from the depot formulation within 5 days in PBS at 37°C under continuous agitation.
• the present invention further provides, in another aspect, a method of increasing the tolerability of GA treatment in a human patient suffering from relapsing-remitting multiple sclerosis, comprising reducing the frequency of subcutaneous injections from daily subcutaneous injections of a 20 mg dose of GA or three subcutaneous injections of a 40 mg dose of GA over a period of seven days with at least one day between every injection, to a therapeutically effective regimen of a single intramuscular injection of a depot formulation of a 40 mg dose of GA every 2 to 6 weeks, so as to thereby increase the tolerability of GA treatment in the patient.
• the depot formulation is administered once every 3 to 5 weeks. In certain embodiments, the depot formulation is administered once every 4 weeks. In certain embodiments, increasing the tolerability of GA treatment in the patient suffering from relapsing-remitting multiple sclerosis comprises reducing the frequency of injection. In certain embodiments, increasing the tolerability of GA treatment in the patient suffering from relapsing- remitting multiple sclerosis comprises reducing the frequency of an injection site reaction.
• the present invention further provides, in another aspect, a method of reducing the frequency of relapses in a human patient suffering from relapsing-remitting multiple sclerosis or a human patient who has experienced a first clinical episode and is determined to be at high risk of developing clinically definite multiple sclerosis, comprising administering to the patient a therapeutically effective regimen of a single injection of a depot formulation of a 40 mg dose of GA every 2 to 6 weeks, the regimen being sufficient to reduce frequency of relapses in the patient.
• the present invention further provides, in another aspect, a method of preventing or slowing progression of relapsing-remitting multiple sclerosis (RRMS) in a human patient suffering from RRMS, comprising administering to the human patient a therapeutically effective regimen of a single intramuscular injection of a depot formulation comprising 40 mg dose of glatiramer acetate (GA) every 2 to 6 weeks.
• RRMS relapsing-remitting multiple sclerosis
• the regimen is sufficient to ameliorate (a) the frequency of relapses, (b) the number or volume of enhancing lesions, (c) the number of new lesions, or (d) the Expanded Disability Status Scale (EDSS) score of the patient. In certain embodiments, the regimen is sufficient to ameliorate the frequency of relapses, the number or volume of enhancing lesions, the number of new lesions, and the Expanded Disability Status Scale (EDSS) score of the patient.
• the present invention further provides, in another aspect, a method of preventing disease activity in a human patient suffering from relapsing-remitting multiple sclerosis, comprising administering to the patient a therapeutically effective regimen of a single injection of a depot formulation of a 40 mg dose of GA every 2 to 6 weeks, the regimen being sufficient to prevent relapses, 12-week confirmed disability progression (CDP), new lesion formation and enhancement of existing lesions in the patient.
• a method of preventing disease activity in a human patient suffering from relapsing-remitting multiple sclerosis comprising administering to the patient a therapeutically effective regimen of a single injection of a depot formulation of a 40 mg dose of GA every 2 to 6 weeks, the regimen being sufficient to prevent relapses, 12-week confirmed disability progression (CDP), new lesion formation and enhancement of existing lesions in the patient.
• CDP 12-week confirmed disability progression
• the present invention further provides, in another aspect, a kit, comprising a first container comprising GA encapsulated with a poly(lactic-co-glycolic acid) (PLGA), and a second separate container comprising a pharmaceutically acceptable diluent for injection.
• a kit comprising a first container comprising GA encapsulated with a poly(lactic-co-glycolic acid) (PLGA), and a second separate container comprising a pharmaceutically acceptable diluent for injection.
• PLGA poly(lactic-co-glycolic acid)
• the kit comprises 40 mg GA and 2-10 ml WFI. In certain embodiments, mixing the content of the first container with 2 ml of diluent provides 40 mg GA per 2 ml of suspension. In certain embodiments, the kit is for use in a method of alleviating at least one symptom of relapsing-remitting multiple sclerosis (RRMS), increasing the tolerability of GA treatment, preventing or slowing progression of RRMS, or preventing RRMS activity.
• RRMS relapsing-remitting multiple sclerosis
• the present invention provides long acting depot formulations of glatiramer acetate, which afford equal or superior therapeutic efficacy compared to the daily or thrice weekly injections of COPAXONE ® , and thus result in improved patient compliance.
• the long acting injections or implants of the present invention reduce the adverse side effects resulting from frequent injections.
• the invention is based on the surprising finding that the current standard treatment for MS patients, i.e. the daily administration of 20 mg GA by injection, is unnecessarily aggressive in terms of the total drug used and the frequency of invasive administration. Specifically, it has been surprisingly found that 40 mg of GA, administered once every 28 days, where sufficient to achieve beneficial clinical efficacy, which is at least comparable with the beneficial clinical efficacy of GA administered every day over a period of 28 days for a total dose of 560 mg.
• the present invention thus provides a method of treating MS with a 14-fold decrease in the administered dose and a 28-fold decrease in the frequency of administration, compared to the original and still ongoing standard of care.
• the present invention is further superior over the more recent COPAXONE ® therapy regimen, which includes a thrice weekly administration of 40 mg GA.
• treating RRMS according to the present invention provides a 12-fold reduction in the total administered dose and in the frequency of GA administration.
• the present invention provides, in one aspect, a method of alleviating at least one symptom of relapsing-remitting multiple sclerosis (RRMS) in a human patient suffering from RRMS or a human patient who has experienced a first clinical episode or a human patient who is determined to be at high risk of developing clinically definite multiple sclerosis, comprising administering to the patient a therapeutically effective regimen of a single injection of a long acting depot formulation comprising at least 20 mg dose of glatiramer or any pharmaceutically acceptable salt of glatiramer every 2 to 6 weeks, the regimen being sufficient to alleviate the at least one symptom of the patient, wherein the symptom is selected from the group consisting of the frequency of relapses, the number of enhancing lesions or the number of new lesions images of brain MRI, and the Expanded Disability Status Scale (EDSS) score of the patient.
• RRMS relapsing-remitting multiple sclerosis
• the present invention provides, in one aspect, a method of alleviating at least one symptom of relapsing-remitting multiple sclerosis (RRMS) in a human patient suffering from RRMS or a human patient who has experienced a first clinical episode or a human patient who is determined to be at high risk of developing clinically definite multiple sclerosis, comprising administering to the patient a therapeutically effective regimen of a single injection of a long acting depot formulation comprising at least 20 mg dose of glatiramer or any pharmaceutically acceptable salt of glatiramer every 2 to 6 weeks, the regimen being sufficient to alleviate the at least one symptom of the patient, wherein the symptom is selected from the group consisting of the frequency of relapses, the number of enhancing lesions or the number of new lesions images of brain MRI, and the Expanded Disability Status Scale (EDSS) score of the patient.
• RRMS relapsing-remitting multiple sclerosis
• the depot formulation is administered once every 3 to 5 weeks. In certain embodiments, the depot formulation is administered once every 4 weeks.
• each depot or implantable device of the present invention will typically contain between about 40 and 520 mg of the active ingredient, designed to be released once over a period of 4 weeks to 13 times over a period of a year, every four weeks.
• treating refers to suppression or alleviation of at least one symptom after the onset of multiple sclerosis.
• Common symptoms after the onset of multiple sclerosis include, but are not limited to, reduced or loss of vision, stumbling and uneven gait, slurred speech, as well as urinary frequency and incontinence.
• multiple sclerosis can cause mood changes and depression, muscle spasms and severe paralysis.
• the phrase "alleviating at least one symptom of RRMS" as used herein refers to any beneficial change in the severity of a symptom or in the frequency of a symptom of RRMS. This phrase further includes preventing or delaying the progress of RRMS symptoms compared to untreated RRMS patients or compared to RRMS patients treated by other therapies, drugs or regimens.
• a human patient who is determined to be at high risk of developing clinically definite multiple sclerosis refers to patient(s) which are defined to be in at least one risk group to develop RRMS. RRMS risk groups are long known, and are reviewed e.g. by McKay et al. (Biomed. Res. Int., 2015, Vol. 2015, Article ID 817238).
• a human patient who is determined to be at high risk of developing clinically definite multiple sclerosis has MRI features consistent with multiple sclerosis.
• a human patient who is determined to be at high risk of developing clinically definite multiple sclerosis has experienced a first clinical episode and has MRI features consistent with multiple sclerosis.
• multiple sclerosis refers to an auto-immune disease of the central nervous system which is accompanied by one or more of the symptoms described hereinabove.
• glatiramer acetate refers to a compound formerly known as Copolymer 1 that is sold under the trade name COPAXONE ® and includes the acetate salts of synthetic polypeptides, containing four naturally occurring amino acids: L-glutamic acid, L- alanine, L-tyrosine, and L-lysine with an average molar fraction of 0.141, 0.427, 0.095, and 0.338, respectively.
• the average molecular weight of glatiramer acetate in COPAXONE ® is 4,700-11,000 Daltons (FDA COPAXONE ® label) and the number of amino acid ranges between about 15 to about 100 amino acids.
• the term also refers to chemical derivatives and analogues of the compound.
• the compound is prepared and characterized as specified in any one of US Patent Nos. 5,981,589; 6,054,430; 6,342,476; 6,362,161; 6,620,847; and 6,939,539.
• the glatiramer acetate comprises the acetate salt of L-alanine, L-glutamic acid, L-lysine, and L-tyrosine in the molar ratios of about 0.14 glutamic acid, about 0.43 alanine, about 0.10 tyrosine and about 0.33 lysine.
• the glatiramer acetate or other pharmaceutically acceptable salt of glatiramer comprises about 15 to about 100 amino acids.
• the implantable depot is suitable for subcutaneous or intramuscular implantation.
• the long acting parenteral pharmaceutical composition comprises a pharmaceutically acceptable biodegradable or non-biodegradable carrier for glatiramer salts.
• the carrier is selected from PLGA, PLA, PGA, polycaprolactone, polyhydroxybutyrate, polyorthoesters, polyalkaneanhydrides, gelatin, collagen, oxidized cellulose, and polyphosphazene.
• the carrier is selected from PLGA, PLA, PGA and any combination thereof. Each possibility represents a separate embodiment of the invention.
• the at least one symptom alleviated is the frequency of relapses and the number of enhancing lesions or the number of new lesions images of brain MRI.
• the at least one symptom alleviated is the number of enhancing lesions or the number of new lesions images of brain MRI and the Expanded Disability Status Scale (EDSS) score of the patient. In certain embodiments, the at least one symptom alleviated is the frequency of relapses and the Expanded Disability Status Scale (EDSS) score of the patient. In certain embodiments, the at least one symptom alleviated the frequency of relapses, the number of enhancing lesions or the number of new lesions images of brain MRI, and the Expanded Disability Status Scale (EDSS) score of the patient.
• the copolymers can be made by any procedure available to one of skill in the art.
• the copolymers can be made under condensation conditions using the desired molar ratio of amino acids in solution, or by solid phase synthetic procedures.
• Condensation conditions include the proper temperature, pH, and solvent conditions for condensing the carboxyl group of one amino acid with the amino group of another amino acid to form a peptide bond.
• Condensing agents for example, dicyclohexylcarbodiimide, can be used to facilitate the formation of the peptide bond.
• the composition may comprise any other pharmaceutically acceptable salt of glatiramer including, but not limited to, sulfate, pyrosulfate, bisulfate, sulfite, bisulfite, phosphate, monohydrogenphosphate, dihydrogenphosphate, metaphosphate, pyrophosphate, hydrochloride, hydrobromide, hydroiodide, acetate, nitrate, propionate, decanoate, caprylate, acrylate, formate, isobutyrate, caprate, heptanoate, propiolate, oxalate, malonate, succinate, tocopheryl succinate, suberate, sebacate, fumarate, maleate, butyne-l,4-dioate, hexyne-1 ,6- dioate, benzoate, chlorobenzoate, methylbenzoate, dinitrobenzoate, hydroxybenzoate, methoxybenzoate, phthalate, ter
• the dosage forms include, but are not limited to, biodegradable injectable depot systems such as, PLGA based injectable depot systems; non-PLGA based injectable depot systems, and injectable biodegradable gels or dispersions.
• biodegradable refers to a component which erodes or degrades at its surfaces over time due, at least in part, to contact with substances found in the surrounding tissue fluids, or by cellular action.
• the biodegradable component is a polymer such as, but not limited to, lactic acid-based polymers such as polylactides e.g. poly(D,L-lactide) i.e.
• PLA glycolic acid-based polymers such as polyglycolides or poly(glycolic acid) (PGA) e.g. LACTEL®; poly(D,L-lactide-co-glycolide) i.e. PLGA, (RESOMER® RG-504, RESOMER® RG-502, RESOMER® RG-504H, RESOMER® RG- 502H, RESOMER® RG-504S, RESOMER® RG-502S, LACTEL®); polycaprolactones such as Poly(e-caprolactone) i.e.
• PCL (LACTEL®); polyanhydrides; poly(sebacic acid) SA; poly(ricenolic acid) RA; poly(fumaric acid), FA; poly(fatty acid dimmer), FAD; poly(terephthalic acid), TA; poly(isophthalic acid), IPA; poly(p- ⁇ carboxyphenoxy ⁇ methane),
• DETOU (3,9-diethylidene-2,4,8, 10- tetraoxaspiro undecane) ⁇ ; polydioxanones; polyhydroxybutyrates; polyalkylene oxalates; polyamides; polyesteramides; polyurethanes; polyacetals; polyketals; polycarbonates; polyorthocarbonates; polysiloxanes; polyphosphazenes; succinates; hyaluronic acid; poly(malic acid); poly(amino acids); polyhydroxyvalerates; polyalkylene succinates; polyvinylpyrrolidone; polystyrene; synthetic cellulose esters; polyacrylic acids; polybutyric acid; triblock copolymers (PLGA-PEG-PLGA), triblock copolymers (PEG-PLGA-PEG), poly(N-isopropylacrylamide) (PNIPAAm), poly(ethylene oxide)- poly(propylene oxide)- poly(ethylene oxide) tri-block cop
• PPO-PEO poly valeric acid
• polyethylene glycol polyhydroxyalkylcellulose
• chitin chitosan
• polyorthoesters and copolymers, terpolymers lipids such as cholesterol, lecithin; poly(glutamic acid-co-ethyl glutamate) and the like, or mixtures thereof.
• the compositions of the present invention comprise a biodegradable polymer selected from, but not limited to, PLGA, PLA, PGA, polycaprolactone, polyhydroxybutyrate, polyorthoesters, polyalkaneanhydrides, gelatin, collagen, oxidized cellulose, polyphosphazene and the like.
• a biodegradable polymer selected from, but not limited to, PLGA, PLA, PGA, polycaprolactone, polyhydroxybutyrate, polyorthoesters, polyalkaneanhydrides, gelatin, collagen, oxidized cellulose, polyphosphazene and the like.
• the biodegradable polymer is a lactic acid-based polymer, for example polylactide, or poly(D, L-lactide-co-glycolide) i.e. PLGA.
• the biodegradable polymer is present in an amount between about 10% to about 98% w/w of the composition.
• the lactic acid-based polymer has a monomer ratio of lactic acid to glycolic acid in the range of 100:0 to about 0: 100, for example 100:0 to about 10:90 and has an average molecular weight of from about 1,000 to 200,000 Daltons.
• the amount of biodegradable polymer is determined by parameters such as the duration of use and the like.
• the long acting pharmaceutical compositions of the present invention are in the form of microparticles prepared by a water-in oil-in water double emulsification process.
• the long acting pharmaceutical compositions of the present invention comprise an internal aqueous phase comprising a therapeutically effective amount of a pharmaceutically acceptable salt of glatiramer, a water immiscible polymeric phase comprising a carrier selected from a biodegradable and a non-biodegradable polymer, and an external aqueous phase.
• the water immiscible polymeric phase comprises a biodegradable polymer selected from PLGA, PLA and combinations thereof.
• the external aqueous phase comprises a surfactant selected from poly(vinyl alcohol) (PVA), polysorbate, polyethylene oxide-polypropylene oxide block copolymers and cellulose esters.
• PVA poly(vinyl alcohol)
• PVP poly(vinyl alcohol)
• polysorbate polyethylene oxide-polypropylene oxide block copolymers
• cellulose esters a surfactant selected from poly(vinyl alcohol) (PVA), polysorbate, polyethylene oxide-polypropylene oxide block copolymers and cellulose esters.
• compositions of the present invention may further comprise one or more pharmaceutically acceptable excipient(s) selected from, but not limited to, co-surfactants, solvents/co-solvents, water immiscible solvents, water, water miscible solvents, oily components, hydrophilic solvents, emulsifiers, preservatives, antioxidants, anti-foaming agents, stabilizers, buffering agents, pH adjusting agents, osmotic agents, channel forming agents, osmotic adjustment agents, or any other excipient known in the art.
• excipient(s) selected from, but not limited to, co-surfactants, solvents/co-solvents, water immiscible solvents, water, water miscible solvents, oily components, hydrophilic solvents, emulsifiers, preservatives, antioxidants, anti-foaming agents, stabilizers, buffering agents, pH adjusting agents, osmotic agents, channel forming agents, osmotic adjustment agents,
• Suitable co-surfactants include, but are not limited to, polyethylene glycols, polyoxyethylene- polyoxypropylene block copolymers known as "poloxamer", polyglycerin fatty acid esters such as decaglyceryl monolaurate and decaglyceryl monomyristate, sorbitan fatty acid ester such as sorbitan monostearate, polyoxyethylene sorbitan fatty acid ester such as polyoxyethylene sorbitan monooleate (Tween), polyethylene glycol fatty acid ester such as polyoxyethylene monostearate, polyoxyethylene alkyl ether such as polyoxyethylene lauryl ether, polyoxyethylene castor oil and hardened castor oil such as polyoxyethylene hardened castor oil, and the like or mixtures thereof.
• polyethylene glycols polyoxyethylene- polyoxypropylene block copolymers known as "poloxamer”
• polyglycerin fatty acid esters such as decaglyceryl monolaurate and de
• Suitable solvents/co-solvents include, but not limited to, alcohols, triacetin, dimethyl isosorbide, glycofurol, propylene carbonate, water, dimethyl acetamide, and the like or mixtures thereof.
• Suitable anti-foaming agents include, but are not limited to, silicon emulsions or sorbitan sesquioleate.
• Suitable stabilizers to prevent or reduce the deterioration of the components in the compositions of the present invention include, but are not limited to, antioxidants such as glycine, a-tocopherol or ascorbate, BHA, BHT, and the like or mixtures thereof.
• Suitable tonicity modifiers include, but are not limited to, mannitol, sodium chloride, and glucose.
• Suitable buffering agents include, but are not limited to, acetates, phosphates, and citrates with suitable cations. Each possibility represents a separate embodiment of the invention.
• the particle size of the "water-in oil-in water (w/o/w) double emulsion" can be determined by various parameters including, but not limited to, the amount of applied force at this step, the speed of mixing, surfactant type and concentration, etc. Suitable particle sizes range from about 1 to 100 ⁇ .
• the depot systems of the present invention encompass any forms known to a person of skill in the art. Suitable forms include, but are not limited to, biodegradable or non-biodegradable microspheres, implantable rods, implantable capsules, and implantable rings. Each possibility represents a separate embodiment of the invention. Further contemplated are prolonged release gel depot and erodible matrices. Each possibility represents a separate embodiment of the invention. Suitable implantable systems are described for example in US 2008/0063687. Implantable rods can be prepared as is known in the art using suitable micro-extruders.
• the depot formulations of the present invention include, but are not limited to, suspensions of glatiramer acetate in water, oil or wax phase; poorly soluble polyelectrolyte complexes of glatiramer acetate; "in-situ" gel-forming matrices based on the combination of water-miscible solvent with glatiramer acetate; and biodegradable polymeric microparticles with incorporated glatiramer acetate.
• the compositions of the present invention are in the form of injectable microparticles wherein the glatiramer acetate is entrapped in a biodegradable or non-biodegradable carrier.
• microparticulate compositions of the present invention may comprise a water-in oil-in water double emulsion.
• a microparticulate composition comprising an internal aqueous phase comprising glatiramer or any pharmaceutically acceptable salt thereof, an oil phase or water-immiscible phase comprising a biodegradable or non-biodegradable polymer and an external aqueous phase.
• the external aqueous phase may further comprise a surfactant, for example poly(vinyl alcohol) (PVA), polysorbate, polyethylene oxide -polypropylene oxide block copolymers or cellulose esters.
• PVA poly(vinyl alcohol)
• the terms "oil phase” and “water-immiscible phase” may be used interchangeably herein.
• the glatiramer acetate comprises the acetate salt of L-alanine, L-glutamic acid, L-lysine, and L-tyrosine in the molar ratios of about 0.14 glutamic acid, about 0.43 alanine, about 0.10 tyrosine and about 0.33 lysine.
• the glatiramer acetate or other pharmaceutically acceptable salt of glatiramer comprises about 15 to about 100 amino acids.
• the depot formulation is administered once every 2 weeks. In certain embodiments, the depot formulation is administered once every 3 weeks. In certain embodiments, the depot formulation is administered once every 4 weeks. In certain embodiments, the depot formulation is administered once every 5 weeks. In certain embodiments, the depot formulation is administered once every 6 weeks.
• the long acting pharmaceutical composition is suitable for a dosing schedule from once weekly to once in every 6 months. According to particular embodiments, the composition is suitable for dosing from once every 2 weeks to once monthly. According to some embodiments, the long acting compositions comprise a dose between 20 to 750 mg of glatiramer acetate per injection.
• the long acting compositions comprise a dose between 20 to 160 mg of glatiramer acetate per injection. According to some embodiments, the long acting compositions comprise a dose between 30 to 50 mg of glatiramer acetate per injection.
• alleviating a symptom comprises reducing the frequency of relapses. In certain embodiments, alleviating a symptom comprises reducing the frequency of relapses in the patient by 30% or more compared to the frequency of relapses measured in a period of 12 months before starting the regimen. In certain embodiments, alleviating a symptom comprises increasing the time to a confirmed relapse in the patient compared to the time between relapses measured in a period of 12 months before starting the regimen. In certain embodiments, alleviating a symptom comprises reducing the total number of confirmed relapses in the patient measured in a period of 12 months during the regimen compared to a period of 12 months before starting the regimen.
• alleviating a symptom comprises reducing the number or volume of enhancing lesions in the brain. In certain embodiments, alleviating a symptom comprises reducing the number of new lesions in the brain. In certain embodiments, alleviating a symptom comprises reducing the number of enhancing lesions images of brain MRI, measured in a period of 12 months. In certain embodiments, alleviating a symptom comprises reducing the number of new lesions images of brain MRI, measured in a period of 12 months. In certain embodiments, alleviating a symptom comprises reducing brain atrophy, reducing the number or volume of Gd- enhancing lesions, reducing the number or volume of Ti-weighted enhancing lesions, or reducing the number of new T2-weighted lesions, in the patient.
• alleviating a symptom comprises reducing the mean cumulative number of Gd-enhancing lesions, reducing the mean number of new T2 lesions, reducing the total volume of T2 lesions, or reducing the cumulative number of enhancing lesions on Tl -weighted images in the brain of the patient.
• alleviating a symptom comprises reducing the number of new hypointense lesions on enhanced Tl scans in the patient or reducing the total volume of hypointense lesions on enhanced Tl scans in the patient.
• alleviating a symptom comprises reducing the progression of MRI-monitored disease activity in the patient.
• the Kurtzke Expanded Disability Status Scale is a method of quantifying disability in multiple sclerosis.
• the EDSS quantifies disability in eight Functional Systems (FS) and allows neurologists to assign a Functional System Score (FSS) in each of these.
• alleviating a symptom comprises reducing the EDSS score of the patient.
• alleviating a symptom comprises reducing the EDSS score of the patient, measured in a period of 12 months.
• alleviating a symptom comprises reducing the EDSS score of the patient by at least 0.5.
• alleviating a symptom comprises reducing the EDSS score of the patient by at least 1.
• alleviating a symptom comprises reducing the EDSS score of the patient from a score in the range of 5.0-9.5 to a score in the range of 0.0-4.5.
• alleviating a symptom comprises reducing a level of disability, as measured by the work productivity and activities impairment-General Health (WPAI-GH) questionnaire, or as measured by EuroQoL (EQ5D) questionnaire, in the patient. In certain embodiments, alleviating a symptom comprises reducing a change in Ambulation Index in the patient.
• WPAI-GH work productivity and activities impairment-General Health
• EQ5D EuroQoL
• alleviating a symptom comprises reducing the level of disability as measured by EDSS Score in the patient. In another embodiment, alleviating a symptom comprises reducing the change in EDSS Score in the patient.
• the method alleviates the symptom at least as effectively as daily subcutaneous administrations of 20 mg GA or thrice weekly subcutaneous injections of 40 mg GA.
• the long acting pharmaceutical compositions of the present invention provide equal or superior therapeutic efficacy to the commercially available daily injectable dosage forms, with reduced incidence of side effects and with reduced severity of side effects at the local and/or systemic level.
• the compositions of the present invention provide prolonged release or prolonged action of glatiramer in a subject as compared to a substantially similar dose of an immediate release formulation of glatiramer acetate.
• the depot formulation is self-administered intramuscularly by the patient. In certain embodiments, the depot formulation is injected into the deltoid muscle. In certain embodiments, the patient has not received GA therapy prior to initiation of the regimen. In certain embodiments, the patient has received GA therapy prior to initiation of the regimen.
• Encompassed by the present invention is a combination therapy of glatiramer acetate or any other pharmaceutically acceptable salt of glatiramer with at least one other active agent. Active agents within the scope of the present invention include, but are not limited to interferons, e.g. pegylated or non-pegylated a-interferons, or ⁇ -interferons, e.g.
• interferon ⁇ -la or interferon ⁇ -lb, or ⁇ -interferons immuno-suppressants with optionally antiproliferative/antineoplastic activity, e.g. mitoxantrone, methotrexate, azathioprine, cyclophosphamide, or steroids, e.g. methylprednisolone, prednisone or dexamethasone, or steroid-secreting agents, e.g. ACTH; adenosine deaminase inhibitors, e.g. cladribine; IV immunoglobulin G (e.g.
• T-cell surface markers e.g. natalizumab (ANTEGREN ® ) or alemtuzumab
• TH2 promoting cytokines e.g. IL-4, IL-10
• compounds which inhibit expression of TH1 promoting cytokines e.g. phosphodiesterase inhibitors, e.g.
• antispasticity agents including baclofen, diazepam, piracetam, dantrolene, lamotrigine, rifluzole, tizanidine, clonidine, beta blockers, cyproheptadine, orphenadrine or cannabinoids; AMPA glutamate receptor antagonists, e.g.
• ⁇ 4 ⁇ 1 integrin VLA-4 and/or ⁇ -4- ⁇ -7 integrins e.g. natalizumab (ANTEGREN ® ); anti-macrophage migration inhibitory factor (Anti-MIF); xii) Cathepsin S inhibitors; xiii) mTor inhibitors.
• natalizumab ANTEGREN ®
• Anti-MIF anti-macrophage migration inhibitory factor
• xii) Cathepsin S inhibitors xiii) mTor inhibitors.
• An example of one other active agent is FTY720 (2-amino-2-[2-(4- octylphenyl)ethyl] propane-l,3-diol; fingolimod) belonging to the class of immuno-suppressants.
• the patient prior to administration the patient has at least 1 cerebral lesion detectable by an MRI scan and suggestive of multiple sclerosis.
• the lesion is associated with brain tissue inflammation, myelin sheath damage or axonal damage.
• the lesion is a demyelinating white matter lesion visible on brain MRI.
• the white matter lesions are at least 3 mm in diameter.
• the patient has at least 1 cerebral lesion detectable by an MRI scan and wherein the lesion is associated with brain tissue inflammation, myelin sheath damage or axonal damage.
• the lesion is a demyelinating white matter lesion visible on brain MRI and the white matter lesion is at least 3 mm in diameter.
• the patient has experienced a first clinical episode and the first clinical episode includes a clinical episode of optic neuritis, blurring of vision, diplopia, involuntary rapid eye movement, blindness, loss of balance, tremors, ataxia, vertigo, clumsiness of a limb, lack of coordination, weakness of one or more extremity, altered muscle tone, muscle stiffness, spasms, tingling, paraesthesia, burning sensations, muscle pains, facial pain, trigeminal neuralgia, stabbing sharp pains, burning tingling pain, slowing of speech, slurring of words, changes in rhythm of speech, dysphagia, fatigue, bladder problems (including urgency, frequency, incomplete emptying and incontinence), bowel problems (including constipation and loss of bowel control), impotence, diminished sexual arousal, loss of sensation,
• the frequency of an immediate post injection reaction is reduced relative to daily subcutaneous administration of 20 mg GA or a thrice weekly subcutaneous injection of 40 mg GA.
• the severity of an immediate post injection reaction is reduced relative to daily subcutaneous administration of 20 mg GA or a thrice weekly subcutaneous injection of 40 mg GA.
• the frequency of an injection site reaction is reduced relative to daily subcutaneous administration of 20 mg GA or a thrice weekly subcutaneous injection of 40 mg GA.
• the depot formulation is administered in 2 mL of water for injection (WFI), or a buffer containing a suspending agent (e.g. carboxymethylcellulose, CMC), a buffering agent (e.g. citrate salts) and a tonicity agent (e.g. NaCl).
• WFI water for injection
• a suspending agent e.g. carboxymethylcellulose, CMC
• a buffering agent e.g. citrate salts
• a tonicity agent e.g. NaCl
• the depot formulation comprises 20% to 30% solids.
• water for injection means sterile, purified water that meets regulatory standards for particulates, dissolved solids, organics, inorganics, microbial and endotoxin contaminants.
• the glatiramer in PBS at 37°C under continuous agitation, (i) about 14% of the glatiramer is released from the depot formulation within 0 days, and/or (ii) about 15% of the glatiramer is released from the depot formulation within 1 day, and/or (iii) about 21% of the glatiramer is released from the depot formulation within 5 days, and/or (iv) about 25% of the glatiramer is released from the depot formulation within 8 days, and/or (v) about 34% of the glatiramer is released from the depot formulation within 13 days, and/or (vi) about 43% of the glatiramer is released from the depot formulation within 15 days, and/or (vii) about 80% of the glatiramer is released from the depot formulation within 22 days, and/or (viii) about 96% of the glatiramer is released from the depot formulation within 27 days, and/or (ix) about 99% of the glatiramer is released from the depot formulation within 32 days.
• the glatiramer in PBS at 37°C under continuous agitation, (i) about 14% of the glatiramer is released from the depot formulation within 0 days, and (ii) about 15% of the glatiramer is released from the depot formulation within 1 day, and (iii) about 21% of the glatiramer is released from the depot formulation within 5 days, and (iv) about 25% of the glatiramer is released from the depot formulation within 8 days, and (v) about 34% of the glatiramer is released from the depot formulation within 13 days, and (vi) about 43% of the glatiramer is released from the depot formulation within 15 days, and (vii) about 80% of the glatiramer is released from the depot formulation within 22 days, and (viii) about 96% of the glatiramer is released from the depot formulation within 27 days, and (ix) about 99% of the glatiramer is released from the depot formulation within 32 days.
• the present invention further provides, in another aspect, a method of increasing the tolerability of GA treatment in a human patient suffering from relapsing-remitting multiple sclerosis, comprising reducing the frequency of subcutaneous injections from daily subcutaneous injections of a 20 mg dose of GA or three subcutaneous injections of a 40 mg dose of GA over a period of seven days with at least one day between every injection, to a therapeutically effective regimen of a single intramuscular injection of a depot formulation of a 40 mg dose of GA or any other pharmaceutically acceptable salt of glatiramer every 2 to 6 weeks, so as to thereby increase the tolerability of GA treatment in the patient.
• the depot formulation is administered once every 3 to 5 weeks. In certain embodiments, the depot formulation is administered once every 4 weeks.
• increasing the tolerability of GA treatment in the patient suffering from relapsing-remitting multiple sclerosis comprises reducing the frequency of injection. In certain embodiments, increasing the tolerability of GA treatment in the patient suffering from relapsing- remitting multiple sclerosis comprises reducing the frequency of an injection site reaction. In a further embodiment, the injection site reaction is erythema, hemorrhage, induration, inflammation, mass, pain, pruritus, urticaria, or welt that occurs immediately around the site of injection.
• increasing the tolerability of GA treatment in the human patient suffering from a relapsing form of multiple sclerosis comprises reducing the frequency of an immediate post injection reaction.
• the immediate post injection reaction is palpitations, feeling hot, flushing, hot flushes, tachycardia, dyspnoea, chest discomfort, chest pain, non-cardiac chest , asthenia, back pain, bacterial infection, chills, cyst, face edema, fever, flu syndrome, infection, injection site erythema, injection site hemorrhage, injection site induration, injection site inflammation, injection site mass, injection site pain, injection site pruritus, injection site urticaria, injection site welt, neck pain, pain, migrane, syncope, tachycardia, vasodilatation, anorexia, diarrhea, gastroenteritis, gastrointestinal disorder, nausea, vomiting, ecchymosis, peripheral edema, arthralgia, agitation, anxiety, confusion,
• the frequency of an immediate post injection reaction or the frequency of an injection site reaction is reduced relative to daily subcutaneous administration of 20 mg glatiramer acetate or thrice weekly subcutaneous administration of 40 mg glatiramer acetate.
• the present invention further provides, in another aspect, a method of reducing the frequency of relapses in a human patient suffering from relapsing-remitting multiple sclerosis or a human patient who has experienced a first clinical episode and is determined to be at high risk of developing clinically definite multiple sclerosis, comprising administering to the patient a therapeutically effective regimen of a single injection of a depot formulation of a 40 mg dose of GA or any other pharmaceutically acceptable salt of glatiramer every 2 to 6 weeks, the regimen being sufficient to reduce frequency of relapses in the patient.
• the present invention further provides, in another aspect, a method of preventing or slowing progression of relapsing-remitting multiple sclerosis (RRMS) in a human patient suffering from RRMS, comprising administering to the human patient a therapeutically effective regimen of a single intramuscular injection of a depot formulation comprising 40 mg dose of glatiramer acetate (GA) every 2 to 6 weeks.
• RRMS relapsing-remitting multiple sclerosis
• the regimen is sufficient to ameliorate (a) the frequency of relapses, (b) the number or volume of enhancing lesions, (c) the number of new lesions, or (d) the Expanded Disability Status Scale (EDSS) score of the patient.
• EDSS Expanded Disability Status Scale
• the regimen is sufficient to ameliorate the frequency of relapses, the number or volume of enhancing lesions, the number of new lesions, and the Expanded Disability Status Scale (EDSS) score of the patient.
• EDSS Expanded Disability Status Scale
• the present invention further provides, in another aspect, a method of preventing disease activity in a human patient suffering from relapsing-remitting multiple sclerosis, comprising administering to the patient a therapeutically effective regimen of a single injection of a depot formulation of a 40 mg dose of GA every 2 to 6 weeks, the regimen being sufficient to prevent relapses, 12-week confirmed disability progression (CDP), new lesion formation and enhancement of existing lesions in the patient.
• preventing RRMS activity comprises achieving No Evidence of Disease Activity (NED A).
• the present invention further provides, in another aspect, a kit, comprising a first container comprising GA or any other pharmaceutically acceptable salt of glatiramer encapsulated with a poly(lactic-co-glycolic acid) (PLGA), and a second separate container comprising a pharmaceutically acceptable diluent for injection.
• the kit comprises 40 mg GA and 2 mL WFI.
• the kit further comprises a syringe and a needle.
• mixing the content of the first container and the second container provides 40 mg GA per 2 mL of diluent.
• the kit is for use in a method of alleviating at least one symptom of relapsing- remitting multiple sclerosis (RRMS), increasing the tolerability of GA treatment, preventing or slowing progression of RRMS, or preventing RRMS activity.
• the kit is for use in a method of alleviating at least one symptom of relapsing-remitting multiple sclerosis (RRMS), increasing the tolerability of GA treatment, preventing or slowing progression of RRMS, or preventing RRMS activity, the method comprising a single intramuscular injection of a depot formulation comprising 40 mg dose of glatiramer acetate (GA) every 2 to 6 weeks.
• GA Depots are administered in 21G or 20G needles.
• the therapeutically effective dose of glatiramer acetate is 40 mg.
• the therapeutically effective amount of the glatiramer corresponds to ranges from about 1 mg to about 2 mg/day.
• such therapeutically effective amount of the glatiramer corresponds to about 1.5 mg/day.
• the dosing regimen ranges from once a week, twice monthly (approximately once in every 2 weeks) to once monthly.
• each depot or implantable device of the present invention will typically contain between about 20 and 750 mg of the active ingredient, designed to be released over a period ranging from a couple of weeks to a number of months.
• the pharmaceutical composition is in the form of a sterile solution.
• the pharmaceutical composition further comprises mannitol.
• the pharmaceutical composition has a pH in the range of 5.5 to 8.5.
• the pharmaceutical composition has a pH in the range of 5.5 to 7.0.
• the present invention provides, in one aspect, a depot formulation comprising 40 mg dose of glatiramer acetate (GA) for use in a method of alleviating at least one symptom of relapsing- remitting multiple sclerosis (RRMS) in a human patient suffering from RRMS or a human patient who has experienced a first clinical episode and is determined to be at high risk of developing clinically definite multiple sclerosis.
• GA glatiramer acetate
• the depot formulation is administered to the patient in a therapeutically effective regimen of a single intramuscular injection of the depot formulation every 2 to 6 weeks, the regimen being sufficient to alleviate the at least one symptom of the patient, wherein the symptom is selected from the group consisting of the frequency of relapses, the number of enhancing lesions or the number of new lesions images of brain MRI, and the Expanded Disability Status Scale (EDSS) score of the patient
• the depot formulation is administered once every 3 to 5 weeks.
• the depot formulation is administered once every 4 weeks.
• alleviating a symptom comprises reducing the frequency of relapses. According to any one of the above embodiments, alleviating a symptom comprises reducing the number or volume of enhancing lesions or the number of new lesions in the brain. According to any one of the above embodiments, alleviating a symptom comprises reducing brain atrophy, reducing the number or volume of Gd-enhancing lesions, reducing the number or volume of Tl -weighted enhancing lesions, or reducing the number of new T2- weighted lesions, in the patient. According to any one of the above embodiments, alleviating a symptom comprises reducing the EDSS score of the patient.
• the method alleviates the symptom at least as effectively as daily subcutaneous administrations of 20 mg GA or thrice weekly subcutaneous injections of 40 mg GA.
• the patient has received GA therapy prior to initiation of the regimen.
• the depot formulation further comprises a pharmaceutically acceptable biodegradable carrier selected from the group consisting of poly(lactic-co-glycolic acid) (PLGA), poly(lactic acid) (PLA), poly(glycolic acid) (PGA), and any combination thereof.
• a pharmaceutically acceptable biodegradable carrier selected from the group consisting of poly(lactic-co-glycolic acid) (PLGA), poly(lactic acid) (PLA), poly(glycolic acid) (PGA), and any combination thereof.
• the biodegradable carrier is PLGA.
• depot formulation is in the form of microparticles comprising an internal aqueous phase comprising the GA, a water immiscible polymeric phase comprising a biodegradable or non-biodegradable polymer, and an external aqueous phase.
• depot formulation is in the microparticles prepared by a water-in oil-in water (w/o/w) double emulsification process.
• the internal aqueous phase comprises the GA.
• the water immiscible polymeric phase comprises PLGA.
• the external water phase comprises a surfactant selected from poly(vinyl alcohol) (PVA), polysorbate, polyethylene oxide-polypropylene oxide block copolymers and cellulose esters.
• PVA poly(vinyl alcohol)
• PVP poly(vinyl alcohol)
• polysorbate polyethylene oxide-polypropylene oxide block copolymers
• cellulose esters a surfactant selected from poly(vinyl alcohol) (PVA), polysorbate, polyethylene oxide-polypropylene oxide block copolymers and cellulose esters.
• the depot formulation comprises 20% to 30% solids.
• the weight ratio between the GA and the pharmaceutically acceptable biodegradable carrier is between 1 : 1 to 1 : 100.
• the GA and the pharmaceutically acceptable biodegradable carrier is between 1 :5 to 1:25.
• the GA and the pharmaceutically acceptable biodegradable carrier is about 11.
• the depot formulation provides prolonged release or prolonged action of glatiramer in a subject as compared to a substantially similar dose of an immediate release formulation of glatiramer.
• about 80% of the glatiramer is released from the depot formulation within 22 days in PBS at 37°C under continuous agitation.
• about 20% of the glatiramer is released from the depot formulation within 5 days in PBS at 37°C under continuous agitation.
• the present invention provides, in another aspect, a therapeutically effective regimen of a single intramuscular injection of a depot formulation of a 40 mg dose of GA every 2 to 6 weeks, for use in a method of increasing the tolerability of GA treatment in a human patient suffering from relapsing-remitting multiple sclerosis.
• the method comprises reducing the frequency of subcutaneous injections from daily subcutaneous injections of a 20 mg dose of GA or three subcutaneous injections of a 40 mg dose of GA over a period of seven days with at least one day between every injection, to a therapeutically effective regimen of a single intramuscular injection of a depot formulation of a 40 mg dose of GA every 2 to 6 weeks
• the present invention provides, in another aspect, a depot formulation comprising 40 mg dose of glatiramer acetate (GA), for use in a method of preventing or slowing progression of relapsing- remitting multiple sclerosis (RRMS) in a human patient suffering from RRMS.
• the method comprises administering to the human patient a therapeutically effective regimen of a single intramuscular injection of the depot formulation every 2 to 6 weeks
• the method is sufficient to ameliorate (a) the frequency of relapses, (b) the number or volume of enhancing lesions, (c) the number of new lesions, or (d) the Expanded Disability Status Scale (EDSS) score of the patient.
• EDSS Expanded Disability Status Scale
• the method is sufficient to ameliorate the frequency of relapses, the number or volume of enhancing lesions, the number of new lesions, and the Expanded Disability Status Scale (EDSS) score of the patient.
• EDSS Expanded Disability Status Scale
• the present invention provides, in another aspect, a depot formulation of a 40 mg dose of GA, for use in a method of preventing disease activity in a human patient suffering from relapsing- remitting multiple sclerosis.
• the method comprises administering to the patient a therapeutically effective regimen of a single injection of the depot formulation every 2 to 6 weeks, the regimen being sufficient to prevent relapses, 12-week confirmed disability progression (CDP), new lesion formation and enhancement of existing lesions in the patient.
• a therapeutically effective regimen of a single injection of the depot formulation every 2 to 6 weeks, the regimen being sufficient to prevent relapses, 12-week confirmed disability progression (CDP), new lesion formation and enhancement of existing lesions in the patient.
• the present invention provides, in another aspect, a kit, comprising a first container comprising GA encapsulated with a poly(lactic-co-glycolic acid) (PLGA), and a second separate container comprising a pharmaceutically acceptable diluent for injection.
• a kit comprising a first container comprising GA encapsulated with a poly(lactic-co-glycolic acid) (PLGA), and a second separate container comprising a pharmaceutically acceptable diluent for injection.
• PLGA poly(lactic-co-glycolic acid)
• the kit comprises 40 mg GA and 2 mL water for injection (WFI).
• the content of the first container and the second container provides 40 mg GA per 2 mL of diluent.
• the kit is for use in a method of alleviating at least one symptom of relapsing-remitting multiple sclerosis (RRMS), increasing the tolerability of GA treatment, preventing or slowing progression of RRMS, or preventing RRMS activity.
• RRMS relapsing-remitting multiple sclerosis
• Example 1 Preparation method of Depot of 40 mg GA in-vitro.
• External water phase preparation Partially hydrolyzed poly(vinyl alcohol) (PVA) solution at a concentration of 2% w/w in sterile WFI was prepared in a reactor and filtered through a 0.22 ⁇ membrane.
• PVA poly(vinyl alcohol)
• a solution of NaCl in sterile WFI was prepared and filtered through a 0.22 ⁇ membrane into the reactor containing the PVA.
• Organic phase preparation Organic phase composed of dichloromethane and poly(lactide-co-glycolide) was prepared in a reactor and filtered through a 0.22 ⁇ membrane.
• Internal water phase preparation A solution containing sterile WFI and glatiramer acetate was prepared and filtered through a 0.22 ⁇ membrane.
• Water-in-oil (w/o) emulsion preparation Internal water phase was added to the organic phase and processed using IKA Ultra-Turrax T50 homogenizer equipped with a rotor stator dispersion device at 7,200 RPM for 10 minutes (high shear mixing).
• Water-in-oil-in-water (w/o/w) emulsion preparation Water in oil emulsion (w/o) prepared in step 5 was added to half of the external water phase during continuing mixing of the w/o emulsion.
• the w/o/w double emulsion was processed using IKA Ultra-Turrax UTS80 homogenizer with a rotor stator head at 2,900 RPM for 3 minutes from the end of w/o transfer into the external water phase. Following, another 30 liters of the external water phase was added to the emulsion (quench). (7) Solvent removal/evaporation: The w/o/w double emulsion formed in step (6) was mixed using the IKA UTS80 homogenizer at different speeds for 15-17 hours. Compressed air was bubbled at 0.5 Pa through the emulsion for 10-12 hours. Vacuum was applied for the portion of the process. (8) Separation and washing: The suspension was centrifuged at 5,300 RPM for 10 minutes.
• the release of the incorporated glatiramer acetate was carried out in tightly closed 20 ml glass vials, using incubator at 37°C, equipped with a multi -point magnetic stirrer. Phosphate buffered saline (PBS) with pH 7.4 was used as a release media.
• PBS Phosphate buffered saline
• Table 1 summarizes the release profile of GA from a PLGA Depot.
• Example 3 Depot of 4 mg GA vs. commercially available GA (COPAXONE ® ) m-vivo. Material and Methods
• EAE Complete Freund's adjuvant
• Body weight was measured every two days from day 0 to day 28. EAE was assessed by clinical scoring of the mice once daily from Day 0 to Day 28 post immunization (table 2). For analysis, dead animals received clinical score of 5 and the weight recorded at the last measurement before animal death. Table 2: EAE clinical Score.
• GA Depot Glatiramer Acetate Depot was suspended in water for injection (WFI) and immediately injected intramuscularly (IM) at the indicated dose. Dose of GA Depot are given according to amount of active ingredient (i.e. GA Depot 4 mg contains 4 mg GA).
• ELISA plates were prepared as following: flat bottom ELISA plates (Nunc) were coated with lOOul of 50 ⁇ GA in borate buffer (BB) 0.17M pH 8.0 overnight at 4° C. Wells were emptied and washed with phosphate buffer saline (PBS) containing 0.05% Tween 20 at room temperature. Following the washing 1% BSA was applied for 2 hours at room temperature (RT), for blocking of non-specific binding sites. Subsequently, wells were washed three times with wash solution.
• PBS phosphate buffer saline
• ELISA test was performed as follows: 100 ⁇ of sera samples were diluted 1 : 1,000 added to wells for 18 hours at 4°C (sera dilution was performed using PBS containing 1% BSA and 0.05% Tween 20), followed by three washes with phosphate buffer saline (PBS) containing 0.05% Tween 20 at room temperature. Subsequently, 100 ⁇ 1 :50,000 diluted alkaline phosphatase conjugated AffinityPure Goat anti-mouse IgG+IgM (H+L) (Jackson Laboratories) was added to the wells and incubated for 2 hours at RT.
• PBS phosphate buffer saline
• Binding Index mean optical density of tested serum/ mean optical density of control serum.
• the mean value for normal mice serum was 0.230 OD and the cut off values for Binding Index is 2.0 ⁇ 1.0. Thus, values above 3.0 were considered as positive.
• Figure 1 shows mean clinical score results for saline control (black sphere marker), 2 mg COPAXONE ® (black square marker) and GA Depot 4 mg (gray triangle marker) groups, as those groups represent the range of the proposed human dose (using an allometric 1 : 10 scale, as deducted from previous studies) of 0, 20 and 40 mg, respectively.
• *P ⁇ 0.05 for all treatment groups compared with untreated control Single Factor ANOVA followed by one -tailed T Test assuming unequal variance.
• N 20 / group, +/- standard error.
• Mean clinical score AUC area under curve), mean day of onset and mean disease duration were significantly reduced in the GA Depot group and in the COPAXONE ® group compared with untreated control (Table 4, p ⁇ 0.05).
• this experiment shows that intramuscular administration of the GA Depot induced a humoral response of anti-GA antibodies, at similar levels as with standard daily subcutaneous injection of GA (see Table 5). Therefore, the similar humoral responses to GA Depot as compared to standard GA injections might represent a similarity in the immunologic response to the GA Depot. This may therefore indicate also equivalent clinical immuno -modulatory therapeutic effects, as can be seen in this EAE study of which the AUC between COPAXONE ® and GA Depot are not different in statistical significant manner (see Table 4). Therefore, the existence of anti-GA antibodies can serve as a biomarker to the therapeutic bio -availability of the drug, when with a new formulation and administered via a new route.
• Inclusion Criteria Male or female subjects with a diagnosis of RRMS; diagnosis of multiple sclerosis (MS) consistent with the McDonald Criteria (revisions of 2010); treatment with 20 mg or 40 mg of GA (COPAXONE) during the previous 12 months with ongoing treatment at the Screening Visit; normal renal function; normal liver function; normal hemoglobin concentration; absence of any clinically significant medical, psychiatric or laboratory abnormalities; ability to provide written informed consent.
• Exclusion Criteria Any relevant medical, surgical, or psychiatric condition, laboratory value, or concomitant medication which, in the opinion of the investigator, makes the subject unsuitable for study entry or potentially unable to complete all aspects of the study; Severe anemia (hemoglobin ⁇ 10 g/dL); abnormal renal function (serum creatinine > 1.5xULN); pregnant or breastfeeding women; women capable of child bearing must have a negative urine pregnancy test at screening visit and use an adequate contraceptive method throughout the study. Women who are surgically sterile (hysterectomy or tubal ligation) or whose last menstruation was 12 months or more prior to the Screening Visit are considered to be of non-child-bearing potential.
• Acceptable forms of contraception include oral, implanted, or injected contraceptives; intrauterine devices in place for at least 3 months; estrogen patch; and adequate barrier methods in conjunction with spermicide. Abstinence is considered an acceptable contraceptive regimen; history of any anaphylactic reaction and/or serious allergic reaction following a vaccination, a proven hypersensitivity to any component of the study drug, e.g.
• GA poly(lactic-co-glycolic acid)
• PVA poly(vinyl alcohol)
• known or suspected history of drug or alcohol abuse positive test for HIV, hepatitis, venereal disease research laboratory test (VDRL), or tuberculosis
• participation in an investigational drug study within 30 days prior to start of this study treatment with any kind of steroids during the last 30 days; confirmed relapse during the last 30 days.
• AEs Adverse events
• ISRs injection site reactions
• Endpoint #1 Relapse rate compared to relapse rate observed in the 12 months prior to study entry. During the study: 1 relapse (which did not include changes in EDSS) detected for the entire study population. Same subjects during one year prior to the trial, while treated with COPAXONE ® : 2 relapses.
• Endpoint #2 Brain MRI scans compared to baseline, change defined as either new lesions (by T2 -FLAIR), change in enhancing lesions (by SPGR Tl GdE), or both.
• One 80 mg patient showed 7 new enhancing lesions at 6 months MRI scan; ** One 40 mg patient showed a reduction of enhancing lesions from 3 at baseline to 0 at 6 months; considered as "no change"; *** One 40 mg patient showed 1 new enhancing lesion at early termination MRI scan; * One 80 mg patient showed 2 new enhancing lesions at 12 months MRI scan; ⁇ One 80 mg patient diagnosed with breast cancer did not performed MRI scans at early termination.
• Endpoint #3 EDSS Score.
• Table 7 EDSS scores.
• Treatment with a single intramuscular injection of 40 mg GA depot was superior to a corresponding treatment with 80 mg GA in preventing formation of new lesions and enhancement of lesions (Table 6). Treatment with a single intramuscular injection of 40 mg GA depot was comparable to a corresponding treatment with 80 mg GA in preventing an increased EDSS score (Table 7).

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