Title of Invention | A PHARMACEUTICAL COMPOSITION HAVING A MASKED TASTE AND METHOD FOR THE PRODUCTION THEREOF |
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Abstract | The present invention relates to a phannaceutical composition having a masked taste, the masking of which persists during administration of the composition, in particular in the form of a suspension in an aqueous vehicle, characterized in that it comprises at least the following elements: a) -a cellulosic polymer which is soluble in organic solvents but practically insoluble in water, regardless of the pH; -a methacrylic polymer which is soluble in an acid medium and practically in~oluble at a neutral or alkaline pH and -an active ingredient distributed in a homogeneous manner and in the molecular state in the mixture, which is in the form of an atomized matrix; b) an alkaline agent of an organic nature or an alkaline salt, which is phannaceutically acceptable; c) an adsorbent agent. The invention also relates to a method for the production thereof. |
Full Text | PHARMACEUTICAL FORMULATION WITH A MASKED TASTE AND A PROCESS FOR ITS PREPARATION A subject of the present invention is a pharmaceutical formulation in the form of a powder intended for oral administration in an aqueous suspension, having a masked taste, a process for its preparation and a method for masking the taste of pharmaceutical products. It is well known that numerous pharmaceutical products intended for oral administration have a very unpleasant taste and sometimes a very high persistence. This is the case in particular with antibiotic products commonly called by the name of macrolides or macrolide-like, such as ketolides, or of cephalosporins or quinolones. This of course assumes a particular importance in the case where the said pharmaceutical products are intended to be administered.to children. Several processes for masking the taste of pharmaceutical products have been described in the literature. These processes roost often consist of covering the microparticles of products with a film which disappears after passage through the mouth. There may be mentioned, for example, the article by Roy "Taste masking in oral pharmaceuticals", Pharmaceutical Technology - April 1994 - p. 84 - 99 or the Patent Application WO 98/14179. There are also processes in which the active materials are included in materials which allow their release in the body under defined conditions. Such matrices are described, for example, by C. Brossard in Actualites Pharmaceutiques - No. 388 - July-August 2 000, or in the Patent Applications WO 99/08660, WO 99/17742 or EP 1027887. One problem to be solved in the case of a matrix is to ensure that the bioavailability of the active material included in a matrix remains acceptable, taking into account the fact that the components (excluding the active ingredient) of the matrix which can be used are not necessarily favourable, for various inherent reasons, A subject of the present invention is a pharmaceutical formulation having a masked taste, the masking of which persists during administration of the formulation, in particular in the form of a suspension in an aqueous vehicle, characterized in that it comprises at least the following elements: a) - a cellulosic polymer which is soluble in organic solvents but practically insoluble in water, regardless of the pH; - a methacrylic polymer which is soluble in an acid medium and practically insoluble at a neutral or alkaline pH and - an active ingredient distributed in a homogeneous manner and in the molecular state in the mixture, which is in the form of an atomized matrix; b) an alkaline agent of an organic nature, or an alkaline salt, which is pharmaceutically acceptable; c) an adsorbent agent. As indicated above, the formulation according to the invention is intended to be suspended in water and then, where appropriate, stored in this state for some days, in practice 5 to 10 days, during its absorption period. It is important to note that each of the three elements of the formulation cooperates with the other two, but that the entirety of the three elements, however, is essential to obtain the required effect of masking the taste at the time of absorption of the formulation according to the invention. In a non-limitative manner, the various constituents of the formulation according to the invention, which must of course be pharmaceutically acceptable, can be chosen as follows: The cellulosic polymer is, in particular, ethylcellulose. It must be soluble in the organic solvents used in the process according to the invention and as insoluble as possible in water, regardless of the pH. The methacrylic polymer must be soluble in water at an acid pH (5 or less than 5) and as insoluble as possible at a neutral and alkaline pH, and its function is firstly to ensure that only the relatively small proportion of the active ingredient present on the surface of the microparticles which make up the formulation are accessible to dissolution after being suspended in water for the purpose of absorption, and secondly to ensure a good bioavailability of the active ingredient after its ingestion. It is chosen, in particular, from polymers which are known by the name Eudragit E and are available from the company Rohm Pharma GmbH, these being cationic polymers formed from 2-dimethylaminoethyl methacrylate and neutral methacrylates, The alkaline agent ensures an alkaline pH in the formulation after suspension thereof in water for the purpose of its absorption, and ensures that the majority of the active ingredient dispersed in the matrix remains inaccessible to dissolution after suspension in water. In acting in this manner, it contributes towards limiting the unpleasant taste. It is chosen, in particular, from the group consisting of meglumine, lysine and sodium and potassium citrate and carbonate. The adsorbent agent ensures adsorption on its surface of the amounts of active ingredient released after suspension of the formulation in water, while allowing its release in the stomach and thus ensuring its good bioavailability. In acting in this manner, it also contributes towards limiting the unpleasant taste. It is chosen, in particular, from talc and magnesium aluminium silicate, the latter being more particularly preferred, in particular in a fine particle size. The active ingredient can be, in particular, an antibiotic of the macrolide or macrolide-like type, that is to say erythromycin and its derivatives, such as, for example, roxithromycin, telithromycin, azithromycin or clarithromycin. or of the cephalosporin, penicillin, tetracycline or quinolone type, but also any other type of substance administered orally and having an unpleasant taste which is required to be masked, as long as it has a sufficient solubility in the organic solvent used in the preparation of the formulation. A particular subject of the present invention is a formulation as defined above, characterized in that the active ingredient is an antibiotic of the macrolide or macrolide-like type such as those mentioned above, and more particularly, a ketolide such as telithromycin. This compound is described, for example, in European Patent EP 0 680 967. The cellulosic polymer is present in the atomized matrix in a proportion which preferably ranges from 30 % to 50 % by weight, and the methacrylic polymer is present in a proportion of 10 % to 25 % by weight. The active ingredient is present in the atomized matrix at a maximum level of 50 % by weight. A nrare particular subject of the present invention is a formulation as defined above, characterized in that the proportions of cellulosic and methacrylic polymers in the matrix range respectively from 40 % to 45 % and from 15 % to 20 % by weight, and in that the proportion of the active ingredient in the matrix ranges up to 30 % by weight, It is acknowledged that for a product such as telithromycin, a concentration of 10 µl/ml is already unacceptable because of its unpleasant taste and its very high persistence. Taking into account the significant amount of the active ingredient which is present on the surface of the microparticles of the matrix and which consequently is accessible to dissolution, that is to say an amount which is very much greater than the 10 µl/ml above, it is thus surprising that masking of the taste is already obtained by simple "imprisonment" in the matrix. The formulation according to the invention can also comprise one or more other elements known individually to a person skilled in the art, in particular a hydrophobic plasticizing agent and an antioxidant agent, as regards the matrix itself, and one or more preservative agents, one or more sweetening agents, a thickening agent, and one or more flavouring agents. The above elements can be chosen, in particular, as follows: The hydrophobic plasticizing agent is, for example, dibutyl sebacate or diethyl phthalate. The antioxidant agent is, for example, a-tocopherol, BHT or ■2* 6-di-tert-butyl-4-methylphenol or BHA or 2-tert-butyl-4-methoxyphenol. The preservative agent is, for example, methyl or propyl parahydroxybenzoate. The sweetening agent or agents are chosen from those which are usually used in the pharmaceuticals or foodstuffs industry, for example maltitol, sodium saccharinate or saccharose. The thickening agent is, for example, a xanthan gum or the sodium salt of carboxyraethylcellulose. The flavouring agent or agents are chosen from those which are usually used in the pharmaceuticals or foodstuffs industry. It is known that a compound such as ethylcellulose which is insoluble in water, regardless of the pH, if present inside a matrix reduces the bioavailability of the active ingredient by impeding its diffusion towards the mucous membranes where it is absorbed. It is also known that an adsorbent agent such as magnesium aluminium silicate also reduces the bioavailability of an active ingredient due to the potent adsorption effect which manifests itself on its surface (see, for example, Handbook of Pharmaceutical Excipients p. 269-273,7, 11 and 12 (1994)). A person skilled in the art therefore should not be prompted to use such compounds to formulate an active ingredient under the conditions of the invention. The beneficial effect of masking of taste obtained by means of the use in pharmaceutical formulations of such compounds should thus logically be adversely affected by the reduced bioavailability of the active ingredient, and it should thus be expected that the formulation according to the invention has a delayed effect as regards the therapeutic efficacy of the active ingredient- In fact, this is not the case and, unexpectedly, the formulation on the contrary demonstrates a very good in vivo bioavailability of the active ingredient while masking the bad taste in amounts which are quite remarkable. It has thus been found in tests in vivo that the bioavailability can range from 60 to 100 % in the case of traditional tablets, and indeed can be better with a proportion which can reach about 30 %. A subject of the present invention is also a process for the preparation of a pharmaceutical formulation as defined above, characterized in that a cellulosic polymer and a methacrylic polymer as defined above and, where appropriate, a plasticizing agent and an antioxidant agent as defined above are mixed in an organic solvent, the active ingredient is then added, the solution obtained is then passed through an atomizer to obtain a powder in the form of an atomized matrix, the said powder is mixed with an alkaline agent and an adsorbent agent as defined above and, where appropriate, with one or more elements chosen from the group consisting of preservative agents, sweetening agents, thickening agents and flavouring agents as defined above, and the expected formulation is obtained. The organic solvent is chosen such that it is a good solvent simultaneously for the cellulosic polymer, the methacrylic polymer, the active ingredient and, where appropriate, the plasticizing and antioxidant agents. It is thus possible to use, in particular, solvents such as halogenated hydrocarbons, in particular methylene chloride, alcohols, in particular ethanol and isopropanol, and ketones, in particular acetone and methyl ethyl ketone. A subject of the present invention is also a process for masking the taste of a pharmaceutical active ingredient intended for oral administration in an aqueous suspension, characterized in that the said active ingredient is imprisoned homogeneously inside a matrix comprising at least a cellulosic polymer and a methacrylic polymer as defined above and is combined there with at least an alkaline agent and an adsorbent agent as defined above. The following example illustrates the invention, without however limiting it: 1/ Preparation of a solution for atomization The following starting ingredients are used: The dibutyl sebacate, a-tocopherol, Eudragit E 100® and ethylcellulose NIO are introduced into 20 litres of methylene chloride with moderate agitation. Agitation is continued overnight. One hour before the start of the atomization, the telithromycin is dissolved in the solution of polymers and the solution is made up to the desired weight with methylene chloride. 2/ Atomization The operation is carried out in an atomizer in accordance with the following parameters: Inlet temperature: 85°C Outlet temperature: 45-55°C Two-fluid of single-fluid nozzle The nozzle and the drying chamber are placed entirely under nitrogen. 3/ Secondary drying The atomization product is spread out on plates and placed in an oven under a flow of nitrogen at room temperature for 24 hours. An atomization product comprising 30 % active ingredient is finally obtained. (1) Magnesium aluminium silicate of fine particle size. (2) Xanthan gum (3) P 90 designates a particular particle size of the maltitol. A so-called "return" mixer is used. Before the products are introduced into the mixer, they are passed through a sieve with a mesh opening of 850 µm. Mixing is then carried out as follows: - Premixing: all the excipients and only 1/3 of the maltitol are mixed for 10 minutes at 20 rpm; - Mixing: the remainder of the maltitol and the atomization product are then mixed for 30 minutes at 20 rpm. The final mixture is then distributed into the bottles. It should be noted that the names Eudragit E, Veegum F and Rhodigel ultra are registered trade marks. CLAIMS 1) A pharmaceutical formulation having a masked taste, the masking of which persists during administration of the formulation, in particular in the form of a suspension in an aqueous vehicle, characterized in that it comprises at least the following elements: a) - a cellulosic polymer which is soluble in organic solvents but practically insoluble in water, regardless of the pH; - a methacrylic polymer which is soluble in an acid medium and practically insoluble at a neutral or alkaline pH and - an active ingredient distributed in a homogeneous manner and in the molecular state in the mixture, which is in the form of an atomized matrix; b) an alkaline agent of an organic nature or an alkaline salt, which is pharmaceutically acceptable; c) an adsorbent agent. 2) A formulation according to claim 1, characterized in that the cellulosic polymer and the methacrylic polymer are respectively ethylcellulose and a cationic polymer formed from 2-dimethylaminoethyl methacrylate and neutral methacrylates. 3) A formulation according to claim 1 or 2, characterized in that the alkaline agent and the adsorbent agent are chosen respectively from the group consisting of meglumine, lysine, sodium and potassium citrate and sodium and potassium carbonate, and from the group consisting of magnesium aluminium silicate and talc. 4) A formulation according to claim 3, characterized in that the alkaline agent and the adsorbent agent are respectively meglumine and magnesium aluminium silicate. 5) A formulation according to any one of claims 1 to 4, characterized in that the active ingredient is an antibiotic of the macrolide or macrolide-like, cephalosporin. penicillin, tetracycline or quinolone type. 6) A formulation according to claim 5, characterized in that the active ingredient is telithromycin. 7) A formulation according to any one of claims 1 to 6, characterized in that: - the cellulosic polymer is present in the atomized matrix in a proportion ranging from 30 % to 50 % by weight and the methacrylic polymer is present in a proportion ranging from 10 % to 25 % by weight, and - the active ingredient is present in the atomized matrix at a maximum level of 50 % by weight. 8) A formulation according to claim 1, characterized in that the proportions of cellulosic and methacrylic polymers in the matrix range respectively from 40 % to 45 % and from 15 % to 20 % fay weight, and in that the maximum amount of the active ingredient in the matrix is 30 % by weight. 9) A formulation according to any one of claims 1 to 8, characterized in that it also comprises within the matrix a hydrophobic plasticizing agent and/or an antioxidant agent. 10) A formulation according to any one of claims 1 to 9, characterized in that it also comprises one or more elements chosen from preservative agents, sweetening agents, thickening agents and flavouring agents. 11) Process for the preparation of a pharmaceutical formulation as defined in any one of claims 1 to 10, characterized in that a cellulosic polymer and a methacrylic polymer as defined in claim 1 and, where appropriate, a hydrophobic plasticizing agent and an antioxidant agent are mixed in an organic solvent, the active ingredient is then added, the solution obtained is then passed through an atomizer in order to obtain a product in the form of an atomized matrix, the said powder is mixed with an alkaline agent and an adsorbent agent as defined above and, where appropriate, with one or more elements chosen from the group consisting of preservative agents, sweetening agents, thickening agents and flavouring agents and the expected formulation is obtained. 12) Process according to claim 11, characterized in that the organic solvent used is chosen from the group consisting of halogenated hydrocarbons, alcohols and ketones. 13) Process according to claim 12, characterized in that the solvent is methylene chloride. 14) Process for masking the taste of a pharmaceutical product intended for oral administration in an aqueous suspension, characterized in that the said active ingredient is imprisoned homogeneously inside a matrix comprising at least a cellulosic polymer and a methacrylic polymer as defined in claim 1 and is combined there with at least an alkaline agent as defined in claim 1 and an adsorbent agent. 15. A pharmaceutical formulation substantially as herein above described and exemplified. 16. Process for the preparation of a pharmaceutical formulation substantially as herein above described and exemplified. |
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2019-chenp-2003 description (complete) grand.pdf
2019-chenp-2003-correspondnece-others.pdf
2019-chenp-2003-correspondnece-po.pdf
2019-chenp-2003-description(complete).pdf
2019-chenp-2003-other documents.pdf
Patent Number | 227933 | ||||||||||||
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Indian Patent Application Number | 2019/CHENP/2003 | ||||||||||||
PG Journal Number | 10/2009 | ||||||||||||
Publication Date | 06-Mar-2009 | ||||||||||||
Grant Date | 27-Jan-2009 | ||||||||||||
Date of Filing | 19-Dec-2003 | ||||||||||||
Name of Patentee | AVENTIS PHARMA S.A | ||||||||||||
Applicant Address | 20, AVENUE RAYMOND ARON, F-92160 ANTONY, | ||||||||||||
Inventors:
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PCT International Classification Number | A61K9/00 | ||||||||||||
PCT International Application Number | PCT/FR02/02158 | ||||||||||||
PCT International Filing date | 2002-06-21 | ||||||||||||
PCT Conventions:
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