FR2656525A1 - Controlled-release pharmaceutical dosage forms and process for manufacturing them - Google Patents

Abstract

Controlled-release dosage form, which comprises an active principle in combination with a hydroxypropylmethylcellulose and at least one glyceryl ester.

Description

Controlled release drug delivery forms and method of manufacture
The present invention relates to controlled release drug delivery forms and methods for their manufacture. As used herein, the term "controlled release administration forms" embraces sustained release, sustained release, and extended release administration forms.

 The formulation of solid controlled release (L / C) administration forms, such as tablets or capsules, continues to be of interest when high levels of pharmaceutical active ingredients are to be administered. Controlled release forms may have a number of benefits such as improvements in therapeutic efficacy, reduction of side effects, or fewer daily doses compared to conventional immediate release tablets or capsules. . This results in improvements in the clinical management of the patient and improved compliance with his prescribed regime of administration.

 Many solid forms of controlled release administration are formulated as matrix units in which the active ingredient is dispersed. When placed in an aqueous environment, water is absorbed by the administration form, a proportion of the active ingredient contained in it dissolves and diffusion processes take place thereafter to release said active ingredient: this is only when all these processes have occurred that a certain amount of the ingested active ingredient is available for absorption. The speed control operation is thus regulated by the diffusion rate of the active ingredient in the system. In turn, this diffusion rate is controlled in the formulation by the incorporation of one or more excipients acting as a release control agent (LCD).

 Liberation control agent incorporation levels of 20% to 50% of the weight of the final administration form are common. This means that the amount of active ingredient, which can be incorporated into a unit dose of reasonable size, is limited. It follows that with active ingredients, used at relatively high dose levels, large tablets or capsules are needed which may be difficult to swallow for the patient or that a therapeutically useful single dose is to be subdivided in addition to a unit of administration: these two factors are contrary to the advantages, perceived by the patient, of an ideal product with controlled release.

 Disadvantages arise with many controlled release matrix delivery forms due to the need to incorporate high levels of release control agent to provide a therapeutically advantageous rate of release of active ingredient from tablets or tablets. individual capsules.

 The Applicant has found that, by a suitable choice of release control agents and production method, very satisfactory controlled release tablets can be made with low levels of release control agent by allowing the formulation of principles. active agents commonly administered at relatively high dose levels in tablets which are easily swallowed by the patient and where the required dose is contained in such an administration unit.

 In accordance with the present invention, a controlled release delivery form is produced by combining an active ingredient and a hydroxypropylmethylcellulose (HPMC) with at least one glyceryl ester. The glyceryl ester is used in solution in a solvent, preferably a relatively nonpolar hot solvent such as hot alcohol. The resulting mixture can then be subjected to an appropriate tableting process.

 Preferably, the active ingredient in pulverulent form is mixed with the hydroxypropylmethylcellulose and the solution of the glyceryl ester is then added.

 Controlled release formulations, produced by the above method, preferably comprise from 5% to 30% by weight of release control agents but, in particularly preferred embodiments, the release control agent represents 12% or less of the total composition.

 The relative amounts of hydroxypropylmethylcellulose and glyceryl ester (s) in the formulation may be chosen to vary the mode of release of the active ingredient. Preferably, the ratio of hydroxypropylmethylcellulose to the ester or glyceryl esters is from 5: 1 to 0.3: 1 and preferably from 3: 1 to 0.5: 1 and in particular preferably from 2 to : 1 to 0.5: 1.

The materials are used together in a specific proportion since the Applicant has surprisingly found that when small amounts of hydroxypropylmethylcellulose are incorporated into controlled release tablets made with glyceryl ester as the control agent of release, an increase in dissolution rate of the active ingredient is found. However, when larger amounts of hydroxypropylmethylcellulose are used, the rate of release is similar to or somewhat less than that using glyceryl ester alone but the mode of release is improved.
Applicant has also observed that by increasing the amount of hydroxypropylmethylcellulose in the formulation, there is an unexpected and surprising change in the mechanism by which the active ingredient is released, this change occurring at relatively low concentrations of hydroxypropylmethyl -cellulose. At low weight ratios of hydroxypropyl methylcellulose to glyceryl ester, the release mechanism is essentially the same as that for glyceryl monostearate (GMS) alone. As the weight ratio is increased above about 0.3: 1, the release mechanism changes and the kinetics become much more similar to that of a system containing hydroxypropylmethylcellulose alone as a release control agent. By appropriate selection of the amounts of glyceryl ester and hydroxypropylmethylcellulose, the release can be carried out to show elements of both the controlled release and controlled erosion release mechanisms thereby improving the most serious problems. associated with either of these mechanisms alone.

 By the correct choice of the amount of glyceryl ester and hydroxypropylmethylcellulose, release from the tablet can have a direct linear relationship with time over a substantial portion of the total release. This is a particularly advantageous situation in that the active ingredient is made available for absorption at a constant rate. In addition, for hydroxypropyl methylcellulose to glyceryl ester ratios above about 0.3: 1, the dissolution kinetics remain predictable over a wide range of glycerol ester hydroxypropylmethylcellulose weight ratios. and indicates that minor process variations will have little effect on the release properties of the final product.

 Concentrations of hydroxypropylmethylcellulose are selected to give ratios in the aforementioned fields and suitable concentrations of the hydroxypropylmethylcellulose component may be from 5% to 20%, preferably from 5% to 1% by weight and Suitable glyceryl ester derivatives are from 1% to 10%, preferably from 1% to 7% by weight of the composition and in particular preferably from 3% to 7% by weight.

 The glyceryl ester is suitably a mono-, di- or tri-glyceride of a fatty acid, for example glyceryl monostearate or a mixture of variously substituted glycerides. Suitable hydroxypropylmethylcelluloses include Methocel E and Methocel K.

 Other innocuous food or pharmaceutical grade carrier materials may be included in the formulation in accordance with conventional drug manufacturing technology.

 For example up to 2% magnesium stearate may be added as a lubricant to facilitate tablet compression.

Polyvinylpyrrolidone can also be added to facilitate tableting.

 We have found that the use of other commonly applied methods such as the "hot melt" technique or direct compression rather than the method of the present invention tend to produce tablets with much lower release characteristics. Indeed, by the use of such methods, the required amounts of release control agent to achieve adequate release control unsatisfactorily correspond to the high levels mentioned above.

 One possible explanation for this observation is that the use of a glyceryl ester solution results in the particles of hydroxypropylmethylcellulose and active ingredient becoming coated to each give discrete particles with a fatty coating.

Hydroxypropylmethylcellulose is thus prevented from making channels in the formulation for the penetration of water. It will thus be apparent that the present invention also provides a controlled release formulation comprising an active ingredient and a release control agent, said release control agent comprising discrete particles of a hydroxypropyl methylcellulose and a glyceryl ester , the glyceryl ester providing each particle with a fatty coating
In the case where alcohol is used as a solvent for the glyceryl ester, the coating may be particularly effective because the polarity of the solvent is intermediate between those of the hydroxypropyl methylcellulose and the coating.

Embodiments of the present invention are described below by way of example. In the following examples, the glyceryl ester component of the release control agent system comprises a mixture of glyceryl monostearate (GMM) meeting the specifications given in the monograph of the
Glyceryl monostearate of the European Pharmacopoeia which is a mixture of monoglycerides of stearic and palmitic acids together with varying amounts of di- and triglycerides. It contains not less than 35.0 percent of monoglycerides calculated as C20H4004 and not more than 6.0 percent of free glycerol. Such material is available and sold by Dynamit Nobel under the trademark "Imwitor 900".

It is used together with hydroxypropylmethylcellulose (HPMC) meeting the specifications given in the monograph of Hydroxypropylmethylcellulose 2910
Pharmacopeia of the United States XXI (1985).

 Among suitable hydroxypropylmethylcellulose grades are those having a methoxyl substitution level of 1.36 to 1.90 to give a methoxyl content of 22% to 30% and a hydroxypropyl molar substitution of 0.18 to 0. To give a hydroxypropyl content of from 8.1% to 8.5%. Qualities of these materials having nominal viscosity values of 100 cP to 15000 cP as a 2% aqueous solution at 20 C can be employed satisfactorily.

In the examples which follow, tablets according to one embodiment of the invention were made by (a) mixing the active ingredients in the form of a fine powder with
hydroxypropylmethylcellulose and other selected materials
excipient required by the particular formulation for
forming a uniformly distributed powdery mixture (b) dissolving glyceryl monostearate in alcohol or in a
other volatile lipid solvent leaving no
residue during evaporation and suitable for food use
or pharmaceutical, at a high temperature so as to form a
optically clear solution (c) adding an appropriate amount of purified water to the mixture
powder to form a suitable final wet granule as established
by normal pharmaceutical practice (d) adding the solution of glyceryl monostearate in the solvent
suitable for moistened powder mass with continuous stirring
to obtain an even distribution of monostearate
glyceryl in the mass; the resulting granulate can be sieved
to form a granule of appropriate grain size (e) drying the resulting wet granulate and sifting a new one
time, if necessary, to adjust the grain size
final (f) mixing the resulting dry granulate with a suitable lubricant
such as magnesium stearate (g) compacting the granule into tablets.

In the figures
Figure 1 shows the percentage of theophylline released as a function of time for tablets made in accordance with one embodiment of the method of the present invention. The amount of hydroxypropyl methylcellulose added in the formulation was varied, but in each case the amount of glyceryl monostearate in the formulation was six percent.
FIG. 2 shows the percentage of theophylline released as a function of time for a 416 mg tablet containing 350 mg theophylline and made in accordance with the method of the present invention and for a commercially available "Lasma" tablet, weighing 810 mg, containing 300 mg theophylline and employing hydroxypropylmethylcellulose alone as a release control agent.

Example 1 Tablets Containing Theophylline
Two mixtures (mixture A and mixture B) were prepared with the following ingredients
Quantity per tablet (mg)
Mixture A Blend B - Theophylline (European Pharmacopoeia) 500.00 350.00 - Povidone (British Pharmacopoeia) 23.75 16.62 - Glyceryl Monostearate (Pharmacopoeia
European) 16,86 11,80 - Hydroxypropylmethylcellulose (Pharmacopoeia)
of United States) 47,18 33,03 - Magnesium Stearate (Pharmacopoeia
European) 5.94 4.16
The total content of release control agents in these formulations is 10.8 r: the content of active pharmaceutical active ingredient is 84.2%.

 Theophylline, povidone and hydroxypropylmethylcellulose were mixed together and first granulated with cold purified water to form a granule of appropriate consistency and then with the glyceryl monostearate dissolved at about 65 ° C to 70 ° C. approximately three times its own weight of alcohol (ethanol, 96%, satisfying the specifications of the European Pharmacopoeia) The resulting mass was sieved through a sieve having 1 mm orifices and dried at a temperature of 45 ° C. in a dryer The resulting dry granulate was sieved again through a sieve having apertures of 0.8 mm to dislocate any agglomerates which formed, mixed with magnesium stearate in a drum mixer and compressed using Capsule-shaped punches on a rotary tablet machine The resulting tablets had a weight of about 594 mg in the case of the use of melan and about 416 mg in the case of the use of the mixture B and each contained a therapeutically usable dose of 500 mg theophylline in the case of using the mixture A and 350 mg theophylline in the case of the use of the mixture B.

 The tablets were subjected to a solution rate test using US Pharmacopoeia Apparatus XXI at a paddle speed of 80 rpm in acidic medium (pH: 1.2) for 2 hours. followed by a neutral pH medium (pH: 7).

The in vitro release characteristics of these tablets were as follows
TABLE 1
Theophylline release regimen of controlled release tablets
Time (h)% of nominal theophylline content released
Blend A Blend B
1 13.9 13.2
22.3 22.2
3 27.5 30.9
4 33.2 37.6
5 37.9 43.7
6 42.5 49.7
7 46.5 55.3
8 50.4 60.9
9 53.9 66.4
10 57.5 71.4
11 61.0 77.6
12 64.8 82.7
13 68.9 87.7
14 75.6 91.1
15 84.2 94.1
16 93.1 96.8
17 99.0 98.8
18 102.9 102.3
The active agent release regimen, theophylline, of these tablets clearly indicates a satisfactory release profile over time. The scheme is indicative of a therapeutically useful extension of the active ingredient's entry time and availability when administered to a human. Similar theophylline tablets were made according to the method described above. In each case, the tablets contained 6% glyceryl monostearate along with varying amounts of added hydroxypropylmethylcellulose. Theophylline release from the tablets was measured according to the method described above and the percentage of theophylline released was graphed as a function of time. The results are shown in Figure 1. It is apparent from the data that at very low levels of hydroxypropylmethylcellulose added, the release rate from the tablets is increased relative to that from the formulation containing glyceryl monostearate. only.However, as the level of hydroxypropylmethylcellulose increases, the release gradually slows down.

 This slowing down of the release rate is accompanied by the desirable kinetics described above. The advantageous effects associated with the tablets of the present invention are also clearly shown in Figure 2. The dashed broken line in the graph represents the release pattern for a commercially available theophylline tablet, weighing 810 mg, of which 300 mg is the theophylline active ingredient. The tablet contains hydroxypropyl methylcellulose as a release control agent.

The solid line in the figure represents the very similar release pattern for a 416 mg tablet made according to the process of the present invention and containing 350 mg theophylline together with hydroxypropyl methylcellulose / glyceryl monostearate as a control agent. of liberation. Substantially the same release pattern is obtained with a tablet having just over half the mass of the commercially available product and more of the active ingredient.

 Samples of the tablets of mixture A and mixture B described above on page 9 were administered to 12 healthy human volunteers who had fasted for 12 hours before taking the tablet and on a second occasion after they took a breakfast having a high lipid content to simulate known conditions with other unsatisfactory controlled release formulations to cause an inadvertent release of active ingredient that may give rise to toxic side effects. On a third occasion, volunteers received theopylline in aqueous solution to provide a baseline representing an immediate release product. The important pharmacokinetic parameters of this study are given in Table 2 below.

 It is evident from the table that not only does the product, manufactured in accordance with the present invention, give very satisfactory patterns of in vitro release but, when administered to a man, reveals a very satisfactory prolongation of the time of release. input of active ingredient, which should be of considerable therapeutic benefit to the patient. The data presented in the table also indicate that the absorption of active ingredients from a tablet, when administered to a patient, occurs at a desired almost constant rate.

TABLE 2
Mean parameters defining the pharmacokinetics of theophylline administered to 12 healthy male volunteers in the form of a solution or a controlled release product administered on an empty stomach and after a high-fat meal

<tb><SEP> Tablet <SEP> to <SEP> release
<tb><SEP> Controlled <SEP> SOLUTION <SEP> *
<tb><SEP> PARAMETER
<tb><SEP> 500 <SEP> mg
<tb><SEP> 500 <SEP> mg <SEP> 350 <SEP> mg
<tb><SEP> to <SEP> fast <SEP> after <SEP> to <SEP> fast
<tb><SEP> meal
<tb><SEP> 2h <SEP> 0.248 <SEP> 0.223 <SEP> 0.355
<tb> Fraction <SEP> of <SEP> t <SEP> 0.08 <SEP> t <SEP> 0.15 <SEP> t <SEP> 0.12
<tb> the <SEP> quantity
<tb> ultimate <SEP> of <SEP> 4h <SEP> 0.493 <SEQ> 0.458 <SEP> 0.633 <SEP> - <SEP>
<tb> theophylline <SEP> t <SEP> 0.15 <SEP> t <SEP> 0.18 <SEP> t <SEP> 0.10
<tb> absorbed
<tb><SEP> 10h <SEP> 0.938 <SEP> 0.967 <SEP> 0.986
<tb><SEP> i <SEP> 0.15 <SEP> t <SEP> 0.07 <SEP> t <SEP><SEP> 0.03
<tb> Concentration <SEP> maximum <SEP> of
<tb> theophylline <SEP> in <SEP> plasma <SEP> 5.69 <SEP> 7.71 <SEP> 4.15 <SEP> 7.92 <SEP> t <SEP> 1.1
<tb> (Cmax <SEP> - <SEP> mg / l <SEP> t <SEP> difference <SEP> type) <SEP>! <SEP> 1.3 <SEP> + <SEP> 2.2 <SEP> t <SEP> 1.0 <SEP><SEP> 11.31 <SEP> t <SEP> 1.6 ** <SEP>
<tb> Time <SEP> for <SEP> to achieve <SEP> Cmax <SEP> 8.85 <SEP> 7.52 <SEP> 7.18 <SEP> 1.38 <SEP> + <SEP> 0.8
<tb> (tmax <SEP> - <SEP> h <SEP> t <SEP> deviation <SEP> type) <SEP> 4,4 <SEP> 1,9 <SEP> t3 <SEP>
<tb> Half-life <SEP> terminal <SEP> 6.19 <SEP> 5.89 <SEP> 6.02 <SEP> 5.72 <SEP>'<SEP> 1.5
<tb> (t <SEP> - <SEP> h <SEP> t <SEP> deviation <SEP> type) <SEP> z <SEP> 2,3 <SEP> t <SEP> 1,7 <SEP> t <SEP> 2.1
<tb> Purification <SEP> - <SEP> - <SEP> - <SEP> 76,13 <SEP> t <SEP> 22,2
<tb> (Cl <SEP> - <SEP> ml / h / kg <SEP> t <SEP> difference <SEP> ype)
<tb> Volume <SEP> of <SEP> distribution <SEP> - <SEP> - <SEP> - <SEP> 0.59 <SEP> + <SEP> 0.09
<tb> (Vz <SEP> - <SEP> 1 / kg <SEP> t <SEP> difference <SEP> type) <SEP><SEP> I <SEP> I <SEP> I <SEP>
<Tb>
* 2-way ANOVA ** 350 mg administered: standardized results at a dose of 500 mg
allow comparison with data on controlled release tablets
Example 2 Tablets Containing Indomethacin
A lot of tablets, containing indomethacin which is a non-steroidal and anti-inflammatory active ingredient having a very low solubility in water, was developed to determine if the controlled release system according to the present invention is applicable. to substances with extremely poor solubility.

The batch was prepared with the following ingredients
Quantity per tablet (mg) - Indomethacin (British Pharmacopoeia) 82.5 - Povidone (British Pharmacopoeia) 10.0 - Glyceryl Monostearate (Pharmacopoeia)
European) 24,5 - Hydroxypropylmethylcellulose
(United States Pharmacopoeia) 24.5 - Calcium Hydrogen Phosphate
(European Pharmacopoeia) 267.5 - Magnesium Stearate (Pharmacopoeia
European) 3.0
The total content of release control agents in this formulation is 11.9%: the content of active ingredient is 20%.

Calcium hydrogen phosphate (64.9%) was used as a physiologically inert filler.

 Indomethacin, povidone, hydroxypropyl methylcellulose and calcium hydrogenphosphate were mixed to give a uniform and granulated mixture as described in Example 1. Tablets, each weighing approximately 412 mg, were made by compression. and the release scheme of the active ingredient, indomethacin, determined using the US Pharmacopoeia Apparatus XXI. The results obtained are shown in Table 3 below and indicate a satisfactory profile of release over time of the active principle of potential therapeutic utility.

TABLE 3
Indomethacin release schedule from controlled release tablets
Time (min)% nominal content of released indomethacin
30 1.3
45 1.8
60 2.0
75 2.8
90 5.7
105 6.5
120 7.1
135 8.0
150 9.0
Example 3 Tablets Containing Ethamsylate
A lot of tablets, containing ethamsylate, which is a non-hormonal antihemorrhagic agent with a very high solubility in water, was manufactured to determine if the controlled release system according to the present invention is applicable to substances having an extremely high aqueous solubility.

The batch was prepared with the following ingredients
Quantity per tablet (mg) - Ethamsylate 82.5 - Povidone (British Pharmacopoeia) 10.0 - Glyceryl Monostearate (Pharmacopoeia
European) 24,5 - Hydroxypropylmethylcellulose (Pharmacopoeia
of the United States) 24,5 - Calcium hydrogen phosphate (Pharmacopoeia
European) 267,5 - Magnesium stearate (European Pharmacopoeia) 3,0
The total content of release control agents in this formulation is 11.9%; the content of active ingredient is 20%; calcium hydrogen phosphate (64.9%) is used as a physiologically inert filler.

 Ethamsylate, povidone, hydroxypropylmethylcellulose and calcium hydrogenphosphate were mixed to give a uniform and granulated mixture as described in Example 1. Tablets, each weighing about 412 mg, were made by compression. and the release scheme of the active ingredient, ethamsylate, determined using the US Pharmacopoeia Apparatus XXI. The results are shown in Table 4 below and indicate a significant prolongation of release of the active ingredient compared with an immediate release product, in which all the drug product is released in solution in 5 minutes.

TABLE 4
Ethamsylate Release Scheme from Controlled Release Tablets
Time (min)% of nominal content of ethamsylate released
30 42.7
45 51.1
60 57.4
75 62.1
90 68.0
105 72.1
120 75.2
135 78.8
150 81.8

Claims (11)

 1. A controlled release administration form, characterized in that it comprises an active ingredient in combination with a hydroxypropylmethylcellulose and at least one glyceryl ester.  2. A form of administration according to claim 1, characterized in that it comprises 5 to 30% by weight of hydroxypropylmethylcellulose and ester (s) of glyceryl.  3. A form of administration according to claim 2, characterized in that it comprises from 5 to 12% by weight of hydroxypropylmethylcellulose and ester (s) of glyceryl.  4. A form of administration according to one of claims 1 to 3, characterized in that the ratio of hydroxypropylmethylcellulose to the ester or glyceryl esters is 5: 1 to 0.3: 1.  5. The form of administration according to claim 4, characterized in that the ratio of hydroxypropylmethylcellulose to the ester or esters of glyceryl is from 3: 1 to 0.5: 1.  The form of administration according to claim 5, characterized in that the ratio of hydroxypropylmethylcellulose to ester or glyceryl esters is from 2: 1 to 0.5: 1.  7. A method of manufacturing the administration form according to one of claims 1 to 6, characterized in that it comprises the combination of an active ingredient and a hydroxypropylmethylcellulose with at least one glyceryl ester.  8. Process according to claim 7, characterized in that the glyceryl ester is used in solution in a solvent.  9. The method of claim 8, characterized in that the solvent is a relatively non-polar hot solvent.  10. Method according to any one of claims 7 to 9, characterized in that it further comprises a step of tabletting.  11. Method according to any one of claims 7 to 10, characterized in that it comprises the steps of bringing the active ingredient in a powder form, to mix the resulting active pulverulent ingredient with hydroxypropylmethylcellulose and to add a solution of glyceryl ester.