EP2928462A2 - Procédés d'administration de compositions comprenant de l'acide docosapentaénoïque - Google Patents

Procédés d'administration de compositions comprenant de l'acide docosapentaénoïque

Info

Publication number
EP2928462A2
EP2928462A2 EP13861305.4A EP13861305A EP2928462A2 EP 2928462 A2 EP2928462 A2 EP 2928462A2 EP 13861305 A EP13861305 A EP 13861305A EP 2928462 A2 EP2928462 A2 EP 2928462A2
Authority
EP
European Patent Office
Prior art keywords
alternatively
dpa
composition
dha
fatty acids
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Withdrawn
Application number
EP13861305.4A
Other languages
German (de)
English (en)
Other versions
EP2928462A4 (fr
Inventor
George Bobotas
Abdel Aziz FAWZY
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Matinas Biopharma Inc
Original Assignee
Matinas Biopharma Inc
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by Matinas Biopharma Inc filed Critical Matinas Biopharma Inc
Publication of EP2928462A2 publication Critical patent/EP2928462A2/fr
Publication of EP2928462A4 publication Critical patent/EP2928462A4/fr
Withdrawn legal-status Critical Current

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Classifications

    • AHUMAN NECESSITIES
    • A23FOODS OR FOODSTUFFS; TREATMENT THEREOF, NOT COVERED BY OTHER CLASSES
    • A23DEDIBLE OILS OR FATS, e.g. MARGARINES, SHORTENINGS, COOKING OILS
    • A23D9/00Other edible oils or fats, e.g. shortenings, cooking oils
    • A23D9/06Preservation of finished products
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/185Acids; Anhydrides, halides or salts thereof, e.g. sulfur acids, imidic, hydrazonic or hydroximic acids
    • A61K31/19Carboxylic acids, e.g. valproic acid
    • A61K31/20Carboxylic acids, e.g. valproic acid having a carboxyl group bound to a chain of seven or more carbon atoms, e.g. stearic, palmitic, arachidic acids
    • A61K31/202Carboxylic acids, e.g. valproic acid having a carboxyl group bound to a chain of seven or more carbon atoms, e.g. stearic, palmitic, arachidic acids having three or more double bonds, e.g. linolenic
    • AHUMAN NECESSITIES
    • A23FOODS OR FOODSTUFFS; TREATMENT THEREOF, NOT COVERED BY OTHER CLASSES
    • A23DEDIBLE OILS OR FATS, e.g. MARGARINES, SHORTENINGS, COOKING OILS
    • A23D9/00Other edible oils or fats, e.g. shortenings, cooking oils
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/33Heterocyclic compounds
    • A61K31/395Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
    • A61K31/40Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having five-membered rings with one nitrogen as the only ring hetero atom, e.g. sulpiride, succinimide, tolmetin, buflomedil
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/4816Wall or shell material
    • A61K9/4825Proteins, e.g. gelatin
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/4841Filling excipients; Inactive ingredients
    • A61K9/4858Organic compounds
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/4841Filling excipients; Inactive ingredients
    • A61K9/4875Compounds of unknown constitution, e.g. material from plants or animals
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P29/00Non-central analgesic, antipyretic or antiinflammatory agents, e.g. antirheumatic agents; Non-steroidal antiinflammatory drugs [NSAID]
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P3/00Drugs for disorders of the metabolism
    • A61P3/06Antihyperlipidemics
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P3/00Drugs for disorders of the metabolism
    • A61P3/08Drugs for disorders of the metabolism for glucose homeostasis
    • A61P3/10Drugs for disorders of the metabolism for glucose homeostasis for hyperglycaemia, e.g. antidiabetics
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • A61P9/10Drugs for disorders of the cardiovascular system for treating ischaemic or atherosclerotic diseases, e.g. antianginal drugs, coronary vasodilators, drugs for myocardial infarction, retinopathy, cerebrovascula insufficiency, renal arteriosclerosis
    • CCHEMISTRY; METALLURGY
    • C11ANIMAL OR VEGETABLE OILS, FATS, FATTY SUBSTANCES OR WAXES; FATTY ACIDS THEREFROM; DETERGENTS; CANDLES
    • C11BPRODUCING, e.g. BY PRESSING RAW MATERIALS OR BY EXTRACTION FROM WASTE MATERIALS, REFINING OR PRESERVING FATS, FATTY SUBSTANCES, e.g. LANOLIN, FATTY OILS OR WAXES; ESSENTIAL OILS; PERFUMES
    • C11B5/00Preserving by using additives, e.g. anti-oxidants
    • C11B5/0007Organic substances
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/06Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite
    • A61K47/22Heterocyclic compounds, e.g. ascorbic acid, tocopherol or pyrrolidones

Definitions

  • the present invention relates to a method comprising administration of docosapentaenoic acid compositions for the reduction of lipid parameters, such as triglycerides, total cholesterol, low density lipoprotein (LDL) cholesterol, non-HDL cholesterol, free fatty acids, and other lipids.
  • the present invention also relates to a method comprising administration of docosapentaenoic acid compositions for the increase of high density lipoprotein (HDL) cholesterol.
  • lipid parameters such as triglycerides, total cholesterol, low density lipoprotein (LDL) cholesterol, non-HDL cholesterol, free fatty acids, and other lipids.
  • LDL low density lipoprotein
  • HDL high density lipoprotein
  • the methods of the present invention may be useful for the treatment of a condition selected from the group consisting of: hypertriglyceridemia; hypercholesterolemia; mixed dyslipidemia; coronary heart disease (CHD); vascular disease; cardiovascular disease; acute coronary syndrome; atherosclerotic disease and related conditions; heart failure; cardiac arrhythmias; coagulatory conditions associated with cardiac arrhythmias; ischemic dementia; vascular dementia; hypertension; coagulation related disorders; nephropathy; kidney or urinary tract disease; retinopathy; cognitive and other CNS disorders; autoimmune diseases; inflammatory diseases; asthma or other respiratory disease; dermatological disease; metabolic syndrome; diabetes, diabetes mellitis or other form of metabolic disease; liver disease; non-alcoholic fatty liver disease; disease of the gastrointestinal tract; disease of the male or female reproductive system or related secondary sexual organs; a cancer of any type, including lymphomas and myelomas; an infection caused by a virus, bacterium, fungus, protozoa or other organism; and the treatment and/
  • cholesterol and triglycerides are part of lipoprotein complexes in the bloodstream, and can be separated via ultracentrifugation into high-density lipoprotein (HDL), intermediate-density lipoprotein (IDL), low-density lipoprotein (LDL) and very-low-density lipoprotein (VLDL) fractions.
  • HDL high-density lipoprotein
  • IDL intermediate-density lipoprotein
  • LDL low-density lipoprotein
  • VLDL very-low-density lipoprotein
  • Total-C total cholesterol
  • LDL-cholesterol LDL-cholesterol
  • apolipoprotein B a membrane complex for LDL-cholesterol and VLDL-cholesterol, as well as IDL- cholesterol in rare individuals suffering from a disorder resulting in significant IDL- cholesterol levels
  • hypercholesterolemia Decreased levels of HDL-cholesterol and its transport complex, apolipoprotein A, as well as elevated levels of apolipoprotein C-lll and serum triglycerides (TG) are also associated with the development of atherosclerosis.
  • cardiovascular morbidity and mortality in humans can vary directly with the level of total-C, LDL-cholesterol and TG and inversely with the level of HDL- cholesterol.
  • non-HDL-cholesterol is an important indicator of hypertriglyceridemia (elevated triglycerides), vascular disease, atherosclerotic disease and related conditions. Therefore, non-HDL- cholesterol and fasting TG reduction has also been specified as a treatment objective in NCEP ATP III.
  • Fasting TG is commonly used as a key measure for TG in lipid management, because it minimizes the confounding factor of TG recently absorbed from meals, including the high variability of the content of meals and high variability of post-meal (post-prandial) spikes in TG.
  • fasting TG levels when we refer to triglycerides or TG.
  • HMG-CoA reductase inhibitors (“statins") as the primary treatment option for hypercholesterolemia.
  • LDL-cholesterol is the primary treatment parameter.
  • Patients with hypercholesteremia or mixed dyslipidemia often present with high blood levels of LDL-cholesterol (i.e. greater than 190 mg/dl) and TG (i.e. levels of 200 mg/dl or higher).
  • the use of diet and single-drug therapy does not always decrease LDL- cholesterol and TG adequately enough to reach targeted values in patients with
  • AFDOCS/l 0582446.1 mixed dyslipidemia with or without a concomitant increase in triglycerides.
  • a combined therapy regimen of a statin and a second anti-dyslipidemic agent is often desired.
  • This second agent has historically been a fibrate (i.e. gemfibrozil, bezafibrate, or fenofibrate) or extended release niacin.
  • the use omega-3 fatty acid concentrates in combination with a statin has been growing rapidly due to concerns about the lack of outcome benefits with fibrates (i.e. the FIELD study) or extended release niacin (i.e. the AIM-HIGH study).
  • the use of omega-3 fatty acid concentrates has also grown versus fibrates and extended release niacin.
  • Marine oils also commonly referred to as fish oils, are a good source of the two main omega-3 fatty acids, eicosapentaenoic acid (EPA) and docosahexaenoic acid (DHA), which have been found to regulate lipid metabolism.
  • Omega-3 fatty acids have been found to have beneficial effects on the risk factors for cardiovascular diseases, especially mild hypertension, hypertriglyceridemia and on the coagulation factor VII phospholipid complex activity.
  • Omega-3 fatty acids lower serum triglycerides (TG), increase serum HDL-cholesterol, lower systolic and diastolic blood pressure and the pulse rate, and lower the activity of the blood coagulation factor Vll-phospholipid complex.
  • omega-3 fatty acids seem to be well tolerated, without giving rise to any severe side effects.
  • omega-3 fatty acids is a concentrate of omega-3, long chain, polyunsaturated fatty acids from fish oil containing DHA ethyl esters, EPA ethyl esters as well as ethyl esters of other omega-3 fatty acids (described in USP35 for LOVAZA®) and is sold under the trademarks OMACOR® and LOVAZA®.
  • omega-3 fatty acid comprises at least 90% omega-3 fatty acids of which at least 80% EPA+DHA (in a ratio of 1 .2:1 ) and is described, for example, in U.S. Pat. Nos... 5,502,077, 5,656,667 and 5,698,594.
  • LOVAZA® (omega-3-acid ethyl esters) is indicated for the treatment of patients with hypertriglyceridemia with TG levels of 500mg/dl_ or higher.
  • EPADEL® omega-3 fatty acid concentrate
  • This product is described as 98% EPA ethyl ester in Lancet (Vol.369; March 31 , 2007; 1090-1098) reporting on a large outcome study with EPADEL®.
  • EPADEL® is known to contain less than 1 % of any fatty acid other than EPA.
  • omega-3 fatty acid concentrate also consists almost entirely of EPA ethyl ester and is known under its developmental stage name AMR101 or its trade name VASCEPA®.
  • AMR101 is described in US patent application 2010/0278879 as comprising at least 95% EPA (typically referred to as 97% or at least 96% in company releases and references) and less than 1 % of any other fatty acid.
  • AMR101 was previously under development for the treatment of Huntingdon's Disease but failed in phase III clinical development. Subsequently, AMR101 was entered in a development program for hypertriglyceridemia and mixed dyslipidemia.
  • EPANOVATM omega-3, long chain, polyunsaturated fatty acids from fish oil containing approximately 75% DHA and EPA as free fatty acids. This product is described as comprising approximately 55% EPA and 20% DHA. EPANOVATM was previously under development for the treatment of Crohn's Disease but failed in phase III clinical development. Subsequently, EPANOVATM was entered in a development program for hypertriglyceridemia and mixed dyslipidemia.
  • omega-3 fatty acid compositions are dose dependent, i.e., the higher the dose, the greater the therapeutic affect and bioavailability.
  • the effect of each specific omega-3 fatty acid composition may be different, and therefore the level of therapeutic effect of one
  • AFDOCS/l 0582446.1 composition at a given dose cannot necessarily be inferred from the level of therapeutic effects of other omega-3 fatty acid compositions at the same or similar dose.
  • Non-HDL-C -10.2 p ⁇ 0.05 -17.7 p ⁇ 0.0001 -8.1 p .0182
  • VLDL-C -20.3 p ⁇ 0.05 -24.4 p ⁇ 0.0001 -10.5 p 0.0093
  • Non-HDL-C -6.8 p ⁇ 0.0001 -13.6 p ⁇ 0.0001 -5.5 p 0.0054
  • LOVAZA® Under low fat meal conditions, LOVAZA® has only 15% AUC and 12% Cmax of the bioavailability versus LOVAZA® under high fat meal conditions, whereas EPANOVATM under low fat meal conditions has 78% AUC and 53% Cmax of the bioavailability versus LOVAZA® under high fat meal conditions. EPANOVATM under low fat meal conditions has 62% AUC and 46% Cmax of the bioavailability versus EPANOVATM under high fat meal conditions.
  • Omega-3 fatty acids are known to be "essential fatty acids".
  • EFAs essential fatty acids
  • the main EFAs in the diet are linoleic acid of the omega-6 series and alpha-linolenic acid of the omega-3 series.
  • these "parent" EFAs must be metabolised to the other longer chain fatty acids.
  • Each fatty acid probably has a specific role in the body.
  • the scientific literature suggests that particularly important in the n-6 series are dihomo-
  • DGLA gammalinolenic acid
  • ARA arachidonic acid
  • EPA eicosapentaenoic acid
  • DHA docosahexaenoic acid
  • U.S. Patent No. 6,479,544 describes an invention in which it is found that ARA is highly desirable rather than undesirable and it may be helpful to administer ARA in association with EPA.
  • This invention provides pharmaceutical formulations containing eicosapentaenoic acid or any appropriate derivative (hereinafter collectively referred to as EPA) and arachidonic acid (ARA), as set out in the granted claims for this patent.
  • EPA eicosapentaenoic acid or any appropriate derivative
  • ARA arachidonic acid
  • ARA may be replaced by one or more of its precursors, DGLA or GLA.
  • the ratio of EPA to ARA is preferably between 1 :1 and 20:1 .
  • Patent application PCT/GB 2004/000242 describes the treatment or prevention of psoriasis with a formulation comprising more than 95% EPA and less than 2% DHA.
  • the EPA is replaced with DPA.
  • Patent application PCT/NL 2006/050291 (WO/2007/058538, GB 0301701 .9) describes combinations of idigestible oligosaccharides and long chain polyunsaturated fatty acids such as ARA, EPA, DA, and combinations thereof to improve intestinal barrier integrity, improving barrier function, stimulating gut maturation and/or reducing intestinal barrier permeability.
  • Holub et al. discloses a study assessing the effect of oral supplementation with docosapentaenoic acid (DPA) on levels of serum and tissue lipid classes and their fatty acid compositions in rat liver, heart, and kidney
  • DPA docosapentaenoic acid
  • omega-3 fatty acid concentrates Given the highly beneficial efficacy and side-effect profile of omega-3 fatty acid concentrates, these compositions are increasingly popular for the treatment of patients with dyslipidemias. However, with the increased popularity of omega-3 fatty acid concentrates, there is an unmet medical need for omega-3 fatty acid containing compositions with improved bioavailability and a more optimal ratio of potency in reducing TG versus the resulting cholesterol profile. Specifically, agents with both a
  • Fasting triglyceride levels have been found to be correlated with the risk of cardiovascular diseases and conditions. For example, high fasting triglycerides levels have been associated with an increased risk of myocardial infarction. Gaziano et al. (Circulation, 1997; 96:2520-2525) discusses fasting triglyceride levels as a risk factor for coronary heart disease. Love-Osborne et al. (Pediatr Diabetes, 2006: 7:205-210) discloses the role of elevated fasting triglyceride levels in the development of type 2 diabetes mellitus.
  • the present invention provides a method of reducing lipid parameters, such as triglyceride levels, in a subject in need thereof, comprising administering to the subject a composition comprising docosapentaenoic acid (DPA) in an amount of at least about 20 mg/day, alternatively at least about 30 mg/day, alternatively at least about 40 mg/day, alternatively at least about 50 mg/day, alternatively at least about 60 mg/day alternatively, at least about 70 mg/day alternatively at least about 75 mg/day, alternatively at least about 80 mg/day, alternatively at least about 90 mg/day, alternatively at least about 100 mg/day, alternatively at least about 120 mg/day, alternatively at least about 150 mg/day, alternatively at least about 200 mg/day, alternatively at least about 300 mg/day, or alternatively at least about 400 mg/day.
  • DPA docosapentaenoic acid
  • the present invention also provides a method of reducing triglyceride levels in a subject in need thereof, comprising administering to the subject a composition comprising at least about 45% docosapentaenoic acid (DPA) relative to the total amount of fatty acids present in the composition.
  • DPA docosapentaenoic acid
  • the composition comprises at least about 45% or at least about 50% or at least about 55% or at least about 60% or at least about 65% or at least about 70% or at least about 75% or at least about 80% or at least about 85% or at least about 90% or at least about 95% of DPA.
  • the present invention also provides a method of reducing triglyceride levels in a subject in need thereof, comprising administering to the subject a composition comprising no more than about 20% docosahexaenoic acid
  • the composition comprises no more than about 15% or no more than about 12% or no more than about 10% or no more than about 8% or no more than about 7%, no more than about 6%, no more than about 5%, no more than about 4%, no more than about 3%, no more than about 2%, or no more than about 1 % DHA relative to the total amount of fatty acids present in the composition.
  • the present invention also provides a method of reducing triglyceride levels in a subject in need thereof, comprising administering to the subject a composition comprising docosapentaenoic acid (DPA) in a significant or higher relative amount as compared to docosahexaenoic acid (DHA) such that the DPA:DHA ratio in the composition is 1 :2 or greater.
  • DPA docosapentaenoic acid
  • DHA docosahexaenoic acid
  • the ratio of DPA:DHA in the composition is at least 1 :1 , or at least 2:1 or at least 3:1 , or at least 4:1 or at least 5:1 .
  • the present invention also provides a method of reducing other lipid parameters, such as total cholesterol, low density lipoprotein cholesterol, non-HDL cholesterol, and free fatty acids, in a subject in need thereof, comprising administering to the subject an orally administrable composition comprising docosapentaenoic acid (DPA) in an amount of at least about 20 mg/day, alternatively at least about 30 mg/day, alternatively at least about 40 mg/day, alternatively at least about 50 mg/day, alternatively at least about 60 mg/day alternatively, at least about 70 mg/day alternatively at least about 75 mg/day, alternatively at least about 80 mg/day, alternatively at least about 90 mg/day, alternatively at least about 100 mg/day, alternatively at least about 120 mg/day, alternatively at least about 150 mg/day, alternatively at least about 200 mg/day, alternatively at least about 300 mg/day, or alternatively at least about about 400 mg/day.
  • DPA docosapentaenoic acid
  • the present invention also provides a method of reducing other lipid parameters, such as total cholesterol, non-HDL cholesterol, low density lipoprotein cholesterol, and free fatty acids in a subject in need thereof, comprising administering to the subject a composition comprising at least about 45% docosapentaenoic acid (DPA) relative to the total amount of fatty acids present in the composition.
  • DPA docosapentaenoic acid
  • the composition comprises at least about 45% or at least about 50% or at least about 55% or at least about 60% or at least about 65% or at least about 70% or at least about 75% or at least about 80% or at least about 85% or at least about 90% or at least about 95% of DPA.
  • AFDOCS/l 0582446.1 invention also provides a method of reducing other lipid parameters in a subject in need thereof, comprising administering to the subject a composition comprising no more than about 20% docosahexaenoic acid (DHA) relative to the total amount of fatty acids present in the composition.
  • DHA docosahexaenoic acid
  • the composition comprises no more than about 15% or no more than about 12% or no more than about 10% or no more than about 8% or no more than about 7%, no more than about 6%, no more than about 5%, no more than about 4%, no more than about 3%, no more than about 2%, or no more than about 1 % DHA relative to the total amount of fatty acids present in the composition.
  • the present invention also provides a method of reducing other lipid parameters, such as total cholesterol, non-HDL cholesterol, low density lipoprotein cholesterol, and free fatty acids in a subject in need therefore, comprising administering to the subject a composition comprising docosapentaenoic acid (DPA) in a significant or higher relative amount as compared to docosahexaenoic acid (DHA) such that the DPA:DHA ratio in the composition is 1 :2 or greater.
  • the ratio of DPA:DHA in the composition is at least 1 :1 , or at least 2:1 or at least 3:1 , or at least 4:1 or at least 5:1 .
  • the methods may relate to lipid parameters measured in a fasted state, or in a fed state.
  • FIG. 1 shows the fasting plasma lipid values after seven days of dosing, relating to the study described in Example 33.
  • FIG. 2 shows the fasting plasma insulin levels after 28 days of administration, relating to the study described in Example 33.
  • FIG. 3 shows the relative liver gene expression following 28 days of administration, relating to the study described in Example 33.
  • the present invention provides a method of reducing lipid levels in a subject, preferably a human subject, comprising administration of docosapentaenoic acid (DPA).
  • DPA docosapentaenoic acid
  • the lipids include, but are not limited to, triglycerides, total cholesterol, low density (LDL) lipoprotein, free fatty acids, and other lipoproteins that are not high- density lipoprotein (non-HDL).
  • the present invention provides a method of
  • AFDOCS/l 0582446.1 increasing high-density lipoprotein (HDL) cholesterol in a subject, preferably a human subject, comprising administration of docosapentaenoic acid (DPA).
  • DPA docosapentaenoic acid
  • Fasting lipid levels refer to levels of the lipids in the plasma of a subject after a fasting period, which is a period of 8 to 12 hours without food.
  • the baseline fasting triglyceride level in the subject prior to administration of DPA is greater than 150 mg/dL. In some embodiments, the baseline fasting triglyceride level is 150 mg/dL to 199 mg/dl, alternatively 200-499 mg/dL, alternatively over 500 mg/dL.
  • the DPA may be administered in an orally administrable composition comprising DPA.
  • the compositions comprise DPA in an amount between 1 % and 99% relative to the total amount of fatty acids present in the composition, alternatively between 1 % and 95%, alternatively between 1 % and 90%, alternatively between 1 % and 85%, alternatively between 1 % and 80%, alternatively between 1 % and 75%, alternatively between 1 % and 70%, alternatively between 1 % and 65%, alternatively between 1 % and 60%, alternatively between 1 % and 55%, alternatively between 1 % and 50%, alternatively between 1 % and 45%, alternatively between 1 % and 40%, alternatively between 1 % and 35%, alternatively between 1 % and 30%, alternatively between 1 % and 25%, alternatively between 1 % and 20%, alternatively between 1 % and 15%, alternatively between 1 % and 10%, alternatively between 1 % and 5%, alternatively between 2% and 99%, alternatively between 2% and 95%
  • AFDOCS/l 0582446.1 alternatively between 3% and 65%, alternatively between 3% and 60%, alternatively between 3% and 55%, alternatively between 3% and 50%, alternatively between 3% and 45%, alternatively between 3% and 40%, alternatively between 3% and 35%, alternatively between 3% and 30%, alternatively between 3% and 25%, alternatively between 3% and 20%, alternatively between 3% and 15%, alternatively between 3% and 10%, alternatively between 3% and 5%, alternatively between 4% and 99%, alternatively between 4% and 95%, alternatively between 4% and 90%, alternatively between 4% and 85%, alternatively between 4% and 80%, alternatively between 4% and 75%, alternatively between 4% and 70%, alternatively between 4% and 65%, alternatively between 4% and 60%, alternatively between 4% and 55%, alternatively between 4% and 50%, alternatively between 4% and 45%, alternatively between 4% and 40%, alternatively between 4% and 35%, alternatively between 4% and 30%, alternatively between 4%
  • AFDOCS/l 0582446.1 alternatively between 6% and 12%, alternatively between 6% and 1 1 %, alternatively between 6% and 10%, alternatively between 7% and 99%, alternatively between 7% and 95%, alternatively between 7% and 90%, alternatively between 7% and 85%, alternatively between 7% and 80%, alternatively between 7% and 75%, alternatively between 7% and 70%, alternatively between 7% and 65%, alternatively between 7% and 60%, alternatively between 7% and 55%, alternatively between 7% and 50%, alternatively between 7% and 45%, alternatively between 7% and 40%, alternatively between 7% and 35%, alternatively between 7% and 30%, alternatively between 7% and 25%, alternatively between 7% and 20%, alternatively between 7% and 15%, alternatively between 7% and 12%, alternatively between 7% and 1 1 %, alternatively between 7% and 10%, alternatively between 8% and 99%, alternatively between 8% and 95%, alternatively between 8% and 90%, alternatively between 8% and 85%
  • compositions comprise DPA in an amount of at least about 45% of DPA. In some alternative embodiments, the composition comprises at least 45% or at least 50% or at least 55% or at least 60% or at least 65% or at least 70% or at least 75% or at least 80% or at least 85% or at
  • the composition comprises at least 20 mg of DPA, alternatively at least 30 mg, alternatively at least 40 mg, alternatively at least 50 mg, alternatively at least 60 mg, alternatively at least 90 mg, alternatively at least 100 mg, alternatively at least 120 mg, alternatively at least 150 mg, alternatively at least 200 mg, alternatively at least 300mg, alternatively at least 400 mg of DPA.
  • the composition comprises DPA in ester form or in free fatty acid form.
  • the compositions comprise docosapentaenoic acid (DPA) in a significant or higher relative amount as compared to docosahexaenoic acid (DHA) such that the DPA:DHA ratio in the composition is 1 :2 or greater.
  • DPA docosapentaenoic acid
  • DHA docosahexaenoic acid
  • the ratio of DPA:DHA in the composition is at least 1 :1 , or at least 2:1 or at least 3:1 , or at least 4:1 or at least 5:1 .
  • the methods of treatment provides a dose of at least 20 mg DPA-N3, alternatively at least 30 mg DPA-N3, alternatively at least 40 mg DPA-N3, alternatively at least 50 mg DPA-N3, alternatively at least 60mg DPA-N3 per day, alternatively at least 70mg DPA-N3 per day, alternatively at least 75mg DPA-N3 per day, alternatively at least 80mg DPA-N3 per day, alternatively at least 90mg DPA-N3 per day, alternatively at least 100mg DPA-N3 per day, alternatively at least 120mg DPA-N3 per day, alternatively at least 150mg DPA-N3 per day, alternatively at least 160mg DPA-N3 per day, alternatively at least 180mg DPA-N3 per day, alternatively at least 200mg DPA-N3 per day, alternatively at least 250mg DPA-N3 per day, alternatively at least 300mg DPA-N3 per day, alternatively at least 350mg D
  • the method of treatment provides a daily dose of at least about at least 20 mg of DPA, alternatively at least 30 mg, alternatively at least 40 mg, alternatively at least 50 mg, alternatively at least 60 mg, alternatively at least 90 mg, alternatively at least 100 mg, alternatively at least 120 mg, alternatively at least 150 mg, alternatively at least 200 mg, alternatively at least 300mg, alternatively at least 400 mg of DPA.
  • the method of treatment provides a daily dose of at least about 1 ,000 mg DPA-N3 per day, alternatively at least about 1 ,500 mg DPA-N3 per day, alternatively at least about 2,000 mg DPA-N3 per day, alternatively at least about 2,500 mg DPA-N3 per day, alternatively at least about 3,000 mg DPA-N3 per day, alternatively at least about
  • AFDOCS/l 0582446.1 3,500 mg DPA-N3 per day, alternatively at least about 3,750 mg DPA-N3 per day, alternatively at least about 4,000 mg DPA-N3 per day, alternatively at least about 4,250 mg DPA-N3 per day.
  • the method of treatment provides a dose of at least about 1 mg/kg of DPA-N3 per day, alternatively about 2 mg/kg of DPA-N3 per day, alternatively about 3 mg/kg of DPA-N3 per day, alternatively about 4 mg/kg of DPA- N3 per day, alternatively about 6 mg/kg of DPA-N3 per day, alternatively about 8 mg/kg of DPA-N3 per day, alternatively about 10 mg/kg of DPA-N3 per day, alternatively about 20 mg/kg of DPA-N3 per day, alternatively about 30 mg/kg of DPA-N3 per day, and alternatively about 40 mg/kg alternatively about 50 mg/kg of DPA-N3 per day, alternatively about 75 mg/kg of DPA-N3 per day, and alternatively about 100 mg/kg.
  • the present invention provides an administrable composition comprising fatty acids, wherein at least 50% by weight of the fatty acids comprise omega-3-fatty acids, salts, esters, or derivatives thereof, wherein the omega-3 fatty acids comprise eicosapentaenoic acid (EPA; C20:5-n3), docosapentaenoic acid (DPA; C22:5-n3), and docosahexaenoic acid (DHA; C22:6-n3), wherein the ratio of DHA to EPA (DHA:EPA) is less than 1 :20, and wherein the ratio of DHA to DPA (DHA:DPA) is less than 2:1 .
  • omega-3 fatty acids comprise eicosapentaenoic acid (EPA; C20:5-n3), docosapentaenoic acid (DPA; C22:5-n3), and docosahexaenoic acid (DHA; C22:6-n3), wherein the ratio
  • compositions of the present invention comprise at least 50% omega-3 fatty acids, alternatively at least 55%, alternatively at least 60%, alternatively at least 65%, alternatively at least 70%, alternatively at least 75%, alternatively at least 80%, alternatively at least 85%, alternatively at least 95%, most preferably at least 90% omega-3 fatty acids of the total amount of fatty acids.
  • EPA and DPA are jointly present in the compositions of the present invention at between 55% and 100% of total fatty acids, alternatively between 60% and 100%, alternatively between 65% and 100%, alternatively between 70% and 100%, alternatively between 75% and 100%, alternatively between 80% and 100%, alternatively between 85% and 95%, alternatively between 85% and 97%, alternatively between 88% and 95%, alternatively between 88% and 97%, alternatively between 90% and 95%, alternatively between 90% and 97% of the total amount of fatty acids.
  • the fatty acids such as EPA and DPA, may be present in free fatty acid form, or as a salt, ester, or derivative.
  • the fatty acids are preferably composed as a
  • Other forms of the fatty acids which may be useful include salts, esters of any type, amides, mono-, di- or triglycerides, phospholipids or any other form which can lead to metabolization of the fatty acids (such as EPA and/or DPA), or the incorporation of the fatty acids (such as EPA and/or DPA) into body fluids, tissues or organs.
  • the compositions of the present invention comprise at least 0.01 % HPA of total fatty acids in the composition, alternatively at least 0.05% HPA, alternatively at least 0.10% HPA, alternatively at least 0.15% HPA, alternatively at least 0.2% HPA, alternatively at least 0.3% HPA, alternatively at least 0.4% HPA, alternatively at least 0.5% HPA, alternatively at least 0.75% HPA, alternatively at least 1 % HPA, alternatively at least 1 .5% HPA, alternatively at least 2% HPA, alternatively at least 2.5% HPA, alternatively at least 3% HPA, alternatively at least 3.5% HPA, alternatively at least 4% HPA, alternatively at least 4.5% HPA, alternatively at least 5% HPA, alternatively at least 6% HPA, alternatively at least 7% HPA, alternatively the compositions of the present invention comprise at least 9% HPA of total fatty acids in the composition.
  • the compositions of the present invention comprise no more than 20% HPA of total fatty acids in the composition, alternatively no more than 15% HPA, alternatively no more than 12% HPA, alternatively no more than 10% HPA, alternatively no more than 8% HPA, alternatively no more than 7% HPA, alternatively no more than 6% HPA, alternatively no more than 5% HPA, alternatively no more than 4% HPA, alternatively no more than 3% HPA, alternatively no more than 2% HPA, alternatively no more than 1 .5% HPA, alternatively the compositions of the present invention comprise at least 1 % HPA of total fatty acids in the composition. In some embodiments, the compositions of the present invention comprise 1 % to 20% of the total fatty acids in the composition.
  • the compositions comprise EPA and DPA in an EPA:DPA ratio between 99:1 and 1 :99 EPA:DPA, alternatively between 90:1 and 1 :90, alternatively between 60:1 and 1 :60, alternatively between 60:1 and 1 :20, alternatively between 60:1 and 1 :4, alternatively between 40:1 and 1 :20, alternatively between 30:1 and 1 :20, alternatively between 30:1 and 1 :10, alternatively between 30:1 and 1 :5, alternatively between 40:1 and 1 :4, alternatively between 30:1 and 1 :4, alternatively between 30:1 and 1 :2, alternatively between 30:1 and 1 :1 , alternatively between 30:1 and 2:1 , alternatively between 30:1 and 5:1 ,
  • AFDOCS/l 0582446.1 alternatively between 20:1 and 1 :20, alternatively between 20:1 and 1 :10, alternatively between 20:1 and 1 :5, alternatively between 20:1 and 1 :2, alternatively between 20:1 and 1 :1 , alternatively between 20:1 and 2:1 , alternatively between 20:1 and 5:1 , alternatively between 20:1 and 10:1 , alternatively between 20:1 and 10:1 , alternatively between 30:1 and 10:1 , alternatively between 60:1 and 10:1 , alternatively comprise EPA and DPA in an EPA:DPA ratio between 40:1 and 10:1 .
  • the ratio of EPA:DPA is greater than 1 :1 , preferably greater than 2:1 , and more preferably greater than 5:1 . In some embodiments, the ratio of EPA:DPA is 1 :1 to 25:1 , preferably 5:1 to 20:1 , more preferably 8:1 to 15:1 , even more preferably 9:1 to 13:1 , even more most preferably about 10:1 to 1 1 :1 , and most preferably about 10:1 .
  • a relatively small amount of DHA relative to the total amount of fatty acids present in the composition is present.
  • the compositions of the present invention comprise no more than 20% DHA, alternatively no more than 15% DHA, alternatively no more than 12% DHA, alternatively no more than 10% DHA, alternatively no more than 8% DHA, alternatively no more than 7% DHA, alternatively no more than 6% DHA, alternatively no more than 5% DHA, alternatively no more than 4% DHA, alternatively no more than 3% DHA, alternatively no more than 2% DHA, alternatively no more than 1 % DHA relative to the total amount of fatty acids present in the composition.
  • the ratio of DPA: H PA is about 250:1 to 1 :1 , alternatively 200:1 to 2:1 , alternatively 150:1 to 3:1 , alternatively 100:1 to 4:1 , alternatively 50:1 to 5:1 , alternatively 25:1 to 6:1 , and alternatively 10:1 to 7:1 .
  • the ratio of DPA:HPA is about 8:1 .
  • the ratio of DPA:HPA is about 3:0.
  • compositions of the present invention comprise no more than 15:1 of DHA:DPA, alternatively no more than 12:1 of DHA:DPA, alternatively no more than 10:1 of DHA:DPA, alternatively no more than 8:1 of DHA:DPA, alternatively no more than 5:1 of DHA:DPA, alternatively no more than 3:1 of DHA:DPA, alternatively no more than 2:1 of DHA:DPA, alternatively no more than 1 :1 of DHA:DPA, alternatively no more than 1 :2 of DHA:DPA, alternatively no more than 1 :3 of DHA:DPA, alternatively no more than 1 :4 of DHA:DPA,
  • AFDOCS/l 0582446.1 alternatively no more than 1 :5 of DHA:DPA, alternatively no more than 1 :6 of DHA:DPA, alternatively no more than 1 :7 of DHA:DPA, alternatively no more than 1 :8 of DHA:DPA, alternatively no more than 1 :10 of DHA:DPA, alternatively no more than 1 :12 of DHA:DPA, alternatively no more than 1 :15 of DHA:DPA, alternatively no more than 1 :20 of DHA:DPA, alternatively no more than 1 :25 of DHA:DPA, alternatively no more than 1 :50 of DHA:DPA, alternatively no more than 1 :75 of DHA:DPA, alternatively no more than 1 :90 of DHA:DPA, alternatively no more than 1 :95 of DHA:DPA, alternatively no more than 1 :100 of DHA:DPA.
  • the ratio of DHA:DPA is preferably less than 2:1
  • compositions of the present invention comprise no more than 10% omega-6 fatty acids relative to the total amount of fatty acids, alternatively no more than 9%, alternatively no more than 8%, alternatively no more than 7%, alternatively no more than 6%, alternatively no more than 5%, alternatively no more than 4.5%, alternatively no more than 4%, alternatively no more than 3.5%, alternatively no more than 3%, alternatively no more than 2.5%, alternatively no more than 2%, alternatively no more than 1 .7%, alternatively no more than 1 .5%, alternatively no more than 1 .2%, alternatively no more than 1 %, alternatively no more than 0.5% omega-6 fatty acids versus the total amount of fatty acids comprised by the compositions of the present invention.
  • Omega-6 fatty acids include, but are not limited to: linoleic acid (LA; C18:2- n6); gamma-linoleic acid (GLA; C18:3-n6); eicosadienoic acid (C20:2-n6); dihomo- gamma-linoleic acid (DGLA; C20:3-n6); arachiconic acid (ARA; C20:4-n6); and omega-6 docosapentaenoic acid (DPA; C22:5-n6).
  • LA linoleic acid
  • GLA gamma-linoleic acid
  • C20:2-n6 eicosadienoic acid
  • DGLA dihomo- gamma-linoleic acid
  • ARA arachiconic acid
  • DPA omega-6 docosapentaenoic acid
  • compositions of the present invention comprise no more than 10% omega-6 fatty acids relative to the total amount of omega-3 fatty acids plus omega-6 fatty acids, alternatively no more than 9%, alternatively no more than 8%, alternatively no more than 7%, alternatively no more than 6%, alternatively no more than 5%, alternatively no more than 4.5%, alternatively no more than 4%, alternatively no more than 3.5%, alternatively no more than 3%, alternatively no more than 2.5%, alternatively no more than 2%, alternatively no more than 1 .7%, alternatively no more than 1 .5%, alternatively no more than 1 .2%, alternatively no more than 1 %, alternatively no more than 0.5% omega-6 fatty acids versus the total amount of omega-3 fatty acids plus omega-6 fatty acids comprised by the compositions of the present invention.
  • the compositions of the present invention comprise no more than 8% arachidonic acid (ARA; C20:4-n6) relative to the total amount of omega-3 fatty acids plus omega-6 fatty acids, alternatively no more than 7%, alternatively no more than 6%, alternatively no more than 5%, alternatively no more than 4.5%, alternatively no more than 4%, alternatively no more than 3.5%, alternatively no more than 3%, alternatively no more than 2.5%, alternatively no more than 2%, alternatively no more than 1 .7%, alternatively no more than 1 .5%, alternatively no more than 1 .2%, alternatively no more than 1 %, alternatively no more than 0.5% arachidonic acid (ARA; C20:4-n6) versus the total amount of omega-3 fatty acids plus omega-6 fatty acids comprised by the compositions of the present invention.
  • ARA arachidonic acid
  • a relatively small amount of omega-3 fatty acids in aggregate other than EPA, ETA, HPA and DPA (alternatively indicated as non-EPA, non-ETA, non-HPA and non-DPA omega-3 fatty acids in aggregate) relative to the total amount of fatty acids present in the composition is present.
  • compositions of the present invention comprise no more than 20% non-EPA, non-ETA, non-HPA and non-DPA omega-3 fatty acids, alternatively no more than 15% non-EPA, non-ETA, non-HPA and non-DPA omega-3 fatty acids, alternatively no more than 12% non-EPA, non-ETA, non-HPA and non-DPA omega- 3 fatty acids, alternatively no more than 10% non-EPA, non-ETA, non-HPA and non- DPA omega-3 fatty acids, alternatively no more than 8% non-EPA, non-ETA, non- HPA and non-DPA omega-3 fatty acids, alternatively no more than 7% non-EPA, non-ETA, non-HPA and non-DPA omega-3 fatty acids, alternatively no more than 6% non-EPA, non-ETA, non-HPA and non-DPA omega-3 fatty acids, alternatively no more than 5% non-EPA, non-ETA, non-HPA and non-DPA omega-3 fatty acids, alternatively no more than 5% non-EPA,
  • a relatively small amount of the sum of ALA, SDA and DHA relative to the total amount of fatty acids present in the composition is present, while at the same time large amounts of the sum of EPA, DPA-n3, HPA and
  • compositions of the present invention comprise no more than 20% of the sum of ALA, SDA and DHA, alternatively no more than 15% of the sum of ALA, SDA and DHA, alternatively no more than 12% of the sum of ALA, SDA and DHA, alternatively no more than 10% of the sum of ALA, SDA and DHA, alternatively no more than 8% of the sum of ALA, SDA and DHA, alternatively no more than 7% of the sum of ALA, SDA and DHA, alternatively no more than 6% of the sum of ALA, SDA and DHA, alternatively no more than 5% of the sum of ALA, SDA and DHA, alternatively no more than 4% of the sum of ALA, SDA and DHA, alternatively no more than 3% of the sum of ALA, SDA and DHA, alternatively no more than 2% of the sum of ALA, SDA and DHA, alternatively no more than 1 % of the sum
  • compositions of the present invention comprise no more than 8% arachidonic acid (ARA; C20:4-n6) relative to the total amount of fatty acids, alternatively no more than 7%, alternatively no more than 6%, alternatively no more than 5%, alternatively no more than 4.5%, alternatively no more than 4%, alternatively no more than 3.5%, alternatively no more than 3%, alternatively no more than 2.5%, alternatively no more than 2%, alternatively no more than 8% arachidonic acid (ARA; C20:4-n6) relative to the total amount of fatty acids, alternatively no more than 7%, alternatively no more than 6%, alternatively no more than 5%, alternatively no more than 4.5%, alternatively no more than 4%, alternatively no more than 3.5%, alternatively no more than 3%, alternatively no more than 2.5%, alternatively no more than 2%, alternatively no more than 8% arachidonic acid (ARA; C20:4-n6) relative to the total amount of fatty acids, alternatively no more than 7%, alternative
  • AFDOCS/l 0582446.1 more than 1 .7%, alternatively no more than 1 .5%, alternatively no more than 1 .2%, alternatively no more than 1 %, alternatively no more than 0.5% arachidonic acid (ARA; C20:4-n6) relative the total amount of fatty acids comprised by the compositions of the present invention.
  • ARA arachidonic acid
  • compositions of the present invention comprise no more than 2.5% arachidonic acid (ARA; C20:4-n6), no more than 0.4% omega-6- docosapentaenoic acid (DPA; C22:5-n6) and no more than 0.2% gamma-linoleic acid (GLA; C18:3-n6) relative the total amount of fatty acids comprised by the compositions of the present invention.
  • ARA arachidonic acid
  • DPA omega-6- docosapentaenoic acid
  • GLA gamma-linoleic acid
  • fatty acid compositions comprising no more than 2.5% arachidonic acid (ARA; C20:4-n6), no more than 0.3% omega-6 docosapentaenoic acid (DPA; C22:5-n6) and no more than 0.1 % gamma-linoleic acid (GLA; C18:3-n6) relative the total amount of fatty acids comprised by the compositions of the present invention.
  • ARA arachidonic acid
  • DPA docosapentaenoic acid
  • GLA gamma-linoleic acid
  • the active ingredient of the formulations of the present invention consists essentially wholly of the EPA and DPA or precursors thereof (ethyl ester, triglyceride, or any other pharmaceutically acceptable salt or derivative thereof).
  • no large amounts preferably less than 15%, alternatively less than 12%, alternatively less than 10%, alternatively less than 9%, alternatively less than 8%, alternatively less than 7%, alternatively less than 6%, alternatively less than 5%, alternatively less than 4%, alternatively less than 3%, alternatively less than 2%, alternatively less than 1 %, alternatively less than 0.5%, alternatively less than 0.25%
  • any other fatty acids are present.
  • the fatty acid percentage is determined on a weight/weight, mol/mol, or chromatography area percent basis relative to all fatty acids present in the composition as determined by methods such as disclosed in the European Pharmacopeia monograph for omega-3 fatty acid concentrates, European Pharmacopeia monograph for omega-3-acid ethyl esters 90%, or European Pharmacopeia monograph method 2.4.29, USP monograph for fish oil dietary supplements, USP 35 omega-3-acid ethyl esters (LOVAZA®) monograph, or any essentially equivalent methods (whether by gas chromatography, HPLC, FPLC or any other chromatographic method).
  • the fatty acid percentage is determined not as a percentage of all fatty acids present in the composition but as a specific type of fatty
  • phospholipids such as phosphatidylserine or phosphatidylcholine
  • polysorbates such as Tween 80, Tween 20, or polysorbate 40.
  • the fatty acid percentage is determined not as a percentage of all fatty acids present in the composition but as a specific type of free fatty acid as percentage of all free fatty acids present in the composition, thus excluding from the fatty acid percentage determination such fatty acids present as, for instance: fatty acid ethyl esters; mono-, di-, and tri-glycerides; or fatty acids present in phospholipids (such as phosphatidylserine or phosphatidylcholine) or polysorbates (such as Tween 80, Tween 20, or polysorbate 40).
  • fatty acids present for instance: fatty acid ethyl esters; mono-, di-, and tri-glycerides; or fatty acids present in phospholipids (such as phosphatidylserine or phosphatidylcholine) or polysorbates (such as Tween 80, Tween 20, or polysorbate 40).
  • the fatty acid percentage is determined not as a percentage of all fatty acids present in the composition but as a specific type of glycerol fatty acid ester as percentage of all glycerol fatty acid esters present in the composition, thus excluding from the fatty acid percentage determination such fatty acids present as, for instance: fatty acid ethyl esters; free fatty acids; or fatty acids present in phospholipids (such as phosphatidylserine or phosphatidylcholine) or polysorbates (such as Tween 80, Tween 20, or polysorbate 40).
  • fatty acids present for instance: fatty acid ethyl esters; free fatty acids; or fatty acids present in phospholipids (such as phosphatidylserine or phosphatidylcholine) or polysorbates (such as Tween 80, Tween 20, or polysorbate 40).
  • the fatty acid percentage is determined not as a percentage of all fatty acids present in the composition but as di- or tri-fatty acid esters with glycerol as percentage of all glycerol di- and tri-fatty acid esters present in the composition, thus excluding from the fatty acid percentage determination such fatty acids present as, for instance: glycerol-mono-fatty acid esters; fatty acid ethyl esters; free fatty acids; or fatty acids present in phospholipids (such as phosphatidylserine or phosphatidylcholine) or polysorbates (such as Tween 80, Tween 20, or polysorbate 40).
  • phospholipids such as phosphatidylserine or phosphatidylcholine
  • polysorbates such as Tween 80, Tween 20, or polysorbate 40.
  • the fatty acid percentage is determined not as a percentage of all fatty acids present in the composition but as a tri-fatty acid esters with glycerol as percentage of all glycerol tri-fatty acid esters present in the composition, thus excluding from the fatty acid percentage determination such fatty acids present as, for instance: mono- and di-fatty acid esters of glycerol; fatty acid ethyl esters; free fatty acids; or fatty acids present in phospholipids (such as
  • the EPA, HPA, DPA, or omega-3-pentaenoic acids may be derived from any appropriate source including plant seed oils, microbial oils from algae or fungal or marine oils from fish or other marine animals. Certain species are a particular good source of oils containing DPA, for example seal oil. They may be used in the form of the natural oil, if that oil meets the required purity requirements of the present invention, or may be purified to give products containing the fatty acid composition of the present invention.
  • compositions of the present invention may be produced through a range of the methods.
  • Such methods may include: distillation, including short path distillation; urea precipitation; enzymatic conversion concentration; conventional chromatography; HPLC/FPLC; supercritical carbondioxide extraction; supercritical carbondioxide chromatography; simulated moving bed chromatography; supercritical carbondioxide simulated moving bed chromatography; or chemical conversion methods such as iodolactonization.
  • distillation including short path distillation; urea precipitation; enzymatic conversion concentration; conventional chromatography; HPLC/FPLC; supercritical carbondioxide extraction; supercritical carbondioxide chromatography; simulated moving bed chromatography; supercritical carbondioxide simulated moving bed chromatography; or chemical conversion methods such as iodolactonization.
  • Such methods are generally known to those skilled in the art of purifying and isolating omega-3 fatty acids ⁇
  • the omega-3 fatty acid concentration/purification process is initiated by esterifying the fatty acids comprised by the marine oil raw material (such as crude fish oil) with ethanol (to form fatty acid ethyl esters) in order to separate omega-3 fatty acids from other fatty acids covalently bound together in the natural triglyceride molecules of the source oil. Subsequently, the material may be distilled once or several times to achieve omega-3-acid ethyl ester concentrations above 60%-70%. Alternatively, enzymatic concentration, urea precipitation or supercritical extraction may be used alone or in conjunction with distillation to reach omega-3 levels above 70%-90%.
  • chromatography In order to prepare a highly pure concentrate of a single omega-3 fatty acid, methods such as chromatography, supercritical chromatography, simulated moving bed chromatography, supercritical simulated moving bed chromatography, or chemical conversion methods such as iodolactolization are typically most practical to reach levels above 50%, alternatively above 60%, alternatively above 70%, alternatively above 80%, alternatively above 90%, alternatively above 95%, of a single omega-3 fatty acid such as ETA, EPA, HPA, DPA, TPA, or DHA.
  • a single omega-3 fatty acid such as ETA, EPA, HPA, DPA, TPA, or DHA.
  • EPA is relatively abundant in fish oils or other marine oils and can be relatively easy obtained through the application of concentration and purification technologies from such fish or marine oils.
  • DPA and HPA are present at much lower concentrations.
  • DPA or HPA may be concentrated and purified from fish or other marine oils according to the methods referred to above, either alone or DPA combined with EPA and/or HPA.
  • the DPA or HPA may be chemically prepared from a high purity EPA concentrate by elongation of the EPA fatty-acid chain with two or one hydrogen- saturated carbons (C2-elongation or C1 -elongation) on the carboxyl side of the molecule (for instance with a method similar to or alternate methods with equivalent results such as described by Kuklev DV and Smith WL in Chem Phys Lipids, 2006; 144(2): 172-177).
  • a high purity EPA concentrate may be partially converted to DPA (or HPA) using a method for C2-elongation (or C1 -elongation) of EPA similar to those described above, thus directly yielding compositions of the present invention or intermediates therefore.
  • oils containing one or more of the desired fatty acids may be blended to give the desirable relative amounts of EPA, DPA, HPA, DHA, TPA, other omega-3 fatty acids and omega-6 fatty acids to obtain the compositions of the present invention described in detail above.
  • Fish oils may also contain by-products and contaminants such as pesticides, chlorinated or brominated hydrocarbons, heavy metals, cholesterol and vitamins. During the production of the concentrate, the concentrations of these components are significantly reduced compared to untreated fish oils. Such reduction is inherent
  • AFDOCS/10582446.1 due to the nature of purification methods and their ability to concentrate of several or specific omega-3 fatty acids, thus removing other compounds.
  • Triglycerides comprising more than 60% of the omega-3 fatty acids in the composition may be produced from ethyl esters and glycerol by well known, published, or alternative chemical synthetic or enzymatic procedures.
  • the free acids may be produced from ethyl esters by well known hydrolization or saponification procedures. Methods for converting ethyl esters to triglycerides, free fatty acids, and other molecular forms comprising fatty acids, are generally known to those skilled in the art chemically or enzymatically converting omega-3 fatty acids from one form to another.
  • compositions of the present invention may be used for the treatment of patients by administering an effective amount of such compositions to a subject in need thereof, such as a subject prone to or afflicted with a disease or condition or in need of treatment for a disease or condition.
  • the present invention provides methods of treating, preventing, and reducing symptoms associated with a disease or condition comprising administration of a composition of the present invention.
  • Exemplary diseases or conditions include, but are not limited to: hypertriglyceridemia (for example, by those skilled in the art typically established by assessing fasting triglyceride (TG) levels); hypertriglyceridemia with TG ⁇ 500mg/dL (VHTG); hypertriglyceridemia with TG 200-499mg/dL; hypertriglyceridemia with TG 200-499mg/dL while on statin treatment (HTG); hypercholesterolemia; mixed dyslipidemia; coronary heart disease (CHD); vascular disease; atherosclerotic disease and related conditions; heart failure; cardiac arrhythmias; blood coagulatory conditions associated with cardiac arrhytmias; hypertension; coagulation related disorders, including post-surgical deep vein thrombosis or other high risk thrombosis conditions; nephropathy; kidney or urinary tract disease; retinopathy; cognitive, psychiatric, neurological and other CNS disorders, including but not limited to schizophrenia, depression, bipolar disorder
  • AFDOCS/l 0582446.1 type including lymphomas, myelomas and solid tumor cancers; any infections caused by a virus, bacterium, fungus, protozoa or other organism.
  • the present invention also provides for the treatment and/or prevention of cardiac events and/or cardiovascular events and/or vascular events and/or symptoms.
  • the present invention also provides for the reduction of number of such events, as well as a reduction or amelioration of symptoms associated with such events.
  • Cardiovascular and/or cardiac events may include, but are not limited to: myocardial infarction, ischemic cardiac attack, ischemic attack, acute angina, hospitalization due to acute angina, stroke, transient ischemic cerebral attack, cardiac revascularization, cardiac revascularization with stent placement, carotid artery revascularization, carotid artery revascularization with stent placement, peripheral artery revascularization, peripheral artery revascularization with stent placement, plaque rupture, death due to cardiovascular event, and hospitalization due to cardiovascular event. Cardiovascular and/or cardiac events may also include other events deemed to fall in such catergory by those skilled in the art.
  • DPA-n3 omega-3 docosapentaenoic acid
  • the present invention also provides for a method for reducing fasting lipid parameters, such as triglycerides, low-density lipoprotein (LDL) cholesterol, total cholesterol, non-HDL cholesterol, free fatty acids, and total non- high-lipoprotein cholesterol (non-HDL) cholesterol.
  • the present invention also provides method for increasing high-lipoprotein (HDL) cholesterol levels.
  • the methods of treatment provides a dose of at least 60mg DPA-N3 per day, alternatively at least 80mg DPA-N3 per day, alternatively at least 90mg DPA-N3 per day, alternatively at least 100mg DPA-N3 per day, alternatively at least 120mg DPA- N3 per day, alternatively at least 150mg DPA-N3 per day, alternatively at least 160mg DPA-N3 per day, alternatively at least 180mg DPA-N3 per day, alternatively at least 200mg DPA-N3 per day, alternatively at least 250mg DPA-N3 per day, alternatively at least 300mg DPA-N3 per day, alternatively at least 350mg DPA-N3 per day, alternatively at least 400mg DPA-N3 per day, alternatively at least 500mg
  • DPA-N3 per day alternatively at least 600mg DPA-N3 per day, alternatively at least
  • the method of treatment provides a dose of at least about 1 ,000 mg DPA-N3 per day, alternatively at least about 1 ,500 mg DPA-N3 per day, alternatively at least about 2,000 mg DPA-N3 per day, alternatively at least about 2,500 mg DPA-N3 per day, alternatively at least about 3,000 mg DPA-N3 per day, alternatively at least about 3,500 mg DPA-N3 per day, alternatively at least about 3,750 mg DPA-N3 per day, alternatively at least about 4,000 mg DPA-N3 per day, alternatively at least about 4,250 mg DPA-N3 per day.
  • the compositions comprise docosapentaenoic acid (DPA) in a significant or higher relative amount as compared to docosahexaenoic acid (DHA) such that the DPA:DHA ratio in the composition is 1 :2 or greater.
  • DPA docosapentaenoic acid
  • DHA docosahexaenoic acid
  • the ratio of DPA:DHA in the composition is at least 1 :1 , or at least 2:1 or at least 3:1 , or at least 4:1 or at least 5:1 .
  • the method of treatment provides a dose of at least about 1 mg/kg of DPA-N3 per day, alternatively about 2 mg/kg of DPA-N3 per day, alternatively about 3 mg/kg of DPA-N3 per day, alternatively about 4 mg/kg of DPA- N3 per day, alternatively about 6 mg/kg of DPA-N3 per day, alternatively about 8 mg/kg of DPA-N3 per day, alternatively about 10 mg/kg of DPA-N3 per day, alternatively about 20 mg/kg of DPA-N3 per day, alternatively about 30 mg/kg of DPA-N3 per day, and alternatively about 40 mg/kg alternatively about 50 mg/kg of DPA-N3 per day, alternatively about 75 mg/kg of DPA-N3 per day, and alternatively about 100 mg/kg.
  • compositions of the present invention which may comprise significant amounts of omega-3 docosapentaenoic acid (DPA-n3) or its glycerol or ethyl esters, may be used for the treatment of hypertriglyceridemia (either TG ⁇ 500mg/dl_, TG ⁇ 200mg/dl_, TG ⁇ 150mg/dl_, TG200-499mg/dl_, TG300-499mg/dl_, TG350-499mg/dl_,, or TG150-199mg/dl_), mixed dyslipidemia, or any other diseases or medical conditions specified above.
  • DPA-n3 docosapentaenoic acid DPA-n3
  • glycerol or ethyl esters may be used for the treatment of hypertriglyceridemia (either TG ⁇ 500mg/dl_, TG ⁇ 200mg/dl_, TG ⁇ 150mg/dl_, TG200-4
  • Such method of treatment provides to a subject in need thereof a dose of at least 20mg DPA-N3 per day, alternatively at least 25mg DPA-N3 per day, alternatively at least 30mg DPA-N3 per day, alternatively at least 40mg DPA-N3 per day, alternatively at least 50mg DPA-N3 per day, alternatively at least 60mg DPA-N3 per day, alternatively at least 70mg DPA- N3 per day, alternatively at least 80mg DPA-N3 per day, alternatively at least
  • AFDOCS/l 0582446.1 least 120mgDPA-N3 per day, alternatively at least 150mg DPA-N3 per day, alternatively at least 160mg DPA-N3 per day, alternatively at least 180mg DPA-N3 per day, alternatively at least 200mg DPA-N3 per day, alternatively at least 250mg DPA-N3 per day, alternatively at least 300mg DPA-N3 per day, alternatively at least 350mg DPA-N3 per day, alternatively at least 400mg DPA-N3 per day, alternatively at least 500mg DPA-N3 per day, alternatively at least 600mg DPA-N3 per day, alternatively at least 800mg DPA-N3 or its glycerol or ethyl esters per day.
  • the methods of the present invention relate to decreasing plasma lipid parameters in a subject in need thereof.
  • the lipid parameters may be measured in a fasting state or a fed state.
  • the methods comprise administration of DPA in the free fatty acid form or an ester form.
  • the methods comprise a reduction in triglyceride levels of at least 10%, alternatively at least 15%, alternatively at least 20%, alternatively at least 25%, alternatively at least 30%, alternatively at least 35%, alternatively at least 40%, alternatively at least 45%, and alternatively at least 50% compared to baseline.
  • the methods comprise a reduction in total cholesterol levels of at least 1 %, alternatively at least 2%, alternatively at least 3%, alternatively at least 4%, alternatively at least 5%, alternatively at least 6%, alternatively at least 7%, alternatively at least 8%, alternatively at least 9%, alternatively at least 10% compared to baseline.
  • the methods comprise a reduction in low-density lipoprotein (LDL) levels of at least 10%, alternatively at least 15%, alternatively at least 20%, alternatively at least 25%, alternatively at least 30%, alternatively at least 35%, alternatively at least 40%, alternatively at least 45%, and alternatively at least 50% compared to baseline.
  • LDL low-density lipoprotein
  • the methods comprise a reduction in free fatty acid levels of at least 5%, alternatively at least 7%, alternatively at least 10%, alternatively at least 15%, alternatively at least 20% compared to baseline. In some embodiments, the methods comprise a reduction in non-HDL cholesterol levels of at least 1 %, alternatively at least 2%, alternatively at least 3%, alternatively at least 4%, alternatively at least 5%, alternatively at least 6%, alternatively at least 7%, alternatively at least 8%, alternatively at least 9%, alternatively at least 10% compared to baseline.
  • the methods comprise an increase in high density lipoprotein (HDL) cholesterol levels of at least 1 %, alternatively at least 2%, alternatively at least 3%, alternatively at least 4%, alternatively at least 5%, alternatively at least 6%,
  • HDL high density lipoprotein
  • this change in lipid parameters can be achieved after a period of daily administration, such as one week, alternatively one month, alternatively two months, alternatively three months or more.
  • Such method of treatment provides to a subject in need thereof a dose of at least 20mg DPA-N3 per day, alternatively at least 25mg DPA-N3 per day, alternatively at least 30mg DPA-N3 per day, alternatively at least 40mg DPA-N3 per day, alternatively at least 50mg DPA-N3 per day, alternatively at least 60mg DPA-N3 per day, alternatively at least 80mg DPA-N3 per day, alternatively at least 90mg DPA-N3 per day, alternatively at least 120mg DPA-N3 per day, alternatively at least 150mg DPA- N3 per day, alternatively at least 160mg DPA-N3 per day, alternatively at least 180mg DPA-N3 per day, alternatively at least 200mg DPA-N3 per day, alternatively at least 250mg DPA-N3 per day, alternatively at least 300mg DPA-N3 per day, alternatively at least 350mg DPA-N3 per day,
  • Such method of treatment provides to a subject in need thereof a dose of at least 30mg DPA-N3 per day, alternatively at least 40mg DPA-N3 per day, alternatively at least 50mg DPA-N3 per day, alternatively at least 60mg DPA-N3 per day, alternatively at least 80mg DPA-N3 per day, alternatively at least 90mg DPA-N3 per day, alternatively at least 120mg DPA-N3 per day, alternatively at least 150mg DPA-N3 per day, alternatively at least 160mg DPA-N3 per day, alternatively at least 180mg DPA-N3 per day, alternatively at least 200mg DPA-N3 per day, alternatively at least 250mg DPA-N3 per day, alternatively at least 300mg DPA-N3 per day, alternatively at least 350mg DPA-N3 per day, alternatively at least 400mg DPA-N3 per day, alternatively at least 500mg DPA-N3 per day,
  • the improved profile of the compositions of the present invention may be demonstrated upon treatment of a subject by differentially altering the ration between blood platelets and fragments thereof (also known as
  • Such fragments may be evaluated as a whole or examined and described as fragment sub-categories.
  • the improved profile of the compositions of the present invention may be demonstrated upon treatment of a subject by differentially altering the surface charge of blood platelets and fragments thereof, either in resting state (non-activated platelets) or activated stage.
  • treatment of a subject or patient with compositions of the present invention affect the coagulatory cascade and differentially alter coagulation or bleeding times or platelet aggregation times and density.
  • treatment with compositions of the present invention improves the vascular healing process in response to atherogenic disease.
  • Such healing may be demonstrated by reduced stenosis and/or restenosis over time, reduced or lesser increase in intima-media thickness (IMT) of the arterial wall, larger lumen size and/or larger vascular diameter at vascular sites with stenosis or clot built-up, as determined by either by intravascular ultrasound (IVUS), radiographic, radiologic, non-invasive ultrasound, tomography, magnetic resonance interference (MRI), or other acceptable methods.
  • IVUS intravascular ultrasound
  • MRI magnetic resonance interference
  • such improved healing may be demonstrated by the vascular wall composition, such as a reduced foam cell presence or fibrillated tissue in the vessel wall.
  • such improved vascular healing is demonstrated by improved inflammatory markers in the vascular wall.
  • the improved profile resulting from treatment with the compositions of the present invention may also be demonstrated by a differentiated impact on blood/serum/plasma lipid and lipoprotein levels in a mammal; these include, but are not limited to: Triglycerides (TG), total-cholesterol, non-HDL-cholesterol, LDL- cholesterol, VLDL-cholesterol, apolipoprotein B, apolipoprotein A, apolipoprotein C- III, HDL-cholesterol, and Lp-PLA2.
  • TG Triglycerides
  • compositions of the present invention may also be used to provide a beneficial impact on the one or more of the following: apolipoprotein A-l (apo A-l), apolipoprotein B (apo B), apo A-l/apo B ratio, lipoprotein(a) (Lp[a]), lipoprotein-associated phospholipase A2 (Lp-PLA2), low density lipoprotein (LDL) particle number and size, oxidized LDL, C-reactive protein (CRP), high sensitivity C-reactive protein (HSCRP), intracellular adhesion molecule-
  • apolipoprotein A-l apo A-l
  • apo B apolipoprotein B
  • apo A-l/apo B ratio lipoprotein(a)
  • Lp[a] lipoprotein-associated phospholipase A2
  • LDL low density lipoprotein
  • CRP C-reactive protein
  • HCRP high sensitivity C-reactive protein
  • ICM-1 vascular cell adhesion molecule 1
  • VCAM-1 vascular cell adhesion molecule 1
  • AFDOCS/l 0582446.1 cluster of differentiation 106 CD106
  • interleleukin -1 ⁇ IL- ⁇ ⁇
  • interleukin-2 IL-2
  • interleukin-6 IL-6
  • interleukin-8 IL-8
  • interleukin-10 IL-10
  • interleukin-12 IL-12
  • interleukin-15 IL-15
  • interleukin-18 IL-18
  • tumor necrosis factor-alpha tumor necrosis factor-beta
  • PAI-1 plasminogen activator inhibitor-1
  • PAI-1 plasminogen activator inhibitor-1
  • homocysteine thromboxane B2 (TXB2)
  • thromboxane A2 TXA2
  • 2,3-dinor thromboxane B2 free fatty acids
  • FFA free fatty acids
  • serum amyloid A1 serum amyloid A2
  • serum amyloid A3 serum amyloid A4, thiobarbituric acid (TBA) reacting material
  • treatment with the compositions of the present invention is more potent than other omega-3 compositions known in the prior art (such as LOVAZA®, EPANOVATM or AMR101 ) in reducing as compared to placebo or baseline: TG levels, Total-cholesterol levels, non-HDL-cholesterol levels, VLDL- cholesterol levels, LDL-cholesterol levels, apolipoprotein B levels, apolipoprotein C- III levels, Lp-PLA2 levels, or any combinations thereof.
  • omega-3 compositions known in the prior art such as LOVAZA®, EPANOVATM or AMR101
  • TG levels Total-cholesterol levels
  • non-HDL-cholesterol levels VLDL- cholesterol levels
  • LDL-cholesterol levels LDL-cholesterol levels
  • apolipoprotein B levels apolipoprotein C- III levels
  • Lp-PLA2 levels or any combinations thereof.
  • such more potent effects in reducing these pararemeters are achieved in patients with baseline TG over 500 mg
  • AFDOCS/l 0582446.1 cholesterol of 190 mg/dL or higher and with TG in the 300-700 mg/dL range in patients not on statin treatment with baseline LDL-cholesterol of 190 mg/dL or higher and with TG in the 350-700 mg/dL range, in patients not on statin treatment with baseline LDL-cholesterol of 190 mg/dL or higher and with TG in the 300-750 mg/dL range, in patients not on statin treatment with baseline LDL-cholesterol of 190 mg/dL or higher and with TG in the 350-750 mg/dL range, or in patients not on statin treatment with baseline non-HDL-cholesterol of 200 mg/dL or higher and with TG in the 300-700 mg/dL range, or in patients not on statin treatment with baseline non- HDL-cholesterol of 200 mg/dL or higher and with TG in the 350-700 mg/dL range , or in patients not on statin treatment with baseline non-HDL-cholesterol of
  • treatment with the compositions of the present invention together with statin therapy is more potent than other omega-3 compositions known in the prior art (such as LOVAZA®, EPANOVATM or AMR101 ) in reducing as compared to placebo or baseline: TG levels, Total-cholesterol levels, non-HDL-cholesterol levels, VLDL-cholesterol levels, LDL-cholesterol levelsapolipoprotein B levels, apolipoprotein C-lll levels, Lp-PLA2 levels, or any combinations thereof.
  • omega-3 compositions known in the prior art such as LOVAZA®, EPANOVATM or AMR101
  • such more potent effects in reducing these pararemeters are achieved in patients with baseline TG over 500 mg/dL, in patients on statin treatment with baseline TG in the 200-499 mg/dL range, in patients not on baseline statin treatment with baseline LDL-cholesterol of 190 mg/dL or higher and with TG in the 300-700 mg/dL range, in patients not on baseline statin treatment with baseline LDL-cholesterol of 190 mg/dL or higher and with TG in the 350-700 mg/dL range, in patients not on baseline statin treatment with baseline LDL- cholesterol of 190 mg/dL or higher and with TG in the 300-750 mg/dL range, in patients not on baseline statin treatment with baseline LDL-cholesterol of 190 mg/dL or higher and with TG in the 350-750 mg/dL range, or in patients not on baseline statin treatment with baseline non-HDL-cholesterol of 200 mg/dL or higher and with TG in the 300-700 mg/dL range ,
  • AFDOCS/l 0582446.1 patients not on baseline statin treatment with baseline Non-HDL-cholesterol of 200 mg/dL or higher and with TG in the 350-750 mg/dL range.
  • the present invention also provides methods of reducing triglycerides levels in a subject, wherein the non-HDL cholesterol levels, such as LDL-cholesterol levels, of the subject are reduced or not significantly increased from, for example, baseline levels before treatment.
  • treatment with the compositions of the present invention results in a minor (less than 10% change from baseline, alternatively less than 5%) and/or non-significant change in non-HDL cholesterol levels (such as LDL-cholesterol levels) as compared to placebo in patients with baseline TG levels above 500 mg/dL.
  • treatment with the compositions of the present invention results in reductions of LDL-cholesterol levels as compared to placebo in patients with baseline TG levels above 500 mg/dL.
  • the methods involve coadministration of a statin.
  • treatment with the compositions of the present invention as compared to placebo does not increase LDL-cholesterol levels in patients with baseline TG levels of 200-499 mg/dL while on statin therapy.
  • treatment with the compositions of the present invention as compared to placebo results in significant reductions in LDL-cholesterol levels in patients with baseline TG levels of 200-499 mg/dL while on statin therapy.
  • compositions of the present invention as compared to placebo result in significant reductions in LDL-cholesterol levels in patients not on statin treatment with LDL-cholesterol of 190 mg/dL or higher and with TG in the 300-700 mg/dL range, in patients not on statin treatment with LDL- cholesterol of 190 mg/dL or higher and with TG in the 350-700 mg/dL range, in patients not on statin treatment with LDL-cholesterol of 190 mg/dL or higher and with TG in the 300-750 mg/dL range, or in patients not on statin treatment with LDL- cholesterol of 190 mg/dL or higher and with TG in the 350-750 mg/dL range.
  • compositions of the present invention as compared to placebo result in significant reductions in LDL-cholesterol levels in patients not on statin treatment with non-HDL-cholesterol of 200 mg/dL or higher and with TG in the 300-700 mg/dL range, in patients not on statin treatment with Non-HDL-cholesterol of 200 mg/dL or higher and with TG in the 350-700 mg/dL range, in patients not on statin treatment with non-HDL-cholesterol of 200 mg/dL or higher and with TG in the
  • treatment with the compositions of the present invention together with statin therapy results in significant reductions in LDL- cholesterol levels as compared to placebo in patients not on statin treatment at baseline with baseline LDL-cholesterol of 190 mg/dL or higher and with TG in the 300-700 mg/dL range, in patients not on baseline statin treatment with baseline LDL- cholesterol of 190 mg/dL or higher and with TG in the 350-700 mg/dL range, in patients not on baseline statin treatment with baseline LDL-cholesterol of 190 mg/dL or higher and with TG in the 300-750 mg/dL range, or in patients not on baseline statin treatment with baseline LDL-cholesterol of 190 mg/dL or higher and with TG in the 350-750 mg/dL range.
  • treatment with the compositions of the present invention together with statin therapy results in significant reductions in LDL- cholesterol levels as compared to placebo in patients not on baseline statin treatment with baseline non-HDL-cholesterol of 200 mg/dL or higher and with TG in the 300-700 mg/dL range, in patients not on baseline statin treatment with baseline non-HDL-cholesterol of 200 mg/dL or higher and with TG in the 350-700 mg/dL range, in patients not on baseline statin treatment with baseline non-HDL-cholesterol of 200 mg/dL or higher and with TG in the 300-750 mg/dL range, or in patients not on baseline statin treatment with baseline Non-HDL-cholesterol of 200 mg/dL or higher and with TG in the 350-750 mg/dL range.
  • compositions of the present invention are more potent than other omega-3 compositions known in the prior art (such as LOVAZA®, EPANOVATM or AMR101 ) in increasing as compared to placebo or baseline HDL- cholesterol levels, apolipoprotein-A levels, or a combination thereof.
  • compositions of the present invention are more potent than other omega-3 compositions known in the prior art (such as LOVAZA®, EPANOVATM or AMR101 ) in decreasing as compared to placebo or baseline Apolipoprotein-B (Apo-B) levels, Apolipoprotein-CIII levels, Lp-PLA2 levels or any combination thereof.
  • omega-3 compositions known in the prior art such as LOVAZA®, EPANOVATM or AMR101
  • compositions of the present invention as compared to placebo or baseline are more potent than other omega-3 compositions known in the prior art (such as LOVAZA®, EPANOVATM or AMR101 ) in reducing TG
  • the use of the compositions of the present invention may allow for a reduction in the dose of the statin required for a subject.
  • the coadministration of the composition of the present invention in a subject receiving statin therapy may allow for the reduction of the dose of the statin, compared to subject not being co-administered a composition of the present invention.
  • the dose of the statin may be reduced by at least 10%, alternatively at least 25%, alternatively at least 50%, or alternatively at least 75%.
  • the use of the compositions of the present invention may reduce the time needed for a subject to reach the recommended blood levels.
  • the administration of compositions of the present invention may allow a subject to reach goal lipid levels, for example, those described in the NCEP ATP III Guidelines, or any levels recommended by a health care practitioner.
  • the reduction of time is greater than 5%, alternatively greater than 15%, alternatively greater than 25%, alternatively greater than 50%, and alternatively greater than 75%.
  • compositions of the present invention are also useful to treat coronary heart disease (CHD), vascular disease, atherosclerotic disease or related conditions.
  • CHD coronary heart disease
  • the compositions of the present invention may also be use for the treatment and/or prevention and/or reduction of cardiac events and/or cardiovascular events and/or vascular events and/or symptoms. Determination of such cardiovascular diseases/conditions and prevention of events/symptoms in mammals and methods to determine treatment and preventative/therapeutic effects therefore are generally know to those skilled in the art.
  • the present invention also relates to treatment of such conditions in with concomitant treatments regimes or combination products with other active pharmaceutical ingredients.
  • concomitant or fixed combination treatments may include a statin, an anticoagulant (such as aspirin or clopidogrel), an antihypertensive (such as a diuretic, beta-blocker, calcium channel blocker, ACE- inhibitor, angiotensin II receptor (ARB) antagonist), or other treatments for cardiovascular diseases.
  • the present invention also includes pharmaceutical compositions, for example, a unit dosage, comprising one or more HMG-CoA reductase inhibitors ("statins") and the omega-3 fatty acid composition of the present invention.
  • statins HMG-CoA reductase inhibitors
  • the present invention may incorporate now known or future known statins in an amount generally recognized as safe. There are currently seven statins that are widely available: atorvastatin, rosuvastatin, fluvastatin, lovastatin, pravastatin, pitavastatin, and simvastatin. An eight statin, cerivastatin, has been removed from the U.S. market at the time of this writing.
  • cerivastatin may be used in conjunction with some embodiments of the present invention if cerivastatin is ultimately determined to be safe and effective in certain treatment regimens.
  • Such statins are typically used at their common daily doses, which include, but are not limited to lovastatin 10mg, 20mg, 40mg; pravastatin 10mg, 20mg, 40mg, 80mg; simvastatin 5mg, 10mg, 20mg, 40mg, 80mg; fluvastatin 20mg, 40mg, 80mg; atorvastatin 10mg, 20mg, 40mg, 80mg; rosuvastatin 5mg, 10mg, 20mg, 40mg; and pitavastatin 1 mg, 2mg, 4mg, 8mg.
  • statins are dose dependent, i.e., the higher the dose, the greater the therapeutic affect.
  • the effect of each statin is different, and therefore the level of therapeutic effect of one statin cannot be necessarily be directly correlated to the level of therapeutic effects of other statins.
  • bioavailability varies widely among the statins. Specifically, it has been shown that simvastatin is less than 5% bioavailable, while fluvastatin is approximately 24% bioavailable. Statins are absorbed at rates ranging from about 30% with lovastatin to 98% with fluvastatin. First-pass metabolism occurs in all statins except pravastatin.
  • Pravastatin is also the least protein-bound of the statins (about 50%), compared with the others, which are more than 90% protein-bound. Accordingly, the statins possess distinct properties from one another.
  • the combination products of this invention involving each statin or a plurality of statins are also distinct.
  • the present invention also includes methods of treatment, comprising dosing of one or more statins and the omega-3 fatty acid composition of the present invention, either as concomitant therapy or in a fixed dose combination product comprising both a statin and the composition of the present invention.
  • This method of treatment combines the administration of one or more statins at its common dose or an alternative dose with the composition of the present invention.
  • compositions of the present invention which comprise significant amounts of omega-3 docosapentaenoic acid (DPA-n3) or its glycerol or ethyl esters, together with a common or alternative statin dose, may be used for the treatment of hypertriglyceridemia (either TG ⁇ 500mg/dL, TG ⁇ 200mg/dL, TG ⁇ 150mg/dl_, TG 200-499mg/dl_, or TG 150-199mg/dl_), mixed dyslipidemia, or any other diseases or medical conditions specified above.
  • DPA-n3 docosapentaenoic acid
  • ethyl esters ethyl esters
  • Such methods of treatment provide to a subject in need thereof a dose of at least 30 mg DPA-N3 per day, alternatively at least 40mg DPA-N3 per day, alternatively at least 50mg DPA-N3 per day, alternatively at least 60mg DPA-N3 per day, alternatively at least 70mg DPA-N3 per day, alternatively at least 80mg DPA-N3 per day, alternatively at least 90mg DPA-N3 per day, alternatively at least 100mg DPA-N3 per day, alternatively at least 120mg DPA-N3 per day, alternatively at least 150mg DPA-N3 per day, alternatively at least 160mg DPA-N3 per day, alternatively at least 180mg DPA-N3 per day, alternatively at least 200mg DPA-N3 per day, alternatively at least 250mgDPA-N3 per day, alternatively at least 300mg DPA-N3 per day, alternatively at least 350mg DPA-N3 per day, alternative
  • compositions of the present invention which comprise significant amounts of omega-3 docosapentaenoic acid (DPA-n3) or its glycerol or ethyl esters and which comprise relatively small amounts of omega-3 docosahexaenoic acid (DHA-n3), together with a common or alternative statin dose, may be used for the treatment of hypertriglyceridemia (either TG ⁇ 500mg/dL, TG ⁇ 200mg/dl_, TG ⁇ 150mg/dl_, TG 200-499mg/dl_, or TG 150-199mg/dl_), mixed dyslipidemia, or any other diseases or medical conditions specified above.
  • hypertriglyceridemia either TG ⁇ 500mg/dL, TG ⁇ 200mg/dl_, TG ⁇ 150mg/dl_, TG 200-499mg/dl_, or TG 150-199mg/dl_
  • mixed dyslipidemia or any other diseases or medical conditions specified above
  • Such method of treatment provides to a subject in need thereof a common or alternative statin dose together with a dose of at least 30mg DPA-N3 per day, alternatively at least 40mg DPA-N3 per day, alternatively at least 50mg DPA-N3 per day, alternatively at least 60mg DPA-N3 per day, alternatively at least 80mg DPA-N3 per day, alternatively at least 90mg DPA-N3 per day, alternatively at least 120mg DPA- N3 per day, alternatively at least 150mg DPA-N3 per day, alternatively at least 160mg DPA-N3 per day, alternatively at least 180mg DPA-N3 per day, alternatively at least 200mg DPA-N3 per day, alternatively at least 250mg DPA-N3 per day,
  • AFDOCS/l 0582446.1 alternatively at least 300mg DPA-N3 per day, alternatively at least 350mg DPA-N3 per day, alternatively at least 400mg DPA-N3 per day, alternatively at least 500mg DPA-N3 per day, alternatively at least 600mg DPA-N3 per day, alternatively at least 800mg DPA-N3 or its glycerol or ethyl esters per day, while providing less than 2000mg of DHA, alternatively less than 1900mg of DHA, alternatively less than 1500mg of DHA, alternatively less than 1200mg of DHA, alternatively less than 1000mg of DHA, alternatively less than 800mg of DHA, alternatively less than 700mg of DHA, alternatively less than 600mg of DHA, alternatively less than 500mg of DHA, alternatively less than 400mg of DHA, alternatively less than 350mg of DHA, alternatively less than 300mg of DHA, alternatively less than 250
  • compositions of the present invention which comprise significant amounts of omega-3 docosapentaenoic acid (DPA-n3) or its glycerol or ethyl esters and which comprise relatively small amounts of omega-3 docosahexaenoic acid (DHA-n3), together with a common or alternative statin dose, may be used for the treatment of hypertriglyceridemia (either TG ⁇ 500mg/dL, TG ⁇ 200mg/dl_, TG ⁇ 150mg/dl_, TG 200-499mg/dl_, or TG 150-199mg/dl_), mixed dyslipidemia, or any other diseases or medical conditions specified above.
  • hypertriglyceridemia either TG ⁇ 500mg/dL, TG ⁇ 200mg/dl_, TG ⁇ 150mg/dl_, TG 200-499mg/dl_, or TG 150-199mg/dl_
  • mixed dyslipidemia or any other diseases or medical conditions specified above
  • Such method of treatment provides to a subject in need thereof a common or alternative statin dose together with a dose of at least 30mg DPA-N3 per day, alternatively at least 40mg DPA-N3 per day, alternatively at least 50mg DPA-N3 per day, alternatively at least 60mg DPA-N3 per day, alternatively at least 70mg DPA-N3 per day, alternatively at least 80mg DPA-N3 per day, alternatively at least 90mg DPA-N3 per day, alternatively at least 100mg DPA-N3 per day, alternatively at least 120mg DPA-N3 per day, alternatively at least 150mg DPA-N3 per day, alternatively at least 160mg DPA-N3 per day, alternatively at least 180mg DPA-N3 per day, alternatively at least 200mg DPA-N3 per day, alternatively at least 250mg DPA-N3 per day, alternatively at least 300mg DPA-N3 per day, alternatively at least 350
  • DHA-N3 per day alternatively at least 600mg DPA-N3 per day, alternatively at least 800mg DPA-N3 per day, alternatively at least 1000mg DPA-N3 per day, alternatively at least 1200mg DPA-N3 per day, alternatively at least 1500mg DPA-N3 or its glycerol or ethyl esters per day, while providing a relatively small amount of DHA-N3 such that the DHA:DPA dose ratio is no more than 15:1 of DHA:DPA, alternatively no more than 12:1 of DHA:DPA, alternatively no more than 10:1 of DHA:DPA, alternatively no more than 8:1 of DHA:DPA, alternatively no more than 5:1 of DHA:DPA, alternatively no more than 3:1 of DHA:DPA, alternatively no more than 2:1 of DHA:DPA, alternatively no more than 1 :1 of DHA:DPA, alternatively no more than 1
  • the composition of the present invention further comprises TPA at concentration of at least 0.05%.
  • the TPA concentration is about 0.01 % to about 5%, alternatively about 0.05% to about 2%, alternatively about 0.1 % to about 1 %, alternatively about 0.2% to about 0.8%, alternatively about 0.4% to about 0.6%, alternatively about 0.5%.
  • compositions of the present invention may also be taken as a general nutritional supplement.
  • compositions of the present invention are preferably provided in a dose of between 100 mg and 10,100 mg/day, alternatively between 200 mg and 8,100 mg/day, alternatively between 300 mg and 6,100 mg/day, alternatively between 400 mg and 5,100 mg/day, alternatively between 500 mg and 4,100 mg/day.
  • compositions of the present invention are preferably provided in a dose of between 100 mg and 10,100 mg/day, alternatively between 200 mg and 8,100 mg/day, alternatively between 300 mg and 6,100 mg/day, alternatively between 400 mg and 5,100 mg/day, alternatively between 500 mg and 4,100 mg/day.
  • the formulation may be a single daily dose preparation to give in one dose the above intakes, or may be in convenient divided doses, for example, a daily dose formed of two to four soft gelatin or other dosage forms, each containing 300-1500 mg of EPA+DPA or EPA+DPA+HPA in any form embodied in the present invention.
  • Flavourants or emulsifiers may be included, for instance, to make the preparation palatable. Other conventional additives, diluents and excipients may be present.
  • the preparation for ingestion may be in the form of a capsule, a dry powder, a tablet, a solution, an oil, an emulsion or any other appropriate form.
  • the capsules may be hard or soft gelatin capsules, agar capsules, or any other appropriate capsule.
  • the omega-3 fatty acid composition optionally includes chemical antioxidants, such as alpha tocopherol, which are administered in pure form or suspended in a vegetable oil, such as soybean oil or corn oil.
  • chemical antioxidants such as alpha tocopherol
  • the blended fatty acid compositions may then be incorporated into any appropriate dosage form for oral, enteral, parenteral, rectal, vaginal, dermal or other route of administration.
  • Soft or hard gelatin capsules, flavoured oil blends, emulsifiers or other liquid forms, and microencapsulate powders or other dry form vehicles are all appropriate ways of administering the products.
  • the formulated final drug product containing the omega-3 fatty acid composition may be administered to a mammal or patient in need thereof in a capsule, a tablet, a powder that can be dispersed in a beverage, or another solid oral dosage form, a liquid, a soft gel capsule or other convenient dosage form such as oral liquid in a capsule, as known in the art.
  • the capsule comprises a hard gelatin.
  • the combination product may also be contained in a liquid suitable for injection or infusion.
  • Example pharmaceutical grade finished dosage forms (a) Soft or hard gelatin capsules each containing 500 mg or 1000 mg of a mix 20 parts of EPA as a free fatty acid to 1 parts of DPA as a free fatty acid; (b) As in (a) but where the EPA and DPA free fatty acids are replaced with the fatty acids in any other appropriate bioassimilable form such as the ethyl esters; (c) As in (a)-(b) but where the material is in the form of a microencapsulated powder which can be used as a powder or compressed into tablets.
  • Such powders may be prepared by a variety of technologies known to those skilled in the art; (d) As in (a)-(b) but where the formulation is a liquid or emulsion, appropriately flavoured for palatable oral administration; (e) As in (a)-(b) but where the material is formulated into a
  • AFDOCS/l 0582446.1 pharmaceutically acceptable vehicle appropriate for topical application such as a cream or ointment.
  • the omega-3 compositions of the present invention may also be administered with a combination of one or more non-active pharmaceutical ingredients (also known generally herein as "excipients").
  • Non-active ingredients serve to solubilize, suspend, thicken, dilute, emulsify, stabilize, preserve, protect, color, flavor, and fashion the active ingredients into an applicable and efficacious preparation that is safe, convenient, and otherwise acceptable for use.
  • the non-active ingredients may include colloidal silicon dioxide, crospovidone, lactose monohydrate, lecithin, microcrystalline cellulose, polyvinyl alcohol, povidone, sodium lauryl sulfate, sodium stearyl fumarate, talc, titanium dioxide and xanthum gum.
  • pharmaceutically acceptable vehicle includes any of the following: a solution where the first API and optional other ingredients are wholly dissolved in a solubilizer (e.g., a pharmaceutically acceptable solvent or mixture of solvents), wherein the solution remains in clear liquid form at about room temperature; a suspension; an oil; or a semi-solid, wherein the first API and optionally other ingredients are dissolved wholly or partially in a solubilizer (an emulsion, cream, etc.).
  • a solubilizer e.g., a pharmaceutically acceptable solvent or mixture of solvents
  • a "pharmaceutical grade finished dosage form” as used herein may be construed as a unit dose form suitable for administration to, for example, human or animal subjects, and having content uniformity acceptable to regulatory authorities.
  • a pharmaceutical grade finished dosage form should have an amount of API within the range of 85% to 1 15% of the desired dosage and an RSD less than or equal to 6.0%.
  • a pharmaceutical grade finished dosage form must be stable (i.e., have a "shelf life") for a pharmaceutically acceptable duration of time, preferably at least six months, alternatively at least one year,or at least two years, when stored at room temperature (about 23 degree Celcius to 27 degree Celcius , preferably about 25 degree Celcius) and 60% relative humidity.
  • stability is determined by physical appearance and/or chemical modification of the ingredients, in accordance with standards well- known in the pharmaceutical arts, including those documented in ICH guidelines.
  • the omega-3 fatty acid dosage form optionally includes chemical antioxidants, such as alpha tocopherol, oils, such as soybean oil and partially
  • AFDOCS/l 0582446.1 hydrogenated vegetable oil, and lubricants such as fractionated coconut oil, lecithin and a mixture of the same.
  • a composition according to the present prevention is prepared by mixing and homogenizing in a ratio of 98:2 the intermediates MEGAPEX E90D00EE (90% EPA ethyl ester,) and MAXOMEGA DPA95 FFA (>95% DPA synthetic fatty acid produced from EPA ethyl ester concentrate) converted to ethyl ester, respectively.
  • MEGAPEX E90D00EE 90% EPA ethyl ester,
  • MAXOMEGA DPA95 FFA >95% DPA synthetic fatty acid produced from EPA ethyl ester concentrate
  • the resulting novel composition comprises 89.10% EPA, 1 .95% DPA, 0.19% HPA, 91 .24% omega-3-pentaenoic acids, less than 0.01 % DHA, 91 .24% omega-3-pentaenoic acids, 93.09% total omega-3 fatty acids, 3.15% ARA and 3. 57% omega-6 fatty acids (all Area%).
  • a composition according to the present prevention is prepared by mixing and homogenizing in a ratio of 96:4 the intermediates MEGAPEX E90D00EE (90% EPA ethyl ester,) and MAXOMEGA DPA95 FFA (>95% DPA synthetic fatty acid produced from EPA ethyl ester concentrate), converted to ethyl ester, respectively.
  • MEGAPEX E90D00EE 90% EPA ethyl ester,
  • MAXOMEGA DPA95 FFA >95% DPA synthetic fatty acid produced from EPA ethyl ester concentrate
  • MAXOMEGA DPA95 FFA
  • a composition according to the present prevention is prepared by mixing and homogenizing in a ratio of 94:6 the intermediates MEGAPEX E90D00EE (90% EPA
  • the resulting novel composition comprises 85.46% EPA, 5.84% DPA, 0.18% HPA, 91 .48% omega-3-pentaenoic acids, less than 0.01 % DHA, 93.26% total omega-3 fatty acids, 3.02% ARA, and 3.42% omega- 6 fatty acids (all Area%).
  • a composition according to the present prevention is prepared by mixing and homogenizing in a ratio of 75:25 the intermediates MEGAPEX E90D00EE (90% EPA ethyl ester,) and MAXOMEGA DPA95 FFA (>95% DPA synthetic fatty acid produced from EPA ethyl ester concentrate, converted to ethyl ester, respectively.
  • MEGAPEX E90D00EE 90% EPA ethyl ester,
  • MAXOMEGA DPA95 FFA >95% DPA synthetic fatty acid produced from EPA ethyl ester concentrate, converted to ethyl ester, respectively.
  • These intermediates were prepared and commercially offered for sale by Chemport Korea (MEGAPEX) and Equateq Ltd from Scotland, UK (MAXOMEGA).
  • the relative amounts of fatty acids present in the starting intermediates and in the resulting novel composition is listed in table 4 below.
  • the resulting novel composition comprises 68.10% EPA, 24.32% DPA, 0.19% HPA, 92.65% omega-3-pentaenoic acids, less than 0.01 % DHA, 94.07% total omega-3 fatty acids, 2.41 % ARA and 2.73% omega-6 fatty acids (all Area%).
  • a composition according to the present prevention isprepared by mixing and homogenizing in a ratio of 60:40 the intermediates KD-PharmaKD-PUR 900EE and MAXOMEGA DPA95 FFA converted to ethyl ester, respectively. These intermediates were prepared and commercially offered for sale by KD-Pharma Germany (KD-Pharma) and Equateq Ltd from Scotland, UK (MAXOMEGA). The relative amounts of fatty acids present in the starting intermediates and in the resulting novel composition is listed in table 5 below. The resulting novel
  • AFDOCS/l 0582446.1 composition comprises 55.74% EPA, 39.26% DPA, 2.39% HPA, 97.44% omega-3- pentaenoic acids, and 98.06% total omega-3 fatty acids (all Area%).
  • a composition according to the present prevention is prepared by mixing and homogenizing in a ratio of 96:4 the intermediates KD-PUR 900EE KD-Pharma and MAXOMEGA DPA95 FFA converted to ethyl ester, respectively. These intermediates were prepared and commercially offered for sale by KD-Pharma Germany (KD-Pharma) and Equateq Ltd from Scotland, UK (MAXOMEGA).
  • KD-Pharma KD-Pharma
  • Equateq Ltd from Scotland, UK
  • AFDOCS/l 0582446.1 relative amounts of fatty acids present in the starting intermediates and in the resulting novel composition is listed in table 6 below.
  • the resulting novel composition comprises 89.27% EPA, 4.45% DPA, 3.82% HPA, 97.54% omega-3- pentaenoic acids, and 98.54% total omega-3 fatty acids (all Area%).
  • the ethyl ester composition of Example 4 may be converted into a free fatty acid composition with essentially the same fatty acid composition according to
  • AFDOCS/l 0582446.1 the type, degree of saturation or length of fatty acid if performed for an adequate amount of time under the described conditions.
  • Fatty Acid Ethyl Ester (FAEE GMP, approx. 3mmol/g) oil is brought into a closed heated/cooled reaction chamber under nitrogen atmosphere (preferably with pressure control), and heated to 50-60 degree Celcius under stirring.
  • Step 4 Repeat Step 4 several times ( ⁇ 2x) to remove ethanol and NaCI.
  • Example 3 The ethyl ester composition of Example 3 is converted into a free fatty acid composition with essentially the same fatty acid composition according to "Conversion Method EE to FFA" above. This method is indiscriminate with respect to the type, degree of saturation or length of fatty acid if performed for an adequate amount of time under the described conditions.
  • Example 6 The ethyl ester composition of Example 6 is converted into a free fatty acid composition with essentially the same fatty acid composition according to "Conversion Method EE to FFA" above. This method is indiscriminate with respect to the type, degree of saturation or length of fatty acid if performed for an adequate amount of time under the described conditions.
  • Example 4 The composition of Example 4 is formulated into a soft gelatin capsule. Prior to encapsulation, an anti-oxidant preparation (composed of 4000 mg alpha-D- tocopherol in one liter of corn oil; corn oil is a triglyceride low in omega-3) is added to the composition of Example 4, by mixing and homogenizing 100ml_ of this antioxidant preparation into 100 liters of the oil composition of Example 4 followed by thorough homogenization. The resulting pre-encapsulation formulated oil contains approximately 4mg/gram alpha-D-tocopherol.
  • an anti-oxidant preparation composed of 4000 mg alpha-D- tocopherol in one liter of corn oil; corn oil is a triglyceride low in omega-3
  • the resulting pre-encapsulation formulated oil contains approximately 4mg/gram alpha-D-tocopherol.
  • the formulated oil is encapsulated into soft gelatin capsules with printed logo according to general methods typically used by Accucaps in Canada for fish oils or by any other documented and operational encapsulation method.
  • the fill mass of the oil is approximately 1 .08 gram/capsule, providing a dose of approximately 1000mg omega-3-pentaenoic-acids ethyl esters per capsule.
  • the capsules are bottled in HDPE bottles with induction seal and child resistant cap.
  • Example 8 The composition of Example 8 is formulated into a soft gelatin capsule. Prior to encapsulation, an anti-oxidant preparation (composed of 4000 mg alpha-D- tocopherol in one liter of corn oil; corn oil is a triglyceride low in omega-3) is added to the composition of Example 4, by mixing and homogenizing 100ml_ of this anti- Page 53
  • AFDOCS/l 0582446.1 oxidant preparation into 100 liters of the oil composition of Example 4 followed by thorough homogenization.
  • the resulting pre-encapsulation formulated oil contains approximately 4mg/gram alpha-D-tocopherol.
  • the formulated oil is encapsulated into soft gelatin capsules with printed logo according to general methods typically used by Banner in High Point, NC, for fish oils or by any other documented and operational encapsulation method.
  • the fill mass of the oil is approximately 1 .09 gram/capsule, providing a dose of approximately 1000mg omega-3-pentaenoic-acids per capsule.
  • the capsules are bottled in HDPE bottles with induction seal and child resistant cap.
  • Example 5 The composition of Example 5 isjormulated into a soft gelatin capsule. Prior to encapsulation, an anti-oxidant preparation (composed of 4000 mg alpha-D- tocopherol in one liter of corn oil; corn oil is a triglyceride low in omega-3) is added to the composition of Example 4, by mixing and homogenizing 100ml_ of this antioxidant preparation into 100 liters of the oil composition of Example 4 followed by thorough homogenization. The resulting pre-encapsulation formulated oil contains approximately 4mg/gram alpha-D-tocopherol. Subsequently, the formulated oil is encapsulated into soft gelatin capsules with printed logo according to general methods typically used by Catalent in St.
  • an anti-oxidant preparation composed of 4000 mg alpha-D- tocopherol in one liter of corn oil; corn oil is a triglyceride low in omega-3
  • the resulting pre-encapsulation formulated oil contains approximately 4mg/gram alpha-D-tocopherol.
  • the fill mass of the oil is approximately 1 .05 gram/capsule, providing a dose of approximately 1000mg omega-3-pentaenoic-acids ethyl esters per capsule.
  • the capsules are bottled in HDPE bottles with induction seal and child resistant cap.
  • Example 9 The composition of Example 9 isjormulated into a soft gelatin capsule.
  • an anti-oxidant preparation (composed of 4000 mg alpha-D- tocopherol in one liter of corn oil; corn oil is a triglyceride low in omega-3) is added to the composition of Example 4, by mixing and homogenizing 100ml_ of this antioxidant preparation into 100 liters of the oil composition of Example 4 followed by thorough homogenization.
  • the resulting pre-encapsulation formulated oil contains approximately 4mg/gram alpha-D-tocopherol.
  • the formulated oil is encapsulated into soft gelatin capsules with printed logo according to general
  • AFDOCS/l 0582446.1 methods typically used by Banner in High Point, NC, for fish oils or by any other documented and operational encapsulation method.
  • the fill mass of the oil is 1 .06 gram/capsule, providing a dose of approximately 1000mg omega-3-pentaenoic-acids per capsule.
  • the capsules are bottled in HDPE bottles with induction seal and child resistant cap.
  • a patient is diagnosed with severe hypertriglyceridemia (TG>500mg/dL). Thereupon, the patient may be initiated on daily treatment with one of the encapsulated compositions according to Examples 10, 1 1 , 12 or 13. Four capsules per day are administered to this patient (4g/d).
  • a patient is treated as per Example 14.
  • the treatment results in significant reduction of TG as well as non-HDL- and VLDL-cholesterol levels while the LDL- cholesterol level changes insignificantly.
  • a patient is treated as per Example 14. The treatment results in significant reduction of TG as well as ⁇ -HDL-, LDL- and VLDL-cholesterol levels.
  • a patient already undergoing treatment with a statin is diagnosed with high triglycerides (TG between 200 and 500mg/dL). Thereupon, the patient isjnitiated on daily treatment with one of the encapsulated compositions according to Examples 10, 1 1 , 12 or 13. Four capsules per day are administered to this patient (4 g/d).
  • a patient is treated as per Example 17.
  • the treatment results in significant reduction of TG as well as ⁇ -HDL-, VLDL- and LDL-cholesterol levels.
  • a patient is diagnosed with mixed dyslipidemia (TG between 200 and 700 mg/dL and LDL-cholesterol above 190 mg/dL). Thereupon, the patient is initiated on
  • AFDOCS/10582446.1 concomitant daily treatment with a statin and one of the encapsulated compositions according to Examples 10, 1 1 , 12 or 13. Four capsules per day are administered to this patient (4 g/d).
  • a patient is treated as per Example 19.
  • the treatment results in significant reduction of TG as well as ⁇ -HDL-, VLDL- and LDL-cholesterol levels.
  • a patient is diagnosed with mixed dyslipidemia (TG between 200 and 700 mg/dL and non-HDL-cholesterol above 200 mg/dL). Thereupon, the patient is initiated on concomitant daily treatment with a statin and one of the encapsulated compositions according to Examples 10, 1 1 , 12 or 13. Four capsules per day are administered to this patient (4 g/d).
  • a patient is treated as per Example 21 .
  • the treatment results in significant reduction of TG as well as ⁇ -HDL-, VLDL- and LDL-cholesterol levels.
  • a patient is diagnosed to be at significant risk for a cardiovascular event according to the NCEP guidelines and has TG levels above 150mg/dL . Thereupon, the patient is initiated on daily treatment with one of the encapsulated compositions according to Examples 10, 1 1 , 12 or 13. Four capsules per day are administered to this patient (4 g/d).
  • a patient is treated as per Example 23.
  • the treatment results in significant reduction of TG as well as ⁇ -HDL-, VLDL- and LDL-cholesterol levels.
  • a patient diagnosed as per Example 14, 17, 19, 21 or 23 is treated with 3 capsules per day (instead of 4) of one of the encapsulated compositions according to
  • AFDOCS/l 0582446.1 Examples 10, 1 1 , 12 or 13.
  • the treatment results in significant reduction of TG as well as non-HDL- and VLDL-cholesterol levels.
  • a patient diagnosed as per Example 14, 17, 19, 21 or 23 is treated with 3 capsules per day (instead of 4) of one of the encapsulated compositions according to Examples 10, 1 1 , 12 or 13.
  • the treatment results in significant reduction of TG as well as ⁇ -HDL-, VLDL- and LDL-cholesterol levels.
  • a patient diagnosed as per Example 14, 17, 19, 21 or 23 is treated with 2 capsules per day (instead of 3 or 4) of one of the encapsulated compositions according to Examples 10, 1 1 , 12 or 13.
  • the treatment results in significant reduction of TG as well as non-HDL- and VLDL-cholesterol levels.
  • a patient diagnosed as per Example 14, 17, 19, 21 or 23 is treated with 2 capsules per day (instead of 3 or 4) of one of the encapsulated compositions according to Examples 10, 1 1 , 12 or 13.
  • the treatment results in significant reduction of TG as well as ⁇ -HDL-, VLDL- and LDL-cholesterol levels.
  • the EPA: HPA ratio is between 13 and 190, the EPA:DPA ratio is between 8 and 15, the HPA: DPA ration between 0.05 and 1 , the DPA:DHA ratio
  • the EPA, HPA, DPA and DHA may be composed as a glyceride (such as triglyceride), an ester (such as ethyl ester), or a free fatty acid.
  • the EPA: HPA ratio is between 0.25 and 12
  • the DPA:EPA ratio is between 13 and 63
  • the DPA: HPA ration between 13 and 190
  • the EPA:DHA ratio more than 00.6, preferably more than 1 .5, more preferably more than 2.4, most preferably more than 6.
  • the EPA, HPA, DPA and DHA may be composed as a glyceride (such as triglyceride), an ester (such as ethyl ester), or a free fatty acid.
  • the DPA may be composed as a glyceride (such as triglyceride), an ester (such as ethyl ester), or a free fatty acid.
  • a mixture of DPA and EPA was prepared by combining 1g DPA Ethyl Ester (SE-133-III) with 10g EPA Ethyl Ester, 914 mg/g (KD Pharma FM13001 ) in 150ml of 95% ethanol/water containing 35ml of 2M sodium hydroxide. This reaction mixture was stirred overnight at ambient temperature. Tic analysis showed complete conversion of the ethyl esters to the corresponding acids. The reaction mixture was cooled in an ice bath, acidified with 6N hydrochloric acid and concentrated on a rotavap under reduced pressure. Water and ethyl acetate were added, the phases separated and the aqueous residue extracted with ethyl acetate.
  • a DPA testing batch containing roughly 87% DPA ethyl ester was used to study pharmacodynamic effects in the Charles River Zucker fa/fa non-diabetic rat (strain code 185), which is known to diplay characteristics of insulin resistance, glucose intolerance, hyperinsulineamia, obesity and dyslipidemia.
  • All animals were placed on chow + 0.5% cholesterol diet (D13022002: Research Diets, New Brunswick, NJ).
  • Corn oil was used as a diluent for the omega-3 compounds, and methylcellulose to prepare the statin (atorvastatin) for dosing.
  • statin atorvastatin
  • AFDOCS/l 0582446.1 at 50 mg/kg, 200 mg/kg, 400 mg/kg, and 1000 mg/kg. Animals were dosed daily for 14 days. For reference, a rat dose of 400 mg/kg would be equivalent to a human daily dose of approximately 4 grams (as shown in Reagan-Shaw et al. "Dose translation from animal to human studies revisited," FASEB J. 22, 659-661 (2007), which is incorporated by reference in its entirety).
  • the second phase was initiated on day 15, with the group receiving DPA 400 mg/kg solution being co-administered statin at 10 mg/kg.
  • Another group previously dosed with corn oil vehicle, receive atorvastatin to serve as an appropriate control.
  • This second phase consisted of 14 days of daily, oral administration.
  • Plasma total cholesterol, LDL, HDL, VLDL, triglycerides and NEFA non- esterified free fatty acids
  • Plasma total cholesterol, LDL, HDL, VLDL, triglycerides and NEFA non- esterified free fatty acids
  • Plasma total cholesterol, LDL, HDL, VLDL, triglycerides and NEFA non- esterified free fatty acids
  • levels of lipid parameters are determined in a 96-well multiplexed system using standard clinical chemistry techniques. Non-HDL cholesterol is calculated by subtracting the HDL value from the total cholesterol value.
  • insulin levels are determined at day 28.
  • FIG. 1 shows the fasting plasma lipid values after seven days of dosing.
  • FIG. 2 shows the fasting plasma insulin levels after 28 days of administration.
  • HMGCoA 3-hydroxy-3-methylglutaryl-coenzyme A; key regulatory enzyme for new cholesterol biosynthesis
  • PCSK9 pro-protein convertase subtilisin kexin 9; associated with LDL receptor functioning and increased levels of LDL
  • SREB-2 sterol regulatory enhancing binding protein 2; regulates transcription of a wide variety of genes involved with new cholesterol synthesis
  • the mRNA messenger RNA
  • cDNA complementary DNA
  • FIG. 3 shows the relative liver gene expression following 28 days of administration.
  • Inclusion criteria for tested subjects include volunteers between ages 18-65, with a BMI of 30-35 (alternatively a BMI of 27-35) and triglyceride levels less than 350 mg/dL, who consume no more than 1 fish meal per week and who are not currently prescribed pharmaco-therapy for lowering triglycerides, including but not limited to fibrates, omega-3 agents, and niacin. Volunteers on stable anti-hypertensive, anti-diabetic and thyroid therapy re allowed for consideration. Any person on stable statin therapy is considered if their triglyceride levels are less than 350 mg/dL. However, the total composition of subjects in the study with this particular profile is limited to no more than 30%.
  • COMPOSITION 1 or the reference compound are dosed at approximately 4 grams/day in the morning by administration of 4 capsules containing approximately 1 gram of each compound.
  • volunteers are housed at the testing facility in order to ensure well- controlled experimental conditions.
  • Plasma levels of omega-3 fatty acids of interest from the study are determined utilizing an analytical LC/MS technique under GLP laboratory conditions in order to determine Cmax, Tmax and AUC for the omega-3 fatty acids of interest, including EPA, DPA, HPA, DHA, and other omega-3 fatty acids.
  • COMPOSITION 1 has a better bioavalability (as measured by AUC and Cmax) than the reference compound. This effect is seen under fasting and/or fed administration conditions.
  • this Study #2 is conducted with a certain dose level of COMPOSITION 2 OR COMPOSITION 3 instead of COMPOSITION 1 .
  • This Phase 3, multi-center study consists of a 6- to 8-week screening/washout period (to include a diet and lifestyle stabilization period), which includes a fasting triglyceride (TG) qualifying period of 2-3 weeks, followed by a 12- week double-blind treatment period.
  • Patients on statin therapy (with or without ezetimibe) at screening are evaluated by the investigator as to whether this therapy could be safely discontinued at screening, or if it is to be continued. Patients on any other dyslipidemia therapy need to discontinue these in order to qualify for the study. If statin therapy (with or without ezetimibe) is to be continued, dose(s) must be stable for >4 weeks prior to the fasting TG baseline qualifying measurements for randomization.
  • the screening visit is to occur at either 6 weeks before randomization for patients not on lipid-altering therapy at screening or for patients
  • the population for this study is men and women >18 years of age with a body mass index (BMI) ⁇ 45 kg/m2. Patients on lipid-lowering therapy and patients not on lipid-lowering therapy are eligible to enroll in the study. Patients had to have an average TG level >500 mg/dL and ⁇ 2000 mg/dL during the screening period to be eligible for randomization.
  • BMI body mass index
  • COMPOSITION 1 at a approximately 2 g daily dose, approximately 3 g daily dose and approximately 4 g daily dose, compared to placebo, in lowering fasting TG levels in patients with fasting TG levels >500 mg/dL and ⁇ 2000 mg/dL
  • HDL-C very low-density lipoprotein cholesterol
  • VLDL-C very low-density lipoprotein cholesterol
  • apo B apolipoprotein B
  • apo A-l/apo B ratio lipoprotein(a)
  • Lp[a] lipoprotein(a)
  • Lp-PLA2 lipoprotein-associated phospholipase A2
  • AFDOCS/l 0582446.1 [0219] 4. To determine the effect of COMPOSITION 1 on low-density lipoprotein (LDL) particle number and size, on oxidized LDL and on C-reactive protein (CRP).
  • LDL low-density lipoprotein
  • CRP C-reactive protein
  • ICM-1 intracellular adhesion molecule-1
  • VCAM_1 vascular cell adhesion molecule 1
  • IL-1 ⁇ interleukin-1 ⁇
  • IL-2 interleukin-2
  • IL-6 interleukin-6
  • IL-8 interleukin-8
  • IL-10 interleukin-10
  • IL-12 interleukin-12
  • IL-15 interleukin-15
  • IL-18 interleukin-18
  • TNF-a tumor necrosis factor-alpha
  • TNF- ⁇ tumor necrosis factor-beta
  • PAI-1 plasminogen activator inhibitor-1
  • the primary efficacy variable for the double-blind treatment period is percent change in fasting TG from baseline to the Week 12 endpoint.
  • the secondary efficacy variable for the double-blind treatment period includes the following: Percent changes in fasting Non-HDL-C, LDL-C, VLDL-C, HDL-C, Lp-PLA2, and apo B from baseline to Week 12 endpoint.
  • the primary and secondary efficacy analyses will be performed using an analysis of covariance (ANCOVA) model with treatment, gender, and the use of statin therapy at randomization as factors and baseline fasting TG value as a covariate.
  • ANCOVA analysis of covariance
  • this Study #3 is conducted with one or more dose levels of COMPOSITION 2 OR 3 instead of COMPOSITION 1 .
  • This multi-center study consists of a 4- to 6-week screening and washout period (to include a diet and lifestyle stabilization period, and to wash-out any non- statin/ezetimibe dyslipidemia medications), which also includes a 2-3 week fasting triglyceride (TG) level qualifying period, followed by a 6- to 12-week double-blind treatment period.
  • Patients on statin therapy (with or without ezetimibe) at screening are evaluated by the investigator as to whether this therapy does maintain low- density lipoprotein (LDL) levels of >40 mg/dl and ⁇ 100 mg/dl.
  • LDL low- density lipoprotein
  • statin therapy (with or without ezetimibe) is to be initiated, in those patients who are not on statin therapy in order to achieve LDL levels of >40 mg/dl and ⁇ 100 mg/dl .
  • Dose(s) of statin therapy must be stable for >4 weeks prior to the TG baseline qualifying measurements for randomization.
  • the population for this study is men and women >18 years of age with a body mass index (BMI) ⁇ 45 kg/m2. Patients on lipid-lowering therapy and patients
  • AFDOCS/l 0582446.1 not on lipid-lowehng therapy are eligible to enroll in the study. Patients had to have an average fasting TG level >200 mg/dL and ⁇ 499 mg/dL during the qualifying period to be eligible for randomization.
  • eligible patients will enter a 6- to 12-week randomized, double-blind treatment period.
  • patients will be randomly assigned to one of the following treatment groups: COMPOSITION 1 at an approximately 2 gram daily dose, COMPOSITION 1 at an approximately 3 gram daily dose, COMPOSITION 1 at an approximately 4 gram daily dose, or placebo.
  • the daily dose may be taken as either a single dose or distributed over two doses per day.
  • the primary objective of the study is to determine the efficacy of COMPOSITION 1 at approximately 2 grams daily, approximately 3 grams daily and approximately 4 grams daily, compared to placebo, in lowering fasting TG levels in statin-treated patients with fasting TG levels >200 mg/dL and ⁇ 499 mg/dL.
  • the secondary and exploratory objectives of the study may include but are not limited to the following objectives:
  • TC total cholesterol
  • non-HDL-C non-high-density lipoprotein cholesterol
  • LDL-C low-density lipoprotein cholesterol
  • HDL-C high-density lipoprotein cholesterol
  • VLDL-C very low-density lipoprotein cholesterol
  • ICM-1 intracellular adhesion molecule-1
  • VCAM_1 vascular cell adhesion molecule 1
  • IL-1 ⁇ interleukin-2
  • IL-6 interleukin-6
  • IL-8 interleukin-8
  • interleukin-10 interleukin-10
  • IL-12 interleukin-12
  • IL-15 interleukin-15
  • IL-18 interleukin-18
  • TNF-a tumor necrosis factor-alpha
  • TNF- ⁇ tumor necrosis factor-beta
  • PAI-1 plasminogen activator inhibitor-1
  • the primary efficacy variable for the double-blind treatment period is percent change in fasting TG from baseline to the Week 6 to 12 endpoint.
  • the secondary efficacy variable for the double-blind treatment period include but are not limited to the following: Percent changes in fasting Non-HDL-C, LDL-C, VLDL-C, HDL-C, Lp-PLA2, and apo B from baseline to Week 6 to 12 endpoint.
  • the primary and secondary efficacy analyses will be performed using an analysis of covariance (ANCOVA) model with treatment, gender, the type of statin therapy and diagnosis of diabetes at randomization as factors and baseline fasting TG value as a covariate.
  • ANCOVA analysis of covariance
  • this Study #4 is conducted with one or more dose levels of COMPOSITION 2 OR 3 instead of COMPOSITION 1 .
  • Study #4 is conducted, enrolling patients with a baseline triglyceride level of about 300 to 499 mg/dL or about 350 too 400 mg/dL, instead of 200 to 499 mg/dL.
  • Inclusion criteria for tested subjects include volunteers between ages 18-65, with a BMI of 30-35 (alternatively a BMI of 27-35) and triglyceride levels less than 350 mg/dL, who consume no more than 1 fish meal per week and who are not currently prescribed pharmaco-therapy for lowering triglycerides, including but not limited to fibrates, omega-3 agents, and niacin. Volunteers on stable anti-hypertensive, antidiabetic and thyroid therapy re allowed for consideration. Any person on stable statin therapy is considered if his or her triglyceride levels are less than 350 mg/dL. However, the total composition of subjects in the study with this particular profile is limited to no more than 30%.
  • AFDOCS/l 0582446.1 other than acetaminophen are asked to abstain and switch to acetaminophen for relief of pain, or are excluded from study consideration. Subjects are excluded if they receive any type of hormone therapy, weight loss agents, HIV therapy, beta- blockers, or are diagnosed with known cardiovascular disease, including heart failure, arrhythmia, any incidence of acute coronary syndrome, myocardial infarct, coronary artery bypass graft surgery, and/or angioplasty.
  • COMPOSITION 1 or the reference compound are dosed at approximately 4 grams/day in the morning by administration of 4 capsules containing 1 gram of each compound.
  • Baseline plasma levels of fasting serum triglycerides are determined on day 1 and just prior to initiation and completion of either the fasting or fed multi-dosing period. Additional lipid and other parameters (see below under “Results”) that are analyzed included total cholesterol, LDL, HDL, VLDL, non-HDL, and NEFA as previously described.
  • COMPOSITION 1 has a better fasting triglyceride lowering effect than the reference compound. This effect is seen under fasting and/or fed administration conditions.
  • Administration of COMPOSITION 1 have a beneficial effect, versus baseline and versus the reference compound, on other lipid parameters (such as HDL cholesterol, total cholesterol, non-HDL cholesterol, VLDL cholesterol), on platelet function, and one or more of the following: apolipoprotein A-l (apo A-l), apolipoprotein B (apo B), apo A-l/apo B ratio, lipoprotein(a) (Lp[a]), lipoprotein-associated phospholipase A2 (Lp-PLA2), low density lipoprotein (LDL) particle number and size, oxidized LDL, C-reactive protein (CRP), high sensitivity C- reactive protein (HSCRP), intracellular adhesion molecule-1 (ICAM-1 ), E-selectin, P- selectin
  • COMPOSITION 1 has a beneficial impact, or a minimal impact, or no impact, on other non-HDL lipid parameters, such as LDL cholesterol versus baseline and the reference compound.
  • this Study #5 is conducted with a certain dose level of COMPOSITION 2 OR COMPOSITION 3 instead of COMPOSITION 1 .
  • a fatty acid composition comprising at least 50% omega-3-fatty acids, salts or derivatives thereof, while comprising eicosapentaenoic acid (EPA; C20:5-n3) and docosapentaenoic acid (DPA; C22:5-n3) and wherein the EPA:DHA ratio is higher than 20:1 .
  • EPA eicosapentaenoic acid
  • DPA docosapentaenoic acid
  • a fatty acid composition comprising at least 60% omega-3-fatty acids, salts or derivatives thereof, while comprising eicosapentaenoic acid (EPA; C20:5-n3) and docosapentaenoic acid (DPA; C22:5-n3) and wherein the EPA:DHA ratio is higher than 20:1 .
  • EPA eicosapentaenoic acid
  • DPA docosapentaenoic acid
  • a fatty acid composition comprising at least 70% omega-3-fatty acids, salts or derivatives thereof, while comprising eicosapentaenoic acid (EPA; C20:5-n3) and docosapentaenoic acid (DPA; C22:5-n3) and wherein the EPA:DHA ratio is higher than 20:1 .
  • EPA eicosapentaenoic acid
  • DPA docosapentaenoic acid
  • a fatty acid composition comprising at least 75% omega-3-fatty acids, salts or derivatives thereof, while comprising eicosapentaenoic acid (EPA; C20:5-n3) and docosapentaenoic acid (DPA; C22:5-n3) and wherein the EPA:DHA ratio is higher than 20:1 .
  • EPA eicosapentaenoic acid
  • DPA docosapentaenoic acid
  • a fatty acid composition comprising at least 80% omega-3-fatty acids, salts or derivatives thereof, while comprising eicosapentaenoic acid (EPA; C20:5-n3) and docosapentaenoic acid (DPA; C22:5-n3) and wherein the EPA:DHA ratio is higher than 20:1 .
  • EPA eicosapentaenoic acid
  • DPA docosapentaenoic acid
  • a fatty acid composition comprising at least 85% omega-3-fatty acids, salts or derivatives thereof, while comprising eicosapentaenoic acid (EPA; C20:5-n3) and docosapentaenoic acid (DPA; C22:5-n3) and wherein the EPA:DHA ratio is higher than 20:1 .
  • EPA eicosapentaenoic acid
  • DPA docosapentaenoic acid
  • a fatty acid composition comprising at least 90% omega-3-fatty acids, salts or derivatives thereof, while comprising eicosapentaenoic acid (EPA; C20:5-n3) and docosapentaenoic acid (DPA; C22:5-n3) and wherein the EPA:DHA ratio is higher than 20:1 .
  • EPA eicosapentaenoic acid
  • DPA docosapentaenoic acid
  • a fatty acid composition comprising at least 95% omega-3-fatty acids, salts or derivatives thereof, while comprising eicosapentaenoic acid (EPA; C20:5-n3) and docosapentaenoic acid (DPA; C22:5-n3) and wherein the EPA:DHA ratio is higher than 20:1 .
  • EPA eicosapentaenoic acid
  • DPA docosapentaenoic acid
  • AFDOCS/l 0582446.1 9. A composition according to one of the preferred embodiments 1 through 8, comprising at least 2% docosapentaenoic acid (DPA; C22:5-n3).
  • DPA docosapentaenoic acid
  • composition according to one of the preferred embodiments 1 through 8 comprising at least 4% docosapentaenoic acid (DPA; C22:5-n3).
  • composition according to one of the preferred embodiments 1 through 8 comprising at least 5% docosapentaenoic acid (DPA; C22:5-n3).
  • DPA docosapentaenoic acid
  • DPA docosapentaenoic acid
  • DPA docosapentaenoic acid
  • composition according to one of the preferred embodiments 1 through 8 comprising at least 8% docosapentaenoic acid (DPA; C22:5-n3).
  • composition according to one of the preferred embodiments 1 through 8 comprising at least 10% docosapentaenoic acid (DPA; C22:5-n3).
  • DPA docosapentaenoic acid
  • DPA docosapentaenoic acid
  • composition according to one of the preferred embodiments 1 through 8 comprising at least 15% docosapentaenoic acid (DPA; C22:5-n3).
  • DPA docosapentaenoic acid
  • composition according to one of the preferred embodiments 1 through 17, comprising no more than 95% EPA.
  • composition according to one of the preferred embodiments 1 through 17, comprising no more than 10% omega-6 fatty acids.
  • composition according to one of the preferred embodiments 1 through 17, comprising no more than 7% omega-6 fatty acids.
  • composition according to one of the preferred embodiments 1 through 17, comprising no more than 3% omega-6 fatty acids.
  • composition according to one of the preferred embodiments 1 through 22, comprising no more than 5% arachidonic acid (C22:4-n6).
  • composition according to one of the preferred embodiments 1 through 22, comprising no more than 4% arachidonic acid (C22:4-n6).
  • composition according to one of the preferred embodiments 1 through 22, comprising no more than 3% arachidonic acid (C22:4-n6).
  • AFDOCS/10582446.1 26 A composition according to one of the preferred embodiments 1 through 22, comprising no more than 2% arachidonic acid (C22:4-n6).
  • composition according to one of the preferred embodiments 1 through 22, comprising no more than 1 % arachidonic acid (C22:4-n6).
  • composition according to one of the preferred embodiments 1 through 27, comprising at least 0.01 % heneicosapentaenoic acid (C21 :5-n3).
  • composition according to one of the preferred embodiments 1 through 27, comprising at least 0.1 % heneicosapentaenoic acid (C21 :5-n3).
  • composition according to one of the preferred embodiments 1 through 27, comprising at least 0.3% heneicosapentaenoic acid (C21 :5-n3).
  • composition according to one of the preferred embodiments 1 through 27, comprising at least 0.5% heneicosapentaenoic acid (C2 :5-n3).
  • composition according to one of the preferred embodiments 1 through 27, comprising at least 1 % heneicosapentaenoic acid (C21 :5-n3).
  • composition according to one of the preferred embodiments 1 through 27, comprising at least 2% heneicosapentaenoic acid (C21 :5-n3).
  • composition according to one of the preferred embodiments 1 through 27, comprising at least 3% heneicosapentaenoic acid (C21 :5-n3).
  • composition according to one of the preferred embodiments 1 through 27, comprising at least 4% heneicosapentaenoic acid (C21 :5-n3).
  • composition according to one of the preferred embodiments 1 through 27, comprising at least 5% heneicosapentaenoic acid (C21 :5-n3).
  • composition according to one of the preferred embodiments 1 through 37 comprising no more than 5% omega-3 fatty acids that are not omega-3- pentaenoic acids.
  • composition according to one of the preferred embodiments 1 through 37 comprising no more than 4% omega-3 fatty acids that are not omega-3- pentaenoic acids.
  • composition according to one of the preferred embodiments 1 through 37 comprising no more than 3% omega-3 fatty acids that are not omega-3- pentaenoic acids.
  • composition according to one of the preferred embodiments 1 through 37 comprising no more than 1 .5% omega-3 fatty acids that are not omega-3- pentaenoic acids.
  • composition according to one of the preferred embodiments 1 through 37 comprising no more than 1 .25% omega-3 fatty acids that are not omega-3- pentaenoic acids.
  • composition according to one of the preferred embodiments 1 through 37 comprising no more than 1 % omega-3 fatty acids that are not omega-3- pentaenoic acids.
  • composition according to one of the preferred embodiments 1 through 44 comprising between 65% and 95% EPA.
  • composition according to one of the preferred embodiments 1 through 44 comprising between 75% and 95% EPA.
  • composition according to one of the preferred embodiments 1 through 44 comprising between 90% and 95% EPA.
  • composition according to one of the preferred embodiments 1 through 44 comprising between 2% and 10% DPA.
  • composition according to one of the preferred embodiments 1 through 44 comprising between 3% and 20% DPA.
  • composition according to one of the preferred embodiments 1 through 44 comprising between 3% and 75% DPA.
  • composition according to one of the preferred embodiments 1 through 44 comprising between 3% and 90% DPA.
  • a pharmaceutically suitable formulation comprising one of the compositions according to preferred embodiments 94 through 98, in which the amount of eicosapentaenoic acid plus docosapentaenoic acid is present in an amount between 100 and 10,000 mg.
  • a pharmaceutically suitable formulation or dosage form comprising one of the compositions according to preferred embodiments 94 through 98, in which the amount of eicosapentaenoic acid plus docosapentaenoic acid is present in an amount between 250 and 1 ,250 mg.
  • a pharmaceutically suitable formulation or dosage form comprising one of the compositions according to preferred embodiments 94 through 98, in which the amount of eicosapentaenoic acid plus docosapentaenoic acid is present in an amount between 500 and 1 ,100 mg.
  • a pharmaceutically suitable formulation or dosage form comprising one of the compositions according to preferred embodiments 94 through 98, in which the
  • AFDOCS/l 0582446.1 amount of eicosapentaenoic acid plus docosapentaenoic acid is present in an amount between 100 and 10,000 mg.
  • a method of treatment according to preferred embodiments 103 through 105 in which the subject is a patient already undergoing treatment with a statin and then diagnosed with high triglycerides (equal to or more than 200 mg/dL but less than 500 mg/dL).
  • AFDOCS/l 0582446.1 1 13 A method of treatment according to preferred embodiments 103 through 105, in which the subject is a patient diagnosed with mixed dyslipidemia with TG 200- 499 mg/dL and LDL-cholesterol equal to or more than 160 mg/dL.
  • AFDOCS/l 0582446.1 124 A method of treatment according to one of the preferred embodiments 103 through 123, in which the treatment results in significant reduction of blood, serum or plasma triglyceride levels.
  • AFDOCS/l 0582446.1 134 A method of treatment according to one of the preferred embodiments 103 through 123, in which the treatment results in significant reduction of blood, serum or plasma hs-CRP levels.

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Abstract

La présente invention concerne des procédés de réduction de paramètres lipidiques, tels que les triglycérides, le cholestérol total, le cholestérol à lipoprotéine de faible densité (LDL), le cholestérol non HDL, les acides gras libres et d'autres lipides, comprenant l'administration d'acide docosapentaénoïque oméga-3.
EP13861305.4A 2012-12-06 2013-12-06 Procédés d'administration de compositions comprenant de l'acide docosapentaénoïque Withdrawn EP2928462A4 (fr)

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US201261734331P 2012-12-06 2012-12-06
US201361780948P 2013-03-13 2013-03-13
PCT/US2013/073714 WO2014089511A2 (fr) 2012-12-06 2013-12-06 Procédés d'administration de compositions comprenant de l'acide docosapentaénoïque

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EP21170003.4A Withdrawn EP3888646A1 (fr) 2012-12-06 2013-12-06 Compositions d'acide oméga-3 pentaénoïque et procédés d'utilisation
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JP2018168139A (ja) * 2016-10-21 2018-11-01 マルハニチロ株式会社 n−3系不飽和脂肪酸を含む中性脂肪値の低減または上昇抑制用の組成物、並びに該組成物の製造におけるn−3系不飽和脂肪酸の使用
JP7099821B2 (ja) * 2017-12-20 2022-07-12 ポッカサッポロフード&ビバレッジ株式会社 Pcsk9阻害剤及びコレステロール代謝改善用食品組成物
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AU2021201865A1 (en) 2021-04-22
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KR20150103009A (ko) 2015-09-09
AU2019216634A1 (en) 2019-09-05
EP2929041A1 (fr) 2015-10-14
AU2013354979A1 (en) 2015-06-11
AU2017232203A1 (en) 2017-10-12
CA2894366A1 (fr) 2014-06-12
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MX2015007082A (es) 2016-01-12
AU2018229440A1 (en) 2018-10-04
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JP2019172697A (ja) 2019-10-10
KR20210059779A (ko) 2021-05-25
JP2021120407A (ja) 2021-08-19
CN104902888A (zh) 2015-09-09
WO2014089501A1 (fr) 2014-06-12
KR20150103671A (ko) 2015-09-11
EP3888646A1 (fr) 2021-10-06
CA2894183A1 (fr) 2014-06-12
JP6881893B2 (ja) 2021-06-02
CN113274378A (zh) 2021-08-20
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