JP2010159289A - Compression molding preparation and method for producing the same - Google Patents
Compression molding preparation and method for producing the same Download PDFInfo
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- JP2010159289A JP2010159289A JP2010089563A JP2010089563A JP2010159289A JP 2010159289 A JP2010159289 A JP 2010159289A JP 2010089563 A JP2010089563 A JP 2010089563A JP 2010089563 A JP2010089563 A JP 2010089563A JP 2010159289 A JP2010159289 A JP 2010159289A
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- Prior art keywords
- preparation
- pullulan
- compression
- compression molding
- sugar
- Prior art date
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Landscapes
- Medicinal Preparation (AREA)
Abstract
Description
本発明は、医薬及び食品用の圧縮成型用組成物を利用した少量の水分でも速やかに崩壊する圧縮成型製剤およびその製造方法に関する。 The present invention relates to a compression molding preparation that rapidly disintegrates even with a small amount of water using a compression molding composition for medicine and food, and a method for producing the same.
医薬品分野のほか、近年では健康食品や栄養食品の分野においても多くの商品が経口製剤として提供されているが、これら経口製剤の多くは、錠剤、カプセル剤、顆粒、粉末等の乾燥状態の製剤として提供されているのが現状である。しかし、このような経口製剤の多くは、高齢者、小児や嚥下困難な患者にとって服用しづらいものである。 In recent years, in addition to the pharmaceutical field, many products have been provided as oral preparations in the fields of health foods and nutritional foods. Many of these oral preparations are dry preparations such as tablets, capsules, granules, and powders. It is currently provided as However, many of these oral preparations are difficult to take for the elderly, children and patients with difficulty swallowing.
このため、服用を容易にするため、服用に当たっては水に懸濁し、シロップとすることのできるドライシロップ剤等も提供されているが、粉末または顆粒状の場合には、一回の服用量毎に包装してあっても、包装内への内容物の残留、開封時にその一部をこぼしてしまう等の恐れがあり、適正量を服用するには問題があった。 For this reason, dry syrup preparations that can be suspended in water and made into syrups are also provided for ease of taking, but in the case of powder or granules, for each dose Even if it is packaged, the contents may remain in the package, or a part of the contents may be spilled when opened, and there is a problem in taking an appropriate amount.
最近、この服用の困難さの問題を解決する目的で、水なしでも服用でき口腔内で速やかに崩壊する錠剤ないしトローチ剤や、水に溶解して服用する場合にも速やかに水性溶媒に溶ける錠剤ないしトローチ剤の開発が進められている。 Recently, tablets or lozenges that can be taken without water and quickly disintegrate in the oral cavity, or tablets that dissolve quickly in aqueous solvents even when taken in water for the purpose of solving this difficulty of taking. The development of lozenges is ongoing.
例えば、上記のような錠剤ないしトローチ剤の製造方法として、粒子表面が湿潤する程度の水分を含む混合物を打錠する口腔内崩壊錠の製造方法(例えば、特許文献1参照)や、非晶質糖類を主体とし、低圧で圧縮成型した後、加湿下に錠剤を置いて湿潤させ、更に乾燥することにより得られる口腔内崩壊錠の製造方法(例えば、特許文献2、および3参照)などが知られている。また、糖類と同一質量の無機制酸剤を均一に分散させた懸濁液を噴霧乾燥して得られる組成物を利用した速崩壊性圧縮組成物(例えば、特許文献4参照)も知られている。更に、一定条件のもと、生理活性物質、糖類、低置換度ヒドロキシプロピルセルロースを組み合わせることによる口腔内速崩錠の製造方法(例えば、特許文献5参照)、結晶化した糖と非晶質化した糖を用いた口腔内速崩錠及びその製造方法(例えば、特許文献6参照)、メタケイ酸アルミン酸塩でコーティングした糖を用いた口腔内速崩錠(例えば、特許文献7参照)なども知られている。 For example, as a method for producing a tablet or a troche as described above, a method for producing an orally disintegrating tablet that compresses a mixture containing water at such a level that the particle surface is moistened (see, for example, Patent Document 1), amorphous Known is a method for producing an orally disintegrating tablet (see, for example, Patent Documents 2 and 3) obtained by compression-molding under low pressure, placing the tablet under humidification, moistening, and further drying. It has been. Also known is a rapidly disintegrating compressed composition using a composition obtained by spray drying a suspension in which an inorganic antacid having the same mass as a saccharide is uniformly dispersed (see, for example, Patent Document 4). Yes. Furthermore, a method for producing an orally rapidly disintegrating tablet by combining a physiologically active substance, a saccharide, and a low-substituted hydroxypropylcellulose under certain conditions (see, for example, Patent Document 5), crystallized sugar and amorphization Oral quick disintegrating tablets using the prepared sugar and its production method (see, for example, Patent Document 6), Oral quick disintegrating tablets using sugar coated with metasilicate aluminate (for example, refer to Patent Document 7), etc. Are known.
上記した従来技術では、水性溶媒中での速やかな崩壊性、及び携帯に必要な硬度が一応保たれた製剤が得られるものの、いずれも製造工程中における水分の取扱や、高湿度下での放置を必要とするなど、使用する生理活性成分との関係で安定性に問題を来す可能性があり、また、製造工程管理の点からも、必ずしも満足できるものではなかった。更に、無機制酸剤を利用する例では、無機制酸剤を多量に使用しなければならないことから、製造工程や消化管内のpHに影響を及ぼすことが懸念されていた。その上、従来技術での製剤の調製に当たっては、圧縮成型の際の圧力の調整を一定にする必要があり、製造条件の設定と操作が複雑となることがあった。更に、このような従来技術によっても、口腔内で崩壊した後の口当たりにざらつき感、粉のような感触が残るなど、服用時の使用感に更に改善の余地があった。 Although the above-mentioned conventional techniques can provide a preparation that maintains quick disintegration in an aqueous solvent and the hardness required for portability, both handle water during the manufacturing process and leave it under high humidity. May cause a problem in stability due to the relationship with the physiologically active ingredient used, and it is not always satisfactory from the viewpoint of manufacturing process management. Furthermore, in an example using an inorganic antacid, since a large amount of the inorganic antacid must be used, there is a concern that the production process and the pH in the digestive tract may be affected. In addition, when preparing a preparation according to the prior art, it is necessary to make the pressure adjustment constant during compression molding, which may complicate the setting and operation of manufacturing conditions. Furthermore, even with such a conventional technique, there is room for further improvement in the feeling of use at the time of taking, such as a feeling of roughness and a powdery feeling remaining after disintegrating in the oral cavity.
従って、本発明は、簡単な手段によって、口中や水性溶媒中での速やかな崩壊性を有しながら、しかも、服用時の使用感に優れ、かつ携帯に必要な硬度が保たれた、錠剤、トローチ剤等の圧縮成型製剤、およびかかる圧縮成型製剤を製造する技術の提供することを目的とするものである。 Therefore, the present invention provides tablets that have quick disintegration in the mouth and aqueous solvent by simple means, yet have excellent usability when taken, and maintain hardness required for carrying, An object of the present invention is to provide a compression-molded preparation such as a troche and a technique for producing such a compression-molded preparation.
本発明者らは、かかる従来技術の問題点を解決すべく検討した結果、錠剤やトローチ剤などの圧縮成型製剤にプルランを含有させることにより、適度な強度と硬度を有して流通過程において損耗がなく、かつ、少量の水にも速やかに崩壊する圧縮成型物が得られること、更に、通常の方法による圧縮成型にも拘わらず、得られた圧縮成型製剤はある程度の硬度を保ちつつも少量の水にも速やかに崩壊するような崩壊性も兼ね備えたものであることを見出し、本発明を完成した。 As a result of studying to solve the problems of the prior art, the present inventors have included pullulan in a compression molding preparation such as a tablet or a troche so that it has a suitable strength and hardness and is worn out in the distribution process. In addition, a compression-molded product that can be rapidly disintegrated in a small amount of water is obtained. The present invention was completed by discovering that it also has a disintegrating property that rapidly disintegrates in water.
即ち、本発明は、以下の内容をその要旨とするものである。
(1)砂糖、澱粉糖、乳糖、発蜜及び糖アルコールからなる群から選ばれる糖類、及びケイ酸化合物を含む製剤用基剤にプルランを添加してなる、速崩壊性の圧縮成型製剤。
(2)プルランの含有量が、圧縮成型製剤に対して0.0001から0.1質量部であることを特徴とする、前記(1)に記載の圧縮成形組成物。
(3)プルランの含有量が、製剤用基剤1質量部に対して0.0002から0.15質量部であることを特徴とする、前記(1)または(2)記載の速崩壊性の圧縮成型製剤。
(4)更に、生理活性物質を含有することを特徴とする、前記(1)ないし(3)のいずれか記載の速崩壊性の圧縮成型製剤。
(5)生理活性物質が、医薬活性成分であることを特徴とする、前記(4)記載の速崩壊性の圧縮成型製剤。
(6)砂糖、澱粉糖、乳糖、発蜜及び糖アルコールからなる群から選ばれた糖類、及びケイ酸化合物を含む製剤用基剤を含み更にその他の適当な製剤化助剤を含む粒状物を、プルランを水性溶媒に溶解した溶解液で造粒するか、または、該製剤用基剤を含み更に他の適当な製剤化助剤を含む粒状物を、プルランと共に水性溶媒で造粒し、得られた造粒物を圧縮成形することを特徴とする、速崩壊性の圧縮成型製剤の製造方法。
That is, the gist of the present invention is as follows.
(1) A rapidly disintegrating compression-molded preparation obtained by adding pullulan to a preparation base comprising a sugar selected from the group consisting of sugar, starch sugar, lactose, honey and sugar alcohol, and a silicate compound .
(2) The compression molding composition as described in (1) above , wherein the pullulan content is 0.0001 to 0.1 parts by mass with respect to the compression molding preparation.
(3) The rapidly disintegrating composition according to (1) or (2) above, wherein the content of pullulan is 0.0002 to 0.15 parts by mass with respect to 1 part by mass of the pharmaceutical base. Compression molding formulation.
(4) The rapidly disintegrating compression-molded preparation according to any one of (1) to (3) , further comprising a physiologically active substance.
(5) The rapidly disintegrating compression-molded preparation according to (4) , wherein the physiologically active substance is a pharmaceutically active ingredient.
(6) Granules containing a saccharide selected from the group consisting of sugar, starch sugar, lactose, honey and sugar alcohol, and a preparation base containing a silicate compound, and further containing other appropriate formulation aids. Granulated with a solution obtained by dissolving pullulan in an aqueous solvent, or granulated with an aqueous solvent together with pullulan in an aqueous solvent containing the formulation base and further suitable formulation aids. A method for producing a rapidly disintegrating compression-molded preparation characterized by compression-molding the granulated product.
本発明の圧縮成形製剤は、少量の水分で速やかに溶解し、例えば、この圧縮成形製剤を口に含むと60秒以内に崩壊し、しかも崩壊した後の口腔内にざらつき感等の好ましくない感触が残留しない。しかも、この成形品は適度な強度と硬度を有しており、流通や保管の過程において形が崩れたりする恐れが少ない。 The compression-molded preparation of the present invention dissolves rapidly with a small amount of water. For example, when the compression-molded preparation is included in the mouth, it disintegrates within 60 seconds, and the mouth feels rough after the disintegration. Does not remain. In addition, this molded product has an appropriate strength and hardness, and is less likely to lose its shape during distribution and storage.
本発明は、製剤用基剤にプルランを添加し、さらに必要に応じて生理活性成分を加え、また更に必要に応じて製剤化助剤としてその他の種々の添加剤を添加した圧縮成型用組成物において、この圧縮成型用組成物を圧縮成形して得られる、少量の水分で短時間に崩壊することのできる、速崩壊性の圧縮成型製剤と、その製造方法である。 The present invention relates to a composition for compression molding in which pullulan is added to a pharmaceutical base, a physiologically active ingredient is further added as necessary, and various other additives are further added as formulation aids as necessary. Are a rapidly disintegrating compression-molded preparation that can be disintegrated in a short time with a small amount of water, obtained by compression-molding the composition for compression molding, and a method for producing the same.
本発明の圧縮成型製剤において用いられるプルランは、デンプンを原料とし、マルトトリオースが規則正しくα-1,6結合した天然多糖類である。
プルランを使用する場合には、圧縮成形製剤1質量部に対して、0.0001〜0.1質量部であることが好ましく、0.001〜0.05質量部であることがより好ましく、0.003〜0.03質量部であることが更に好ましい。また、製剤用基剤1質量部に対して、0.0002〜0.15質量部であることが好ましく、0.001〜0.07質量部であることがより好ましく、0.003〜0.05質量部であることが更に好ましい。グルコノラクトンとプルランを同時に使用する場合には、グルコノラクトン:プルランが、その質量比で0.1〜10:0.01〜5となるように配合することが好ましい。
The pullulan used in the compression-molded preparation of the present invention is a natural polysaccharide in which maltotriose is regularly α-1,6-linked using starch as a raw material.
When pullulan is used, it is preferably 0.0001 to 0.1 parts by weight, more preferably 0.001 to 0.05 parts by weight, with respect to 1 part by weight of the compression-molded preparation. More preferably, the amount is 0.003 to 0.03 parts by mass. Moreover, it is preferable that it is 0.0002-0.15 mass part with respect to 1 mass part of bases for formulation, It is more preferable that it is 0.001-0.07 mass part, 0.003-0. More preferably, it is 05 mass parts. When gluconolactone and pullulan are used at the same time, it is preferable that gluconolactone: pullulan be blended so that the mass ratio is 0.1-10: 0.01-5.
本発明の圧縮成型製剤において用いられる製剤用基剤は、錠剤やトローチ剤などの固形の成形製剤にするための基剤であり、その一部若しくはすべてが水に溶解する添加剤が含有されていればよく、通常賦形剤と呼ばれる添加剤であれば格段特定するものではない。これらのうちで本発明の目的のためには糖類が特に好ましい。また、ケイ酸化合物も好ましく用いることができる。 The pharmaceutical base used in the compression-molded preparation of the present invention is a base for making a solid molded preparation such as a tablet or troche, and a part or all of it contains an additive that dissolves in water. Any additive that is usually called an excipient is not particularly specified. Of these, saccharides are particularly preferred for the purposes of the present invention. Silicate compounds can also be preferably used.
本発明で用いられる糖類は、特に制約はなく種々の糖類が使用される。これらの糖類としては、例えば砂糖、澱粉糖、乳糖、蜂蜜、糖アルコールなどが挙げられ、これらは、その2種以上を適宜の割合で混合して用いてもよい。砂糖としては、例えば白糖、カップリングシュガー、フラクトオリゴ糖、パラチノースなどが挙げられる。澱粉糖としては、例えばブドウ糖、麦芽糖、粉飴、水飴、果糖などが挙げられる。乳糖としては、例えば乳糖、異性化乳糖(ラクチュロース)、還元乳糖(ラクチトール)などが挙げられる。蜂蜜としては、一般に食用として用いられる各種蜂蜜が挙げられる。糖アルコールとしては、例えばソルビトール、マンニトール、マルチトール、還元澱粉糖化物、キシリトール、還元パラチノース、エリスリトールなどが挙げられる。中でも糖アルコール類と、水飴が好ましく、糖アルコール類では、特にマンニトール、トレハロース、キシリトール、ソルビトールが好ましい。 The saccharide used in the present invention is not particularly limited, and various saccharides are used. Examples of these saccharides include sugar, starch sugar, lactose, honey, sugar alcohol, and the like, and two or more of these may be used in an appropriate ratio. Examples of the sugar include sucrose, coupling sugar, fructooligosaccharide, palatinose and the like. Examples of starch sugar include glucose, maltose, powdered koji, starch syrup, and fructose. Examples of lactose include lactose, isomerized lactose (lactulose), and reduced lactose (lactitol). Examples of honey include various honeys that are generally used for food. Examples of the sugar alcohol include sorbitol, mannitol, maltitol, reduced starch saccharified product, xylitol, reduced palatinose, and erythritol. Of these, sugar alcohols and starch syrup are preferred, and saccharides such as mannitol, trehalose, xylitol, and sorbitol are particularly preferred.
本発明で用いられるケイ酸化合物としては、ケイ酸もしくは、メタケイ酸のアルカリ金属もしくはアルカリ土類金属塩が挙げられる。具体的にはケイ酸カルシウム、ケイ酸マグネシウム、ケイ酸アルミニウムがあり、メタケイ酸アルミン酸マグネシウムが好ましい。 Examples of the silicic acid compound used in the present invention include silicic acid or alkali metal or alkaline earth metal salt of metasilicic acid. Specific examples include calcium silicate, magnesium silicate, and aluminum silicate, and magnesium metasilicate aluminate is preferable.
本発明の速崩壊性の圧縮成型製剤には、必要に応じて生理活性成分を加えることができる。生理活性成分としては、医薬活性成分、嗜好成分、栄養補給成分等が挙げられる。
この生理活性成分のうち、医薬活性成分としては、例えば、滋養強壮保健薬、解熱・鎮痛・消炎薬、向精神病薬、抗不安薬、抗うつ薬、催眠鎮静薬、鎮痙薬、胃腸薬、制酸剤、鎮咳去痰剤、歯科口腔用薬、抗ヒスタミン剤、アレルギー用剤、強心剤、不整脈用剤、利尿剤、血圧降下剤、血管収縮剤、冠血管拡張剤、末梢血管拡張剤、利胆剤、抗生物質、化学療法剤、糖尿病用剤、骨粗しょう症用剤、骨格筋弛緩薬などから選ばれた1種または2種以上の成分が用いられる。
A physiologically active ingredient can be added to the rapidly disintegrating compression-molded preparation of the present invention as needed. Examples of the physiologically active ingredient include a pharmaceutically active ingredient, a preference ingredient, a nutritional supplement ingredient, and the like.
Among these physiologically active ingredients, examples of pharmaceutically active ingredients include nourishing tonic health drugs, antipyretic / analgesic / anti-inflammatory drugs, psychotropic drugs, anxiolytics, antidepressants, hypnotic sedatives, antispasmodics, gastrointestinal drugs, Acid, antitussive expectorant, dental and oral medicine, antihistamine, allergy, cardiotonic, arrhythmia, diuretic, antihypertensive, vasoconstrictor, coronary vasodilator, peripheral vasodilator, antibacterial, antibiotic One or more components selected from substances, chemotherapeutic agents, diabetic agents, osteoporosis agents, skeletal muscle relaxants and the like are used.
滋養強壮保健薬には、例えば、ビタミンA、ビタミンD、ビタミンE(酢酸d−α−トコフェロールなど)、ビタミンB1(ジベンゾイルチアミン、フルスルチアミン塩酸塩など)、ビタミンB2(酪酸リボフラビンなど)、ビタミンB6(塩酸ピリドキシンなど)、ビタミンC(アスコルビン酸、L−アスコルビン酸ナトリウムなど)、ビタミンB12(酢酸ヒドロキソコバラミンなど)などのビタミン;カルシウム、マグネシウム、鉄などのミネラル;タンパク;アミノ酸;オリゴ糖;生薬などが含まれる。 For example, vitamin A, vitamin D, vitamin E (such as d-α-tocopherol acetate), vitamin B 1 (such as dibenzoylthiamine, fursultiamine hydrochloride), vitamin B 2 (such as riboflavin butyrate) ), Vitamin B 6 (such as pyridoxine hydrochloride), vitamin C (such as ascorbic acid, sodium L-ascorbate), vitamin B 12 (such as hydroxocobalamin acetate); minerals such as calcium, magnesium, iron; protein; amino acids Oligosaccharides; herbal medicines and the like.
解熱・鎮痛・消炎薬としては、例えば、アスピリン、アセトアミノフェン、エテンザミド、イブプロフェン、塩酸ジフェンヒドラミン、dl−マレイン酸クロルフェニラミン、リン酸ジヒドロコデイン、ノスカピン、塩酸メチルエフェドリン、塩酸フェニルプロパノールアミン、カフェイン、セラペプターゼ、塩化リゾチーム、トルフェナム酸、メフェナム酸、ジクロフェナクナトリウム、フルフェナム酸、サリチルアミド、アミノピリン、ケトプロフェン、インドメタシン、ブコローム、ペンタゾシン、トラネキサム酸などが挙げられる。 Antipyretic / analgesic / anti-inflammatory drugs include, for example, aspirin, acetaminophen, ethenamide, ibuprofen, diphenhydramine hydrochloride, chlorpheniramine dl-maleate, dihydrocodeine phosphate, noscapine, methylephedrine hydrochloride, phenylpropanolamine hydrochloride, caffeine, Examples include serrapeptase, lysozyme chloride, tolfenamic acid, mefenamic acid, diclofenac sodium, flufenamic acid, salicylamide, aminopyrine, ketoprofen, indomethacin, bucolome, pentazocine, and tranexamic acid.
向精神病薬としては、例えば、クロルプロマジン、レセルピンなどが挙げられる。抗不安薬としては、例えば、クロルジアゼポキシド、ジアゼパムなどが例示される。抗うつ薬としては、例えば、イミプラミン、マプロチリン、アンフェタミンなどが例示される。催眠鎮静薬としては、例えば、エスタゾラム、ニトラゼパム、ジアゼパム、フェノバルビタールナトリウム、トリアゾラム、ブロチゾラムなどが例示される。鎮痙薬には、例えば、臭化水素酸スコポラミン、塩酸ジフェンヒドラミン、塩酸パパベリンなどが含まれる。 Examples of the psychotropic drug include chlorpromazine, reserpine and the like. Examples of anti-anxiety drugs include chlordiazepoxide, diazepam and the like. Examples of the antidepressant include imipramine, maprotiline, amphetamine and the like. Examples of the hypnotic sedative include estazolam, nitrazepam, diazepam, phenobarbital sodium, triazolam, brotizolam and the like. Antispasmodic agents include, for example, scopolamine hydrobromide, diphenhydramine hydrochloride, papaverine hydrochloride, and the like.
胃腸薬には、例えば、ジアスターゼ、含糖ペプシン、ロートエキス、リパーゼAP、ケイヒ油などの健胃消化剤;塩化ベルベリン、耐性乳酸菌、ビフィズス菌などの整腸剤;ドンペリドンなどの制吐剤などが含まれる。制酸剤としては、例えば、炭酸マグネシウム、炭酸水素ナトリウム、メタケイ酸アルミン酸マグネシウム、合成ヒドロタルサイト、沈降炭酸カルシウム、酸化マグネシウムなどが挙げられる。また、ゲファルナート、塩酸セトラキサート、テプレノン、ソファルコン、レバミピド、シメチジン、塩酸ラニチジン、ファモチジン、ニザチジン、オメプラゾール、ランソプラゾールなどの消化性潰瘍治療剤も挙げられる。更に、ピコスルファートナトリウム、センナエキス、ビサコジルなどの下剤も挙げられる。 Gastrointestinal drugs include, for example, healthy gastrointestinals such as diastase, sugar-containing pepsin, funnel extract, lipase AP, and cinnamon oil; intestinals such as berberine chloride, resistant lactic acid bacteria, and bifidobacteria; and antiemetics such as domperidone. . Examples of the antacid include magnesium carbonate, sodium hydrogen carbonate, magnesium aluminate metasilicate, synthetic hydrotalcite, precipitated calcium carbonate, magnesium oxide and the like. In addition, therapeutic agents for peptic ulcers such as gefarnate, cetraxate hydrochloride, teprenone, sofalcone, rebamipide, cimetidine, ranitidine hydrochloride, famotidine, nizatidine, omeprazole, lansoprazole and the like can also be mentioned. Further, laxatives such as sodium picosulfate, senna extract, bisacodyl and the like can be mentioned.
鎮咳去痰剤としては、例えば、塩酸クロペラスチン、臭化水素酸デキストロメトルファン、テオフィリン、グァヤコールスルホン酸カリウム、グアイフェネシンなどが挙げられる。歯科口腔用薬としては、例えば、オキシテトラサイクリン、トリアムシノロンアセトニド、塩酸クロルヘキシジン、リドカインなどが例示される。 Examples of the antitussive expectorant include cloperastine hydrochloride, dextromethorphan hydrobromide, theophylline, potassium guaiacol sulfonate, and guaifenesin. Examples of the dental and oral medicine include oxytetracycline, triamcinolone acetonide, chlorhexidine hydrochloride, lidocaine and the like.
抗ヒスタミン剤としては、例えば、塩酸ジフェンヒドラミン、プロメタジン、塩酸イソチペンジル、dl−マレイン酸クロルフェニラミンなどが挙げられる。強心剤としては、例えば、塩酸エチレフリンなどが挙げられる。アレルギー用剤としては、例えば、オキサミド、トラニラスト、メキタジン、フマル酸ケトチフェン、塩酸エピナスチン、塩酸セチリジンなどが挙げられる。不整脈用剤としては、例えば、塩酸プロカインアミド、塩酸プロプラノロール、ピンドロールなどが含まれる。利尿剤としては、例えば、イソソルビド、フロセミドなどが挙げられる。血圧降下剤としては、例えば、塩酸デラプリル、カプトプリル、臭化ヘキサメトニウム、塩酸ヒドララジン、塩酸ラベタロール、メチルドーパなどが挙げられる。 Examples of the antihistamine include diphenhydramine hydrochloride, promethazine, isothipentyl hydrochloride, dl-chlorpheniramine maleate, and the like. Examples of the cardiotonic agent include ethylephrine hydrochloride. Examples of allergic agents include oxamide, tranilast, mequitazine, ketotifen fumarate, epinastine hydrochloride, cetirizine hydrochloride and the like. Examples of the arrhythmic agent include procainamide hydrochloride, propranolol hydrochloride, pindolol and the like. Examples of the diuretic include isosorbide and furosemide. Examples of the blood pressure lowering agent include delapril hydrochloride, captopril, hexamethonium bromide, hydralazine hydrochloride, labetalol hydrochloride, methyldopa, and the like.
血管収縮剤としては、例えば、塩酸フェニレフリンなどが挙げられる。冠血管拡張剤としては、例えば、塩酸カルボクロメン、モルシドミン、塩酸ベラパミルなどが挙げられる。末梢血管拡張剤としては、例えば、シンナリジンなどが例示される。利胆剤としては、例えば、デヒドロコール酸、トレピブトンなどが例示される。 Examples of the vasoconstrictor include phenylephrine hydrochloride. Examples of the coronary vasodilator include carbochromene hydrochloride, molsidomine, verapamil hydrochloride and the like. Examples of the peripheral vasodilator include cinnarizine and the like. Examples of the astringent include dehydrocholic acid and trepibutone.
抗生物質には、例えば、セファレキシン、アモキシシリン、塩酸ピブメシリナム、塩酸セフォチアムなどのセフェム系、ペネム系およびカルバペネム系抗生物質などが含まれる。化学療法剤としては、例えば、スルファメチゾール、チアゾスルホンなどが挙げられる。糖尿病用剤としては、例えば、トルブタミド、ボグリボーズなどが挙げられる。骨粗しょう症用剤としては、例えば、イプリフラボンなどが挙げられる。骨格筋弛緩薬としては、メトカルバモールなどが挙げられる。 Antibiotics include, for example, cephem, penem and carbapenem antibiotics such as cephalexin, amoxicillin, pibmesilinum hydrochloride and cefotiam hydrochloride. Examples of the chemotherapeutic agent include sulfamethizole and thiazosulfone. Examples of the diabetic agent include tolbutamide, voglibose and the like. Examples of the osteoporosis agent include ipriflavone. Examples of skeletal muscle relaxants include metocarbamol.
上記した各生理活性成分のうち、本発明の圧縮成型製剤において、好ましく配合される生理活性成分としては、例えば上述した各成分のうち、ビタミン、生薬、解熱・鎮痛・消炎薬、抗不安薬、催眠鎮静薬、鎮痙薬、胃腸薬、消化性潰瘍薬、鎮咳去痰剤、抗ヒスタミン剤、アレルギー用剤、血圧降下剤、糖尿病用剤、骨粗しょう症用剤、骨格筋弛緩薬などが挙げられる。これら活性成分は、一般に医薬、食品分野などで用いられる希釈剤などによって希釈されたものであってもよい。また、本発明の圧縮成型製剤中の生理活性成分の少なくとも一種が油状のものであってもよい。 Among the physiologically active ingredients described above, in the compression-molded preparation of the present invention, as the physiologically active ingredients that are preferably blended, for example, among the aforementioned ingredients, vitamins, herbal medicines, antipyretic / analgesic / anti-inflammatory drugs, anxiolytics, Hypnotic sedatives, antispasmodic drugs, gastrointestinal drugs, peptic ulcer drugs, antitussive expectorants, antihistamines, allergic drugs, antihypertensive drugs, diabetes drugs, osteoporosis drugs, skeletal muscle relaxants and the like. These active ingredients may be diluted with a diluent or the like generally used in the fields of medicine, food, and the like. In addition, at least one of the physiologically active ingredients in the compression-molded preparation of the present invention may be oily.
以上のようにして得られる本発明の圧縮成型製剤は、医薬品や食品分野でのトローチ剤や、錠剤等として使用され、この圧縮成型製剤の形状、用途は特に限定されるものではない。しかしながら、水中、特に少量の水分での速やかに崩壊することを目的とする圧縮成型製剤に特に好ましく使用することができる。即ち、この本発明の圧縮成型製剤は、少量の水分と接触して短時間で崩壊し、一般的には1〜60秒、好ましくは1〜30秒という短い時間で崩壊するという特徴を有する。 The compression-molded preparation of the present invention obtained as described above is used as a troche, a tablet or the like in the pharmaceutical and food fields, and the shape and use of this compression-molded preparation are not particularly limited. However, it can be particularly preferably used for a compression-molded preparation intended to rapidly disintegrate in water, particularly with a small amount of water. That is, the compression-molded preparation of the present invention has a characteristic that it disintegrates in a short time upon contact with a small amount of water, and generally disintegrates in a short time of 1 to 60 seconds, preferably 1 to 30 seconds.
本発明の圧縮成型製剤は、まず、圧縮成型用の粒状物を得てから調製する。圧縮成型用の粒状物は、単純に製剤用基剤に、生理活性物質とその他本発明の圧縮成型製剤に所望の成分を単に混合するだけでも得られるが、湿式造粒することが望ましい。湿式造粒にあたっては、製剤用基剤に、必要に応じて生理活性物質から選ばれる一種以上、およびその他の適当な製剤化助剤を含む粒状物を、プルランを水性溶媒に溶解した溶解液で造粒するか、プルランと共に水性溶媒で造粒することがよりのぞましい。また、プルランを含む水性溶液中にその他の適当な製剤化助剤を混合してもよい。或いは、上記のようにして製剤用基剤とプルランを含む粒状物を調製し、生理活性物質を別途添加した粒状物とし、これを圧縮成形してもよい。 The compression molding preparation of the present invention is first prepared after obtaining a granule for compression molding. The granules for compression molding can be obtained by simply mixing the desired ingredients with the base for formulation, the physiologically active substance and other compression molding formulations of the present invention, but it is desirable to perform wet granulation. In wet granulation, a granular material containing one or more substances selected from physiologically active substances and other appropriate formulation aids, if necessary, in a formulation base, is a solution obtained by dissolving pullulan in an aqueous solvent. or granulated, more desirable to be granulated together with an aqueous solvent and pullulan. Moreover, you may mix other suitable formulation aids in the aqueous solution containing a pullulan . Alternatively, a granular material containing a pharmaceutical base and pullulan may be prepared as described above to obtain a granular material separately added with a physiologically active substance, and this may be compression molded.
また、湿式造粒に使用する水性溶媒には、使用する生理活性物質や、その他の製剤化助剤の種類によって、水混和性の有機溶媒を使用してもよい。水混和性の有機溶媒としては、エタノール、プロパノール等が好ましい。また、造粒方法については、一般に使用される方法であれば特に限定はないが、撹拌造粒、流動層造粒、転動造粒等が上げられ、特に流動層造粒が好ましい。 Further, as the aqueous solvent used for wet granulation, a water-miscible organic solvent may be used depending on the type of physiologically active substance to be used and other formulation aids. As the water-miscible organic solvent, ethanol, propanol and the like are preferable. The granulation method is not particularly limited as long as it is a generally used method, but stirring granulation, fluidized bed granulation, rolling granulation and the like can be raised, and fluidized bed granulation is particularly preferable.
このように得られた粒状物は常法によって打錠その他の成形方法によって圧縮成形され、本発明の圧縮成型製剤となる。この圧縮成形の際の、成形圧は、少量の水で、1〜60秒以内に崩壊する錠剤が得られる成形圧を適宜選択すればよいが、流通時の損耗などを考慮すると、1,000N〜20,000Nが好ましく、3,000N〜15,000Nがより好ましい。本発明の圧縮成形製剤は、打錠その他の通常の方法によって製造できるにもかかわらず、得られた成形品が適度な強度と硬度を有しており、輸送や保管中の取り扱いによって型崩れしたりしない。 The granular material thus obtained is compression-molded by a conventional method such as tableting or other molding methods to obtain the compression-molded preparation of the present invention. The molding pressure at the time of this compression molding may be selected as appropriate so that a tablet that disintegrates within 1 to 60 seconds can be obtained with a small amount of water. -20,000N are preferable, and 3,000N-15,000N are more preferable. Although the compression-molded preparation of the present invention can be produced by tableting or other ordinary methods, the obtained molded product has an appropriate strength and hardness, and is deformed by handling during transportation and storage. Do not do.
また、更に、本発明の圧縮成型製剤の製造に当たっては、本発明の効果に支障がない限り、上記の部分でその他の製剤化助剤として記載した、圧縮成型製剤の製造に一般に使用される種々の添加剤を含んでいても良い。 Furthermore, in the production of the compression-molded preparation of the present invention, as long as there is no hindrance to the effect of the present invention, various types generally used for the production of compression-molded preparations described as other formulation aids in the above part. The additive may be included.
このような製剤化助剤である添加剤として、例えば、崩壊剤、結合剤、滑沢剤、矯味成分、香料並びに補助剤などが挙げられる。 Examples of such additives that are formulation aids include disintegrants, binders, lubricants, taste-masking ingredients, fragrances, and adjuvants.
崩壊剤としては、例えば、コーンスターチやバレイショデンプンなどのデンプン、部分アルファー化澱粉、カルボキシメチルスターチナトリウム、カルメロース、カルメロースカルシウム、クロスカルメロースナトリウム、ポリビニルアルコール、クロスポビドン、低置換度ヒドロキシプロピルセルロース、結晶セルロース、ヒドロキシプロピルスターチなどが例示される。結合剤としては、例えば、ヒドロキシプロピルセルロース、ヒドロキシプロピルメチルセルロース、カルボキシビニルポリマー、カルメロースナトリウム、アルファー化澱粉、ポリビニルピロリドン、アラビアゴム末、ゼラチン、プルランなどが挙げられる。増量剤としては、ショ糖、ブドウ糖、乳糖、マンニトール、マルトース、ソルビトール、リン酸カルシウム、硫酸カルシウム等が挙げられる。 Disintegrants include, for example, starch such as corn starch and potato starch, partially pregelatinized starch, sodium carboxymethyl starch, carmellose, carmellose calcium, croscarmellose sodium, polyvinyl alcohol, crospovidone, low-substituted hydroxypropylcellulose, crystals Examples include cellulose and hydroxypropyl starch. Examples of the binder include hydroxypropylcellulose, hydroxypropylmethylcellulose, carboxyvinyl polymer, carmellose sodium, pregelatinized starch, polyvinylpyrrolidone, gum arabic powder, gelatin, pullulan and the like. Examples of the bulking agent include sucrose, glucose, lactose, mannitol, maltose, sorbitol, calcium phosphate, calcium sulfate and the like.
矯味成分としては、例えば、クエン酸、酒石酸、リンゴ酸などが挙げられる。発泡剤としては、例えば、重曹などが挙げられる。人口甘味料としては、例えば、サッカリンナトリウム、グリチルリチン二カリウム、アスパルテーム、ステビア、ソーマチンなどが挙げられる。マスキング剤としては、例えば、エチルセルロース等の水不溶性高分子、メタアクリル酸メチル・メタアクリル酸ブチル・メタアクリル酸ジエチルアミノエチル・コポリマー等の抗唾液性胃溶性高分子などが挙げられる。 Examples of the taste-masking component include citric acid, tartaric acid, malic acid and the like. Examples of the foaming agent include sodium bicarbonate. Examples of artificial sweeteners include saccharin sodium, dipotassium glycyrrhizin, aspartame, stevia, and thaumatin. Examples of the masking agent include water-insoluble polymers such as ethyl cellulose and anti-salivary gastric polymers such as methyl methacrylate / butyl methacrylate / diethylaminoethyl methacrylate / copolymer.
香料としては、例えば、レモン、レモンライム、オレンジ、メントール、ハッカ油、バニリンなど、あるいはこれをデキストリンもしくはシクロデキストリンに吸着させた粉末香料などが挙げられる。滑沢剤としては、例えば、ステアリン酸マグネシウム、ショ糖脂肪酸エステル、ポリエチレングリコール、タルク、ステアリン酸などが例示される。 Examples of the fragrance include lemon, lemon lime, orange, menthol, mint oil, vanillin, and powdered fragrance obtained by adsorbing it on dextrin or cyclodextrin. Examples of the lubricant include magnesium stearate, sucrose fatty acid ester, polyethylene glycol, talc, stearic acid and the like.
補助剤としては、着色剤、生理活性成分安定化剤、溶解補助剤等が挙げられる。例えば、着色剤としては、食用黄色5号、食用赤色3号、食用青色2号などの食用色素;食用レーキ色素;ベンガラなどが挙げられる。安定化剤又は溶解補助剤は、使用する生理活性成分によって異なるが、例えば、アスコルビン酸、トコフェロールなどの抗酸化剤、ポリソルベート80等の界面活性剤が挙げられる。 Examples of the auxiliary agent include a colorant, a physiologically active ingredient stabilizer, and a solubilizing agent. Examples of the colorant include edible pigments such as edible yellow No. 5, edible red No. 3 and edible blue No. 2; edible lake pigments; Stabilizers or solubilizers vary depending on the physiologically active components used, and examples include antioxidants such as ascorbic acid and tocopherol, and surfactants such as polysorbate 80.
次に実施例及び試験例を挙げ、本発明を更に詳しく説明するが、本発明はこれら実施例に何ら制約されるものではない。
製造例:製剤用基剤の造粒品の製造
メタケイ酸アルミン酸マグネシウム(商品名:ノイシリンFL2、富士化学工業(株)製)の240gを精製水2,400gに懸濁させた。D−マンニトール(商品名:マンニットP、東和化成工業(株)製)の5,484gに対して、上記のノイシリンFL2懸濁液2,400gを用い、流動層造粒機(FLO−5型流動層造粒機:フロイント産業(株)製)を用い製剤用基剤の造粒品を製造した。
EXAMPLES Next, although an Example and a test example are given and this invention is demonstrated in more detail, this invention is not restrict | limited at all by these Examples.
Production Example: Production of Granulated Product of Formulation Base 240 g of magnesium aluminate metasilicate (trade name: Neusilin FL2, manufactured by Fuji Chemical Industry Co., Ltd.) was suspended in 2,400 g of purified water. The above-mentioned Neusilin FL2 suspension (2,400 g) is used for 5,484 g of D-mannitol (trade name: Mannit P, manufactured by Towa Kasei Kogyo Co., Ltd.), and a fluidized bed granulator (FLO-5 type). Using a fluidized bed granulator: manufactured by Freund Sangyo Co., Ltd., a granulated product of a pharmaceutical base was produced.
実施例1:プルランを用いた圧縮成形製剤の製造
プルラン微粉末(商品名:プルランPI−21、(株)林原製)15.32gを精製水306.4gに溶解した。このプルラン水溶液に、上記製造例で製造した製剤用基剤造粒品800gを加えて、流動層造粒機にて造粒を行った。得られた造粒物46.79gに、架橋性ポリビニルピロリドン(商品名:コリドンCL、クロスポビドン、BASF(株)製)2.92gと、ステアリン酸マグネシウム(ステアリン酸マグネシウム:日本油脂(株)製)0.29gを加えた。この顆粒を用い、打錠圧2,500Nでオイルプレスにて直径8.0mmの錠剤を製造した。
Example 1: Production of a compression-molded preparation using pullulan
15.32 g of pullulan fine powder (trade name: Pullulan PI-21, manufactured by Hayashibara Co., Ltd.) was dissolved in 306.4 g of purified water. To this aqueous solution of pullulan , 800 g of the base granulated product for preparation produced in the above production example was added, and granulated by a fluidized bed granulator. To 46.79 g of the obtained granulated product, 2.92 g of a crosslinkable polyvinylpyrrolidone (trade name: Kollidon CL, crospovidone, manufactured by BASF Corp.) and magnesium stearate (magnesium stearate: manufactured by Nippon Oil & Fats Co., Ltd.) ) 0.29 g was added. Using these granules, tablets with a diameter of 8.0 mm were produced with an oil press at a tableting pressure of 2,500 N.
実施例2:グルコノラクトンとプルランを用いた圧縮成形製剤の製造
グルコノラクトン(商品名:グルクノδラクトン:藤沢製薬(株)製)7.66g及びプルラン7.66gを精製水306.4gに溶解した。このグルクノラクトンとプルランの水溶液に、上記製造例で調製した製剤用基剤の造粒品800gを加えて、流動層造粒機にて造粒を行った。得られた造粒物46.79gにコリドンCL
2.92gと、ステアリン酸マグネシウム0.29gを加えた。この顆粒を打錠圧15,000Nでオイルプレスにて打錠を行い、直径8.0mmの錠剤を製造した。
Example 2 : Production of a compression-molded preparation using gluconolactone and pullulan 7.66 g of gluconolactone ( trade name: Glucno δ lactone: manufactured by Fujisawa Pharmaceutical Co., Ltd. ) and 7.66 g of pullulan were added to 306.4 g of purified water. Dissolved. To this aqueous solution of glucunolactone and pullulan, 800 g of the granulated product of the preparation base prepared in the above production example was added, and granulated by a fluidized bed granulator. Kollidon CL was added to 46.79 g of the granulated product.
2.92 g and 0.29 g of magnesium stearate were added. The granules were tableted with an oil press at a tableting pressure of 15,000 N to produce tablets with a diameter of 8.0 mm.
比較例1:
実施例1のグルコノラクトン15.32gを、アルギン酸プロピレングリコールエステル(商品名:キミロイド、(株)キミカ製)15.32gとして、そのほかは実施例1と同一の条件に従って打錠を行い、直径8.0mmの錠剤を製造した。
Comparative Example 1:
Tableting was performed according to the same conditions as in Example 1 except that 15.32 g of gluconolactone in Example 1 was changed to 15.32 g of propylene glycol alginate (trade name: Kimiroid, manufactured by Kimika Co., Ltd.), and the diameter was 8 0.0 mm tablets were produced.
比較例2:
実施例1のグルコノラクトン15.32gを、ポリオキシエチレンポリオキシプロピレングリコール(商品名:アデカプルロニックF68、旭電化工業(株)製)15.32gとして、そのほかは実施例1と同一の条件に従って打錠を行い、直径8.0mmの錠剤を製造した。
Comparative Example 2:
According to the same conditions as Example 1 except that 15.32 g of gluconolactone of Example 1 is 15.32 g of polyoxyethylene polyoxypropylene glycol (trade name: Adeka Pluronic F68, manufactured by Asahi Denka Kogyo Co., Ltd.). Tableting was performed to produce a tablet having a diameter of 8.0 mm.
比較例3:
実施例1のグルコノラクトン15.32gを、デキストリン(商品名:デキストリン、松谷化学工業(株)製)15.32gとして、そのほかは実施例1と同一の条件に従って打錠を行い、直径8.0mmの錠剤を製造した。
Comparative Example 3:
Tableting is performed according to the same conditions as in Example 1 except that 15.32 g of gluconolactone of Example 1 is 15.32 g of dextrin (trade name: dextrin, manufactured by Matsutani Chemical Co., Ltd.), and the diameter is 8. 0 mm tablets were produced.
比較例4:
実施例1のグルコノラクトン15.32gを、水飴(商品名:水飴、日本食品化工(株)製)15.32gとして、そのほかは実施例1と同一の条件に従って打錠を行い、直径8.0mmの錠剤を製造した。
Comparative Example 4:
Tableting was performed according to the same conditions as in Example 1 except that 15.32 g of gluconolactone in Example 1 was changed to 15.32 g of syrup (brand name: Minamata, manufactured by Nippon Shokuhin Kako Co., Ltd.). 0 mm tablets were produced.
試験例:
実施例1〜実施例2、および比較例1〜比較例4で製造した各錠剤を用いて、
3名のパネラーによってその崩壊性等の評価を行なった。具体的には、各パネラーが試料の錠剤を口腔内に含み、その崩壊時間と口腔内における崩壊の様子を評価した。各パネラーの評価の平均の結果を表1に示す。
Test example:
Using each tablet produced in Example 1 to Example 2 and Comparative Example 1 to Comparative Example 4,
The disintegration property was evaluated by three panelists. Specifically, each panel included a sample tablet in the oral cavity, and the disintegration time and the state of disintegration in the oral cavity were evaluated. Table 1 shows the average results of the evaluation of each panel.
実施例3:
医薬活性成分としてファモチジン100gと乳糖(商品名:乳糖DMV200M:DMV(株)製)45gを2Lの精製水に、ヒドロキシプロピルセルロース(商品名:HPC−ssL、日本曹達(株)製)10.5gとともに溶解させた水溶液を用いて常法により造粒した。この造粒物にアクリル酸エチル・メタクリル酸メチルコポリマーエマルジョン(商品名:オイドラギットNE30D、ローム(株)製)46.4g、およびタルク(商品名:タルカンハヤシ、林化成(株)製)8.4gを精製水104gに懸濁させた溶液を用い、常法によってファモチジン含有顆粒を製した。このファモチジン含有顆粒6.089gを実施例1で得られた顆粒40.7gと共に、実施例1の方法により、打錠して錠剤を製造した。
Example 3 :
As active pharmaceutical ingredients, 100 g of famotidine and 45 g of lactose (trade name: lactose DMV200M: manufactured by DMV Co., Ltd.) in 2 L of purified water, hydroxypropylcellulose (trade name: HPC-ssL, manufactured by Nippon Soda Co., Ltd.) 10.5 g Granulation was carried out by an ordinary method using an aqueous solution dissolved together. 46.4 g of ethyl acrylate / methyl methacrylate copolymer emulsion (trade name: Eudragit NE30D, manufactured by Rohm Co., Ltd.) and talc (trade name: manufactured by Talkan Hayashi, Hayashi Kasei Co., Ltd.) 8.4 g Was used to prepare famotidine-containing granules by a conventional method. Tablets were produced by compressing 6.089 g of this famotidine-containing granule together with 40.7 g of the granule obtained in Example 1 by the method of Example 1.
実施例4:
実施例4のファモチジン100gをランソプラゾール100gに代えて、更にアクリル酸エチル・メタクリル酸メチルコポリマーエマルジョンをメタアクリル酸コポリマーLD(商品名:オイドラギットL30D−55、ローム(株)製)に代え、他は実施例3同様にして錠剤を製造した。
Example 4 :
Instead famotidine 100g of Example 4 to lansoprazole 100g, further methyl ethyl methacrylate acrylate copolymer emulsion methacrylic acid copolymer LD: instead of (trade name Eudragit L30D-55, Rohm Co., Ltd.) and the other embodiment Tablets were produced in the same manner as in Example 3 .
実施例5:
実施例3のファモチジン100gをトリアゾラム100gに代えて、他は実施例3と同様にして錠剤を製造した。
Example 5 :
A tablet was produced in the same manner as in Example 3 except that 100 g of famotidine in Example 3 was replaced with 100 g of triazolam.
実施例6:
実施例1の造粒品を製する際に水飴を加える他は、実施例3に従って、錠剤を製した。
Example 6 :
Tablets were produced according to Example 3 , except that starch syrup was added when producing the granulated product of Example 1.
実施例3ないし実施例6によって得られた錠剤はいずれも口腔内で60秒以内に崩壊し、口触りもなめらかであった。 All of the tablets obtained in Examples 3 to 6 disintegrated in the oral cavity within 60 seconds, and the touch was smooth.
本発明の速崩壊性の圧縮成型製剤は、口腔内などにて少量の水分で速やかに崩壊し、かつ崩壊した後にざらつき感等の残留しない成型製剤として、種々の薬剤成分を含む錠剤やトローチタイプの医薬品として有用である。 The rapidly disintegrating compression-molded preparation of the present invention is a tablet or troche type containing various drug components as a molded preparation that rapidly disintegrates with a small amount of water in the oral cavity and does not remain after the disintegration. It is useful as a pharmaceutical product.
Claims (6)
A granular material containing a formulation base containing a saccharide selected from the group consisting of sugar, starch sugar, lactose, honey and sugar alcohol, and a silicate compound, and further containing a formulation aid, pullulan as an aqueous solvent granulated either in solution dissolved in, or, further comprises a formulation for base granules contain other formulation aids, pullulan and both granulated with an aqueous solvent, the granules obtained A method for producing a rapidly disintegrating compression molding preparation, characterized by compression molding.
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| JP2010089563A Pending JP2010159289A (en) | 2010-04-08 | 2010-04-08 | Compression molding preparation and method for producing the same |
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Cited By (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| WO2017170763A1 (en) * | 2016-04-01 | 2017-10-05 | 株式会社クレハ | Disintegrable tablet and method for manufacturing same |
Citations (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| JP2005053792A (en) * | 2003-08-01 | 2005-03-03 | Taiyo Yakuhin Kogyo Kk | Compression-molded preparation and method for producing the same |
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Patent Citations (1)
| Publication number | Priority date | Publication date | Assignee | Title |
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| JP2005053792A (en) * | 2003-08-01 | 2005-03-03 | Taiyo Yakuhin Kogyo Kk | Compression-molded preparation and method for producing the same |
Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| WO2017170763A1 (en) * | 2016-04-01 | 2017-10-05 | 株式会社クレハ | Disintegrable tablet and method for manufacturing same |
| JPWO2017170763A1 (en) * | 2016-04-01 | 2019-01-10 | 株式会社クレハ | Disintegrating tablet and method for producing the same |
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