Classifications

• • A—HUMAN NECESSITIES
  • A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
  • A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
  • A61K9/00—Medicinal preparations characterised by special physical form
  • A61K9/0012—Galenical forms characterised by the site of application
  • A61K9/007—Pulmonary tract; Aromatherapy
  • A61K9/0073—Sprays or powders for inhalation; Aerolised or nebulised preparations generated by other means than thermal energy
  • A61K9/0075—Sprays or powders for inhalation; Aerolised or nebulised preparations generated by other means than thermal energy for inhalation via a dry powder inhaler [DPI], e.g. comprising micronized drug mixed with lactose carrier particles
• • A—HUMAN NECESSITIES
  • A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
  • A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
  • A61K31/00—Medicinal preparations containing organic active ingredients
  • A61K31/13—Amines
  • A61K31/135—Amines having aromatic rings, e.g. ketamine, nortriptyline
• • A—HUMAN NECESSITIES
  • A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
  • A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
  • A61P25/00—Drugs for disorders of the nervous system
  • A61P25/24—Antidepressants

Definitions

• the present invention relates to a composition comprising ketamine, in particular dry powder formulation for use in a method of treatment of depression by pulmonary administration.
• Prior art Depression especially major depressive disorder, bipolar disorder and treatment- resistant depression (TRD) is a serious problem in a modern society.
• Many treatment options have been developed for treating depression, including monotherapy or combination therapy in a convenient for patients oral administration regimen.
• monotherapy or combination therapy in a convenient for patients oral administration regimen.
• at present the only real choice in such severe cases can be electroshocks.
• Ketamine is a known anesthetic and analgetic, used for anesthesia and in the treatment of chronic pain.
• Ketamine is a chiral compound and can exist as a racemate and as S-enantiomer (known as esketamine) or R-enantiomer (known as arketamine).
• Ketamine can form a pharmaceutically acceptable salts and in pharmaceutical applications is generally used as preferred hydrochloride salt.
• the optical rotation of an enantiomer varies between ketamine and its salts. For example, while esketamine free base is d extra rotatory S-(+), esketamine hydrochloride is levorotatory S-(-).
• Treatment-resistant depression is a term used in clinical psychiatry to describe cases of major depressive disorder that do not respond adequately to appropriate courses of at least two antidepressants in a suitable dose for a suitable time.
• ketamine and esketamine Data collected up to now show exceptional properties of ketamine and esketamine.
• the effect is very quick (after 2-3 hours from administration) and relatively long- lasting - a few days after single dose of a medicament.
• the rapidity of the clinical effect is surprisingly high and unexpected, since the effect of antidepressants present on the market appears after at least two weeks, even three to four weeks of day-to-day administration. Therefore, ketamine or esketamine could be used as a drug of first choice in patients with major depression with enhanced suicide risk that are resistant to existing oral antidepressants.
• the scale of the effect is also very high; about 2/3 of the patients with treatment-resistant depression is responsive to ketamine treatment.
• Literature describes many examples of ketamine pharmacokinetics depending on the administration route.
• Administration route with currently expected minimum level of metabolites is an intravenous one.
• the parent drug After intravenous infusion of racemic ketamine at 0.5 mg/kg for 40 minutes, the parent drug maintains its systemic concentration about 200 ng/ml for about 40 minutes, afterwards the concentration falls down quickly with a half- period below 2 hours.
• norketamine reaches its maximum concentration at the level of 10-20% of ketamine concentration.
• the percentage of area-under-curve (AUC) norketamine to ketamine is about 20-40%.
• Oral administration is the administration route, after which maximum concentration of metabolites is expected. However, after oral administration the drug rapidly undergoes metabolism to norketamine. Norketamine level is equal to 500-1000% of ketamine level. Area-under-curve (AUC) for norketamine is even higher, exceeding 1000%.
• AUC Area-under-curve
• US2007/0287753A1 discloses the use of ketamine for treating treatment-resistant or refractory depression.
• the only formulation tested is the intravenous infusion, and transdermal administration is contemplated as well.
• Intranasal administration is only generally described, including intranasal administration of a dry powder aerosol formulation comprising finely divided powder of ketamine, a dispersant and bulking agent.
• ketamine to oropharyngeal area significant amounts of ketamine will be swallowed by a patient by oral route and can undergo systemic metabolism to norketamine to cause undesired side effects.
• DE102007009888 discloses the use of S-ketamine in the treatment of depression, in the dosage of 0.3 to 1.0 mg/kg.
• WO2013/138322 discloses the use of esketamine in the treatment of treatment- refractory or treatment-resistant depression. Test for efficacy of esketamine was described in prophetic example with esketamine intravenous infusion.
• WO2014/143646 and WO2014/152196 disclose pharmaceutical composition of esketamine in the form of the aqueous formulation of esketamine hydrochloride, preferably for nasal administration, for use in the treatment of treatment-refractory or treatment-resistant depression.
• Mucoadhesive oral forms of esketamine and pharmacokinetics of esketamine after oral, intranasal and intravenous administration are described in WO2014/020155.
• ketamine formulation that is both highly effective as well as convenient and easy to everyday self-administration by the patient including self- administration on out-patient basis to ensure high patient compliance.
• a formulation should first of all deliver therapeutic ketamine dose to the blood, should be characterized with high effectiveness, including rapid therapeutic effect and low risk of undesired effects, such as DP, due to precise dosing.
• Such a formulation should allow only a minimum level of systemic first-pass metabolites such as norketamine and hydroxylated metabolites, especially assure acceptable (es)ketamine to (es)norketamine ratio, both in view of avoiding reduction of ketamine level actually administered and unwanted metabolites effects.
• the target was to achieve similar ketamine plasma concentration and hence similar antidepressant effect as that by Sing et al. with intravenous infusion of 0.20 mg/kg lasting 40 minutes using route of administration more convenient for a patient and producing less adverse effects.
• the invention provides a dry powder pharmaceutical composition comprising ketamine or a pharmaceutically acceptable salt thereof as a medicine for use in a method of treatment of depression by pulmonary administration.
• the invention provides ketamine or its pharmaceutically acceptable salt for use in a method of treatment of depression, wherein ketamine or its pharmaceutically acceptable salt is administered by pulmonary route as a dry powder pharmaceutical formulation.
• the invention provides a method of treatment depression in a subject in need thereof, wherein ketamine or its pharmaceutically acceptable salt is administered to a subject by pulmonary route as a dry powder pharmaceutical formulation.
• Figure 1 presents NGI deposition data for the composition of Example 1 ;
• Figure 2 presents NGI deposition data for the composition of Example 2;
• Figure 3 presents NGI deposition data for the composition of Example 3.
• Figure 4 presents NGI deposition data for the composition of Example 4.
• Figure 5 presents NGI deposition data for the composition of Example 5
• Figure 6 presents NGI deposition data for the composition of Example 6
• Figure 7 shows esketamine plasma concentration vs time after administration of various single doses of dry powder composition of Example 2;
• Figure 8 shows esketamine plasma concentration vs time after administration of a sequence of single doses of dry powder composition of Example 2; and Figure 9 presents adverse effect distribution after administration of dry powder composition of Example 2.
• the object of the invention is a dry powder pharmaceutical composition comprising ketamine or its pharmaceutically acceptable salt as a medicine for use in a method of treatment of depression by pulmonary administration, i.e. administration via pulmonary route.
• Another object of the invention is ketamine or its pharmaceutically acceptable salt for use in a method of treatment of depression, wherein ketamine or its pharmaceutically acceptable salt is administered by pulmonary route as a dry powder pharmaceutical formulation.
• Another object of the invention is a method of treatment of depression in a subject in thereof, wherein ketamine or its pharmaceutically acceptable salt is administered to a subject by pulmonary route as a dry powder pharmaceutical formulation.
• esketamine especially esketamine hydrochloride
• a dry powder esketamine composition or formulation in a sequence of administrations consisting of multiple single doses (inhalation events), such as at least 3 single doses, each inhalation event consisting of multiple puffs, such as 1 , 2, 3 or 4 puffs, preferably in 3 or 4 puffs, said sequences being separated from each other by a break period without any inhalation (rest period).
• such as sequence lasts at least 30 minutes, for example lasts 30 minutes, and includes 3 sequences of administration and break periods between are preferably equal, i.e. are 15 minutes break (rest) period.
• esketamine is self-administered pulmonary by a patient by inhalation of a dry powder esketamine composition or formulation in a sequence lasting 30 minutes consisting of 3 single doses (inhalation events), each inhalation event consisting of 3 or 4 puffs, wherein each puff corresponds to esketamine nominal dose of 4 mg in the dry powder composition or formulation.
• a dry powder esketamine composition or formulation in a sequence lasting 30 minutes consisting of 3 single doses (inhalation events), each inhalation event consisting of 3 or 4 puffs, wherein each puff corresponds to esketamine nominal dose of 4 mg in the dry powder composition or formulation.
• Such a composition or formulation is described in Example 2 below.
• a break period without any inhalation preferably there are two equal breaks lasting about 15 minutes, i.e.
• first single dose is administered at time 0
• second single dose is administered after about 15 minutes
• the third single dose is administered at 30 minute.
• Such a sequence allows to obtain plasma concentration profile that provides plasma concentration infusion at the level having antidepressant effect, as known from prior art tests of intravenous infusions.
• ketamine encompasses racemic ketamine and its enantiomers esketamine and arketamine, both as a free base and pharmaceutically acceptable salts thereof.
• ketamine is esketamine. In another embodiment, ketamine is racemic ketamine.
• Preferred pharmaceutically acceptable ketamine salt is hydrochloride.
• the composition of the invention comprises esketamine hydrochloride.
• the composition of the invention comprises racemic ketamine hydrochloride.
• ketamine especially esketamine such as esketamine hydrochloride, is self-administered pulmonary by a patient by inhalation of a dry powder ketamine composition or formulation in a sequence of administrations consisting of multiple single doses (inhalation events), such as at least 3 single doses, each single dose or inhalation event consisting of multiple puffs, such as 1 , 2, 3 or 4 puffs, preferably in 3 or 4 puffs, said sequences being separated from each other by a break period without any inhalation (rest period).
• such as sequence lasts at least 30 minutes, for example lasts 30 minutes, and includes 3 sequences of administration and break periods between are preferably equal, i.e. are 15 minutes break (rest) period.
• esketamine such as esketamine hydrochloride
• a dry powder esketamine composition or formulation in a sequence lasting 30 minutes consisting of 3 single doses (inhalation events), each inhalation event consisting of 3 or 4 puffs, wherein each puff corresponds to esketamine nominal dose of 4 mg in the dry powder composition or formulation.
• a composition or formulation is described in Example 2 below.
• first single dose is administered at time 0
• second single dose is administered after about 15 minutes
• the third single dose is administered at 30 minute.
• Such a sequence allows to obtain plasma concentration profile that provides plasma concentration infusion at the level having antidepressant effect, as known from prior art tests of intravenous infusions.
• treatment-resistant or treatment refractory depression is well known in the art and means depression in patients not responding to at least two prior attempts of adequate antidepressive treatment using commonly known antidepressant therapies.
• the term is generally described for example in US8, 785, 500 and US2015/0056308.
• bipolar disorder is well known in the art and means a disorder that causes periods of depression and periods of abnormally elevated mood.
• major depression is well known in the art and means a disorder characterized by at least two weeks of low mood that is present across most situations.
• composition of the invention comprises from 2 mg to 100 mg of ketamine calculated as a free base per nominal unit dose.
• the composition of the invention comprises from 2 mg to 60 mg of ketamine, especially 2 mg to 40 mg of ketamine, such as from 3 mg to 15 mg of ketamine, calculated as a free base, per nominal unit dose.
• the composition of the invention comprises further one or more additives selected from the group consisting of a carbohydrate bulking agent in the amount of 30 to 95% by weight and a stabilizing agent in the amount of 0.2 - 3% by weight, with respect to the total weight of the composition.
• the composition comprises ketamine, especially esketamine hydrochloride, having median particle diameter d50 of 1 - 10 pm, such as 1 - 8 pm, especially 3 pm, d10 of 0.2 - 5 pm and d90 of 3 - 35 pm.
• Median particle size dso is a parameter obtained by laser diffraction technique with dry dispersion using Sympatec HELOS laser diffractometer attached with ASPIROS feeder.
• raw ketamine especially esketamine hydrochloride, is dispersed with pressure 3.0 bar in total amount of 30 mg per sample.
• composition is a dry powder formulation for administration using dry powder inhalers. Conventional and typical dry powder inhalers can be used for this purpose.
• dry powder is known for a skilled person and should be understood in a manner conventional in the art as a solid mix of particles that is fluidized when the patient inhales after actuation of the inhaler device.
• nominal unit dose in accordance with the invention relates to the ketamine dose as present (loaded) in the composition that is destined for a single administration.
• the nominal unit dose can be a measured dose of the dry powder to be ready for the patient to take, contained in a single unit, such as a capsule or single compartment in a blister, or a dose to be taken from for delivery from the multi-dose dry powder reservoir.
• the term“emitted dose” relates to the proportion of the nominal unit dose that exits/leaves the device after inhalation by a patient.
• the dry powder pharmaceutical composition or formulation for use according to the invention may comprise further pharmaceutical excipients., i.e. one or more additives selected from the group consisting of a carbohydrate bulking agent (a carrier) in the amount of 30 to 95% by weight and a stabilizing agent in the amount of 0.2 - 3% by weight, with respect to the total weight of the composition.
• a carbohydrate bulking agent a carrier
• a stabilizing agent in the amount of 0.2 - 3% by weight
• Suitable carbohydrate bulking agent can be lactose, D-mannitol, glucose monohydrate, trehalose, especially trehalose dihydrate, erythritol, dextrose, maltose, sorbitol or xylitol.
• Especially convenient bulking agent is milled lactose, such as lactose monohydrate or anhydrous lactose, especially lactose monohydrate, having suitable granulometry.
• Suitable granulometry is defined as having dso 30 - 200 pm (Sympatec HELOS) as the main coarse fraction (especially 80 pm).
• lactose monohydrate commercial grades are Lactohale 200 (LH200), Lactohale 100 (LH100) and Lactohale 200LP.
• LH200 Lactohale 200
• LH100 Lactohale 100
• Lactohale 200LP Lactohale 200LP
• lactose grade most suitable for performance thereof. Such a selection is within common skills of a skilled person.
• Typical amount of the bulking agent in the composition of the invention is 30 - 95% by weight, especially 30 to 80% by weight, with respect to the total weight of the composition.
• Pharmaceutical excipients/additives include also a stabilizer (also called force control agent - FCA), i.e. a substance that reduces adhesion and cohesion.
• Suitable stabilizers are for example magnesium stearate, lecithin, and aminoacids, such as leucine.
• Especially preferred stabilizer is magnesium stearate.
• Stabilizer“disturbs” the weak binding forces between the small particles and thus helps to keep the particles separated, reduces self-adhesion of small particles and also adherence to other particles in the formulation if such other particles are present, reduces the adhesion to the inner surfaces of the inhaler, as well as improves rheological properties of powder - powder flowability.
• the amount of the stabilizer in the composition of the invention is 0.2 - 3% by weight, especially 0.8% by weight, with respect to the total weight of the composition.
• Composition or formulation for use according to the invention is prepared by blending in a high-shear mixer a bulking agent/carrier of suitable granulometry with a stabilizer, and then adding ketamine, especially esketamine hydrochloride, of suitable granulometry and again blending in a high-shear mixer.
• ketamine especially esketamine hydrochloride, of suitable granulometry is co-processed (blended) with a stabilizer in a high-shear mixer, and then the bulking agent/carrier is added and again mixed in a high-shear mixer.
• composition is a dry powder formulation for administration using dry powder inhalers. Conventional and typical dry powder inhalers can be used for this purpose.
• the formulation may be administered by three device categories: single-unit dose inhaler in which each dose, such as in a capsule, is loaded into the device before use; a multi-dose reservoir inhaler in which a bulk supply of dry powder with plurality of doses is preloaded into the device; and a multi-unit dose inhaler in which a plurality of single doses are individually sealed in separate compartments such as in a blister cavity, and discharged each time the device is actuated.
• Preferred is the multi-unit dose inhaler in which a plurality of single doses are individually sealed, such as in the blister, and discharged each time the device is actuated.
• the medicine for administration via pulmonary route is a blister with plurality of individual nominal unit doses premetered and individually sealed.
• One preferred example of such an inhaler is Diskus type inhaler.
• the medicine for administration via pulmonary route is a capsule with a single nominal unit dose.
• the medicine for administration of a single dose via pulmonary route is a multi-dose powder reservoir.
• composition for use according to the invention provides emitted dose of at least 1.0 mg of ketamine calculated as a free base, corresponding to 1.2 mg of ketamine hydrochloride.
• the composition for use according to the invention provides the fraction of the dose delivered locally directly to the lungs that is at least 40%, such as from 40 to 50%, especially 40% to 60%, especially up to 85%, of the emitted unit dose.
• Emitted dose is the portion of nominal unit dose that is emitted from the inhaler device and leaves the inhaler device as an aerosol and hence is available to the patient.
• the uniform and stable high-dose ketamine, especially esketamine hydrochloride dry powder composition can be obtained that when administered by pulmonary route provides therapeutic ketamine level in the circulating blood of a patient, i.e. at least 50 to 100 ng/ml, such as 70 to 100 ng/ml, such as 70-80 ng/ml, such as about 100 ng/ml.
• Therapeutic ketamine level relates to the level in the blood that is effective in the treatment of depression, especially major depressive disorder, such as treatment resistant or treatment-refractory depression, and may be dependent on the subject, gender, age, severity of the disease, the type of the inhaler, and may vary depending on whether ketamine is racemic ketamine or enantiomeric ketamine.
• the fraction of the emitted dose delivered to the lungs is surprisingly high, in contrast with typical inhalation compositions wherein the standard is that only 15 to 20% of the emitted dose is delivered to the lungs.
• the fraction of the emitted dose delivered locally directly to the lungs can be determined using well-known and conventional methods and assays. Such methods and assays include any of those described in European Pharmacopeia 9.0, Chapter 2.9.18, Preparations for inhalation; Aerodynamic assessment of fine particles for determination of Fine Particle Dose.
• the Next Generation Pharmaceutical Impactor (NGI) (Ph. Eur. Apparatus E) can be used to assess and control the aerodynamic particle size distribution (APSD).
• NGI apparatus is as presented in Figs 2.9.18.-12 and 2.9.18.-13 on page 333 of European Pharmacopeia 9.0.
• Emitted dose and fine particle dose and fraction are strongly dependent on two factors i.e. on the formulation and on the device.
• the resistance of a dry powder inhaler is an intrinsic value which depends on the design of the inhalation channel, the metering cup and the air inlets. DPIs can be classified into four resistance groups (low, medium, medium-high, high) with respect to the inhalation flow required to produce a pressure drop of 4 kPa. This value was chosen because it is the one recommended by pharmacopoeia for the in vitro characterization of the dose emitted from a DPI. Additionally for capsule-based DPIs can be limited by the powder retention in the capsule and device, which lead to reduction in the emitted dose.
• Emitted dose testing is relatively straightforward.
• the device is ‘fired’ into a sampling apparatus that enables the capture of the measured dose on a filter.
• the aerodynamic particle size distribution of inhaled products is measured using the technique of multistage cascade impaction, here Next Generation Impactor (NGI).
• NKI Next Generation Impactor
• the collected quantity of active ingredient is determined further by FIPLC analysis.
• the inhalers are tested at a predetermined flow rate, and the pressure drop across the inhaler is 4.0 kPa in line with the Ph Eur.
• Efficient particle capture is ensured by coating the particle collection surface of each of stages 1 -7, as well as the MOC and the pre-separator base, with a coating substance.
• the central cup of the pre-separator is filled with adequate diluent.
• Stages 1 to 7 and MOC Each stage is washed with appropriate diluent (extraction of drug substance).
• NGI tray loaded with the cups on a Copley Gentle Rocker is gently shaken for 10 minutes.
• Mouthpiece adapter Deposited inhalation powder on adapter is rinsed with appropriate diluent a volumetric flask and sonicated for 10 minutes.
• Induction port Deposited inhalation powder from induction port is rinsed with appropriate diluent into a volumetric flask and sonicated for 10 minutes.
• Preseparator Deposited inhalation powder from these component is rinsed with appropriate diluent into a volumetric flask and sonicated for 10 minutes. Finally collected samples from each stage of impactor are filtered analyzed by high-performance liquid chromatography
• Composition of for use according to the invention has an appropriate ketamine, in particular esketamine hydrochloride pharmacokinetics profile that enables achievement of approximately 50 to 100 ng/ml of the ketamine plasma concentration over 40 minutes after pulmonary administration directly to the lungs by inhalation. Said plasma concentration corresponds to antidepressive effect. Maintaining this concentration over time mimics 40-minute intravenous infusion known to be effective in depression and well-tolerated.
• a sum of lactose monohydrate and magnesium stearate are sieved through 0.25 mm mesh and mixed in high-shear mixer for 3 minutes. Obtained mixture is sieved with active substance through 0.5 mm mesh and mixed in high-shear mixer for 5 minutes. To eliminate electrostatic charges, antistatic PE bags are used during the process.
• Vacuum-drum technology dose forming process is used for blister filling.
• the blister cavity is in volume range of 15 to 45 mm 3 (especially ca. 30 mm 3 ).
• Powder which is filled into cavity is in amount of 10 - 30 mg (especially 23 mg).
• vacuum-drum device During process parameters of vacuum-drum device are:
• Vacuum pressure -0 - 500 mBar, especially 50 - 400 mBar
• Fluidization time 50 - 2000 ms, especially 50 -300 ms
• Capsules to be filled are placed in the sockets closed ends down. Powder is discharged from the dosator and comes directly to the capsules. The powder with which the capsules are to be filled is placed in the dosator, may be tamped and discharged into the capsules.
• capsule filling device During the process parameters of capsule filling device are:
• compositions has been prepared in accordance with the above general procedure in the scale of 0.9 kg.
• Esketamine hydrochloride 3.45 (corresponds to 2.99 mg esketamine)
• Esketamine hydrochloride 4.61 (corresponds to 4 mg esketamine) Lactose monohydrate LH200 LP 18.20
• Esketamine hydrochloride 5.06 (corresponds to 4.39 mg esketamine) Lactose monohydrate LH200 LP 17.581
• Aerodynamic Particle Size Distribution test of the compositions of the Examples 1 , 2 and 3 of the invention.
• the compositions of Examples 1 , 2 and 3 of the invention have been tested using the Next Generation Pharmaceutical Impactor (NGI) (Ph. Eur. Apparatus E) in accordance with the procedure for powder inhalers.
• NMI Next Generation Pharmaceutical Impactor
• ISM - Impactor sized mass mass entering the impactor excluding non-sizing portions
• MMAD (pm) mass median aerodynamic diameter. Defined as the diameter at which 50% of the particles by mass are larger and 50% are smaller.
• the obtained results showed a product with expected quality attributes.
• composition of the invention demonstrated appropriate homogeneity and a very high level of fine particle fractions, with:
• compositions has been prepared in accordance with the above general procedure in the scale of 0.9 kg.
• Esketamine hydrochloride 5.00 (corresponds to 4.34 mg esketamine) Lactose monohydrate LH200 LP 19.8
• the obtained results showed a product with expected quality attributes.
• the invented formulation demonstrated appropriate homogeneity and a very high level of fine particle fractions, with:
• the dry powder pharmaceutical composition of the invention provided emitted esketamine hydrochloride dose at the level up to 97%, such as up to 85% of the nominal dose and at least 40% of fine particle fraction (fraction delivered to the lungs) for emitted esketamine dose.
• Example 7
• Esketamine hydrochloride dry powder formulation of Example 2 was administered to healthy volunteers pulmonary, i.e. directly to the lungs using dry powder inhaler (DPI) (by self-administration).
• DPI dry powder inhaler
• One puff of dry powder formulation contained 4.6 mg of esketamine hydrochloride, corresponding to 4 mg of esketamine free base and excipients 18.22 mg of lactose monohydrate and 0.18 mg of magnesium stearate.
• a single dose was an inhalation events consisting of 1 to 6 puffs, i.e. 4 to 24 mg of esketamine free base nominal dose.
• part A of the study designed as a one-centre single ascending dose, the medicine was delivered in a single dose once daily (up to 6 consecutive puffs) to 18 healthy volunteer subjects. Subjects were divided into 6 cohorts, cohorts receiving 1 , 2, 3, 4, 5 or 6 puffs in a single doses (inhalation events), respectively. Collection of blood samples for determination of esketamine and esnorketamine concentration and calculation of pharmacokinetic parameters was performed for up 24 hours following the start of the test.
• the aim of the study was to determine the amount of puffs needed to obtain plasma concentration similar to that sufficient to achieve antidepressant effect as for 0.20 mg/kg 40 minutes intravenous infusion. It can be predicted on the basis of literature data that this corresponds to concentration at 40 min of infusion between about 60 to 100 ng/ml. It was also the aim to determine the number of puffs that allow to avoid a sharp peak of plasma concentration that is considered an important factor inducing adverse psychomimetic and dissociative effects.
• Example 2 a single dose (inhalation event) consisting of 1 to 4 puffs was selected for the next Part B of the test.
• the composition of Example 2 was administered to 12 healthy volunteer subjects divided into 4 cohorts in four different single doses each cohort (i.e. each single dose consisting of 1 , 2, 3 or 4 puffs, respectively) in one day in the administration sequence consisting of three administrations of single dose (inhalation event) in the period of 30 minutes, Between inhalation events there were 15 minutes break periods, i.e. first single dose was administered at 0 min., second single dose was administered at 15 min, and third single dose was administered at 30 min.
• Part B The aim of Part B was to investigate pharmacokinetic properties of esketamine following different dosing schemes in healthy subjects and determine the scheme that enables achievement of the appropriate plasma concentration over time to mimic the 40-minute intravenous infusion (part B),
• Figure 8 shows esketamine plasma concentration over time after administration of various single doses of dry powder composition of Example 2 in a sequence of 3 administrations of single doses during 30 minutes.
• Figure 8 shows also (the area between two bold black lines) a simulation of esketamine plasma concentration after 0.2 mg/kg 40 minutes i.v. infusion.
• sequence of administration of 3 single doses consisting of 3 or 4 puffs allowed to obtain plasma concentration profile mimicking quite well esketamine intravenous infusion at the level corresponding to antidepressant effect.
• Plasma concentration profile is quite smooth, consistent with a target profile and safe for chronic administration.

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