JP2013121951A - Stable solid preparation and method for producing the same - Google Patents

Stable solid preparation and method for producing the same Download PDF

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JP2013121951A
JP2013121951A JP2012245349A JP2012245349A JP2013121951A JP 2013121951 A JP2013121951 A JP 2013121951A JP 2012245349 A JP2012245349 A JP 2012245349A JP 2012245349 A JP2012245349 A JP 2012245349A JP 2013121951 A JP2013121951 A JP 2013121951A
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solid preparation
weight
preparation
candesartan cilexetil
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JP5680607B2 (en
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Hiroshi Sakamoto
浩 坂本
Hiroto Terada
浩人 寺田
Toshiya Taniguchi
俊哉 谷口
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Ohara Pharmaceutical Co Ltd
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Abstract

PROBLEM TO BE SOLVED: To provide a tablet that can retain a principal ingredient even after being formulated for a long period of time by reducing unstabilization to such as pressure, impact, friction and heating applied when formulating candesartan cilexetil containing solid preparation which causes the reduction in storage stability of the principal ingredient after formulation by the influence of such as the impact, the friction and the heating.SOLUTION: In the solid preparation produced by using the candesartan cilexetil and an additive generally used, water equivalent to 2-10 wt.% of the total weight of a composition for formulating the solid preparation is contained for the formulation.

Description

本発明は、カンデサルタンシレキセチル(医薬品一般的名称)を含有する安定固形製剤に関する。   The present invention relates to a stable solid preparation containing candesartan cilexetil (generic drug name).

アンジオテンシンII受容体拮抗薬であるカンデサルタンシレキセチルは、高血圧症の治療においてアンジオテンシンI変換酵素阻害薬よりも高い有効性を示す薬剤として注目を集めている。
後述の特許文献1によると、カンデサルタンシレキセチルを包含するベンズイミダゾール−7−カルボン酸またはその誘導体は、固体単独の静置状態では、温度、湿度等に対して安定であるが、製剤化工程における粉砕、混合、撹拌、乾燥、加熱、圧縮などによる衝撃、摩擦、加熱、加圧等により結晶に歪みが生じ、保存時には経時的に含量低下をきたすこと、しかし低融点油脂状物質を配合しておくと、製剤化後の保存時も経時的な分解を抑制できることが記載されている。
また、カンデサルタンシレキセチルは水に対して難溶性であるため、一定の粒子径以下(例えば、平均粒子径で約4μm以下)に粉砕し溶解性を改善することが必須であり、さらに二次凝集塊のない均一分散や微粉末化することにより体内での吸収を容易にすることが必要となる。しかし、カンデサルタンシレキセチルは、上述のとおり、製剤化時の圧力、衝撃、摩擦、加熱等の影響によって保存安定性が低下するため、結晶を微粉末化する際の粉砕によっても主薬の経時的な含量低下をきたす可能性がある。 Candesartan cilexetil, an angiotensin II receptor antagonist, has attracted attention as a drug that exhibits higher efficacy than angiotensin I converting enzyme inhibitors in the treatment of hypertension.
According to Patent Document 1 described later, benzimidazole-7-carboxylic acid or a derivative thereof including candesartan cilexetil is stable with respect to temperature, humidity, and the like in a stationary state of a solid alone. The crystals are distorted by impact, friction, heating, pressurization, etc. due to crushing, mixing, stirring, drying, heating, compression, etc., and the content decreases with time during storage, but a low melting point oily substance is added. In other words, it is described that degradation over time can be suppressed even during storage after formulation.
In addition, since candesartan cilexetil is sparingly soluble in water, it is essential to improve solubility by pulverization to a certain particle size or less (for example, an average particle size of about 4 μm or less). It is necessary to facilitate absorption in the body by uniformly dispersing and finely powdering without agglomerates. However, as described above, candesartan cilexetil has a lower storage stability due to the effects of pressure, impact, friction, heating, etc. during formulation. There is a possibility of causing a significant decrease in content.

特許第2682353号公報Japanese Patent No. 2682353

本発明の課題は、カンデサルタンシレキセチル含有製剤の製剤化工程における摩擦、衝撃、加熱、加圧等に起因する結晶の歪みを抑制し、製剤化後も長期間安定に保持できるカンデサルタンシレキセチル含有固形製剤を提供することにある。   An object of the present invention is to suppress the distortion of crystals caused by friction, impact, heating, pressurization, etc. in the preparation process of a candesartan cilexetil-containing preparation, and candesartan cilexetil that can be stably maintained for a long time after preparation It is to provide a containing solid preparation.

本発明者らは、前記課題を解決するため鋭意検討した。その結果、カンデサルタンシレキセチルを含む製剤化用の組成物中に2〜10重量%の水分を含有させることにより製剤化工程、特に粉砕、圧縮成形後の主剤の経時的な安定性を飛躍的に改善できることを見出した。本発明者らは、その知見に基づいてさらに研究を重ね、本発明を完成するに至った。   The present inventors diligently studied to solve the above problems. As a result, by incorporating 2 to 10% by weight of water into the formulation composition containing candesartan cilexetil, the stability over time of the main component after the formulation process, especially after pulverization and compression molding, is dramatically improved. I found that it can be improved. The present inventors have further studied based on the knowledge, and have completed the present invention.

すなわち、本発明によれば、下記の固形製剤及びその製造法を提供することができる。
(1)カンデサルタンシレキセチル、製剤上の添加物及び組成物全重量に対して2〜10重量%の水分を含有する製剤用組成物を製剤化することにより得られる固形製剤。
(2)製剤上の添加物が、結合剤及び可塑剤の少なくとも1種である(1)記載の固形製剤。
(3)結合剤がヒドロキシプロピルセルロース又はポリビニルピロリドンであり、可塑剤がクエン酸トリエチル、クエン酸トリブチル、トリアセチン又はグリセリンである(1)または2記載の固形製剤。
(4)固形製剤が圧縮錠剤である(1)〜(3)のいずれかに記載の固形製剤。
(5)固形製剤が口腔内崩壊錠である(1)〜(4)のいずれかに記載の固形製剤。
(6)固形製剤中のカンデサルタンシレキセチルの含有率が0.3〜20重量%である請求項(1)〜(5)のいずれかに記載の固形製剤。
(7)カンデサルタンシレキセチル、製剤上の添加物及び組成物全重量に対して2〜10重量%の水分を含有する製剤用組成物を製剤化する固形製剤の製造法。
(8)製剤上の添加物が、結合剤及び可塑剤の少なくとも1種である(7)記載の固形製剤の製造法。
(9)製剤化が圧縮錠剤である(7)又は(8)記載の固形製剤の製造法。
(10)固形製剤中のカンデサルタンシレキセチルの含有率が0.3〜20重量%である(7)〜(9)のいずれかに記載の固形製剤の製造法。 That is, according to this invention, the following solid formulation and its manufacturing method can be provided.
(1) A solid preparation obtained by formulating candesartan cilexetil, an additive on the preparation, and a composition for preparation containing 2 to 10% by weight of water based on the total weight of the composition.
(2) The solid preparation according to (1), wherein the additive on the preparation is at least one of a binder and a plasticizer.
(3) The solid preparation according to (1) or 2, wherein the binder is hydroxypropylcellulose or polyvinylpyrrolidone, and the plasticizer is triethyl citrate, tributyl citrate, triacetin, or glycerin.
(4) The solid preparation according to any one of (1) to (3), wherein the solid preparation is a compressed tablet.
(5) The solid preparation according to any one of (1) to (4), wherein the solid preparation is an orally disintegrating tablet.
(6) The solid preparation according to any one of (1) to (5), wherein the content of candesartan cilexetil in the solid preparation is 0.3 to 20% by weight.
(7) A method for producing a solid preparation for preparing a pharmaceutical composition containing 2 to 10% by weight of water relative to the total weight of candesartan cilexetil, an additive on the preparation, and the composition.
(8) The method for producing a solid preparation according to (7), wherein the additive on the preparation is at least one of a binder and a plasticizer.
(9) The method for producing a solid preparation according to (7) or (8), wherein the preparation is a compressed tablet.
(10) The method for producing a solid preparation according to any one of (7) to (9), wherein the content of candesartan cilexetil in the solid preparation is 0.3 to 20% by weight.

製剤用組成物中の水分含量は、2〜10重量%、好ましくは2.0〜8.4重量%、特に好ましくは2.0〜5.5重量%である。上記含量未満では保存中の総分解物の割合が増えて安定効果が不充分となり、上記含量を超える場合は、錠剤の強度が低下するため、市場における流通過程で錠剤の割れや欠け等の問題が生じる可能性がある。   The water content in the pharmaceutical composition is 2 to 10% by weight, preferably 2.0 to 8.4% by weight, particularly preferably 2.0 to 5.5% by weight. If the content is less than the above, the ratio of the total decomposition products during storage increases and the stability effect is insufficient.If the content exceeds the above content, the strength of the tablet is reduced, so there are problems such as cracking and chipping of the tablet in the distribution process in the market. May occur.

本発明において使用される製剤上の添加物としては、賦形剤、結合剤、可塑剤、崩壊剤、滑沢剤、着色剤、界面活性剤、安定剤、嬌味嬌臭剤などが挙げられる。
賦形剤としては乳糖、結晶セルロース、トウモロコシデンプン、バレイショデンプン、部分アルファー化デンプン、D−マンニトール、白糖、ショ糖、ブドウ糖等が挙げられ、この賦形剤の使用量は製剤用組成物中、通常5〜90重量%、好ましくは10〜80重量%である。 Examples of additives on the preparation used in the present invention include excipients, binders, plasticizers, disintegrants, lubricants, colorants, surfactants, stabilizers, and miso odorants. .
Examples of excipients include lactose, crystalline cellulose, corn starch, potato starch, partially pregelatinized starch, D-mannitol, sucrose, sucrose, glucose, and the like. Usually 5 to 90% by weight, preferably 10 to 80% by weight.

本発明において使用される結合剤としてはヒドロキシプロピルセルロース、ヒドロキプロピルメチルセルロース、メチルセルロース、エチルセルロース、アルファー化デンプン、ポリビニルピロリドン、ポリビニルアルコール、ポリビニルアルコール・アクリル酸・メタクリル酸メチル共重合体等が挙げられ、その結合剤の使用量は、固形剤全重量に対して通常0.1〜10重量%、好ましくは0.5〜6.0重量%である。   Examples of the binder used in the present invention include hydroxypropylcellulose, hydroxypropylmethylcellulose, methylcellulose, ethylcellulose, pregelatinized starch, polyvinylpyrrolidone, polyvinyl alcohol, polyvinyl alcohol / acrylic acid / methyl methacrylate copolymer, etc. The amount of the binder used is usually 0.1 to 10% by weight, preferably 0.5 to 6.0% by weight, based on the total weight of the solid agent.

本発明において使用される可塑剤として好ましくは、アジピン酸ジオクチル、クエン酸トリエチル、クエン酸トリブチル、トリアセチン又はグリセリン、フタル酸ジエチル、フタル酸ジオクチル、プロピレングリコール等が挙げられ、なかでもクエン酸トリエチルが特に好ましい。可塑剤の使用量は、製剤の重量中、通常0.1〜10重量%、好ましくは0.2〜6重量%である。   Preferred examples of the plasticizer used in the present invention include dioctyl adipate, triethyl citrate, tributyl citrate, triacetin or glycerin, diethyl phthalate, dioctyl phthalate, propylene glycol, and the like. preferable. The usage-amount of a plasticizer is 0.1 to 10 weight% normally in the weight of a formulation, Preferably it is 0.2 to 6 weight%.

また、本発明において使用される崩壊剤、特に口腔内崩壊剤としては、カルメロース、カルメロースカルシウム、カルボキシメチルスターチナトリウム、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、部分アルファー化デンプン等が挙げられ、この崩壊剤の使用量は、製剤の重量中、通常0.1〜10重量%、好ましくは0.5〜6.0重量%である。
その他の添加物として、必要により、滑沢剤、着色剤、界面活性剤、安定剤、嬌味嬌臭剤などを適量配合することもできる。 Examples of the disintegrating agent used in the present invention, particularly the oral disintegrating agent, include carmellose, carmellose calcium, sodium carboxymethyl starch, crospovidone, low-substituted hydroxypropylcellulose, and partially pregelatinized starch. The usage-amount of a disintegrating agent is 0.1 to 10 weight% normally in the weight of a formulation, Preferably it is 0.5 to 6.0 weight%.
As other additives, lubricants, colorants, surfactants, stabilizers, and miso odorants can be blended in appropriate amounts as necessary.

製剤化とは、薬理効果を有する主剤を人体に投与するに適した剤形にすることを意味しているが、本発明の固形製剤には錠剤、カプセル剤、顆粒剤、粉剤などが含まれ、製剤化の工程には、各成分や組成物の粉砕、混練、噴霧、撹拌、整粒、篩過、乾燥、圧縮打錠等が含まれる。それらの工程自体は、従来公知の方法に従って行うことができる。
また、口腔内崩壊剤を製造する方法としては、例えば、糖類の水分散液を型に流し込んで乾燥して製造する方法、糖類、結合剤等を水やアルコールで湿潤させた粉末を成形した後乾燥して製造する方法、糖類、結合剤等を用いて造粒、乾燥したものを低圧力で成形した後、加湿乾燥処理して製造する方法、打錠用臼杵表面に微量の滑沢剤を塗布しながら打錠して製造する方法、成形性の高い賦形剤と崩壊性の強い崩壊剤を配合し打錠して製造する方法等が挙げられる。 Formulation means making the main agent having a pharmacological effect into a dosage form suitable for administration to the human body, but the solid preparation of the present invention includes tablets, capsules, granules, powders and the like. The preparation process includes pulverization, kneading, spraying, stirring, sizing, sieving, drying, compression tableting and the like of each component and composition. These steps themselves can be performed according to a conventionally known method.
In addition, as a method for producing an orally disintegrating agent, for example, a method in which an aqueous dispersion of saccharides is poured into a mold and dried, and a powder in which saccharides, a binder, etc. are wetted with water or alcohol is formed A method of drying and manufacturing, a method of granulating and drying using saccharides, a binder, etc. after molding at low pressure, then humidifying and drying, a small amount of lubricant on the surface of a mortar for tableting Examples thereof include a method of tableting while coating, a method of blending a highly moldable excipient and a highly disintegrating disintegrant, and tableting and manufacturing.

本発明によれば、長期間品質を保証し、かつ、体内での吸収を担保し得るカンデサルタンシレキセチルを含有する固形製剤、特に錠剤を提供することができる。   According to the present invention, it is possible to provide a solid preparation, particularly a tablet, containing candesartan cilexetil that can guarantee long-term quality and ensure absorption in the body.

(1)ヒドロキシプロピルセルロース30.0gおよびクエン酸トリエチル6gを精製水570.0gに溶解し、さらに、平均粒子径11.96μmのカンデサルタンシレキセチル12.0gを加えて均一に分散した液を、高圧剪断式ホモジナイザー(パウレック社製:MICROFLUIDIZER M−110P型)を用い、圧力207Mpaにて、均一分散、湿式粉砕した。
(2)乳糖552.0g、トウモロコシデンプン120.0g及びカルメロースカルシウム24.0gを流動層造粒機(パウレック社製:MP−01型)に投入し、流動化させ、(1)で得た湿式粉砕薬液を噴霧して造粒した。薬液噴霧終了後、引き続き流動層乾燥機にて造粒物中の水の含有率が2.0重量%になるまで乾燥した後、24メッシュ篩で整粒した。得られた整粒品の一部である129.0gにステアリン酸マグネシウム1.0gを加え、ポリエチレン製の袋にて混合した。次いで、この混合物をロータリー式打錠機(菊水製作所製:VIRGO型)を用いて打錠圧力8kNで直径7mmに圧縮成型し下記組成の錠剤を得た。なお、造粒物中の水の含有率は、赤外水分計を用いて測定した。

[成 分] [1錠当たりの重量(mg)]
カンデサルタンシレキセチル 2.0
乳糖 92.0
トウモロコシデンプン 20.0
カルメロースカルシウム 4.0
ヒドロキシプロピルセルロース 5.0
クエン酸トリエチル 1.0
(上記添加剤の全体で水2.5mg分を保水)
ステアリン酸マグネシウム 1.0
(1) A solution in which 30.0 g of hydroxypropyl cellulose and 6 g of triethyl citrate are dissolved in 570.0 g of purified water, and 12.0 g of candesartan cilexetil having an average particle size of 11.96 μm is added and uniformly dispersed. Using a high-pressure shearing homogenizer (manufactured by Paulec, Inc .: MICROFLUIDIZER M-110P type), the mixture was uniformly dispersed and wet-pulverized at a pressure of 207 MPa.
(2) 552.0 g of lactose, 120.0 g of corn starch, and 24.0 g of carmellose calcium were put into a fluidized bed granulator (manufactured by Paulek, Inc .: MP-01 type), fluidized, and obtained in (1). The wet pulverized chemical solution was sprayed and granulated. After the chemical solution spraying was finished, it was dried with a fluidized bed dryer until the water content in the granulated product became 2.0% by weight, and then sized with a 24 mesh sieve. 1.0 g of magnesium stearate was added to 129.0 g, which is a part of the obtained sized product, and mixed in a polyethylene bag. Next, this mixture was compression-molded to a diameter of 7 mm at a tableting pressure of 8 kN using a rotary tableting machine (manufactured by Kikusui Seisakusho: VIRGO type) to obtain tablets having the following composition. In addition, the content rate of the water in a granulated material was measured using the infrared moisture meter.

[Components] [Weight per tablet (mg)]
Candesartan cilexetil 2.0
Lactose 92.0
Corn starch 20.0
Carmellose calcium 4.0
Hydroxypropyl cellulose 5.0
Triethyl citrate 1.0
(2.5 mg of water is retained for the whole additive)
Magnesium stearate 1.0

実施例1と同様の操作を行い、造粒物中の水の含有率が2.4重量%の整粒品を得た。得られた整粒品を用いて、以下実施例1と同様に操作し錠剤を得た。   The same operation as in Example 1 was performed to obtain a sized product having a water content of 2.4% by weight in the granulated product. Using the obtained sized product, a tablet was obtained in the same manner as in Example 1 below.

実施例1と同様の操作を行い、造粒物中の水の含有率が2.9重量%の整粒品を得た。得られた整粒品を用いて、以下実施例1と同様に操作し錠剤を得た。   The same operation as in Example 1 was performed to obtain a sized product having a water content of 2.9% by weight in the granulated product. Using the obtained sized product, a tablet was obtained in the same manner as in Example 1 below.

実施例1と同様の操作を行い、造粒物中の水の含有率が3.3重量%の整粒品を得た。得られた整粒品を用いて、以下実施例1と同様に操作し錠剤を得た。   The same operation as in Example 1 was performed to obtain a sized product having a water content of 3.3% by weight in the granulated product. Using the obtained sized product, a tablet was obtained in the same manner as in Example 1 below.

実施例1と同様の操作を行い、造粒物中の水の含有率が5.1重量%の整粒品を得た。得られた整粒品を用いて、以下実施例1と同様に操作し錠剤を得た。   The same operation as in Example 1 was performed to obtain a sized product having a water content of 5.1% by weight in the granulated product. Using the obtained sized product, a tablet was obtained in the same manner as in Example 1 below.

実施例1と同様の操作を行い、造粒物中の水の含有率が8.4重量%の整粒品を得た。得られた整粒品を用いて、以下実施例1と同様に操作し錠剤を得た。   The same operation as in Example 1 was performed to obtain a sized product having a water content of 8.4% by weight in the granulated product. Using the obtained sized product, a tablet was obtained in the same manner as in Example 1 below.

〔比較例〕
実施例1と同様の操作を行い、造粒物中の水の含有率が1.6重量%の整粒品を得た。得られた整粒品を用いて、以下実施例1と同様に操作し錠剤を得た。 [Comparative Example]
The same operation as in Example 1 was performed to obtain a sized product having a water content of 1.6% by weight in the granulated product. Using the obtained sized product, a tablet was obtained in the same manner as in Example 1 below.

〔試験例〕錠剤の苛酷試験による分解物量の測定
実施例及び比較例の錠剤をそれぞれ硝子瓶に入れ、密栓後、温度60℃の条件下に保存した。保存開始から7日および14日経過後、各錠剤中の分解物を高速液体クロマトグラフィーにより測定した。その結果から、それぞれ総分解物量(面積百分率)を算出し、結果を表1に示した。
表1から、本発明に係る実施例の錠剤は、水分含量の少ない比較例と比べ、カンデサルタンシレキセチルを安定に保持し得ることが判った。 [Test Example] Determination of Degradation Amount by Tablet Severe Test Each of the tablets of Examples and Comparative Examples was placed in a glass bottle, sealed, and stored at a temperature of 60 ° C. After 7 days and 14 days from the start of storage, degradation products in each tablet were measured by high performance liquid chromatography. From the results, the total amount of decomposed products (area percentage) was calculated, and the results are shown in Table 1.
From Table 1, it was found that the tablets of the examples according to the present invention can stably hold candesartan cilexetil as compared with the comparative example having a low water content.

本発明によれば、主剤の長期間品質を保証することができるカンデサルタンシレキセチル含有錠剤を医療現場に提供することができる。   ADVANTAGE OF THE INVENTION According to this invention, the candesartan cilexetil containing tablet which can guarantee the long-term quality of a main ingredient can be provided to a medical field.

Claims (10)

カンデサルタンシレキセチル、製剤上の添加物及び組成物全重量に対して2〜10重量%の水分を含有する製剤用組成物を製剤化することにより得られる固形製剤。 A solid preparation obtained by formulating a composition for preparation containing candesartan cilexetil, an additive on the preparation, and water of 2 to 10% by weight relative to the total weight of the composition. 製剤上の添加物が、結合剤及び可塑剤の少なくとも1種である請求項1記載の固形製剤。 The solid preparation according to claim 1, wherein the additive on the preparation is at least one of a binder and a plasticizer. 結合剤がヒドロキシプロピルセルロース又はポリビニルピロリドンであり、可塑剤がクエン酸トリエチル、クエン酸トリブチル、トリアセチン又はグリセリンである請求項1または2記載の固形製剤。 The solid preparation according to claim 1 or 2, wherein the binder is hydroxypropylcellulose or polyvinylpyrrolidone, and the plasticizer is triethyl citrate, tributyl citrate, triacetin or glycerin. 固形製剤が圧縮錠剤である請求項1〜3のいずれかに記載の固形製剤。 The solid preparation according to any one of claims 1 to 3, wherein the solid preparation is a compressed tablet. 固形製剤が口腔内崩壊錠である請求項1〜4のいずれかに記載の固形製剤。 The solid preparation according to any one of claims 1 to 4, wherein the solid preparation is an orally disintegrating tablet. 固形製剤中のカンデサルタンシレキセチルの含有率が0.3〜20重量%である請求項1〜5のいずれかに記載の固形製剤。 The solid preparation according to any one of claims 1 to 5, wherein the content of candesartan cilexetil in the solid preparation is 0.3 to 20% by weight. カンデサルタンシレキセチル、製剤上の添加物及び組成物全重量に対して2〜10重量%の水分を含有する製剤用組成物を製剤化する固形製剤の製造法。 A method for producing a solid preparation, wherein candesartan cilexetil, an additive on the preparation, and a composition for preparation containing 2 to 10% by weight of water based on the total weight of the composition are formulated. 製剤上の添加物が、結合剤及び可塑剤の少なくとも1種である請求項7記載の固形製剤の製造法。 The method for producing a solid preparation according to claim 7, wherein the additive on the preparation is at least one of a binder and a plasticizer. 製剤化が圧縮錠剤である請求項7又は8記載の固形製剤の製造法。 The method for producing a solid preparation according to claim 7 or 8, wherein the preparation is a compressed tablet. 固形製剤中のカンデサルタンシレキセチルの含有率が0.3〜20重量%である請求項7〜9のいずれかに記載の固形製剤の製造法。 The method for producing a solid preparation according to any one of claims 7 to 9, wherein the content of candesartan cilexetil in the solid preparation is 0.3 to 20% by weight.
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Cited By (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2017175855A1 (en) 2016-04-08 2017-10-12 Shionogi & Co., Ltd. Stabilized solid dosage form
WO2021230308A1 (en) 2020-05-15 2021-11-18 塩野義製薬株式会社 Impurity production-inhibited drug composition

Citations (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
JP2008526855A (en) * 2005-01-06 2008-07-24 エラン ファーマ インターナショナル リミテッド Nanoparticulate candesartan formulation
JP2009292843A (en) * 1997-05-27 2009-12-17 Takeda Chem Ind Ltd Solid pharmaceutical preparation
CN101669940A (en) * 2008-09-08 2010-03-17 北京瑞伊人科技发展有限公司 Candesartan cilexetil/hydrochlorothiazide capsule and preparation method thereof
JP2012171954A (en) * 2011-02-24 2012-09-10 Elmed Eisai Kk Stabilized composition of candesartan cilexetil and method for producing the same

Patent Citations (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
JP2009292843A (en) * 1997-05-27 2009-12-17 Takeda Chem Ind Ltd Solid pharmaceutical preparation
JP2008526855A (en) * 2005-01-06 2008-07-24 エラン ファーマ インターナショナル リミテッド Nanoparticulate candesartan formulation
CN101669940A (en) * 2008-09-08 2010-03-17 北京瑞伊人科技发展有限公司 Candesartan cilexetil/hydrochlorothiazide capsule and preparation method thereof
JP2012171954A (en) * 2011-02-24 2012-09-10 Elmed Eisai Kk Stabilized composition of candesartan cilexetil and method for producing the same

Cited By (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2017175855A1 (en) 2016-04-08 2017-10-12 Shionogi & Co., Ltd. Stabilized solid dosage form
WO2021230308A1 (en) 2020-05-15 2021-11-18 塩野義製薬株式会社 Impurity production-inhibited drug composition

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