TREA

Lactose and cellulose-based tableting aid

Follow

Information

  • Patent Grant
  • 8663684
  • Patent Number
    8,663,684
  • Date Filed
    Monday, September 21, 2009
    15 years ago
  • Date Issued
    Tuesday, March 4, 2014
    10 years ago
Information
Abstract
The present invention concerns a process for producing a granulate based on lactose and cellulose (derivative), a granulate obtainable by the process and its use as a tabletting excipient.
Description
CROSS-REFERENCE TO RELATED APPLICATIONS

This application is a U.S. national phase under 35 U.S.C. §371 of International Patent Application No. PCT/EP09/62203 filed Sep. 21, 2009, which in turn claims priority of German Patent Application No. 102008047910.1 filed Sep. 19, 2008. The disclosures of such international patent application and German priority patent application are hereby incorporated herein by reference, in their respective entireties, for all purposes.


DESCRIPTION

The present invention concerns a process for producing a granulate based on lactose and cellulose (derivatives), a granulate that can be obtainable by the process and its use as a tabletting excipient.


Tablets are defined from a technological perspective as solid single dosage forms of pharmaceuticals which are produced by compressing powders or granulates into various forms. The composition of tablets can be extremely varied and must be individually developed for each active ingredient, for each intended use and for each manufacturing technology.


Typical tablet formulations contain, in addition to the pharmaceutically active component, so-called tabletting excipients such as e.g. fillers (lactose, cellulose powder, calcium diphosphate, microcrystalline cellulose, sugar alcohols, e.g. mannitol, sorbitol and starch), disintegrants (starch (derivatives), croscarmellose, cross-linked PVP, carboxymethyl cellulose, lubricants (stearic acid, magnesium stearate), glidants (silicon dioxide (aerosil)) or mixtures thereof. Tabletting excipients are additives which enable tablets to be manufactured at all in a practical manner and have an important effect on the processability of the tablet formulation and on the properties of the finished tablet. The tabletting excipients are selected depending on the dosage form and on the active components that are used.


Usually the pharmaceutically active components are processed together with the respective tabletting excipients to form a granulate with the aid of a solvent, the tablet being compressed in a subsequent step to form a tablet.


The simplest and most economical way of producing tablets is, however, direct tabletting i.e. tabletting without previous granulation of an active component or active components and tabletting excipients. Tablet formulations which are suitable for direct tabletting must have a sufficient plastic deformability and good flow properties and should not exhibit any segregation tendency. It is extremely difficult to manage these three requirements which is why it has previously only rarely been possible to carry out direct tabletting (K. Bauer, “Pharmazeutische Technologie”, 1993, publisher Georg Thieme, Stuttgart).


In the case of tablet formulations that can be directly compressed, the particle size of the pharmaceutically active component and the direct (tabletting excipient) should be between 10 and 1000 μm in order to minimize segregation of the components in the tablet formulation. Different particle size distributions of pharmaceutically active components, direct tabletting excipients and optionally additionally of auxiliary substances are especially critical when the tablet formulation consists of at least three components.


However, in addition to cost effectiveness, another advantage of direct tabletting is that no granulation of the pharmaceutically active component is necessary and thus solvent-sensitive components can also readily be processed.


Hence, there is a great demand for tabletting excipients which can be simply mixed with the pharmaceutically active component and optionally with additional tabletting excipients and subsequently be directly compressed (direct tabletting excipient).


The property profile of directly compressible tablet formulations described above is in most cases not achieved by simply mixing commercially available individual components of a tablet formulation (physical mixing). Mixed granulates comprising different tabletting excipients are therefore often used.


Such mixed granulates are especially suitable for use as a direct tabletting excipient but are also advantageous as tabletting excipients for the conventional production of tablets.


U.S. Pat. No. 6,770,368 describes a granulate consisting of starch and lactose as excipients for direct tabletting. For this a solution or suspension of the two components is dried in a spray drying process.


U.S. Pat. No. 4,693,750 describes an excipient for direct tabletting which is essentially composed of lactose and cellulose. For this cellulose powder and lactose is mixed in hot water and subsequently spray dried. The powder that is obtained is characterized by its flow properties and, in a compressed form, by its tablet hardness.


EP 0 948 321 discloses the production of a lactose/ethyl cellulose preparation in which the two components are dispersed in water with the aid of a stirrer and are subsequently sprayed in a laboratory spray tower. A readily flowable spray agglomerate is obtained and is used among others as a direct tabletting excipient.


Lactose (milk sugar) is used nowadays on a large scale as a tabletting excipient among others in pharmaceuticals, in foods and also in the technical industry. Lactose belongs to the group of disaccharides and consists of the two molecules β-D-galactose and α/β-D-glucose which are linked together by a β-1,4-glycosidic bond.


An advantage of lactose as a tabletting excipient is its low hygroscopicity, its favourable price, its good water solubility and its inertness towards most pharmaceutically active components.


Lactose is available on the market in two modifications i.e. as anhydrous lactose and as lactose monohydrate. Lactose monohydrate is preferred since it is less hygroscopic compared to anhydrous lactose and is thus more suitable in compositions which contain water-sensitive pharmaceutically active components.


Cellulose is a polysaccharide which is composed of a large number of β-D-glucose molecules which are linked by a 1,4-β-glycosidic bond. The hydroxyl groups present in the polysaccharide can be chemically converted in a variety of ways. Thus, the hydroxyl groups of cellulose can independently of one another be at least partially alkylated, hydroxyalkylated, sulfonated, nitrated, carboxyalkylated or/and xanthogenated under certain reaction conditions.


The modified celluloses obtained in this manner are cellulose derivatives whose profile of properties e.g. with regard to water solubility and active substance compatibility can be customized for the respective application.


Cellulose and cellulose derivatives and in particular hypromellose (hydroxypropylmethyl cellulose (HPMC)), hypromellose phthalate, hydroxypropyl cellulose (HPC), hydroxyethyl cellulose (HEC), carboxymethyl cellulose (CMC), carboxyethyl cellulose (CEC), ethyl cellulose (EC) as well as salts thereof are suitable as excipients in the tablet formulation.


In order to produce sustained-release tablet cores it is desirable to increase the content of cellulose derivatives to at least 15%, preferably at least 20%. However, at this concentration the flow properties of the formulation are often very limited and it is difficult or even impossible to process the formulation to make tablets especially by way of direct pressing.


With regard to the prior art, it is therefore desirable to provide tabletting excipients and in particular direct tabletting excipients by means of which the profile of properties of tablet formulations with regard to flow behaviour and/or compressibility and the profile of properties of the tablets produced therefrom are further improved with regard to tablet hardness, friability resistance, release profile and/or compressing force-hardness profile.


Hence the present invention provides a process for producing a granulate comprising the steps


i) suspending or/and at least partially dissolving lactose and optionally at least one component consisting of cellulose or/and cellulose derivative in at least one liquid and


ii) atomizing the solution or suspension obtained in i) in an environment above room temperature in the presence of cellulose (derivative) particles and optionally lactose particles during which the liquid is at least partially removed.


It was found that the flow properties and the particle sizes of the granulate according to the invention can be easily adjusted in step ii) such that they allow a simple direct tabletting which is not possible with a physical mixture of the corresponding components. Furthermore, tablets whose friability resistance and tablet hardness are significantly increased at the same compaction pressure compared to a tablet in which a physical mixture of the granulate components is used can be surprisingly obtained in the direct tabletting process by using the granulate according to the invention consisting of lactose and cellulose (derivative).


Lactose can be used in an anhydrous form or as lactose monohydrate for the process according to the invention. Lactose monohydrate is preferably used because of its already mentioned lower hygroscopicity compared to anhydrous lactose.


The cellulose or/and cellulose derivatives used in step ii) and optionally in step i) can be selected independently of one another and are the same or different.


Cellulose is preferably obtained from natural sources and is optionally purified in subsequent steps.


Cellulose derivatives are chemically modified celluloses in which the hydroxyl groups are at least partially alkylated, hydroxyalkylated, sulfonated, nitrated, carboxyalkylated or/and xanthogenated independently of one another.


In particular natural cellulose or/and cellulose derivatives or mixtures thereof in which the hydroxyl groups of the cellulose are independently of one another at least partially alkylated, hydroxyalkylated, sulfonated, carboxyalkylated or/and xanthogenated are used in the process according to the invention. Cellulose derivatives in which the hydroxyl groups of the cellulose are independently of one another at least partially methylated, ethylated, hydroxypropylated, hydroxypropylmethylated, hydroxyethylated, carboxymethylated or/and carboxyethylated are particularly preferably used in the process according to the invention.


Cellulose ethers are preferably used as cellulose derivatives due to their good compressibility. Examples of these are hypromellose (hydroxypropylmethyl cellulose (HPMC), hypromellose pthalate, hydroxypropyl cellulose (HPC), hydroxyethyl cellulose (HEC), carboxymethyl cellulose (CMC), carboxyethyl cellulose (CEC), ethyl cellulose (EC) as well as salts thereof (sodium or/and calcium salts.


Hypromellose (HPMC), hydroxypropyl cellulose (HPC) and hydroxyethyl cellulose (HEC) and in particular hypromellose (HPMC) are particularly preferably used.


The molecular weight of the cellulose (derivatives) can vary within wide ranges and is preferably between 1×103 and 2×106 g/mol and more preferably between 5×105 and 1.5×106 g/mol (Mn).


Lactose and optionally at least one component consisting of cellulose or/and cellulose derivative are suspended or/and at least partially dissolved in at least one liquid. Any medium which is present in a liquid aggregate state under certain pressure and temperature conditions and is inert towards the starting materials that are used (lactose and optionally cellulose (derivative)) can be used as the liquid.


Water or organic solvents can for example be used as the liquid. Suitable organic solvents are for example methanol, ethanol or acetone. Mixtures of liquids can also be used in another embodiment.


Water, ethanol and mixtures thereof are preferably used as the liquid in step i). Water is a particularly preferred liquid.


In order to produce the solution or/and suspension, the starting materials (lactose and optionally cellulose (derivative)) are incorporated into at least one liquid for example while stirring mechanically. Standard stirring devices are used for the incorporation.


In order to accelerate the dissolving of the starting materials, the liquid can be heated to 30° C. to 90° C., preferably to 40° C. to 70° C. during the incorporation step.


The weight ratio between lactose and cellulose (derivative) in step i) is for example between 100/0 to 5/95, preferably between 100/0 to 10/90, particularly preferably between 100/0 to 30/70 and more preferably of 100/0 to 60/40.


In a particularly preferred embodiment the ratio between lactose and cellulose (derivative) in step i) is 100/0, i.e. only lactose is at least partially dissolved or/and suspended in at least one liquid.


The proportion by weight of lactose and optionally cellulose (derivative) in the liquid is in a range of about 2 to 80% by weight, preferably between 5 and 70% by weight and particularly preferably between 10 and 60% by weight.


In step i) it is also preferred that at least 5% by weight, preferably at least 20% by weight, more preferably at least 80% by weight and most preferably 100% by weight based on the total content of lactose is present in a dissolved form in the liquid.


The average particle size of a suspension obtained in i) should be in a range between 0.1 μm and about 1000 μm, preferably between 1 μm and 500 μm, particularly preferably between 2 μm and 200 μm.


The solution or/and suspension obtained in step i) which can have a temperature of 20 to 90° C., preferably of 20 to 70° C., more preferably of 40 to 70° C. is subsequently atomized in step ii) for example by means of a nozzle into droplets with an average diameter of 15 μm to 1250 μm, preferably of 20 μm to 1000 μm, particularly preferably of 40 μm to 750 μm in an environment with a temperature of about 30 to 250° C., preferably of about 40 to 170° C.


The pressure in the environment in which the droplets are introduced is in a range of about 0 to 1.0 bar, preferably of 0.003 to 0.7 bar and particularly preferably of 0.005 to 0.5 bar.


Suitable atomizing nozzles are for example one-material, two-material or multiple-material pressure nozzles such as for example turbulence, flat-jet, rebound or hollow cone pressure nozzles, pneumatic nozzles and also ultrasonic nozzles. In a preferred embodiment single-material nozzles are operated at a nozzle pressure of 20 to 250 bar, preferably of 30 to 200 bar and two- or multiple-material nozzles are operated at a nozzle pressure of 0.1 to 10 bar, preferably of 0.3 to 5 bar.


Atomizing a liquid or/and suspension in an environment having an elevated temperature and optionally reduced pressure, has the effect that the liquid is at least partially removed from the droplets. This process is technically known as spray drying.


The solution or/and suspension obtained in step i) is preferably atomized in the presence of cellulose (derivative) particles and optionally lactose particles, preferably on cellulose (derivative) particles and optionally lactose particles. The cellulose (derivative) particles and lactose particles have an average diameter of about 1 μm to about 500 μm, preferably of 2 μm to 300 μm and particularly preferably of 5 μm to 200 μm.


A preferred weight ratio of cellulose (derivative) particles to lactose particles in step ii) is in a range of 100/0 to 5/95, particularly preferably of about 100/0 to about 50/50. In a preferred embodiment the suspension or/and solution obtained in i) is only atomized on cellulose (derivative) particles (cellulose (derivative) particles/lactose particles is 100/0).


In one embodiment the cellulose (derivative) particles or/and lactose particles can be in a suitable mixer while the solution or/and suspension obtained in step i) is atomized thereon. The liquid is at least partially removed from the droplets by suitable drying processes under the above-mentioned conditions of wet granulation.


In another embodiment the suspension or/and solution obtained in step i) is atomized on the cellulose (derivative) particles and optionally lactose particles while the totality of the cellulose (derivative) particles and optionally lactose particles are present in a flow bed or fluidized bed.


The fluidized bed is a filling of cellulose (derivative) particles and optionally lactose particles which is fluidized by a directed flow of a gas.


When the suspension or/and solution obtained in step i) is sprayed onto a fluidized bed (fluidized bed granulation process), the individual cellulose (derivative) particles or/and lactose particles are present essentially separate from one another so that the solution or/and suspension obtained in step i) can be homogeneously and completely distributed on the surface of the fluidized cellulose (derivative) particles and optionally lactose particles. The liquid is at least partially removed during the fluidized bed granulation process.


In another embodiment the suspension or/and solution obtained in step i) is atomized on the cellulose (derivative) particles and optionally lactose particles which are in an air current. In this process the amount of fine material in the particles can be reduced in order to achieve a further agglomeration of the particles. The liquid is at least partially removed during this process.


The fluidized bed granulation process is preferred in the present invention.


The wet granulation process is preferred in another embodiment.


Usually pressure and temperature in the environment are adjusted such that the droplets are not already completely dry before they impact the cellulose (derivative) particles or/and optionally lactose particles. This results in a homogeneous dispersion of the solution or/and suspension used in step i) on the cellulose (derivative) particles and optionally lactose particles.


After the atomization of the solution or/and suspension obtained in step i) on the cellulose (derivative) particles or/and lactose particles, liquid can continue to be removed from the product obtained under the environmental conditions until the content of free liquid in the granulate is <8% by weight, preferably <6% by weight and particularly preferably <4% by weight based on the total mass of the granulate.


The granulate obtained has a ratio of lactose to cellulose (derivative) of about 95/5 to 1/99, preferably 90/10 to 5/95 and more preferably between 60/40 and 40/60.


The granulate particles obtained are preferably spherical or spheroid. Such a morphology is advantageous for the flow properties of the granulate. The granulate particles have a d50 particle size distribution of 25 to 750 μm, preferably of 30 to 500 μm, more preferably of 40 to 350 μm. A person skilled in the art is aware that the particle size of the granulate can be adjusted within wide ranges by the process parameters (environmental conditions, spray rate, particle size in the suspension, particle size of the cellulose (derivative) particles and lactose particles etc.).


The process according to the invention enables a granulate of cellulose (derivative) and lactose to be prepared with a high proportion of cellulose (derivative).


It was found that the flowability of the granulate according to the invention is considerably improved compared to the flowability of the physical mixture.


Another subject matter of the invention is a granulate which is obtainable by the process described above.


Furthermore, the present invention concerns a composition which comprises the granulate according to the invention, at least one pharmaceutically active component and optionally further excipients.


The weight ratio of granulate to pharmaceutically active component can vary within any ranges and is preferably between 99.9 and 5, more preferably between 99 and 30 (weight ratio quotient). In another embodiment the weight ratio of granulate to pharmaceutically active component is 99.9 to 0.1 and 20 to 80.


The weight ratio of granulate to excipients can vary in any ranges and is preferably for example between 100 and 0.5, preferably between 100 and 5 (weight ratio quotient). In another embodiment the weight ratio of granulate to excipients is 100 to 0 and 21 to 79.


Suitable excipients can for example be lubricants or glidants such as e.g. stearic acid, magnesium stearate or talcum, fillers such as e.g. lactose, cellulose powder, microcrystalline cellulose, additional cellulose (derivative) compounds, preferably hydroxypropyl cellulose or calcium diphosphate, flow regulation agents such as e.g. silicon dioxide (Aerosil®), antistatic agents such as e.g. aluminium oxide, PEG, solubilizers such as e.g. saponins and humectants such as e.g. glycerol or PEG.


The granulate according to the invention can be used as a tabletting excipient. In this case the granulate according to the invention can, on the one hand, be granulated together with the pharmaceutically active component and optionally further tabletting excipients, on the other hand, the granulate according to the invention can be mixed with a granulate containing the pharmaceutically active component before the formulation is compressed.


In particular the granulate according to the invention can be used as a direct tabletting excipient. For this purpose the pharmaceutically active component and optionally further tabletting excipients are simply mixed with the granulate according to the invention and directly compressed.


It has turned out that a granulate is obtained by the process according to the invention which can be used to increase the content of cellulose (derivatives) in the tablet formulation without significantly influencing the flowability of the tablet formulation.


This can be explained inter alia by the fact that the surface of the lactose particles or/and cellulose particles is modified by the process according to the invention as a result of which the tendency of the particles to agglomerate is greatly reduced and correspondingly the flow behaviour of the granulate or the tablet formulation is improved.


It has turned out that the use of the granulate according to the invention as a (direct) tabletting excipient in standard tablet formulations results in a significant improvement of the tablet hardness and friability resistance compared to tablets in which the components of the granulate according to the invention have been used as individual components in their production.


Thus, the tablet hardness at a comparable compression force is usually increased by at least 20%, preferably at least 50% in granulate-containing tablets compared to tablets in which the granulate components are present as a physical mixture.


The abrasion of the granulate-containing tablets is usually reduced by at least 20%, preferably by at least 50% at a comparable compression force compared to tablets in which the granulate components are present as a physical mixture.


The compression force-hardness profile as well as the compression force-friability resistance profile can be adjusted to the respective application by use of the granulate according to the invention as a tabletting excipient and in particular as a direct tabletting excipient.


Furthermore, it has turned out that the use of the granulate according to the invention as a (direct) tabletting excipient allows a control of the release profile of the pharmaceutically active component.


The proportion of cellulose (derivative) in the formulation is in particular responsible (see above) for a delayed release of the pharmaceutically active component. Due to the fact that the content of cellulose (derivative) can be adjusted over a wide range in the granulate and correspondingly in the tablet formulation, it is possible to adjust the release of a pharmaceutically active component without a poorly flowing tablet formulation making a direct tabletting process impossible. In particular the granulate according to the invention is suitable for use in sustained release formulations.





FIGURES


FIG. 1 shows the effect of compression force on tablet hardness in examples A and B.



FIG. 2 shows the effect of compression force on friability in examples A and B.



FIG. 3 shows the effect of compression force on tablet hardness in examples C and D.



FIG. 4 shows the effect of compression force on friability in examples C and D.



FIG. 5 shows the effect of compression force on tablet hardness in examples W1-W3.



FIG. 6 shows the release of theophylline from tablets W1-W3 as a function of time.



FIG. 7
a shows a scanning electron micrograph (SEM) of the physical mixture B0.



FIG. 7
b shows an SEM micrograph of the granulate B1.



FIG. 8 shows the particle size distribution of the granulate B1.



FIG. 9 shows the flow behaviour of the granulate B1 (Ericksen funnel model 321, 6 mm funnel opening).



FIG. 10 shows the release of Metformin HCl from the tablets M1-M3 as a function of time in 0.1M HCl.



FIG. 11 shows the release of Metformin HCl from the tablets M1-M3 as a function of time in acetate buffer (pH 4.5) USP.



FIG. 12 shows the release of Metformin HCl from the tablets M1-M3 as a function of time in 0.05 M phosphate buffer (pH 6.8) USP.





EXAMPLES
1. Measurement Methods

The stated particle sizes were determined according to the European Pharmacopeia using a vibrating sieve.


The Carr index is calculated by the formula C=100 [(VB−VT)/VB], where VB is the bulk volume and VT is the tamped volume and is a measure for the compressibility.


If not stated otherwise the flowability of the formulations, the friability resistance of the tablets, the tablet hardness, the bulk volume and the tamped density is determined on the basis of the European Pharmacopeia (Ph. Eur.).


The release is determined using apparatus II (Erweka, Germany DT 808 LH). The tests take place in 1000 ml 0.01 HCl, 0.05 M phosphate buffer (pH 6.8 [produced according to the United States Pharmacopeial Convention (USP)] or acetate buffer (pH 4.5) [USP] at a rotation speed of 50 rpm. The quantitative measurement of the released active substance is carried out by means of UV spectroscopy.


The particle size (distributions) are measured with a Sympatec Helios (H1511) in the measuring range R 5 0.5/4.5 . . . 875 μm using a Sympatec Rhodos dispersing system. The dispersion pressure is 0.5 bar. A vibration unit VIBRI (funnel height 2.5 mm, power 60%) is used for the feeding.


2. Preparation of the Granulate
Example A
Granulac 70: HPMC=50:50

62.5 g of a 40% aqueous lactose solution (25 g lactose; Granulac 70, Meggle, Wasserburg) are atomized in a fluid bed granulator from Huuttlin Mycrolab onto 50 g HPMC particles (Benecel K 4 M Pharm CR, Hercules) and 25 g lactose (Granulac 70, Meggle, Wasserburg). The granulation conditions are shown in Table 1. The reference sample in which the corresponding granulate components are present as a physical mixture is referred to as sample No. A0. The granulation conditions are summarized in Table 1.









TABLE 1







Granulation parameters














Inlet
Inlet
Ambient

Environ-




air
temper-
temper-
Nozzle
mental
Spray



flow
ature
ature
pressure
pressure
rate


Sample
[m3/h]
[° C.]
[° C.]
[bar]
[bar]
[g/min]
















A1
17
80
48-52
0.4
0.11
1.8


A2
17
70
42-46
0.4
0.11
2.2


B1
16
80
52-54
 0.41
0.2 
2.4


C1
17
80
52-54
0.4
0.1-0.2
2.8


C2
17
80
50-53
0.4-0.5
0.11-0.15
2.2


C3
15
68
41-43
0.4
0.11
3.6


C4
17
46
33-35
0.4
0.11
1.9


D1
13.5
80
52-55
 0.45
0.2 
2.2









Example B
Granulac 140: HPMC=50:50

62.5 g of a 40% aqueous lactose solution (25 g lactose; Granulac 140, Meggle, Wasserburg) is atomized in a fluid bed granulator from Hüttlin Mycrolab onto 50 g HPMC particles (Benecel K 4 M Pharm CR, Hercules) and 25 g lactose (Granulac 140, Meggle, Wasserburg). The granulation conditions are shown in Table 1. The reference sample in which the corresponding granulate components are present as a physical mixture is referred to as sample No. B0. The granulation conditions are summarized in Table 1.


Example C
Granulac 70: HPMC=40:60

62.5 g of a 40% aqueous lactose solution (25 g lactose; Granulac 70, Meggle, Wasserburg) is atomized in a fluid bed granulator from Hüttlin Mycrolab onto 60 g HPMC particles (Benecel K 4 M Pharm CR, Hercules) and 15 g lactose (Granulac 70, Meggle, Wasserburg). The granulation conditions are shown in Table 1. The reference sample in which the corresponding granulate components are present as a physical mixture is referred to as sample No. C0. The granulation conditions are summarized in Table 1.


Example D
Granulac 140: HPMC=40:60

62.5 g of a 40% aqueous lactose solution (25 g lactose; Granulac 140, Meggle, Wasserburg) is atomized in a fluid bed granulator from Hüttlin Mycrolab onto 60 g HPMC particles (Benecel K 4 M Pharm CR, Hercules) and 15 g lactose (Granulac 140, Meggle, Wasserburg). The granulation conditions are shown in Table 1. The reference sample in which the corresponding granulate components are present as a physical mixture is referred to as sample No. D0. The granulation conditions are summarized in Table 1.


The properties of the granulates obtained and of the starting materials are listed in Table 2.









TABLE 2







Powder and granulate properties












Particle size [μm]
Density [g/l]
Carr
Flowability [s/100 g]
























63-
100-
150-
180-
250-
355-
500-

bulk
tapped
index
d =
d =
d =


Sample
<63
100
150
180
250
355
500
630
>630
density
density
[%]
10 mm
15 mm
25 mm

























Benecel K 4 M
44.16
34
18.84
1.92
0.94
0.19
0.08
0.05
0.05
345
475
25.47





Pharm CR


Granulac 70
8.98
26.91
30.06
15.13
17.8
1.4
0.23
0.04
0.04
699
877
20.3


2.3


Granulac 140
11.24
26.64
32.94
22.51
6.33
0.47
0.27
0.08
0.05
613
862
28.89





A0
23.3
26.75
29.72
11.42
8.28
0.98
0.51
0.16
0.12
463
606
23.6

7.53
n/a


A1
12.14
26.65
35.12
15.06
10.46
1.14
0.17
0.12
0.2
467
575
18.78
21.47
6.83
n/a


A2
11.63
24.07
32.81
15.24
13.37
2.05
0.56
0.3
0.88
459
568
19.19
22.2 
6.93
n/a


B0
32.69
36.06
24.57
4.28
1.92
0.46
0.26
0.21
0.12
467
641
27.15





B1
23.44
27.83
24.04
7.79
6.77
2.91
1.44
0.92
5.58
478
578
17.3
n/a
n/a
n/a


C0
26.86
27.99
28.08
9.27
6.88
0.91
0.28
0.11
0.1
439
571
23.12

8.83
n/a


C1
10.5
21.23
32.18
15.7
17.17
3.7
0.38
0.04
0.1
397
469
15.35
n/a
n/a
n/a


C2
10.41
21.94
32.44
16.3
16.48
2.64
0.44
0.2
0.25
413
478
13.6
24.3 
7.53
n/a


C3
13.36
21.97
27.62
14.57
17.67
4.91
0.63
0.05
0.09
422
510
17.25
24.37
7.5 
n/a


C4
8.7
19.43
31.18
19.5
19.01
1.91
0.15
0.1
0.6
394
467
15.63
23.47
8.07
n/a


D0
36.69
34,86
22.68
4.11
1.82
0.46
0.11
0
0.1
435
602
27.74





D1
27.04
29.15
22.28
6.58
6.79
4.07
1.55
0.5
3.11
457
578
20.93
n/a
n/a
n/a





n/a not applicable






Example E
Granulac 200: HPMC=60:40

90 l water is heated in a mixing vessel to 80° C.+/−10° C. and subsequently 60 kg lactose (e.g. Granulac 200) is dissolved therein. 100 kg Benecel (K 4 M Pharm CR, Hercules) and 90 kg lactose (Granulac 200) are mixed for about 5 min in a granulator (e.g. Fielder Aeromatic) by blowing in air. Afterwards the lactose solution is sprayed on at an average of 90 l/h (pressure of the atomizing air 3 bar) at an air intake temperature of 120+/−10° C. After completion of the granulation step, the granulate is dried at an air intake temperature of 130+/−10° C. It is dried until the exhaust air temperature reaches at least 85° C.


3. Preparation of the Tablets

3.1. Tablets without an Active Substance


3.1.1. Formulation with Granulate


The granulates obtained (example A to E) are mixed in a Turbula mixer (Bachofen Co. WAB T2F) for 5 minutes. Subsequently magnesium stearate is added in a weight ratio of 99.5:0.5 and it is mixed for a further minute. The mixture obtained is then tabletted.


3.1.2. Formulation with a Physical Mixture


The components listed in Table 3 (except for magnesium stearate) are mixed together for 5 minutes in the respective weight ratio in a Turbula mixer (Bachofen Company WAB T2F). Subsequently magnesium stearate is added and it is mixed again for one minute. The formulation obtained is subsequently tabletted.









TABLE 3







Composition of the tablets without active substance


(physical mixture)










Formulation














Substance
A0
B0
C0
D0






Benecel K 4 M
49.75%
49.75%
59.75%
59.75%



Pharm CR







Granulac 70
49.75%

39.75%




Granulac 140

49.75%

39.75%



Magnesium stearate
 0.5%
 0.5%
 0.5%
 0.5%










3.2 Tablets Containing the Active Substance Theophylline


The components listed in Table 4 (except for magnesium stearate) are mixed for 5 minutes in the respective weight ratio in a Turbula mixer (Bachofen Company WAB T2F). Subsequently magnesium stearate is added and it is again mixed for one minute. The mixture obtained is subsequently tabletted.









TABLE 4







Tablet formulation containing the active substance theophylline












Substance
W1*
W2*
W3*






Theophylline
24.5%  
24.5% 
24.5%  



Benecel K 4 M
30%





Pharm CR






MCC






Granulate E

 75%
50%



Flowlac 90
45%

25%



Magnesium
0.5% 
0.5%
0.5% 



stearate





*direct compression






The flow properties of the formulations containing the active substance theophylline is summarized in Table 5.


Only the two formulations containing the granulate W2 and W3 according to the invention fulfil the requirement for directly compressible formulations with regard to flow properties.









TABLE 5







Flow properties of the formulations containing


the active substance theophylline










Outflow quantity sec/100 g




at a funnel opening of










Formulation
d = 10 mm
d = 15 mm





W1
—*
—*


W2
29
9


W3
24
8





—* formulation does not flow through the funnel







3.3 Tablets Containing the Active Substance Metformin HCl


The components listed in samples M1 and M3 (Table 6) (without magnesium stearate) are mixed for 5 minutes in the respective weight ratios in a Turbula mixer. Magnesium stearate is added and it is mixed again for one minute.


The mixture obtained is subsequently directly compressed at the compression pressure stated in table 6.


As a comparison the physical mixture consisting of HPMC (Benecel), Granulac 200 (standard material for wet granulation) and active substance is subjected to a wet granulation in sample M2 before the granulate obtained is mixed with magnesium stearate and compressed into tablets. The respective tablet hardnesses are stated in Table 6.











TABLE 6









Sample











M1
M2
M3













substance
%
mg
%
mg
%
mg
















Metformin HCl
50.0
500
50.0
500.0
50.0
500


HPMC compound
49.5
495


43.5
435


granulate B1


HPMC (Benecel)


24.75
247.5


Granulac 200


24.75
24.75


Klucel EXF




5.0
50


Aerosil




1.0
10


magnesium stearate
0.5
5
0.5
5
0.5
5


total
100
1000
100
1000
100
1000










preparation
direct pressing
wet granulation
direct pressing


compression force
27
29
28


(KN)


tablet hardness (N)
45
54
87









As shown in Table 6 the directly compressed tablets M1 have about the same tablet hardness as the tablets M2 of the physical mixture which had to be prepared via the intermediate step of wet granulation. A direct tabletting of the physical mixture M2 is not possible.


Furthermore, a considerable increase in the tablet hardness (and therefore the friability resistance) compared to M1 or M2 can be achieved by partial substitution of the granulate B1 by the additional excipient Klucel EXF (hydroxypropyl cellulose) and Aerosil. Formulation M3 can be directly pressed without problems.


3.4 Tabletting


The tabletting takes place on a Korsch EK 0, Germany (tablet punch: oblong 22×11 mm tablet weight 1000 mg).


3.5 Results


The tablet hardness of examples A to D is plotted in FIGS. 1 and 3 versus the compression force. All examples in which the granulate according to the invention was used as a direct tabletting excipient in the tabletting process have a greater tablet hardness compared to tablets which were prepared under the same conditions but using a physical mixture of the granulate components.


The friability resistance of tablets A to D is plotted in FIGS. 2 and 4 versus the compression force. All examples in which the granulate according to the invention was used as a direct tabletting excipient in the tabletting process exhibit less friability compared to tablets which were prepared under the same conditions but using a physical mixture of the granulate components.


The tablet hardness of examples W1 to W3 is plotted in FIG. 5 as a function of the compression force. The greatest hardness yield is obtained with granulate E in the active substance formulation. The hardness can be modified by adding spray-dried lactose (W3).


The release of theophylline from the tablets W1 to W3 with respect to time is shown in FIG. 6. For this the tablets were added to 0.05 molar phosphate buffer solution having a pH of 6.8. FIG. 6 shows that the granulate results in a delayed release of the active substance compared to the physical mixture. The release profile can be modified by adding further excipients such as e.g. spray-dried lactose (W3).



FIG. 7 shows REM micrographs of the physical mixture B0 (FIG. 7a) compared to the granulate B1 according to the invention (FIG. 7b). The images show that the finely divided starting materials of the physical mixture are formed into larger spheroid granulate particles by the process according to the invention.


The particle size distribution in granulate B1 is shown in FIG. 8. This yields a d50 value of about 200 μm.



FIG. 9 shows the flow property of granulate B1. The amount of granulate flowing from the funnel is plotted against time. The corresponding physical composition B0 cannot be measured because the formulation completely blocks the funnel.


The results of the release experiments of Metformin from the tablets M1 to M3 are shown graphically in FIGS. 10 to 12. The release experiments were each carried out in 0.1M HCl as well as in an acetate or phosphate buffer. As shown by the graphs, the tablets M1 to M3 exhibit a comparable release profile. Differences in the release profile between the direct compression (M1, M3) and the sample M2 prepared by the wet granulation process are not observed.

Claims
  • 1. A process for producing a granulate, comprising: (i) suspending and/or at least partially dissolving lactose and optionally at least one cellulose derivative in at least one liquid, to form a solution or suspension; and(ii) atomizing said solution or suspension in an environment above room temperature onto cellulose derivative particles and optionally lactose particles during which said atomized liquid is at least partially removed.
  • 2. The process according to claim 1, wherein said lactose is selected from the group consisting of lactose monohydrate and anhydrous lactose.
  • 3. The process according to claim 1, wherein the cellulose derivative is selected from the group consisting of cellulose whose hydroxyl groups are independently of one another at least partially alkylated, hydroxyalkylated, sulfonated, carboxyalkylated and/or xanthogenated.
  • 4. The process according to claim 1, wherein the cellulose derivative is selected from the group consisting of hypromellose (HPMC), hypromellose phthalate, hydroxypropyl cellulose (HPC), hydroxyethyl cellulose (HEC), ethyl cellulose (EC), carboxymethyl cellulose (CMC), carboxyethyl cellulose (CEC) and/or sodium and/or calcium salts thereof.
  • 5. The process according to claim 1, wherein said liquid is selected from the group consisting of water and organic solvents.
  • 6. The process according to claim 1, wherein said lactose and cellulose derivative in step (i) have a weight ratio of lactose/cellulose derivative of from about 100:0 to about 5:95.
  • 7. The process according to claim 1, wherein at least 5% by weight, based on total content of lactose, is present in a dissolved form in step (i).
  • 8. The process according to claim 1, wherein said suspension is characterized by an average particle size in a range of from 0.1 μm to about 1000 μm.
  • 9. The process according to claim 1, wherein said solution or suspension in step (ii) is atomized by a nozzle to form droplets having an average diameter of from 15 μm to 1250 μm.
  • 10. The process according to claim 1, wherein said solution or suspension is atomized in an environment at temperature of from about 30° C. to 250° C.
  • 11. The process according to claim 10, wherein said environment has a pressure of from about 0 bar to 1.0 bar.
  • 12. The process according to claim 1, wherein said solution or suspension is sprayed onto cellulose derivative particles and/or lactose particles having average diameter of from about 1 μm to about 500 μm.
  • 13. The process according to claim 1, wherein said cellulose derivative particles and lactose particles in step (ii) have a ratio of cellulose derivative particles/lactose particles in a range of from about 100:0 to about 5:95.
  • 14. The process according to claim 1, wherein said liquid of said solution or suspension is at least partially removed by a spray drying process.
  • 15. The process according to claim 1, wherein all of said cellulose derivative particles and optional lactose particles are present in a fluidized bed or a stationary fluidized bed.
  • 16. The process according to claim 1, wherein said liquid of said solution or suspension is at least partially removed in a fluidized bed granulation process.
  • 17. The process according to claim 1, wherein said liquid of said solution or suspension is at least partially removed in a wet granulation process.
  • 18. The process according to claim 1, wherein free liquid content in said granulate is less than 8% by weight, based on total mass of the granulate.
  • 19. The process according to claim 1, wherein said granulate has a ratio of lactose/cellulose derivative of from about 95:5 and 1:99.
  • 20. The process according to claim 1, wherein said granulate has a spherical or spheroid morphology.
  • 21. The process according to claim 1, wherein said granulate comprises granulate particles having a d50 particle size distribution of from 25 μm to 750 μm.
Priority Claims (1)
Number Date Country Kind
10 2008 047 910 Sep 2008 DE national
PCT Information
Filing Document Filing Date Country Kind 371c Date
PCT/EP2009/062203 9/21/2009 WO 00 5/9/2011
Publishing Document Publishing Date Country Kind
WO2010/031866 3/25/2010 WO A
US Referenced Citations (14)
Number Name Date Kind
4693750 Bauer et al. Sep 1987 A
5006345 Lang Apr 1991 A
6667059 Sue et al. Dec 2003 B2
6716453 Harden et al. Apr 2004 B1
20030206978 Sherwood et al. Nov 2003 A1
20030211148 Chen et al. Nov 2003 A1
20040019122 Takano et al. Jan 2004 A1
20040057993 Jain et al. Mar 2004 A1
20040097484 Cantillion et al. May 2004 A1
20060127479 Kumaraperumal et al. Jun 2006 A1
20060159747 Schumacher et al. Jul 2006 A1
20070014853 Zalit et al. Jan 2007 A1
20070053978 Sherwood et al. Mar 2007 A1
20070202172 Gold et al. Aug 2007 A1
Foreign Referenced Citations (78)
Number Date Country
3045488 Jul 1982 DE
249186 Sep 1987 DE
4428986 Feb 1996 DE
19651734 May 1999 DE
19749897 Aug 1999 DE
101 52 351 Sep 2005 DE
0610848 Aug 1994 EP
0948321 Oct 1999 EP
1136254 Sep 2001 EP
0996449 Feb 2002 EP
1028730 Apr 2002 EP
0877605 Oct 2002 EP
1075263 Mar 2003 EP
1295595 Mar 2003 EP
1083901 Apr 2003 EP
0879049 May 2003 EP
1332757 Aug 2003 EP
1194124 Sep 2003 EP
0948321 Oct 2003 EP
1300394 Feb 2004 EP
1647275 Apr 2006 EP
1282399 Jul 2006 EP
1389212 Jul 2006 EP
1575604 Dec 2006 EP
1438024 Jun 2007 EP
1581237 Jun 2007 EP
1622612 Mar 2008 EP
9726865 Jul 1997 WO
WO9825590 Jun 1998 WO
0018375 Apr 2000 WO
0018406 Apr 2000 WO
0030616 Jun 2000 WO
0108686 Feb 2001 WO
0182897 Nov 2001 WO
0189485 Nov 2001 WO
0191999 Dec 2001 WO
0247607 Jun 2002 WO
02065991 Aug 2002 WO
02069888 Sep 2002 WO
02100407 Dec 2002 WO
03020241 Mar 2003 WO
03035037 May 2003 WO
03039515 May 2003 WO
03047551 Jun 2003 WO
03048666 Jun 2003 WO
03057133 Jul 2003 WO
03070224 Aug 2003 WO
03082204 Oct 2003 WO
03086343 Oct 2003 WO
03097058 Nov 2003 WO
2004016252 Feb 2004 WO
2004017976 Mar 2004 WO
2004060353 Jul 2004 WO
2004066982 Aug 2004 WO
2004082664 Sep 2004 WO
2004089343 Oct 2004 WO
2004096214 Nov 2004 WO
2005007105 Jan 2005 WO
2005009407 Feb 2005 WO
2005032553 Apr 2005 WO
2005041941 May 2005 WO
2005051489 Jun 2005 WO
2005065661 Jul 2005 WO
2005065662 Jul 2005 WO
2005070467 Aug 2005 WO
2005082330 Sep 2005 WO
2005082331 Sep 2005 WO
2005123041 Dec 2005 WO
2005123043 Dec 2005 WO
2006082499 Aug 2006 WO
2006089674 Aug 2006 WO
2006092255 Sep 2006 WO
2006101536 Sep 2006 WO
2006113631 Oct 2006 WO
2007047047 Apr 2007 WO
2007065441 Jun 2007 WO
2007096906 Aug 2007 WO
2007138301 Dec 2007 WO
Non-Patent Literature Citations (3)
Entry
Remon, J.P., et al., “Effect of Raw Materials and Processing on the Quality of Granules Prepared From Microcrystalline Cellulose-Lactose . . . ”, “Drug Development and Industrial Pharmacy”, 1987, pp. 1-14, vol. 13, No. 1.
Takeuchi, H., et al., “Temperature-Induced Crystallization and Compactibility of Spray Dried Composite Particles Composed of Amorphous . . . ”, “Chem. Pharm. Bull”, 2000, pp. 585-588, vol. 48, No. 4.
Tewari, D., et al., “The Role of Polymer Hydrophilicity, Molecular Weight and Drug Solubility in Modified Release Matrix Systems”, Presented at the Annual Meeting of the American Association of Pharmaceutical Scientists in Nashville, Tennessee, Nov. 6-10, 2005, pp. 1-10.
Related Publications (1)
Number Date Country
20110207826 A1 Aug 2011 US