Patent Grant
11071835
This application is the National Stage of International Application No. PCT/EP2014/075058, filed Nov. 19, 2014, which claims the benefit of Great Britain application number 1321717.9, filed Dec. 9, 2013, the disclosures of which are incorporated herein by reference in their entireties.
The present invention relates to inhalable medicaments, and particularly to inhalable β2-agonists, like formoterol.
Inhalable β2adrenoceptor agonists (often abbreviated to “β2-agonists”) are widely used to treat respiratory diseases and particularly asthma and COPD. They are typically divided into short-acting β2-agonists (SABAs) and long-acting β2-agonists (LABAs). Examples of SABAs include salbutamol, levosalbutamol, terbutaline, pirbuterol, procaterol, clenbuterol, metaproterenol, fenoterol, bitolterol, ritodrine and isoprenaline. Examples of LABAs include formoterol, salmeterol, bambuterol, indacaterol and carmoterol. Many are used as pharmaceutically acceptable salts. An example of particular interest is formoterol fumarate.
Inhalable β2-agonists are typically administered using a dry powder inhaler (DPI), a pressurised metered dose inhaler (pMDI) or a nebuliser. In these approaches, the active ingredient must be in the form of particles which are small enough to be inhaled via the mouth and into the lungs. In many instances, the active ingredients are micronised prior to formulation. This is essential where the active ingredient is not in solution. The particle size of the inhalable β2-agonist is typically in the region of 1-5 microns (mass median aerodynamic diameter).
Inhalable β2-agonists treat respiratory disorders by acting on β2-adrenoceptors in the respiratory tract. However, these receptors are also located, inter alia, in the heart and blood vessels, and administration of β2-agonists is widely documented as leading to adverse cardiac side effects. It is believed that these adverse events occur when the β2-agonists enter the bloodstream. A common mechanism for entry of β2-agonists into the bloodstream is that some of the particles which are too large to be inhaled deposit in the throat and are swallowed by the patient. There is a need in the art for formulations of inhalable β2-agonists which provide the required therapeutic effect whilst minimising cardiac side effects.
This requirement is magnified for combination products. Combination products are well established in the art and are known to improve patient convenience and compliance. One example is the combination of an inhalable β2-agonist and an inhalable corticosteroid, e.g. formoterol fumarate and budesonide. A drawback of combination products are that control over the dose of the individual active ingredients is reduced. For the inhaled corticosteroid, this is not a serious concern because the therapeutic window of inhaled corticosteroids is wide. That is, it is difficult for a patient to exceed the recommended daily intake of inhaled corticosteroid. However, the β2-agonist is more of a concern since the therapeutic window is narrower and β2-agonists, as previously mentioned, are associated with serious adverse effects, including cardiac side-effects.
Accordingly, the present invention provides a dry powder inhaler comprising:
a reservoir containing a dry powder formulation and an arrangement for delivering a metered dose of the medicament from the reservoir;
a cyclone deagglomerator for breaking up agglomerates of the dry powder medicament; and
a delivery passageway for directing an inhalation-induced air flow through a mouthpiece, the delivery passageway extending to the metered dose of medicament,
wherein the formulation comprises an inhalable β2-agonist having a particle size distribution of d10<1 μm, d50=1-3 μm, d90=3.5-6 μm and NLT 99%<10 μm and a lactose carrier.
The combination of this DPI and formulation surprisingly shows a reduced systemic exposure leading to reduced side effects.
The present invention will now be described with reference to the drawings, in which:
The present invention is based on a DPI providing active metering and a cyclone deagglomerator combined with a β2-agonist formulation which has a narrowly defined particle size distribution. The d90 value in particular is closely controlled to provide a coarser than usual powder and it has been surprisingly found that such a powder reduces systemic exposure to the β2-agonist and hence minimises cardiac side effects.
The inhalable β2-agonist is preferably selected form salbutamol, levosalbutamol, terbutaline, pirbuterol, procaterol, clenbuterol, metaproterenol, fenoterol, bitolterol, ritodrine, isoprenaline, formoterol, salmeterol, bambuterol, indacaterol, carmoterol or pharmaceutically acceptable salts thereof. This list includes SABAs and LABAs (defined hereinabove). An example of particular interest is formoterol fumarate, e.g. formoterol fumarate dihydrate.
The inhalable β2-agonist may be prepared by jet milling. The process comprises the steps of providing the β2-agonist in particulate form, jet milling the β2-agonist and collecting the resultant micronised powder.
First, the β2-agonist is provided in particulate form. Particulate forms of β2-agonists are widely used in the milling process. The particles of the β2-agonist are hard enough to be fractured during the milling process. The inhalable β2-agonist in particulate form preferably has a Young's modulus of >0.5 GPa, more preferably >1 GPa, more preferably >5 GPa and most preferably >10 GPa. Young's modulus may be determined by nanoindentation, e.g. using an atomic force microscope (AFM).
The powder is preferably prepared by jet milling. As shown in
The resulting powder is collected and is in a form suitable for inhalation.
The resulting β2-agonist powder has the following particle size distribution d10<1 μm, d50=1-3 μm, d90=3.5-6 μm and NLT 99%<10 μm. Preferably, the β2-agonist powder has the following particle size distribution d10=0.4-0.6, d50=1.5-2.5 and d90=3.6-5.1. Most preferably, it has the following particle size distribution d10=0.46-0.53, d50=1.68-1.92 and d90=3.68-5.07. These particle size distributions most preferably apply to the β2-agonist, formoterol fumarate.
The particle size of the β2-agonist powder may be measured by laser diffraction as a dry dispersion, e.g. in air, such as with a Sympatec HELOS/BF equipped with a RODOS disperser.
The formulation of the present invention is administered using a DPI. The carrier is lactose. The lactose carrier preferably has a particle size distribution of d10=20-65 μm, d50=80-120 μm, d90=130-180 μm and <10 μm=<10%. Preferably, the particle size distribution of the lactose is d10=20-65 μm, d50=80-120 μm, d90=130-180 μm and <10 μm=<6%. The lactose is preferably lactose monohydrate (α-lactose monohydrate) and may be prepared by standard techniques, e.g. sieving. The particle size distribution of the lactose may be measured by laser diffraction as a dry dispersion, using the technique described hereinabove.
The formulation may further comprise one or more additional inhalable active ingredients, preferably a corticosteroid, e.g. budesonide, beclomethasone dipropionate or fluticasone. A particularly preferred combination is formoterol fumarate and budesonide.
It is preferable that substantially all of the particles of the corticosteroid are less than 10 μm in size. This is to ensure that the particles are effectively entrained in the air stream and deposited in the lower lung, which is the site of action. Preferably, the particle size distribution of the corticosteroid is d10<1 μm, d50=<5 μm, d90=<10 μm and NLT 99%<10 μm.
The delivered dose of the β2-agonist (the “labelled” quantity, i.e. the amount actually delivered to the patient) will depend on the nature of the β2-agonist. By way of example, the delivered dose of formoterol fumarate, as base, is preferably 1-20 μg per actuation, with specific examples being 4.5 and 9 μg per actuation. The doses are based on the amount formoterol present (i.e. the amount is calculated without including contribution to the mass of the counterion). The delivered dose of budesonide is preferably 50-500 μg per actuation, with specific examples being 80, 160 and 320 μg per actuation. Particularly preferred delivered doses of budesonide/formoterol in μg are 80/4.5, 160/4.5 and 320/9.
The delivered dose of the active agent is measured as per the USP <601>, using the following method. A vacuum pump (MSP HCP-5) is connected to a regulator (Copley TPK 2000), which is used for adjusting the required drop pressure P1 in a DUSA sampling tube (Dosage Unit Sampling Apparatus, Copley). The inhaler is inserted into a mouthpiece adaptor, ensuring an airtight seal. P1 is adjusted to a pressure drop of 4.0 KPa (3.95-4.04 KPa) for the purposes of sample testing. After actuation of the inhaler, the DUSA is removed and the filter paper pushed inside with the help of a transfer pipette. Using a known amount of solvent (acetonitrile:methanol:water (40:40:20)), the mouthpiece adaptor is rinsed into the DUSA. The DUSA is shaken to dissolve fully the sample. A portion of the sample solution is transferred into a 5 mL syringe fitted with Acrodisc PSF 0.45 μm filter. The first few drops from the filter are discarded and the filtered solution is transferred into a UPLC vial. A standard UPLC technique is then used to determine the amount of active agent delivered into the DUSA. The delivered doses of the inhaler are collected at the beginning, middle and end of inhaler life, typically on three different days.
The present invention also provides a dry powder inhaler comprising the formulation as defined herein. Several types of DPI are known in the art. In a preferred embodiment of the present invention, the dry powder inhaler comprises the following features.
The preferred inhaler comprises a reservoir containing a dry powder medicament and an arrangement for delivering a metered dose of the medicament from the reservoir; a cyclone deagglomerator for breaking up agglomerates of the dry powder medicament; and a delivery passageway for directing an inhalation-induced air flow through a mouthpiece, the delivery passageway extending to the metered dose of medicament.
In a preferred form, the deagglomerator comprises:
an inner wall defining a swirl chamber extending along an axis from a first end to a second end;
a dry powder supply port in the first end of the swirl chamber for providing fluid communication between the delivery passageway of the inhaler and the first end of the swirl chamber;
at least one inlet port in the inner wall of the swirl chamber adjacent to the first end of the swirl chamber providing fluid communication between a region exterior to the deagglomerator and the first end of the swirl chamber;
an outlet port providing fluid communication between the second and of the swirl chamber and a region exterior to the deagglomerator; and
vanes at the first end of the swirl chamber extending at least in part radially outwardly from the axis of the chamber, each of the vanes having an oblique surface facing at least in part in a direction transverse to the axis; whereby a breath-induced low pressure at the outlet port causes air flows into the swirl chamber through the dry powder supply port and the inlet port.
In a further preferred embodiment, the reservoir is a sealed reservoir including a dispensing port, and the inhaler further comprises
a channel communicating with the dispensing port and including a pressure relief port;
a conduit providing fluid communication between an interior of the sealed reservoir and the pressure relief port of the channel; and
a cup assembly movably received in the channel and including, a recess adapted to receive medicament when aligned with the dispensing port, a first sealing surface adapted to seal the dispensing port when the recess is unaligned with the dispensing port, and a second sealing surface adapted to sealing the pressure relief port when the recess is aligned with the dispensing port and unseal the pressure relief port when the recess is unaligned with the dispensing port.
The dose metering system includes a cup received in the channel, which is movable between the dispenser port and the delivery passageway, a cup spring biasing the cup towards one of the dispenser port and the passageway, and a yoke movable between at least two positions. The yoke includes a ratchet engaging the cup and preventing movement of the cup when the yoke is in one of the positions, and allowing movement of the cup when the yoke is in another of the positions.
The inhaler includes a cyclone deagglomerator for breaking up agglomerates of the active ingredients and carrier. This occurs prior to inhalation of the powder by a patient. The deagglomerator includes an inner wall defining a swirl chamber extending along an axis from a first end to a second end, a dry powder supply port, an inlet port, and an outlet port.
The supply port is in the first and of the swirl chamber for providing fluid communication between a dry powder delivery passageway of the inhaler and the first end of the swirl chamber. The inlet port is in the inner wall of the swirl chamber adjacent to the first end of the swirl chamber and provides fluid communication between a region exterior to the deagglomerator and the swirl chamber. The outlet port provides fluid communication between the second end of the swirl chamber and a region exterior to the deagglomerator.
A breath induced low pressure at the outlet port causes air flows into the swirl chamber through the dry powder supply port and the inlet port. The air flows collide with each other and with the wall of the swirl chamber prior to exiting through the outlet port, such that the active is detached from the carrier (lactose). The deagglomerator further includes vanes at the first end of the swirl chamber for creating additional collisions and impacts of entrained powder.
A first breath-actuated air flow is directed for entraining a dry powder from an inhaler into a first end of a chamber extending longitudinally between the first end and a second end, the first air flow directed in a longitudinal direction.
A second breath-actuated airflow is directed in a substantially transverse direction into the first end of the chamber such that the air flows collide and substantially combine.
Then, a portion of the combined air flows is deflected in a substantially longitudinal direction towards a second end of the chamber, and a remaining portion of the combined air flows is directed in a spiral path towards the second end of the chamber. All the combined air flows and any dry powder entrained therein are then delivered from the second end of the chamber to a patient's mouth.
The deagglomerator ensures that particles of the actives are small enough for adequate penetration of the powder into a bronchial region of a patient's lungs during inhalation by the patient.
The inhaler preferably has a dose counter. The inhaler includes a mouthpiece for patient inhalation, a dose-metering arrangement including a pawl movable along a predetermined path during the metering of a dose of medicament to the mouthpiece by the dose-metering arrangement, and a dose counter.
In a preferred form, the dose counter includes a bobbin, a rotatable spool, and a rolled ribbon received on the bobbin, rotatable about an axis of the bobbin. The ribbon has indicia thereon successively extending between a first end of the ribbon secured to the spool and a second end of the ribbon positioned on the bobbin. The dose counter also includes teeth extending radially outwardly from the spool into the predetermined path of the pawl so that the spool is rotated by the pawl and the ribbon advanced onto the spool during the metering of a dose to the mouthpiece.
The preferred inhaler includes a simple, accurate and consistent mechanical dose metering system that dispenses dry powdered medicament in discrete amounts or doses for patient inhalation, a reservoir pressure system that ensures consistently dispensed doses, and a dose counter indicating the number of doses remaining in the inhaler.
With reference to the drawings, the inhaler 10 generally includes a housing 18, and an assembly 12 received in the housing (see
The internal assembly 12 includes a reservoir 14 for containing dry powered medicament in bulk form, a deagglomerator 10′ that breaks down the medicament between a delivery passageway 34 and the mouthpiece 24, and a spacer 38 connecting the reservoir to the deagglomerator.
The reservoir 14 is generally made up of a collapsible bellows 40 and a hopper 42 having an dispenser port 44 (see
The hopper 42 is for holding the dry powder medicament in bulk form and has an open end 46 closed by the flexible accordion-like bellows 40 in a substantially air-tight manner.
An air filter 48 covers the open end 46 of the hopper 42 and prevents dry powder medicament from leaking from the hopper 42 (see
A base 50 of the hopper 42 is secured to a spacer 38, which is in turn secured to the deagglomerator 10′ (see
The hopper 42, the spacer 38 and the deagglomerator 10′ are connected in a manner that provides an air tight seal between the parts. For this purpose heat or cold sealing, laser welding or ultrasonic welding could be used, for example.
The spacer 38 and the hopper 42 together define the medicament delivery passageway 34, which preferably includes a venturi 36 (see
The deagglomerator 10′ breaks down agglomerates of dry powder medicament before the dry powder leaves the inhaler 10 through the mouthpiece 24.
Referring to
In general, the deagglomerator 10′ includes an inner wall 12′ defining a swirl chamber 14′ extending along an axis A′ from a first and 18′ to a second and 20′. The swirl chamber 14′ includes circular cross-sectional areas arranged transverse to the axis A′, that decrease from the first and 18′ to the second end 20′ of the swirl chamber 14′, such that any air flow traveling from the first end of the swirl chamber to the second end will be constricted and at least in part collide with the inner wall 12′ of the chamber.
Preferably, the cross-sectional areas of the swirl chamber 14′ decrease monotonically. In addition, the inner wall 12′ is preferably convex, i.e., arches inwardly towards the axis A′, as shown best in
As shown in
Referring to
Referring to
As shown in
During use of the deagglomerator 10′ in combination with the inhaler, patient inhalation at the outlet port 32′ causes air flows 1′,2′,3′ to enter through, respectively, the dry powder supply port 22′ and the inlet ports. Although not shown, the air flow 1′ through the supply port 22′ entrains the dry powder into the swirl chamber 14′. The air flow 1′ and entrained dry powder are directed by the supply port 22′ into the chamber in a longitudinal direction, while the air flows 2′,3′ from the inlet ports are directed in a transverse direction, such that the air flows collide and substantial combine.
A portion of the combined air flow 4′ and the entrained dry powder then collide with the oblique surfaces 28′ of the vanes 26′ causing particles and any agglomerates of the dry powder to impact against the oblique surfaces and collide with each other. The geometry of the swirl chamber 14′ causes the combined air flow 4′ and the entrained dry powder to follow a turbulent, spiral path, or vortex, through the chamber. As will be appreciated, the decreasing cross-sections of the swirl chamber 14′ continuously changes the direction and increases the velocity of the spiralling combined air flow 4′ and entrained dry powder. Thus, particles and any agglomerates of the dry powder constantly impact against the wall 12′ of the swirl chamber 14′ and collide with each other, resulting in a mutual grinding or shattering action between the particles and agglomerates. In addition, particles and agglomerates deflected off the oblique surfaces 28′ of the vanes 26′ cause further impacts and collisions.
Upon exiting the swirl chamber 14′, the direction of the combined air flow 4 and the entrained dry powder is again changed to a transverse direction with respect to the axis A′, through the outlet port 32′. The combined air flow 4′ and the entrained dry powder retain a swirl component of the flow, such that the air flow 4′ and the entrained dry powder spirally swirls through the outlet port 32′. The swirling flow causes additional impacts in the outlet port 32′ so as to result in further breaking up of any remaining agglomerates prior to being inhaled by a patient.
As shown in
The base 40′ and the cover 42′ of the deagglomerator are preferably manufactured from a plastic such as polypropylene, acetal or moulded polystyrene, but may be manufactured from metal or another suitable material. Preferably, the cover 42′ includes an anti-static additive, so that dry powder will not cling to the vanes 26′. The base 40′ and the cover 42′ are then connected in a manner that provides an air tight seal between the parts. For this purpose heat or cold sealing, laser welding or ultra-sonic welding could be used, for example.
Although the inhaler 10 is shown with a particular deagglomerator 10′, the inhaler 10 is not limited to use with the deagglomerator shown and can be used with other types of deagglomerators or a simple swirl chamber.
The dose metering system includes a first yoke 66 and a second yoke 68 mounted on the internal assembly 12 within the housing 18, and movable in a linear direction parallel with an axis “A” of the inhaler 10 (see
The first yoke 66 includes an opening 72 that receives and retains a crown 74 of the bellows 40 such that the first yoke 66 pulls and expands the bellows 40 when moved towards the cap 26, i.e., against the actuation spring 69 (see
The dose metering system also includes the two cams 70 mounted on the mouthpiece cover 28 (see
Each cam 70 also includes first, second and third cam surfaces 90,92,94, and the cam followers 78 of the second yoke 68 are biased against the cam surfaces by the actuation spring 69. The cam surfaces 90,92,94 are arranged such the cam followers 78 successively engage the first cam surfaces 90 when the cover 28 is closed, the second cam surfaces 92 when the cover 28 is partially opened, and the third cam surfaces 94 when the cover 28 is fully opened. The first cam surfaces 90 are spaced further from the hinges 82 than the second and the third cam surfaces, while the second cam surfaces 92 are spaced further from the hinges 82 than the third cam surfaces 94. The cams 70, therefore, allow the yokes 66,68 to be moved by the actuation spring 69 parallel with the axis “A” of the inhaler 10 in the first direction (towards the mouthpiece 24) through first, second and third positions as the cover 28 is opened. The cams 70 also push the yokes 66, 68 in a second direction parallel with the axis “A” (against the actuation spring 69 and towards the cap 26 of the housing 18) through the third, the second and the first positions as the cover 28 is closed.
The dose metering system further includes a cup assembly 96 movable between the dispenser port 44 of the reservoir 14 and the delivery passageway 34. The cup assembly 96 includes a medicament cup 98 mounted in a sled 100 slidably received in the slide channel 52 of the spacer 38 below the hopper 42 (see
The dose metering system also includes a ratchet 106 and a push bar 108 on one of the cam followers 78 of the second yoke 68 that engage a boss 110 of the cup sled 100 (see
The reservoir pressure system includes a pressure relief conduit 114 in fluid communication with the interior of the reservoir 14 (see
The medicament cup assembly 96 includes a first sealing surface 118 adapted to seal the dispenser port 44 upon the cup assembly being moved to the delivery passageway 34 (see
The sled 100 includes a second sealing surface 124 adapted to seal the pressure relief port 116 when the recess 102 of the cup 98 is aligned with the dispenser port 44, and an indentation 126 (see
The dose counting system 16 is mounted to the hopper 42 and includes a ribbon 128, having successive numbers or other suitable indicia printed thereon, in alignment with a transparent window 130 provided in the housing 18 (see
The spool 134 is arranged to rotate upon movement of the yokes 66,68 to effect delivery of a dose of medicament from the reservoir 14 into the delivery passageway 34, such that the number on the ribbon 128 is advanced to indicate that another dose has been dispensed by the inhaler 10. The ribbon 128 can be arranged such that the numbers, or other suitable indicia, increase or decrease upon rotation of the spool 134. For example, the ribbon 128 can be arranged such that the numbers, or other suitable indicia, decrease upon rotation of the spool 134 to indicate the number of doses remaining in the inhaler 10.
Alternatively, the ribbon 128 can be arranged such that the numbers, or other suitable indicia, increase upon rotation of the spool 134 to indicate the number of doses dispensed by the inhaler 10.
The indexing spool 134 preferably includes radially extending teeth 136, which are engaged by a pawl 138 extending from one of the cam followers 78 (see
The dose counting system 16 also includes a chassis 140 that secures the dose counting system to the hopper 42 and includes shafts 142,144 for receiving the bobbin 132 and the indexing spool 134. The bobbin shaft 142 is preferably forked and includes radially nubs 146 for creating a resilient resistance to rotation of the bobbin 132 on the shaft 142. A clutch spring 148 is received on the end of the indexing spool 134 and locked to the chassis 140 to allow rotation of the spool 134 in only a single direction (anticlockwise as shown in
Upon the cover 28 being partially opened such that the second cam surfaces 92 of the cams 70 engage the cam followers 78, the actuator spring 69 is allowed to move the yokes 66,68 linearly towards the mouthpiece 24 to the second position and partially collapse the bellows 40 of the medicament reservoir 14. The partially collapsed bellows 40 pressurizes the interior of the reservoir 14 and ensures medicament dispensed from the dispenser port 44 of the reservoir fills the recess 102 of the medicament cup 98 such that a predetermined dose is provided. In the second position, however, the ratchet 106 prevents the cup sled 100 from being moved to the delivery passageway 34, such that the recess 102 of the medicament cup 98 remains aligned with the dispenser port 44 of the reservoir 14 and the pressure relief port 116 of the spacer 38 remains sealed by the second sealing surface 124 of the cup assembly 96.
Upon the cover 28 being fully opened such that the third cam surfaces 94 engage the cam followers 78, the actuator spring 69 is allowed to move the yokes 66,68 further towards the mouthpiece 24 to the third position. When moved to the third position, the ratchet 106 disengages, or falls below the boss 110 of the cup sled 100 and allows the cup sled 100 to be moved by the cup spring 104, such that the filled recess 102 of the cup 98 is position in the venturi 36 of the delivery passageway 34 and the dispenser port 44 of the reservoir 14 is sealed by the first sealing surface 118 of the cup assembly 96. In addition, the pressure relief port 116 is uncovered by the indentation 126 in the side surface of the sled 100 to release pressure from the reservoir 14 and allow the bellows 40 to further collapse and accommodate the movement of the yokes 66,68 to the third position. The inhaler 10 is then ready for inhalation by a patient of the dose of medicament placed in the delivery passageway 34.
As shown in
Once inhalation is completed, the mouthpiece cover 28 can be closed. When the cover 28 is closed, the trigger cams 70 force the yokes 66,68 upwardly such that the first yoke 66 expands the bellows 40, and the pawl 138 of the second yoke 68 advances the indexing spool 134 of the dose counting system 16 to provide a visual indication of a dose having been dispensed. In addition, the cup assembly 96 is forced back to the first position by the pusher bar 108 of the upwardly moving second yoke 68 (see
The present invention also provides the inhaler of any aspect and embodiment of the invention for use in treating a respiratory disease. In particular, the respiratory disease may be asthma or chronic obstructive pulmonary disease (COPD).
In any aspect of the invention, it is envisaged that the asthma may be any severity of asthma, for example the asthma may be mild, mild to moderate, moderate, moderate to severe, or severe asthma. Such asthma may be classified as GINA stage 1, 2, 3 or 4 according to the Global Initiative for Asthma (GINA) guidelines, as would be understood by a person of skill in the art.
The present invention will now be described with reference to the examples, which are not intended to be limiting.
Two samples of formoterol fumarate dihydrate were micronised by jet milling. The two batches were assigned codes 7544MA (conventional milling) and 7544MO (invention). The micronisation conditions are set out in Table 1.
The process for batch 7544MO uses a lower grinding pressure and a higher feed rate than for batch 7544MA. As such, the process for batch 7544MO utilises a lower energy to micronise formoterol than for batch 7544MA. This is the reason that the batches made by the 7544MO process have consistently higher d90 diameter than those of the batches made by the 7544MA process.
The particle sizes of the two batches were measured using a laser light scattering and a dry particle dispersion method, e.g. in air, such as with a Sympatec HELOS/BF equipped with a RODOS disperser and the results are set out in Table 2 and
The particle size distribution of different batches of micronised formoterol, show an average median diameter (d50) of ca. 1.7 mm with a range of 1.6-1.9 mm. The two micronised codes, 7544MA and 7544MO, are not significantly different in fine particle size fraction, below approximately d50. However, the two micronisation codes do show clear differences in terms of their coarse particle fraction; this is clearly seen in
A pharmacokinetic (PK) clinical study was conducted. The PK study assessed a number of key formulation parameters, metered dose (device dose cup volume), formulation blend strength, drug substance particle size and lactose particle size, using a stepwise approach. The PK study was carried out on the middle strength product (160/4.5 μg). Batch A contained formoterol 7544MA and batch B contained formoterol 7544MO. For both batch A and batch B, the inhaler, the budesonide and the lactose were the same.
The key findings of the PK study are highlighted in
| Number | Date | Country | Kind |
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| Publishing Document | Publishing Date | Country | Kind |
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| WO2015/086278 | 6/18/2015 | WO | A |
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