US20090110729A1 - Solid oral compositions based on s-adenosyl methionine and/or nadh and process for obtaining them - Google Patents

Solid oral compositions based on s-adenosyl methionine and/or nadh and process for obtaining them Download PDF

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US20090110729A1
US20090110729A1 US12/240,002 US24000208A US2009110729A1 US 20090110729 A1 US20090110729 A1 US 20090110729A1 US 24000208 A US24000208 A US 24000208A US 2009110729 A1 US2009110729 A1 US 2009110729A1
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Daniele Giovannone
Carlo De Angelis
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Gnosis SpA
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/70Carbohydrates; Sugars; Derivatives thereof
    • A61K31/7042Compounds having saccharide radicals and heterocyclic rings
    • A61K31/7052Compounds having saccharide radicals and heterocyclic rings having nitrogen as a ring hetero atom, e.g. nucleosides, nucleotides
    • A61K31/706Compounds having saccharide radicals and heterocyclic rings having nitrogen as a ring hetero atom, e.g. nucleosides, nucleotides containing six-membered rings with nitrogen as a ring hetero atom
    • A61K31/7064Compounds having saccharide radicals and heterocyclic rings having nitrogen as a ring hetero atom, e.g. nucleosides, nucleotides containing six-membered rings with nitrogen as a ring hetero atom containing condensed or non-condensed pyrimidines
    • A61K31/7076Compounds having saccharide radicals and heterocyclic rings having nitrogen as a ring hetero atom, e.g. nucleosides, nucleotides containing six-membered rings with nitrogen as a ring hetero atom containing condensed or non-condensed pyrimidines containing purines, e.g. adenosine, adenylic acid
    • 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
    • A61K31/495Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with two or more nitrogen atoms as the only ring heteroatoms, e.g. piperazine or tetrazines
    • A61K31/505Pyrimidines; Hydrogenated pyrimidines, e.g. trimethoprim
    • A61K31/519Pyrimidines; Hydrogenated pyrimidines, e.g. trimethoprim ortho- or peri-condensed with heterocyclic rings
    • A61K31/52Purines, e.g. adenine
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/70Carbohydrates; Sugars; Derivatives thereof
    • A61K31/7084Compounds having two nucleosides or nucleotides, e.g. nicotinamide-adenine dinucleotide, flavine-adenine dinucleotide
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/0002Galenical forms characterised by the drug release technique; Application systems commanded by energy
    • A61K9/0007Effervescent
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/2004Excipients; Inactive ingredients
    • A61K9/2009Inorganic compounds
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/2095Tabletting processes; Dosage units made by direct compression of powders or specially processed granules, by eliminating solvents, by melt-extrusion, by injection molding, by 3D printing
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/28Dragees; Coated pills or tablets, e.g. with film or compression coating
    • A61K9/2806Coating materials
    • A61K9/282Organic compounds, e.g. fats
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • A61P25/24Antidepressants

Definitions

  • SAMe S-adenosyl methionine
  • This substance therefore has a very important biological role and is essentially used in clinical practice as an antidepressant.
  • SAMe is meant both the racemic mixture and the individual diastereoisomers (RS)-(+)-S-adenosyl-L-methionine [(RS)-(+)-SAMe)] and (SS)-(+)-S-adenosyl-L-methionine [(SS)-(+)-SAMe)], as well as mixtures other than the racemic mixture.
  • S-adenosyl methionine as a drug and/or dietetic is however known because it is extremely unstable at temperatures above 0° C. or in the presence of moisture, through both degradation of the active ingredient, understood to be the sum of the two diastereoisomers, and through the conversion of active (SS)-(+)-S-adenosyl-L-methionine to inactive (RS)-(+)-S-adenosyl-L-methionine (racemisation of the substance).
  • Italian Patent no. 829906 describes a process for the preparation of pharmaceutically acceptable salts of (SS,RS)-S-adenosyl-L-methionine with quantities of inactive diastereoisomer (RS)-(+)-S-adenosyl-L-methionine of 3% or less with respect to the active diastereoisomer (SS)-(+)-S-adenosyl-L-methionine of 97% or more.
  • SS,RS diastereoisomer SS-(+)-S-adenosyl-L-methionine
  • the patent confirms that although more than 97% of active S,S diastereoisomer is obtained at ambient temperature, the racemic mixture is unstable over time, with conversion of the (SS)-(+)-S-adenosyl-L-methionine into (RS)-(+)-S-adenosyl-L-methionine in a relatively short time.
  • FIG. 1 represents a graph illustrating the water absorption capacity of several materials over time.
  • FIG. 2 illustrates the water absorbency of several materials at a varying Relative Humidity.
  • U.S. Pat. Nos. 13,627, 663,943, 98,102 and 354,263 describe a method for stabilising pharmaceutically acceptable salts of S-adenosyl methionine comprising S-adenosyl methionine paratoluene sulphonate, S-adenosyl methionine-1,4-butene disulphonate, S-adenosyl methionine sulphate, S-adenosyl methionine tosylate with a group of substances comprising chitosan, dextrin, carboxymethylcellulose, fumaric acid, azelaic acid and tryptophan.
  • the rate of racemisation of SAMe as a salt of S-adenosyl methionine paratoluene sulphonate differs from the racemisation of SAMe in the form of S-adenosyl methionine-1,4-butene disulphonate salt, or S-adenosyl methionine sulphate or as S-adenosyl methionine tosylate.
  • formulations based on S-adenosyl methionine reflect the abovementioned instability and racemisation of the active ingredient, (conversion of the active S,S diastereoisomer into the inactive R,S diastereoisomer), with obvious adverse repercussions for the preservation and storage of the material, even for short periods of time.
  • U.S. Pat. Nos. 3,954,726 and 4,057,672 describe relatively stable salts of S-adenosyl methionine, that is up to 25° C. and 45° C., respectively.
  • U.S. Pat. No. 4,465,672 also describes stable salts of S-adenosyl methionine with 5 mols of a sulphonic acid with a pK of less than 2.5.
  • the process of preparing the product comprises preparation of a concentrated aqueous solution of an impure salt of SAMe, purification of the solution and its elution with a dilute aqueous solution of the preselected sulphonic acid, titration of the resulting eluate, concentration and lyophilisation or spraying.
  • NADH is an active ingredient normally used as an energising agent and antioxidant.
  • compositions based on NADH such as those for example described in U.S. Pat. Nos. 5,332,727 and 7,034,011 are based on stabilising the active ingredient through association with other antioxidants.
  • Calcium oxide and/or hydroxide directly mixed with atomised SAMe and/or NADH powder, or with solid formulations based on SAMe and/or NADH, are successful in removing water through a chemical reaction with the powder or the preparation itself.
  • Calcium oxide is instead a natural desiccant with very high reactivity in relation to water. It reacts with it and changes to a calcium hydroxide, eliminating it permanently in preparations.
  • FIG. 1 shows the rate of absorption of H 2 O with different absorbent substances including calcium oxide.
  • FIG. 2 shows the absorption capacity for water vapour of various desiccants as the environmental humidity (RH) varies.
  • Table 1 summarises the absorbent capacities of various desiccants under different relative humidity and temperature conditions.
  • Table 2 provides moisture content values for five lots of starting material of SAMe (S-adenosyl methionine paratoluene sulphonate) with its corresponding analysis prior to mixing with calcium oxide and storage at 20° C. for 21 days, and the relative accelerated stability at 53° C. for 5 days.
  • Table 3 shows moisture content values for five lots of starting material of SAMe (S-adenosyl methionine paratoluene sulphonate) with its corresponding analysis after mixing with calcium oxide and storage at 20° C. for 21 days, and the relative accelerated stability at 53° C. for 5 days.
  • SAMe S-adenosyl methionine paratoluene sulphonate
  • Table 4 shows moisture content values for five lots of starting material of SAMe (S-adenosyl methionine-1,4-butene disulphonate) with corresponding analysis prior to mixing with calcium oxide and storage at 20° C. for 21 days, and the relative accelerated stability at 53° C. for 5 days.
  • SAMe S-adenosyl methionine-1,4-butene disulphonate
  • Table 5 shows moisture content values for five lots of starting material of SAMe (S-adenosyl methionine-1,4-butene disulphonate) with corresponding analysis after mixing with calcium oxide and storage for 23° C. for 21 days, and the relative accelerated stability at 53° C. for 5 days.
  • SAMe S-adenosyl methionine-1,4-butene disulphonate
  • Table 6 shows moisture content values for five lots of starting material of NADH with corresponding analysis prior to mixing with calcium oxide and storage at 20° C. for 21 days, and the relative accelerated stability at 53° C. for 5 days.
  • Table 7 shows moisture content values for five lots of starting material of NADH with corresponding analysis after mixing with calcium oxide and storage at 20° C. for 21 days, and the relative accelerated stability at 53° C. for 5 days.
  • one object of this invention relates to compositions comprising SAMe and/or NADH, or their salts, in association with calcium oxide and/or calcium hydroxide, and optionally pharmaceutically acceptable excipients.
  • SAMe is meant both the racemic mixture and the individual (RS)-(+)-S-adenosyl-L-methionine [(RS)-(+)-SAMe)] and (SS)-(+)-S-adenosyl-L-methionine [(SS)-(+)-SAMe)] diastereoisomers, including the mixtures other than the racemic mixture.
  • compositions according to this invention contain SAMe, or its salts, in a quantity of between 30 and 90% by weight, preferably between 50 and 85% by weight, with respect to the weight of the composition, in association with calcium oxide and/or calcium hydroxide in a quantity of between 1 and 40% by weight, preferably between 2 and 20% by weight, with respect to the weight of the composition.
  • compositions according to this invention contain NADH, or its salts, in a quantity between 1 and 90% by weight, preferably between 5 and 50% by weight, with respect to the weight of the composition, in association with calcium oxide and/or calcium hydroxide in a quantity of between 1 and 40% by weight, preferably between 2 and 20% by weight, with respect to the weight of the composition.
  • the said SAMe, or its salts is S-adenosyl methionine paratoluene sulphonate, S-adenosyl methionine-1,4-butene disulphonate, S-adenosyl methionine sulphate, S-adenosyl methionine tosylate.
  • the NADH is present in the form of its pharmaceutically acceptable salts.
  • the said calcium oxide and/or calcium hydroxide is calcium oxide alone, calcium hydroxide alone, or a mixture thereof.
  • the pharmaceutically acceptable excipients used according to this invention are preferably selected from calcium sulphate hemihydrate, magnesium oxide, malic acid, glutamic acid, glucono-delta-lactone, xylitol and/or their mixtures.
  • compositions according to this invention may optionally comprise at least one further active ingredient, preferably selected from melatonin, 1-theanine and/or 1-tryptophan and/or 5-hydroxytryptophan and/or their mixtures.
  • compositions according to this invention may be in the form of a direct mixture, tablets, capsules, granules and/or powder.
  • direct mixture is meant a mixture of atomised powder of SAMe and/or NADH, or their salts, in association with calcium oxide and/or calcium hydroxide alone, without the addition of other excipients.
  • compositions according to this invention are in the form of tablets, more preferably in the form of ordinary, coated, film-coated and/or gastroresistant tablets.
  • ordinary tablet is meant a tablet obtained by direct compression or compression after granulation without coating
  • coated tablet is meant a tablet coated with non-gastroresistant substances
  • film-coated tablet is meant a coated tablet which is further covered with water-based varnishes, which varnishes may have a gastroresistant action.
  • compositions according to this invention may be film-coated with water-based varnishes preferably selected from gum Lac (ShellacTM) and/or its salts, methacrylic acid, cellulose acetophthalates, titanium dioxide, talc, triethyl citrate, PVP K30, curcumin, lutein, hydroxypropylcellulose, hydroxypropylmethylcellulose and/or mixtures thereof.
  • gum Lac ShinyTM
  • methacrylic acid cellulose acetophthalates
  • titanium dioxide titanium dioxide
  • talc triethyl citrate
  • PVP K30 triethyl citrate
  • curcumin curcumin
  • lutein lutein
  • hydroxypropylcellulose hydroxypropylmethylcellulose and/or mixtures thereof.
  • gastroresistant tablets are meant tablets capable of passing unchanged through the gastric barrier.
  • the said film coating with varnishes when provided through ShellacTM, salts, cellulose acetophthalates and/or other coatings which are insoluble in an acid environment, may render the compositions according to the invention resistant to passage through the stomach.
  • the varnishes according to this invention may be present in a quantity varying from 1.0 to 1.98% by weight with respect to the composition.
  • compositions according to this invention have approximately 60% less moisture content (KF) than the compositions based on SAMe known hitherto and are approximately 12 times less hygroscopic than shown in Table 6 above.
  • compositions according to this invention are preferably intended for the treatment of depressive states.
  • a further object of this invention is a process for the preparation of solid compositions for oral use comprising SAMe and/or NADH, or their salts, in association with calcium oxide and/or calcium hydroxide which comprises the following stages:
  • the process according to this invention is carried out in an environment in which the relative humidity lies below 20% and the temperature is held between 18 and 25° C., preferably around 20° C.
  • Granulation according to this invention is preferably carried out using a rotating blade granulator fitted with a stainless mesh having holes of between 1.2 mm and 3.2 mm in diameter.
  • SAMe or its salts, is used in a quantity varying from 30 to 90% by weight, preferably from 50 to 85% by weight, with respect to the weight of the composition.
  • NADH or its salts
  • NADH is used in a quantity varying from 1 to 90% by weight, preferably from 5 to 50% by weight, with respect to the weight of the composition.
  • the pharmaceutically acceptable excipients used in the process according to the invention are preferably selected from calcium sulphate hemihydrate, magnesium oxide, calcium carbonate, malic acid, glutamic acid, xylitol, saccharose, anhydrous microcrystalline cellulose, hydrogenated fatty acids, magnesium stearate, glycerol behenate, precipitated silica.
  • the active ingredient is preferably mixed with calcium oxide from approximately 1.0 to approximately 10% by weight and/or magnesium stearate from approximately 0.5 to approximately 5% by weight and/or precipitated silica from approximately 0.5 to approximately 2.0% by weight calculated with respect to the active ingredient.
  • the granulate obtained in b) is preferably mixed with magnesium hydroxide from approximately 1.0 to 10.0% by weight and/or microcrystalline cellulose from approximately 1.0 to approximately 20.0% by weight and/or hydrogenated fatty acids from approximately 1.0 to approximately 10% by weight and/or malic acid from approximately 1 to approximately 10% by weight and/or glutamic acid from approximately 1 to approximately 10% by weight and/or glucono-delta-lactone from approximately 1 to approximately 10% by weight, magnesium stearate from approximately 0.5 to approximately 5% by weight and/or glycerol behenate from approximately 1.0 to approximately 5.0% calculated with respect to the active ingredient.
  • magnesium hydroxide from approximately 1.0 to 10.0% by weight and/or microcrystalline cellulose from approximately 1.0 to approximately 20.0% by weight and/or hydrogenated fatty acids from approximately 1.0 to approximately 10% by weight and/or malic acid from approximately 1 to approximately 10% by weight and/or glutamic acid from approximately 1 to approximately 10% by weight and/or glucono-delta-lactone from approximately 1 to approximately 10% by
  • At least one further active ingredient preferably selected from melatonin, 1-theanine and/or 1-tryptophan and/or 5-hydroxytryptophan and/or their mixtures may be added to the mixture for the treatment of depressive states.
  • coating with hydrogenated fatty acids may be performed using conventional processes known in the art, with if appropriate the addition of surfactants which are miscible in the oily liquid.
  • the coating mentioned in stage e) may be performed using hydrogenated fatty acids, preferably molten hydrogenated vegetable fatty acids, in a quantity of between approximately 0.4 and approximately 1.5% by weight with respect to the weight of the composition.
  • stage h) in the process according to this invention makes it possible to reduce the hygroscopic nature of the tablet obtained in stage g) by approximately twelve times, bringing about appreciable advantages in any subsequent stage of aqueous phase film-forming.
  • Aqueous phase film-forming (stage i) may be carried out using a substance or varnish preferably selected from gum Lac (ShellacTM) and/or its salts, methacrylic acid, cellulose acetophthalates, titanium dioxide, talc, triethyl citrate, PVP K30, curcumin, lutein, hydroxypropylcellulose, hydroxypropylmethylcellulose and/or mixtures thereof.
  • gum Lac ShineTM
  • methacrylic acid methacrylic acid
  • cellulose acetophthalates titanium dioxide
  • talc triethyl citrate
  • PVP K30 triethyl citrate
  • curcumin curcumin
  • lutein lutein
  • hydroxypropylcellulose hydroxypropylmethylcellulose and/or mixtures thereof.
  • the said film-forming may be carried out using substances preferably selected from gum Lac (ShellacTM) and/or its salts.
  • a further object of this invention is the use of SAMe or its salts in association with calcium and magnesium for the preparation of pharmaceutical, dietetic and/or nutritional/pharmaceutical compositions for the treatment of depressive states.
  • Yet a further object of this invention is a method for stabilising SAMe and/or NADH, preferably the (S,S) enantiomer, or its salts, which comprises the use of calcium oxide and/or calcium hydroxide in the percentages indicated above.
  • SAMe ion/tablet Composition based on SAMe sulphate p-toluene sulphonate A. SAMe sulphate p-toluene sulphonate 800.00 mg B Calcium oxide 70.00 mg C. Magnesium hydroxide 80.00 mg D. Saccharose 100.00 mg E. Calcium carbonate 80.00 mg F. Magnesium stearate 20.00 mg G. Malic acid 40.00 mg E. Hydrogenated fatty acid 50.00 mg Total weight of core 1240.00 mg F. Hydrogenated vegetable fatty acids 4.00 mg G. Shellac ® 30.00 mg H. PVP K 30 6.0 mg I. Titanium dioxide 5.00 mg L. Talc 10.00 mg M. Triethyl citrate 5.00 mg N. Curcumin 0.050 mg Total weight of tablet 1300.50 mg
  • the working environment was conditioned to a temperature of 20° C. and a relative humidity value of approximately 20% RH.
  • A, B, C, D, E and G and 50% of F were then transferred to the mixer in the quantities indicated above, leaving them with stirring for approximately 30 minutes.
  • the resulting mixture was transferred to dry containers, always controlling moisture content and temperature.
  • Precompression of the mixture was effected using a rotary machine equipped with round punches of 25.0 mm.
  • the hardness of the tablets produced had to be regulated to subsequently produce a granulate having good flow characteristics.
  • the tablets produced during the first processing stage were granulated on a 1000-1500 ⁇ m mesh, again in a humidity-controlled environment.
  • stage 1 . 3 The granulate obtained in stage 1 . 3 was transferred into the mixer, adding magnesium stearate and leaving it with stirring for approximately 30 minutes. At the end of this operation the resulting mixture was transferred into dry containers.
  • Final compression of the granulate was carried out using a rotary machine equipped with oblong punches of 21.0 ⁇ 9.8 mm adjusting the weight to 1240 mg/tablet and the compression force to at least 25 KP.
  • the tablets produced had a hardness of between 25 and 35 Kp.
  • Friability ⁇ 1.0%; disaggregation time: ⁇ 15 minutes (measured using the method described in U.S.P. 24 th ed.)
  • the tablets resulting from the preceding processing stages were coated in a bowl with a mixture of hydrogenated fatty acids (4.0 mg/tablet).
  • Hydrogenated fatty acid melting at 70° C. was placed in a glass container of 2.0 litres and the temperature of the mixture was raised to approximately 75° C. obtaining a homogeneous fused mass.
  • ShellacTM and PVP were dissolved in a container of suitable size until a solution of 20% w/v was obtained, and triethyl citrate was added slowly with constant stirring.
  • talc, titanium dioxide and curcumin were dispersed in 4.0 l of deionised water.
  • the resulting suspension was poured into the ShellacTM solution, washing the container with approximately 1.0 l of deionised water, subsequently diluting with a further 4.0 l of deionised water.
  • the temperature of the cores was held at 54° C. for approximately 40 minutes, and this was then reduced in regular steps down to a value of 45° C. in the final stage.
  • SAMe ion/tablet Compositions based on SAMe sulphate p-toluene sulphonate A. SAMe sulphate p-toluene sulphonate 800.00 mg B. L-melatonin 2.00 mg C Calcium oxide 70.00 mg D. Magnesium hydroxide 100.00 mg E. Calcium sulphate hemihydrate 100.00 mg F. Calcium carbonate 160.00 mg G. Magnesium stearate 20.00 mg H. Malic acid 40.00 mg I. Hydrogenated fatty acid 40.00 mg Total weight of core 1332.00 mg L. Hydrogenated vegetable fatty acids 4.00 mg M. Shellac ® 30.00 mg N. PVP K 30 6.0 mg O. Titanium dioxide 5.00 mg P. Talc 10.00 mg Q. Triethyl citrate 5.00 mg R. Curcumin 0.050 mg Total weight of tablet 1302.50 mg
  • the quantities relate to the preparation of a standard industrial lot of 250.00 kg of tablets.
  • the tablets were prepared in the manner described in Example 1 using the components and quantities indicated above.
  • SAMe ion/tablet Composition based on SAMe sulphate p-toluene sulphonate A. SAMe sulphate p-toluene sulphonate 800.00 mg B. L-theanine 200.00 mg C Calcium oxide 70.00 mg D. Magnesium hydroxide 100.00 mg E. Xylitol 50.00 mg F. Calcium carbonate 100.00 mg G. Microcrystalline cellulose 60.00 mg H. Magnesium stearate 20.00 mg I. Malic acid 40.00 mg L. Hydrogenated fatty acid 40.00 mg Total weight of core 1480.00 mg M. Hydrogenated vegetable fatty acids 4.00 mg N. Shellac ® 30.00 mg O. PVP K 30 6.0 mg P. Titanium dioxide 5.00 mg Q. Talc 10.00 mg R. Triethyl citrate 5.00 mg S. Hydroxypropylmethylcellulose 10.00 mg T. Curcumin 0.050 mg Total weight of tablet 1550.05 mg
  • the quantities relate to the preparation of a standard industrial lot of 250.00 kg of tablets.
  • the tablets were prepared in the manner described in Example 1 using the components and quantities indicated above.
  • SAMe ion/tablet Composition based on SAMe sulphate p-toluene sulphonate A. SAMe sulphate p-toluene sulphonate 800.00 mg B Calcium oxide 70.00 mg C. Magnesium hydroxide 100.00 mg D. Calcium carbonate 150.00 mg E. Magnesium stearate 20.00 mg F. Malic acid 40.00 mg G. Hydrogenated fatty acid 40.00 mg Total weight of core 1220.00 mg H. Hydrogenated vegetable fatty acids 8.00 mg I. Hydroxypropylmethylcellulose 30.00 mg L. PVP K 30 6.0 mg M Titanium dioxide 5.00 mg N. Talc 10.00 mg O. Triethyl citrate 5.00 mg P. Curcumin 0.050 mg Total weight of tablet 1284.05 mg
  • the quantities relate to the preparation of a standard industrial lot of 250.00 kg of tablets.
  • the tablets were prepared in the manner described in Example 1 using the components and quantities indicated above.
  • the quantities relate to the preparation of a standard industrial lot of 250.00 kg of tablets.
  • the tablets were prepared in the manner described in Example 1 using the components and quantities indicated above.
  • SAMe ion/tablet Composition based on SAMe sulphate p-toluene sulphonate A. SAMe sulphate p-toluene sulphonate 800.00 mg B. Folic acid 3.00 mg C. Melatonin 2.00 mg C Calcium oxide 70.00 mg D. Magnesium hydroxide 100.00 mg E. Calcium carbonate 100.00 mg F. Calcium sulphate 100.00 mg G. Magnesium stearate 20.00 mg H. Malic acid 40.00 mg I. Hydrogenated fatty acid 40.00 mg Total weight of core 1275.00 mg
  • the quantities relate to the preparation of a standard industrial lot of 250.00 kg of tablets.
  • the tablets were prepared in the manner described in Example 1 using the components and quantities indicated above.
  • the quantities relate to the preparation of a standard industrial lot of 20.00 kg of tablets
  • the tablets were prepared in stoppered glass bottles and enclosed in such a way as to reproduce the conditions of final packaging (generally aluminium/aluminium blister).
  • the samples so prepared were stored for six months in a stove thermostatted to a temperature of 40 ⁇ 2° C. and 75% RH.
  • the tablets were packed in stoppered glass bottles and enclosed in such a way as to reproduce the conditions of final packaging (generally aluminium/aluminium blister).
  • the samples were selected in the same way and in the same quantities as described for the stress test and kept in an environment thermostatted to a temperature of 25 ⁇ 2° C. and a humidity of 60% RH.
  • SAMe ion/tablet Composition based on SAMe sulphate p-toluene sulphonate A. SAMe sulphate p-toluene sulphonate 800.00 mg B Calcium oxide absent 00.00 mg C. Magnesium hydroxide 150.00 mg D. Saccharose 100.00 mg E. Calcium carbonate 80.00 mg F. Magnesium stearate 20.00 mg G. Malic acid 40.00 mg E. Hydrogenated fatty acid 50.00 mg Total weight of core 1240.00 mg F. Hydrogenated vegetable fatty acids 4.00 mg G. Shellac ® 30.00 mg H. PVP K 30 6.0 mg I. Titanium dioxide 5.00 mg L. Talc 10.00 mg M. Triethyl citrate 5.00 mg N. Curcumin 0.050 mg Total weight of tablet 1300.50 mg
  • SAMe ion/tablet Compositions based on SAMe sulphate p-toluene sulphonate A. SAMe sulphate p-toluene sulphonate 800.00 mg B. L-melatonin 2.00 mg C Calcium oxide absent 00.00 mg D. Magnesium hydroxide 170.00 mg E. Calcium sulphate hemihydrate 100.00 mg F. Calcium carbonate 160.00 mg G. Magnesium stearate 20.00 mg H. Malic acid 40.00 mg I. Hydrogenated fatty acid 40.00 mg Total weight of core 1332.00 mg L. Hydrogenated vegetable fatty acids 4.00 mg M. Shellac ® 30.00 mg N. PVP K 30 6.0 mg O. Titanium dioxide 5.00 mg P. Talc 10.00 mg Q. Triethyl citrate 5.00 mg R. Curcumin 0.050 mg Total weight of tablet 1302.50 mg
  • the quantities relate to the preparation of a standard industrial lot of 250.00 kg of tablets.
  • the tablets were prepared in the manner described in Example 1 using the components and quantities indicated above.
  • SAMe ion/tablet Composition based on SAMe sulphate p-toluene sulphonate A. SAMe sulphate p-toluene sulphonate 800.00 mg B. L-theanine 200.00 mg C Calcium oxide absent 00.00 mg D. Magnesium hydroxide 170.00 mg E. Xylitol 50.00 mg F. Calcium carbonate 100.00 mg G. Microcrystalline cellulose 60.00 mg H. Magnesium stearate 20.00 mg I. Malic acid 40.00 mg L. Hydrogenated fatty acid 40.00 mg Total weight of core 1480.00 mg M. Hydrogenated vegetable fatty acids 4.00 mg N. Shellac ® 30.00 mg O. PVP K 30 6.0 mg P. Titanium dioxide 5.00 mg Q. Talc 10.00 mg R. Triethyl citrate 5.00 mg S. Hydroxypropylmethylcellulose 10.00 mg T. Curcumin 0.050 mg Total weight of tablet 1550.05 mg
  • the quantities relate to the preparation of a standard industrial lot of 250.00 kg of tablets.
  • the tablets were prepared in the manner described in Example 1 using the components and quantities indicated above.
  • the tablets were prepared in stoppered glass bottles and enclosed in such a way as to reproduce the conditions of final packaging (generally aluminium/aluminium blister).
  • the samples so prepared were stored for six months in a stove thermostatted to a temperature of 40 ⁇ 2° C. and 75% RH.
  • Example 1A Nine samples from three different lots were used for the 400 mg tablets (Examples 1A, 2A, 3A,), and each sample from each lot was sampled after 0, 1, 3 and 6 months.
  • the tablets were packed in stoppered glass bottles and enclosed in such a way as to reproduce the conditions of final packaging (generally aluminium/aluminium blister).
  • the samples were selected in the same way and in the same quantities as described for the stress test and kept in an environment thermostatted to a temperature of 25 ⁇ 2° C. and a humidity of 60% RH.
  • Example 1A Nine samples originating from three different lots were used for the 400 mg tablets (Examples 1A, 2A, 3A,), and each sample from each lot was sampled after 0, 3, 6, 12 months.

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Abstract

This invention relates to solid oral compositions based on SAMe and/or NADH or their salts in association with calcium oxide and/or calcium hydroxide and a process for obtaining them.
This invention also relates to a method for stabilising a solid oral composition based on SAMe and/or NADH or their salts, making use of calcium oxide, calcium hydroxide optionally in association with malic acid, glutamic acid, xylitol, calcium sulphate hemihydrate, magnesium oxide and/or mixtures thereof.
This invention also relates to the use of SAMe or its salts in association with calcium oxide and/or calcium hydroxide with the possible further addition of melatonin and/or 1-theanine and/or 1-tryptophan and/or 5-hydroxytryptophan for the treatment of depressive states.

Description

  • This application is a continuation-in-part of PCT application IT2006/000610 filed Aug. 8, 2006, which claims priority benefit of Italian application Serial No. MI2006A000629, file Mar. 31, 2006, the contents of which are hereby incorporated by referenced into the present disclosure as if fully put forth therein.
  • S-adenosyl methionine (SAMe) is a physiological donor of methyl groups present in all living organisms and is involved in enzyme transmethylation reactions.
  • This substance therefore has a very important biological role and is essentially used in clinical practice as an antidepressant.
  • By “SAMe” is meant both the racemic mixture and the individual diastereoisomers (RS)-(+)-S-adenosyl-L-methionine [(RS)-(+)-SAMe)] and (SS)-(+)-S-adenosyl-L-methionine [(SS)-(+)-SAMe)], as well as mixtures other than the racemic mixture.
  • The difficulty of using S-adenosyl methionine as a drug and/or dietetic is however known because it is extremely unstable at temperatures above 0° C. or in the presence of moisture, through both degradation of the active ingredient, understood to be the sum of the two diastereoisomers, and through the conversion of active (SS)-(+)-S-adenosyl-L-methionine to inactive (RS)-(+)-S-adenosyl-L-methionine (racemisation of the substance).
  • Italian Patent no. 829906 describes a process for the preparation of pharmaceutically acceptable salts of (SS,RS)-S-adenosyl-L-methionine with quantities of inactive diastereoisomer (RS)-(+)-S-adenosyl-L-methionine of 3% or less with respect to the active diastereoisomer (SS)-(+)-S-adenosyl-L-methionine of 97% or more. The same applies with regard to the need to use racemic mixtures with a high percentage of the active S,S diastereoisomer as this is the only one which is pharmacologically active. However, the patent confirms that although more than 97% of active S,S diastereoisomer is obtained at ambient temperature, the racemic mixture is unstable over time, with conversion of the (SS)-(+)-S-adenosyl-L-methionine into (RS)-(+)-S-adenosyl-L-methionine in a relatively short time.
    • BRIEF DESCRIPTION OF THE DRAWINGS
  • FIG. 1 represents a graph illustrating the water absorption capacity of several materials over time.
  • FIG. 2 illustrates the water absorbency of several materials at a varying Relative Humidity.
    •
  • U.S. Pat. Nos. 13,627, 663,943, 98,102 and 354,263 describe a method for stabilising pharmaceutically acceptable salts of S-adenosyl methionine comprising S-adenosyl methionine paratoluene sulphonate, S-adenosyl methionine-1,4-butene disulphonate, S-adenosyl methionine sulphate, S-adenosyl methionine tosylate with a group of substances comprising chitosan, dextrin, carboxymethylcellulose, fumaric acid, azelaic acid and tryptophan. In particular the first of these patents indicates that it is important to have a product with the highest amount of S,S diastereoisomer which is the most stable possible over time because the R,S diastereoisomer is not only inactive but has a pharmacological effect which opposes that of the S,S. However, U.S. Pat. Nos. 13,627 and 98,102 describe methods for stabilising S-adenosyl methionine salts using the abovementioned substances in a percentage by weight with respect to the active ingredient which is very much higher than 50%, and adding them in reconstituted aqueous solution to S-adenosyl methionine salts, with final lyophilisation. This gives rise to high production costs and very low yields because the % of ions in the final product falls from approximately 50% to approximately 25%.
  • Racemisation of the S-adenosyl methionine is linked to three basic parameters:
      • 1. The nature of S-adenosyl-L-methionine salt formation.
      • 2. The residual moisture content in the powder after drying.
      • 3. The temperature at which the product is stored.
  • The rate of racemisation of SAMe as a salt of S-adenosyl methionine paratoluene sulphonate differs from the racemisation of SAMe in the form of S-adenosyl methionine-1,4-butene disulphonate salt, or S-adenosyl methionine sulphate or as S-adenosyl methionine tosylate.
  • Although they have different pH for the same residual moisture content, these four salts have very different stabilities and racemisation. The reason for this has to be sought in the mechanisms of diastereoisomer degradation and conversion in the various salts.
  • It is known that the drier the starting material the more stable the product will be.
  • The same consideration applies to rate of racemisation. Theoretically, with zero moisture content, the conversion rate of the S,S diastereoisomer at a given storage temperature is at a minimum.
  • It is also known that the rate of degradation and therefore also racemisation is associated with the thermal energy of the material. This is reflected in the fact that the higher the storage temperature for the material, the more rapidly it degrades and racemises.
  • If not formulated on the basis of specific procedures and using specific measures, formulations based on S-adenosyl methionine reflect the abovementioned instability and racemisation of the active ingredient, (conversion of the active S,S diastereoisomer into the inactive R,S diastereoisomer), with obvious adverse repercussions for the preservation and storage of the material, even for short periods of time.
  • U.S. Pat. Nos. 3,954,726 and 4,057,672 describe relatively stable salts of S-adenosyl methionine, that is up to 25° C. and 45° C., respectively. U.S. Pat. No. 4,465,672 also describes stable salts of S-adenosyl methionine with 5 mols of a sulphonic acid with a pK of less than 2.5.
  • In this latter United States patent, the process of preparing the product comprises preparation of a concentrated aqueous solution of an impure salt of SAMe, purification of the solution and its elution with a dilute aqueous solution of the preselected sulphonic acid, titration of the resulting eluate, concentration and lyophilisation or spraying. Because of the high instability of SAMe and its derivatives the use of an aqueous environment makes the limitations of this process obvious, and even if residual moisture content is successfully contained it is still unsuitable because of the properties of the inactive ingredient.
  • Also these patents do not describe the rate of conversion of the active S,S enantiomer at various operating and storage temperatures for the product. Up to now no methods for stabilising the active (SS)-(+)-S-adenosyl-L-methionine diastereoisomer in acceptable percentages in solid oral formulations, particularly tablets, are known. The only known concept is the need to keep moisture content, impurities and the active (SS)-(+)-S-adenosyl-L-methionine diastereoisomer under strict control, protecting the tablets by either compression or film-forming.
  • NADH is an active ingredient normally used as an energising agent and antioxidant. Currently known compositions based on NADH, such as those for example described in U.S. Pat. Nos. 5,332,727 and 7,034,011 are based on stabilising the active ingredient through association with other antioxidants.
  • There has therefore hitherto been felt a need to identify a simple and economic process which will make it possible to obtain a product based on SAMe and/or NADH, with the removal of moisture and low hygroscopic properties, with as a consequence increased stability in terms of both the active ingredient and reduced racemisation in favour of stabilisation of the reduced (S,S) enantiomer and NADH.
  • Surprisingly it has been found that the addition of calcium oxide and/or calcium hydroxide brings about improved stability of both the SAMe, regarded as the sum of the two S,S and R,S diastereoisomers, and the (S,S) diastereoisomer and the NADH, through reducing the water content of the SAMe and the NADH and by reducing its hygroscopic properties, further favoring synergistic antidepressant action through the provision of calcium.
  • Calcium oxide and/or hydroxide directly mixed with atomised SAMe and/or NADH powder, or with solid formulations based on SAMe and/or NADH, are successful in removing water through a chemical reaction with the powder or the preparation itself.
  • In fact no other excipients which succeed in removing moisture in direct mixture with the powder and/or preparations of SAMe and/or NADH over time at relatively lower temperatures (15-20° C.), reaching values of close to zero, are known.
  • The main reason is due to the highly hygroscopic nature of the SAMe which is even greater than that of substances which are well known as excellent desiccants such as silica gel, calcium chloride and others. This means that by mixing SAMe with excipients having a moisture content of close to zero, the residual water in mixtures and/or preparations based on SAMe is the same in absolute terms as that present in the initial SAMe powder. As a consequence there is only a percentage reduction in moisture content in the preparations through the dilution effect, but the same percentage by weight of water with respect to the weight of SAMe used. For this reason, in a direct mixture and/or SAMe preparations, it has never hitherto been possible to achieve higher stability of the active ingredient, and therefore a reduced racemisation rate, than that of the starting material, but at the limit this stability can be achieved.
  • Calcium oxide is instead a natural desiccant with very high reactivity in relation to water. It reacts with it and changes to a calcium hydroxide, eliminating it permanently in preparations.

  • CaO+2H2O→Ca(OH)2
  • FIG. 1 shows the rate of absorption of H2O with different absorbent substances including calcium oxide.
  • It will be seen that calcium oxide absorbs slowly but constantly up to 28% of its weight.
  • FIG. 2 shows the absorption capacity for water vapour of various desiccants as the environmental humidity (RH) varies.
  • In this case it will be seen that calcium oxide absorbs approximately 28% of water in a highly reactive way in an environment with a very low relative humidity.
  • Table 1 summarises the absorbent capacities of various desiccants under different relative humidity and temperature conditions.
  • TABLE 1
    Properties of adsorbents
    Montmorillonite
    Property Molecular sieve Silica gel clay CaO CaSO4
    Adsorption capacity at low Excellent Poor Slight Excellent Good
    concentrations of H2O
    Absorption ratio Excellent Good Good Poor Good
    Capacity for water @77° F. High High Medium High Low
    40% RH
    Separation by molecular Yes No No No No
    dimensions
    Adsorption capacity at high Excellent Poor Poor Good Good
    temperatures
  • Specifically the shape of the two FIGS. 1 and 2 and the summary values in Table 1 demonstrate that calcium oxide is the only substance which is consistently capable of removing the very small quantities of residual moisture content of SAMe or the relatively high moisture content of NADH, or its salts (approximately 1-1.5% K.F./approximately 5-7% K.F.) by chemical conversion purely by physical contact, reducing it to values close to zero.
  • This therefore reduces the second instability factor in SAMe, or its salts, because of the high rate of racemisation of its active S,S diastereoisomer. Table 2 provides moisture content values for five lots of starting material of SAMe (S-adenosyl methionine paratoluene sulphonate) with its corresponding analysis prior to mixing with calcium oxide and storage at 20° C. for 21 days, and the relative accelerated stability at 53° C. for 5 days.
  • TABLE 2
    stress test 5 days at 53° C.
    Moisture Moisture Total Moisture
    content % content % K.F. % S, S SAMe titre % impurities % content % SAMe Total
    Lot K.F. t = 0 t = 21 days at 20° C. t = 0 t = 0 t = 0 K.F. % S, S titre % impurities %
    001 1.15 1.13 80.87 52.96 0.66 1.09 56.21 51.19 5.17
    002 1.08 1.05 80.02 51.98 0.73 1.05 56.31 50.84 5.54
    003 1.06 1.03 80.21 52.76 1.03 1.03 56.12 50.11 4.55
    004 1.09 1.09 79.82 52.23 0.94 0.99 55.79 49.58 4.34
    005 1.04 1.12 81.54 52.29 1.04 1.00 55.28 49.99 5.02
  • Table 3 shows moisture content values for five lots of starting material of SAMe (S-adenosyl methionine paratoluene sulphonate) with its corresponding analysis after mixing with calcium oxide and storage at 20° C. for 21 days, and the relative accelerated stability at 53° C. for 5 days.
  • TABLE 3
    Stress test 5 days at 53° C.
    Moisture Moisture content Total Moisture
    content % K.F. % K.F. t = 21 days % S, S SAMe titre % impurities content % Total
    Lot t = 0 at 20° C. t = 0 t = 0 % t = 0 K.F. % S, S SAMe titre % impurities %
    001 0.98 0.63 80.67 50.22 0.66 0.43 66.47 50.09 3.17
    002 1.16 0.55 80.32 50.02 0.73 0.41 65.43 50.00 2.78
    003 1.00 0.70 80.11 50.16 1.03 0.39 66.56 49.81 2.65
    004 1.04 0.59 79.99 50.23 0.94 0.35 65.79 49.98 2.89
    005 0.95 0.61 81.23 50.19 1.04 0.38 67.25 49.87 3.02
  • Table 4 shows moisture content values for five lots of starting material of SAMe (S-adenosyl methionine-1,4-butene disulphonate) with corresponding analysis prior to mixing with calcium oxide and storage at 20° C. for 21 days, and the relative accelerated stability at 53° C. for 5 days.
  • TABLE 4
    Stress test 5 days at 53° C.
    Moisture Moisture content Total Moisture
    content % K.F. % K.F. t = 21 days % S, S SAMe titre % impurities % content % SAMe Total
    Lot t = 0 at 20° C. t = 0 t = 0 t = 0 K.F. % S, S titre % impurities %
    001 2.03 2.03 84.58 51.34 0.44 2.09 59.43 50.94 4.06
    002 2.01 2.31 85.34 51.54 0.56 2.21 60.02 50.93 4.23
    003 1.98 1.99 83.89 52.34 0.45 2.00 60.32 51.03 4.05
    004 1.89 1.99 84.82 52.02 0.67 1.96 59.49 51.72 4.63
    005 1.94 2.02 85.34 51.78 0.64 1.93 58.98 50.79 4.47
  • Table 5 shows moisture content values for five lots of starting material of SAMe (S-adenosyl methionine-1,4-butene disulphonate) with corresponding analysis after mixing with calcium oxide and storage for 23° C. for 21 days, and the relative accelerated stability at 53° C. for 5 days.
  • TABLE 5
    Stress test 5 days at 53° C.
    Moisture Moisture content Total Moisture
    content % % K.F. t = 21 days % S, S SAMe titre % impurities % content Total
    Lot K.F. t = 0 at 20° C. t = 0 t = 0 t = 0 % K.F. % S, S SAMe titre % impurities %
    001 1.94 1.33 84.21 50.01 0.49 0.78 70.34 50.00 2.03
    002 1.89 1.45 85.02 49.78 0.50 0.87 70.02 50.01 1.98
    003 1.87 1.27 83.49 50.12 0.49 0.93 71.32 49.89 2.00
    004 1.80 1.38 84.54 50.34 0.57 0.81 71.89 50.04 2.13
    005 1.84 1.40 85.25 50.08 0.53 0.88 70.94 50.00 1.35
  • Table 6 shows moisture content values for five lots of starting material of NADH with corresponding analysis prior to mixing with calcium oxide and storage at 20° C. for 21 days, and the relative accelerated stability at 53° C. for 5 days.
  • TABLE 6
    Stress test 5 days at 53° C.
    NADH NADH
    Moisture Moisture content (sodium salt) Total Moisture (sodium salt)
    content % K.F. % K.F. t = 21 days titre % impurities % content % titre % Total
    Lot t = 0 at 20° C. t = 0 t = 0 K.F. t = 0 impurities %
    001 6.45 6.34 92.43 1.66 6.09 82.19 7.17
    002 6.38 6.32 91.98 1.73 6.05 83.84 7.54
    003 6.66 6.34 92.73 1.33 6.23 83.11 8.55
    004 7.09 6.87 92.23 1.44 6.54 84.58 7.34
    005 5.94 5.76 92.45 1.64 5.00 83.99 7.02
  • Table 7 shows moisture content values for five lots of starting material of NADH with corresponding analysis after mixing with calcium oxide and storage at 20° C. for 21 days, and the relative accelerated stability at 53° C. for 5 days.
  • TABLE 7
    Stress test 5 days at 53° C.
    NADH NADH
    Moisture Moisture content (sodium salt) Total Moisture (sodium salt)
    content % K.F. % K.F. t = 21 days titre % impurities % content % titre % Total
    Lot t = 0 at 20° C. t = 0 t = 0 K.F. t = 0 impurities %
    001 6.21 3.20 84.53 (*) 1.50 3.49 81.19 2.45
    002 6.33 4.32 85.32 (*) 1.48 3.45 82.34 3.54
    003 6.44 4.01 83.93 (*) 1.44 3.23 80.56 2.67
    004 7.23 4.39 84.23 (*) 1.54 3.54 82.56 3.14
    005 6.87 3.98 83.95 (*) 1.43 3.10 82.49 3.02
    (*) Lower titre because mixed with 10% of calcium oxide.
  • From the data shown in Tables 2, 3, 4, 5, 6, 7 it will be seen that the mixture of calcium oxide in combination with SAMe (S-adenosyl methionine paratoluene sulphonate and S-adenosyl methionine-1,4-butene disulphonate) or with NADH causes the stability of the material at 53° C. for 5 days to increase with permanent removal of approximately 40% of the moisture content when the mixture is stored for 21 days at 20° C., and approximately 60% after the stress test at 53° C. for 5 days.
  • Thus, one object of this invention relates to compositions comprising SAMe and/or NADH, or their salts, in association with calcium oxide and/or calcium hydroxide, and optionally pharmaceutically acceptable excipients.
  • According to this invention, by “SAMe” is meant both the racemic mixture and the individual (RS)-(+)-S-adenosyl-L-methionine [(RS)-(+)-SAMe)] and (SS)-(+)-S-adenosyl-L-methionine [(SS)-(+)-SAMe)] diastereoisomers, including the mixtures other than the racemic mixture.
  • In particular, the compositions according to this invention contain SAMe, or its salts, in a quantity of between 30 and 90% by weight, preferably between 50 and 85% by weight, with respect to the weight of the composition, in association with calcium oxide and/or calcium hydroxide in a quantity of between 1 and 40% by weight, preferably between 2 and 20% by weight, with respect to the weight of the composition.
  • In particular, the compositions according to this invention contain NADH, or its salts, in a quantity between 1 and 90% by weight, preferably between 5 and 50% by weight, with respect to the weight of the composition, in association with calcium oxide and/or calcium hydroxide in a quantity of between 1 and 40% by weight, preferably between 2 and 20% by weight, with respect to the weight of the composition.
  • Preferably the said SAMe, or its salts, is S-adenosyl methionine paratoluene sulphonate, S-adenosyl methionine-1,4-butene disulphonate, S-adenosyl methionine sulphate, S-adenosyl methionine tosylate.
  • Preferably, the NADH is present in the form of its pharmaceutically acceptable salts.
  • Preferably the said calcium oxide and/or calcium hydroxide is calcium oxide alone, calcium hydroxide alone, or a mixture thereof.
  • The pharmaceutically acceptable excipients used according to this invention are preferably selected from calcium sulphate hemihydrate, magnesium oxide, malic acid, glutamic acid, glucono-delta-lactone, xylitol and/or their mixtures.
  • Compositions according to this invention may optionally comprise at least one further active ingredient, preferably selected from melatonin, 1-theanine and/or 1-tryptophan and/or 5-hydroxytryptophan and/or their mixtures.
  • The compositions according to this invention may be in the form of a direct mixture, tablets, capsules, granules and/or powder. In this invention by direct mixture is meant a mixture of atomised powder of SAMe and/or NADH, or their salts, in association with calcium oxide and/or calcium hydroxide alone, without the addition of other excipients.
  • Preferably, the compositions according to this invention are in the form of tablets, more preferably in the form of ordinary, coated, film-coated and/or gastroresistant tablets.
  • In this invention, by ordinary tablet is meant a tablet obtained by direct compression or compression after granulation without coating; by coated tablet is meant a tablet coated with non-gastroresistant substances; by film-coated tablet is meant a coated tablet which is further covered with water-based varnishes, which varnishes may have a gastroresistant action.
  • Thus, the compositions according to this invention may be film-coated with water-based varnishes preferably selected from gum Lac (Shellac™) and/or its salts, methacrylic acid, cellulose acetophthalates, titanium dioxide, talc, triethyl citrate, PVP K30, curcumin, lutein, hydroxypropylcellulose, hydroxypropylmethylcellulose and/or mixtures thereof.
  • By gastroresistant tablets according to this invention are meant tablets capable of passing unchanged through the gastric barrier.
  • The said film coating with varnishes, when provided through Shellac™, salts, cellulose acetophthalates and/or other coatings which are insoluble in an acid environment, may render the compositions according to the invention resistant to passage through the stomach. The varnishes according to this invention may be present in a quantity varying from 1.0 to 1.98% by weight with respect to the composition.
  • The compositions according to this invention have approximately 60% less moisture content (KF) than the compositions based on SAMe known hitherto and are approximately 12 times less hygroscopic than shown in Table 6 above.
  • TABLE 8
    Known tablets Known tablets based
    based on SAMe on SAMe SAMe/CaO SAMe/CaO
    SAMe 400 mg SAMe 400 mg tablets tablets
    tablets tablets (Example 1) (Example 1)
    KF % T = 0 KF % T = 24 h* KF % T = 0 KF % T = 24 h*
    Lot 01 1.24 3.76 0.45 0.76
    Lot 02 1.21 3.87 0.51 0.68
    Lot 03 1.10 3.98 0.52 0.70
    Lot 04 1.33 3.75 0.43 0.64
    Lot 05 1.39 3.76 0.57 0.74
    at 40° C. −75Rh KF (moisture content according to the Karl Fischer method)
    T = time
  • The compositions according to this invention are preferably intended for the treatment of depressive states.
  • A further object of this invention is a process for the preparation of solid compositions for oral use comprising SAMe and/or NADH, or their salts, in association with calcium oxide and/or calcium hydroxide which comprises the following stages:
      • a) mixing of the SAMe, or its salts, with calcium oxide and pharmaceutically acceptable excipients,
      • b) precompression and subsequent granulation of the mixture obtained in stage a),
      • c) mixing of the granulate obtained in stage b) with pharmaceutically acceptable excipients such as calcium sulphate hemihydrate, xylitol, malic acid, glutamic acid, magnesium oxide, hydrogenated fatty acids, precipitated silica, magnesium stearate, saccharose, glycerol behenate,
      • d) compression of the mixture obtained in stage c), with the optional addition of sweeteners and/or flavourings,
      • e) optional coating of the tablet obtained in stage d) with hydrogenated fatty acids,
      • f) optional aqueous phase film-forming on the tablet obtained in stage e).
  • The process according to this invention is carried out in an environment in which the relative humidity lies below 20% and the temperature is held between 18 and 25° C., preferably around 20° C.
  • Granulation according to this invention is preferably carried out using a rotating blade granulator fitted with a stainless mesh having holes of between 1.2 mm and 3.2 mm in diameter.
  • SAMe, or its salts, is used in a quantity varying from 30 to 90% by weight, preferably from 50 to 85% by weight, with respect to the weight of the composition.
  • NADH, or its salts, is used in a quantity varying from 1 to 90% by weight, preferably from 5 to 50% by weight, with respect to the weight of the composition.
  • In particular, the pharmaceutically acceptable excipients used in the process according to the invention are preferably selected from calcium sulphate hemihydrate, magnesium oxide, calcium carbonate, malic acid, glutamic acid, xylitol, saccharose, anhydrous microcrystalline cellulose, hydrogenated fatty acids, magnesium stearate, glycerol behenate, precipitated silica.
  • More particularly, in step a) the active ingredient is preferably mixed with calcium oxide from approximately 1.0 to approximately 10% by weight and/or magnesium stearate from approximately 0.5 to approximately 5% by weight and/or precipitated silica from approximately 0.5 to approximately 2.0% by weight calculated with respect to the active ingredient.
  • In stage c), the granulate obtained in b) is preferably mixed with magnesium hydroxide from approximately 1.0 to 10.0% by weight and/or microcrystalline cellulose from approximately 1.0 to approximately 20.0% by weight and/or hydrogenated fatty acids from approximately 1.0 to approximately 10% by weight and/or malic acid from approximately 1 to approximately 10% by weight and/or glutamic acid from approximately 1 to approximately 10% by weight and/or glucono-delta-lactone from approximately 1 to approximately 10% by weight, magnesium stearate from approximately 0.5 to approximately 5% by weight and/or glycerol behenate from approximately 1.0 to approximately 5.0% calculated with respect to the active ingredient.
  • Optionally, in said stage c) of the process according to the invention at least one further active ingredient preferably selected from melatonin, 1-theanine and/or 1-tryptophan and/or 5-hydroxytryptophan and/or their mixtures may be added to the mixture for the treatment of depressive states.
  • At stage e) coating with hydrogenated fatty acids, preferably molten hydrogenated vegetable fatty acids, may be performed using conventional processes known in the art, with if appropriate the addition of surfactants which are miscible in the oily liquid.
  • According to this invention the coating mentioned in stage e) may be performed using hydrogenated fatty acids, preferably molten hydrogenated vegetable fatty acids, in a quantity of between approximately 0.4 and approximately 1.5% by weight with respect to the weight of the composition.
  • The said stage h) in the process according to this invention, makes it possible to reduce the hygroscopic nature of the tablet obtained in stage g) by approximately twelve times, bringing about appreciable advantages in any subsequent stage of aqueous phase film-forming.
  • Aqueous phase film-forming (stage i) may be carried out using a substance or varnish preferably selected from gum Lac (Shellac™) and/or its salts, methacrylic acid, cellulose acetophthalates, titanium dioxide, talc, triethyl citrate, PVP K30, curcumin, lutein, hydroxypropylcellulose, hydroxypropylmethylcellulose and/or mixtures thereof.
  • In particular the said film-forming may be carried out using substances preferably selected from gum Lac (Shellac™) and/or its salts.
  • A further object of this invention is the use of SAMe or its salts in association with calcium and magnesium for the preparation of pharmaceutical, dietetic and/or nutritional/pharmaceutical compositions for the treatment of depressive states.
  • Yet a further object of this invention is a method for stabilising SAMe and/or NADH, preferably the (S,S) enantiomer, or its salts, which comprises the use of calcium oxide and/or calcium hydroxide in the percentages indicated above.
    • EXAMPLES Example 1
  • TABLETS OF 400 mg SAMe ion/tablet
    Composition based on SAMe sulphate p-toluene sulphonate
    A. SAMe sulphate p-toluene sulphonate 800.00 mg
    B Calcium oxide 70.00 mg
    C. Magnesium hydroxide 80.00 mg
    D. Saccharose 100.00 mg
    E. Calcium carbonate 80.00 mg
    F. Magnesium stearate 20.00 mg
    G. Malic acid 40.00 mg
    E. Hydrogenated fatty acid 50.00 mg
    Total weight of core 1240.00 mg
    F. Hydrogenated vegetable fatty acids 4.00 mg
    G. Shellac ® 30.00 mg
    H. PVP K 30 6.0 mg
    I. Titanium dioxide 5.00 mg
    L. Talc 10.00 mg
    M. Triethyl citrate 5.00 mg
    N. Curcumin 0.050 mg
    Total weight of tablet 1300.50 mg
    • 1.1. Mixing
  • The working environment was conditioned to a temperature of 20° C. and a relative humidity value of approximately 20% RH. A, B, C, D, E and G and 50% of F were then transferred to the mixer in the quantities indicated above, leaving them with stirring for approximately 30 minutes. At the end of this operation the resulting mixture was transferred to dry containers, always controlling moisture content and temperature.
    • 1.2. Precompression
  • Precompression of the mixture was effected using a rotary machine equipped with round punches of 25.0 mm. The hardness of the tablets produced had to be regulated to subsequently produce a granulate having good flow characteristics.
    • 1.3 Granulation
  • The tablets produced during the first processing stage were granulated on a 1000-1500 μm mesh, again in a humidity-controlled environment.
    • 1.4 Mixing
  • The granulate obtained in stage 1.3 was transferred into the mixer, adding magnesium stearate and leaving it with stirring for approximately 30 minutes. At the end of this operation the resulting mixture was transferred into dry containers.
    • 1.5 Compression
  • Final compression of the granulate was carried out using a rotary machine equipped with oblong punches of 21.0×9.8 mm adjusting the weight to 1240 mg/tablet and the compression force to at least 25 KP. The tablets produced had a hardness of between 25 and 35 Kp.
  • Friability: ≦1.0%; disaggregation time: ≦15 minutes (measured using the method described in U.S.P. 24th ed.)
  • Moisture content according to K.F.≦1.50%
  • Stability tests on uncoated tablets were performed at only 40° C. and 75% RH for six months and for a single lot because this is not a finished product. The samples were stored in alu/alu blisters.
  • TABLE 9
    Lot 001 - cores of 400 mg ion/tablet qualitative/quantitative composition
    in Example 1)
    Moisture
    content %
    Lot (T/t)1 (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    001 0.66 79.9 0.21 0.43 409.98
    (20/0)
    001A 0.56 75.7 0.33 0.67 409.58
    (40/1)
    001B 0.44 72.5 0.54 0.78 407.02
    (40/3)
    001C 0.35 70.3 0.76 0.98 404.78
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • The data in Table 9 show that the tablets have optimum stability.
    • 1.6: Tablet Coating
  • The tablets resulting from the preceding processing stages were coated in a bowl with a mixture of hydrogenated fatty acids (4.0 mg/tablet).
  • Hydrogenated fatty acid melting at 70° C. was placed in a glass container of 2.0 litres and the temperature of the mixture was raised to approximately 75° C. obtaining a homogeneous fused mass.
  • After the bowl had been preheated to approximately 65° C., approximately 250 kg of tablets were added and allowed to heat up to 60° C. The cores were then protected by causing the previously prepared fused mass to adhere to the moving tablets. The cores so treated were again left at 60° C. for approximately 3 minutes, until the waxy layer had been completely cleaned from the basket of the bowl.
    • 1.7: Film-Forming on the Tablets
  • Shellac™ and PVP were dissolved in a container of suitable size until a solution of 20% w/v was obtained, and triethyl citrate was added slowly with constant stirring.
  • In another steel container again fitted with a stirrer, talc, titanium dioxide and curcumin were dispersed in 4.0 l of deionised water. The resulting suspension was poured into the Shellac™ solution, washing the container with approximately 1.0 l of deionised water, subsequently diluting with a further 4.0 l of deionised water.
  • During the first coating stage the temperature of the cores was held at 54° C. for approximately 40 minutes, and this was then reduced in regular steps down to a value of 45° C. in the final stage.
  • After coating of the protected cores was complete, they were allowed to dry for a further 10 minutes, again at 45° C. Finally reduction in the temperature to 42-43° C. was awaited so that emptying of the bowl could begin, taking care to store the tablets in suitable envelopes which were impermeable to moisture. No increase in percentage water content was observed in the tablets produced in this way. All the checks specified by the quality specifications were also carried out on these.
    • Example 2
  • TABLETS OF 400 mg SAMe ion/tablet
    Compositions based on SAMe sulphate p-toluene sulphonate
    A. SAMe sulphate p-toluene sulphonate 800.00 mg
    B. L-melatonin 2.00 mg
    C Calcium oxide 70.00 mg
    D. Magnesium hydroxide 100.00 mg
    E. Calcium sulphate hemihydrate 100.00 mg
    F. Calcium carbonate 160.00 mg
    G. Magnesium stearate 20.00 mg
    H. Malic acid 40.00 mg
    I. Hydrogenated fatty acid 40.00 mg
    Total weight of core 1332.00 mg
    L. Hydrogenated vegetable fatty acids 4.00 mg
    M. Shellac ® 30.00 mg
    N. PVP K 30 6.0 mg
    O. Titanium dioxide 5.00 mg
    P. Talc 10.00 mg
    Q. Triethyl citrate 5.00 mg
    R. Curcumin 0.050 mg
    Total weight of tablet 1302.50 mg
  • The quantities relate to the preparation of a standard industrial lot of 250.00 kg of tablets.
  • The tablets were prepared in the manner described in Example 1 using the components and quantities indicated above.
  • TABLE 10
    Lot 002 - cores of 400 mg/ion/tablet (qualitative/quantitative
    composition in Example 2)
    Moisture
    Lot content % AD2 MTAD3 L-melatonin
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    002 0.71 81.2 0.29 0.39 413.11 2.04
    (20/0)
    002A 0.50 76.8 0.35 0.58 410.21 2.03
    (40/1)
    002B 0.52 73.0 0.49 0.65 411.54 2.03
    (40/3)
    002C 0.42 71.0 0.79 0.83 409.40 2.01
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • The data in Table 10 indicate that the tablets have optimum stability.
    • Example 3
  • TABLETS OF 400 mg SAMe ion/tablet
    Composition based on SAMe sulphate p-toluene sulphonate
    A. SAMe sulphate p-toluene sulphonate 800.00 mg
    B. L-theanine 200.00 mg
    C Calcium oxide 70.00 mg
    D. Magnesium hydroxide 100.00 mg
    E. Xylitol 50.00 mg
    F. Calcium carbonate 100.00 mg
    G. Microcrystalline cellulose 60.00 mg
    H. Magnesium stearate 20.00 mg
    I. Malic acid 40.00 mg
    L. Hydrogenated fatty acid 40.00 mg
    Total weight of core 1480.00 mg
    M. Hydrogenated vegetable fatty acids 4.00 mg
    N. Shellac ® 30.00 mg
    O. PVP K 30 6.0 mg
    P. Titanium dioxide 5.00 mg
    Q. Talc 10.00 mg
    R. Triethyl citrate 5.00 mg
    S. Hydroxypropylmethylcellulose 10.00 mg
    T. Curcumin 0.050 mg
    Total weight of tablet 1550.05 mg
  • The quantities relate to the preparation of a standard industrial lot of 250.00 kg of tablets.
  • The tablets were prepared in the manner described in Example 1 using the components and quantities indicated above.
  • TABLE 11
    Lot 003 - cores of 400 mg ion/tablet (qualitative/quantitative
    composition in Example 3)
    Moisture
    content % AD2 MTAD3
    Lot (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 L-theanine
    003 0.59 80.4 0.23 0.34 411.32 204.54
    (20/0)
    003A 0.53 76.6 0.32 0.61 410.54 203.54
    (40/1)
    003B 0.45 73.4 0.45 0.72 410.02 203.01
    (40/3)
    003C 0.37 71.3 0.69 0.88 407.56 201.92
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • The data in Table 11 show that the tablets have optimum stability.
    • Example 4
  • TABLETS OF 400 mg SAMe ion/tablet
    Composition based on SAMe sulphate p-toluene sulphonate
    A. SAMe sulphate p-toluene sulphonate 800.00 mg
    B Calcium oxide 70.00 mg
    C. Magnesium hydroxide 100.00 mg
    D. Calcium carbonate 150.00 mg
    E. Magnesium stearate 20.00 mg
    F. Malic acid 40.00 mg
    G. Hydrogenated fatty acid 40.00 mg
    Total weight of core 1220.00 mg
    H. Hydrogenated vegetable fatty acids 8.00 mg
    I. Hydroxypropylmethylcellulose 30.00 mg
    L. PVP K 30 6.0 mg
    M Titanium dioxide 5.00 mg
    N. Talc 10.00 mg
    O. Triethyl citrate 5.00 mg
    P. Curcumin 0.050 mg
    Total weight of tablet 1284.05 mg
  • The quantities relate to the preparation of a standard industrial lot of 250.00 kg of tablets.
  • The tablets were prepared in the manner described in Example 1 using the components and quantities indicated above.
    • Example 5
  • TABLETS OF 400 mg SAMe ion/tablet
    Composition based on SAMe sulphate p-toluene sulphonate
    A. SAMe sulphate p-toluene sulphonate 800.00 mg
    B. Folic acid 3.00 mg
    C Calcium oxide 70.00 mg
    D. Magnesium hydroxide 100.00 mg
    E. Calcium carbonate 100.00 mg
    F. Calcium sulphate 100.00 mg
    G. Magnesium stearate 20.00 mg
    H. Malic acid 40.00 mg
    I. Hydrogenated fatty acid 40.00 mg
    Total weight of core 1273.00 mg
    L. Hydrogenated vegetable fatty acids 8.00 mg
    M. Hydroxypropylmethylcellulose 30.00 mg
    N. PVP K 30 6.0 mg
    O Titanium dioxide 5.00 mg
    P. Talc 10.00 mg
    Q. Triethyl citrate 5.00 mg
    R. Curcumin 0.050 mg
    Total weight of tablet 1284.05 mg
  • The quantities relate to the preparation of a standard industrial lot of 250.00 kg of tablets.
  • The tablets were prepared in the manner described in Example 1 using the components and quantities indicated above.
  • TABLE 12
    Lot 004 - cores of 400 mg ion/tablet (qualitative/quantitative
    composition in Example 5)
    Moisture
    Lot content % AD2 MTAD3 Folic acid
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    004 0.59 80.11 0.33 0.23 410.89 3.23
    (20/0)
    004A 0.53 75.4 0.45 0.55 410.43 3.24
    (40/1)
    004B 0.45 72.8 0.55 0.67 409.76 3.21
    (40/3)
    004C 0.37 69.6 0.79 0.99 408.67 3.19
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • The data in Table 12 indicate that the tablets have optimum stability.
    • Example 6
  • TABLETS OF 400 mg SAMe ion/tablet
    Composition based on SAMe sulphate p-toluene sulphonate
    A. SAMe sulphate p-toluene sulphonate 800.00 mg
    B. Folic acid 3.00 mg
    C. Melatonin 2.00 mg
    C Calcium oxide 70.00 mg
    D. Magnesium hydroxide 100.00 mg
    E. Calcium carbonate 100.00 mg
    F. Calcium sulphate 100.00 mg
    G. Magnesium stearate 20.00 mg
    H. Malic acid 40.00 mg
    I. Hydrogenated fatty acid 40.00 mg
    Total weight of core 1275.00 mg
  • The quantities relate to the preparation of a standard industrial lot of 250.00 kg of tablets.
  • The tablets were prepared in the manner described in Example 1 using the components and quantities indicated above.
  • TABLE 13
    Lot 005 - cores of 400 mg ion/tablet (qualitative/quantitative
    composition in Example 6).
    Moisture
    content % AD2 MTAD3 Folic acid L-melatonin
    Lot (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg mg
    005 0.53 81.3 0.29 0.40 415.12 3.12 2.21
    (20/0)
    005A 0.50 76.2 0.38 0.59 414.21 3.03 2.12
    (40/1)
    005B 0.41 73.2 0.51 0.73 413.34 3.02 2.04
    (40/3)
    005C 0.29 69.2 0.83 1.09 412.21 3.00 2.08
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • The data in Table 13 reveal that the tablets have optimum stability.
    • Example 7
  • TABLETS OF 5.5 mg of NADH/tablet as sodium salt
    Compositions based on NADH without calcium oxide
    QUANTITY
    DESCRIPTION OF COMPONENTS PER UNIT
    Active ingredient
    A) NADH mg 5.50
    Excipients (core)
    B) Microcrystalline cellulose mg 7.00
    C) Mannitol mg 26.0
    D) Glycerol behenate mg 2.00
    E) “Light” magnesium oxide* mg 8.0
    F) Magnesium stearate mg 0.50
    G) Calcium carbonate mg 1.00
    Total weight of core mg 50.00
    Excipients (coating)
    H) Schellac mg 2.00
    I) Povidone (PVP) mg 0.20
    L) Titanium dioxide mg 0.10
    M) Anhydrous colloidal silica mg 0.20
    N) Talc mg 0.20
    O) Triethyl citrate mg 0.15
    Overall weight of the coated tablets mg 52.85
    *= Magnesium oxide light is a better lubricant than the heavy form
    • Example 8
  • TABLETS OF 5.5 mg of NADH/tablet as sodium salt
    Composition based on NADH with calcium oxide
    QUANTITY
    DESCRIPTION OF COMPONENTS PER UNIT
    Active ingredient
    A) NADH mg 5.50
    Excipients (core)
    B) Microcrystalline cellulose mg 7.00
    C) Mannitol mg 20.0
    D) Glycerol behenate mg 2.00
    E) Calcium oxide mg 6.00
    F) “Light” magnesium oxide* mg 8.00
    G) Magnesium stearate mg 0.50
    H) Calcium carbonate mg 1.00
    Total weight of core mg 50.00
    Excipients (coating)
    I) Schellac mg 2.00
    L Povidone (PVP) mg 0.20
    M) Titanium dioxide mg 0.10
    N) Anhydrous colloidal silica mg 0.20
    O) Talc mg 0.20
    P) Triethyl citrate mg 0.15
    Overall weight of the coated tablets mg 52.85
    *= Magnesium oxide light is a better lubricant than the heavy form
  • The quantities relate to the preparation of a standard industrial lot of 20.00 kg of tablets
    • Experimental Part Stability Tests on the Finished Product
  • Stability at 40° C. 75% RH (STRESS TEST) and at ambient temperature over a long period (SHELF LIFE) for the compositions in Examples 1, 2, 3, 4, 5, 6, 7, 8 obtained according to the process according to the invention were evaluated for changes in appearance (essentially change in colour), titre of SAMe sulphate p-toluene sulphonate and NADH and other active ingredients (mg/tablet), increase in degradation purities, moisture content (K.F.) and % of the active (SS)-(+)-S-adenosyl-L-methionine diastereoisomer; the presence of any degradation products, which can be substantially identified as adenosine and methylthioadenosine and oxidised NADH, expressed as a percentage with respect to the mg of SAMe-toluene sulphonate per tablet and reduced NADH, was further checked by HPLC.
    • Stress Test
  • The tablets were prepared in stoppered glass bottles and enclosed in such a way as to reproduce the conditions of final packaging (generally aluminium/aluminium blister).
  • The samples so prepared were stored for six months in a stove thermostatted to a temperature of 40±2° C. and 75% RH.
  • Nine samples from three different lots were used for the 400 mg tablets (Examples 1, 2, 3, 4, 5, 6), and each sample from each lot was sampled after 0, 1, 3 and 6 months.
  • The following tables (14-37) report the results of the stress test.
  • TABLE 14
    Lot 006 - tablets of 400 mg ion/tablet (Example 1)
    Moisture
    Lot content %
    (T/t)1 (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    006 0.73 78.4 0.24 0.41 411.98
    (20/0)
    006 0.59 74.2 0.36 0.63 409.45
    (40/1)
    006B 0.54 71.5 0.59 0.73 409.02
    (40/3)
    006C (40/6) 0.43 68.9 0.87 0.91 405.71
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 15
    Lot 007 - tablets of 400 mg ion/tablet (Example 1)
    Moisture
    Lot content %
    (T/t)1 (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    007 0.61 79.2 0.31 0.55 412.32
    (20/0)
    007A 0.62 75.4 0.39 0.69 411.88
    (40/1)
    007B 0.57 73.1 0.52 0.72 410.67
    (40/3)
    007C (40/6) 0.49 70.1 0.77 0.89 408.65
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 16
    Lot 008 - tablets of 400 mg ion/tablet (Example 1)
    Moisture
    Lot content %
    (T/t)1 (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    008 0.81 77.9 0.34 0.49 408.54
    (20/0)
    008A 0.76 73.4 0.53 0.59 407.58
    (40/1)
    008B 0.61 71.1 0.74 0.74 407.04
    (40/3)
    008C (40/6) 0.55 68.8 0.88 0.84 404.21
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 17
    Lot 009 - tablets of 400 mg ion/tablet (EXAMPLE 2)
    Moisture
    Lot content % AD2 MTAD3 L-melatonin
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    009 0.54 80.3 0.34 0.33 412.13 2.02
    (20/0)
    009A 0.50 77.4 0.39 0.45 410.54 2.01
    (40/1)
    009B 0.43 72.5 0.54 0.67 410.01 2.00
    (40/3)
    009C 0.32 70.3 0.84 0.93 408.44 1.98
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 18
    Lot 010 - tablets of 400 mg ion/tablet (EXAMPLE 2)
    Moisture
    Lot content % AD2 MTAD3 L-melatonin
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    010 0.61 80.0 0.52 0.53 410.54 2.03
    (20/0)
    010A 0.57 75.4 0.55 0.58 408.65 2.03
    (40/1)
    010B 0.51 72.3 0.67 0.69 408.56 2.00
    (40/3)
    010C 0.48 70.0 0.86 0.98 406.98 1.95
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 19
    Lot 011 - tablets of 400 mg ion/tablet (EXAMPLE 2)
    Moisture
    Lot content % AD2 MTAD3 L-melatonin
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    011 0.75 78.3 0.24 0.34 412.21 2.00
    (20/0)
    011A 0.55 75.8 0.35 0.55 410.29 2.02
    (40/1)
    011B 0.50 73.1 0.44 0.77 409.65 1.98
    (40/3)
    011C 0.47 71.3 0.75 0.97 407.65 1.95
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 20
    Lot 012 - tablets of 400 mg ion/tablet (Example 3)
    Moisture
    Lot content % AD2 MTAD3
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 L-theanine
    012 0.66 80.3 0.34 0.54 414.43 205.65
    (20/0)
    003A 0.61 75.4 0.43 0.66 413.43 203.54
    (40/1)
    012B 0.58 72.2 0.54 0.76 411.32 203.32
    (40/3)
    012C 0.43 70.2 0.64 0.89 410.98 202.46
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 21
    Lot 013 - tablets of 400 mg ion/tablet (Example 3)
    Moisture
    Lot content % AD2 MTAD3
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 L-theanine
    013 0.73 79.5 0.25 0.53 412.45 203.01
    (20/0)
    003A 0.64 76.1 0.38 0.64 412.01 202.83
    (40/1)
    013B 0.55 72.5 0.65 0.72 410.52 202.01
    (40/3)
    013C 0.47 69.9 0.79 0.96 409.74 201.21
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 22
    Lot 014 - tablets of 400 mg ion/tablet (Example 3)
    Moisture
    Lot content % AD2 MTAD3
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 L-theanine
    014 0.62 79.2 0.35 0.44 412.22 202.01
    (20/0)
    003A 0.60 76.4 0.45 0.55 411.01 201.43
    (40/1)
    014B 0.57 72.9 0.67 0.76 410.52 200.01
    (40/3)
    014C 0.47 70.7 0.85 0.93 409.44 198.21
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 23
    Lot 015 - tablets of 400 mg ion/tablet (Example 4)
    Moisture
    Lot content %
    (T/t)1 (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    018 0.63 79.4 0.43 0.52 412.54
    (20/0)
    018A 0.52 74.7 0.44 0.69 411.58
    (40/1)
    018B 0.41 71.5 0.58 0.78 49.78
    (40/3)
    018C (40/6) 0.31 68.9 0.72 0.99 407.75
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 24
    Lot 016 - tablets of 400 mg ion/tablet (Example 4)
    Moisture
    Lot content %
    (T/t)1 (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    016 0.56 79.2 0.33 0.49 410.54
    (20/0)
    001A 0.46 75.9 0.39 0.67 410.11
    (40/1)
    016B 0.42 72.9 0.50 0.69 409.67
    (40/3)
    016C (40/6) 0.39 70.7 0.86 0.87 408.65
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 25
    Lot 017 - tablets of 400 mg ion/tablet (Example 4)
    Moisture
    Lot content %
    (T/t)1 (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    017 0.69 78.9 0.35 0.49 413.54
    (20/0)
    017A 0.59 75.4 0.45 0.69 412.58
    (40/1)
    017B 0.56 72.9 0.59 0.79 409.02
    (40/3)
    017C (40/6) 0.49 71.7 0.87 0.96 407.59
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 26
    Lot 018 - tablets of 400 mg ion/tablet (Example 5)
    Moisture
    content % AD2 MTAD3 Folic acid
    Lot (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    018 0.69 80.4 0.29 0.36 412.45 3.13
    (20/0)
    018A 0.56 75.7 0.35 0.58 411.98 3.04
    (40/1)
    018B 0.50 73.2 0.54 0.87 410.71 3.01
    (40/3)
    018C 0.38 70.3 0.66 1.05 407.37 3.09
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 27
    Lot 019 - tablets of 400 mg ion/tablet (Example 5)
    Moisture
    Lot content % AD2 MTAD3 Folic acid
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    019 0.59 80.1 0.55 0.33 410.00 3.10
    (20/0)
    019A 0.53 75.4 0.65 0.45 410.02 3.03
    (40/1)
    019B 0.45 72.8 0.87 0.61 408.43 3.06
    (40/3)
    019C 0.37 69.6 1.01 0.79 40627 3.07
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 28
    Lot 020 - tablets of 400 mg ion/tablet (Example 5)
    Moisture
    content % AD2 MTAD3 Folic acid
    Lot (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    020 0.49 80.8 0.23 0.33 414.89 3.00
    (20/0)
    020A 0.50 75.8 0.37 0.51 412.29 2.89
    (40/1)
    020B 0.37 72.3 0.51 0.63 409.76 2.98
    (40/3)
    020C 0.28 69.1 0.63 0.87 408.63 2.78
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 29
    Lot 021 - tablets of 400 mg ion/tablet (Example 6)
    Moisture
    content % Folic L-
    Lot (K. S, AD2 MTAD3 acid melatonin
    (T/t)1 Fischer) S % (%) (%) SAMe4 mg mg
    021 0.65 78.9 0.21 0.49 415.12 3.19 2.11
    (20/0)
    021A 0.53 76.1 0.34 0.57 414.21 3.23 2.02
    (40/1)
    021B 0.41 72.1 0.50 0.63 413.34 3.03 2.04
    (40/3)
    021C 0.26 69.0 0.81 0.94 412.21 3.00 2.01
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 30
    Lot 022 - tablets of 400 mg ion/tablet (Example 6)
    Moisture
    content % Folic L-
    Lot (K. S, AD2 MTAD3 acid melatonin
    (T/t)1 Fischer) S % (%) (%) SAMe4 mg mg
    022 0.76 80.2 0.25 0.42 412.34 3.32 2.11
    (20/0)
    022A 0.64 75.9 0.27 0.54 411.21 3.23 2.10
    (40/1)
    022B 0.59 72.4 0.43 0.77 410.12 3.12 2.09
    (40/3)
    022C 0.46 70.1 0.55 0.90 408.91 3.08 2.05
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 31
    Lot 023 - tablets of 400 mg ion/tablet (Example 6)
    Moisture
    content % Folic L-
    Lot (K. S, AD2 MTAD3 acid melatonin
    (T/t)1 Fischer) S % (%) (%) SAMe4 mg mg
    023 0.53 81.0 0.22 0.47 411.87 3.05 2.13
    (20/0)
    023A 0.50 76.0 0.33 0.69 409.27 3.03 2.12
    (40/1)
    023B 0.41 73.7 0.55 0.73 405.34 3.08 2.07
    (40/3)
    023C 0.29 69.9 0.74 0.87 404.71 3.03 2.04
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 32
    Lot 001 - tablets of 5.5 mg (Example 7)
    Moisture
    content %
    Lot (T/t)1 (K. Fischer) NAD2 (%) NADH 3
    001 3.30 1.41 5.43
    (20/0)
    001A 3.89 2.03 4.98
    (40/1)
    001B 3.84 2.43 3.21
    (40/3)
    001C 3.63 3.61 2.21
    (40/6)
    1Temperature (° C.)/time (months);
    2Oxidised NADH;
    3NADH sodium salt (mg/tablet);
  • TABLE 33
    Lot 002 - tablets of 5.5 mg (Example 7)
    Moisture
    content %
    Lot (T/t)1 (K. Fischer) NAD2 (%) NADH3
    002 3.10 1.55 5.23
    (20/0)
    002A 3.87 2.22 4.34
    (40/1)
    002B 3.99 2.67 3.00
    (40/3)
    002C 3.77 3.89 2.02
    (40/6)
    1Temperature (° C.)/time (months);
    2Oxidised NADH;
    3NADH sodium salt (mg/tablet);
  • TABLE 34
    Lot 003 - tablets of 5.5 mg (Example 7)
    Moisture
    content %
    Lot (T/t)1 (K. Fischer) NAD2 (%) NADH3
    003 3.90 1.21 5.33
    (20/0)
    003A 3.65 2.23 4.58
    (40/1)
    003B 3.44 2.5 3.31
    (40/3)
    003C 3.93 3.81 2.51
    (40/6)
    1Temperature (° C.)/time (months);
    2Oxidised NADH;
    3NADH sodium salt (mg/tablet);
  • TABLE 35
    Lot 001 - tablets of 5.5 mg (Example 8)
    Moisture
    content %
    Lot (T/t)1 (K. Fischer) NAD2 (%) NADH 3
    001 2.10 1.31 5.40
    (20/0)
    001A 1.99 1.43 5.32
    (40/1)
    001B 1.80 1.53 5.21
    (40/3)
    001C 1.33 1.81 5.00
    (40/6)
    1Temperature (° C.)/time (months);
    2Oxidised NADH;
    3NADH sodium salt (mg/tablet);
  • TABLE 36
    Lot 002 - tablets of 5.5 mg (Example 8)
    Moisture
    content %
    Lot (T/t)1 (K. Fischer) NAD2 (%) NADH3
    002 2.00 1.23 5.52
    (20/0)
    002A 1.36 1.32 5.34
    (40/1)
    002B 1.45 1.57 5.12
    (40/3)
    002C 1.27 1.99 4.89
    (40/6)
    1Temperature (° C.)/time (months);
    2Oxidised NADH;
    3NADH sodium salt (mg/tablet);
  • TABLE 37
    Lot 003 - tablets of 5.5 mg (Example 8)
    Moisture
    content %
    Lot (T/t)1 (K. Fischer) NAD2 (%) NADH3
    003 2.90 1.29 5.35
    (20/0)
    003A 1.65 1.56 5.21
    (40/1)
    003B 1.44 1.99 4.98
    (40/3)
    003C 1.12 2.31 4.67
    (40/6)
    1Temperature (° C.)/time (months);
    2Oxidised NADH;
    3NADH sodium salt (mg/tablet);
  • From the stability data at 40° C. and 75% RH (STRESS TEST) it will be seen that all the lots examined after six months had suffered degradation equal to approximately 2.5% of both SAMe and the other active ingredients with a reduction of approximately 10% in the active (SS)-(+)-S-adenosyl-L-methionine diastereoisomers;
  • From the stability data at 40° C. and 75% RH (STRESS TEST) it will be seen that all the lots of NADH examined containing calcium oxide had undergone approximately 50% less degradation than the lots without calcium oxide after six months.
    • Shelf Life
  • The tablets were packed in stoppered glass bottles and enclosed in such a way as to reproduce the conditions of final packaging (generally aluminium/aluminium blister).
  • The samples were selected in the same way and in the same quantities as described for the stress test and kept in an environment thermostatted to a temperature of 25±2° C. and a humidity of 60% RH.
  • Nine samples originating from three different lots were used for the 400 mg tablets (Examples 1, 2, 3, 4, 5, 6, 7, 8) and each sample from each lot was sampled after 0, 3, 6, 12 months.
  • The following tables (38-61) show the results for SHELF LIFE.
  • TABLE 38
    Lot 024 - tablets of 400 mg ion/tablet (Example 1)
    Moisture
    content
    Lot (T/t)1 % (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    024 0.65 79.4 0.32 0.28 413.48
    (20/0)
    024A 0.56 75.3 0.44 0.34 413.23
    (25/3)
    024B 0.52 72.5 0.59 0.65 411.89
    (25/6)
    024C 0.44 69.9 0.83 0.79 409.76
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 39
    Lot 025 - tablets of 400 mg ion/tablet (Example 1)
    Moisture
    content
    Lot (T/t)1 % (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    006 0.69 78.9 0.27 0.46 410.67
    (20/0)
    025 0.65 74.6 0.39 0.67 408.78
    (25/3)
    025B 0.56 73.5 0.65 0.74 409.02
    (25/6)
    025C 0.34 70.4 0.79 0.89 405.32
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 40
    Lot 026 - tablets of 400 mg ion/tablet (Example 1)
    Moisture
    content
    Lot (T/t)1 % (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    026 0.78 78.7 0.20 0.47 411.65
    (20/0)
    006 0.65 74.9 0.39 0.60 409.43
    (25/3)
    026B 0.54 72.5 0.69 0.70 408.02
    (25/6)
    026C 0.48 68.45 0.88 0.94 404.43
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 41
    Lot 027 - tablets of 400 mg ion/tablet (Example 2)
    Moisture
    Lot content % AD2 MTAD3 L-melatonin
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    027 0.70 80.0 0.41 0.20 410.24 2.12
    (20/0)
    010A 0.64 75.7 0.54 0.47 408.65 2.04
    (25/3)
    027B 0.55 72.7 0.69 0.58 405.56 2.05
    (25/6)
    027C 0.43 70.4 0.83 0.85 406.58 1.99
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 42
    Lot 028 - tablets of 400 mg ion/tablet (Example 2)
    Moisture
    Lot content % AD2 MTAD3 L-melatonin
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    010 0.64 80.4 0.33 0.35 413.44 2.07
    (20/0)
    028A 0.54 76.73 0.45 0.54 412.35 2.09
    (25/3)
    028B 0.50 73.9 0.67 0.56 408.46 2.04
    (25/6)
    028C 0.37 73.0 0.85 0.67 406.58 2.02
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 43
    Lot 029 - tablets of 400 mg ion/tablet (Example 2)
    Moisture
    Lot content % AD2 MTAD3 L-melatonin
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    029 0.64 78.7 0.33 0.45 408.43 2.13
    (20/0)
    029A 0.57 75.3 0.34 0.54 407.55 2.12
    (25/3)
    029B 0.51 72.5 0.54 0.56 404.45 2.05
    (25/6)
    029C 0.39 71.2 0.67 0.76 403.23 1.99
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 44
    Lot 030 - tablets of 400 mg ion/tablet (Example 3)
    Moisture
    content % AD2 MTAD3
    Lot (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 L-theanine
    030 0.71 79.76 0.22 0.34 413.49 209.35
    (20/0)
    030A 0.61 74.7 0.33 0.46 412.33 203.54
    (25/3)
    030B 0.55 73.2 0.51 0.66 410.32 202.32
    (25/6)
    030C 0.49 71.4 0.69 0.79 404.98 200.32
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 45
    Lot 031 - tablets of 400 mg ion/tablet (Example 3)
    Moisture
    content % AD2 MTAD3
    Lot (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 L-theanine
    031 0.62 80.4 0.37 0.43 412.43 205.21
    (20/0)
    031A 0.56 74.4 0.40 0.54 410.45 204.54
    (25/3)
    031B 0.58 71.2 0.50 0.65 407.78 203.23
    (25/6)
    031C 0.49 68.5 0.61 0.79 407.21 201.34
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 46
    Lot 032 - tablets of 400 mg ion/tablet (Example 3)
    Moisture
    content % AD2 MTAD3
    Lot (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 L-theanine
    032 0.63 81.5 0.44 0.24 409.99 203.65
    (20/0)
    032A 0.65 75.5 0.43 0.46 406.78 202.45
    (25/3)
    032B 0.59 73.4 0.64 0.56 406.54 203.00
    (25/6)
    032C 0.50 70.0 0.84 0.75 404.21 201.23
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 47
    Lot 033 - tablets of 400 mg ion/tablet (Example 4)
    Moisture
    Lot content % AD2
    (T/t)1 (K. Fischer) S, S % (%) MTAD3 (%) SAMe4
    033 0.74 79.9 0.39 0.29 411.23
    (20/0)
    033A 0.64 74.4 0.44 0.38 409.45
    (25/3)
    033B 0.59 73.5 0.63 0.57 406.02
    (25/6)
    033C 0.34 70.6 0.88 0.89 404.23
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 48
    Lot 034 - tablets of 400 mg ion/tablet (Example 4)
    Moisture
    Lot content % AD2
    (T/t)1 (K. Fischer) S, S % (%) MTAD3 (%) SAMe4
    034 0.59 78.3 0.25 0.39 410.23
    (20/0)
    034A 0.60 73.4 0.35 0.57 408.58
    (25/3)
    034B 0.53 70.9 0.49 0.88 404.32
    (25/6)
    034C 0.39 68.5 0.68 0.90 402.12
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 49
    Lot 035 - tablets of 400 mg ion/tablet (Example 4)
    Moisture
    Lot content % AD2
    (T/t)1 (K. Fischer) S, S % (%) MTAD3 (%) SAMe4
    035 0.59 78.7 0.38 0.39 408.56
    (20/0)
    035A 0.49 74.9 0.49 0.57 409.65
    (25/3)
    035B 0.50 72.0 0.65 0.68 404.73
    (25/6)
    035C 0.36 70.2 0.97 0.87 402.12
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 50
    Lot 036 - tablets of 400 mg ion/tablet (Example 5)
    Moisture
    Lot content % AD2 MTAD3 Folic acid
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    036 0.70 80.4 0.47 0.37 413.00 3.05
    (20/0)
    036A 0.58 74.4 0.56 0.40 410.45 3.03
    (25/3)
    036B 0.42 72.0 0.78 0.66 408.99 3.06
    (25/6)
    036C 0.39 69.8 0.89 0.72 404.67 3.01
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 51
    Lot 037 - tablets of 400 mg ion/tablet (Example 5)
    Moisture
    Lot content % AD2 MTAD3 Folic acid
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    037 0.69 78.7 0.49 0.39 411.30 3.05
    (20/0)
    037A 0.63 74.5 0.64 0.55 408.57 3.01
    (25/3)
    037B 0.59 71.8 0.81 0.67 405.98 3.00
    (25/6)
    037C 0.48 69.2 1.00 0.89 402.56 2.89
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 52
    Lot 038 - tablets of 400 mg ion/tablet (Example 5)
    Moisture
    Lot content % AD2 MTAD3 Folic acid
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    038 0.70 81.2 0.52 0.31 410.99 3.11
    (20/0)
    038A 0.63 75.4 0.60 0.43 407.32 3.08
    (25/3)
    038B 0.58 73.2 0.76 0.68 405.89 3.03
    (25/6)
    038C 0.49 70.6 0.80 0.93 401.34 3.01
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 53
    Lot 039 - tablets of 400 mg ion/tablet (Example 6)
    Moisture
    content Folic L-
    Lot % (K. S, AD2 MTAD3 acid melatonin
    (T/t)1 Fischer) S % (%) (%) SAMe4 mg mg
    039 0.63 81.4 0.29 0.43 410.43 3.03 2.06
    (20/0)
    039A 0.53 74.7 0.39 0.65 406.89 3.05 2.07
    (25/3)
    039B 0.57 72.7 0.58 0.79 403.69 3.00 2.03
    (25/6)
    039C 0.42 70.9 0.79 0.89 401.34 2.89 2.02
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 54
    Lot 040 - tablets of 400 mg ion/tablet (Example 6)
    Moisture
    content Folic L-
    Lot % (K. S, AD2 MTAD3 acid melatonin
    (T/t)1 Fischer) S % (%) (%) SAMe4 mg mg
    040 0.63 78.8 0.35 0.40 408.88 3.10 2.05
    (20/0)
    040A 0.58 74.5 0.45 0.67 404.47 3.07 2.02
    (25/3)
    040B 0.48 72.5 0.60 0.70 403.34 3.03 2.07
    (25/6)
    040C 0.37 69.3 0.78 0.89 400.45 3.00 2.00
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 55
    Lot 041 - tablets of 400 mg ion/tablet (Example 6)
    Moisture
    content Folic L-
    Lot % (K. S, AD2 MTAD3 acid melatonin
    (T/t)1 Fischer) S % (%) (%) SAMe4 mg mg
    041 0.73 81.6 0.42 0.38 410.48 3.15 2.10
    (20/0)
    023A 0.70 75.3 0.43 0.49 407.56 3.09 2.12
    (25/3)
    041B 0.58 72.4 0.58 0.70 406.65 3.08 2.08
    (25/6)
    041C 0.49 70.4 0.73 0.88 402.39 3.05 2.03
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 56
    Lot 001 - tablets of 5.5 mg (Example 7)
    Moisture
    content %
    Lot (T/t)1 (K. Fischer) NAD2 (%) NADH 3
    001 3.30 1.41 5.43
    (20/0)
    001A 3.34 1.53 5.23
    (25/1)
    001B 3.54 1.73 5.11
    (25/3)
    001C 3.23 2.21 4.65
    (25/6)
    1Temperature (° C.)/time (months);
    2Oxidised NADH;
    3NADH sodium salt (mg/tablet);
  • TABLE 57
    Lot 002 - tablets of 5.5 mg (Example 7)
    Moisture
    content %
    Lot (T/t)1 (K. Fischer) NAD2 (%) NADH3
    002 3.10 1.55 5.23
    (20/0)
    002A 3.02 1.65 5.02
    (25/1)
    002B 3.00 1.87 4.70
    (25/3)
    002C 3.17 2.79 4.45
    (25/6)
    1Temperature (° C.)/time (months);
    2Oxidised NADH;
    3NADH sodium salt (mg/tablet);
  • TABLE 58
    Lot 003 - tablets of 5.5 mg (Example 7)
    Moisture
    content %
    Lot (T/t)1 (K. Fischer) NAD2 (%) NADH3
    003 3.90 1.21 5.33
    (20/0)
    003A 3.75 1.43 5.21
    (25/1)
    003B 3.84 1.50 5.11
    (25/3)
    003C 3.34 2.61 4.87
    (25/6)
    1Temperature (° C.)/time (months);
    2Oxidised NADH;
    3NADH sodium salt (mg/tablet);
  • TABLE 59
    Lot 001 - tablets of 5.5 mg (Example 8)
    Moisture
    content %
    Lot (T/t)1 (K. Fischer) NAD2 (%) NADH 3
    001 2.10 1.31 5.40
    (20/0)
    001A 1.87 1.33 5.38
    (25/1)
    001B 1.89 1.43 5.31
    (25/3)
    001C 1.43 1.51 5.20
    (25/6)
    1Temperature (° C.)/time (months);
    2Oxidised NADH;
    3NADH sodium salt (mg/tablet);
  • TABLE 60
    Lot 002 - tablets of 5.5 mg (Example 8)
    Moisture
    content %
    Lot (T/t)1 (K. Fischer) NAD2 (%) NADH3
    002 2.00 1.23 5.52
    (20/0)
    002A 1.76 1.30 5.44
    (25/1)
    002B 1.85 1.47 5.42
    (25/3)
    002C 1.57 1.67 5.29
    (25/6)
    1Temperature (° C.)/time (months);
    2Oxidised NADH;
    3NADH sodium salt (mg/tablet);
  • TABLE 61
    Lot 003 - tablets of 5.5 mg (Example 8)
    Moisture
    content %
    Lot (T/t)1 (K. Fischer) NAD2 (%) NADH3
    003 2.90 1.29 5.35
    (20/0)
    003A 1.75 1.36 5.29
    (25/1)
    003B 1.84 149 5.12
    (25/3)
    003C 1.62 1.78 5.07
    (25/6)
    1Temperature (° C.)/time (months);
    2Oxidised NADH;
    3NADH sodium salt (mg/tablet);
  • From the stability data at 25° C. and 60% RH (SHELF LIFE) it will be seen that all the lots examined after twelve months had suffered very little degradation of the SAMe with a reduction of approximately 10% in the active (SS)-(+)-S-adenosyl-L-methionine diastereoisomer;
  • From the stability data at 25° C. and 60% RH (SHELF LIFE) it will be seen that all the lots of NADH examined which contained calcium oxide had undergone approximately 50% less degradation than the lots without calcium oxide after six months.
    • COMPARATIVE EXAMPLES
  • The following three comparative examples reproducing the formulation of examples 1, 2, and 3 without the presence of calcium oxide have been introduced.
    • EXAMPLES Example 1A
  • TABLETS OF 400 mg SAMe ion/tablet
    Composition based on SAMe sulphate p-toluene sulphonate
    A. SAMe sulphate p-toluene sulphonate 800.00 mg
    B Calcium oxide absent 00.00 mg
    C. Magnesium hydroxide 150.00 mg
    D. Saccharose 100.00 mg
    E. Calcium carbonate 80.00 mg
    F. Magnesium stearate 20.00 mg
    G. Malic acid 40.00 mg
    E. Hydrogenated fatty acid 50.00 mg
    Total weight of core 1240.00 mg
    F. Hydrogenated vegetable fatty acids 4.00 mg
    G. Shellac ® 30.00 mg
    H. PVP K 30 6.0 mg
    I. Titanium dioxide 5.00 mg
    L. Talc 10.00 mg
    M. Triethyl citrate 5.00 mg
    N. Curcumin 0.050 mg
    Total weight of tablet 1300.50 mg
  • Stability tests on uncoated tablets were performed at only 40° C. and 75% RH for six months and for a single lot because this is not a finished product. The samples were stored in alu/alu blisters.
  • TABLE 9A
    Lot 001A - cores of 400 mg ion/tablet (qualitative/quantitative
    composition in Example 1A)
    Moisture
    content %
    Lot (T/t)1 (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    001 0.69 79.6 0.25 0.49 412.32
    (20/0)
    001A 0.66 73.2 0.65 0.97 409.23
    (40/1)
    001B 0.87 63.4 1.98 3.23 386.32
    (40/3)
    001C 0.79 53.2 3.32 9.56 365.67
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • The data in Table 9A show that the tablets have non good stability.
    • Example 2A
  • TABLETS OF 400 mg SAMe ion/tablet
    Compositions based on SAMe sulphate p-toluene sulphonate
    A. SAMe sulphate p-toluene sulphonate 800.00 mg
    B. L-melatonin 2.00 mg
    C Calcium oxide absent 00.00 mg
    D. Magnesium hydroxide 170.00 mg
    E. Calcium sulphate hemihydrate 100.00 mg
    F. Calcium carbonate 160.00 mg
    G. Magnesium stearate 20.00 mg
    H. Malic acid 40.00 mg
    I. Hydrogenated fatty acid 40.00 mg
    Total weight of core 1332.00 mg
    L. Hydrogenated vegetable fatty acids 4.00 mg
    M. Shellac ® 30.00 mg
    N. PVP K 30 6.0 mg
    O. Titanium dioxide 5.00 mg
    P. Talc 10.00 mg
    Q. Triethyl citrate 5.00 mg
    R. Curcumin 0.050 mg
    Total weight of tablet 1302.50 mg
  • The quantities relate to the preparation of a standard industrial lot of 250.00 kg of tablets.
  • The tablets were prepared in the manner described in Example 1 using the components and quantities indicated above.
  • TABLE 10A
    Lot 002A - cores of 400 mg/ion/tablet (qualitative/quantitative
    composition in Example 2A)
    Moisture
    Lot content % AD2 MTAD3 L-melatonin
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    002 0.87 80.0 0.34 0.69 412.21 2.00
    (20/0)
    002A 0.91 66.5 0.76 1.38 403.45 2.01
    (40/1)
    002B 0.92 63.2 2.02 4.75 381.64 2.01
    (40/3)
    002C 0.90 51.0 3.79 10.73 360.32 1.98
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • The data in Table 10A indicate that the tablets have non good stability.
    • Example 3A
  • TABLETS OF 400 mg SAMe ion/tablet
    Composition based on SAMe sulphate p-toluene sulphonate
    A. SAMe sulphate p-toluene sulphonate 800.00 mg
    B. L-theanine 200.00 mg
    C Calcium oxide absent 00.00 mg
    D. Magnesium hydroxide 170.00 mg
    E. Xylitol 50.00 mg
    F. Calcium carbonate 100.00 mg
    G. Microcrystalline cellulose 60.00 mg
    H. Magnesium stearate 20.00 mg
    I. Malic acid 40.00 mg
    L. Hydrogenated fatty acid 40.00 mg
    Total weight of core 1480.00 mg
    M. Hydrogenated vegetable fatty acids 4.00 mg
    N. Shellac ® 30.00 mg
    O. PVP K 30 6.0 mg
    P. Titanium dioxide 5.00 mg
    Q. Talc 10.00 mg
    R. Triethyl citrate 5.00 mg
    S. Hydroxypropylmethylcellulose 10.00 mg
    T. Curcumin 0.050 mg
    Total weight of tablet 1550.05 mg
  • The quantities relate to the preparation of a standard industrial lot of 250.00 kg of tablets.
  • The tablets were prepared in the manner described in Example 1 using the components and quantities indicated above.
  • TABLE 11A
    Lot 003A - cores of 400 mg ion/tablet (qualitative/quantitative
    composition in Example 3A)
    Moisture
    content % AD2 MTAD3
    Lot (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 L-theanine
    003 0.98 78.2 0.34 0.74 408.39 203.53
    (20/0)
    003A 0.93 72.3 0.75 1.34 399.74 202.54
    (40/1)
    003B 1.05 62.3 2.45 4.72 378.32 202.11
    (40/3)
    003C 1.07 51.9 4.69 12.78 354.67 200.62
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • The data in Table 11A show that the tablets have non good stability.
    • Experimental Part Stability Tests on the Finished Product
  • Stability at 40° C. 75% RH (STRESS TEST) and at ambient temperature over a long period (SHELF LIFE) for the compositions in Examples 1A, 2A, 3A, obtained according to the process according to the invention were evaluated for changes in appearance (essentially change in colour), titre of SAMe sulphate p-toluene sulphonate, increase in degradation purities, moisture content (K.F.) and % of the active (SS)-(+)-S-adenosyl-L-methionine diastereoisomer; the presence of any degradation products, which can be substantially identified as adenosine and methylthioadenosine, expressed as a percentage with respect to the mg of SAMe-toluene sulphonate per tablet, was further checked by HPLC.
    • Stress Test
  • The tablets were prepared in stoppered glass bottles and enclosed in such a way as to reproduce the conditions of final packaging (generally aluminium/aluminium blister).
  • The samples so prepared were stored for six months in a stove thermostatted to a temperature of 40±2° C. and 75% RH.
  • Nine samples from three different lots were used for the 400 mg tablets (Examples 1A, 2A, 3A,), and each sample from each lot was sampled after 0, 1, 3 and 6 months.
  • The following tables (14A-22A) report the results of the stress test.
  • TABLE 14A
    Lot 006A - tablets of 400 mg ion/tablet (Example 1A)
    Moisture
    Lot content %
    (T/t)1 (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    006 0.99 78.1 0.35 0.81 410.23
    (20/0)
    006 1.16 71.2 0.85 1.37 404.45
    (40/1)
    006B 1.18 60.1 2.54 4.63 379.34
    (40/3)
    006C 1.29 50.8 4.82 11.98 350.78
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 15A
    Lot 007A- tablets of 400 mg ion/tablet (Example 1A)
    Moisture
    Lot content %
    (T/t)1 (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    007 1.00 77.3 0.43 0.79 411.01
    (20/0)
    007A 0.96 71.8 0.85 1.65 406.29
    (40/1)
    007B 1.09 62.0 2.33 2.98 380.11
    (40/3)
    007C 1.09 52.1 4.01 10.90 355.99
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 16A
    Lot 008A- tablets of 400 mg ion/tablet (Example 1A)
    Moisture
    Lot content %
    (T/t)1 (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    008 1.02 75.7 0.33 0.85 410.11
    (20/0)
    008A 1.03 70.3 0.95 1.47 403.98
    (40/1)
    008B 1.23 61.4 2.98 4.45 376.29
    (40/3)
    008C 1.56 51.1 5.02 13.54 345.87
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 17A
    Lot 009A - tablets of 400 mg ion/tablet (EXAMPLE 2A)
    Moisture
    Lot content % AD2 MTAD3 L-melatonin
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    009 0.99 78.1 0.41 0.88 409.55 2.03
    (20/0)
    009A 1.21 68.4 0.96 1.65 401.33 2.01
    (40/1)
    009B 0.98 59.8 2.23 4.45 376.64 2.11
    (40/3)
    009C 1.11 52.3 3.99 11.23 351.34 1.98
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 18A
    Lot 010A - tablets of 400 mg ion/tablet (EXAMPLE 2A)
    Moisture
    Lot content % AD2 MTAD3 L-melatonin
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    010 0.87 77.3 0.46 0.83 409.59 2.12
    (20/0)
    010A 1.11 67.2 1.06 1.55 402.66 2.08
    (40/1)
    010B 1.18 59.4 2.55 4.67 381.23 2.01
    (40/3)
    010C 1.31 51.2 3.67 10.45 367.34 2.03
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 19A
    Lot 011A - tablets of 400 mg ion/tablet (EXAMPLE 2A)
    Moisture
    Lot content % AD2 MTAD3 L-melatonin
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    011 1.07 76.8 0.57 0.89 409.00 2.10
    (20/0)
    011A 1.14 67.5 1.33 1.72 400.87 2.04
    (40/1)
    011B 1.23 58.9 2.87 4.87 376.29 2.04
    (40/3)
    011C 1.38 53.5 4.88 11.89 362.54 2.03
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 20A
    Lot 012A - tablets of 400 mg ion/tablet (Example 3A)
    Moisture
    Lot content % AD2 MTAD3
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 L-theanine
    012 1.21 76.7 0.36 0.84 407.00 202.72
    (20/0)
    003A 1.18 69.1 0.88 1.54 397.64 201.39
    (40/1)
    012B 1.35 63.4 2.75 4.87 379.98 200.41
    (40/3)
    012C 1.57 52.7 4.43 11.68 361.82 198.42
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 21A
    Lot 013A - tablets of 400 mg ion/tablet (Example 3A)
    Moisture
    Lot content % AD2 MTAD3
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 L-theanine
    013 1.04 77.3 0.39 0.89 408.34 203.56
    (20/0)
    003A 1.07 68.4 0.85 1.57 399.84 202.49
    (40/1)
    013B 1.24 62.3 2.45 4.38 383.67 201.83
    (40/3)
    013C 1.37 51.9 4.23 9.87 370.52 199.27
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 22A
    Lot 014A - tablets of 400 mg ion/tablet (Example 3A)
    Moisture
    Lot content % AD2 MTAD3
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 L-theanine
    014 1.00 75.3 0.53 0.92 406.23 205.52
    (20/0)
    003A 1.02 67.3 1.03 1.71 395.29 203.67
    (40/1)
    014B 1.13 61.2 2.82 3.89 371.28 202.61
    (40/3)
    014C 1.29 50.6 4.65 10.21 356.72 201.56
    (40/6)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
    • Shelf Life
  • The tablets were packed in stoppered glass bottles and enclosed in such a way as to reproduce the conditions of final packaging (generally aluminium/aluminium blister).
  • The samples were selected in the same way and in the same quantities as described for the stress test and kept in an environment thermostatted to a temperature of 25±2° C. and a humidity of 60% RH.
  • Nine samples originating from three different lots were used for the 400 mg tablets (Examples 1A, 2A, 3A,), and each sample from each lot was sampled after 0, 3, 6, 12 months.
  • The following tables (38A-46A) show the results for SHELF LIFE.
  • TABLE 38A
    Lot 024A - tablets of 400 mg ion/tablet (Example 1A)
    Moisture
    Lot content %
    (T/t)1 (K. Fischer) S, S % AD2 (%) MTAD3 (%) SAMe4
    024 0.99 78.1 0.35 0.81 410.23
    (20/0)
    024A 1.02 68.2 0.59 1.24 404.21
    (25/3)
    024B 1.05 64.1 0.78 1.75 399.32
    (25/6)
    024C 1.14 60.2 1.83 2.88 396.65
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 39A
    Lot 025A - tablets of 400 mg ion/tablet (Example 1A)
    Moisture
    Lot content % MTAD3
    (T/t)1 (K. Fischer) S, S % AD2 (%) (%) SAMe4
    006 1.00 77.3 0.43 0.79 411.01
    (20/0)
    025 1.02 67.2 0.65 1.36 407.67
    (25/3)
    025B 1.15 65.5 0.87 1.97 401.87
    (25/6)
    025C 1.19 61.3 1.78 2.85 396.34
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 40A
    Lot 026A - tablets of 400 mg ion/tablet (Example 1A)
    Moisture
    Lot content % MTAD3
    (T/t)1 (K. Fischer) S, S % AD2 (%) (%) SAMe4
    026 1.02 75.7 0.33 0.85 410.11
    (20/0)
    006 1.09 66.4 0.83 1.54 405.45
    (25/1)
    026B 1.23 63.4 1.08 2.03 400.43
    (25/6)
    026C 1.49 59.9 1.99 2.77 395.87
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 41A
    Lot 027A - tablets of 400 mg ion/tablet (Example 2A)
    Moisture
    Lot content % AD2 MTAD3 L-melatonin
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    027 0.99 76.7 0.46 0.83 409.59 2.12
    (20/0)
    010A 1.12 68.2 0.93 1.52 401.43 2.08
    (25/3)
    027B 0.98 62.6 1.59 2.54 397.53 2.07
    (25/6)
    027C 1.04 52.6 2.21 4.95 391.28 2.04
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 42A
    Lot 028A - tablets of 400 mg ion/tablet (Example 2A)
    Moisture
    Lot content % AD2 MTAD3 L-melatonin
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    010 0.87 75.8 0.46 0.83 409.59 2.12
    (20/0)
    028A 1.02 66.6 0.97 1.59 404.67 2.06
    (25/3)
    028B 0.99 61.4 1.74 2.83 398.93 2.03
    (25/6)
    028C 1.24 53.6 2.23 5.54 395.68 2.02
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 43A
    Lot 029A - tablets of 400 mg ion/tablet (Example 2A)
    Moisture
    Lot content % AD2 MTAD3 L-melatonin
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 mg
    029 1.07 76.8 0.57 0.89 409.00 2.10
    (20/0)
    029A 1.06 67.7 1.42 1.93 403.28 2.06
    (25/3)
    029B 1.09 61.2 1.91 2.78 397.81 2.06
    (25/6)
    029C 1.26 52.6 2.43 4.76 393.98 2.04
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 44A
    Lot 030A - tablets of 400 mg ion/tablet (Example 3A)
    Moisture
    Lot content % AD2 MTAD3
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 L-theanine
    030 1.21 76.7 0.36 0.84 407.00 202.72
    (20/0)
    030A 1.32 68.7 1.23 1.43 402.23 203.33
    (25/3)
    030B 1.52 63.2 1.91 2.63 397.37 202.11
    (25/6)
    030C 1.43 53.8 2.53 4.77 394.88 201.09
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 45A
    Lot 031A - tablets of 400 mg ion/tablet (Example 3A)
    Moisture
    Lot content % AD2 MTAD3
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 L-theanine
    031 1.04 77.3 0.39 70.89 408.34 203.56
    (20/0)
    031A 1.11 66.9 1.41 1.63 403.83 202.23
    (25/3)
    031B 1.34 621 1.98 2.93 398.44 201.61
    (25/6)
    031C 1.27 54.0 2.71 4.79 395.98 200.18
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet);
  • TABLE 46A
    Lot 032A - tablets of 400 mg ion/tablet (Example 3A)
    Moisture
    Lot content % AD2 MTAD3
    (T/t)1 (K. Fischer) S, S % (%) (%) SAMe4 L-theanine
    032 1.00 75.3 0.53 0.92 406.23 205.52
    (20/0)
    032A 1.31 65.6 1.37 1.88 402.99 204.65
    (25/3)
    032B 1.30 57.1 1.79 2.79 396.47 203.51
    (25/6)
    032C 1.43 50.0 2.55 4.67 390.38 202.58
    (25/12)
    1Temperature (° C.)/time (months);
    2adenosine;
    3methylthioadenosine;
    4SAMe sulphate p-toluene sulphonate (mg/tablet).
    • Results
  • The stability at 40° C. 75% RH (STRESS TEST) and at temperature over a long period (SHELF LIFE) for the compositions of Examples 1A, 2A and 3A (without calcium oxide) is lower than the stability for the compositions of Examples 1, 2 and 3 (with calcium oxide), valued at the same conditions (STRESS TEST and SHELF LIFE).

Claims (35)

1. A composition comprising SAMe and/or NADH or its salts in association with calcium oxide and optionally pharmaceutically acceptable excipients.
2. A composition according to claim 1, in which the said SAMe is S-adenosyl methionine paratoluene sulphonate, S-adenosyl methionine-1,4-butene disulphonate, S-adenosyl methionine sulphate, S-adenosyl methionine tosylate.
3. A composition according to claim 1, in which the SAMe is present in a quantity varying from approximately 30 to approximately 90% by weight with respect to the weight of the composition.
4. A composition according to claim 3, in which the SAMe is present in a quantity varying from approximately 50 to 85% by weight with respect to the weight of the composition.
5. A composition according to claim 1, in which the NADH is present in a quantity varying from approximately 1 to approximately 90% by weight with respect to the weight of the composition.
6. A composition according to claim 5, in which the NADH is present in a quantity varying from approximately 5 to 50% by weight with respect to the weight of the composition.
7. A composition according to claim 1, in which the calcium oxide is present in a quantity varying from approximately 1 to approximately 40% by weight with respect to the weight of the composition.
8. A composition according to claim 1, in which the calcium oxide is present in a quantity varying from approximately 2 to approximately 20% by weight with respect to the weight of the composition.
9. A composition according to claim 1, comprising at least one further active ingredient preferably selected from 1-melatonin, 1-theanine and/or 1-tryptophan and/or 5-hydroxytryptophan or mixtures thereof.
10. A composition according to claim 1, in which at least one of the pharmaceutically acceptable excipients is calcium sulphate hemihydrate and/or glucono-delta-lactone.
11. A composition according to claim 1, in the form of a direct mixture, tablet, capsule, granulate or powder.
12. A composition according to claim 1, in the form of a tablet, preferably an ordinary, coated, film-coated and/or gastroresistant tablet.
13. A composition according to claim 1, characterised in that it is in the form of a gastroresistant tablet.
14. A process for the preparation of a tablet according to claim 1, comprising the following stages:
a) mixing of the SAMe and/or NADH and/or their salts with calcium oxide and pharmaceutically acceptable excipients,
b) precompression and subsequent granulation of the mixture obtained in stage a),
c) mixing of the granulate obtained in stage b) with pharmaceutically acceptable excipients such as calcium sulphate hemihydrate, xylitol, malic acid, glutamic acid, glucono-delta-lactone, magnesium oxide, hydrogenated fatty acids, precipitated silica, magnesium stearate, saccharose, glycerol behenate,
d) compression of the mixture obtained in stage c), with the optional addition of sweeteners and/or flavourings,
e) optional coating of the tablet obtained in stage d) with hydrogenated fatty acids,
f) optional aqueous phase film-coating of the tablet obtained in stage e).
15. A process according to claim 14 in which the SAMe is S-adenosyl methionine paratoluene sulphonate, S-adenosyl methionine-1,4-butene disulphonate, S-adenosyl methionine sulphate, S-adenosyl methionine tosylate.
16. A process according to claim 14, in which the said calcium oxide is calcium oxide alone.
17. A process according to claim 14, in which the absolute moisture content is less than approximately 50%-60% and the temperature is maintained around 20° C. and 25° C., in particular around 20° C.
18. A process according to claim 14, in which in stage c) at least one further active ingredient preferably selected from 1-melatonin, 1-theanine and/or 1-tryptophan and/or 5-hydroxytryptophan and/or mixtures thereof may be added to the mixture.
19. A process according to claim 14, in which the coating mentioned in stage e) is applied using hydrogenated fatty acids in a quantity of between 0.4 and 1.5% by weight with respect to the weight of the tablet.
20. A process according to claim 14, in which the aqueous phase film-forming mentioned in stage f) is performed using a varnish preferably selected from gum Lac and/or its salts (Shellac™), methacrylic acid, cellulose acetophthalates, titanium dioxide, talc, triethyl citrate, PVP K30, curcumin, lutein, hydroxypropylcellulose, hydroxypropylmethylcellulose and/or mixtures thereof.
21. A process according to claim 20, in which the varnish lies within a range between approximately 1.0 and approximately 5.0% by weight with respect to the composition.
22. Compositions which can be obtained through the process in claims 14.
23. A method for the treatment of depressive states which comprises the administration of SAMe or its salts in association with calcium oxide to a patient in such a need.
24. A method according to claim 23 in which magnesium oxide is further added to the said calcium oxide.
25. A method according to claim 23, in which the said SAMe is S-adenosyl methionine paratoluene sulphonate, S-adenosyl methionine-1,4-butene disulphonate, S-adenosyl methionine sulphate, S-adenosyl methionine tosylate.
26. A method according to claim 23, in which the said calcium oxide is calcium oxide alone.
27. A method for stabilising a composition based on SAMe or its salts comprising use of the mixture of SAMe and its salts with calcium oxide.
28. A method for stabilising a composition based on NADH or its salts comprising use of the mixture of NADH and its salts with calcium oxide.
29. A method according to claim 27, in which SAMe or its salts is present in a quantity of between approximately 30 and approximately 90% by weight calculated in relation to the weight of the composition.
30. A method according to claim 27, in which SAMe or its salts is present in a quantity of between approximately 50 and approximately 85% by weight calculated in relation to the weight of the composition.
31. A method according to claim 28, in which NADH or its salts is present in a quantity of between approximately 1 and approximately 90% by weight calculated in relation to the weight of the composition.
32. A method according to claim 28, in which NADH or its salts is present in a quantity of between approximately 5 and approximately 50% by weight calculated in relation to the weight of the composition.
33. A method according to claim 27 in which the calcium oxide is present in a quantity which varies from approximately 1 to approximately 40% by weight with respect to the weight of the composition.
34. A method according to claim 33, in which the calcium oxide is present in a quantity which varies from approximately 2 to approximately 20% by weight with respect to the weight of the composition.
35. A method according to claim 33, comprising the addition of pharmaceutically acceptable excipients.
US12/240,002 2006-03-31 2008-09-29 Solid oral compositions based on s-adenosyl methionine and/or nadh and process for obtaining them Abandoned US20090110729A1 (en)

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US8802628B2 (en) 2008-08-15 2014-08-12 Ironwood Pharmaceuticals, Inc. Stable solid formulation of a GC-C receptor agonist polypeptide suitable for oral administration
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