ZA200501703B - Pharmaceutical products and compositions comprising specific anticholinergic agents, beta-2-agonists and corti-costeroids. - Google Patents
Pharmaceutical products and compositions comprising specific anticholinergic agents, beta-2-agonists and corti-costeroids. Download PDFInfo
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- ZA200501703B ZA200501703B ZA200501703A ZA200501703A ZA200501703B ZA 200501703 B ZA200501703 B ZA 200501703B ZA 200501703 A ZA200501703 A ZA 200501703A ZA 200501703 A ZA200501703 A ZA 200501703A ZA 200501703 B ZA200501703 B ZA 200501703B
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- South Africa
- Prior art keywords
- budesonide
- tiotropium
- ipratropium
- formoterol
- salmeterol
- Prior art date
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- 239000000825 pharmaceutical preparation Substances 0.000 title claims description 7
- 229940127557 pharmaceutical product Drugs 0.000 title claims description 7
- 239000003246 corticosteroid Substances 0.000 title description 5
- 239000000812 cholinergic antagonist Substances 0.000 title description 4
- 229960001334 corticosteroids Drugs 0.000 title description 4
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Description
PHARMACEUTICAL PRODUCTS AND COMPOSITIONS COMPRISING SPECIFIC ANTICHOLINERGIC
AGENTS, BETA-2 AGONISTS AND CORTICOSTEROIDS
This invention relates to pharmaceutical products and compositions for use in the ! treatment of asthma and related disorders, and especially but not exclusively for the treatment of chronic obstructive pulmonary disease (COPD).
The pathophysiology of asthma and related disorders involves various distinct symptoms, including bronchoconstriction, inflammation of the airways, and increased mucous secretion, which results in wheezing, coughing and shortness of breath. A persistent or recurrent cough may exacerbate the problem by causing further irritation and inflammation of the airways. The causes of asthma are wide-ranging and not yet fully understood.
Bronchoconstriction occurs due to bronchial smooth muscle spasm and airway inflammation with mucosal edema. Asthma and other related disorders, have been known to be treated with f-2 adrenergic receptor agonists (B-2 agonist) as they provide a bronchodilator effect to the patients, resulting in relief from the symptoms of breathlessness.
B-2 Agonists can be short acting for immediate relief, or long acting for long-term prevention, of asthma symptoms. Short acting B-2 agonists currently available include: salbutamol, biltolterol, pirbuterol and terbutaline. Long acting B-2 agonists currently available include salmeterol and formoterol.
Whilst it is also known that B-2 agonists provide symptomatic relief of bronchoconstriction in patients, another component of asthma, ie. inflammation, often requires separate treatment. Typically this involves treatment with a steroid. Indeed, treatment with a corticosteroid is considered one of the most potent and effective therapies currently available for persistent asthma. Currently available corticosteroids include: beclomethasone, budesonide, flunisolide, fluticasone, mometasone and triamcinolone.
Bronchoconstriction and inflammation are also associated with bronchial plugging with secretions, which may be treated with anti-cholinergic agents, such as troventol, . ipratropium, oxitropium and tiotropium.
These medicaments can be administered in different ways, such as in MDIs (metered- ' dosage inhalers), in DPIs (dry powder inhalers), and in oral and liquid formulations.
Treatment in these different ways calls for the patient to comply with different dosage regimens, different frequencies of administration, etc. Also, since most of the medications are in the form of aerosols, the patient is required to carry several formulations and dispensers, one for each of these medicaments. . To assist patient compliance, combination products are known, e.g. an inhalation combination medication of fluticasone propionate and salmeterol, the combination being ’ provided in one easy-to-use device. This combination product provides simultaneous treatment of airway constriction by means of the B-2 agonist (salmeterol), and treatment of inflammation by means of the steroid (fluticasone propionate).
A combination of ipratropium bromide and salbutamol is also known. This combination therapy provides an anti-cholinergic (ipratropium bromide) to reduce the bronchial secretions and a B-2 agonist (salbutamol) to reduce constriction. Other described combinations include ipratropium and salbutamol (WO 01/76601) and tiotropium and formoterol (WO 00/47200).
It would be highly desirable, however, to provide a combination therapy suitable to reduce bronchial inflammation, bronchial constriction and bronchial secretions in a single product or dosage form. It would also be desirable to provide such a combination product or composition in a form whereby the correct dosage of the various components is easily and safely administered.
We have now found that certain therapeutic three-in-one combinations comprising specific B-2 agonists, anti-cholinergics and steroids surprisingly provide an enhanced, synergistic, effect in terms of treatment of bronchoconstriction, inflammation and mucous secretions of airways. Also the three-in-one combination therapy as provided by the present invention is an extremely patient-friendly combination, which results in maximum patient compliance and better control of asthma than the known combinations or single therapies.
The present invention further provides, therefore, a pharmaceutical product comprising any one of the following combinations of therapeutic agents, as a combined preparation for simultaneous, separate or sequential use in the treatment of conditions for which administration of one or more of the therapeutic agents is indicated: v @) salmeterol, ciclesonide and tiotropium; (ii) formoterol, budesonide and ipratropium; . (iii) formoterol, ciclesonide and tiotropium, (iv) formoterol, budesonide and oxitropium; (v) salbutamol, beclomethasone and ipratropium;
(vi) salbutamol, budesonide and tiotropium; (vii) terbutaline, fluticasone and tiotropium; . (viii) terbutaline, fluticasone and ipratropium, (ix) salbutamol, budesonide and ipratropium, ' (x) salmeterol, fluticasone and ipratropium, (xi) salmeterol, budesonide and ipratropium; (xii) salmeterol, fluticasone and tiotropium; and (xiii) formoterol, budesonide and tiotropium.
It will also be appreciated from the above, that the respective therapeutic agents of the combined preparations can be administered simultaneously, either in the same or different pharmaceutical formulations, or separately or sequentially. If there is separate or sequential administration, it will also be appreciated that the subsequently administered therapeutic agents should be administered to a patient within a time scale so as to achieve, or more particularly optimise, the above referred to advantageous synergistic therapeutic effect of a combined preparation as present in a pharmaceutical product according to the present invention.
The present invention also provides a pharmaceutical composition comprising any one of the following combinations of therapeutic agents: @) salmeterol, ciclesonide and tiotropium; (ii) formoterol, budesonide and ipratropium; (iii) formoterol, ciclesonide and tiotropium,; (iv) formoterol, budesonide and oxitropium; wv) salbutamol, beclomethasone and ipratropium; (vi) salbutamol, budesonide and tiotropium; (vii) terbutaline, fluticasone and tiotropium; (viii) terbutaline, fluticasone and ipratropium; (ix) salbutamol, budesonide and ipratropium; . (x) salmeterol, fluticasone and ipratropium; (xi) salmeterol, budesonide and ipratropium; . (xii) salmeterol, fluticasone and tiotropium; and (xiii) formoterol, budesonide and tiotropium.
together with a pharmaceutically acceptable carrier or excipient therefor.
The abovementioned compounds may exist, and be used in the present invention, in ‘ various active forms, whilst retaining the same physiological function. For example, the anticholinergic agents, B-2 agonists and corticosteroids may exist as various acid addition ! salts, such as those formed from hydrochloric, hydrobromic, sulphuric, acetic, lactic, maleic, tartaric, oxalic, methanesulphonic, p-toluenesulpbonic and benzenesulphonic acids. The skilled person will also appreciate that the abovementioned compounds may also exist as esters and (R) and (S) enantiomers and provided the desired activity is maintained, they may be used in the present invention.
Specific triple combinations of the invention as illustrated by the Examples are: 6) salmeterol, ciclesonide and tiotropium bromide; (i) formoterol, budesonide and ipratropium; (iii) formoterol, ciclesonide and tiotropium bromide; (iv) formoterol, budesonide and oxitropium,; (v) salbutamol sulphate, beclomethasone and ipratropium; (vi) salbutamol sulphate, budesonide and tiotropium bromide; (vii) terbutaline sulphate, fluticasone and tiotropium bromide; (viii) terbutaline sulphate, fluticasone and ipratropium bromide; (ix) salbutamol sulphate, budesonide and ipratropium bromide; x) salmeterol, fluticasone propionate and ipratropium bromide; (xi) salmeterol, budesonide and ipratropium bromide; (xii) salmeterol, fluticasone propionate and tiotropium bromide; and (xiii) formoterol, budesonide and tiotropium bromide.
The pharmaceutical composition may be provided in any suitable dosage form.
Preferably the composition is in the form of a suspension, a particulate suspension or a clear solution. The pharmaceutical composition of the present invention may alternatively be provided as an inhalation powder. . The pharmaceutical composition of the present invention may be administered by any suitable administration method and it may be preferred that the composition is administered . as an aerosol. The composition of the present invention can comprise a propellant-containing dosage aerosol, an inhalation powder or a propellant free inhalation solution or suspension.
The compositions of the present invention may thus be provided by, for example, a metered dose inhaler (MDI), dry powder inhaler (DPI), nebules, nebuliser or nasal spray.
In the case of a propellant-containing dosage aerosol, typically the propellant can be ; selected from the group consisting of 1,1,1,2-tetrafluoroethane, 1,1,1,2,3,3,3- heptafluoroethane, monofluorotrichloromethane and dichlorodifluoromethane. * In the case of a particulate suspension or a solution for the propellant-containing aerosol composition, the composition may further comprise one or more co-solvents. The composition may comprise both a propellant and a co-solvent, in which case it is desirable that the co-solvent has a greater polarity than the propellant. The co-solvent used may be any suitable solvent. Typically the co-solvent is ethanol. Generally the ratio of propellant to solvent is between 50:50 to 99:1.
If aerosolized, the formulation may consist of a surface-active agent to stabilize the formulation and for the lubrication of a valve system in the inhaler/nebuliser/nasal spray.
Some of the most commonly used surface-active agents in the aerosol formulations are oils derived from natural sources, such as corn oil, olive oil, cotton seed oil and sunflower seed oil and phospholipids. Preferred surfactants for use according to the present invention are oleic acid, lecithin or sorbitol trioleate. In these embodiments, the surface-active agents are preferably used in the formulations in the ratio of 0.00002 wt% wt to 20 wt% of the active ingredients. The surface-active agents may exceed this weight ratio in cases where drug concentration in the formulation is very low.
The active ingredients in all the above aerosol formulations are preferably in the concentration of 0.001 wt% to 5 wt% of the total formulation.
The active ingredients are provided in an appropriate particle size, generally in the range from nano-size to about 12 um. Preferably, approximately 95% are below 5 or 6 um (micrometers), with the all particles being below 12 um (when measured by laser), or approximately 95% below 2.5 um and the rest of the particles between 2.5-5 pum (when measured by microscope).
According to another aspect of the invention there is provided an aerosol device, . comprising a housing containing a composition as described above, and a dispensing mechanism for dispensing the composition from the housing in a metered dose. : The dispensing mechanism may include a valve capable of releasing a metered dosage of the composition. Preferably the housing is sealed and pressurized at a pressure exceeding atmospheric pressure.
The housing may be metallic, preferably aluminum. Preferably, the housing is plastic-coated, lacquer-coated or anodised. The composition of the present invention may be ‘ placed in the housing through a suitable metering device.
Preferred combinations of active ingredients for administration by way of a propellant-containing dosage aerosols according to the present invention are further illustrated by the Examples and can include any one of the following combinations: 1) salmeterol, ciclesonide and tiotropium; (ii) formoterol, budesonide and ipratropium; (ili) formoterol, ciclesonide and tiotropium; (iv) formoterol, budesonide and oxitropium; (v) salbutamol, beclomethasone and ipratropium; (vi) salbutamol, budesonide and tiotropium; (vil) terbutaline, fluticasone and tiotropium; {viil) salmeterol, fluticasone and tiotropium; and (ix) formoterol, budesonide and tiotropium.
More specifically the following may be administered by way of propellant-containing dosage aerosols according to the present invention: §)) salmeterol, ciclesonide and tiotropium bromide; (ii) formoterol, budesonide and ipratropium; (iif) formoterol, ciclesonide and tiotropium bromide; (iv) formoterol, budesonide and oxitropium; (v) salbutamol sulphate, beclomethasone and ipratropium; (vi) salbutamol sulphate, budesonide and tiotropium bromide; (vii) terbutaline sulphate, fluticasone and tiotropium bromide; (viii) salmeterol, fluticasone propionate and tiotropium bromide; (ix) formoterol, budesonide and tiotropium bromide.
In the case where the triple combinations of the present invention are provided as ; inhalation powders, typically suitable pharmaceutically acceptable excipients may be selected from monosaccharides, disaccharides, oligosaccharides, polysaccharides or the like, with the - use of lactose as the excipient in the inhalation powders of the present invention being preferred. The inhalation powders of the present invention can typically be administered by means of dry powder inhalers known in the art. Preferred combinations of active ingredients for administration by way of inhalation powders according to the present invention are further illustrated by the Examples and can include any one of the following combinations: ‘ @d) salmeterol, ciclesonide and tiotropium; (ii) formoterol, budesonide and ipratropium; ’ (iii) formoterol, ciclesonide and tiotropium; (iv) salbutamol, beclomethasone and ipratropium; (v) salbutamol, budesonide and tiotropium; and (vi) terbutaline, fluticasone and tiotropium.
More specifically the following may be administered by way of inhalation powders according to the present invention: 6) salmeterol, ciclesonide and tiotropium bromide; (if) formoterol, budesonide and ipratropium; (iii) formoterol, ciclesonide and tiotropium bromide; (iv) salbutamol sulphate, beclomethasone and ipratropium; (v) salbutamol sulphate, budesonide and tiotropium bromide; and (vi) terbutaline sulphate, fluticasone and tiotropium bromide.
The propellant free inhalation solutions of the present invention are typically suitable for administration by way of nebulisation, employing nebulisers well known in the art that can advantageously be employed to produce inhalable aerosols comprising the triple combinations of active ingredients according to the present invention. Preferred combinations of active ingredients for administration by way of propellant free inhalation solutions according to the present invention are further illustrated by the Examples and can include any one of the following combinations: (i) terbutaline, fluticasone and ipratropium; (ii) salbutamol, budesonide and ipratropium; (iii) salmeterol, fluticasone and ipratropium; and (iv) salmeterol, budesonide and ipratropium. . More specifically the following may be administered by way of propellant free inhalation solutions according to the present invention: : (i) terbutaline sulphate, fluticasone and ipratropium bromide; (ii) salbutamol sulphate, budesonide and ipratropium bromide; (iii) salmeterol, fluticasone propionate and ipratropium bromide; and
(iv) salmeterol, budesonide and ipratropium bromide.
According to another aspect of the invention, there is provided the use of any one of the following combinations in the manufacture of a medicament for the prophylaxis or treatment of conditions for which administration of one or more of the therapeutic agents is indicated: 1) salmeterol, ciclesonide and tiotropium, (ii) formoterol, budesonide and ipratropium; (iii) formoterol, ciclesonide and tiotropium; (iv) formoterol, budesonide and oxitropium; (v) salbutamol, beclomethasone and ipratropium; (vi) salbutamol, budesonide and tiotropium; (vii) terbutaline, fluticasone and tiotropium; (viii) terbutaline, fluticasone and ipratropium; (ix) salbutamol, budesonide and ipratropium; (x) salmeterol, fluticasone and ipratropium; (xi) salmeterol, budesonide and ipratropium; (xii) salmeterol, fluticasone and tiotropium; and (xiii) formoterol, budesonide and tiotropium.
The triple combinations as provided by the present invention are useful for the treatment of inflammatory or respiratory tract diseases, especially asthma and / or chronic obstructive pulmonary disease (COPD), by simultaneous or successive administration.
According to another aspect of the invention there is provided a method for the prophylaxis or treatment of inflammatory or respiratory tract diseases, said method comprising administering either sequentially or simultaneously, to a patient in need thereof, a therapeutically effective amount of any one of the following combinations: @) salmeterol, ciclesonide and tiotropium; (ii) formoterol, budesonide and ipratropium; } (iii) formoterol, ciclesonide and tiotropium; (iv) formoterol, budesonide and oxitropium,; : (v) salbutamol, beclomethasone and ipratropium; (vi) salbutamol, budesonide and tiotropium; (vii) terbutaline, fluticasone and tiotropium;
(viii) terbutaline, fluticasone and ipratropium; (ix) salbutamol, budesonide and ipratropium; ‘ x) salmeterol, fluticasone and ipratropium; (xi) salmeterol, budesonide and ipratropium; ' (xii) salmeterol, fluticasone and tiotropium; and (xiii) formoterol, budesonide and tiotropium.
Any of the following specific triple combinations of the invention as illustrated by the
Examples are suitable to be employed in the manufacture of a medicament, or a method of treatment, as referred to above: @@) salmeterol, ciclesonide and tiotropium bromide; (ii) formoterol, budesonide and ipratropium; (iit) formoterol, ciclesonide and tiotropium bromide; (iv) formoterol, budesonide and oxitropium; (v) salbutamol sulphate, beclomethasone and ipratropium; (vi) salbutamol sulphate, budesonide and tiotropium bromide; (vii) terbutaline sulphate, fluticasone and tiotropium bromide; (viii) terbutaline sulphate, fluticasone and ipratropium bromide; (ix) salbutamol sulphate, budesonide and ipratropium bromide; (x) salmeterol, fluticasone propionate and ipratropium bromide; (xi) salmeterol, budesonide and ipratropium bromide; (xii) salmeterol, fluticasone propionate and tiotropium bromide; and (xiii) formoterol, budesonide and tiotropium bromide.
These products or compositions as provided by the present invention are especially useful in the treatment of COPD. They will normally be administered by inhalation, once or twice daily. By way of example, a preferred dosage for twice daily administrations would be: a) formoterol (6 mcg)/budesonide (200 mcg) ipratropium (40 mcg) b) formoterol (6 mcg)/budesonide (200 mcg)/oxitropium (200 mcg). . The invention will now be described with reference to the following examples, which do not limit the scope of the invention in any way.
Example 1 1,1,1,2-Tetrafluoroethane 18.2 gms
Example 2 1,1,1,2-Tetrafluoroethane 18.2 gms
In the above formulations (Examples 1 and 2), the active ingredients were initially weighed in an aluminum can. Then a metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA 134a was charged through the metering valve. :
Example 3 273 1,1,1,2-Tetrafluoroethane 15.47 gms
In the above formulation the active ingredients were first weighed in an aluminum can, then the ethanol was added and the solution was sonicated for 5 min. The metering valve was : placed on the can and crimped with a vacuum crimper, and then propellant HFA 134a was charged through the metering valve.
Example 4 al
Oleic acid (10%) 5.04 mg 1,1,1,2-Tetrafluoroethane 15.47 gms
In the above formulation the active ingredients were first weighed in an aluminum can then the ethanol and the surfactant were added and solution was sonicated for 5 min. The metering valve was placed on the can and crimped with a vacuum crimper and then the HFA 134a was charged through the metering valve.
Example 5
O35 em ) 1,1,1,2-Tetrafluoroethane 18.2 gms
Example 6 oto
Oleic acid (0.02%) 0.014 mg 1,1,1,2-Tetrafluorocthane 17.83 gms
The above formulations (Examples 5 and 6) were weighed in an aluminum can, and a metering valve was crimped on the can and the propellant added.
Example 7
Qanity seo bong
Top ori 1,1,1,2-Tetrafluoroethane 122g
The active ingredients were initially weighed in an aluminum can. The metering valve was then placed on the can and crimped with a vacuum crimper and then the propellant HFA 134a was charged through the metering valve.
Example 8
TC
Seal [sim
Ethanol (2%) 0244 g
The active ingredients were initially weighed in an aluminum can, then ethanol was added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA134a was charged through the metering valve.
Example 9 nity Fr sal oi)
Sime
Ethanol (2%) 0.244 g
Oleic acid (0.02%) 0.003 mg
The active ingredients were initially weighed in an aluminum can, then ethanol and oleic acid were added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA134a was charged through the metering valve.
Example 10
Gani er sow Bow) 1,1,1,2-Tetrafluoroethane 122g
The active ingredients were initially weighed in an aluminum can. The metering valve was then placed on the can and crimped with a vacuum crimper and then the propellant HFA134a : was charged through the metering valve. ’ Example 11
Tay Fe dre in)
Ethanol (15%) 183¢ 1,1,1,2-Tetrafluoroethane 182g
The active ingredients were initially weighed in an aluminum can, then ethanol was added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA134a was charged through the metering valve.
Example 12 iy Fer ssl ving
Lecithin (1%) 0.122 mg 1,1,1,2-Tetrafluoroethane 182¢
The active ingredients were initially weighed in an aluminum can, then ethanol and lecithin were added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA 134a was charged through the metering valve.
Example 13
Gy srl od 1,1,1,2-Tetrafluoroethane 122g
The active ingredients were initially weighed in an aluminum can. The metering valve was then placed on the can and crimped with a vacuum crimper and then the propellant HFA 134a was charged through the metering valve.
Example 14 ay sro Bow)
Ethanol (15%) 1.83 ¢g 1,1,1,2-Tetrafluoroethane 104 ¢
The active ingredients were initially weighed in an aluminum can, then ethanol was added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA134a was charged through the metering valve. - Example 15 pins [Gay rr bow)
Lecithin (1%) 0.10 mg 1,1,1,2-Tetrafluoroethane 104g
The active ingredients were initially weighed in an aluminum can, then ethanol and lecithin were added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA 134a was charged through the metering valve,
Example 16
Gui ev ong 1,1,1,2-Tetrafluoroethane 122g
The active ingredients were initially weighed in an aluminum can. The metering valve was then placed on the can and crimped with a vacuum crimper and then the propellant HFA 134a was charged through the metering valve.
Example 17 ui ers Fowin
Ethanol (15%) 183g 1,1,1,2-Tetrafluoroethane 104g
The active ingredients were initially weighed in an aluminum can, then ethanol was added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA134a was charged through the metering valve.
Example 18
Git ers og
Ethanol (15%) 1.83 g
Lecithin (1%) 0.138 mg 1,1,1,2-Tetrafluoroethane 104g
The active ingredients were initially weighed in an aluminum can, then ethanol and lecithin were added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA134a was charged through the metering valve.
Example 19
Cl er)
Salbutamol sulphate 28.8 mg 1,1,1,2-Tetrafluoroethane 182g
The active ingredients were initially weighed in an aluminum can. The metering valve was then placed on the can and crimped with a vacuum crimper and then the propellant HFA134a was charged through the metering valve.
Example 20
Salbutamol sulphate 28.8 mg
Ethanol (2.5 %) 0455¢g 1,1,1,2-Tetrafluoroethane 17.75 g
The active ingredients were initially weighed in an aluminum can, then ethanol was added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA 134a was charged through the metering valve.
Example 21 iy Pr ro bo)
Salbutamol sulphate 28.8 mg
Ethanol (2.5 %) 0455¢g
Oleic acid (0.02%) 0.009mg 1,1,1,2-Tetrafluoroethane 17.75 g
The active ingredients were initially weighed in an aluminum can, then ethanol and oleic acid were added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA134a was charged ; through the metering valve.
Example 22
Tsien [Quy Goro owing
Salbutamol sulphate 28.8 mg 1,1,1,2-Tetrafluoroethane 182g
The active ingredients were initially weighed in an aluminum can. The metering valve was then placed on the can and crimped with a vacuum crimper and then the propellant HFA134a was charged through the metering valve.
Example 23 ity or srl ong
Salbutamol sulphate 28.8 mg
Ethanol (2%) 0.364 g 1,1,1,2-Tetrafluoroethane 17.83 g
The active ingredients were initially weighed in an aluminum can, then ethanol was added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA134a was charged through the metering valve.
Example 24
Qty Perr i)
Salbutamol sulphate 28.8 mg
Ethanol (2%) 0.364 g
Oleic acid (0.02%) 0.0087 mg 1,1,1,2-Tetrafluoroethane 17.83 g
The active ingredients were initially weighed in an aluminum can, then ethanol and oleic acid were added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA 134a was charged through the metering valve.
Example 25 iy oro hoe) 1,1,1,2-Tetrafluorocthane 182g
The active ingredients were initially weighed in an aluminum can. The metering valve was then placed on the can and crimped with a vacuum crimper and then the propellant HFA134a was charged through the metering valve.
Example 26
Git Goro bowie) ) 1,1,1,2-Tetrafluoroethane 122¢g
The active ingredients were initially weighed in an aluminum can, then ethanol was added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA 134a was charged through the metering valve.
Example 27
Gy Fos hoe
Teun sip 1,1,1,2-Tetrafluoroethane 15.83 g
The active ingredients were initially weighed in an aluminum can, then ethanol and lecithin were added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA134a was charged through the metering valve.
Example 28 1,1,1,2-Tetrafluoroethane
The active ingredients were initially weighed in an aluminum can. Metering valve was then placed on the can and crimped with a vacuum crimper and then the propellant HFA 134a was charged through the metering valve.
Example 29
Ingredients | Quantity (Per aerosol housing)
Tiotropium bromide
Ethanol (2% 0244g 1,1,1,2-Tetrafluoroethane
The active ingredients were initially weighed in an aluminum can, then ethanol was added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA134a was charged through the metering valve.
Example 30 5.81 mg
Fluticasone ~~ [200mg
Ethanol (2% 0244 g
Oleic acid (0.02% 0.003 mg 1,1,1,2-Tetrafluoroethane
The active ingredients were initially weighed in an aluminum can, then ethanol and the surfactant were added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA 134a was charged through the metering valve.
Example 31 : 1,1,1,2-Tetrafluoroethane
The active ingredients were initially weighed in an aluminum can. Metering valve was then placed on the can and crimped with a vacuum crimper and then the propellant HFA 134a was charged through the metering valve.
Example 32 [Formoterol ____ |img
Ethanol (15% (183g 1,1,1,2-Tetrafluoroethane [182g
The active ingredients were initially weighed in an aluminum can, then ethanol was added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA134a was charged through the metering valve.
Example 33
Quantity (Per aerosol housing
Formoterol [10mg
Tiotropium Bromide | 18mg
Budesonide [80mg (Ethanol [183g
Lecithin (1% 012mg 1,1,1,2-Tetrafluoroethane (182g
The active ingredients were initially weighed in an aluminum can, then ethanol and the surfactant were added and the solution was sonicated for 5 minutes. The metering valve was placed on the can and crimped with a vacuum crimper and then the propellant HFA 134a was charged through the metering valve.
The following Examples are inhalation powders suitable for DPIs, and were prepared by techniques well known in the art. . Example 34
Togs [Gun Gm prc
Tiotropium bromide 0.018 mg
Example 35
Example 36
Quit mg or a
Tiotropium Bromide 0.018 mg
Example 37
Quy me pr ap . Example 38
Toso [uy (repro
Claims (33)
- CLAIMS: 1 A pharmaceutical product comprising any one of the following combinations of therapeutic agents, as a combined preparation for simultaneous, separate or sequential use in . the treatment of conditions for which administration of one or more of the therapeutic agents is indicated: @) salmeterol, ciclesonide and tiotropium; (ii) formoterol, budesonide and ipratropium; (iii) formoterol, ciclesonide and tiotropium; (iv) formoterol, budesonide and oxitropium; wv) salbutamol, beclomethasone and ipratropium; (vi) salbutamol, budesonide and tiotropium; (vii) terbutaline, fluticasone and tiotropium, (viii) terbutaline, fluticasone and ipratropium, (ix) salbutamol, budesonide and ipratropium; (x) salmeterol, fluticasone and ipratropium; (xi) salmeterol, budesonide and ipratropium; (xii) salmeterol, fluticasone and tiotropium; and (xiii) formoterol, budesonide and tiotropium; wherein the above therapeutic agents can optionally be present as a pharmaceutically acceptable salt or ester thereof, or in enantiomerically pure form or as a racemic mixture. 2, A pharmaceutical product according to claim 1, which comprises any one of the following combinations of therapeutic agents: (i) salmeterol, ciclesonide and tiotropium bromide; (if) formoterol, budesonide and ipratropium; (iii) formoterol, ciclesonide and tiotropium bromide; ] (iv) formoterol, budesonide and oxitropium; Ww salbutamol sulphate, beclomethasone and ipratropium; . (vi) salbutamol sulphate, budesonide and tiotropium bromide; (vii) terbutaline sulphate, fluticasone and tiotropium bromide; (viii) terbutaline sulphate, fluticasone and ipratropium bromide;
- (ix) salbutamol sulphate, budesonide and ipratropium bromide; (x) salmeterol, fluticasone propionate and ipratropium bromide; (xi) salmeterol, budesonide and ipratropium bromide; (xii) salmeterol, fluticasone propionate and tiotropium bromide; and . (xiii) formoterol, budesonide and tiotropium bromide.
- 3. A pharmaceutical composition comprising any one of the following combinations of therapeutic agents: 6) salmeterol, ciclesonide and tiotropium; (ii) formoterol, budesonide and ipratropium; (iii) formoterol, ciclesonide and tiotropium; (iv) formoterol, budesonide and oxitropium; wv) salbutamol, beclomethasone and ipratropium; (vi) salbutamol, budesonide and tiotropium; (vii) terbutaline, fluticasone and tiotropium; (viii) terbutaline, fluticasone and ipratropium; (ix) salbutamol, budesonide and ipratropium; (x) salmeterol, fluticasone and ipratropium; (xi) salmeterol, budesonide and ipratropium; (xii) salmeterol, fluticasone and tiotropium; and (xiii) formoterol, budesonide and tiotropium; wherein the above therapeutic agents can optionally be present as a pharmaceutically acceptable salt or ester thereof, or in enantiomerically pure form or as a racemic mixture, together with a pharmaceutically acceptable carrier or excipient therefor.
- 4. A composition according to claim 3, which comprises any one of the following combinations of therapeutic agents: (i) salmeterol, ciclesonide and tiotropium bromide; (ii) formoterol, budesonide and ipratropium, } (iii) formoterol, ciclesonide and tiotropium bromide; (iv) formoterol, budesonide and oxitropium; (v) salbutamol sulphate, beclomethasone and ipratropium;(vi) salbutamol sulphate, budesonide and tiotropium bromide; (vii) terbutaline sulphate, fluticasone and tiotropium bromide; (viii) terbutaline sulphate, fluticasone and ipratropium bromide; (ix) salbutamol sulphate, budesonide and ipratropium bromide; . (x) salmeterol, fluticasone propionate and ipratropium bromide; (xi) salmeterol, budesonide and ipratropium bromide; (xii) salmeterol, fluticasone propionate and tiotropium bromide; and (xiii) formoterol, budesonide and tiotropium bromide.
- 5. A composition according to claim 3 or 4, wherein the anti-cholinergic of the composition is present in an amount 0.001wt% to 0.5wi% based on the weight of the total composition.
- 6. A composition according to any of claims 3 to 5, wherein the B-2 agonist of the composition is present in an amount 0.001wt% to 0.5wt% based on the weight of the total composition.
- 7. A composition according to any of claims 3 to 6, wherein the steroid of the composition is present in an amount 0.001wt% to 0.5wt% based on the weight of the total composition.
- 8. A composition according to any of claims 3 to 7, in a form suitable for administration by inhalation.
- 9. A composition according to claim 8, in the form of an aerosol.
- 10. A composition according to claim 9, which further comprises a propellant selected from the group consisting of 1,1,1,2-tetrafluoroethane, 1,1,1,2,3,3,3-heptafluoropropane, monofluorotrichloromethane and dichlorodifluoromethane, or any mixture of two or more - x thereof.
- 11. A composition according to claim 9 or 10, further comprising a co-solvent.
- 12. A composition according to claim 11, wherein the co-solvent is ethanol.
- 13. A composition according to any of claims 9 to 12, further comprising a surface-active . agent.
- 14. A composition according to claim 13, wherein the surface-active agent is oleic acid, lecithin, or sorbitol trioleate.
- 15. A composition according to any of claims 9 to 14, which comprises any one of the following combinations of therapeutic agents: 1) salmeterol, ciclesonide and tiotropium; (1) formoterol, budesonide and ipratropium; (iii) formoterol, ciclesonide and tiotropium; (iv) formoterol, budesonide and oxitropium; wv) salbutamol, beclomethasone and ipratropium; (vi) salbutamol, budesonide and tiotropium; (vii) terbutaline, fluticasone and tiotropium,; (viii) salmeterol, fluticasone and tiotropium; and (ix) formoterol, budesonide and tiotropium; wherein the above therapeutic agents can optionally be present as a pharmaceutically acceptable salt or ester thereof, or in enantiomerically pure form or as a racemic mixture.
- 16. A composition according to claim 15, which comprises any one of the following combinations of therapeutic agents: (A) salmeterol, ciclesonide and tiotropium bromide; (ii) formoterol, budesonide and ipratropium; (iii) formoterol, ciclesonide and tiotropium bromide; (iv) formoterol, budesonide and oxitropium; (v) salbutamol sulphate, beclomethasone and ipratropium; (vi) salbutamol sulphate, budesonide and tiotropium bromide; (vii) terbutaline sulphate, fluticasone and tiotropium bromide;(viii) salmeterol, fluticasone propionate and tiotropium bromide; and (ix) formoterol, budesonide and tiotropium bromide.
- 17. A metered dose inhaler which contains a composition as defined in any of claims 9 to . 16.
- 18. A composition according to claim 8, in the form of an inhalation powder.
- 19. A composition according to claim 18, which comprises lactose as the excipient.
- 20. A composition according to claim 18 or 19, which comprises any one of the following combinations of therapeutic agents: (i) salmeterol, ciclesonide and tiotropium; (i) formoterol, budesonide and ipratropium; (iii) formoterol, ciclesonide and tiotropium; (iv) salbutamol, beclomethasone and ipratropium; wv) salbutamol, budesonide and tiotropium; (vi) terbutaline, fluticasone and tiotropium; (vii) salmeterol, fluticasone and tiotropium; and (viii) formoterol, budesonide and tiotropium; wherein the above therapeutic agents can optionally be present as a pharmaceutically acceptable salt or ester thereof, or in enantiomerically pure form or as a racemic mixture.
- 21. A composition according to claim 20, which comprises any one of the following combinations of therapeutic agents: ® salmeterol, ciclesonide and tiotropium bromide; (i) formoterol, budesonide and ipratropium; (iii) formeoterol, ciclesonide and tiotropium bromide; (iv) salbutamol sulphate, beclomethasone and ipratropium; } (v) salbutamol sulphate, budesonide and tiotropium bromide; (vi) terbutaline sulphate, fluticasone and tiotropium bromide. (vii) salmeterol, fluticasone and tiotropium; and(viii) formoterol, budesonide and tiotropium.
- 22. A dry powder inhaler which contains a composition as defined in any of claims 18 to21.
- 23. A composition according to claim 8, in the form of a propellant free inhalation solution or suspension.
- 24. A composition according to claim 23, which comprises any one of the following combinations of therapeutic agents: 6) terbutaline, fluticasone and ipratropium; (ii) salbutamol, budesonide and ipratropium; (iii) salmeterol, fluticasone and ipratropium, (iv) salmeterol, budesonide and ipratropium; ) salmeterol, fluticasone and tiotropium; and (vi) formoterol, budesonide and tiotropium; wherein the above therapeutic agents can optionally be present as a pharmaceutically acceptable salt or ester thereof, or in enantiomerically pure form or as a racemic mixture.
- 25. A composition according to claim 24, which comprises any one of the following combinations of therapeutic agents: 6) terbutaline sulphate, fluticasone and ipratropium bromide; (ii) salbutamol sulphate, budesonide and ipratropium bromide; (iii) salmeterol, fluticasone propionate and ipratropium bromide; (iv) salmeterol, budesonide and ipratropium bromide; (v) salmeterol, fluticasone propionate and tiotropium bromide; and (vi) formoterol, budesonide and tiotropium bromide.
- 26. A composition according to any of claims 23 to 25, in a form suitable for use with a . nebuliser.
- 27. Use of any one of the following combinations in the manufacture of a medicament for the prophylaxis or treatment of conditions for which administration of one or more of the therapeutic agents is indicated: 6) salmeterol, ciclesonide and tiotropium; (ii) formoterol, budesonide and ipratropium; : (ii) formoterol, ciclesonide and tiotropium; (iv) formoterol, budesonide and oxitropium; Ww) salbutamol, beclomethasone and ipratropium; (vi) salbutamol, budesonide and tiotropium; (vii) terbutaline, fluticasone and tiotropium; (viii) terbutaline, fluticasone and ipratropium; (ix) salbutamol, budesonide and ipratropium; (x) salmeterol, fluticasone and ipratropium; (xi) salmeterol, budesonide and ipratropium; (xii) salmeterol, fluticasone and tiotropium; and (xiii) formoterol, budesonide and tiotropium,; wherein the above therapeutic agents can optionally be present as a pharmaceutically acceptable salt or ester thereof, or in enantiomerically pure form or as a racemic mixture.
- 28. Use according to claim 27, which comprises any one of the following: (i) salmeterol, ciclesonide and tiotropium bromide; (ii) formoterol, budesonide and ipratropium; (iii) formoterol, ciclesonide and tiotropium bromide; (iv) formoterol, budesonide and oxitropium; (v) salbutamol sulphate, beclomethasone and ipratropium; (vi) salbutamol sulphate, budesonide and tiotropium bromide; (vii) terbutaline sulphate, fluticasone and tiotropium bromide; (viii) terbutaline sulphate, fluticasone and ipratropium bromide; (ix) salbutamol sulphate, budesonide and ipratropium bromide; (x) salmeterol, fluticasone propionate and ipratropium bromide; - (xi) salmeterol, budesonide and ipratropium bromide; (xii) salmeterol, fluticasone propionate and tiotropium bromide; and (xiii) formoterol, budesonide and tiotropium bromide.
- 29. Use according to claim 27 or 28, for the manufacture of a medicament for the treatment of inflammatory or respiratory tract diseases, by simultaneous or successive . administration.
- 30. Use according to claim 29, for the manufacture of a medicament for the treatment of asthma and/or chronic obstructive pulmonary disease (COPD), by simultaneous or successive administration.
- 31. A method for the prophylaxis or treatment of inflammatory or respiratory tract diseases, said method comprising administering either sequentially or simultaneously, to a patient in need thereof, a therapeutically effective amount of any one of the following combinations: @) salmeterol, ciclesonide and tiotropium,; (ii) formoterol, budesonide and ipratropium; (iii) formoterol, ciclesonide and tiotropium,; (iv) formoterol, budesonide and oxitropium; w) salbutamol, beclomethasone and ipratropium, (vi) salbutamol, budesonide and tiotropium; (vii) terbutaline, fluticasone and tiotropium; (viii) terbutaline, fluticasone and ipratropium; (ix) salbutamol, budesonide and ipratropium; (x) salmeterol, fluticasone and ipratropium; (xi) salmeterol, budesonide and ipratropium; (xii) salmeterol, fluticasone and tiotropium; and (xiii) formoterol, budesonide and tiotropium,; wherein the above therapeutic agents can optionally be present as a pharmaceutically acceptable salt or ester thereof, or in enantiomerically pure form or as a racemic mixture.
- 32. A method according to claim 31, which comprises administering either sequentially or simultaneously, to a patient in need thereof, a therapeutically effective amount of any one of the following combinations: (i) salmeterol, ciclesonide and tiotropium bromide; (ii) formoterol, budesonide and ipratropium; (iii) formoterol, ciclesonide and tiotropium bromide; . (iv) formoterol, budesonide and oxitropium; (v) salbutamol sulphate, beclomethasone and ipratropium; (vi) salbutamol sulphate, budesonide and tiotropium bromide; (vii) terbutaline sulphate, fluticasone and tiotropium bromide; (viii) terbutaline sulphate, fluticasone and ipratropium bromide; (ix) salbutamol sulphate, budesonide and ipratropium bromide; (x) salmeterol, fluticasone propionate and ipratropium bromide; (xi) salmeterol, budesonide and ipratropium bromide; (xii) salmeterol, fluticasone propionate and tiotropium bromide; and : (xiii) formoterol, budesonide and tiotropium bromide.
- 33. A method according fo claim 31 or 32, for the treatment of asthma and / or chronic obstructive pulmonary disease (COPD), by simultaneous or successive administration.
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| GB0220095A GB0220095D0 (en) | 2002-08-29 | 2002-08-29 | Pharmaceutical composition |
Publications (1)
| Publication Number | Publication Date |
|---|---|
| ZA200501703B true ZA200501703B (en) | 2005-09-06 |
Family
ID=9943163
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| ZA200501703A ZA200501703B (en) | 2002-08-29 | 2005-02-28 | Pharmaceutical products and compositions comprising specific anticholinergic agents, beta-2-agonists and corti-costeroids. |
Country Status (2)
| Country | Link |
|---|---|
| GB (1) | GB0220095D0 (en) |
| ZA (1) | ZA200501703B (en) |
-
2002
- 2002-08-29 GB GB0220095A patent/GB0220095D0/en not_active Ceased
-
2005
- 2005-02-28 ZA ZA200501703A patent/ZA200501703B/en unknown
Also Published As
| Publication number | Publication date |
|---|---|
| GB0220095D0 (en) | 2002-10-09 |
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