Link: Pharm/Biotech Resources
Title: Process for preparing powder formulations
United States Patent: RE38,912
Issued: December 6, 2005
Inventors: Walz; Michael (Bingen, DE); Boeck; Georg (Mainz, DE)
Assignee: Boehringer Ingelheim Pharma KG (Ingelheim, DE)
Appl. No.: 766748
Filed: January 28, 2004
Abstract
The invention relates to a new process for producing powdered preparations for inhalation.
DETAILED DESCRIPTION OF THE INVENTION
It was found that, surprisingly, the problem outlined above can be solved
by means of a process in which the substance with the smaller particle size
distribution can be added to the substance with the coarser particle size
distribution by a layered mixing process.
The process according to the invention for preparing inhalable powders is
characterised in that N+m substantially equal portions of the substance
having a larger particle size distribution and N equal portions of the
substance having a smaller particle size distribution are placed in
alternate layers in a suitable mixing vessel and after they have all been
added the 2N+m layers of the two components are mixed together using a
suitable mixer, a portion of the substance having the larger particle size
being put in first, while N is an integer >0, preferably >5, and m denotes 0
or 1.
Preferably, the individual fractions are added in layers through a suitable
screening apparatus. If desired, once the mixing process is finished, the
entire powder mixture can be subjected to one or more additional screening
processes. In the process according to the invention, N is naturally
dependent inter alia on the total quantity of powder mixture to be produced.
When producing smaller batches, the desired effect of high homogeneity in
the sense of uniformity of content can be achieved with a smaller N. In
principle, it is preferable according to the invention if N is at least 10
or more, more preferably 20 or more, better still 30 or more. The greater N
is and, as a result, the greater the total number of layers of the powder
fractions formed, the more homogeneous the powder mixture becomes in the
sense of uniformity of content.
The number m may represent 0 or 1 within the scope of the process according
to the invention. If m denotes 0 the last fraction added to the mixing
apparatus, preferably screened into it, in a layer is the last portion of
the substance with a smaller particle size distribution. If m represents the
number 1, the last fraction added to the mixing apparatus, preferably
screened into it, in a layer is the last portion of the substance with a
larger particle size distribution. This may prove advantageous inasmuch as,
when m=1, any residues of the last fraction of the substance with the finer
particle size distribution still remaining in the screening unit can be
carried into the mixing unit by means of the last portion of excipient.
Within the scope of the present invention, unless otherwise defined, the
substance with the smaller particle size distribution, which is very finely
ground and is present in the resulting powder formulation in a very small
proportion by mass, represents the active substance. Within the scope of the
present invention, unless otherwise defined, the substance with the larger
particle size distribution, which is coarsely ground and is present in the
resulting powder formulation in a large proportion by mass, represents the
excipient.
The present invention relates in particular to a process for preparing
inhalable powders containing less than 5%, preferably less than 2%, most
preferably less than 1% of active substance mixed with a physiologically
acceptable excipient. A preferred process according to the invention is a
process for preparing inhalable powders containing 0.04 to 0.8%, most
preferably 0.08 to 0.64%, better still 0.16 to 0.4% of active substance
mixed with a physiologically acceptable excipient.
The active substance used according to the invention preferably has an
average particle size of 0.5 to 10 μm, preferably 1 to 6 μm, most preferably
2 to 5 μm. The excipient which may be used in the process according to the
invention preferably has an average particle size of 10 to 100 μm,
preferably 15 to 80 μm, most preferably 17 to 50 μm. Particularly preferred
according to the invention are processes for preparing inhalable powders
wherein the excipient has an average particle size of 20-30 μm.
The two components are preferably added through a screening granulator with
a mesh size of 0.1 to 2 mm, most preferably 0.3 to 1 mm, even more
preferably 0.3 to 0.6 mm.
Preferably, the first portion of the N+m portions of the excipient is put in
first, and then the first portion of the N portions of the active substance
is placed in the mixing container. Whereas within the scope of the process
according to the invention the individual components are normally added in
roughly equal portions, it may be advantageous in some cases if the first of
the N+m portions of excipient which is put into the mixing apparatus has a
larger volume than the subsequent portions of excipient. Preferably, the two
components are added alternately through a screening unit and in more than
20, preferably more than 25, most preferably more than 30 layers. For
example, with a desired total amount of powder of 30-35 kg containing
0.3-0.5% of active substance, for example, and using common excipients, the
two components can be screened in in about 30 to 60 layers each (N=30-60).
The upper limit of 60 layers mentioned above is given purely from the point
of view of economy of the process. It should not be regarded in any way as
restricting the number of possible layers according to the invention. As
will be clearly apparent to anyone skilled in the art, the process can
equally well be carried out with N>60 to achieve the desired effect of the
maximum possible homogeneity of the powder mixture.
In some cases the excipient may also consist of a mixture of coarser
excipient with an average particle size of 15 to 80 μm and finer excipient
with an average particle size of 1 to 9 μm, wherein the proportion of finer
excipient in the total quantity of excipient may be 1 to 20%. If the
inhalable powders which may be produced using the process according to the
invention contain a mixture of coarser and finer excipient fractions, it is
preferable according to the invention to prepare inhalable powders wherein
the coarser excipient has an average particle size of 17 to 50 μm, most
preferably 20 to 30 μm, and the finer excipient has an average particle size
of 2 to 8 μm, most preferably 3 to 7 μm. By average particle size is meant
here the 50% value of the volume distribution measured with a laser
diffractometer using the dry dispersion method. In the case of an excipient
mixture of coarser and finer excipient fractions, the preferred processes
according to the invention are those that produce inhalable powders in which
the proportion of finer excipient constitutes 3 to 15%, most preferably 5 to
10% of the total amount of excipient.
The percentages given within the scope of the present invention are always
percent by weight.
If the excipient used is one of the abovementioned mixtures of coarser
excipient and finer excipient, it is again expedient according to the
invention to produce the excipient mixture using the process according to
the invention from N roughly equal portions of the finer excipient fraction
with N+m roughly equal portions of the coarser excipient fraction. In such a
case it is advisable first to generate the abovementioned excipient mixture
from the abovementioned excipient fractions, and then to produce from it the
total mixture including the active substance using the process according to
the invention.
For example, the excipient mixture may be obtained as follows, using the
process according to the invention. The two components are preferably added
through a screening granulator with a mesh size of 0.1 to 2 mm, most
preferably 0.3 to 1 mm, even more preferably 0.3 to 0.6 mm. Preferably the
first fraction of the N+m portions of the coarser excipient is put in first
and then the first portion of the N portions of the finer excipient fraction
is added to the mixing container. The two components are added alternately
by screening them in in layers.
After the preparation of the excipient mixture, the inhalable powder is
produced from the mixture and the desired active substance using the process
according to the invention. The two components are preferably added through
a screening granulator with a mesh size of 0.1 to 2 mm, most preferably 0.3
to 1 mm, even more preferably 0.3 to 0.6 mm.
Preferably, the first portion of the N+m portions of the excipient mixture
is put in and then the first portion of the N portions of the active
substance is added to the mixing container. The two components are
preferably added through a screening unit in alternate layers, in more than
20, preferably more than 25, most preferably more than 30 layers. For
example, with a desired total amount of powder of 30-35 kg containing
0.3-0.5% of active substance, for example, and using common excipients, the
two components can be screened in in about 30 to 60 layers each (N=30-60).
As will be clearly apparent to anyone skilled in the art, the process can
equally well be carried out with N>60 to achieve the desired effect of the
maximum possible homogeneity of the powder mixture. The inhalable powders
which may be obtained using the method of preparation according to the
invention may contain, in general, any active substances which may
reasonably be administered by inhalation for therapeutic purposes.
Preferably, the active substances used are selected, for example, from among
the betamimetics, anticholinergics, corticosteroids and dopamine agonists.
Example of betamimetics which may be used are preferably compounds selected
from among bambuterol, bitolterol, carbuterol, clenbuterol, fenoterol,
formoterol, hexoprenaline, ibuterol, pirbuterol, procaterol, reproterol,
salmeterol, sulphonterol, terbutaline, tulobuterol, mabuterol,
4-hydroxy-7-[2-{[2-{[3-(2-
phenylethoxy)propyl]sulphonyl}ethyl]-amino}ethyl]-2(3H)-benzothiazolone,
1-(2-
fluoro-4-hydroxyphenyl)-2-[4-(1-benzimidazolyl)-2-methyl-2-butylamino]ethanol,
1-
[3-(4-methoxybenzylamino)-4-hydroxyphenyl]-2-[4-(1-benzimidazolyl)-2-methyl-2-
butylamino]ethanol,
1-[2H-5-hydroxy-3-oxo-4H-1,4-benzoxazin-8-yl]-2-[3-(4-N,N-
dimethylaminophenyl)-2-methyl-2-propylamino]ethanol,
1-[2H-5-hydroxy-3-oxo-4H-
1,4-benzoxazin-8-yl]-2-[3-(4-methoxyphenyl)-2-methyl-2-propylamino]ethanol,
1-
[2H-5-hydroxy-3-oxo-4H-1,4-benzoxazin-8-yl]-2-[3-(4-n-butyloxyphenyl)-2-methyl-
2-propylamino]ethanol,
1-[2H-5-hydroxy-3-oxo-4H-1,4-benzoxazin-8-yl]-2-{4-[3-
(4-methoxyphenyl)-1,2,4-triazol-3-yl]-2-methyl-2-butylamino}ethanol,
5-hydroxy-8-
(1-hydroxy-2-isopropylaminobutyl)-2H-1,4-benzoxazin-3-(4H)-on, 1-(4-amino-3-
chloro-5-trifluoromethylphenyl)-2-tert.butylamino)ethanol and 1-(4-
ethoxycarbonylamino-3-cyano-5-fluorophenyl)-2-(tert.butylamino)ethanol,
optionally in the form of their racemates, their enantiomers, their
diastereomers, as well as optionally their pharmacologically acceptable acid
addition salts and hydrates. It is particularly preferable to use, as
betamimetics, active substances of this kind selected from among fenoterol,
formoterol, salmeterol, mabuterol, 1-[3-(4-methoxybenzylamino)-4-
hydroxyphenyl]-2-[4-(1-benzimidazolyl)-2-methyl-2-butylamino]-ethanol,
1-[2H-5-
hydroxy-3-oxo-4H-1,4-benzoxazin-8-yl]-2-[3-(4-N,N-dimethylaminophenyl)-2-
methyl-2-propylamino]ethanol,
1-[2H-5-hydroxy-3-oxo-4H-1,4-benzoxazin-8-yl]-2-
[3-(4-methoxyphenyl)-2-methyl-2-propylamino]ethanol,
1-[2H-5-hydroxy-3-oxo-4H-
1,4-benzoxazin-8-yl]-2-[3-(4-n-butyloxyphenyl)-2-methyl-2-propylamino]ethanol,
1-
[2H-5-hydroxy-3-oxo-4II-1,4-benzoxazin-8-yl]-2-{4-[3-(4-methoxyphenyl)-1,2,4-
triazol-3-yl]-2-methyl-2-butylamino}ethanol, optionally in the form of their
racemates, their enantiomers, their diastereomers, as well as optionally
their pharmacologically acceptable acid addition salts and hydrates. Of the
betamimetics mentioned above, the compounds formoterol and salmeterol,
optionally in the form of their racemates, their enantiomers, their
diastereomers, as well as optionally their pharmacologically acceptable acid
addition salts and hydrates, are particularly important.
The acid addition salts of the betamimetics selected from among the
hydrochloride, hydrobromide, sulphate, phosphate, fumarate,
methanesulphonate and xinafoate are preferred according to the invention. In
the case of salmeterol, the salts selected from among the hydrochloride,
sulphate and xinafoate are particularly preferred, especially the sulphates
and xinafoates. Of outstanding importance according to the invention are
salmeterol×˝II2SO4 and salmeterol xinafoate. In the
case of formoterol, the salts selected from among the hydrochloride,
sulphate and fumarate are particularly preferred, especially the
hydrochloride and fumarate. Of outstanding importance according to the
invention is formoterol fumarate.
Anticholinergics which may be used in the processes according to the
invention are preferably salts selected from among tiotropium salts,
oxitropium salts and ipratropium salts, of which tiotropium and ipratropium
salts are particularly preferred. In the abovementioned salts the cations
tiotropium, oxitropium and ipratropium are the pharmacologically active
ingredients. By the salts which may be used within the scope of the present
invention are meant the compounds which contain, in addition to tiotropium,
oxitropium or ipratropium as counter-ion (anion) chloride, bromide, iodide,
sulphate, methanesulphonate or para-toluenesulphonate. Within the scope of
the present invention, of all the salts of the abovementioned
anticholinergics, the methanesulphonate, chloride, bromide and iodide are
preferred, the methanesulphonate or bromide being especially preferred. Of
outstanding importance according to the invention are the anticholinergics
selected from among tiotropium bromide, oxitropium bromide and ipratropium
bromide. Tiotropium bromide is particularly preferred. The abovementioned
anticholinergics may optionally occur in the form of their solvates or
hydrates. In the case of tiotropium bromide, for example, tiotropium bromide
monohydrate is particularly important according to the invention.
Within the scope of the present invention, the term corticosteroids denotes
compounds selected from among flunisolide, beclomethasone, triamcinolone,
budesonide, fluticasone, mometasone, ciclesonide, rofleponide, GW 215864,
KSR 592, ST-126 and dexamethasone. The preferred corticosteroids within the
scope of the present invention are those selected from among flunisolide,
beclomethasone, triamcinolone, budesonide, fluticasone, mometasone,
ciclesonide and dexamethasone, while budesonide, fluticasone, mometasone and
ciclesonide, especially budesonide and fluticasone, are of particular
importance. The term steroids may be used on its own, within the scope of
the present patent application, instead of the term corticosteroids. Any
reference to steroids within the scope of the present invention also
includes a reference to salts or derivatives which may be formed from the
steroids. Examples of possible salts or derivatives include: sodium salts,
sulphobenzoates, phosphates, isonicotinates, acetates, propionates,
dihydrogen phosphates, palmitates, pivalates or furoates. The
corticosteroids may optionally also be in the form of their hydrates.
Within the scope of the present invention, the term dopamine agonists
denotes compounds selected from among bromocriptine, cabergolin, alpha-dihydroergocryptine,
lisuride, pergolide, pramipexol, roxindol, ropinirol, talipexol, tergurid
and viozan. It is preferable within the scope of the present invention to
use dopamine agonists selected from among pramipexol, talipexol and viozan,
pramipexol being of particular importance. Any reference to the
abovementioned dopamine agonists also includes, within the scope of the
present invention, a reference to any pharmacologically acceptable acid
addition salts and hydrates thereof which may exist. By the physiologically
acceptable acid addition salts thereof which may be formed by the
abovementioned dopamine agonists are meant, for example, pharmaceutically
acceptable salts selected from among the salts of hydrochloric acid,
hydrobromic acid, sulphuric acid, phosphoric acid, methanesulphonic acid,
acetic acid, fumaric acid, succinic acid, lactic acid, citric acid, tartaric
acid and maleic acid.
The process according to the invention for preparing powder mixtures for
inhalation may be used to prepare powders which contain one or more of the
abovementioned active ingredients. If, for example, inhalable powders are to
be prepared in which the pharmaceutically active ingredients consist of two
different active substances, this can be achieved using the process
according to the invention, for example, by screening N+m roughly equal
portions of excipient or excipient mixture with O roughly equal portions of
one active substance component and P roughly equal portions of the other
active substance component into the mixing apparatus in alternate layers.
The number of fractions P and O may be selected, for example, so that P+O=N.
If the process according to the invention is to be used to prepare inhalable
powders which contain two active ingredients, for example, preferred
possible combinations of active substances might consist of a combination of
one of the abovementioned anticholinergics with one of the abovementioned
corticosteroids or a combination of one of the abovementioned
anticholinergics with one of the abovementioned betamimetics.
Examples of physiologically acceptable excipients which may be used to
prepare the inhalable powders according to the invention include, for
example, monosaccharides (e.g. glucose or arabinose), disaccharides (e.g.
lactose, saccharose, maltose), oligo- and polysaccharides (e.g. dextrane),
polyalcohols (e.g. sorbitol, mannitol, xylitol), salts (e.g. sodium
chloride, calcium carbonate) or mixtures of these excipients with one
another. Preferably, mono- or disaccharides are used, while the use of
lactose or glucose is preferred, particularly, but not exclusively, in the
form of their hydrates. For the purposes of the invention, lactose is the
particularly preferred excipient, while lactose monohydrate is most
particularly preferred.
The inhalable powders which may be obtained by the preparation process
according to the invention are characterised by an exceptional degree of
homogeneity in terms of uniformity of content. This is in a range of <8%,
preferably <6%, most preferably <4%. The inhalable powders which may be
prepared according to the invention may possibly even have levels of
homogeneity, in the sense of single dose accuracy, of <3%, possibly <2%.
Thus, in a further aspect, the present invention relates to inhalable
powders as such which may be obtained by the preparation process according
to the invention.
The inhalable powders which may be obtained by the process according to the
invention may for example be administered using inhalers which meter a
single dose from a reservoir by means of a measuring chamber (e.g. according
to U.S. Pat. No. 4,570,630A) or by other means (e.g. according to DE 36 25
685 A). Preferably, however, the inhalable powders which may be obtained
according to the invention are packed into capsules (to make so-called
inhalettes), which are used in inhalers such as those described in WO
94/28958, for example. If the inhalable powder obtained by the process
according to the invention is to be packed into capsules (inhalettes) in
accordance with the preferred application mentioned above, it is advisable
to fill the capsules with amounts of from 3 to 10 mg, preferably from 4 to 6
mg of inhalable powder per capsule, this amount depending to a large extent
on the choice of active substance used. In the case of the active substance
tiotropium bromide, the capsules contain between 1.2 and 80 μg of tiotropium
cation, for the amounts of filling mentioned above. With a filling of 4 to 6
mg of inhalable powder per capsule, the preferred amount for tiotropium
bromide, the content of tiotropium per capsule is between 1.6 and 48 μg,
preferably between 3.2 and 38.4 μg, most preferably between 6.4 and 24 μg. A
content of 18 μg of tiotropium, for example, corresponds to a content of
about 21.7 μg of tiotropium bromide.
Consequently, capsules containing 3 to 10 mg of powder for inhalation
preferably hold between 1.4 and 96.3 μg of tiotropium bromide, according to
the invention. When the filling is from 4 to 6 mg of inhalable powder per
capsule, as is preferred, each capsule contains between 1.9 and 57.8 μg,
preferably between 3.9 and 46.2 μg, most preferably between 7.7 and 28.9 μg
of tiotropium bromide. A content of 21.7 μg of tiotropium bromide, for
example, corresponds to a content of about 22.5 μg of tiotropium bromide
monohydrate.
Consequently, capsules containing 3 to 10 mg of powder for inhalation
preferably hold between 1.5 and 100 μg of tiotropium bromide monohydrate.
When the filling is from 4 to 6 mg of inhalable powder per capsule, as is
preferred, each capsule contains between 2 and 60 μg, preferably between 4
and 48 μg, most preferably between 8 and 30 μg of tiotropium bromide
monohydrate.
The Examples which follow describe a possible method of carrying out the
process according to the invention, taking a powder mixture containing
tiotropium bromide monohydrate as the example. The fact that this process
described by way of example can be used directly for preparing inhalable
powders which contain one or more of the other active substances mentioned
above will be apparent to anyone skilled in the art. Accordingly, the
following Examples serve only to illustrate the present invention further
without restricting its scope to the embodiments provided hereinafter by way
of example.
Starting Materials
In the Examples which follow, lactose-monohydrate (200M) is used as the
coarser excipient. It may be obtained, for example, from Messrs DMV
International, 5460 Veghel/NL under the product name Phannatose 200M.
In the Examples which follow, lactose-monohydrate (5μ) is used as the finer
excipient. It may be obtained from lactose-monohydrate 200M by conventional
methods (micronising). Lactose-monohydrate 200M may be obtained, for
example, from Messrs DMV International, 5460 Veghel/NL under the product
name Pharmatose 200M.
Preparation of Tiotropium Bromide Monohydrate:
15.0 kg of tiotropium bromide, which may be prepared as disclosed in EP 418
716 A1, are added to 25.7 kg of water in a suitable reaction vessel. The
mixture is heated to 80-90° C. and stirred at constant temperature until a
clear solution is formed. Activated charcoal (0.8 kg), moistened with water,
is suspended in 4.4 kg of water, this mixture is added to the solution
containing the tiotropium bromide and rinsed with 4.3 kg of water. The
mixture thus obtained is stirred for at least 15 min at 80-90° C. and then
filtered through a heated filter into an apparatus which has been preheated
to an outer temperature of 70° C. The filter is rinsed with 8.6 kg of water.
The contents of the apparatus are cooled at 3-5° C. every 20 minutes to a
temperature of 20-25° C. The apparatus is further cooled to 10-15° C. using
cold water and crystallisation is completed by stirring for at least one
hour. The crystals are isolated using a suction drier, the crystal slurry
isolated is washed with 9 liters of cold water (10-15° C.) and cold acetone
(10-15° C.). The crystals obtained are dried in a nitrogen current at 25° C.
over 2 hours. Yield: 13.4 kg of tiotropium bromide monohydrate (86% of
theory)
The crystalline tiotropium bromide monohydrate thus obtained is micronised
by known methods, to bring the active substance into the average particle
size which meets the specifications according to the invention.
For the purposes of the present invention, the average particle size is the
value in μm at which 50% of the particles from the volume distribution have
a particle size which is smaller than or equal to the value specified. The
laser diffraction/dry dispersal method of measurement is used to determine
the total distribution of the particle size distribution.
The method of determining the average particle size of the various
ingredients of the formulation according to the invention is described as
follows.
The equipment is operated according to the manufacturer's instructions.
| Measuring equipment: | HELOS Laser-diffraction spectrometer |
| (SympaTec) | |
| Dispersing unit: | RODOS dry disperser with suction |
| funnel, (SympaTec) | |
| Sample quantity: | from 100 mg |
| Product feed: | Vibri Vibrating channel, Messrs. |
| Sympatec | |
| Frequency of vibrating channel: | 40 rising to 100% |
| Duration of sample feed: | 1 to 15 sec. (in the case of 100 mg) |
| Focal length: | 100 mm (measuring range: 0.9-175 μm) |
| Measuring time: | about 15 s (in the case of 100 mg) |
| Cycle time: | 20 ms |
| Start/stop at: | 1% on channel 28 |
| Dispersing gas: | compressed air |
| Pressure: | 3 bar |
| Vacuum: | maximum |
| Evaluation method: | HRLD |
Sample Preparation/Product Feed:
At least 100 mg of the test substance are weighed onto a piece of card.
Using another piece of card all the larger lumps are broken up. The powder
is then sprinkled finely over the front half of the vibrating channel
(starting about 1 cm from the front edge). After the start of the
measurement the frequency of the vibrating channel is varied from about 40%
up to 100% (towards the end of the measurement). The time taken to feed in
the entire sample is 10 to 15 sec.
Determining the Particle Size of Micronised Tiotropium Bromide Monohydrate:
Measuring Equipment and Settings:
The equipment is operated according to the manufacturer's instructions.
| Measuring equipment: | Laser diffraction spectrometer |
| (HELOS), Sympatec | |
| Dispersing unit: | RODOS dry disperser with suction |
| funnel, Sympatec | |
| Sample quantity: | 50 mg-400 mg |
| Product feed: | Vibri Vibrating channel, Messrs. |
| Sympatec | |
| Frequency of vibrating channel: | 40 rising to 100% |
| Duration of sample feed: | 15 to 25 sec. (in the case of 200 mg) |
| Focal length: | 100 mm (measuring range: 0.9-175 μm) |
| Measuring time: | about 15 s (in the case of 200 mg) |
| Cycle time: | 20 ms |
| Start/stop at: | 1% on channel 28 |
| Dispersing gas: | compressed air |
| Pressure: | 3 bar |
| Vacuum: | maximum |
| Evaluation method: | HRLD |
Sample Preparation/Product Feed:
About 200 mg of the test substance are weighed onto a piece of card. Using
another piece of card all the larger lumps are broken up. The powder is then
sprinkled finely over the front half of the vibrating channel (starting
about 1 cm from the front edge). After the start of the measurement the
frequency of the vibrating channel is varied from about 40% up to 100%
(towards the end of the measurement). The sample should be fed in as
continuously as possible. However, the amount of product should not be so
great that adequate dispersion cannot be achieved. The time over which the
entire sample is fed in is about 15 to 25 seconds for 200 mg, for example.
Measuring Equipment and Settings:
The equipment is operated according to the manufacturer's instructions.
| Measuring equipment: | Laser diffraction spectrometer |
| (HELOS), Sympatec | |
| Dispersing unit: | RODOS dry disperser with suction |
| funnel, Sympatec | |
| Sample quantity: | 500 mg |
| Product feed: | Vibri Vibrating channel, Messrs. |
| Sympatec | |
| Frequency of vibrating channel: | 18 rising to 100% |
| Focal length (1): | 200 mm (measuring range: 1.8-350 μm) |
| Focal length (2): | 500 mm (measuring range: 4.5-875 μm) |
| Measuring time: | 10 s |
| Cycle time: | 10 ms |
| Start/stop at: | 1% on channel 19 |
| Pressure: | 3 bar |
| Vacuum: | maximum |
| Evaluation method: | HRLD |
Sample Preparation/Product Feed:
About 500 mg of the test substance are weighed onto a piece of card. Using
another piece of card all the larger lumps are broken up. The powder is then
transferred into the funnel of the vibrating channel. A gap of 1.2 to 1.4 mm
is set between the vibrating channel and funnel. After the start of the
measurement the amplitude setting of the vibrating channel is increased from
0 to 40% until a continuous flow of product is obtained. Then it is reduced
to an amplitude of about 18%. Towards the end of the measurement the
amplitude is increased to 100%.
Apparatus
The following machines and equipment, for example, may be used to prepare
the inhalable powders according to the invention:
| Mixing container or | Gysowbeel mixer 200 L; type: DFW80N-4; |
| powder mixer: | made by: Messrs Engelsmann, D-67059 |
| Ludwigsbafen. | |
| Granulating sieve: | Quadro Cosnil; type: 197-S; made by: |
| Messrs Joisten & Kettenbaum, | |
| D-51429 Bergisch-Gimdbach. | |
Claim 1 of 15 Claims
1. A process for preparing an inhalable powder, wherein N+m substantially
equal portions of an excipient having a larger are added in alternate
layers into a suitable mixing vessel and after all the excipient and
active substance have been added the 2N+m layers of the two components are
mixed together using a suitable mixer, wherein a portion of the excipient
having the larger particle size is added first, and wherein N is an
integer >5 and m denotes 0 or 1.
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