JP7304691B2 - Tablets containing Zopiclone, its optical isomers, or salts thereof as active ingredients - Google Patents

Tablets containing Zopiclone, its optical isomers, or salts thereof as active ingredients Download PDF

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JP7304691B2
JP7304691B2 JP2018229293A JP2018229293A JP7304691B2 JP 7304691 B2 JP7304691 B2 JP 7304691B2 JP 2018229293 A JP2018229293 A JP 2018229293A JP 2018229293 A JP2018229293 A JP 2018229293A JP 7304691 B2 JP7304691 B2 JP 7304691B2
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hydrogen phosphate
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eszopiclone
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年紀 増田
貴光 龍野
麻衣 鳥山
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Nippon Chemiphar Co Ltd
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本発明は、ゾピクロン、その光学異性体又はこれらの塩の何れかを有効成分として含有する錠剤に関する。 TECHNICAL FIELD The present invention relates to a tablet containing Zopiclone, an optical isomer thereof, or a salt thereof as an active ingredient.

次式、

Figure 0007304691000001
the following formula,
Figure 0007304691000001

で表されるゾピクロン(Zopiclone;(±)6-(5-クロロピリジン-2-イル)-7-オキソ-6,7-ジヒドロ-5H-ピロロ[3,4-b]ピラジン-5-イル 4-メチルピペラジン-1-カルボキシレート;(±)-6-(5-Chloropyridin-2-yl)-7-oxo-6,7-dihydro-5H-pyrrolo[3,4-b]pyrazin-5-yl 4-methylpiperazine-1-carboxylate)、及びその5S体、エスゾピクロン(Eszopiclone)は、ベンゾジアゼピン受容体に結合し、GABA受容体に影響を及ぼすことでGABA系の抑制機構を増強することにより、睡眠改善治療剤として現在、本邦をはじめとして幅広く世界中で使用されている。(特許文献1、非特許文献1及び2)
非特許文献1及び2によれば、これらの有効成分である、原薬のゾピクロン及びエスゾピクロンは、光苛酷試験において、前者は色が微褐色となり、24時間後には4パーセント含量が低下すること、後者も類縁物質が生成することが報告されている。
また、非特許文献1によれば、アモバン(登録商標)錠7.5は、PTP包装下、直射日光下、320時間の苛酷試験において、含量が4%低下し、主光分解物として、類縁物質VIが生成し、不純物Vも増加した旨の記載がある。
一方、非特許文献2によれば、ルネスタ(登録商標)錠1mg,同2mg,同3mgは、無包装下、25℃75%RHの保存安定性試験において、何れも1か月後に水分が増加した旨の記載がある。 Zopiclone represented by (±) 6-(5-chloropyridin-2-yl)-7-oxo-6,7-dihydro-5H-pyrrolo[3,4-b]pyrazin-5-yl 4 -methylpiperazine-1-carboxylate; (±)-6-(5-Chloropyridin-2-yl)-7-oxo-6,7-dihydro-5H-pyrrolo[3,4-b]pyrazin-5-yl 4-methylpiperazine-1-carboxylate), and its 5S form, eszopiclone, improve sleep by binding to benzodiazepine receptors and enhancing the inhibitory mechanism of the GABA system by affecting GABA receptors. As a therapeutic agent, it is now widely used in Japan and around the world. (Patent Document 1, Non-Patent Documents 1 and 2)
According to Non-Patent Documents 1 and 2, the active ingredients of these drug substances, zopiclone and eszopiclone, were found to be slightly brown in color in a light stress test, and the content decreased by 4% after 24 hours. , the latter has also been reported to produce an analogue.
In addition, according to Non-Patent Document 1, Amoban (registered trademark) Tablets 7.5 decreased in content by 4% in a severe test of 320 hours under direct sunlight under PTP packaging, and as the main photodegradant, There is a description that substance VI was produced and impurity V was also increased.
On the other hand, according to Non-Patent Document 2, Lunesta (registered trademark) tablets 1 mg, 2 mg, and 3 mg were subjected to a storage stability test at 25°C and 75% RH without packaging. There is a statement to that effect.

特表平6-504548Special table 6-504548

「アモバン(登録商標)錠7.5、10」のインタビューフォームInterview form for “Amoban (registered trademark) tablets 7.5, 10” 「ルネスタ(登録商標)錠1、2及び3mg」のインタビューフォームInterview form for "Lunesta (registered trademark) tablets 1, 2 and 3 mg"

ゾピクロンやエスゾピクロンを含有する錠剤については、保存安定性試験で、類縁物質等の増大が報告されており、安定な製剤の提供が求められている。
本発明者らは、エスゾピクロンを含有する保存安定性に優れた錠剤に関する鋭意研究を進めた結果、本発明を完成した。 Regarding tablets containing zopiclone or eszopiclone, it has been reported that related substances increased in storage stability tests, and there is a demand for the provision of stable formulations.
The present inventors completed the present invention as a result of extensive research on tablets containing eszopiclone and having excellent storage stability.

即ち、本発明は、
(1)ゾピクロン、その光学異性体又はこれらの塩の何れか1つ、
(2)無水リン酸水素カルシウム、D-マンニトール又は乳糖水和物の少なくとも1つ、
(3)L-メチオニン、硬化油又はショ糖脂肪酸エステルの少なくとも1つを
含有する錠剤に関する。
また、本発明は、エスゾピクロン、無水リン酸水素カルシウム及び硬化油を含有する錠剤に関する。 That is, the present invention
(1) any one of zopiclone, an optical isomer thereof, or a salt thereof;
(2) at least one of anhydrous calcium hydrogen phosphate, D-mannitol or lactose hydrate;
(3) A tablet containing at least one of L-methionine, hydrogenated oil and sucrose fatty acid ester.
The present invention also relates to tablets containing eszopiclone, anhydrous calcium hydrogen phosphate and hydrogenated oil.

本発明の錠剤においては、保存期間中において、類縁物質の増加が抑制される。 In the tablet of the present invention, the increase of related substances is suppressed during the storage period.

図1は、40℃75%RH解放条件における、硬化油の有無による保存安定性の違いを確認した試験結果を表す図である。図中、実線は硬化油非添加製剤(参考製剤A)を、点線は硬化油添加製剤(製剤1)を表し、そして、縦軸は総類縁(%)を、横軸は試験期間(週)を表す。FIG. 1 is a diagram showing test results confirming the difference in storage stability depending on the presence or absence of hydrogenated oil under open conditions of 40° C. and 75% RH. In the figure, the solid line represents the formulation without hydrogenated oil (reference formulation A), the dotted line represents the formulation with hydrogenated oil (formulation 1), the vertical axis represents the total affinity (%), and the horizontal axis represents the test period (weeks). represents 図2は、40℃密栓条件における、安定性試験結果を表す図である。図中、実線は無水リン酸水素カルシウム30%含有製剤(製剤3)を、点線は無水リン酸水素カルシウム45%含有製剤(製剤4)を、1点鎖線は無水リン酸水素カルシウム15%含有製剤(製剤2)を表し、そして縦軸は総類縁(%)を、横軸は試験期間(週)を表す。FIG. 2 is a diagram showing the stability test results under the 40° C. sealed condition. In the figure, the solid line is the preparation containing 30% anhydrous calcium hydrogen phosphate (formulation 3), the dotted line is the preparation containing 45% anhydrous calcium hydrogen phosphate (formulation 4), and the dashed line is the preparation containing 15% anhydrous calcium hydrogen phosphate. (Formulation 2), and the vertical axis represents total affinity (%) and the horizontal axis represents study duration (weeks). 図3は、60℃密栓条件における、安定性試験結果を表す図である。図中、実線は無水リン酸水素カルシウム30%含有製剤(製剤3)を、点線は無水リン酸水素カルシウム45%含有製剤(製剤4)を、1点鎖線は無水リン酸水素カルシウム15%含有製剤(製剤2)を表し、そして縦軸は総類縁(%)を、横軸は試験期間(週)を表す。FIG. 3 is a diagram showing the stability test results under the 60° C. sealed condition. In the figure, the solid line is the preparation containing 30% anhydrous calcium hydrogen phosphate (formulation 3), the dotted line is the preparation containing 45% anhydrous calcium hydrogen phosphate (formulation 4), and the dashed line is the preparation containing 15% anhydrous calcium hydrogen phosphate. (Formulation 2), and the vertical axis represents total affinity (%) and the horizontal axis represents study duration (weeks). 図4は、40℃密栓条件における、安定性試験結果を表す図である。図中、実線は無水リン酸水素カルシウムの内添加(製剤5)を表し、点線は無水リン酸水素カルシウムの外添加(製剤6)を表し、そして縦軸は総類縁(%)を、横軸は試験期間(週)を表す。FIG. 4 is a diagram showing the stability test results under the 40° C. sealed condition. In the figure, the solid line represents the internal addition of anhydrous calcium hydrogen phosphate (Formulation 5), the dotted line represents the external addition of anhydrous calcium hydrogen phosphate (Formulation 6), the vertical axis represents the total affinity (%), and the horizontal axis. represents the test period (weeks). 図5は、60℃密栓条件における、安定性試験結果を表す図である。図中、実線は無水リン酸水素カルシウムの内添加(製剤5)を表し、点線は無水リン酸水素カルシウムの外添加(製剤6)を表し、そして縦軸は総類縁(%)を、横軸は試験期間(週)を表す。FIG. 5 is a diagram showing the stability test results under the 60° C. sealed condition. In the figure, the solid line represents the internal addition of anhydrous calcium hydrogen phosphate (Formulation 5), the dotted line represents the external addition of anhydrous calcium hydrogen phosphate (Formulation 6), the vertical axis represents the total affinity (%), and the horizontal axis. represents the test period (weeks). 図6は、40℃密栓条件における、安定性試験結果を表す図である。図中、実線は製剤7を、点線は製剤8を表し、そして縦軸は総類縁(%)を、横軸は試験期間(週)を表す。FIG. 6 is a diagram showing the stability test results under the 40° C. sealed condition. In the figure, the solid line represents Formulation 7, the dashed line represents Formulation 8, and the vertical axis represents total affinity (%) and the horizontal axis represents study duration (weeks). 図7は、60℃密栓条件における、安定性試験結果を表す図である。図中、実線は製剤7を、点線は製剤8を表し、そして縦軸は総類縁(%)を、横軸は試験期間(週)を表す。FIG. 7 is a diagram showing the stability test results under the 60° C. sealed condition. In the figure, the solid line represents Formulation 7, the dashed line represents Formulation 8, and the vertical axis represents total affinity (%) and the horizontal axis represents study duration (weeks).

以下、本発明について更に詳細に説明する。
(1)本発明は、
(a)ゾピクロン、その光学異性体又はこれらの塩の何れか1つ、
(b)無水リン酸水素カルシウム、D-マンニトール又は乳糖水和物の少なくとも1つ、
(c)L-メチオニン、硬化油又はショ糖脂肪酸エステルの少なくとも1つを
含有する錠剤に関する。
(2)また、本発明は、エスゾピクロン、無水リン酸水素カルシウム及び硬化油を含有する錠剤に関する。
(3)また、本発明は、エスゾピクロンを1錠中、0.5~10mg含有する上記(1)又は(2)記載の錠剤に関する。
(4)また、本発明は、無水リン酸水素カルシウムを錠剤中、5~45%含有する上記(1)~(3)の何れかの項に記載の錠剤に関する。
(5)また、本発明は、無水リン酸水素カルシウムを錠剤中、10~30%含有する上記(1)~(3)の何れかの項に記載の錠剤に関する。
(6)また、本発明は、無水リン酸水素カルシウムのBET表面積が、20m/g以下である上記(1)~(5)の何れかの項に記載の錠剤に関する。
(7)また、本発明は、硬化油を錠剤中、0.5~5%含有する上記(1)~(6)の何れかの項に記載の錠剤に関する。
(8)また、本発明は、さらに賦形剤を含有していても良い上記(1)~(7)の何れかの項に記載の錠剤に関する。
(9)また、本発明は、賦形剤がコムギデンプン、トウモロコシデンプン、乳糖水和物及び結晶セルロースから選択される上記(2)~(8)の何れかの項に記載の錠剤に関する。
(10)また、本発明は、さらに崩壊剤を含有していても良い上記(1)~(9)の何れかの項に記載の錠剤に関する。
(11)また、本発明は、崩壊剤がデンプングリコール酸ナトリウム、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及びL-HPCから選択される上記(10)記載の錠剤に関する。
(12)また、本発明は、さらに結合剤を含有していても良い上記(1)~(11)の何れかの項に記載の錠剤に関する。
(13)また、本発明は、結合剤がHPC及びα化デンプンから選択される上記(12)記載の錠剤に関する。
(14)また、本発明は、さらに滑沢剤を含有していても良い上記(1)~(13)の何れかの項に記載の錠剤に関する。
(15)また、本発明は、滑沢剤が、ステアリン酸マグネシウム、ステアリン酸カルシウム及びフマル酸ステアリルナトリウムから選択される上記(14)記載の錠剤に関する。
(16)また、本発明は、湿式造粒法で製造される上記(1)~(15)の何れかの項に記載の錠剤に関する。
(17)また、本発明は、無水リン酸水素カルシウムが、顆粒外に存在する上記(1)~(16)の何れかの項に記載の錠剤に関する。
(18)さらにまた、本発明は、さらにフィルムコーティングされていても良い上記(1)~(17)の何れかの項に記載の錠剤に関する。 The present invention will be described in more detail below.
(1) The present invention is
(a) any one of zopiclone, an optical isomer thereof or a salt thereof;
(b) at least one of anhydrous calcium hydrogen phosphate, D-mannitol or lactose hydrate;
(c) A tablet containing at least one of L-methionine, hydrogenated oil or sucrose fatty acid ester.
(2) The present invention also relates to tablets containing eszopiclone, anhydrous calcium hydrogen phosphate and hydrogenated oil.
(3) The present invention also relates to the tablet described in (1) or (2) above, which contains 0.5 to 10 mg of eszopiclone per tablet.
(4) The present invention also relates to the tablet according to any one of (1) to (3) above, containing 5 to 45% of anhydrous calcium hydrogen phosphate in the tablet.
(5) The present invention also relates to the tablet according to any one of (1) to (3) above, which contains 10 to 30% of anhydrous calcium hydrogen phosphate in the tablet.
(6) The present invention also relates to the tablet according to any one of (1) to (5) above, wherein the BET surface area of anhydrous calcium hydrogen phosphate is 20 m 2 /g or less.
(7) The present invention also relates to the tablet according to any one of (1) to (6) above, which contains 0.5 to 5% of hydrogenated oil in the tablet.
(8) The present invention also relates to the tablet according to any one of (1) to (7) above, which may further contain an excipient.
(9) The present invention also relates to the tablet according to any one of (2) to (8) above, wherein the excipient is selected from wheat starch, corn starch, lactose hydrate and crystalline cellulose.
(10) The present invention also relates to the tablet according to any one of (1) to (9) above, which may further contain a disintegrant.
(11) The present invention also relates to the tablet according to (10) above, wherein the disintegrant is selected from sodium starch glycolate, carmellose calcium, croscarmellose sodium and L-HPC.
(12) The present invention also relates to the tablet according to any one of (1) to (11) above, which may further contain a binder.
(13) The present invention also relates to the tablet according to (12) above, wherein the binder is selected from HPC and pregelatinized starch.
(14) The present invention also relates to the tablet according to any one of (1) to (13) above, which may further contain a lubricant.
(15) The present invention also relates to the tablet according to (14) above, wherein the lubricant is selected from magnesium stearate, calcium stearate and sodium stearyl fumarate.
(16) The present invention also relates to the tablet according to any one of (1) to (15) above, which is produced by a wet granulation method.
(17) The present invention also relates to the tablet according to any one of (1) to (16) above, wherein the anhydrous calcium hydrogen phosphate is present extragranularly.
(18) Furthermore, the present invention relates to the tablet according to any one of (1) to (17) above, which may be further film-coated.

本発明で用いることができる無水リン酸水素カルシウム以外の賦形剤としては、D-マンニトール、乳糖水和物、コムギデンプン、トウモロコシデンプン、馬鈴薯デンプン、部分α化デンプン、結晶セルロース、ブドウ糖、白糖、果糖、リン酸カルシウム等が挙げられ、好ましくは、D-マンニトール、乳糖水和物、トウモロコシデンプン、結晶セルロースが挙げられ、更に好ましくは結晶セルロースが挙げられる。
本発明で用いることができる崩壊剤としては、カルメロースカルシウム、L-HPC、部分α化デンプン、クロスカルメロースナトリウム、クロスポビドン、ヒドロキシプロピルスターチ、デンプングリコール酸ナトリウム等が挙げられ、好ましくは、カルメロースカルシウム、L-HPC、部分α化デンプンが挙げられる。
本発明で用いることができる結合剤としては、HPC、結晶セルロース、ヒプロメロース、α化デンプン、PVP、ゼラチン、デンプン類等が挙げられ、好ましくは、HPC、結晶セルロース、ヒプロメロース、α化デンプン、PVPが挙げられる。
本発明で用いることができる滑沢剤としては、ステアリン酸マグネシウム、ステアリン酸カルシウム、タルク、フマル酸ステアリルナトリウム、ショ糖脂肪酸エステル等が挙げられ、好ましくは、ステアリン酸マグネシウム、ステアリン酸カルシウム、フマル酸ステアリルナトリウムが挙げられ、更に好ましくはステアリン酸マグネシウムが挙げられる。

本発明の素錠には、さらに流動化剤、界面活性剤、着色剤を含有していても良い。

更に、本発明の錠剤は、フィルムコーティングされていても良い。フィルムコーティング層には、酸化チタン等の遮光剤、三二酸化鉄、黄色三二酸化鉄等の着色剤、PEG,クエン酸トリエチル、トリアセチン等の可塑剤、HPC,ヒプロメロース等のフィルム基剤、カルナウバロウ等の艶出し剤等が使用できる。
エスゾピクロンは苦味を有することが知られおり、フィルムコーティング層、素錠に苦味マスキング剤を添加することもできる。

本発明の錠剤は、顆粒打錠法、直接打錠法(直打法)何れでも使用でき、また普通錠(素錠)の他、フィルムコーティング錠、OD錠であっても良い。
例えば顆粒打錠法では、
(1)エスゾピクロン,賦形剤,崩壊剤,硬化油を混合する。
(2)結合剤溶液により造粒し造粒顆粒を得る。
(3)造粒顆粒を乾燥し、整粒顆粒を得る。
(4)整粒顆粒,無水リン酸水素カルシウム,滑沢剤を混合する。
(5)打錠機で錠剤し錠剤を得る。 Excipients other than anhydrous calcium hydrogen phosphate that can be used in the present invention include D-mannitol, lactose hydrate, wheat starch, corn starch, potato starch, partially pregelatinized starch, crystalline cellulose, glucose, white sugar, Examples include fructose and calcium phosphate, preferably D-mannitol, lactose hydrate, corn starch and crystalline cellulose, and more preferably crystalline cellulose.
Examples of the disintegrant that can be used in the present invention include carmellose calcium, L-HPC, partially pregelatinized starch, croscarmellose sodium, crospovidone, hydroxypropyl starch, sodium starch glycolate and the like, preferably carmellose. Examples include sucrose calcium, L-HPC, and partially pregelatinized starch.
Binders that can be used in the present invention include HPC, crystalline cellulose, hypromellose, pregelatinized starch, PVP, gelatin, starches and the like, and preferably HPC, crystalline cellulose, hypromellose, pregelatinized starch and PVP. mentioned.
Lubricants that can be used in the present invention include magnesium stearate, calcium stearate, talc, sodium stearyl fumarate, sucrose fatty acid esters, etc. Magnesium stearate, calcium stearate and sodium stearyl fumarate are preferred. and more preferably magnesium stearate.

The uncoated tablet of the present invention may further contain a fluidizing agent, a surfactant and a coloring agent.

Furthermore, the tablet of the present invention may be film-coated. The film coating layer contains light-shielding agents such as titanium oxide, coloring agents such as iron sesquioxide and yellow iron sesquioxide, plasticizers such as PEG, triethyl citrate and triacetin, film bases such as HPC and hypromellose, and carnauba wax. Polishing agents and the like can be used.
Eszopiclone is known to have a bitter taste, and a bitterness masking agent can be added to the film coating layer and the uncoated tablet.

The tablet of the present invention can be used by either a granule compression method or a direct compression method (direct compression method), and in addition to ordinary tablets (uncoated tablets), film-coated tablets and OD tablets may also be used.
For example, in the granule tableting method,
(1) Mix eszopiclone, excipients, disintegrant and hydrogenated oil.
(2) Granulation with a binder solution to obtain granules.
(3) Dry the granulated granules to obtain sized granules.
(4) Mix sized granules, anhydrous calcium hydrogen phosphate and lubricant.
(5) Tablets are obtained by tableting with a tableting machine.

本発明のエスゾピクロン製剤において安定化剤としては、硬化油の代わりに、ショ糖脂肪酸エステル、L-メチオニンを使用できる。(実施例1)
本発明のエスゾピクロン製剤において、硬化油が存在すると類縁物質の生成が抑制されることは図1から明らかである。
本発明のエスゾピクロン製剤において、リン酸水素カルシウムの量は、素錠中、10~40%含有することが好ましいが、素錠中、30,40%含有する製剤よりも15%含有する製剤の方が類縁物質の生成が抑制されることは図2,3から判明した。
本発明のエスゾピクロン製剤においてリン酸水素カルシウムの添加は顆粒内よりも顆粒外である方が好ましい。(図4,5)
本発明のエスゾピクロン製剤においてリン酸水素カルシウムの比表面咳はBET表面積が、20m/g以下が好ましい。(図6,7) As a stabilizer in the eszopiclone preparation of the present invention, sucrose fatty acid ester and L-methionine can be used instead of hydrogenated oil. (Example 1)
It is clear from FIG. 1 that in the eszopiclone formulation of the present invention, the presence of hydrogenated oil suppresses the production of related substances.
In the eszopiclone formulation of the present invention, the amount of calcium hydrogen phosphate in the uncoated tablet is preferably 10 to 40%, but the amount of calcium hydrogen phosphate in the uncoated tablet is higher than that of the formulation containing 30 or 40%. 2 and 3 show that the production of analogues is suppressed in the other.
In the eszopiclone formulation of the present invention, the addition of calcium hydrogen phosphate is preferably extragranular rather than intragranular. (Figures 4 and 5)
The BET surface area of calcium hydrogen phosphate in the eszopiclone preparation of the present invention is preferably 20 m 2 /g or less. (Figures 6 and 7)

以下、実施例により本発明をより詳細に説明するが、本発明はこれらに限定されるものではない。
EXAMPLES The present invention will be described in more detail below with reference to Examples, but the present invention is not limited to these.


配合変化試験
エスゾピクロンと添加剤を混合し、60℃密栓下4週間、40℃75%RH4週間における配合変化試験を行った。
類縁物質量はHPLCで測定した。

その結果を表1に記載する。
Blending change test Eszopiclone and additives were mixed and a blending change test was carried out at 60°C for 4 weeks under sealed conditions and at 40°C and 75% RH for 4 weeks.
Amounts of related substances were determined by HPLC.

The results are listed in Table 1.

Figure 0007304691000002
Figure 0007304691000002

表1から明らかなように硬化油、ショ糖脂肪酸エステルは配合変化を起こさないことが明らかになった。
一方、メグルミン、無水クエン酸、酸化マグネシウムは40℃75%RH開放4週間で、配合変化が確認された。
As is clear from Table 1, it was found that hydrogenated oil and sucrose fatty acid ester did not change the composition.
On the other hand, meglumine, anhydrous citric acid, and magnesium oxide were found to change in composition after 4 weeks of exposure to 40°C and 75% RH.


製造方法
エスゾピクロン,結晶セルロース,カルメロースカルシウム,硬化油を混合し、水で溶解したヒドロキシプロピルセルロース溶液により造粒し造粒顆粒を得た。
次いで、造粒顆粒を整粒し,乾燥工程,乾式整粒工程を経て,整粒顆粒を得た。
得られた整粒顆粒,無水リン酸水素カルシウム,軽質無水ケイ酸,ステアリン酸マグネシウムを混合し,ロータリー打錠機で錠剤質量が100mgの表2の錠剤(製剤1)を得た。
Production method Eszopiclone, crystalline cellulose, carmellose calcium and hardened oil were mixed and granulated with a hydroxypropylcellulose solution dissolved in water to obtain granules.
Next, the granulated granules were sized, and through a drying process and a dry sizing process, sized granules were obtained.
The obtained sized granules, anhydrous calcium hydrogen phosphate, light anhydrous silicic acid, and magnesium stearate were mixed, and tablets (formulation 1) shown in Table 2 having a tablet weight of 100 mg were obtained with a rotary tableting machine.

Figure 0007304691000003
Figure 0007304691000003

安定性試験
実施例1で得られた製剤1及び下記表3の参考製剤Aについて、40℃75%RH開放条件における4週間の保存安定性試験を行った。

参考製剤A Stability Test Formulation 1 obtained in Example 1 and Reference Formulation A in Table 3 below were subjected to a storage stability test at 40° C. and 75% RH open conditions for 4 weeks.

Reference formulation A

Figure 0007304691000004
Figure 0007304691000004


(参考製剤Aの製造方法)
エスゾピクロン,結晶セルロース,カルメロースカルシウムを混合し、水で溶解したヒドロキシプロピルセルロース溶液により造粒し造粒顆粒を得た。
次いで、造粒顆粒を整粒し,乾燥工程,乾式整粒工程を経て,整粒顆粒を得た。
得られた整粒顆粒,無水リン酸水素カルシウム,軽質無水ケイ酸,ステアリン酸マグネシウムを混合し,ロータリー打錠機で錠剤質量が100mgの錠剤を得た。
(Manufacturing method of reference formulation A)
Eszopiclone, crystalline cellulose and carmellose calcium were mixed and granulated with a hydroxypropylcellulose solution dissolved in water to obtain granules.
Next, the granulated granules were sized, and through a drying process and a dry sizing process, sized granules were obtained.
The obtained sized granules, anhydrous calcium hydrogen phosphate, light anhydrous silicic acid and magnesium stearate were mixed and tablets with a tablet weight of 100 mg were obtained by a rotary tableting machine.

試験結果
下記の方法で試験を行い、その試験結果を図1に示す。
図1から明らかなように硬化油を配合することで、類縁物質の生成が抑制されることが明らかになった。

(測定方法)
本品を粉末とし、エスゾピクロン10mgに対応する量をとり、pH4.0のリン酸塩溶液/アセトニトリル(62:38)20mLを加えて5分間超音波処理をした後、孔径0.45μm以下のメンブランフィルターでろ過する。初めのろ液2mLを除き、次のろ液を試料溶液とする。この液1mLを正確に量り、pH4.0のリン酸塩溶液/アセトニトリル(62:38)を加えて正確に100mLとし、標準溶液とする。試料溶液及び標準溶液10μLずつを正確にとり、次の条件で液体クロマトグラフィー(HPLC)により試験を行う。 Test Results Tests were carried out by the following methods, and the test results are shown in FIG.
As is clear from FIG. 1, it was found that the addition of hydrogenated oil suppressed the generation of related substances.

(Measuring method)
Powder this product, take an amount corresponding to 10 mg of eszopiclone, add 20 mL of pH 4.0 phosphate solution/acetonitrile (62:38), sonicate for 5 minutes, then Filter through a membrane filter. Remove the first 2 mL of the filtrate and use the next filtrate as the sample solution. Accurately measure 1 mL of this solution, add pH 4.0 phosphate solution/acetonitrile (62:38) to make exactly 100 mL, and use it as a standard solution. Accurately take 10 μL each of the sample solution and the standard solution, and perform the test by liquid chromatography (HPLC) under the following conditions.

(HPLC条件)
検出器:紫外吸光光度計(測定波長:303nm)
カラム:内径4.6mm、長さ15cmのステンレス管に5μmの液体クロマトグラフィー用オクタデシルシリル化シリカゲルを充填する。
カラム温度:30℃付近の一定温度
移動相A:pH4.0のリン酸塩溶液
移動相B:アセトニトリル
移動相の送液:移動相A及び移動相Bの混合比を次のように変えて濃度勾配制御する。 (HPLC conditions)
Detector: UV absorption photometer (measurement wavelength: 303 nm)
Column: A stainless steel tube with an inner diameter of 4.6 mm and a length of 15 cm is packed with 5 μm octadecylsilylated silica gel for liquid chromatography.
Column temperature: Constant temperature around 30°C Mobile phase A: pH 4.0 phosphate solution Mobile phase B: Acetonitrile Gradient control.

Figure 0007304691000005
Figure 0007304691000005

無水リン酸水素カルシウムの含有量の違いによる保存安定性の違い

製造方法
エスゾピクロン,結晶セルロース,無水リン酸水素カルシウム,クロスカルメロースナトリウム,硬化油を混合し、水で溶解したヒドロキシプロピルセルロース溶液により造粒し造粒顆粒を得た。
次いで、造粒顆粒を整粒し,乾燥工程,乾式整粒工程を経て,整粒顆粒を得た.
得られた整粒顆粒,無水リン酸水素カルシウム,軽質無水ケイ酸,ステアリン酸マグネシウムを混合し,錠剤質量が100mgとなるようにロータリー打錠機で打錠し、表5の製剤2,3,4を得た。 Differences in storage stability due to differences in the content of anhydrous calcium hydrogen phosphate

Production method Eszopiclone, crystalline cellulose, anhydrous calcium hydrogen phosphate, croscarmellose sodium and hydrogenated oil were mixed and granulated with a hydroxypropylcellulose solution dissolved in water to obtain granules.
Next, the granulated granules were sized, and through a drying process and a dry sizing process, sized granules were obtained.
The obtained sized granules, anhydrous calcium hydrogen phosphate, light anhydrous silicic acid and magnesium stearate were mixed and tableted with a rotary tableting machine so that the tablet weight was 100 mg. Got 4.

Figure 0007304691000006
Figure 0007304691000006


試験方法
実施例3の試験方法と同様な方法で試験を行った。

試験結果
試験結果を図2,3に記載する。
図2,3から明らかなように、無水リン酸水素カルシウムを15%含有する製剤が類縁物質の生成が抑制された。
Test method The test was conducted in the same manner as the test method of Example 3.

Test results
The test results are shown in Figures 2 and 3.
As is clear from FIGS. 2 and 3, the formulation containing 15% anhydrous calcium hydrogen phosphate inhibited the production of related substances.

無水リン酸水素カルシウムの添加方法の違いによる保存安定性の違

製剤5の製造方法(造粒まで)
エスゾピクロン,結晶セルロース,無水リン酸水素カルシウム,クロスカルメロースナトリウム,硬化油を混合し、水で溶解したヒドロキシプロピルセルロース溶液により造粒し造粒顆粒を得た。

製剤6の製造方法(造粒まで)
エスゾピクロン,結晶セルロース,クロスカルメロースナトリウム,硬化油を混合し、水で溶解したヒドロキシプロピルセルロース溶液により造粒し造粒顆粒を得た。

造粒後(共通)
造粒顆粒を整粒し,乾燥工程,乾式整粒工程を経て,整粒顆粒を得た.
得られた整粒顆粒と後末部を混合し、ロータリー打錠機にて、質量が100mgの表6の錠剤5,6を得た。 Differences in storage stability due to differences in the addition method of anhydrous calcium hydrogen phosphate

Manufacturing method of formulation 5 (up to granulation)
Eszopiclone, crystalline cellulose, anhydrous calcium hydrogen phosphate, croscarmellose sodium and hydrogenated oil were mixed and granulated with a hydroxypropylcellulose solution dissolved in water to obtain granules.

Manufacturing method of formulation 6 (up to granulation)
Eszopiclone, crystalline cellulose, croscarmellose sodium and hydrogenated oil were mixed and granulated with a hydroxypropylcellulose solution dissolved in water to obtain granules.

After granulation (common)
The granulated granules were sieved, dried, and dried to obtain sieved granules.
The obtained sieved granules and the rear portion were mixed, and tablets 5 and 6 of Table 6 having a mass of 100 mg were obtained with a rotary tableting machine.

Figure 0007304691000007
Figure 0007304691000007

試験方法
実施例3の試験方法と同様な方法で試験を行った。

試験結果
試験結果を図4,5に記載する。
図4,5から明らかなように、無水リン酸水素カルシウムを後末添加した製剤の方が、顆粒内に存在する製剤に比べ、保存安定性が優れていた。
Test Method The test was performed in the same manner as the test method of Example 3.

Test results The test results are shown in Figures 4 and 5.
As is clear from FIGS. 4 and 5, the preparation with post-addition of anhydrous calcium hydrogen phosphate had better storage stability than the preparation with intragranular content.

無水リン酸水素カルシウムの比表面積の違いによる保存安定性の相違

製造方法
エスゾピクロン,結晶セルロース,無水リン酸水素カルシウム,クロスカルメロースナトリウム,硬化油を混合し、水で溶解したヒドロキシプロピルセルロース溶液により造粒し造粒顆粒を得た。
次いで、造粒顆粒を整粒し,乾燥工程,乾式整粒工程を経て,整粒顆粒を得た。
得られた整粒顆粒と後末(ステアリン酸マグネシウム)を混合し,ロータリー打錠機で質量が100mgの表7の製剤7,8を得た。 Difference in storage stability due to difference in specific surface area of anhydrous calcium hydrogen phosphate

Production method
Eszopiclone, crystalline cellulose, anhydrous calcium hydrogen phosphate, croscarmellose sodium and hydrogenated oil were mixed and granulated with a hydroxypropylcellulose solution dissolved in water to obtain granules.
Next, the granulated granules were sized, and through a drying process and a dry sizing process, sized granules were obtained.
The obtained sieved granules and the powder (magnesium stearate) were mixed, and formulations 7 and 8 of Table 7 having a mass of 100 mg were obtained with a rotary tableting machine.

Figure 0007304691000008
Figure 0007304691000008


製剤7,8は表8の物性値を有する無水リン酸水素カルシウムを使用した。

無水リン酸水素カルシウムの物性値
Formulations 7 and 8 used anhydrous calcium hydrogen phosphate having physical properties shown in Table 8.

Physical properties of anhydrous calcium hydrogen phosphate

Figure 0007304691000009
Figure 0007304691000009


試験方法
実施例3の試験方法と同様な方法で試験を行った。

試験結果
試験結果を図6,7に記載する。
図6,7から明らかなように比表面積の小さい無水リン酸水素カルシウムが大きなものに比べ、保存安定性が優れていた。
Test Method The test was performed in the same manner as the test method of Example 3.

Test results The test results are shown in Figures 6 and 7.
As is clear from FIGS. 6 and 7, the storage stability was superior to that of anhydrous calcium hydrogen phosphate having a small specific surface area and having a large specific surface area.

本発明の錠剤は、保存期間中において、類縁物質の増加が抑制され、エスゾピクロンの錠剤として使用できる。 The tablet of the present invention can be used as a tablet of eszopiclone because the increase of related substances is suppressed during the storage period.

Claims (13)

顆粒を含有する普通錠であって、
(a)ゾピクロン、その光学異性体又はこれらの塩の何れか1つ、
(b)無水リン酸水素カルシウム、
(c)硬化油、ショ糖脂肪酸エステル又はL-メチオニンの少なくとも1つ
を含有し、そして
(b)を普通錠中、10~30%含有し、
(b)のBET表面積が、20m/g以下で、
(a)及び(c)が顆粒内に存在し、(b)が、顆粒外に存在する普通錠。 A plain tablet containing granules,
(a) any one of zopiclone, an optical isomer thereof or a salt thereof;
(b) anhydrous calcium hydrogen phosphate;
(c) at least one of hydrogenated oil, sucrose fatty acid ester or L-methionine ;
and
(b) is contained at 10 to 30% in ordinary tablets,
(b) has a BET surface area of 20 m 2 /g or less,
A plain tablet in which (a) and (c) are intragranular and (b) is extragranular. エスゾピクロン、無水リン酸水素カルシウム及び硬化油を含有する請求項1記載の普通錠。 The plain tablet according to claim 1, which contains eszopiclone, anhydrous calcium hydrogen phosphate and hydrogenated oil. エスゾピクロンを1錠中、0.5~10mg含有する請求項1又は2記載の普通錠。 The plain tablet according to claim 1 or 2, wherein one tablet contains 0.5 to 10 mg of eszopiclone. 硬化油を普通錠中、0.5~5%含有する請求項1~3の何れかの項に記載の普通錠。 The plain tablet according to any one of claims 1 to 3, which contains 0.5 to 5% of hydrogenated oil in the plain tablet. さらに賦形剤を含有している請求項1~4の何れかの項に記載の普通錠。 The plain tablet according to any one of claims 1 to 4, further comprising an excipient. 賦形剤がコムギデンプン、トウモロコシデンプン、乳糖水和物又は結晶セルロースから選択される請求項2~5の何れかの項に記載の普通錠。 The plain tablet according to any one of claims 2 to 5, wherein the excipient is selected from wheat starch, corn starch, lactose hydrate or microcrystalline cellulose. さらに崩壊剤を含有している請求項1~6の何れかの項に記載の普通錠。 The plain tablet according to any one of claims 1 to 6, further comprising a disintegrant. 崩壊剤がデンプングリコール酸ナトリウム、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又はL-HPCから選択される請求項7記載の普通錠。 The plain tablet according to claim 7, wherein the disintegrant is selected from sodium starch glycolate, carmellose calcium, croscarmellose sodium or L-HPC. さらに結合剤を含有している請求項1~8の何れかの項に記載の普通錠。 The plain tablet according to any one of claims 1 to 8, further comprising a binder. 結合剤がHPC又はα化デンプンから選択される請求項9記載の普通錠。 Plain tablet according to claim 9, wherein the binder is selected from HPC or pregelatinized starch. さらに滑沢剤を含有していても良い請求項1~10の何れかの項に記載の普通錠。 The plain tablet according to any one of claims 1 to 10, which may further contain a lubricant. 滑沢剤が、ステアリン酸マグネシウム、ステアリン酸カルシウム又はフマル酸ステアリルナトリウムから選択される請求項11記載の普通錠。 12. Plain tablet according to claim 11, wherein the lubricant is selected from magnesium stearate, calcium stearate or sodium stearyl fumarate. さらにフィルムコーティングされている請求項1~12の何れかの項に記載の錠剤。 The tablet according to any one of claims 1 to 12, which is further film-coated.
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