FR2814679A1 - DISPERSIBLE PHARMACEUTICAL COMPOSITIONS BASED ON CEPHALOSPORINS, PROCESS FOR THE PREPARATION THEREOF AND USE THEREOF - Google Patents

Abstract

The invention concerns dispersible cephalosporin compositions, in particular in the form of tablets, their preparation method and their use for improving sensory perception of patients when such compositions are orally administered.

Description

<Desc / Clms Page number 1>

The present invention relates to cephalosporin-based pharmaceutical compositions, especially in the form of dispersible tablets, as well as to their use for improving the sensory perception of patients with the oral administration of such compositions.

 In the pharmaceutical industry, cephalosporins are widely used as anti-bacterial agents and are therefore offered by a very large number of chemical suppliers. Among these cephalosporins, there may be mentioned, by way of example, the active ingredients known by the International Nonproprietary Names (INNs) cefadroxil, cephadrine or even cefalexin. To date, the active ingredient cefadroxil alone is offered by 28 chemical suppliers.

 Cephalosporins and their derivatives can be manufactured according to various synthetic methods.

 Thus, in the patent application FR 1 603 618, there is described a process for the preparation of cephalosporin derivatives by reacting a 7-aminodesacetoxycephalosporanic acid derivative (7-ADCA) with an acylating agent. comprising an amine function protected by a protective group which can be in particular a t-butyloxycarbonyl group (t-BOC), the expected cephalosporin derivative then being obtained by hydrolysis of the protective group in an inert solvent. These cephalosporin derivatives are obtained in anhydrous form with a very low yield. In addition, the use of an acylating agent comprising a protective group such as t-BOC is very expensive.

 US Pat. No. 3,985,741 describes another process for the preparation of cephalosporins in which the acylating agent used is chosen from compounds in which the alpha-amino group is protected by a s-keto group such as, for example, acetylate. of methyl. This acetylating agent is a mixed anhydrous acid obtained by reaction between a carboxylic acid salt (Dane salt) and an ethyl chloroformate in the presence of a catalyst, N-methylmorpholine.

 Another synthetic method, as described, for example, in patent application FR 2,365,570, consists schematically of a) silylating 7-ADCA, then b) acylating silylated 7-ADCA in step a) with D- (-) - α-amino-α- (p-hydroxyphenyl) acetyl chloride hydrochloride in the presence of an acid acceptor such as

<Desc / Clms Page number 2>

la triéthylamine, la diméthylamine, la diméthylaniline, la quinoléine, la lutidine ou la pyridine, puis c) à cliver tous les groupes silyle du produit d'acylation de l'étape b) pour obtenir l'acide céphalosporanique désiré.

triethylamine, dimethylamine, dimethylaniline, quinoline, lutidine or pyridine, then c) cleaving all the silyl groups of the acylation product of step b) to obtain the desired cephalosporanic acid.

 The cephalosporins obtainable by these various methods must then undergo one or more crystallization and purification steps before they can be incorporated into pharmaceutical compositions.

 For this purpose, many crystallization techniques employing different types of solvents can be used.

 For example, it has been proposed, in particular in US Pat. No. 3,985,741 or in patent application FR 2,365,570, to use a solvent chosen from acetonitrile, methanol, toluene, dimethylformamide (DMF), dimethylacetamide (DMAC) and mixtures thereof.

 Given the diversity of processes for the synthesis, crystallization and purification of cephalosporins, the compounds obtained show significant variations both in terms of their structural characteristics, particularly crystallographic, and the degree of purity they exhibit (presence of traces residual solvents).

 Cephalosporin drugs are generally administered orally and may be in a variety of dosage forms such as capsules, granules or powders for oral suspension, dispersible or non-dispersible tablets.

 Administration of cephalosporins in the form of capsules or nondispersible tablets may not always be considered, especially in children and in persons suffering from the upper digestive tract and having difficulty in swallowing. Non-dispersible capsules and tablets also have a bioavailability that may be less than that of dispersible powders and tablets.

 On the other hand, the administration of cephalosporins in the form of powders or granules for oral suspension requires, before use, the reconstitution of the suspension by adding water, stirring this suspension before each use and measuring the dose. appropriate before each administration.

<Desc / Clms Page number 3>

L'ensemble de ces différentes opérations est une source d'erreurs quant à la dose de céphalosporine administrée.

All of these different operations is a source of errors as to the dose of cephalosporin administered.

 On the other hand, the presentation in the form of dispersible tablets has several advantages: the dispersible tablet, which must be dispersed in water before ingestion, always corresponds to a single and precise dose of the active principle to be administered; - This type of formulation also allows easier administration of the drug in people with swallowing problems, especially the elderly and children.

However, the formulation of active ingredients in the form of dispersible tablets requires the addition of excipients such as flavorings and sweetening agents so as to mask the odor and taste, possibly unpleasant of the active ingredient in itself, and thus improve the olfactory and gustatory perception of the drug when ingested
To date, ORACEFAL (g) is the only available drug based on cephalosporin that can be in the form of dispersible tablets. These dispersible tablets contain 1 g of active principle (cefadroxil) in combination with various excipients necessary for this kind of formulation among which may be mentioned crosslinked polyvinylpyrrolidone (known under the trade name crospovidone (k) and which is a disintegrant, the microcrystalline cellulose (binding agent), magnesium stearate (lubricating agent), sweeteners such as gluconate or sodium cyclamate or sodium saccharin, and flavors such as orange and grapefruit flavors.

 Despite the presence of sweetening agents and flavors, the presentation of ORACEFAL (R) in the form of dispersible tablets is poorly tolerated from a sensory point of view (smell and taste) during ingestion.

 It is to remedy these problems that the inventors have developed what is the subject of the invention.

 The inventors have therefore set themselves the objective of providing a dispersible pharmaceutical composition based on cephalosporin having all the

<Desc / Clms Page number 4>

avantages de ce type de formulation galénique ainsi qu'une odeur et un goût améliorés.

advantages of this type of galenic formulation as well as improved odor and taste.

 The subject of the present invention is therefore a liquid dispersible pharmaceutical composition comprising at least one cephalosporin as active principle, alone or in combination with another active principle, and at least one disintegrating agent, characterized in that said cephalosporin exhibits an N, N-dimethylacetamide (DMAC) impurity level of less than 21.4 ppm and said disintegrating agent is cross-linked sodium carboxymethylcellulose (croscarmellose (t-sodium).

 The inventors have in fact demonstrated that the specific combination of these two compounds makes it possible to obtain a dispersible pharmaceutical composition with substantially improved olfactory and gustatory properties compared to those of the prior art pharmaceutical compositions based on cephalosporins, without it is necessary to act mainly on the aromatization of the latter.

 The pharmaceutical compositions according to the invention have the additional advantage of disintegrating completely in less than 3 minutes when they are brought into contact with a liquid such as water and thus leading to an oral suspension whose homogeneity can be easily obtained by stirring.

 The pharmaceutical composition according to the invention may be in the form of dispersible tablets or dispersible granules.

 According to a particularly advantageous embodiment of the invention, the DMAC impurity level of the cephalosporins is less than 5 ppm.

 The cephalosporins which can be used as active principle in the pharmaceutical composition according to the invention are preferably chosen from cefadroxil, cephadrine, cefalexin, cefatrizine and cefixime.

 These cephalosporins must be prepared according to a synthetic process that does not require the use of dimethylaniline. However, they are preferably prepared according to a synthetic process using a Dane salt, as described for example in US Pat. No. 3,985,741.

<Desc / Clms Page number 5>

According to the invention, the croscarmellose e sodium is preferably from 1 to 25% by weight of the total weight of the pharmaceutical composition and more particularly from 2 to 10% by weight.

 The pharmaceutical composition according to the invention may furthermore contain one or more excipients which may be chosen from flow agents, lubricating agents, binding agents, sweeteners, flavoring agents, flavorings, etc.

 Among the flow agents that can be used in the pharmaceutical composition according to the invention, mention may especially be made of precipitated silica dioxide, colloidal silica, talc, stearic acid, magnesium stearate and mixtures thereof. precipitated silica dioxide being particularly preferred. These flow agents are used to prevent the tablet or granule components from forming aggregates during the preparation of these tablets or granules and also to reduce friction during compression operations. They are generally present in proportions of between 0.1 and 3% of the total weight of the pharmaceutical composition.

 Among the lubricating agents that can be used in the pharmaceutical composition according to the invention, there may be mentioned magnesium stearate, calcium stearate and mixtures thereof. These lubricating agents, whose role is to reduce the friction operations during the compression operations, are advantageously present in proportions of between 0.1% and 3% of the total weight of the pharmaceutical composition.

 Among the binding agents that can be used in the pharmaceutical composition according to the invention, there may be mentioned microcrystalline cellulose, lactose, hydroxypropyl methylcellulose (HPC), pregelatinized starch and mixtures thereof, microcrystalline cellulose being particularly preferred. The binding agents facilitate the compression operations necessary to obtain tablets and impart an adequate hardness to the tablets. When used, these binding agents preferably represent from 5 to 60% of the total weight of the pharmaceutical composition.

 The sweeteners may especially be chosen from aspartame, saccharin sodium, sodium cyclamate, acesulfame potassium,

<Desc / Clms Page number 6>

glycérinate d'ammonium et leurs mélanges. Ces édulcorants représentent de préférence de 1 à 20% du poids total de la composition pharmaceutique.

ammonium glycerinate and mixtures thereof These sweeteners preferably represent from 1 to 20% of the total weight of the pharmaceutical composition.

Although the pharmaceutical composition according to the invention has an improved odor and taste compared to the compositions of the prior art based on cephalosporin, it may nevertheless contain one or more flavors, these being able to be chosen in particular from the flavors fruit such as strawberry, lemon, raspberry, grapefruit, orange, etc. and mint, chocolate, strawberry vanilla, licorice and their mixtures
Of course, those skilled in the art will take care on this occasion that the excipient (s) possibly used are compatible with the intrinsic properties attached to the present pharmaceutical composition.

 The subject of the invention is also a process for the preparation of a dispersible pharmaceutical composition as defined above, said process being characterized in that it comprises: a) a step of premixing at least one cephalosporin having a level of N, N-dimethylacetamide impurity less than 21.4 ppm with crosslinked sodium carboxymethylcellulose optionally in the presence of a binding agent and / or a flow agent, to obtain a premix (A), b ) a step of mixing any additional excipients such as binding agents, lubricating agents, sweetening agents, flavorings, to obtain a mixture of excipients (B), c) a final mixing step of the premix (A) and the mixture of excipients (B), to obtain a final mixture (C), d) a step of granulation and / or compression of the resulting final mixture (C).

 According to the invention, the steps a) to c) of the process described above are preferably carried out with stirring and may comprise sieving sub-operations of the various ingredients used and / or mixtures obtained.

 Step d) granulation or compression can be carried out conventionally according to known methods of granulation or compression.

 Finally, the subject of the invention is the use of at least one dispersible pharmaceutical composition as defined above for

<Desc / Clms Page number 7>

améliorer la perception sensorielle (olfactive et gustative) d'un patient lors de l'administration orale d'une telle composition.

to improve the sensory (olfactory and gustatory) perception of a patient during the oral administration of such a composition.

 In addition to the foregoing, the invention also comprises other arrangements which will emerge from the description which follows, which refers to an example of demonstration of the improvement of sensory perception during the oral administration of a composition. pharmaceutical composition according to the invention compared to the administration of pharmaceutical compositions not forming part of the invention.

 It should be understood, however, that this example is given solely by way of illustration of the subject of the invention, of which it does not in any way constitute a limitation. EXAMPLE: DEMONSTRATION OF THE IMPROVEMENT OF SENSORY PERCEPTION DURING THE ADMINISTRATION OF A DISPERSIBLE PHARMACEUTICAL COMPOSITION BASED ON CEPHALOSPORINE 1) Preparation of dispersible tablets based on cefadroxil Dispersible tablets having the compositions appearing in Table 1 below have been prepared (the quantities are given in mg):

<Desc / Clms Page number 8>

Tableau 1

Table 1

<Tb>
<tb> COMPRESSED <SEP> DISPERSIBLE <SEP> (CD) <SEP> CD2 <SEP> b <SEP> CD <SEP> 3 <SEP> CD <SEP> 4a
<tb> Cefadroxil <SEP> monohydrate <SEP> prepared <SEP> according to <SEP> the <SEP> process
<tb> of the <SEP> patent <SEP> US <SEP> 3 <SEP> 98 <SEP> 741 <SEP> in <SEP> using <SEP> of <SEP> DMF <SEP> to <SEP> title <SEP > 1000 <SEP> 1000
<tb> of <SEP> solvent <SEP> and <SEP> having <SEP><SEP><SEP><SEP> impurity rate <SEP> DMAC
<tb><to<SEP> 1 <SEP> ppm
<tb> Cefadroxil <SEP> monohydrate <SEP> prepared <SEP> according to <SEP> the <SEP> process
<tb> of <SEP> Patent <SEP> US <SEP> 3 <SEP> 98 <SEP> 741 <SEP> in <SEP> using <SEP> of <SEP> DMAC <SEP> to <SEP> 1000
<tb> titer <SEP> of <SEP> solvent <SEP> and <SEP> having <SEP> a <SEP><SEP><SEP> impurity rate in SEP>
<tb> DMAC <SEP> = <SEP> 28 <SEP> ppm
<tb> Crospovidone <SEP> @ - 100
<tb> Croscarmellose <SEP> R <SEP> Sodium <SEP> 100 <SEP> 100 <SEP> Dioxide <SEP> of <SEP> precipitated silica <SEP><SEP> 2.5 <SEP> 2.5 <SEP > Stearate <SEP> of <SEP> Magnesium <SEP> 2.5 <SEP> 2.5 <SEP> 2.5
<tb> Agents <SEP> Sweeteners <SEP>:
<tb> - <SEP> Saccharine <SEP> Sodium <SEP>(SEP> Sweetening Potency <SEP> (PS) <SEP> = <SEP> 400) <SEP> 15 <SEP> 15 <SEP> 15
<tb> - <SEP> cyclamate <SEP> of <SEP> sodium <SEP> (PS <SEP> = <SEP> 25) <SEP> 135 <SEP> 135
<tb> - <SEP> ammonium glycyrrhizinate <SEP><SEP> (PS <SEP> = 50) <SEP> - <SEP> - <SEP> 70
<tb> Gum <SEP> of <SEP> guar - 250
<tb> Cellulose <SEP> microcrystalline <SEP> 1205 <SEP> 1205 <SEP> 1023, <SEP> 5
<tb> Acid <SEP> Citric <SEP> Anhydrous <SEP> 1 <SEP> 1 <SEP> Flavors <SEP> Strawberry, <SEP> Lemon, <SEP> Raspberry <SEP> 39 <SEP> 39 <SEP> 39
<tb> a: <SEP> Composition <SEP> comparative <SEP> not <SEP> doing <SEP> not <SEP> part <SEP> of <SEP> the invention
<tb> b: <SEP> Composition <SEP> according to <SEP> the <SEP> present <SEP> invention
<Tb>

Un comprimé dispersible CD 1, qui sert de référence et qui correspond à la formulation des comprimés dispersibles d'ORACEFAL (g) 1000 de l'édition 1996 du dictionnaire VIDAL & contenant 1000 mg de céfadroxil monohydrate, a également été étudié.

A CD 1 dispersible tablet, which serves as a reference and which corresponds to the formulation of the dispersible tablets of ORACEFAL (g) 1000 of the 1996 edition of the VIDAL & Dictionary containing 1000 mg of cefadroxil monohydrate, was also studied.

 The different excipients mentioned for the dispersible tablet CD 4 correspond to those present in the dispersible tablet CD 1 of ORACEFAL (s) 1000.

 The CD 2 to CD 4 tablets above were prepared as follows:

<Desc / Clms Page number 9>

a) Préparation d'un prémélange A Le céfadroxil, 80% de la quantité totale de cellulose microcristalline, la croscarmellose e sodique ainsi que la moitié de la silice (comprimés CD 2 et CD 3), ont été tamisés sur un calibreur oscillant équipé d'une grille de 1 mm.

a) Preparation of a premix A Cefadroxil, 80% of the total amount of microcrystalline cellulose, croscarmellose sodium and half of the silica (tablets CD 2 and CD 3), were sieved on an oscillating sizer equipped with a grid of 1 mm.

These sieved ingredients were then introduced into a TUMBLER type tumble-type tumble blender and mixed for 30 minutes at a speed of 19 rpm. b) Preparation of a mixture of excipients B
The remaining 20% of microcrystalline cellulose, sweetening agents, anhydrous citric acid and flavors were sieved on an oscillating sizer fitted with a 0.5 mm grid.

These sieved ingredients were then fed to a lodge granulator mixer and mixed for 2 minutes at a speed of 1450 rpm. c) Preparation of a final mixture C c. 1) Preparation of a final premix
Mixtures A and B obtained in the previous steps were calibrated separately on an oscillating sizer equipped with a 1 mm grid operating at 110 oscillations / minute.

Mixtures A and B thus calibrated, as well as the second half of the silica, were introduced into the tank of a TUMBLER type moving-bed mixer and mixed for 30 minutes at a speed of 19 rpm. c. 2) Sieving the flow agent
The flow agent, namely magnesium stearate, was sieved on an oscillating sizer equipped with a 0.25 mm grid. c. 3) Lubrication step
The magnesium stearate thus sieved was then added to the final premix obtained above in step c. 1), in a TUMBLER mobile tank mixer. The whole was mixed for 5 minutes at 19 rpm.

<Desc / Clms Page number 10>

d) Compression du mélange final C Le mélange final obtenu ci-dessus à l'étape c a ensuite été comprimé dans une machine à comprimer rotative de type FETTE P2100 avec des poinçons de diamètre 23 mm, bi plan à facettes avec une barrette de sécabilité.

d) Compression of the final mixture C The final mixture obtained above in step ca was then compressed in a FETTE P2100 type rotary compression machine with punches of diameter 23 mm, bi-plane to facet with a score bar.

 The machine was set to obtain a tablet mass of 2500 mg hardness between 60 and 180 N, and having the following characteristics: - Thickness: 6 mm, - Tensile strength: 60 to 180 N, - Friability: <1%, - Disintegration rate: $; 1 min.

2) Evaluation of the disintegration time of tablets
The total disintegration time of each of the tablets CD 1 to CD 4 above was determined after immersion in 100 ml of water per tablet.

The results obtained are shown in Table II below: Table II

<Tb>
<tb> COMPRESSED <SEP> DISPERSIBLE <SEP> CD1 <SEP> CD2 <SEP> CD3 <SEP> CD4
<tb> Time <SEP> of <SEP> disintegration <SEP> 60 <SEP> s <SEP> 30s <SEP> 35s <SEP> 60 <SEP> s
<Tb>

These results show that tablets containing a disintegrant according to the invention, i.e., sodium croscarmellose have a disintegration time about twice as short as disintegrating tablets containing a disintegrating agent not being part of of the invention, namely crospovidone t.

3) Evaluation of sensory perception during oral administration of tablets CD 1 to CD 4
This evaluation was conducted on a panel of 12 volunteers.

 Each person blindly tests the four CD1 to CD4 tablets each dispersed in half a glass of water, both from the olfactory point of view of the

<Desc / Clms Page number 11>

suspension avant ingestion que du point de vue de l'appréciation globale de celle-ci (goût, finesse, présence ou absence d'arrière goût, etc..) lors de l'ingestion. Chaque personne attribue une note allant de 1 à 10 pour l'appréciation olfactive et une note allant de 1 à 10 pour l'appréciation globale.

suspension before ingestion that from the point of view of the overall appreciation of it (taste, finesse, presence or absence of after taste, etc. ..) during ingestion. Each person assigns a score ranging from 1 to 10 for the olfactory appreciation and a score from 1 to 10 for the overall rating.

 This evaluation test makes it possible to take into account the odor after disintegration of the tablet in water. This factor is important because it reflects the desire to bring the drink to the mouth and administer the product.

The results obtained are grouped as an average in Table III below: Table III

<Tb>
<tb> TABLET <SEP> Odor <SEP> Overall <SEP> Score <SEP> After <SEP> Total
<tb> DISPERSED <SEP> Administration
<tb> A <SEP> 5/10 <SEP> 5/10 <SEP> 10/20
<tb> B <SEP> 8/10 <SEP> 7/10 <SEP> 15/20
<tb> C <SEP> 5/10 <SEP> 4/10 <SEP> 9/20
<tb> D <SEP> 6/10 <SEP> 5/10 <SEP> 11/20
<Tb>

These results demonstrate that the dispersible tablet CD 2 according to the invention, that is to say containing the combination of a cephalosporin having a DMAC impurity level of less than 21.4 ppm as a principle active and croscarmellose (1) sodium as a disintegrating agent, leads to better results, both from the point of view of smell and overall appreciation after ingestion, than those obtained with dispersible tablets CD 1, CD 3 or CD 4 not forming part of the invention.

 These results also show that the use of only one of the two elements of this combination is not sufficient to improve the sensory perception of a patient during the oral administration of such a composition.

 Indeed, a tablet containing the combination of a cephalosporin having a DMAC impurity level greater than 21.4 ppm, in combination with croscarmellose sodium as a disintegrating agent (CD 3 tablet) gives results globally equivalent to the reference (tablet CD 1).

<Desc / Clms Page number 12>

 Similarly, a tablet containing the combination of a cephalosporin having a DMAC impurity level of less than 21.4 ppm, in combination with crospovidone e as a disintegrating agent (CD4 tablet) also overall results are equivalent to the reference (tablet CD 1).

Claims (8)

1. A liquid dispersible pharmaceutical composition comprising at least one cephalosporin as active ingredient, alone or in combination with another active ingredient, and at least one disintegrating agent, characterized in that said cephalosporin has an impurity level. to N, N-dimethylacetamide less than 21.4 ppm and said disintegrating agent is crosslinked sodium carboxymethylcellulose.  2. Pharmaceutical composition according to claim 1, characterized in that it is in the form of tablets or granules.  3. Pharmaceutical composition according to claim 1 or 2, characterized in that said cephalosporin has a level of impurity in N, N-dimethylacetamide less than 5 ppm.  4. Pharmaceutical composition according to any one of the preceding claims, characterized in that said cephalosporin is selected from cefadroxil, cephadrine, cefalexin, cefatrizine and cefixime.  5. Pharmaceutical composition according to any one of the preceding claims, characterized in that the cross-linked sodium carboxymethylcellulose represents from 1 to 25% by weight of the total weight of said composition, and preferably from 2 to 10%.  6. Pharmaceutical composition according to any one of the preceding claims, characterized in that it contains one or more excipients chosen from flow agents, lubricating agents, binding agents, sweeteners, flavoring agents, and the aromas.  7. Process for preparing a dispersible pharmaceutical composition as defined above, said process being characterized in that it comprises: a) a step of premixing at least one cephalosporin having an N-impurity level, N-dimethylacetamide of less than 21.4 ppm with cross-linked sodium carboxymethylcellulose in the presence of a binding agent and / or a flow medium, to obtain a premix (A), <Desc / Clms Page number 14>  b) a step of mixing any additional excipients such as binding agents, lubricating agents, sweetening agents, flavorings, to obtain a mixture of excipients (B), c) a final mixing step of the premix (A) and the mixture of excipients (B), to obtain a final mixture (C), d) a step of granulation or compression of the resulting final mixture (C).

 8. Use of at least one dispersible pharmaceutical composition as defined in any one of claims 1 to 6 for improving the olfactory and gustatory perception of a patient during the oral administration of such a composition.