Pregabalin-containing, high swellable, sustained-release triple layer tablet
11007153 · 2021-05-18
Assignee
Inventors
- Kyung Hun Kim (Gyeonggi-do, KR)
- Kyung Soo LEE (Gyeonggi-do, KR)
- Woo Heon Song (Gyeonggi-do, KR)
- Jun Sang Park (Gyeonggi-do, KR)
Cpc classification
A61K31/197
HUMAN NECESSITIES
A61P25/14
HUMAN NECESSITIES
A61K9/0065
HUMAN NECESSITIES
A61K9/209
HUMAN NECESSITIES
A61P9/10
HUMAN NECESSITIES
A61K9/2086
HUMAN NECESSITIES
A61K9/2031
HUMAN NECESSITIES
A61K9/2054
HUMAN NECESSITIES
International classification
A61K31/197
HUMAN NECESSITIES
A61K9/00
HUMAN NECESSITIES
Abstract
Disclosed a pregabalin-containing, high swellable, oral sustained-release triple layer tablet suitable for administration once daily.
Claims
1. A multilayer tablet comprising: an upper layer and a lower layer both comprising pregabalin or a pharmaceutically acceptable salt thereof and a swellable polymer; and an intermediate layer comprising pregabalin and a medium transfer agent, the intermediate layer being positioned between the upper layer and the lower layer, wherein the tablet swells to at least 250% of its original volume at two hours after the tablet is in contact with an aqueous medium and maintains the 250% of its original volume at 6 hours after the tablet is in contact with the aqueous medium, wherein the tablet is an oral sustained-release composition suitable for once daily administration, wherein an amount of pregabalin in the intermediate layer is 6.25% to 40% of a total amount of pregabalin in the multilayer tablet, and wherein an amount of pregabalin in the upper layer is 30% to 46.88% of the total amount of pregabalin in the multilayer tablet.
2. The multilayer tablet according to claim 1, wherein the tablet has the length of the minor axis of the tablet of 12 mm or more at two hours after the tablet is in contact with the aqueous medium.
3. The multilayer tablet according to claim 2, wherein the tablet has the length of the minor axis of the tablet of 12 mm or more for 2 hours to 6 hours after the tablet is in contact with the aqueous medium.
4. The multilayer tablet according to claim 1, wherein the tablet swells to at least 300% of its original volume at two hours after the tablet is in contact with the aqueous medium.
5. The multilayer tablet according to claim 4, wherein the tablet swells to at least 300% of its original volume for 2 to 6 hours after the tablet is in contact with the aqueous medium.
6. The multilayer tablet according to claim 1, wherein the medium transfer agent has an ability of absorbing the aqueous medium and delivering the aqueous medium to the upper layer and the low layer, and wherein the medium transfer agent is (i) an excipient having hydrophilic property or (ii) an excipient having a solubility that at most 10 mL of water is required to dissolve 1 g of the excipient.
Description
BRIEF DESCRIPTION OF DRAWINGS
(1)
(2)
(3)
Best Mode For Embodiment Of Invention
(4) The present invention relates to a sustained-release triple layer tablet containing pregabalin. More specifically, the present invention relates to a triple layer tablet consisting of an upper layer and a lower layer comprising pregabalin or a pharmaceutically acceptable salt thereof and a swellable polymer; and an intermediate layer comprising pregabalin or a pharmaceutically acceptable salt thereof and a medium transfer agent, wherein the triple layer tablet swells to at least 250% of its original volume at two hours after the tablet is contact with an aqueous medium. The triple layer tablet of the present invention consists of an upper layer and a lower layer comprising a swellable polymer, and an intermediate layer positioned therebetween.
(5) According to the present invention, the aqueous medium is effectively delivered to the swellable polymer of the upper layer and the lower layer through the medium transfer agent of the intermediate layer, so that the triple layer tablet swells to at least 250% of its original volume at two hours after the tablet is contact with the aqueous medium, thereby further increasing swellability. The preparation according to the present invention enables a drug to remain in the gastrointestinal tract for more long time. Thereby, the preparation can improve the absorption efficiency of the drug in the upper gastrointestinal tract, and control the drug to be released continuously. As such, the preparation according to the present invention is a gastro-retentive sustained-release preparation, so this preparation is suitable for administration once daily.
(6) The oral sustained-release triple layer tablet according to the present invention may have a therapeutically effective amount of pregabalin per unit dosage form.
(7) The triple layer tablet of the present invention consists of three layers, and specifically, consists of an upper layer and a lower layer comprising a swellable polymer, and an intermediate layer comprising a medium transfer agent therebetween. However, depending on cases, the tablet can be prepared as a multilayer tablets consisting of three or more layers comprising said three layers.
(8) When the triple layer tablet of the present invention is in contact with the aqueous medium, the medium transfer agent present in the intermediate layer introduces the aqueous medium into the tablet, and then delivers the aqueous medium to the swellable polymer present in the upper layer and the lower layer, thereby improving the swellability of the upper layer and the lower layer, so that the tablet swells to at least 250% of its original volume at two hours after the tablet is in contact with the aqueous medium. Such preparation enables a drug to remain in the gastrointestinal tract for more long time, thereby improving the absorption efficiency of the drug in the upper portion of the gastrointestinal tract and controlling the drug to be released continuously, so as to provide an oral sustained-release preparation suitable for administration once daily.
(9) The tablet rapidly swelled by the intermediate layer comprising the medium transfer agent preferably has the size of 12 mm or more, which is the average diameter of the adult pylorus, in order to prevent the tablet from being rapidly released in the stomach. Herein, depending on the shape that can influence when the tablet passes through the pylorus, in the case of round tablets, the size of the tablet refers to a diameter, and in the case of oval or oblong tablets, the size of the tablet refers to a diameter of the minor axis of the tablet.
(10) Although the gastric emptying time of drugs may vary depending on various conditions such as intake of food, etc., it has been known that orally administered formulations generally pass through the stomach in two hours in the fasted state. Thus, the administered formulation should be swelled to be big within two hours, which is difficult to pass through the pylorus and to this end, the volume increase rate within two hours should be at least 250% (that is, swelling to a volume of 2.5 times larger than its original tablet volume), preferably, at least 300% (that is, swelling to a volume of 3 times larger than its original tablet volume). In addition, in order to implement the drug release speed suitable for administration once daily, the volume increase rate up to 6 hours should be at least 250% (that is, swelling to a volume of 2.5 times larger than its original tablet volume), preferably, at least 300% (that is, swelling to a volume of 3 times larger than its original tablet volume), and the volume increase rate up to 6 hours should be preferably equal to or more than the volume increase rate within 2 hours, and should not be reduced than the volume increase rate within 2 hours.
(11) In addition, in the multilayer tablet of the present invention, the length of the minor axis of the tablet at two hours after the tablet is in contact with the aqueous medium is 12 mm or more, and preferably, the length of the minor axis of the tablet for 2 hours to 6 hours after the tablet is in contact with the aqueous medium is at least 12 mm.
(12) In the tablet of the present invention, the upper layer and the lower layer comprise a swellable polymer. Pregabalin, which is an active ingredient, may be comprised in any one of the upper layer and the lower layer or in both of them. The composition or amount of the upper layer and the lower layer may be identical to or different from each other.
(13) The triple layer tablet of the present invention may have various physical forms such as round, oval, oblong, triangle, etc. In consideration of convenience of intake, the smaller size of the prepared tablet is better; however, since the tablet should be rapidly swelled to a size that does not pass through the pylorus after administration of the tablet, after two hours from the swelling test, the diameter of round tablets (or in the case of tablets in different forms, the diameter of the shortest minor axis among the cross sections of the tablets) is preferably 12 mm or more.
(14) The triple layer tablet of the present invention comprises a swellable polymer in the upper layer and the lower layer and a medium transfer agent in the intermediate layer, and pregabalin, which is an active ingredient, may be comprised in all of the upper layer, the intermediate layer and the lower layer, or comprised only in the intermediate layer or in only the upper layer and the lower layer, or in any one of the upper layer and the lower layer depending on cases, in order to exhibit a release speed or a release pattern suitable for administration once daily.
(15) When the triple layer tablet is in contact with the aqueous medium, the medium is penetrated into all of the upper layer, the intermediate layer and the lower layer. The aqueous medium is rapidly penetrated into the center of the tablet through particularly, the medium transfer agent comprised in the intermediate layer, and the aqueous medium penetrated into the intermediate layer of the tablet is rapidly delivered to the upper layer and the lower layer, so that the tablet swells fast to the targeted size. The upper layer and the lower layer rapidly swelled as such swell also to the side of the intermediate layer so that they can be attached to each other. Thus, the size of the tablet swells not only to the up and down longitudinal direction but also to the transverse direction when viewed from the side direction. Through such process, the release speed of pregabalin can be adjusted to be suitable for administration once daily.
(16) In the triple layer tablet of the present invention, the intermediate layer comprises pregabalin and a medium transfer agent. The intermediate layer does not contain a polymer substance, except for a binder used during the granulation preparation process, for rapid delivery of water-solution medium. Thus, the intermediate layer in the triple layer tablet of the present invention is appropriately disintegrated within 30 minutes which are the reference time for general release preparations, in the case of conducting a test only for the intermediate layer, except for the upper layer and the lower layer, according to the disintegration test method among the Korean Pharmacopoeia Disintegration Test Methods.
(17) The medium transfer agent serves, as implied from its name, as providing a route through which water can be rapidly absorbed into the preparation and delivering the absorbed water to the swellable polymer of the upper layer and the lower layer when the triple layer tablet is in contact with gastric fluid after intake or in contact with the aqueous medium during the dissolution test, thereby increasing the swelling speed of the tablet to increase the size of the triple layer tablet.
(18) It was confirmed that the triple layer tablet of the present invention swelled in such manner has greatly increased swelling speed and swelling maintenance time as compared to general single layer tablets comprising a swellable polymer and a medium transfer agent together.
(19) In the present invention, the amount of the medium transfer agent comprised in the intermediate layer of the triple layer tablet is preferably 10% (w/w) to 70% (w/w), more preferably, 10% (w/w) to 50% (w/w), relative to the total amount of the swellable polymer comprised in the upper layer and the lower layer.
(20) As the medium transfer agent of the present invention, substances with good solubility to water or substances which have wicking of inducing penetration of medium even if its solubility is low are used as pharmaceutically acceptable excipients having high affinity with the aqueous medium.
(21) As excipients having good solubility, excipients having solubility defined as “freely soluble” in the Korean Pharmacopoeia Solubility Standard Table (for example, not less than 1 mL and not more than 10 mL of solvent is required to dissolve solute 1 g) are suitable. As such excipients, sugars (for example, dextrose, dextrate, dextrin, lactose, sucrose, glucose, mannitol, isomalt, xylitol, erythritol and sorbitol, etc.), polyvinylpyrrolidone, salts (for example, sodium chloride, magnesium chloride, sodium phosphate, etc.), organic acids (for example, fumaric acids, tartaric acid, etc.) or a mixture thereof can be used
(22) Substances which have wicking of inducing penetration of an aqueous medium have the hydrophilic property even though its solubility to water is low and have roles as absorbing the aqueous medium and inducing such that the aqueous medium can be penetrated continuously. As excipients corresponding thereto, starch (for example, corn starch, potato starch, pre-gelatinized starch, etc.), microcrystalline cellulose, low-substituted hydroxypropylcellulose or a mixture thereof can be used.
(23) The upper layer, the lower layer and the intermediate layer in the triple layer tablet of the present invention each may optionally comprise a pharmaceutically acceptable binder. The binder is contained in the amount of less than 20% (w/w) relative to the weight of each layer in which the binder is comprised. The binder can be used for preparing a granule containing a pharmaceutical active material and a swellable polymer, as needed. As the binders, polyvinylpyrrolidone, copovidone, low-viscosity hypromellose having a viscosity of 100 cps or less in an aqueous solution 2% (w/w) (at 20° C.) or a mixture thereof can be used.
(24) The triple layer tablet of the present invention may optionally comprise one or more lubricants that are required for the preparation process steps including smooth mixing or tableting process in each layer. The lubricants are comprised in the amount of less than 3% (w/w), preferably, in the range of 1% (w/w) to 3% (w/w), relative to the weight of each layer in which the lubricants are comprised. As the lubricants, talc, stearate or metal salt thereof (for example, calcium stearate, magnesium stearate, etc.), stearic esters (for example, polyoxyethylene stearate, glyceryl monostearate, glyceryl palmitostearate, etc.), glyceryl behenate, polyethylene glycol, benzoic acids or a mixture thereof can be used.
(25) The swellable polymer comprised in the upper layer and the lower layer has a swelling property when the tablet is in contact with an aqueous medium.
(26) In order for an oral sustained-release tablet suitable for administration once daily to maintain the effective blood level even after 24 hours from the administration, a portion of the preparation in progress of gelation is needed to remain in the gastrointestinal tract as long as possible for at least 6 to 8 hours, preferably for at least 12 hours, after the administration.
(27) As the swellable polymer comprised in the upper layer and the lower layer in the triple layer tablet of the present invention, polyethylene glycol, hypromellose, hydroxypropylcellulose, carboxymethylcellulose, polyvinyl alcohol, carbomer, etc. can be used.
(28) The swellable polymer can be used alone or a mixture of two or more kinds of the polymers can be used. Or, two or more kinds of polymer mixtures, having properties suitable for the present invention, or copolymers can be properly used for the present invention.
(29) In addition, the swellable polymer that can be used in the preparation of the present invention preferably shows a high viscosity. For example, the viscosity in 2% (w/w) aqueous solution (25° C.) is preferably 400 cps or more, and the viscosity in 1% (w/w) aqueous solution (25° C.) is more preferably 2,000 cps or more.
(30) The upper layer and the lower layer may further comprise pharmaceutically acceptable excipients, for example, diluents or fillers. The amount of the excipients may be in the range of 50% (w/w) or less, preferably, in the range of 40% (w/w) or less, relative to the weight of each layer. The excipients can increase the physical property of the triple layer tablet while providing the fluidity of granule and hardness improvement of the tablet in the mixing and tableting process. Representative examples of the excipients include sugars (for example, dextrose, dextrate, dextrin, lactose, sucrose, glucose, mannitol, isomalt, xylitol, erythritol and sorbitol, etc.), cellulose (for example, crystalline cellulose, microcrystalline cellulose, microcrystalline cellulose silicide, low-substituted hydroxypropylcellulose, etc.), starch (for example, corn starch, potato starch, pre-gelatinized starch, etc.), salts (for example, sodium chloride, calcium carbonate, calcium hydrogen phosphate, calcium phosphate, magnesium carbonate, etc.), organic acids (for example, fumaric acids, tartaric acid, etc.) or a mixture thereof.
(31) Meanwhile, even if the triple layer tablet of the present invention does not comprise binders, diluents or fillers in the upper layer and the lower layer, the swellable polymer of the upper layer and the lower layer can swell by a medium transfer agent of the intermediate layer.
(32) The oral sustained-release triple layer tablet of the present invention that swells to at least 250% of its original volume at two hours after the tablet is in contact with the aqueous medium can be prepared by a method comprising:
(33) (i) a step of preparing a tableting blend for an upper layer and a lower layer consisting of a mixture in which pregabalin or a pharmaceutically acceptable salt thereof and a swellable polymer are mixed, or granules in which they are granulated;
(34) (ii) a step of preparing a tableting blend for an intermediate layer consisting of a mixture in which pregabalin or a pharmaceutically acceptable salt thereof and a medium transfer agent are mixed, or granules in which they are granulated; and
(35) (iii) a step of preparing a triple layer tablet by tableting the blend prepared at the step (i) and the blend prepared at the step (ii).
(36) In the preparation method, the tableting blend prepared at the step (i) may further comprise excipients, binders or lubricants, and the tableting blend prepared at the step (ii) may also further comprise binders or lubricants.
(37) In addition, also at the step (iii), the tableting can be performed by further comprising lubricants.
(38) The tableting blend prepared at the step (iii) is tableted according to typical methods. For example, the triple layer tablet of the present invention can be prepared by mixing the ingredient of each layer of the upper layer, intermediate layer and lower layer respectively using a mixer and then direct-tableting it using a multilayer tableting machine. Or, the triple layer tablet of the present invention can be prepared by mixing the ingredient of each layer to prepare a granule respectively using a high speed mixer, a fluidized-bed granulator or a roller compressor, etc. and adding a lubricant to make it lubricated, and then tableting it using a multilayer tableting machine.
(39) The sustained-release preparation of the present invention can be prepared in a multilayer tablet consisting of three or more layers depending on cases.
EMBODIMENT OF THE INVENTION
EXAMPLES
(40) Hereinafter, the present invention will be explained in more detail through the following examples. However, the following examples are only to exemplify the present invention, and the scope of the present invention is not limited to the following examples.
Examples 1 to 8
(41) According to the component ratio (unit: mg) of the following table, pregabalin and polyethylene oxide (product name: Polyox WSR, Dow Chemicals) as a mixture to be used in the upper layer and the lower layer were mixed and passed through 25 mesh sieve. Thereafter, this mixture was mixed with magnesium stearate that passed through 30 mesh sieve.
(42) In addition, pregabalin and the medium transfer agent as a mixture of the intermediate layer were mixed and passed through 25 mesh sieve. Thereafter, this mixture was mixed with magnesium stearate that passed through 30 mesh sieve.
(43) The amount of each mixtures to be used in the upper layer, the lower layer and the intermediate layer was measured, and the oblong triple layer tablets (Examples 1 to 8) were prepared using a triple layer tableting machine or compressor.
(44) TABLE-US-00001 TABLE 1 Compositions of Examples 1 to 4 (unit: mg) Example 1 Example 2 Example 3 Example 4 Upper layer pregabalin 45 120 60 60 polyethylene oxide 150 250 200 200 (Polyox WSR 303) magnesium 3 5 4 4 stearate Intermediate layer pregabalin 60 60 30 30 lactose 70 dextrate 150 tartaric acid 70 microcrystalline 70 cellulose magnesium 2 3 1 1 stearate Lower layer pregabalin 45 120 60 60 polyethylene oxide 150 250 200 200 (Polyox WSR 303) magnesium 3 5 4 4 stearate Total amount 528 963 629 629
(45) TABLE-US-00002 TABLE 2 Compositions of Examples 5 to 8 (unit: mg) Example 5 Example 6 Example 7 Example 8 Upper layer pregabalin 60 75 60 60 polyethylene oxide 150 300 150 (Polyox WSR 303) polyethylene oxide 200 (Polyox WSR N12K) magnesium 3 5 4 2 stearate Intermediate layer pregabalin 30 10 30 30 dextrate 150 microcrystalline 70 cellulose hydroxypropyl 20 methylcellulose mannitol 50 150 45 tartaric acid 30 magnesium 1 5 1 1 stearate Lower layer pregabalin 60 75 60 60 polyethylene oxide 150 300 150 (Polyox WSR 303) polyethylene oxide 200 (Polyox WSR N12K) magnesium 3 5 4 2 stearate Total amount 527 1075 629 530
Test Example 1
Swelling Test
(46) A tablet was put into a vessel containing 0.06N HCl 900 mL, and the mixture was stirred at a rotation speed of 50 rpm using USP dissolution method 2 (paddle). Then, the size of the tablet was measured using calipers over the time. The volume and volume increase rate of the tablet were calculated based on the following equation.
*volume (mm.sup.3)=major axis (mm)×minor axis (mm)×height (mm)
*volume increase rate (%)=(volume at the measured time/volume at 0 hour (that is, just before the test))×100(%)
(47) TABLE-US-00003 TABLE 3 Time (hr) Example 1 2 3 4 5 6 7 8 0 major axis 14.0 19.9 18.1 18.0 15.0 19.9 18.0 16.1 (mm) minor axis 8.0 8.8 8.1 8.0 8.5 8.8 8.0 8.1 (mm) Thickness 6.1 7.0 5.8 5.8 5.6 7.4 5.7 5.3 (mm) Volume 689.2 1229.4 844.2 833.7 712.4 1300.4 823.7 686.8 (mm.sup.3) Volume 100.0 100.0 100.0 100.0 100.0 100.0 100.0 100.0 increase rate (%) 2 major axis 23.9 24.6 24.8 28.5 19.8 24.8 24.0 20.7 (mm) minor axis 15.9 13.4 12.3 13.1 12.6 13.3 12.0 13.1 (mm) Thickness 11.3 11.9 9.1 10.6 9.9 13.0 10.7 9.9 (mm) Volume 4273.0 3922.5 2754.6 3959.4 2463.3 4283.4 3078.4 2678.1 (mm.sup.3) Volume 620.0 319.1 326.3 474.9 345.8 329.4 373.7 389.9 increase rate (%) 6 major axis 28.6 28.4 28.8 33.5 22.3 30.3 27.5 24.8 (mm) minor axis 18.1 14.3 14.3 16.4 12.5 14.5 13.4 16.7 (mm) Thickness 10.4 11.9 13.0 12.4 10.1 14.9 11.8 11.3 (mm) Volume 5349.1 4803.4 5348.2 6805.1 2814.6 6531.0 4350.8 4645.4 (mm.sup.3) Volume 776.1 390.7 633.6 816.2 494.7 502.2 528.2 676.4 increase rate (%)
(48) Referring to table 3,
Test Example 2
Pharmacokinetic Test in Beagle Dogs
(49) Pharmacokinetic test in beagle dogs was performed for the table of Example 8 as the test drug and the commercially available Lyrica capsule 75 mg as the control. About 11 kg of beagle dogs were divided into groups of 8 dogs. A capsule as the control drug was administrated twice at initial time and 10 hours later respectively. The tablet (test drug) of example 8 was administrated once daily. Blood was collected for 24 hours after the first administration, and then the blood was analyzed to calculate each pharmacokinetic parameter. The results are shown in the following table 4.
(50) TABLE-US-00004 TABLE 4 percentage (example/ Parameter Example 8 Reference drug reference drug) AUC.sub.24 hr(μg .Math. hr/mL) 169.87 162.40 1.05 C.sub.max(μg/mL) 13.34 15.75 0.85 T.sub.max(hr) 5.9 10.7 (1.sup.stpeak: 0.9)
(51) As the test results of table 4 and
Industrial Applicability
(52) The preparation of the present invention comprising pregabalin can be administered once daily. Accordingly, the compliance can be greatly improved.