TREA

PHARMACEUTICAL FORMULATIONS

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  • Patent Application
  • 20170202837
  • Publication Number
    20170202837
  • Date Filed
    March 07, 2017
    7 years ago
  • Date Published
    July 20, 2017
    7 years ago
Information
Abstract
This invention relates to solid oral pharmaceutical formulations or(S)-methyl ((4(4-(3-(5-chtoro-2-fluoro-3-(methyl-sutfonamido)phenyl)-1-isopropyl-1H-pyrazol-4-yl)pyrimidin-2-yl)amino)propan-2-yl)carbamate (COMPOUND A) and the use of these formulations for treating proliferative diseases, such as solid tumor diseases.
Description
BACKGROUND

This invention relates to solid oral pharmaceutical formulations of (S)-methyl (1-((4-(3-(5-chloro-2-fluoro-3-(methylsulfonamido)phenyl)-1-isopropyl-111- pyrazol-4-yl)pyritnidin-2-yl)amino)propan-2-yl)carbarnate (COMPOUND A) and the use of these formulations for treating proliferative diseases, such as solid tumor diseases.


The COMPOUND A has the chemical structure:




embedded image


Its preparation and its use as an inhibitor of B-RAF for the treatment of proliferative diseases, such as solid tumor diseases, like melanoma and colorectal cancer, are described in WO 2011/025927, which is here incorporated by reference in its entirety.


COMPOUND A is a BCS class II compound exhibiting poor aqueous solubility at weakly acidic and neutral pH which poses a challenge for oral bioavailability and therapeutic effect. The compound exhibits typical weak base solubility characteristics and is highly soluble at low pH, starts to decline at around pH 3.0 and remains low at intrinsic solubility level over the range of neutral pH. Upon emptying from the stomach, COMPOUND A has the tendency to quickly precipitate out of solution due to an abrupt solubility drop in intestinal pH. This significantly reduces COMPOUND A that is available for intestinal absorption, The present invention relates to orally bioavailable pharmaceutical solid dispersion formulations of COMPOUND A.





BRIEF DESCRIPTION OF THE FIGURES


FIG. 1 represents the 2 stage dissolution profile of the formulation described in Example 1.



FIG. 2 represents the 2-Stage (pH 2 first 60 min to 6.8 after 60 min) dissolution of the formulations described in Examples 2-7.



FIG. 3 represents the dissolution profile of the tablet formulation described in Example 8.





DETAILED DESCRIPTION OF THE INVENTION

COMPOUND A is a BCS class II compound which exhibits typical weak base solubility characteristics: higher solubility at low pH, and limited solubility around neutral pH. Therapeutic compounds with such solubility characteristics typically present pharmaceutical formulation scientists with a challenge while attempting to prepare oral formulations capable of improving oral bioavailability of the therapeutic compound. Such challenges in preparing solid oral dosage forms of COMPOUND A are overcome, according to the present invention, by formulating the compound as a solid dispersion.


Solid dispersions are specialized pharmaceutical formulations. The most suitable solid dispersion formulation is the one that enhances solubility and dissolution rate and maintains the stability of the drug substance in an amorphous state. In a typical solid dispersion formulation the drug substance is uniformly dispersed in a solid matrix which promotes dissolution of the drug in the gastrointestinal tract and maintains the drug in a high energy amorphous state.


Pharmaceutical solid dispersions are produced by techniques known in the art, for example, solvent evaporation, kneading and melt extrustion.


According to the present invention, an inner phase is prepared, The inner phase is a solid dispersion comprising COMPOUND A in a Suitable polymer matrix, which is composed, for example, of a hydrophilic binder, a surfactant and optional additional excipients, which are known in the art, followed by milling to reduce particle size.


Prior to tableting or encapsulation, the inner phase is preferably combined with additional excipients, which are collectively referred to herein as the external phase. One or more of an acidifier, a filler, a disintegrant, a flow enhancer and a lubricant are typically included in the external phase.


Thus, the present invention relates to a solid oral pharmaceutical formulation which comprises a solid dispersion comprising COMPOUND A.


In one embodiment, the present invention s a solid oral pharmaceutical formulation which comprises:

    • (a) an inner phase which is a solid dispersion comprising COMPOUND A, and
    • (b) an external phase which comprises additional excipients.


Preferably, the internal phase, or, more preferably, the external phase comprises an acidifier.


The present invention further relates to a solid oral pharmaceutical formulation which comprises:

    • (a) an inner phase which is a solid dispersion comprising COMPOUND A, a hydrophilic binder and a surfactant; and
    • (b) an external phase which comprises additional excipients.


In another embodiment, the present invention is a solid oral pharmaceutical formulation which comprises:

    • (a) an inner phase which is a solid dispersion comprising COMPOUND A, a hydrophilic binder, a surfactant and
    • (b) an external phase which comprises one or more of an acidifier, a filler, a disintegrant, a flow enhancer and a lubricant.


The hydrophilic binder should he suitable for complete miscibility with COMPOUND A and upon formulation dissolution, serve as a precipitation inhibitor of COMPOUND A. Suitable hydrophilic binders for inclusion in the inner phase include copovidone, hydroxypropylmethylcellulose, polyvinylpyrrolidone, hydroxypropylcellulose, and methacrylate copolymer, polyethylene oxide, HPMC acetate succinate, HPIvIC phthalate. Copovidone is especially useful as the hydrophilic binder. KOLLIDON VA64, which is a copolymer of 1-vinyl-2-pyrrolidone and vinyl acetate in a ratio of 6:4 by mass and is available from BASF, is highly suitable for use as a hydrophilic binder in the inner phase.


The surfactant should be suitable for use in melt extrusion to enhance dissolution and solubilization of COMPOUND A. In some cases, the surfactant may help reduce the process temperature through its plasticizing effect. Suitable surfactants for inclusion in the inner phase include poloxamers, such as Poloxamer 188, sodium lauryl sulphate, Tween 80, sorbitol, polysorbate 20, polysorbate 80, Vitamin E TPGS, and polyethylene glycol.


Additional excipients that may optionally be included in the inner phase include acidifiers, and plasticizers.


In the preferred embodiments, the internal phase, or preferably the external phase comprises an acidifier to control the microenvironmental pH in the acidic range. Suitable acidifiers include organic acids such as citric acid, succinic acid, maleic acid, tartaric acid, malic acid and adipic acid.


Suitable fillers, disintegrants, flow enhancers and lubricants are known to those of skill in the art.


Especially useful fillers include lactose, maltodextrin, mannitol, microcrystalline cellulose, pregelatinized starch, and sucrose esters.


Useful disintegrants include crospovidone, croscarmellose sodium, sodium starch glycolate, microcrystalline cellulose, and pregelatinized starch.


Useful flow enhancers include colloidal silicon dioxide, talc, magnesium stearate, and mannitol.


Useful lubricants include magnesium stearate, calcium stearate, glyceryl monostearate, hydrogenated castor oil, sodium laurel sulfate, sodium stearyl fumarate, stearic acid, zinc stearate, talc, microcrystalline cellulose, and sucrose esters.


In different embodiments of the present invention, the inner phase comprises various ranges of % w/w of active agent, hydrophilic binder and surfactant. For instance, the present inner phase can comprise 5-70% Compound A, 10-90% of hydrophilic binder, and 5-30% surfactant, preferably 5-50% Compound A, 30-80% of hydrophilic binder, and 5-30% surfactant, more preferably 5-40% Compound A, 50-80% of hydrophilic binder, and 5-20% surfactant.


In different embodiments of the present invention, the external phase comprises various ranges of % w/w of acidifier, filler, disintegrant, flow enhancer and lubricant. For instance, the present external phase can comprise 1-70% acidifier, 20-70% filler, 0-30% disintegrant, 0-10% flow enhancer and 0-10% lubricant, preferably 2-60% acidifier, 30-70% filler, 5-20% disintegrant, 0.5-5% flow enhancer and 0.5-5% lubricant, more preferably 10-40% acidifier, 20-40% tiller, 1-15% disintegrant, 1-5% flow enhancer and 1-5% lubricant.


In different embodiments of the present invention, the solid oral dosage form, for example, capsules or tablets, are a blend of the internal and external phases in a ratio of from 100:0 to 30:70, preferably 80:20 to 40:60, most preferably 75:25 to 50:50.


Stabilization of an amorphous form of COMPOUND A in a solid dispersion formulation enhances bioavailability, attributable to a higher dissolution rate and kinetic solubility of the amorphous form in comparison to its crystalline form.


When COMPOUND A stays in amorphous form, an increase in kinetic solubility and dissolution rate as well as in oral bioavailability is achieved using the solid dispersion formulation.


In one embodiment, the present invention is formulated as a capsule, such as hard gelatin capsule or a soft elastic capsule. Alternatively, the present invention is in the form of a tablet or a pill. In these solid oral formulations the. amount of COMPOUND A can be present in the ranges of 1-1500 mg, 2.5-800 mg, or 5-400 mg, with preferred examples including 10 mg, 20 mg, 25 mg, 50 mg , 100 mg, 200 mg, 400 mg and 500 mg.


The solid oral formulations of the present invention can he administered to treat diseases which respond to inhibition of B-RAF, particularly diseases that are characterzed by a mutation in B-RAF, particularly melanoma and colorectal cancer.


Thus, the present invention further relates to the use of a solid oral pharmaceutical formulation described above for the preparation of a medicament for the treatment of a proliferative disease, especially wherein the proliferative disease is a solid tumor disease characterized by a mutation in B-RAF, such as melanoma or colorectal cancer.


The present invention thither relates to a method of treating a proliferative disease which comprises administering to a patient in need of treatment a therapeutically effective amount of a formulation described herein, especially wherein the proliferative disease is a solid tumor disease characterized by a mutation in B-RAF, such as melanoma or colorectal cancer.


The following Examples are intended to illustrate, but not to limit, the invention.


EXAMPLE 1

The following composition is prepared at constant drug loading of 15% and formulated into 10, 25, 50 mg and 100 mg capsules.
















Ingredient
% w/w



















Internal




Compound A
15



Kollidon VA64
45



Pluronic F 68
5



External



Succinic acid
13



Cellulose MKGR
16



Crosspovidone
5



Mg Stearate
0.5



Aerosil
0.5



Total
100

























10 mg
25 mg
50 mg
100 mg


Ingredient
capsule
capsule
capsule
capsule















Internal Phase (mg)











Compound A
10.0
25.0
50.0
100.0


Kollidon VA64
29.9
74.8
150.0
300.0


Poloxamer 188
3.3
8.4
16.7
33.3


(Pluronic F68)







External Phase (mg)











Succinic acid
8.7
21.7
43.3
86.7


Cellulose
10.7
26.7
53.3
106.7


microctystalline


Crospovidone
13
8.4
16.7
33.3


Aerosil
0.3
0.9
1.7
3.3


Magnesium Stearate
0.3
0.9
1.7
3.3


Total (mg)
66.6
166.5
333.4
666.6









Manufacturing Process:

The processing is performed by hot-melt extrusion using a 18 mm twin-screw Leistriez extruder, followed by milling the extrudates, blending with the external phase and screening. Following blending, the blend is encapsulated into pink hard gelatin capsules of size 0 and 00 for drug doses of 50 and 100 mg respectively. A step-by step approach is shown below:

    • Weigh the required amount of Compound A, Kollidor VA64 and Poloxamer 188
    • Blend the mixture
    • Extrude the blend on a 18 mm Leistreiz twin-screw extruder at a feed rate of 1 kg/hour maintaining temperatures of 50 to 160 ° C. in the extruder.
    • Mill the extrudate
    • Add screened succinic acid and cellulose microcrystalline
    • Add and blend the milled extrudates, succinic acid and cellulose microcrystalline
    • Add crospovidone and aerosil
    • Blend the mixture
    • Add prescreen magnesium stearate
    • Blend the mixture
    • Encapsulation using FMK encapsulator


In-vivo monkey PK data with the resulting capsules show bioavailability suitable for oral administration with a mean Cmax of 11833 ng/ml, Tmax at 4 hours and an AUC of 32686 ng*hr/ml.


XRPD data indicate physical stability of the amorphous solid dispersion formulation (no indication of conversion to the crystalline drug substance) upon storage at accelerated stability conditions of 40° C/75% RE for 4 weeks.


In-vitro 2-stage dissolution studies indicate no change in dissolution kinetics of the solid dispersion between initial (0 week) and 4-week time point at accelerated stability storage conditions indicating no change in physical stability of the solid dispersion.


The present formulation exhibits a glass transition temperature (Te) of 97° C. which is above the recommended drug product storage temperature of no greater than 30° C., demonstrating physical stability without conversion of the amorphous drug substance into the poorly water soluble crystalline drug substance.


The present formulation shows excellent chemical stability upon. storage at accelerated stability conditions at 40° C./75% RH with no evidence of any degradation products and 100% assay content results for COMPOUND A.


EXAMPLE 2

The following formulation is prepared in a manner similar to that described in Example 1.
















Ingredient
% w/w



















Internal




LGX818
17



PVP-K30
51



Sorbitol
5



External



Succinic Acid
9



Cellulose MKGR
12



Crosspovidone
5



Mg Stearate
0.5



Aerosil
0.5



Total
100










This formulation exhibits a glass transition temperature (Tg) of 109° C. demonstrating physical stability without conversion of the amorphous drug substance into the poorly water soluble crystalline drug substance.


EXAMPLE 3

The following table described the results of a pharmacokinetic study in monkeys of Compound A formulated as a mieroemulsion dosed at 50 mg/kg and the formulations of Example I (Solid Dispersion 1) and Example 2 (Solid Dispersion 2) at a dose of 200 mg of Compound A.


EXAMPLES 2-7

The following formulations are prepared by tehniques similar to those described in Example 1, but with a single phase. The dissolution profiles of the formulations are reported in FIG. 2.


Formulation 2:
















Ingredients
% W/W



















Compound A
25.00



Vitamin E TPGS
41.67



Polyethylene glycol
26.33



4000



Hydroxypropylmethyl
5.00



cellulose



Talc
2.00










Formulation 3:
















Ingredients
% W/W



















Compound A
25.00



Vitamin E TPGS
41.67



Polyethylene glycol
16.33



4000



Hydroxypropylmethyl
15.00



cellulose



Talc
2.00










Formulation 4:
















Ingredients
% W/W



















Compound A
25.00



Vitamin E TPGS
41.67



Polyethylene glycol
5.92



4000



Hydroxypropylmethyl
15.00



cellulose



Maleic acid
5.41



Eudragit L100-55
5.00



Talc
2.00










Formulation 5:
















Ingredients
% W/W



















Compound A
25.00



Vitamin E TPGS
41.67



Polyethylene glycol
5.92



4000



Hydroxypropylmethyl
5.00



cellulose



Maleic acid
5.41



Eudragit L100-55
15.00



Talc
2.00










Formulation 6:
















Ingredients
% W/W



















Compound A
24.00



Vitamin E TPGS
40.00



Hydroxypropylmethyl
14.40



cellulose



Maleic acid
5.20



Eudragit L100-55
14.40



Talc
2.00










Formulation 7:
















Ingredients
% W/W



















Compound A
24.00



Vitamin E TPGS
40.00



Polyethylene glycol
1.20



4000



Hydroxypropylmethyl
14.40



cellulose



Lactic acid
4.00



Eudragit L100-55
14.40



Talc
2.00










EXAMPLE 8

The following formulation is prepared by tehniques similar to those described in Example 1, but in a tablet dosage form. The dissolution profile of the formulation in 0.1N HCl medium is reported in FIG. 3.


Formulation 8:
















Ingredient
% w/w



















Internal




Compound A
10.0



Kollidon VA64
30.1



Pluronic F 68
3.4



External



Kollidon VA64
3.0



Cellulose MKGR
37.5



Crosspovidone
15.0



Mg Stearate
1.0



Total
100









Claims
  • 1. (canceled)
  • 2. A method for treating colorectal cancer, the method comprising administering to a patient in need of treatment a therapeutically effective amount of a solid oral pharmaceutical formulation, wherein the formulation comprises: an inner phase which is a solid dispersion comprising amorphous (S)-methyl (1-((4-(3 -(5 -chloro-2-fluoro-3 -(methyl sul fonami do)phenyl)-1-i sopropyl-1H-pyrazol-4-yl)pyrimidin-2-yl)amino)propan-2-yl)carbamate (COMPOUND A); copovidone; and poloxamer 188 or sorbitol; andan external phase which comprises succinic acid, microcrystalline cellulose, crospovidone, colloidal silicon dioxide, and magnesium stearate.
  • 3. The method of claim 2, wherein the colorectal cancer is characterized by a mutation in B-RAF.
  • 4. The method of claim 2, wherein the inner phase comprises from 5% to 40% by weight of amorphous (S)-methyl (1-((4-(3-(5-chloro-2-fluoro-3-(methyl sulfonamido)phenyl)-1-isopropyl-1H-pyrazol-4-yl)pyrimidin-2-yl)amino)propan-2-yl)carbamate (Compound A), from 50% to 80% by weight of copovidone, and from 5% to 20% by weight of poloxamer 188 or sorbitol.
  • 5. The method of claim 2, wherein the external phase comprises from 2% to 60% by weight of succinic acid, from 30% to 70% by weight of microcrystalline cellulose, from 5% to 20% by weight of crospovidone, from 0.5% to 5% by weight of colloidal silicon dioxide, and from 0.5% to 5% by weight of magnesium stearate.
  • 6. The method of claim 2, comprising a blend of the internal and external phases in a ratio of from 80:20 to 40:60.
  • 7. The method of claim 6, comprising a blend of the internal and external phases in a ratio of from 75:25 to 50:50.
  • 8. The method of claim 2, wherein the formulation comprises 10 mg, 25 mg, 50 mg, or 100 mg of amorphous (S)-methyl (1-((4-(3-(5-chloro-2-fluoro-3-(methyl sulfonamido)phenyl)-1-isopropyl-1H-pyrazol-4-yl)pyrimidin-2-yl)amino)propan-2-yl)carbamate (Compound A).
  • 9. The method of claim 8, wherein the formulation comprises 50 mg of amorphous (S)-methyl (1-((4-(3-(5-chloro-2-fluoro-3-(methylsulfonamido)phenyl)-1-isopropyl-1H-pyrazol-4-yl)pyrimidin-2-yl)amino)propan-2- yl)carbamate (Compound A).
  • 10. The method of claim 8, wherein the formulation comprises 15% by weight of amorphous (S)-methyl (1-((4-(3-(5-chloro-2-fluoro-3-(methylsulfonamido)phenyl)-1-isopropyl-1H-pyrazol-4-yl)pyrimidin-2-yl)amino)propan-2- yl)carbamate (Compound A).
  • 11. The method of claim 2, wherein the formulation is selected from the group consisting of:
  • 12. The method of claim 11, wherein the colorectal cancer is characterized by a mutation in B-RAF.
  • 13. The method of claim 2, wherein the formulation is
  • 14. The method of claim 13, wherein the colorectal cancer is characterized by a mutation in B-RAF.
  • 15. The method of claim 2, wherein the formulation is selected from the group consisting of:
  • 16. The method of claim 15, wherein the colorectal cancer is characterized by a mutation in B-RAF.
  • 17. The method of claim 2, wherein the formulation is:
  • 18. The method of claim 15, wherein the colorectal cancer is characterized by a mutation in B-RAF.
  • 19. The method of claim 2, wherein the formulation is formulated as a capsule or a tablet.
  • 20. The method of claim 11, wherein the formulation is formulated as a capsule or a tablet.
  • 21. The method of claim 13, wherein the formulation is formulated as a capsule or a tablet.
  • 22. The method of claim 15, wherein the formulation is formulated as a capsule or a tablet.
  • 23. The method of claim 17, wherein the formulation is formulated as a capsule or a tablet.
Provisional Applications (1)
Number Date Country
61563229 Nov 2011 US
Continuations (2)
Number Date Country
Parent 15179190 Jun 2016 US
Child 15452239 US
Parent 14359121 May 2014 US
Child 15179190 US