Title of Invention	"A DRY POWDER COMPOSITION"
Abstract	A dry powder composition comprising particles of budesonide and formoterol and particles of a carrier substance, all of which particles: (a) have a mass median diameter of less than 10 µm, (b) are substantially uniformly distributed, and (c) are in the form of a spheronized agglomerate having size in the range of from 100 to 2000 µm, wherein the particles have been substantially uniformly distributed by mixing prior to agglomeration and the composition has a poured bulk density of from 0.30 to 0.36 g/ml.

Title of Invention

"A DRY POWDER COMPOSITION"

Abstract

A dry powder composition comprising particles of budesonide and formoterol and particles of a carrier substance, all of which particles: (a) have a mass median diameter of less than 10 µm, (b) are substantially uniformly distributed, and (c) are in the form of a spheronized agglomerate having size in the range of from 100 to 2000 µm, wherein the particles have been substantially uniformly distributed by mixing prior to agglomeration and the composition has a poured bulk density of from 0.30 to 0.36 g/ml.

Full Text	The present application relates to a dry powder composition. Background to the Invention Potent drugs for administration by inhalation are generally formulated in association with carriers such as lactose because of the problem of preparing accurate doses. When such drugs are diluted, variations in the weight of the formulation result in a smaller drug dosage variation rate compared with when they are not diluted. These formulations have generally consisted of coarse particles of the carrier with fine particles of the drug, which combination is generally known as an ordered mixture. The invention provides an improved formulation which, in systems designed to imitate inhalation has been found to give an improved dispersion of the drug. Description of the Invention According to the invention there is provided a dry powder composition comprising one or more potent pharmaceutically active substances and a carrier substance, all of which are in finely divided form, wherein the formulation has a poured bulk density of from 0.28 to 0.38 g/ml, preferably from 0.30 to 0.36 g/ml. The poured bulk density according to the present invention is measured using known techniques, for example those described in "Powder testing guide: Methods of measuring the physical properties of Bulk powders" L. Svarovsky, Elsevier Applied Science 1987, pp 34-86. A potent pharmaceutically active substance suitable for use in the invention is, for example, an antiarrhythmic drug, tranquiliser, cardiac glycoside, hormone, hypertensive drug, antidiabetic or anticancer drug, sedative or analgesic drug, antibiotic, antirheumatic drug, immunotherapy, antirungal or antihypotension drug, vaccine, antiviral drug, protein (e.g. insulin), peptide, vitamin, or a cell surface receptor blocker. It is preferably a glucocorticosteroid, particularly one which is metabolised rapidly, for example beclomethasone dipropionate (BDP), beclomethasone monopropionate (BMP), flunisolide, triamcinolone acetonide, fluticasone propionate, ciclesonide, budesonide, rofleponide or derivatives thereof, momethasone, tipredane, RPR 106541 and/or a p2-agonist such as terbutaline, salbutamol, formoterol, salmeterol, TA 2005, pircumarol or a pharmaceutically acceptable salt thereof; and/or a prophylactic agent such as sodium chromoglycate or nedocromil sodium. Suitable physiologically acceptable salts include acid addition salts derived from inorganic and organic acids, for example the chloride, bromide, sulphate, phosphate, maleate, fumarate, tartrate, citrate, benzoate, 4-methoxybenzoate, 2- or 4-hydroxybenzoate, 4- chlorobenzoate, p-toluenesulphonate, methanesulphonate, ascorbate, acetate, succinate, lactate, glutarate, gluconate, tricarballylate, hydroxynaphthalene-carboxylate or oleate salts or solvates thereof. The carrier substance is preferably a mono-, di- or polysaccharide, a sugar alcohol or another polyol. Suitable carriers are, for example, lactose, glucose, raffinose, melezitose, lactitol, maltitol, trehalose, sucrose, mannitol; and starch. Lactose is particularly preferred, especially in the form of its monohydrate. The ingredients of the formulation according to the invention must both be in a finely divided form, i.e. their mass median diameter should generally be less than 10 urn, preferably from 1 to 7 urn, as measured by a laser diffraction instrument or a coulter counter. The ingredients may be produced in the desired particle size using methods known to those of skill in the art, e.g. milling, micronisation or direct precipitation. The combination of budesonide and formoterol is particularly preferred. Formoterol is preferably used in the form of its fumarate, especially the dihydrate. When the one or more potent pharmaceutically active substances used in the invention are formoterol and budesonide, the molar ratio of formoterol to budesonide in the composition of the invention is preferably from 1:2500 to 12:1, more preferably from 1:555 to 2:1, most preferably from 1:133 to 1:6. The composition according to the invention is preferably formulated to provide a daily dose of formoterol of from 2 to 120 nmol (more preferably from 7 to 70 nmol). When formoterol is used in the form of formoterol fumarate dihydrate, the composition is preferably formulated to provide a daily dose of formoterol fumarate dihydrate of from 1 to 50 jag, more preferably from 3 to 30 ug. The composition according to the invention is preferably formulated to provide a daily dose of budesonide of from 45 to 2200 ug, more preferably from 65 to 1700 jag. More preferably the composition of the invention comprises, as a unit dose, 6ug of formoterol fumarate dihydrate and 100u.g of budesonide, or 4.5\|ig of formoterol fumarate dihydrate and 80ug of budesonide, either of which can be administered up to four times a day. Alternatively the composition of the invention comprises, as a unit dose, 12ug of formoterol fumarate dihydrate and 200ng of budesonide, or 9ug of formoterol fumarate dihydrate and 160^g of budesonide, either of which is administered once or twice a day. Most preferably the composition used in the invention comprises, as a unit dose, 6jig of formoterol fumarate dihydrate and 200ug of budesonide, or 4.5^ig of formoterol fumarate dihydrate and 160^g of budesonide, either of which is administered up to four times a day. Alternatively the composition of the invention comprises, as a unit dose, 12\|jg of formoterol fumarate dihydrate and 400ug of budesonide, or 9\ig of formoterol fumarate dihydrate and 320^ig of budesonide, either of which is administered once or twice a day. According to the invention there is further provided a process for preparing a composition according to the invention which comprises (a) micronising the one or more potent pharmaceutically active substances and the carrier substance; (b) optionally conditioning the product; and (c) spheronizing until the desired bulk density is obtained. The process preferably further comprises a low energy remicronisation step after step (b). The formulation according to the invention may be made by conventional techniques known per se. Such production processes generally comprise micronising the ingredients to the required size, removing any amorphous areas on the particles obtained by, for example, the methods described in WO 92/18110 or WO 95/05805 and then agglomerating, spheronising and sieving the powder obtained. The size of the agglomerates obtained is preferably in the range of from 100 to 2000 um, more preferably from 100 to 800 u,m. The bulk density of the formulation produced may be adjusted by varying the components and the process empirically, for example the bulk density can be increased by lengthening the time in which the particles are tumbled in a spheronising device. In solid-solid mixing, one of the most important features is to ensure content uniformity. The major problem encountered in the powder mixing of fine powders is the inability of mixers to break down powder agglomerates. It has been found that a remicronisation step after the conditioning step of the fine powder with low energy input is advantageous. It should generally be carried out using enough energy to break down powder agglomerates but not with so much energy that the size of the particles themselves is affected. Such a step gives a composition wherein the active substance and carrier substance are substantially uniformly distributed, having for example a relative standard deviation of less than 3% (preferably less than 1%) and does not disturb the crystaJlinity of the fine particles. The formulation according to the invention may be administered using any known dry powder inhaler, for example the inhaler may be a single or a multi dose inhaler, and may be a breath actuated dry powder inhaler, for example TurbuhaJer (trade mark). The invention further provides use of a composition according to the invention in the manufacture of a medicament for use in therapy. The composition according to the invention is useful in the treatment of respiratory disorders, particularly asthma. The invention also provides a method of treating a patient suffering from a respiratory disorder which comprises administering to the patient a therapeutically effective amount of a composition according to the invention. The invention is illustrated, but not limited, by reference to the following Examples. Example 1 0.0315 Parts of formoterol fumarate dihydrate and 2.969 parts of lactose monohydrate are mixed in a tumbling mixer (Turbula) to an evenly distributed mixture, whereafter the mixture is micronised in a spiral jet mill using a pressure and feeding rate suitable to obtain a particle size of less than 3 um (mass median diameter as measured by a coulter counter). The micronised particles were then treated using the method disclosed in WO 95/05805 to remove amorphous regions in their crystal structure. The powder was then agglomerated by feeding the powder into a twin screw feeder (K-Tron), sieving in an oscillating sieve (0.5 mm mesh size), spheronising in a rotating pan with a peripheral speed of 0.5m/s for minutes and then sieving again using the same sieve, then spheronising once more for 6 minutes before final sieving (mesh size 1.0 mm) giving a powder with a bulk density of 0.32g/ml. Example 2 Example 1 was repeated but the powder was remicronised in a spiral jet mill at a lower pressure (about 1 bar) after micronisation and conditioning such that the step of treating the particles in the manner described in WO 95/05805 was not required giving a powder with a bulk density of 0.32 g/ml. Example 3 9 Parts of budesonide and 91 parts of lactose monohydrate were micronised separately in a spiral jet mill at a pressure of about 6-7 bars to give a particle size of less than 3 um before being mixed thoroughly in a Turbula mixer. Before mixing, the lactose monohydrate powder was conditioned according to the method described in WO 95/05805. The mixture was remicronised in a spiral jet mill at a pressure of only about 1 bar to obtain a uniform mixture. The powder was then agglomerated and spheronised as described in Example 1 to obtain a bulk density of 0.35 g/ml. Example 4 60 Parts of terbutaline sulphate were micronized to a mass medium diameter of less than 2 um in a Alpin mill 100AFG and thereafter conditioned according to the method described in US 5562923. 40 Parts of lactose monohydrate were micronized (Alpin mill 100AFG) down to a mass medium diameter of less than 3 um and thereafter conditioned according to the method described in WO 95/05805. The micronized and conditioned terbutaline sulphate and lactose monohydrate were mixed thoroughly in a Turbula mixer. The mixture was remicronised in a spiral jet mill at a pressure of only about 1 bar to obtain an evenly distributed mixture. The powder was then agglomerated and spheronised as described in Example 1 to obtain a bulk density of 0.28 g/ml. Example 5 Example 4 was repeated with 30 parts of terbutaline sulphate and 70 parts of lactose monohydrate to give a powder with a bulk density of 0.31 g/ml. Example 6 5.2 Parts of formoterol fumarate dihydrate and 896.8 parts of lactose monohydrate were mixed in a tumbling mixer to an evenly distributed mixture, whereafter the mixture was micronised in a spiral mill using a pressure and feeding rate suitable to obtain a particle size of less than 3 urn (mass medium diameter as measured by a coulter counter). The micronised particles were then treated using the method described in WO 95/05805 to remove amorphous regions in their crystal structure. 98 parts of micronised budesonide were added and the mixture was remicronized at a lower pressure in a spiral jet mill to a homogenous mixture. The powder was then agglomerated by feeding into a screw feeder (K-Tron), sieved in an ocillating sieve (0.5 mm mesh size), spheronised in a rotating pan with a speed of 23 rpm for 10 minutes, then sieved again (0.5 mm mesh size), spheronised once more before final sieved (0.8 mm mesh size) to give a powder with a bulk density of 0.34 g/ml. Example 7 Example 6 was repeated with identical conditions but using 5.2 parts of micronized formoterol fumarate dihydrate, 798.8 parts of micronized lactose monohydrate and 196 parts of micronized budesonide. The bulk density obtained was 0.34 g/ml. WE CLAIM: 1. A dry powder composition comprising particles of budesonide and formoterol and particles of a carrier substance, all of which particles: (a) have a mass median diameter of less than 10 µm, (b) are substantially uniformly distributed, and (c) are in the form of a spheronized agglomerate having size in the range of from 100 to 2000 µm, wherein the particles have been substantially uniformly distributed by mixing prior to agglomeration and the composition has a poured bulk density of from 0.30 to 0.36 g/ml. 2. A composition as claimed in claim 1, wherein the formoterol is formoterol fumarate dihydrate. 3. A composition as claimed in claim 1 or 2, wherein the carrier substance is selected from lactose, glucose, raffinose, melezitose, lactitol, maltitol, trehalose, sucrose, mannitol and starch. 4. A composition as claimed in claim 3, where the carrier substance is lactose monohydrate. 5. A composition as claimed in any one of claims 1 to 4 for use in the treatment of a respiratory disorder. 6. A process for preparing a composition as claimed in claim 1, which comprises: (a) micronising the budesonide and formoterol and the carrier substance; (b) optionally conditioning the product; and (c) spheronizing until the desired bulk density is obtained. 7. A process as claimed in claim 6, which comprises a low energy remicronisation step after step (b).

Full Text

The present application relates to a dry powder composition.
Background to the Invention
Potent drugs for administration by inhalation are generally formulated in association with carriers such as lactose because of the problem of preparing accurate doses. When such drugs are diluted, variations in the weight of the formulation result in a smaller drug dosage variation rate compared with when they are not diluted. These formulations have generally consisted of coarse particles of the carrier with fine particles of the drug, which combination is generally known as an ordered mixture.
The invention provides an improved formulation which, in systems designed to imitate inhalation has been found to give an improved dispersion of the drug.
Description of the Invention
According to the invention there is provided a dry powder composition comprising one or more potent pharmaceutically active substances and a carrier substance, all of which are in finely divided form, wherein the formulation has a poured bulk density of from 0.28 to 0.38 g/ml, preferably from 0.30 to 0.36 g/ml.
The poured bulk density according to the present invention is measured using known techniques, for example those described in "Powder testing guide: Methods of measuring the physical properties of Bulk powders" L. Svarovsky, Elsevier Applied Science 1987, pp
34-86.

A potent pharmaceutically active substance suitable for use in the invention is, for
example, an antiarrhythmic drug, tranquiliser, cardiac glycoside, hormone, hypertensive
drug, antidiabetic or anticancer drug, sedative or analgesic drug, antibiotic, antirheumatic
drug, immunotherapy, antirungal or antihypotension drug, vaccine, antiviral drug, protein
(e.g. insulin), peptide, vitamin, or a cell surface receptor blocker. It is preferably a
glucocorticosteroid, particularly one which is metabolised rapidly, for example
beclomethasone dipropionate (BDP), beclomethasone monopropionate (BMP), flunisolide,
triamcinolone acetonide, fluticasone propionate, ciclesonide, budesonide, rofleponide or
derivatives thereof, momethasone, tipredane, RPR 106541 and/or a p2-agonist such as
terbutaline, salbutamol, formoterol, salmeterol, TA 2005, pircumarol or a pharmaceutically
acceptable salt thereof; and/or a prophylactic agent such as sodium chromoglycate or
nedocromil sodium.
Suitable physiologically acceptable salts include acid addition salts derived from inorganic
and organic acids, for example the chloride, bromide, sulphate, phosphate, maleate,
fumarate, tartrate, citrate, benzoate, 4-methoxybenzoate, 2- or 4-hydroxybenzoate, 4-
chlorobenzoate, p-toluenesulphonate, methanesulphonate, ascorbate, acetate, succinate,
lactate, glutarate, gluconate, tricarballylate, hydroxynaphthalene-carboxylate or oleate salts
or solvates thereof.
The carrier substance is preferably a mono-, di- or polysaccharide, a sugar alcohol or
another polyol. Suitable carriers are, for example, lactose, glucose, raffinose, melezitose,
lactitol, maltitol, trehalose, sucrose, mannitol; and starch. Lactose is particularly preferred,
especially in the form of its monohydrate.
The ingredients of the formulation according to the invention must both be in a finely
divided form, i.e. their mass median diameter should generally be less than 10 urn,
preferably from 1 to 7 urn, as measured by a laser diffraction instrument or a coulter
counter. The ingredients may be produced in the desired particle size using methods
known to those of skill in the art, e.g. milling, micronisation or direct precipitation.
The combination of budesonide and formoterol is particularly preferred. Formoterol is
preferably used in the form of its fumarate, especially the dihydrate.
When the one or more potent pharmaceutically active substances used in the invention are
formoterol and budesonide, the molar ratio of formoterol to budesonide in the composition
of the invention is preferably from 1:2500 to 12:1, more preferably from 1:555 to 2:1, most
preferably from 1:133 to 1:6. The composition according to the invention is preferably
formulated to provide a daily dose of formoterol of from 2 to 120 nmol (more preferably
from 7 to 70 nmol). When formoterol is used in the form of formoterol fumarate dihydrate,
the composition is preferably formulated to provide a daily dose of formoterol fumarate
dihydrate of from 1 to 50 jag, more preferably from 3 to 30 ug. The composition according
to the invention is preferably formulated to provide a daily dose of budesonide of from 45
to 2200 ug, more preferably from 65 to 1700 jag.
More preferably the composition of the invention comprises, as a unit dose, 6ug of
formoterol fumarate dihydrate and 100u.g of budesonide, or 4.5|ig of formoterol fumarate
dihydrate and 80ug of budesonide, either of which can be administered up to four times a
day. Alternatively the composition of the invention comprises, as a unit dose, 12ug of
formoterol fumarate dihydrate and 200ng of budesonide, or 9ug of formoterol fumarate
dihydrate and 160^g of budesonide, either of which is administered once or twice a day.
Most preferably the composition used in the invention comprises, as a unit dose, 6jig of
formoterol fumarate dihydrate and 200ug of budesonide, or 4.5^ig of formoterol fumarate
dihydrate and 160^g of budesonide, either of which is administered up to four times a day.
Alternatively the composition of the invention comprises, as a unit dose, 12|jg of
formoterol fumarate dihydrate and 400ug of budesonide, or 9\ig of formoterol fumarate
dihydrate and 320^ig of budesonide, either of which is administered once or twice a day.
According to the invention there is further provided a process for preparing a composition
according to the invention which comprises
(a) micronising the one or more potent pharmaceutically active substances and the
carrier substance;
(b) optionally conditioning the product; and
(c) spheronizing until the desired bulk density is obtained.
The process preferably further comprises a low energy remicronisation step after step (b).
The formulation according to the invention may be made by conventional techniques
known per se. Such production processes generally comprise micronising the ingredients
to the required size, removing any amorphous areas on the particles obtained by, for
example, the methods described in WO 92/18110 or WO 95/05805 and then
agglomerating, spheronising and sieving the powder obtained. The size of the
agglomerates obtained is preferably in the range of from 100 to 2000 um, more preferably
from 100 to 800 u,m. The bulk density of the formulation produced may be adjusted by
varying the components and the process empirically, for example the bulk density can be
increased by lengthening the time in which the particles are tumbled in a spheronising
device.
In solid-solid mixing, one of the most important features is to ensure content uniformity.
The major problem encountered in the powder mixing of fine powders is the inability of
mixers to break down powder agglomerates. It has been found that a remicronisation step
after the conditioning step of the fine powder with low energy input is advantageous. It
should generally be carried out using enough energy to break down powder agglomerates
but not with so much energy that the size of the particles themselves is affected. Such a
step gives a composition wherein the active substance and carrier substance are
substantially uniformly distributed, having for example a relative standard deviation of less
than 3% (preferably less than 1%) and does not disturb the crystaJlinity of the fine
particles.
The formulation according to the invention may be administered using any known dry
powder inhaler, for example the inhaler may be a single or a multi dose inhaler, and may be
a breath actuated dry powder inhaler, for example TurbuhaJer (trade mark). The invention
further provides use of a composition according to the invention in the manufacture of a
medicament for use in therapy. The composition according to the invention is useful in the
treatment of respiratory disorders, particularly asthma. The invention also provides a
method of treating a patient suffering from a respiratory disorder which comprises
administering to the patient a therapeutically effective amount of a composition according
to the invention.
The invention is illustrated, but not limited, by reference to the following Examples.
Example 1
0.0315 Parts of formoterol fumarate dihydrate and 2.969 parts of lactose monohydrate are
mixed in a tumbling mixer (Turbula) to an evenly distributed mixture, whereafter the
mixture is micronised in a spiral jet mill using a pressure and feeding rate suitable to obtain
a particle size of less than 3 um (mass median diameter as measured by a coulter counter).
The micronised particles were then treated using the method disclosed in WO 95/05805 to
remove amorphous regions in their crystal structure. The powder was then agglomerated
by feeding the powder into a twin screw feeder (K-Tron), sieving in an oscillating sieve
(0.5 mm mesh size), spheronising in a rotating pan with a peripheral speed of 0.5m/s for minutes and then sieving again using the same sieve, then spheronising once more for 6
minutes before final sieving (mesh size 1.0 mm) giving a powder with a bulk density of
0.32g/ml.
Example 2
Example 1 was repeated but the powder was remicronised in a spiral jet mill at a lower
pressure (about 1 bar) after micronisation and conditioning such that the step of treating the
particles in the manner described in WO 95/05805 was not required giving a powder with a
bulk density of 0.32 g/ml.
Example 3
9 Parts of budesonide and 91 parts of lactose monohydrate were micronised separately in a
spiral jet mill at a pressure of about 6-7 bars to give a particle size of less than 3 um before
being mixed thoroughly in a Turbula mixer. Before mixing, the lactose monohydrate
powder was conditioned according to the method described in WO 95/05805. The mixture
was remicronised in a spiral jet mill at a pressure of only about 1 bar to obtain a uniform
mixture. The powder was then agglomerated and spheronised as described in Example 1 to
obtain a bulk density of 0.35 g/ml.
Example 4
60 Parts of terbutaline sulphate were micronized to a mass medium diameter of less than 2
um in a Alpin mill 100AFG and thereafter conditioned according to the method described
in US 5562923. 40 Parts of lactose monohydrate were micronized (Alpin mill 100AFG)
down to a mass medium diameter of less than 3 um and thereafter conditioned according to
the method described in WO 95/05805. The micronized and conditioned terbutaline
sulphate and lactose monohydrate were mixed thoroughly in a Turbula mixer. The mixture
was remicronised in a spiral jet mill at a pressure of only about 1 bar to obtain an evenly
distributed mixture. The powder was then agglomerated and spheronised as described in
Example 1 to obtain a bulk density of 0.28 g/ml.
Example 5
Example 4 was repeated with 30 parts of terbutaline sulphate and 70 parts of lactose
monohydrate to give a powder with a bulk density of 0.31 g/ml.
Example 6
5.2 Parts of formoterol fumarate dihydrate and 896.8 parts of lactose monohydrate were
mixed in a tumbling mixer to an evenly distributed mixture, whereafter the mixture was
micronised in a spiral mill using a pressure and feeding rate suitable to obtain a particle
size of less than 3 urn (mass medium diameter as measured by a coulter counter). The
micronised particles were then treated using the method described in WO 95/05805 to
remove amorphous regions in their crystal structure. 98 parts of micronised budesonide
were added and the mixture was remicronized at a lower pressure in a spiral jet mill to a
homogenous mixture. The powder was then agglomerated by feeding into a screw feeder
(K-Tron), sieved in an ocillating sieve (0.5 mm mesh size), spheronised in a rotating pan
with a speed of 23 rpm for 10 minutes, then sieved again (0.5 mm mesh size), spheronised
once more before final sieved (0.8 mm mesh size) to give a powder with a bulk density of
0.34 g/ml.
Example 7
Example 6 was repeated with identical conditions but using 5.2 parts of micronized
formoterol fumarate dihydrate, 798.8 parts of micronized lactose monohydrate and 196
parts of micronized budesonide. The bulk density obtained was 0.34 g/ml.

WE CLAIM:
1. A dry powder composition comprising particles of budesonide and
formoterol and particles of a carrier substance, all of which particles: (a)
have a mass median diameter of less than 10 µm, (b) are substantially
uniformly distributed, and (c) are in the form of a spheronized agglomerate
having size in the range of from 100 to 2000 µm, wherein the particles have
been substantially uniformly distributed by mixing prior to agglomeration
and the composition has a poured bulk density of from 0.30 to 0.36 g/ml.
2. A composition as claimed in claim 1, wherein the formoterol is formoterol fumarate dihydrate.
3. A composition as claimed in claim 1 or 2, wherein the carrier substance is selected from lactose, glucose, raffinose, melezitose, lactitol, maltitol, trehalose, sucrose, mannitol and starch.

4. A composition as claimed in claim 3, where the carrier substance is lactose monohydrate.
5. A composition as claimed in any one of claims 1 to 4 for use in the treatment of a respiratory disorder.
6. A process for preparing a composition as claimed in claim 1, which comprises:

(a) micronising the budesonide and formoterol and the carrier substance;
(b) optionally conditioning the product; and
(c) spheronizing until the desired bulk density is obtained.
7. A process as claimed in claim 6, which comprises a low energy
remicronisation step after step (b).

Documents:

0744-del-2000-abstract.pdf

0744-del-2000-claims.pdf

0744-del-2000-correspondence-others.pdf

0744-del-2000-description (complete)-15-02-2008.pdf

0744-del-2000-description (complete).pdf

0744-del-2000-form-1.pdf

0744-del-2000-form-18.pdf

0744-del-2000-form-2.pdf

0744-del-2000-form-3.pdf

0744-del-2000-form-5.pdf

0744-del-2000-petition-138.pdf

744-DEL-2000-Abstract-(15-02-2008).pdf

744-DEL-2000-Claims-(15-02-2008).pdf

744-DEL-2000-Correspondence-Others-(15-02-2008).pdf

744-DEL-2000-Form-1-(15-02-2008).pdf

744-DEL-2000-Form-2-(15-02-2008).pdf

744-DEL-2000-Form-3-(15-02-2008).pdf

744-DEL-2000-Petition-137-(15-02-2008).pdf

744-DEL-2000-Petition-138-(15-02-2008).pdf

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Patent Number

225755

Indian Patent Application Number

0744/DEL/2000

PG Journal Number

03/2009

Publication Date

16-Jan-2009

Grant Date

27-Nov-2008

Date of Filing

21-Aug-2000

Name of Patentee

ASTRA AKTIEBOLAG

Applicant Address

S-151 85 SODERTALJE, SWEDEN.

Inventors:

#	Inventor's Name	Inventor's Address
1	JAN TROFAST	VAPENKROKEN 34, S-226 47 LUND, SWEDEN.

PCT International Classification Number

A61K 9/14

PCT International Application Number

N/A

PCT International Filing date

PCT Conventions:

#	PCT Application Number	Date of Convention	Priority Country
1	9700135-8	1997-01-20	Sweden