AU2004218728B2 - Stable salts of O-acetylsalicyclic acid with basic amino acids - Google Patents

Stable salts of O-acetylsalicyclic acid with basic amino acids Download PDF

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AU2004218728B2
AU2004218728B2 AU2004218728A AU2004218728A AU2004218728B2 AU 2004218728 B2 AU2004218728 B2 AU 2004218728B2 AU 2004218728 A AU2004218728 A AU 2004218728A AU 2004218728 A AU2004218728 A AU 2004218728A AU 2004218728 B2 AU2004218728 B2 AU 2004218728B2
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particle size
medicament
basic amino
acid
medicament according
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AU2004218728A1 (en
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Hubert Appolt
Gerhard Franckowiak
Wolfram Ledwoch
Gregor Leifker
Hans-Peter Wirges
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Bayer AG
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Bayer Healthcare AG
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Our Ref: 12499861 P/00/011 Regulation 3:2 00 00
AUSTRALIA
Patents Act 1990
ORIGINAL
COMPLETE SPECIFICATION STANDARD PATENT Applicant(s): Address for Service: Invention Title: Bayer HealthCare AG Patents and Licensing Building Q 18 51368 Leverkusen Germany DAVIES COLLISON CAVE Patent Trade Mark Attorneys Level 10, 10 Barrack Street Sydney, New South Wales, Australia, 2000 Stable salts of O-acetylsalicyclic acid with basic amino acids The following statement is a full description of this invention, including the best method of performing it known to me:- IP Australia
SYD
S13 OCT 2004 5951 P:WPDOCS\Hjwspecs 2\12499861div.doc-13/10104 -1- O 0 STABLE SALTS OF O-ACETYLSALICYCLIC ACID WITH BASIC AMINO ACIDS This application is a divisional of Australian Patent Application No. 2001278471, the entire 00 disclosure of which is incorporated herein by reference.
00 SThe present invention relates to medicaments of stable salts of O-acetylsalicylic acid with basic amino acids, use of the stable salts with basic amino acids in the preparation of 0medicaments, and use of the medicaments in therapy.
The analgesic action of O-acetylsalicylic acid (Aspirin®) has been utilized therapeutically for a long time. Thus O-acetylsalicylic acid is used as an analgesic, antipyretic, antirheumatic, and also as a non-steroidal anti-inflammatory agent, for example for the treatment of arthritis, neuralgia and myalgia.
However, O-acetylsalicylic acid is only soluble to a limited extent and thus is only suitable for oral administration. However, it has been disclosed (cf. JP-A-48056815) that salts of Oacetylsalicylic acid with basic amino acids are suitable for parenteral administration. As basic amino acids, in particular L-lysine, D,L-lysine and arginine are employed. A certain proportion of glycine can also be added.
Salts of O-acetylsalicylic acid with basic amino acids have been used for a long time in various indications, for instance in the abovementioned indications. The good solubility of these Oacetylsalicylates is an advantage here compared with O-acetylsalicylic acid, in particular in the case of parenteral administration. Moreover, in the case of relatively long oral administration good tolerability of the O-acetylsalicylates is to be emphasized.
A certain disadvantage of the O-acetylsalicylates until now was their inadequate stability. On the one hand, a restricted shelf life of the pharmaceutical preparations produced from these salts results from this. On the other hand, sterilization of the active compound, which may be necessary, cannot be carried out by means of heat sterilization because of the inadequate thermal stability of these salts, but must be carried out in other ways, for example by introduction of ethylene oxide gas.
The low stability of the O-acetylsalicylates is to be attributed to a back reaction of the product to O-acetylsalicylic acid and the corresponding amino acids known to the person skilled in the P:\WPDOCS\HjMSpms 2\12499861div.doc12/10/04 S-2- 0 art. The amino acid then reacts with the O-acetylsalicylic acid with removal of the acetyl group c, (amidolysis) and release of salicylic acid. The presence of salicylic acid in pharmaceutical preparations, however, is undesirable and therefore to be restricted to a low, acceptable value.
00 It is known that this degradation reaction is pH-dependent Moll, Arch. Pharm. 318 (1985), r- 5 120-127). A lowering of the pH leads to an increased protonation of the amino acid released, 00 so that this is not available or only available to a very restricted extent for the subsequent Sreaction with the O-acetylsalicylic acid. The amidolysis and thus the release of salicylic acid is thereby suppressed.
To increase the stability of pharmaceutical preparations which contain O-acetylsalicylates, the addition of "acidic" stabilizers such as calcium chloride has therefore been proposed in the past (cf. U.S. Pat. No. 4,265,888). The presence of Ca ions in the product, however, is not acceptable for the treatment of cardiovascular diseases.
It has likewise been postulated that the moisture content of the O-acetylsalicylate products has a considerable influence on their stability. Another way to increase the stability of the 0acetylsalicylates would therefore consist in the reduction of the residual moisture content by drying at a high temperature. Intensive drying at elevated temperature, however, because of the instability of the salts already mentioned above at the temperatures necessary therefor, leads to the desired goal only to a limited extent or not at all.
The present invention seeks to provide medicaments in a parenteral application form comprising compositions which comprise a salt of O-acetylsalicylic acid with a basic amino acid. The invention is directed to medicaments which have increased stability and therefore do not have the disadvantages of the O-acetylsalicylates known until now with respect to storage and/or sterilizability.
According to a first aspect of the present invention there is provided medicament in a parenteral application form comprising at least one composition comprising a salt of oacetylsalicylic acid with a basic amino acid, wherein the salt has an average particle size above a particle size of 160 /m and a proportion of more than 60% of the particles having a particle size in a range from 100 to 200 /m in a particle size distribution measured using a Malvern 2600D apparatus under standard conditions.
According to another aspect of the invention there is provided the use of a composition defined P:\WPDOCS\Hjw\Spcs 2\12499861div.doc- 1210/04 -3- O above in the manufacture of a medicament in a parenteral application form.
These and other aspects of the invention are evident from the description which follows.
00 5 According to the invention, compositions are preferred here in which the salt of O- 00 Sacetylsalicylic acid with a basic amino acid contained therein has an average particle size above a particle size of 170 pm and a proportion of more than 70% of the particles having a O particle size in a range from 100 to 200 #m in a particle size distribution measured using a N Malvern 2600D apparatus under standard conditions.
The present invention is illustrated in greater detail by the accompanying figures, in which; FIG. 1 shows a graphic representation of the particle size distribution of the O-acetylsalicylate prepared according to Ex. 1 in comparison with the particle size distribution of a commercially available O-acetylsalicylate (Aspisol®).
FIG. 2 shows the integrals of the curves of the particle size distributions shown in FIG. 1 for Ex. 1 according to the invention and Aspisol®.
FIGS. 3 and 4 show illustrations of crystals of an O-acetylsalicylate according to Ex. 1 of the present invention.
FIGS. 5 and 6 show illustrations of crystals of Aspisol®. The particle size analyses shown in FIGS. 1 and 2 were carried out using the same crystals.
FIG. 7 shows a graphic representation of the stability at various temperatures. The change in the content of free salicylic acid (in in an O-acetylsalicylate according to Ex. 3 of the present invention and in Aspisol® is indicated.
The O-acetylsalicylates according to the invention differ clearly and advantageously in their particle size analysis from the O-acetylsalicylates known until now. The distribution of the particle sizes in the case of the O-acetylsalicylates according to the invention is narrower and the average particle size is shifted to higher particle dimensions (cf. FIGS. 1 and This means that the O-acetylsalicylates according to Le A 34 700-Foreign Countries -4the invention consist of larger and more uniformly shaped (grown) crystals. In o addition to a narrower particle size distribution and higher average particle size, the O 0-acetylsalicylates according to the invention additionally exhibit a highly Spronounced crystal structure (cf. Figs. 3 and In comparison to this, the commercially obtainable O-acetylsalicylate Aspisol@ has a clearly more poorly 00 C pronounced crystal structure (cf. Figs. 5 and 6).
00 The advantageous properties of the O-acetylsalicylates described above surprisingly lead to the fact that the residual moisture content of the O-acetylsalicylates according to the invention can be kept extremely low and thus the back reaction of the 0acetylsalicylates to O-acetylsalicylic acid and the corresponding amino acid described above can be suppressed. This is all the more surprising, as Oacetylsalicylates per se are described as hygroscopic. The O-acetylsalicylates according to the invention, however, surprisingly have a reduced hygroscopicity. The O-acetylsalicylates according to the invention are clearly more stable at the same temperature than known acetylsalicylates having a higher residual moisture content.
The salts according to the invention have a residual moisture content of less than preferably of less than 0.3% and in particular of less than 0.15%, of water.
As can be seen from Fig. 7, O-acetylsalicylates according to the invention which have a residual moisture content of less than 0.3% remain almost unchanged with respect to their proportion of free salicylic acid at a temperature of 25 0 C over a period of 8 weeks, while O-acetylsalicylates having a residual moisture content of, for example, more than 0.4% undergo considerable degradation and an increase in the proportion of free salicylic acid. Thus the O-acetylsalicylates according to the invention prove to be stable over a long period at room temperature or with cooling.
The O-acetylsalicylates according to the invention can be prepared by the following process. All starting compounds are commercially obtainable. The amino acids which can be used according to the invention can occur in the L or in the D configuration or alternatively as a mixture ofD and L forms. The term "amino acids" designates, according to the invention, in particular the a-amino acids occurring in Le A 34 700-Foreign Countries 0 nature, but moreover also includes their homologues, isomers and derivatives.
Enantiomers can be mentioned as an example of isomers. Derivatives can be, for O example, amino acids provided with protective groups. Typical examples of basic amino acids which may be mentioned are: lysine, arginine, omithine, diaminobutyric acid.
00 00 According to the present invention, solutions of the reactants, i.e. of O-acetylsalicylic acid and the corresponding amino acid, are combined as rapidly as possible at a 0temperature below 30 0 C, preferably from 20 to 25 0 C, under normal pressure and C 10 blended to give a homogenous phase. Suitable solvents for the reactants are water or water-miscible organic solvents, for example alcohols such as methanol, ethanol or isopropanol, in particular ethanol, ethers such as tetrahydrofuran (THF) or ketones such as acetone.
The reactants are employed in amounts such that the basic amino acid is present in a slight excess. According to the invention, a ratio of O-acetylsalicylic acid to amino acid of 1:1.05 to 1:1.5 is preferred, a ratio of O-acetylsalicylic acid to amino acid of 1:1.05 to 1:1.2 being particularly preferred.
According to the present invention, the O-acetylsalicylic acid solution should contain from 1 to 10% by weight, preferably 5 to 10% by weight and particularly preferably from 6 to 8% by weight, of O-acetylsalicylic acid. The solution of the basic amino acid should contain from 10 to 40% by weight, preferably 15 to 35% by weight and particularly preferably from 20 to 30% by weight, of amino acid.
The crystallization of the composition according to the invention then takes place from the homogeneous mixture prepared in this way, if appropriate with addition of seed crystals, with addition of a clear excess of acetone in comparison with the reactants, for example of a 20 to 50% strength, preferably of a 30 to 40% strength, excess. It is very important according to the present invention that the temperature of the crystallization phase is kept within limits which are as narrow as possible. The temperature must not exceed 40 0 C and should preferably be kept below 35 0
C.
According to the invention, a temperature below 25 0 C, in particular of 0°C, is Le A 34 700-Foreign Countries -6preferred. As seed crystals, crystals of the desired products, for example Aspisol® crystals, can be used. The crystallization is carried out under normal pressure.
CC)
Likewise important in the process according to the invention is the maintenance of a specific stirring energy during the crystallization. The homogeneous mixture of the 00oO starting products may only be stirred gently. The stirring energy to be applied should 00 be not greater than 0.1 W per litre of reaction medium. According to the invention, an applied stirring energy of 0.04 to 0.06 W per litre of reaction medium is preferred.
SPossible stirrers are all conventional, accordingly controllable, stirrers such as a C1 10 stirring unit container with baffles.
For crystallization, the solution should be kept under the conditions indicated above for not longer than 20 hours. According to the invention a crystallization time of less than 10 hours under the conditions indicated above is preferred, a time of 1 to 8 hours being particularly preferred.
If desired, the composition according to the invention can also contain glycine. The amount of glycine is freely selectable. According to the invention, a proportion of to 30% by weight, particularly preferably of 5 to 15% by weight and especially preferably of 10% by weight, of glycine in the reaction solution is preferred.
According to the present invention, the glycine can be added to the reaction mixture of the reactants as a solution in water or a water-miscible organic solvent, it being possible to use the solvents described above as organic solvents. Glycine shows inert behaviour to these reactants. Under the conditions according to the invention mentioned above, processes of crystallization of the two solids (O-acetylsalicylate and glycine) from the homogeneous phase can thereby be carried out (cocrystallization).
According to the present invention, however, the glycine can also be added in the form of a suspension to an already crystallized suspension of the O-acetylsalicylate.
The glycine suspension can be prepared in a conventional manner. According to the Le A 34 700-Foreign Countries -7- O invention, the preparation of a glycine suspension from a solvent mixture of water and an alcohol such as ethanol is preferred.
O
C),
The manner of the addition of the glycine has no influence on the properties of the composition according to the invention. It is to be noted that the addition of glycine 00 OC to the compositions according to the invention is not necessary. In particular, the 00 presence of glycine has no influence on the stability of the compositions according to CI the invention.
CI 10 The crystallizate is then isolated in a conventional manner, for example by filtering or centrifuging. The solid is washed a number of times with organic solvents, alcohols according to the invention such as ethanol and/or ketones such as acetone or mixtures of alcohols or ketones, for example mixtures of ethanol and acetone, or the use of various solvents of this type being preferred.
The solid is then dried under reduced pressure. The temperature here should be kept below 50 0 C, preferably below 40'C and particularly preferably below 35°C. A pressure of less than 50 mbar, preferably of less than 30 mbar, should be applied to the solid. The drying can be carried out under conventional conditions, for example in a drying apparatus.
The process according to the invention can also be completely carried out under sterile conditions. The differences from the above procedure necessary for this, for example with respect to sterilization of the starting compounds and the apparatus employed, are known to the person skilled in the art.
The compositions according to the invention can be employed as analgesics, antipyretics, antirheumatics, and also as non-steroidal anti-inflammatory agents, for example for the treatment of diseases of the rheumatic type, neuralgia, myalgia, and migraine. In particular, however, they can also be employed as platelet aggregation inhibitors in the prevention and therapy of cardiovascular and cerebrovascular diseases in ischaemic heart diseases, stroke, stable and unstable angina pectoris, acute myocardial infarct, bypass operations, PTCA, stent implantation). Further Le A 34 700-Foreign Countries -8- 1 application areas are stimulation of the immune system in HIV patients and tumour prophylaxis carcinoma of the colon, oesophagus or lung), slowing of the O cognitive deterioration in dementia syndrome Alzheimer's disease), inhibition of gallstone formation and the treatment of diabetic diseases.
00o 0, The present invention also includes pharmaceutical preparations which, in addition to c-- 00 non-toxic, inert pharmaceutically suitable vehicles, contain the compositions C according to the invention, and processes for the production of these preparations.
c, 10 The compositions according to the invention can optionally also be present in microencapsulated form in one or more of the vehicles indicated above.
The compositions according to the invention should be present in the abovementioned pharmaceutical preparations in a concentration of approximately 0.1 to 99.5, preferably of approximately 0.5 to 95, by weight of the total mixture.
In a special embodiment of the invention, the abovementioned pharmaceutical preparations can also contain effective quantities of one or more further pharmaceutical active compounds apart from the- compositions according to the invention as, in particular, one or more ADP receptor antagonists (as, for example, ticlopidine and clopidogrel), GPIIb/IIIa receptor antagonists (as, for example, abciximab, eptifabitide, tirofiban, orofiban, xemilofiban and sibrafiban), phosphodiesterase inhibitors (as, for example, dipyridamole), thrombin receptor antagonists (as, for example, hirudin, hirulog and argatroban), factor Xa inhibitors (as, for example, antistatin, DX-9065 and pentasaccharides), HMG-CoA receptor antagonists (as, for example, simvastatin and cerivastatin) and/or calcium antagonists (as, for example, nifedipine).
In general, it has proved advantageous both in human and in veterinary medicine to administer the active compound(s) according to the invention in total amounts of approximately 0.5 to approximately 500, preferably 5 to 100, mg/kg of body weight every 24 hours, if appropriate in the form of several individual doses, to achieve the desired results. An individual dose contains the active compound(s) according to the Le A 34 700-Foreign Countries -9- Sinvention preferably in amounts from approximately 1 to approximately 80, in particular 3 to 30, mg/kg of body weight.
O
The active compound can act systemically and/or locally. For this purpose, it can be administered in a suitable manner, e.g. orally or parenterally. For these application oo 00 routes the active compound can be administered in suitable administration forms.
00 CI For oral administration, known administration forms releasing the active compound Srapidly and/or in modified form are suitable, such as tablets (uncoated and coated C 10 tablets, e.g. enteric coatings, FDT (fast-dissolve tablets), effervescent tablets, chewable tablets), capsules, coated tablets, granules, pellets, powders, emulsions, suspensions and solutions.
Parenteral administration can be carried out with circumvention of an absorption step (intravenous, intraarterial, intracardiac, intraspinal or intralumbar) or with insertion of an absorption (intramuscular, subcutaneous, intracutaneous or intraperitoneal). For parenteral administration, suitable administration forms are, inter alia, injection and infusion preparations in the form of solutions, suspensions, emulsions, lyophilizates and sterile powders.
Topical application in the form of suppositories or of transdermal systems (e.g.
patches, ETS systems) and also in creams, ointments, gels, sprays or dissolved in organic or inorganic solvents are further administration possibilities.
The active compounds can be converted into the administration forms mentioned in a known manner. This is carried out using inert non-toxic, pharmaceutically suitable excipients. These include, inter alia, vehicles microcrystalline cellulose), solvents liquid polyethylene glycols), emulsifiers sodium dodecylsulphate), dispersants polyvinylpyrrolidone), synthetic and natural biopolymers albumin), stabilizers antioxidants such as ascorbic acid), colourants (e.g.
inorganic pigments such as iron oxides) or taste and/or odour corrigents.
Le A 34 700-Foreign Countries 0 Examples
C-I
O The present invention is presented in greater detail below with the aid of non- ¢c€ restrictive preferred examples. If not stated otherwise, all quantitative data relate to percentages by weight.
00 00 Example 1: Lysine acetylsalicylate 0 A pyrogen-free solution of 9.9 kg of O-acetylsalicylic acid in 120 kg of ethanol is C1 10 added through a sterile filter to a sterile and pyrogen-free stirring unit container with baffles. A sterile-filtered pyrogen-free solution of 9.0 kg of lysine hydrate in 26.5 kg of pyrogen-free water is added within a short time at 20 to 25 0 C and the solutions are mixed such that a temperature of 30 0 C is not exceeded. 50 g of seed crystals are added and the already crystallizing mixture is mixed with 120 kg of sterile-filtered acetone with cooling to 0°C. The mixture is allowed to crystallize for 1 to 8 hours with gentle stirring at 0°C. The crystallizate is isolated under aseptic conditions on a filter or a centrifuge. The moist product is washed a number of times with ethanol in a separating apparatus. The moist product is transferred to a dryer under aseptic conditions and dried therein at a pressure of less than 30 mbar at a temperature of not more than 40 0
C.
89 to 94% of the desired product was obtained, which had a residual moisture content of 0.10 to 0.15%.
Example 2: D,L-Lysine acetylsalicylate with 10% of glycine A pyrogen-free solution of 9.9 kg of O-acetylsalicylic acid in 145 kg of ethanol is added through a sterile filter to a sterile and pyrogen-free stirring unit container with baffles. A sterile-filtered pyrogen-free solution of 9.0 kg of D,L-lysine hydrate and 2.4 kg of glycine in 35 kg of pyrogen-free water is added within a short time at 20 to 0 C and the solutions are mixed such that a temperature of 30 0 C is not exceeded.
g of seed crystals are added and the already crystallizing mixture is mixed with 120 kg of sterile-filtered acetone with cooling to 0°C. The mixture is allowed to Le A 34 700-Foreign Countries -11 O crystallize for 1 to 8 hours with gentle stirring at 0°C. The crystallizate is isolated under aseptic conditions on a filter or a centrifuge. The moist product is washed O successively with ethanol and acetone in a separating apparatus. The moist product is transferred to a dryer under aseptic conditions and dried therein at a pressure of less than 30 mbar at a temperature of not more than 40 0
C.
00 00 90 to 95% of the desired product was obtained, which had a residual moisture content of 0.10 to 0.15%.
0C 10 Example 3: DL-Lysine acetylsalicylate with 10% of glvcine A pyrogen-free solution of 9.9 kg of O-acetylsalicylic acid in 120 kg of ethanol is added through a sterile filter to a sterile and pyrogen-free stirring unit container with baffles. A sterile-filtered pyrogen-free solution of 9.0 kg of lysine hydrate in 26.5 kg of pyrogen-free water is added within a short time at 20 to 25C and the solutions are mixed such that a temperature of 30°C is not exceeded. 50 g of seed crystals are added and the already crystallizing mixture is mixed with 120 kg of sterile-filtered acetone with cooling to 0°C. The mixture is allowed to crystallize for 1 to 8 hours with gentle stirring at 0 C. An aseptic suspension of 2.1 kg of glycine in 8 kg of pyrogen-free water and 25 kg of ethanol is prepared in a separate sterile and pyrogen-free stirring unit container. This is added to the salicylate suspension. The crystal mixture is isolated under aseptic conditions on a filter or a centrifuge. The moist product is washed a number of times with ethanol in a separating apparatus.
The moist product is transferred to a dryer under aseptic conditions and dried therein at a pressure of less than 30 mbar at a temperature of not more than 89 to 94% of the desired product was obtained, which had a residual moisture content of 0.10 to 0.15%.
Le A 34 700-Foreign Countries. By/by/NT -12- 0 Determination of the particle size distribution c- O The compositions according to the invention and commercially available Aspisol® (marketed by Bayer AG) were investigated in a Malvern 2600 D measuring apparatus from Malvern under the following standard conditions.
00 00 The Malvern 2600 measuring apparatus consists of an He/Ne laser, a measuring C cuvette having a thermostatted reservoir system, Fourier lenses and multielement 0detector. The measured light intensities are converted into a particle size distribution.
CN 10 The alignment of laser and lens is adjusted manually before each measurement and the measuring apparatus is checked by means of a blank measurement. The blank pulses must not exceed a highest value of 20 per detector element.
The sample to be investigated is shaken by hand for about 15 s; a sample is then taken with a spatula. The amount of sample depends on the permissible obscuration area of the measuring apparatus. The sample taken is gently predispersed in a beaker (by stirring with a glass rod) using a customary dispersing agent such as Baysilon M10® (Bayer AG) and then filled into the reservoir of the measuring apparatus, which is likewise filled with the dispersant. The beaker is rinsed out completely with the dispersant in order to guarantee representative sampling.
The measurement is carried out using a set focal length of 300 mm, thermostatting at 0 C and a permissible obscuration area of 0.1-0.3.
The product is measured after ultrasonication times of 0, 15 and 60 seconds. For this, the ultrasonic finger is situated in the reservoir of the product circulation. The suspension is pumped through the measuring cuvette in a closed circulation. The signals recorded by the detector are analysed and converted into the particle size distribution.
The results thus obtained are shown in Figs. 1 and 2.
PAWPDOCS\Hjw\Spe-s 2\1249996didoc-I2/10104 S-13- C Throughout this specification and the claims which follow, unless the context requires otherwise, the word "comprise", and variations such as "comprises" or "comprising", will be understood to imply the inclusion of a stated integer or step or group of integers or steps 00 but not the exclusion of any other integer or step or group of integers or steps.
00 C The reference to any prior art in this specification is not, and should not be taken as, an 0 acknowledgment or any form of suggestion that that prior art forms part of the common CN general knowledge in Australia.

Claims (1)

14- 0 THE CLAIMS DEFINING THE INVENTION ARE AS FOLLOWS: 1. Medicament in a parenteral application form comprising at least one composition 00 C comprising a salt of o-acetylsalicylic acid with a basic amino acid, wherein the salt 00 has an average particle size above a particle size of 160 pm and a proportion of c- more than 60% of the particles having a particle size in a range from 100 to 200 lm 0 in a particle size distribution measured using a Malvem 2600D apparatus under c standard conditions. 2. Medicament according to Claim 1, wherein the salt has an average particle size above a particle size of 170 Am and a proportion of more than 70% of the particles having a particle size in a range of 100 to 200 Am in a particle size distribution measured using a Malvern 2600D apparatus under standard conditions. 3. Medicament according to either of Claims 1 and 2, wherein the basic amino acid is selected from the group consisting of lysine, arginine, histidine, ornithine or diaminobutyric acid. 4. Medicament according to Claim 3, wherein the basic amino acid is lysine. Medicament according to any one of Claims 1 to 4, additionally comprising a proportion of 5 to 15% by weight of glycine. 6. Medicament according to any one of Claims 1 to 5, additionally comprising a proportion of 10% by weight of glycine. 7. Medicament according to any one of Claims 1 to 6, as an injection or infusion preparation in the form of a solution, suspension, emulsion, lyophilizate or sterile powder. 8. Medicament according to any one of Claims 1 to 7 in a form for intravenous, P:\WPDOCS\Hjw\specs 2\12499861div.doc-13/10/04 0 intraarterial, intracardiac, intralumbar, intramuscular, subcutaneous, intracutaneous or intraperitoneal administration. 00 0 9. Use of a composition as defined in any one of Claims 1 to 6 for the manufacture of 00 medicament in a parenteral application form. Use according to Claim 9 wherein the medicament is an injection or infusion C preparation in the form of a solution, suspension, emulsion, lyophilizate or sterile powder. 11. Use according to Claim 9 wherein the medicament is in a form for intravenous, intraarterial, intracardiac, intralumbar, intramuscular, subcutaneous, intracutaneous or intraperitoneal application. DATED this 13th day of October 2004 BAYER HEALTHCARE AG By its Patent Attorneys DAVIES COLLISON CAVE
AU2004218728A 2000-07-18 2004-10-13 Stable salts of O-acetylsalicyclic acid with basic amino acids Expired - Fee Related AU2004218728B8 (en)

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Citations (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
FR2115060A1 (en) * 1970-11-26 1972-07-07 Metabio Freeze-dried acetylsalicylates of lysine and arginine - easily prepd derivs of aspirin
US4265888A (en) * 1979-07-06 1981-05-05 The Green Cross Corporation Acetylsalicylate powder preparation for injection

Patent Citations (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
FR2115060A1 (en) * 1970-11-26 1972-07-07 Metabio Freeze-dried acetylsalicylates of lysine and arginine - easily prepd derivs of aspirin
US4265888A (en) * 1979-07-06 1981-05-05 The Green Cross Corporation Acetylsalicylate powder preparation for injection

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