Inhalant formulation containing sulfoalkyl ether cyclodextrin and corticosteroid

a technology of sulfoalkyl ether and corticosteroid, which is applied in the directions of aerosol delivery, application, and immunologic disorders, can solve the problems of inconvenient preparation of medication, reduced portability, and increased cost, so as to reduce the rate of degradation of corticosteroid, increase the output rate and/or the extent of nebulized corticosteroid, and reduce the amount of time

Inactive Publication Date: 2007-01-25
CYDEX PHARMACEUTICALS INC
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Benefits of technology

[0084] The invention provides a method of stabilizing corticosteroid in an aqueous corticosteroid-containing formulation comprising the step of adding SAE-CD to an aqueous corticosteroid-containing suspension or solution formulation in an amount sufficient to reduce the rate of degradation of corticosteroid as compared to a control sample excluding SAE-CD.
[0085] The invention also provides a method of improving the administration of an inhalable aqueous corticosteroid-containing suspension unit dose formulation by nebulization, the method comprising the step of adding SAE-CD to an aqueous corticosteroid-containing suspension unit dose formulation in an amount sufficient to solubilize the corticosteroid to form an inhalable aqueous corticosteroid-containing solution unit dose formulation, the improvement comprising increasing the output rate and/or extent of nebulized corticosteroid.
[0086] The invention provides a method

Problems solved by technology

The main concerns about nebulizers, however, are their increased cost, reduced portability and the inconvenience of needing to prepare medication beforehand and the increased time requirement for administering a treatment.
They conclude that 2%-18% of the nebulizer's charge of budesonide was delivered from the suspension, meaning that budesonide delivery was incomplete resulting in a significant waste of drug.
However, it is well known that using current methods and formulations the greater part of an inhaled corticosteroid dose is swallowed and becomes available for oral absorption, resulting in unwanted systemic effects.
Since this oral component of corticosteroid drug delivery does not provide any beneficial therapeutic effect but can increase systemic side effects, it is desirable for the oral bioavailability of inhaled corticosteroid to be relatively low.
Due to a particular formulation employed, some corticosteroids are more likely to be deposited in the mouth and throat and may cause local adverse effects.
In contrast, particles that are larger than 5 mcm can be deposited in the mouth and throat, both reducing the proportion of particles that reach the lungs and potentially causing local adverse effects such as oral candidiasis and hoarseness (dysphonia).
A further disadvantage to the nebulization of budesonide suspensions is the need to generate very small droplets, MMAD of about <3 μm.
Generation of such particles is difficult.
The inhalation of drug particles as opposed to dissolved drug is known to be disadvantageous.
(Arch. Dis. Child (1986), 61, 1108-1110) suggest that nebulization of corticosteroid (in particular beclomethasone) solutions may be preferred over that of suspensions because the latter may be inefficient if the nebulized particles are too large to enter the lung in therapeutically effective amounts.
However, cosolvents, such as ethanol, polyethylene glycol and propylene glycol are only tolerated in low amounts when administered by inhalation due to irritation of the respiratory tract.
There are limits to acceptable levels of these cosolvents in inhaled products.
In addition, most potential hydrophobic therapeutic agents are not sufficiently soluble in these cosolvent mixtures.
None of the above-identified formulations has provided a method of improving the administration of a suspension-based unit dose formulation containing a cortico steroid.
When cyclodextrin formulations are administered by injection into the blood strea

Method used

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  • Inhalant formulation containing sulfoalkyl ether cyclodextrin and corticosteroid
  • Inhalant formulation containing sulfoalkyl ether cyclodextrin and corticosteroid
  • Inhalant formulation containing sulfoalkyl ether cyclodextrin and corticosteroid

Examples

Experimental program
Comparison scheme
Effect test

example 1

[0269] Exemplary formulations according to the invention were made according to the following general procedures.

Method A

[0270] Cyclodextrin is dissolved in water (or buffer) to form a solution containing a known concentration of cyclodextrin. This solution is mixed with an active agent in solid, suspension, gel, liquid, paste, powder or other form while mixing, optionally while heating to form an inhalable solution.

Method B

[0271] A known amount of substantially dry cyclodextrin is mixed with a known amount of substantially dry active agent. A liquid is added to the mixture to form a suspension, gel, solution, syrup or paste while mixing, optionally while heating and optionally in the presence of one or more other excipients, to form an inhalable solution.

Method C

[0272] A known amount of substantially dry cyclodextrin is added to a suspension, gel, solution, syrup or paste comprising a known amount of active agent while mixing, optionally while heating and optionally in the pr...

example 2

[0282] The MMD of nebulized solutions containing SBE7-β-CD and budesonide was determined as follows.

[0283] Placebo solutions of three different cyclodextrins were prepared at different concentrations. Two ml of the solutions were added to the cup of a Pari LC Plus nebulizer supplied with air from a Pari Proneb Ultra compressor. The particle size of the emitted droplets was determined using a Malvern Mastersizer S laser light scattering instrument.

example 3

[0284] The stability of liquid formulations containing SAE-CD was determined by HPLC chromatography of aliquots periodically drawn from the liquid in storage.

[0285] Citrate-phosphate (Mcllvaines) buffer solutions at a pH of 4, 5, 6, 7, or 8 were prepared by mixing various portions of 0.01M citric acid with 0.02 M Na2HPO4. These stock solutions contained 5% w / w Captisol. Approximately 250 μg / mL of budesonide was dissolved in each buffer solution. Aliquots of the solutions were stored at 40° C., 50° C. and 60° C. Control samples were stored at 5° C. but are not reported here. HPLC analysis of the samples was performed initially and after 1, 2, and 3 months storage.

[0286] The HPLC conditions included:

Instrument:PE Series 200Column:Phenomenex Luna C18(2) 4.6 × 150 mm 3 umMobile Phase:58% Phosphate Buffer pH 3.4 / 39.5%ACN / 2.5% MeOHMobile Phase Program:100% A (isocratic)Wavelength240Flow Rate:0.6 mL / minStandard Range:Seven standards - 1 to 500 μg / mL

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Abstract

An inhalable formulation containing SAE-CD and corticosteroid is provided. The formulation is adapted for administration to a subject by nebulization with any known nebulizer. The formulation can be included in a kit. The formulation is administered as an aqueous solution, however, it can be stored as a dry powder, ready-to-use solution, or concentrated composition. The formulation is employed in an improved nebulization system for administering corticosteroid by inhalation. SAE-CD present in the formulation significantly enhances the chemical stability of budesonide. A method of administering the formulation by inhalation is provided. The formulation can also be administered by conventional nasal delivery apparatus.

Description

CROSS-REFERENCE TO EARLIER FILED APPLICATIONS [0001] The present application is a continuation-in-part of and claims the priority of PCT International Application No. PCT / US05 / 00082 filed Dec. 31, 2004 and provisional application No. 60 / 533,628 filed Dec. 31, 2003, the disclosures of which are hereby incorporated by reference in their entirety.FIELD OF THE INVENTION [0002] The present invention relates to a method of administering, and a formulation for administering, sulfoalkyl ether cyclodextrin and a corticosteroid, such as budesonide, by inhalation. The invention also relates to methods of treating diseases and disorders of the lung. BACKGROUND OF THE INVENTION [0003] The delivery of a drug by inhalation allows deposition of the drug in different sections of the respiratory tract, e.g., throat, trachea, bronchi and alveoli. Generally, the smaller the particle size, the longer the particle will remain suspended in air and the farther down the respiratory tract the drug can be del...

Claims

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Application Information

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IPC IPC(8): A61K31/724A61K31/573
CPCA61K9/0078B82Y5/00A61K31/724A61K45/06A61K47/40A61K31/573C08L5/16C08B37/0015A61K47/48969A61K31/58A61K47/48092A61K2300/00A61K47/6951A61P11/00A61P11/02A61P11/06A61P27/02A61P27/14A61P27/16A61P37/08A61P43/00A61K47/61A61K47/6851A61K9/0073A61K9/08
Inventor PIPKIN, JAMES D.ZIMMERER, RUPERT O.THOMPSON, DIANE O.MOSHER, GEROLD L.
Owner CYDEX PHARMACEUTICALS INC
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