JPH11335286A - Effect-reinforcing medicament for dopamine antagonist - Google Patents
Effect-reinforcing medicament for dopamine antagonistInfo
- Publication number
- JPH11335286A JPH11335286A JP14304998A JP14304998A JPH11335286A JP H11335286 A JPH11335286 A JP H11335286A JP 14304998 A JP14304998 A JP 14304998A JP 14304998 A JP14304998 A JP 14304998A JP H11335286 A JPH11335286 A JP H11335286A
- Authority
- JP
- Japan
- Prior art keywords
- pyrrolidinone
- chlorophenyl
- methoxyethyl
- dopamine antagonist
- methyl
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
- Pending
Links
Landscapes
- Pyrrole Compounds (AREA)
- Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
Abstract
Description
【0001】[0001]
【発明の属する技術分野】本発明は、ドーパミン拮抗薬
の効果増強剤および/または副作用軽減剤に関するもの
である。TECHNICAL FIELD The present invention relates to a dopamine antagonist effect enhancer and / or a side effect reducer.
【0002】[0002]
【従来の技術】ドーパミン拮抗薬は、精神分裂病、躁
病、うつ病、精神薄弱、老年精神病、神経症、自閉性障
害や精神遅滞に伴う各種症状、胃潰瘍、十二指腸潰瘍、
術前術後の悪心や嘔吐、糖尿病性等の疼痛、メニエル症
候群等の治療上有用な薬物である。2. Description of the Related Art Dopamine antagonists include schizophrenia, mania, depression, mental retardation, geriatric psychiatry, neurosis, various symptoms associated with autism and mental retardation, gastric ulcer, duodenal ulcer,
It is a useful drug for the treatment of preoperative and postoperative nausea and vomiting, pain such as diabetic, and Meniere's syndrome.
【0003】しかし、これら薬物の服用により、例えば
精神分裂病の治療においては、約90%の服薬患者にパ
ーキンソンニスム等の錘体外路症状(行動薬理学的には
カタレプシー)が発現(Calev,Br.J.Psychiatry,187,19
83)し、50%以上の患者で服薬中断の原因となってい
る(Casey,Int.Clin.Psychopharmacol.,207,1995)。However, by taking these drugs, for example, in the treatment of schizophrenia, extrapyramidal symptoms such as parkinsonism (catalepsy in behavioral pharmacology) are expressed in about 90% of patients who take the drug (Calev, Br.). .J.Psychiatry, 187,19
83) and causes drug discontinuation in more than 50% of patients (Casey, Int. Clin. Psychopharmacol., 207, 1995).
【0004】これを予防するために、抗精神病薬の治療
開始時には抗コリン作用のある抗パーキンソン薬を併用
するのが普通である。しかしながら、抗パーキンソン薬
の併用により、便秘、口渇、消化器症状等、さらに遅発
性ジスキネジアや巨大結腸症等の慢性副作用が増強する
可能性が指摘されている。[0004] To prevent this, it is common to use an anti-cholinergic anti-Parkinson drug at the beginning of the treatment with an anti-psychotic drug. However, it has been pointed out that concomitant use of anti-Parkinson drugs may enhance chronic side effects such as constipation, dry mouth, digestive symptoms, and even late onset dyskinesia and macrocolon.
【0005】さらにクロルプロマジンやハロペリドール
等のドーパミン拮抗薬は、認知機能を悪化させることが
問題視されている(Cohen & ServanSchreiber,Schizoph
r.Bull.,395,1993 ; Gallhofer,J.Pract.Psychiatr.Be
hav.Health,16,1996)。[0005] Further, it has been considered that dopamine antagonists such as chlorpromazine and haloperidol deteriorate cognitive functions (Cohen & Servan Schreiber, Schizoph.
r.Bull., 395,1993; Gallhofer, J.Pract.Psychiatr.Be
hav. Health, 16, 1996).
【0006】加えて錘体外路性副作用の治療に用いた抗
コリン剤が、相当な記憶障害を引き起こすとの報告もあ
る(Tune,Am.J.Psychiatry,34,1982 ; Calev,Br.J.Psych
iatry,422,1983)。[0006] In addition, it has been reported that anticholinergic agents used for treating extrapyramidal side effects cause considerable memory impairment (Tune, Am. J. Psychiatry, 34, 1982; Calev, Br. J. Psych
iatry, 422, 1983).
【0007】これらの経験が契機となって、錘体外路性
副作用の軽減、あるいは認知機能障害をさらに悪化させ
ることのない薬剤の開発が望まれているが、いまだ有効
な薬物はない。米国特許4767759、特開平7−2
52219号公報および特開平9−40667号公報に
ピロリジノン誘導体が開示されているが、ドーパミン拮
抗薬に対する効果増強、副作用軽減作用についての記載
はない。[0007] These experiences have led to a desire to reduce the extrapyramidal side effects or to develop drugs that do not further exacerbate cognitive dysfunction, but there are still no effective drugs. U.S. Pat. No. 4,767,759, JP-A-7-2
JP-A-52219 and JP-A-9-40667 disclose pyrrolidinone derivatives, but do not describe the effect of enhancing dopamine antagonists or reducing side effects.
【0008】[0008]
【発明が解決しようとする課題】本発明の目的は、ドー
パミン拮抗薬の効果を増強させ、副作用を軽減させる薬
剤を提供することにある。An object of the present invention is to provide a drug which enhances the effect of a dopamine antagonist and reduces side effects.
【0009】[0009]
【課題を解決するための手段】本発明者等は、ドーパミ
ン拮抗薬の副作用を軽減させ、ドーパミン拮抗薬の効果
を増強する化合物を見いだし、ドーパミン拮抗薬を用い
る疾患に対してより効果的な治療剤としての本発明を完
成するに至った。Means for Solving the Problems The present inventors have found compounds that reduce the side effects of dopamine antagonists and enhance the effects of dopamine antagonists, and provide more effective treatment for diseases using dopamine antagonists. The present invention as an agent has been completed.
【0010】すなわち、本発明は、[1] 1−(4−
クロロフェニル)−3−[4−(2−メトキシエチル)
ピペラジン−1−イル]メチル−2−ピロリジノン、ま
たはその薬理学的に許容される塩およびその薬理学的に
許容される塩の水和物を有効成分として含有してなるド
ーパミン拮抗薬の効果増強剤であり、また、[2] 1
−(4−クロロフェニル)−3−[4−(2−メトキシ
エチル)ピペラジン−1−イル]メチル−2−ピロリジ
ノンの絶対配置がRである上記[1]記載のドーパミン
拮抗薬の効果増強剤であり、また、[3] ドーパミン
拮抗薬がD2受容体遮断薬である上記[2]記載のドー
パミン拮抗薬の効果増強剤であり、また、[4] ドー
パミン拮抗薬の効果増強剤が、錠剤、顆粒剤、散剤、懸
濁剤、乳化剤、カプセル剤、またはシロップ剤の経口投
与剤、注射剤、座剤または輸液用等張液である上記
[1]から[3]記載のドーパミン拮抗薬の効果増強剤
であり、また、[5] 1−(4−クロロフェニル)−
3−[4−(2−メトキシエチル)ピペラジン−1−イ
ル]メチル−2−ピロリジノン、またはその薬理学的に
許容される塩およびその薬理学的に許容される塩の水和
物を有効成分として含有してなるドーパミン拮抗薬の副
作用軽減剤であり、また、[6] 1−(4−クロロフ
ェニル)−3−[4−(2−メトキシエチル)ピペラジ
ン−1−イル]メチル−2−ピロリジノンの絶対配置が
Rである上記[5]記載のドーパミン拮抗薬の副作用軽
減剤であり、また、[7] ドーパミン拮抗薬がD2受
容体遮断薬である上記[6]記載のドーパミン拮抗薬の
副作用軽減剤であり、また、[8] ドーパミン拮抗薬
の副作用軽減剤が、錠剤、顆粒剤、散剤、懸濁剤、乳化
剤、カプセル剤、またはシロップ剤の経口投与剤、注射
剤、座剤または輸液用等張液である上記[5]から
[7]記載のドーパミン拮抗薬の副作用軽減剤に関する
ものである。That is, the present invention relates to [1] 1- (4-
Chlorophenyl) -3- [4- (2-methoxyethyl)
[Piperazin-1-yl] methyl-2-pyrrolidinone, or a pharmacologically acceptable salt thereof, and an enhanced effect of a dopamine antagonist comprising a hydrate of the pharmacologically acceptable salt thereof as an active ingredient And [2] 1
The dopamine antagonist effect enhancer according to the above [1], wherein the absolute configuration of-(4-chlorophenyl) -3- [4- (2-methoxyethyl) piperazin-1-yl] methyl-2-pyrrolidinone is R. And [3] the dopamine antagonist is the dopamine antagonist effect enhancer according to the above [2], wherein the dopamine antagonist is a D2 receptor blocker; and [4] the dopamine antagonist effect enhancer is a tablet, The effect of the dopamine antagonist according to the above [1] to [3], which is an oral administration preparation, injection, suppository or infusion for granules, powders, suspensions, emulsifiers, capsules or syrups, injections, suppositories or infusions. And [5] 1- (4-chlorophenyl)-
3- [4- (2-methoxyethyl) piperazin-1-yl] methyl-2-pyrrolidinone, or a pharmacologically acceptable salt thereof, or a hydrate of a pharmacologically acceptable salt thereof, as an active ingredient [6] 1- (4-Chlorophenyl) -3- [4- (2-methoxyethyl) piperazin-1-yl] methyl-2-pyrrolidinone Is a side effect reducer of the dopamine antagonist according to the above [5], wherein the absolute configuration of R is R, and [7] the side effect of the dopamine antagonist according to the above [6], wherein the dopamine antagonist is a D2 receptor blocker. [8] a dopamine antagonist, which is a side effect reducer; a tablet, granule, powder, suspension, emulsifier, capsule, or syrup for oral administration, injection, suppository, or infusion; for A isotonic solution relates agents to attenuate any adverse effects of dopamine antagonists [7], wherein the above [5].
【0011】[0011]
【発明の実施の形態】本発明についてさらに詳しく説明
する。DETAILED DESCRIPTION OF THE INVENTION The present invention will be described in more detail.
【0012】本発明の化合物の塩類としては、医薬とし
て許容される塩であれば特に制限はなく、例えば、塩酸
塩、硫酸塩、燐酸塩、臭化水素酸塩、フマル酸塩、マレ
イン酸塩、酒石酸塩、メタンスルホン酸塩、ベンゼンス
ルホン酸塩、パラトルエンスルホン酸塩、シュウ酸塩、
マンデル酸塩、クエン酸塩、乳酸塩、コハク酸等が挙げ
られる。また、これらの塩を合成するに当たり、用いる
酸に不斉炭素がある場合は光学活性体を用いることもで
きる。The salts of the compound of the present invention are not particularly limited as long as they are pharmaceutically acceptable salts. Examples thereof include hydrochloride, sulfate, phosphate, hydrobromide, fumarate, and maleate. , Tartrate, methanesulfonate, benzenesulfonate, paratoluenesulfonate, oxalate,
Mandelate, citrate, lactate, succinic acid, and the like. In synthesizing these salts, when the acid used has an asymmetric carbon, an optically active substance can also be used.
【0013】次に本発明化合物の効果増強、副作用軽減
の対象となるドーパミン拮抗薬は、ドーパミンの作用に
拮抗する薬剤であれば特に制限はなく、例えば、リスペ
リドン(risperidone)、オランザピン(oranzapine、LY17
0053)、SM-9018、ケチアピン(quetiapine、ICI-204,63
6)、アリピラゾール(aripirazole、OPC-14597)、セルチ
ンドール(sertindole、S-1991)、AD-5423、ジプラシド
ン(CP-88059、ziprasidone)、SM-13496、ファナンセリ
ン(fananserin、RP-62,203)、クロザピン(clozapine)、
クロルプロマジン(chlorpromazine)、フルフェナジン(f
luphenazine)、レボメプロマジン(levomepromazine)、
ペラジン(perazine)、ペルフェナジン(perphenazine)、
プロクロルペラジン(prochlorperazine)、プロペリシア
ジン(propericiazine)、トリフルオペラジン(trifluope
razine)、チオリダジン(thioridazine)、チオチキセン
(thiothixene)、ブロンペリドール(bromperidol)、フロ
ロピパミド(floropipamide)、ハロペリドール(haloperi
dol)、モペロン(moperone)、ピモジド(pimozide)、スピ
ペロン(spiperone)、チミペロン(timiperone)、ネモナ
プリド(nemonapride)、スルピリド(sulpiride)、スルト
プリド(sultopride)、カルピラミン(carpiramine)、ク
ロカプラミン(clocapramine)、クロチアピン(clotiapin
e)、モサプラミン(mosapramine)、オキシペルチン(oxyp
ertine)、ゾテピン(zotepine)等が挙げられる。The dopamine antagonist to be used for enhancing the effects of the compound of the present invention and reducing side effects is not particularly limited as long as it is a drug that antagonizes the action of dopamine. For example, risperidone, olanzapine (oranzapine, LY17)
0053), SM-9018, quetiapine (ICI-204, 63
6), aripirazole (aripirazole, OPC-14597), sertindole (sertindole, S-1991), AD-5423, ziprasidone (CP-88059, ziprasidone), SM-13496, fananserin (fananserin, RP-62,203) , Clozapine,
Chlorpromazine, fluphenazine (f
luphenazine), levomepromazine,
Perazine, perphenazine,
Prochlorperazine, Propericiazine, Trifluoperazine
razine), thioridazine, thiothixene
(thiothixene), bromperidol, floropipamide, haloperidol
dol), moperone (moperone), pimozide (pimozide), spiperone (spiperone), timiperone (timiperone), nemonapride (nemonapride), sulpiride (sulpiride), sultopride (sultopride), carpiramine (carpiramine), clocapramine (clocapramine), clocapramine clotiapin
e), mosapramine, oxypertin (oxyp
ertine), zotepine and the like.
【0014】製剤化は公知の方法によって可能である。
剤形としては、各種の形態が治療目的に応じて選択で
き、その代表的なものとして固形製剤、液剤、その他座
剤等が挙げられる。具体的には、次のような各種製剤で
ある。すなわち、固形製剤としては、錠剤、丸剤、散
剤、顆粒剤、カプセル剤等、液剤としては、溶液として
の注射剤の他、懸濁剤、シロップ剤、乳剤等、その他の
製剤としては、座剤等である。[0014] Formulation can be performed by a known method.
As the dosage form, various forms can be selected according to the purpose of treatment, and representative examples thereof include solid preparations, liquid preparations, and other suppositories. Specifically, there are the following various preparations. That is, as solid preparations, tablets, pills, powders, granules, capsules, etc., as liquid preparations, in addition to injections as solutions, suspensions, syrups, emulsions, etc. Agent and the like.
【0015】錠剤の形態に成形するに際しては、担体と
してこの分野で従来よりよく知られているものを広く使
用することができる。その例としては、乳糖、白糖、ブ
ドウ糖、尿素、デンプン、炭酸カルシウム、カオリン、
結晶セルロース、ケイ酸等の賦形剤、水、エタノール、
プロパノール、単シロップ、ブドウ糖液、デンプン液、
ゼラチン液、セラック液、メチルセルロース溶液、ヒド
ロキシプロピルセルロース溶液、ポリビニルピロリドン
溶液、カルボキシメチルセルロース溶液等の結合剤、乾
燥デンプン、アルギン酸ナトリウム、カンテン末、炭酸
水素ナトリウム、炭酸カルシウム、ポリオキシエチレン
ソルビタン脂肪酸エステル類、ラウリルナトリウム、ス
テアリン酸グリセリド、デンプン、乳糖等の崩壊剤、白
糖、ステアリン酸、カカオバター、水素添加油等の崩壊
抑制剤、第4級アンモニウム塩基、ラウリル硫酸ナトリ
ウム等の吸収促進剤、グリセリン、デンプン等の保湿
剤、デンプン、乳糖、カオリン、ベントナイト、コロイ
ド状ケイ酸、結晶性セルロース、軽質無水ケイ酸等の吸
着剤、タルク、ステアリン酸塩、ホウ酸末、ポリエチレ
ングリコール等の滑沢剤等である。[0015] In the case of molding into a tablet form, carriers well known in the art can be widely used as carriers. Examples include lactose, sucrose, glucose, urea, starch, calcium carbonate, kaolin,
Excipients such as crystalline cellulose and silicic acid, water, ethanol,
Propanol, simple syrup, glucose solution, starch solution,
Gelatin solution, shellac solution, methylcellulose solution, hydroxypropylcellulose solution, polyvinylpyrrolidone solution, binder such as carboxymethylcellulose solution, dried starch, sodium alginate, agar powder, sodium hydrogencarbonate, calcium carbonate, polyoxyethylene sorbitan fatty acid esters, Disintegrators such as sodium lauryl, stearic acid glyceride, starch, lactose, disintegration inhibitors such as sucrose, stearic acid, cocoa butter, hydrogenated oil, quaternary ammonium bases, absorption promoters such as sodium lauryl sulfate, glycerin, starch Sorbents such as starch, lactose, kaolin, bentonite, colloidal silicic acid, crystalline cellulose, light anhydrous silicic acid, etc .; lubricants such as talc, stearate, boric acid powder, polyethylene glycol, etc. It is an agent, and the like.
【0016】さらに錠剤の場合、必要に応じ通常の剤皮
を施した錠剤、例えば糖衣錠、ゼラチン被包錠、腸溶被
錠、フィルムコーティング錠あるいは二層錠、多層錠と
することができる。Further, in the case of tablets, tablets which have been coated with a usual coating, if necessary, such as sugar-coated tablets, gelatin-encapsulated tablets, enteric-coated tablets, film-coated tablets or two-layer tablets or multilayer tablets, can be prepared.
【0017】丸剤の形態に成形するに際しては、担体と
して従来この分野で公知のものを広く使用できる。その
例としては、例えば乳糖、デンプン、結晶セルロース、
カカオ脂、硬化植物油、カオリン、タルク等の賦形剤、
アラビアゴム末、トラガント末、ゼラチン等の結合剤、
カルメロースカルシウム、カンテン等の崩壊剤等を挙げ
ることができる。In molding into the form of pills, a wide variety of carriers conventionally known in this field can be used. Examples include lactose, starch, microcrystalline cellulose,
Excipients such as cocoa butter, hardened vegetable oil, kaolin, talc,
Gum arabic powder, tragacanth powder, binders such as gelatin,
Disintegrators such as carmellose calcium, agar and the like can be mentioned.
【0018】カプセル剤は、常法に従い通常有効成分化
合物を上記で例示した各種の担体と混合して硬質ゼラチ
ンカプセル、軟質カプセル等に充填して調製される。Capsules are prepared by mixing the active ingredient compound with the various carriers exemplified above and filling the mixture into hard gelatin capsules, soft capsules and the like according to a conventional method.
【0019】注射剤として調製する場合、液剤、乳剤お
よび懸濁剤の形態に成形するに際しては、希釈剤として
この分野において汎用されているもの、例えば水、エタ
ノール、マクロゴール、プロピレングリコール、エトキ
シ化イソステアリルアルコール、ポリオキシ化イソステ
アリルアルコール、ポリオキシエチレンソルビタン脂肪
酸エステル類、綿実油、トウモロコシ油、ラッカセイ
油、オリーブ油等が使用できる。さらに本発明の化合物
に水を加え、適切な界面活性剤の存在下に懸濁性水溶
液、さらにはポリオキシエチレン硬化ヒマシ油(HCO
−60)、ポリソルベート80、ポリエチレングリコー
ル等の界面活性剤を用いた乳濁液として調製することが
できる。なお、食塩、ブドウ糖あるいはグリセリンを医
薬製剤中に含有させてもよく、また通常の溶解補助剤、
緩衝剤、無痛化剤等を添加してもよい。When prepared as an injection, when it is formed into a liquid, emulsion or suspension, it is generally used as a diluent in the art, for example, water, ethanol, macrogol, propylene glycol, ethoxylated. Isostearyl alcohol, polyoxylated isostearyl alcohol, polyoxyethylene sorbitan fatty acid esters, cottonseed oil, corn oil, peanut oil, olive oil and the like can be used. Further, water is added to the compound of the present invention, and a suspension of the compound in the presence of a suitable surfactant, or a polyoxyethylene hydrogenated castor oil (HCO
-60), and can be prepared as an emulsion using a surfactant such as polysorbate 80 and polyethylene glycol. In addition, salt, glucose or glycerin may be contained in the pharmaceutical preparation, and a usual solubilizer,
A buffer, a soothing agent and the like may be added.
【0020】座剤の形態に成形するに際しては、担体と
して従来公知のものを広く使用することができる。その
例としては、ポリエチレングリコール、カカオ脂、高級
アルコール、高級アルコールのエステル類、ゼラチン、
半合成グリセライド等を挙げることができる。さらに必
要に応じて着色剤、保存剤、香料、風味剤、甘味剤等や
他の医薬品を医薬製剤中に含有させることもできる。In molding into a suppository, a wide variety of conventionally known carriers can be used. Examples include polyethylene glycol, cocoa butter, higher alcohols, higher alcohol esters, gelatin,
Semi-synthetic glycerides and the like can be mentioned. Further, if necessary, a coloring agent, a preservative, a flavor, a flavoring agent, a sweetening agent or the like and other pharmaceuticals can be contained in the pharmaceutical preparation.
【0021】本発明のこれら医薬製剤の投与方法は特に
制限はなく、各種製剤形態、患者の年齢、性別、その他
の条件、疾患の程度に応じた方法で投与される。例え
ば、錠剤、丸剤、液剤、懸濁剤、乳剤、散剤、顆粒剤、
シロップ剤およびカプセル剤の場合には経口投与され
る。注射剤の場合には、単独でまたはブドウ糖、アミノ
酸等の通常の補液と混合して静脈内投与され、さらに必
要に応じて筋肉内、皮下または腹腔内投与される。座剤
の場合は直腸内投与される。The method of administering these pharmaceutical preparations of the present invention is not particularly limited, and the pharmaceutical preparations are administered according to various preparation forms, the age and sex of the patient, other conditions, and the degree of the disease. For example, tablets, pills, solutions, suspensions, emulsions, powders, granules,
Syrups and capsules are administered orally. In the case of an injection, it is administered intravenously, alone or as a mixture with a normal replenisher such as glucose or amino acid, and if necessary, intramuscularly, subcutaneously or intraperitoneally. Suppositories are administered rectally.
【0022】本発明のこれら医薬製剤の投与量は、用
法、患者の年齢、性別、その他の条件、疾患の程度によ
り適宣選択されるが、通常有効成分化合物の量が1日当
たり成人1人当たり、0.001〜1,000mg程度とするのがよ
い。また投与単位形態の製剤中には有効成分化合物が約
0.001〜1,000mgの範囲で含有されることが望ましい。The dosage of these pharmaceutical preparations of the present invention is appropriately selected depending on the usage, age, sex, other conditions, and the degree of the disease of the patient. It is good to use about 0.001 to 1,000 mg. In addition, the active ingredient compound is contained in a dosage unit form in a formulation.
Desirably, it is contained in the range of 0.001 to 1,000 mg.
【0023】尚、本発明の組成物の有効成分としては、
1−(4−クロロフェニル)−3−[4−(2−メトキ
シエチル)ピペラジン−1−イル]メチル−2−ピロリ
ジノン以外の下記製造例において具体的に例示される化
合物も使用することができる。The active ingredient of the composition of the present invention includes:
Compounds specifically exemplified in the following production examples other than 1- (4-chlorophenyl) -3- [4- (2-methoxyethyl) piperazin-1-yl] methyl-2-pyrrolidinone can also be used.
【0024】[0024]
【実施例】以下に本発明の製造例、製剤例および評価例
を記載するが、本発明はこれらに限定されるものではな
い。評価例には、(R)−(+)−1−(4−クロロフ
ェニル)−3−[4−(2−メトキシエチル)ピペラジ
ン−1−イル]メチル−2−ピロリジノン L−酒石酸
塩を試験化合物として用いた。The production examples, preparation examples and evaluation examples of the present invention are described below, but the present invention is not limited to these examples. In the evaluation examples, (R)-(+)-1- (4-chlorophenyl) -3- [4- (2-methoxyethyl) piperazin-1-yl] methyl-2-pyrrolidinone L-tartrate was used as a test compound. Used as
【0025】製造例1 1−(4−クロロフェニル)−
3−[4−(2−メトキシエチル)ピペラジン−1−イ
ル]メチル−2−ピロリジノン (1) 1−(4−クロロフェニル)−2−ピロリジノ
ンの合成 p−クロロアニリン372gとγ−ブチロラクトン25
1gとを混合し、塩酸75mlを加えた。徐々に加温
し、内温110〜115℃で9時間還流した。さらに還
流液を除きながら内温を徐々に上げ、140℃で8時間
反応し、還流液(約80ml)を留出させた。内温を7
0℃まで冷却後、酢酸エチル2000mlに溶かし、
水、炭酸ナトリウム水溶液、水の順にて洗浄した。硫酸
マグネシウムで乾燥後、約1000mlまで濃縮して析
出晶を濾取した。濾液をさらに約200mlまで濃縮
し、析出晶を先のものと合わせ酢酸エチルで洗浄した。
これを減圧乾燥し、目的物347gを得た。1 H NMR(CDCl3,δppm):2.17(2
H,quintet),2.61(2H,t),3.8
3(2H,t),7.32(2H,d),7.58(2
H,d)Production Example 1 1- (4-chlorophenyl)-
3- [4- (2-methoxyethyl) piperazin-1-yl] methyl-2-pyrrolidinone (1) Synthesis of 1- (4-chlorophenyl) -2-pyrrolidinone 372 g of p-chloroaniline and γ-butyrolactone 25
1 g, and 75 ml of hydrochloric acid was added. The mixture was gradually heated and refluxed at an internal temperature of 110 to 115 ° C. for 9 hours. Further, the internal temperature was gradually raised while removing the reflux liquid, and the reaction was carried out at 140 ° C. for 8 hours, and the reflux liquid (about 80 ml) was distilled off. 7 internal temperature
After cooling to 0 ° C, dissolve in 2000 ml of ethyl acetate,
Washing was carried out in the order of water, aqueous sodium carbonate solution and water. After drying over magnesium sulfate, the mixture was concentrated to about 1000 ml and the precipitated crystals were collected by filtration. The filtrate was further concentrated to about 200 ml, and the precipitated crystals were combined with the previous one and washed with ethyl acetate.
This was dried under reduced pressure to obtain 347 g of the desired product. 1 H NMR (CDCl 3 , δ ppm): 2.17 (2
H, quintet), 2.61 (2H, t), 3.8
3 (2H, t), 7.32 (2H, d), 7.58 (2
H, d)
【0026】(2) 1−(4−クロロフェニル)−3
−エトキシカルボニル−2−ピロリジノンの合成 水素化ナトリウム(60%油性)25gのテトラヒドロ
フラン(100ml)懸濁液に炭酸ジエチル37gを加
え、還流下1−(4−クロロフェニル)−2−ピロリジ
ノン52.0gのテトラヒドロフラン(150ml)溶
液を約1.5時間かけて滴下した。4.5時間還流した
後、冷却し、氷水中に注意深くあけた。希塩酸で弱アル
カリ性とし、酢酸エチル300mlで抽出した。有機層
を水、重曹水、水の順にて洗浄し、無水硫酸マグネシウ
ムで乾燥後、濃縮して油状物を得た。n−ヘキサン20
0mlを加えて析出した結晶を濾取した。次にn−ヘキ
サンで洗浄し、減圧乾燥して目的物60gを得た。1 H NMR(CDCl3,δppm):1.32(3
H,t),2.35−2.61(2H,m),3.60
−3.66(1H,m),3.75−3.86(1H,
m),3.89−4.07(1H,m),4.26(2
H,q),7.33(2H,d),7.58(2H,
d)(2) 1- (4-chlorophenyl) -3
Synthesis of -ethoxycarbonyl-2-pyrrolidinone 37 g of diethyl carbonate was added to a suspension of 25 g of sodium hydride (60% oily) in tetrahydrofuran (100 ml), and 52.0 g of 1- (4-chlorophenyl) -2-pyrrolidinone was refluxed. A tetrahydrofuran (150 ml) solution was added dropwise over about 1.5 hours. After refluxing for 4.5 hours, it was cooled and carefully poured into ice water. The mixture was made weakly alkaline with dilute hydrochloric acid and extracted with 300 ml of ethyl acetate. The organic layer was washed with water, aqueous sodium hydrogen carbonate and water in that order, dried over anhydrous magnesium sulfate, and concentrated to obtain an oil. n-hexane 20
0 ml was added, and the precipitated crystals were collected by filtration. Next, the product was washed with n-hexane and dried under reduced pressure to obtain 60 g of the desired product. 1 H NMR (CDCl 3 , δ ppm): 1.32 (3
H, t), 2.35-2.61 (2H, m), 3.60.
-3.66 (1H, m), 3.75-3.86 (1H,
m), 3.89-4.07 (1H, m), 4.26 (2
H, q), 7.33 (2H, d), 7.58 (2H,
d)
【0027】(3) 1−(4−クロロフェニル)−3
−ヒドロキシメチル−2−ピロリジノンの合成 1−(4−クロロフェニル)−3−エトキシカルボニル
−2−ピロリジノン30.0gおよび無水塩化カルシウ
ム15gのメタノール(150ml)溶液に、氷冷下、
水素化ホウ素ナトリウム3.9gを分割装入した。反応
終了後、濃縮し、水と酢酸エチルを加え、希塩酸で酸性
にした。分液して得た有機層を水洗し、無水硫酸マグネ
シウムで乾燥した。濃縮後、n−ヘキサン−エチルエー
テルにて結晶化させた。結晶を濾取後、n−ヘキサンと
ジエチルエーテルの混合溶媒で洗浄し、減圧乾燥して目
的物23.3gを得た。1 H NMR(CDCl3,δppm):1.94−2.
09(1H,m),2.23−2.35(1H,m),
2.83−2.94(1H,m),2.99(1H,b
s),3.75−3.89(3H,m),3.94−
4.00(1H,m),7.33(2H,dd),7.
59(2H,dd)(3) 1- (4-chlorophenyl) -3
Synthesis of 1- (4-chlorophenyl) -3-ethoxycarbonyl-2-pyrrolidinone 30.0 g and anhydrous calcium chloride 15 g in methanol (150 ml) under ice-cooling
3.9 g of sodium borohydride were charged in portions. After completion of the reaction, the mixture was concentrated, water and ethyl acetate were added, and the mixture was acidified with diluted hydrochloric acid. The organic layer obtained by liquid separation was washed with water and dried over anhydrous magnesium sulfate. After concentration, it was crystallized from n-hexane-ethyl ether. The crystals were collected by filtration, washed with a mixed solvent of n-hexane and diethyl ether, and dried under reduced pressure to obtain 23.3 g of the desired product. 1 H NMR (CDCl 3 , δ ppm): 1.94-2.
09 (1H, m), 2.23-2.35 (1H, m),
2.83-2.94 (1H, m), 2.99 (1H, b
s), 3.75-3.89 (3H, m), 3.94-
4.00 (1H, m), 7.33 (2H, dd), 7.
59 (2H, dd)
【0028】(4) 1−(4−クロロフェニル)−3
−メシルオキシメチル−2−ピロリジノンの合成 1−(4−クロロフェニル)−3−ヒドロキシメチル−
2−ピロリジノン23.2gおよびトリエチルアミン1
2.5gのジクロロメタン(200ml)溶液に、氷冷
下、メタンスルホニルクロリド14.0gを滴下した。
2時間反応後、水洗し、無水硫酸マグネシウムで乾燥し
た。溶液を濃縮して結晶化させ、ジエチルエーテルにて
スラッジした。濾取後さらにジエチルエーテルで洗浄
し、減圧乾燥して目的物29.8gを得た。1 H NMR(CDCl3,δppm):2.16−2.
50(2H,m),2.87−3.18(4H,m),
3.77−3.87(2H,m),4.43−4.67
(2H,m),7.34(2H,d),7.58(2
H,d)(4) 1- (4-chlorophenyl) -3
Synthesis of -mesyloxymethyl-2-pyrrolidinone 1- (4-chlorophenyl) -3-hydroxymethyl-
23.2 g of 2-pyrrolidinone and triethylamine 1
Methanesulfonyl chloride (14.0 g) was added dropwise to a solution of 2.5 g of dichloromethane (200 ml) under ice cooling.
After reacting for 2 hours, the mixture was washed with water and dried over anhydrous magnesium sulfate. The solution was concentrated to crystallize and sludged with diethyl ether. After filtration, the product was further washed with diethyl ether and dried under reduced pressure to obtain 29.8 g of the desired product. 1 H NMR (CDCl 3 , δ ppm): 2.16-2.
50 (2H, m), 2.87-3.18 (4H, m),
3.77-3.87 (2H, m), 4.43-4.67
(2H, m), 7.34 (2H, d), 7.58 (2
H, d)
【0029】(5) 1−ホルミル−4−(2−メトキ
シエチル)ピペラジンの合成 N−ホルミルピペラジン37.1gおよび無水炭酸ナト
リウム37.1gのメタノール(50ml)溶液に、メ
トキシエチルブロミド53.15gを滴下し、3.5時
間還流した。室温まで冷却後、不溶物を濾去し、濾液を
濃縮した。濾液に水、クロロホルムを加えて分液し有機
層を得た。水層をクロロホルムで抽出し、先の有機層と
合わせて無水硫酸マグネシウムで乾燥後、濃縮して目的
物57.2gを得た。1 H NMR(CDCl3,δppm):2.45−2.
54(4H,m),2.59−2.63(2H,m),
3.35−3.43(2H,m),3.36(3H,
s),3.50−3.61(4H,m),8.02(1
H,s)(5) Synthesis of 1-formyl-4- (2-methoxyethyl) piperazine 53.15 g of methoxyethyl bromide was added to a solution of 37.1 g of N-formylpiperazine and 37.1 g of anhydrous sodium carbonate in 50 ml of methanol. The mixture was added dropwise and refluxed for 3.5 hours. After cooling to room temperature, insolubles were removed by filtration, and the filtrate was concentrated. Water and chloroform were added to the filtrate, and the mixture was separated to give an organic layer. The aqueous layer was extracted with chloroform, combined with the previous organic layer, dried over anhydrous magnesium sulfate, and concentrated to obtain 57.2 g of the desired product. 1 H NMR (CDCl 3 , δ ppm): 2.45-2.
54 (4H, m), 2.59-2.63 (2H, m),
3.35-3.43 (2H, m), 3.36 (3H,
s), 3.50-3.61 (4H, m), 8.02 (1
H, s)
【0030】(6) 1−(2−メトキシエチル)ピペ
ラジン二塩酸塩の合成 1−ホルミル−4−メトキシエチルピペラジン57.2
gのメタノール(100ml)溶液に、4N−塩酸/
1,4−ジオキサン180mlを1.5時間かけて滴下
した。室温で1時間攪拌後結晶を濾取し、イソプロピル
エーテルで洗浄、減圧乾燥して、目的物68.8gを得
た。(6) Synthesis of 1- (2-methoxyethyl) piperazine dihydrochloride 1-Formyl-4-methoxyethylpiperazine 57.2
g of methanol (100 ml) in 4N hydrochloric acid /
180 ml of 1,4-dioxane was added dropwise over 1.5 hours. After stirring at room temperature for 1 hour, the crystals were collected by filtration, washed with isopropyl ether, and dried under reduced pressure to obtain 68.8 g of the desired product.
【0031】(7) 1−(2−メトキシエチル)ピペ
ラジンの合成 1−メトキシエチルピペラジン二塩酸塩68.8gの水
溶液(50ml)に、水酸化ナトリウム33.0gの水
溶液(100ml)を滴下した。クロロホルムで抽出、
無水硫酸マグネシウムにて乾燥し、溶媒を溜去して目的
物41.3gを得た。1 H NMR(CDCl3,δppm):1.80(1
H,s),2.47−2.60(6H,m),2.90
−2.94(4H,m),3.36(3H,s),3.
52(2H,t)(7) Synthesis of 1- (2-methoxyethyl) piperazine To an aqueous solution (50 ml) of 68.8 g of 1-methoxyethylpiperazine dihydrochloride, an aqueous solution (100 ml) of 33.0 g of sodium hydroxide was added dropwise. Extract with chloroform,
After drying over anhydrous magnesium sulfate, the solvent was distilled off to obtain 41.3 g of the desired product. 1 H NMR (CDCl 3 , δ ppm): 1.80 (1
H, s), 2.47-2.60 (6H, m), 2.90.
-2.94 (4H, m), 3.36 (3H, s), 3.
52 (2H, t)
【0032】(8) 1−(4−クロロフェニル)−3
−(4−(2−メトキシエチル)ピペラジン−1−イ
ル)メチル−2−ピロリジノンの合成 1−(4−クロロフェニル)−3−メシルオキシメチル
−2−ピロリジノン18.5gおよび1−(2−メトキ
シエチル)ピペラジン17.6gのアセトニトリル(5
0ml)溶液にトリエチルアミン8.0gを加え、4時
間加熱還流した。反応混合物を濃縮後、水を加えて析出
した結晶を濾取し、減圧乾燥して目的物18.5gを得
た。 融点:103〜105℃1 H NMR(CDCl3,δppm):2.01−2.
12(1H,m),2.29−2.62(12H,
m),2.78−2.94(2H,m),3.35(3
H,s),3.51(2H,t),3.74−3.80
(2H,m),7.32(2H,d),7.59(2
H,d)(8) 1- (4-chlorophenyl) -3
Synthesis of-(4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone 1- (4-chlorophenyl) -3-mesyloxymethyl-2-pyrrolidinone 18.5 g and 1- (2-methoxy) Ethyl) piperazine 17.6 g of acetonitrile (5
(0 ml), 8.0 g of triethylamine was added to the solution, and the mixture was heated under reflux for 4 hours. After concentrating the reaction mixture, water was added, and the precipitated crystals were collected by filtration and dried under reduced pressure to obtain 18.5 g of the desired product. Melting point: 103-105 ° C 1 H NMR (CDCl 3 , δ ppm): 2.01-2.
12 (1H, m), 2.29-2.62 (12H,
m), 2.78-2.94 (2H, m), 3.35 (3
H, s), 3.51 (2H, t), 3.74-3.80.
(2H, m), 7.32 (2H, d), 7.59 (2
H, d)
【0033】製造例2 1−(4−クロロフェニル)−
3−(4−(2−メトキシエチル)ピペラジン−1−イ
ル)メチル−2−ピロリジノン二塩酸塩 1−(4−クロロフェニル)−3−(4−(2−メトキ
シエチル)ピペラジン−1−イル)メチル−2−ピロリ
ジノン1.41gのメタノール(10ml)溶液に、4
N塩酸/1,4−ジオキサンを加えて酸性にした。析出
した結晶を濾取後、ジエチルエーテルで洗浄し、減圧乾
燥して目的物1.62gを得た。 融点:261〜262℃1 H NMR(DMSO,δppm):2.00−2.
12(1H,m),2.55(1H,m),3.31
(3H,s),3.31−3.84(17H,m),
7.46(2H,d),7.72(2H,d)Production Example 2 1- (4-chlorophenyl)-
3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone dihydrochloride 1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) To a solution of 1.41 g of methyl-2-pyrrolidinone in 10 ml of methanol was added 4
The mixture was acidified by addition of N hydrochloric acid / 1,4-dioxane. The precipitated crystals were collected by filtration, washed with diethyl ether, and dried under reduced pressure to obtain 1.62 g of the desired product. Melting point: 261-262 ° C. 1 H NMR (DMSO, δ ppm): 2.00-2.
12 (1H, m), 2.55 (1H, m), 3.31
(3H, s), 3.31-3.84 (17H, m),
7.46 (2H, d), 7.72 (2H, d)
【0034】製造例3 (R)−1−(4−クロロフェ
ニル)−3−(4−(2−メトキシエチル)ピペラジン
−1−イル)メチル−2−ピロリジノン(R)−(−)
−マンデル酸塩 加熱した1−(4−クロロフェニル)−3−(4−(2
−メトキシエチル)ピペラジン−1−イル)メチル−2
−ピロリジノン66.6gの酢酸エチル(350ml)
溶液に、加熱した(R)−(−)−マンデル酸の酢酸エ
チル(120ml)溶液を加えた。冷却後析出した結晶
を濾取して酢酸エチルで洗浄し、減圧乾燥して目的物3
6.4gを得た。 融点:137〜138℃ 鏡像異性体過剰率 99%ee以上(HPLC面積比よ
り算出) なお鏡像異性体過剰率は、キラルカラムを用いた液体ク
ロマトグラフィーによりピーク面積から算出した。以下
も同様である。1 H NMR(DMSO,δppm):1.83−1.
97(1H,m),2.19−2.97(14H,
m),3.23(3H,s),3.41−3.48(2
H,m),3.70−3.81(2H,m),4.94
(1H,s),7.21−7.38(5H,m),7.
41(2H,d),7.69(2H,d)Production Example 3 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone (R)-(-)
-Mandelic acid salt heated 1- (4-chlorophenyl) -3- (4- (2
-Methoxyethyl) piperazin-1-yl) methyl-2
66.6 g of ethyl acetate of pyrrolidinone (350 ml)
To the solution was added a heated solution of (R)-(-)-mandelic acid in ethyl acetate (120 ml). After cooling, the precipitated crystals were collected by filtration, washed with ethyl acetate, and dried under reduced pressure to obtain the desired product 3.
6.4 g were obtained. Melting point: 137-138 ° C Enantiomeric excess 99% ee or more (calculated from HPLC area ratio) The enantiomeric excess was calculated from the peak area by liquid chromatography using a chiral column. The same applies to the following. 1 H NMR (DMSO, δ ppm): 1.83-1.
97 (1H, m), 2.19-2.97 (14H,
m), 3.23 (3H, s), 3.41-3.48 (2
H, m), 3.70-3.81 (2H, m), 4.94.
(1H, s), 7.21-7.38 (5H, m), 7.
41 (2H, d), 7.69 (2H, d)
【0035】製造例4 (R)−1−(4−クロロフェ
ニル)−3−(4−(2−メトキシエチル)ピペラジン
−1−イル)メチル−2−ピロリジノン エタノール(100ml)にて再結晶した(R)−1−
(4−クロロフェニル)−3−(4−(2−メトキシエ
チル)ピペラジン−1−イル)メチル−2−ピロリジノ
ン(R)−(−)−マンデル酸塩30.5gを水(30
0ml)に溶解し、炭酸ナトリウムで脱塩後、酢酸エチ
ルで抽出した。有機層を無水硫酸マグネシウムで乾燥
後、濃縮して目的物19.5gを得た。 融点:102〜103℃ 旋光性:+ 鏡像異性体過剰率 99%ee以上1 H NMR(CDCl3,δppm):2.04(1
H,m),2.35(1H,m),2.4−2.7(1
1H,m),2.81(1H,m),2.91(1H,
dd),3.35(3H,s),3.51(2H,
t),3.77(2H,m)7.32(2H,d),
7.59(2H,d)Production Example 4 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone Recrystallized from ethanol (100 ml) ( R) -1-
30.5 g of (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone (R)-(-)-mandelate was added to water (30
0 ml), desalted with sodium carbonate, and extracted with ethyl acetate. The organic layer was dried over anhydrous magnesium sulfate and concentrated to obtain 19.5 g of the desired product. Melting point: 102-103 ° C. Optical rotation: + enantiomeric excess 99% ee or more 1 H NMR (CDCl 3 , δ ppm): 2.04 (1
H, m), 2.35 (1H, m), 2.4-2.7 (1
1H, m), 2.81 (1H, m), 2.91 (1H,
dd), 3.35 (3H, s), 3.51 (2H,
t), 3.77 (2H, m) 7.32 (2H, d),
7.59 (2H, d)
【0036】製造例5 (R)−1−(4−クロロフェ
ニル)−3−(4−(2−メトキシエチル)ピペラジン
−1−イル)メチル−2−ピロリジノン二塩酸塩の製造
(表2の化合物番号50の(R)−体) (R)−1−(4−クロロフェニル)−3−(4−(2
−メトキシエチル)ピペラジン−1−イル)メチル−2
−ピロリジノン18.7gのメタノール(130ml)
溶液に、4N塩酸/1,4−ジオキサンを加えて酸性に
した。析出した結晶を濾取し、ジエチルエーテルで洗浄
し、減圧乾燥して目的物22.6gを得た。 融点:252〜253℃(分解) 旋光性:− 鏡像異性体過剰率 99%ee以上1 H NMR(D2O,δppm):2.06(1H,
m),2.52(1H,m),3.41(3H,s),
3.32−4.03(17H,m),7.48(4H,
s)Production Example 5 Production of (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone dihydrochloride (compound of Table 2) (R) -form of No. 50) (R) -1- (4-chlorophenyl) -3- (4- (2
-Methoxyethyl) piperazin-1-yl) methyl-2
-18.7 g of pyrrolidinone methanol (130 ml)
The solution was acidified by adding 4N hydrochloric acid / 1,4-dioxane. The precipitated crystals were collected by filtration, washed with diethyl ether, and dried under reduced pressure to obtain 22.6 g of the desired product. Melting point: 252 to 253 ° C. (decomposition) Optical rotation:-enantiomeric excess 99% ee or more 1 H NMR (D 2 O, δ ppm): 2.06 (1H,
m), 2.52 (1H, m), 3.41 (3H, s),
3.32-4.03 (17H, m), 7.48 (4H,
s)
【0037】製造例6 (R)−1−(4−クロロフェ
ニル)−3−(4−(2−メトキシエチル)ピペラジン
−1−イル)メチル−2−ピロリジノン二塩酸塩二水和
物 (R)−1−(4−クロロフェニル)−3−(4−(2
−メトキシエチル)ピペラジン−1−イル)メチル−2
−ピロリジノン二塩酸塩1.98gを相対湿度75%、
温度25℃に保った恒温槽に24時間放置し、目的物
2.14gを得た。 融点:264.6〜265.1℃(分解) 旋光性:− 鏡像異性体過剰率 99%ee以上1 H NMR(D2O,δppm):2.06(1H,
m),2.52(1H,m),3.41(3H,s),
3.32−4.03(17H,m),7.48(4H,
s) 本化合物は、以下の方法でも合成できる。Production Example 6 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone dihydrochloride dihydrate (R) -1- (4-chlorophenyl) -3- (4- (2
-Methoxyethyl) piperazin-1-yl) methyl-2
1.98 g of pyrrolidinone dihydrochloride at 75% relative humidity,
It was left in a thermostat maintained at a temperature of 25 ° C. for 24 hours to obtain 2.14 g of the desired product. Melting point: 264.6-265.1 ° C. (decomposition) Optical activity:-enantiomeric excess 99% ee or more 1 H NMR (D 2 O, δ ppm): 2.06 (1H,
m), 2.52 (1H, m), 3.41 (3H, s),
3.32-4.03 (17H, m), 7.48 (4H,
s) This compound can also be synthesized by the following method.
【0038】還流下、(R)−1−(4−クロロフェニ
ル)−3−(4−(2−メトキシエチル)ピペラジン−
1−イル)メチル−2−ピロリジノン二塩酸塩100m
gのエタノール(3ml)懸濁液に、反応系が均一にな
るまで水を滴下した。室温まで放冷後、析出した固体を
濾取し、乾燥して目的物88.5mgを得た。Under reflux, (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazine-
1-yl) methyl-2-pyrrolidinone dihydrochloride 100m
Water was added dropwise to a suspension of g (3 ml) of ethanol until the reaction system became homogeneous. After allowing to cool to room temperature, the precipitated solid was collected by filtration and dried to obtain 88.5 mg of the desired product.
【0039】製造例7 (R)−1−(4−クロロフェ
ニル)−3−(4−(2−メトキシエチル)ピペラジン
−1−イル)メチル−2−ピロリジノン二臭化水素酸塩 47%臭化水素酸水溶液379mgとエタノール(10
ml)の混合物中に、(R)−1−(4−クロロフェニ
ル)−3−(4−(2−メトキシエチル)ピペラジン−
1−イル)メチル−2−ピロリジノン352mgのエタ
ノール(10ml)溶液を加えた。室温で攪拌後冷却
し、析出した固体を濾取、乾燥して目的物488mgを
得た。 融点:244.1〜245.1℃1 H NMR(DMSO,δppm):1.90−2.
60(1H,m),2.40−2.55(1H,m),
2.78−4.00(20H,m),7.46(2H,
d),7.73(2H,d)Production Example 7 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone dihydrobromide 47% bromide Hydrogen acid aqueous solution 379 mg and ethanol (10
(R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazine-
A solution of 352 mg of 1-yl) methyl-2-pyrrolidinone in ethanol (10 ml) was added. After stirring at room temperature and cooling, the precipitated solid was collected by filtration and dried to obtain 488 mg of the desired product. Melting point: 244.1-244.1 ° C. 1 H NMR (DMSO, δ ppm): 1.90-2.
60 (1H, m), 2.40-2.55 (1H, m),
2.78-4.00 (20H, m), 7.46 (2H,
d), 7.73 (2H, d)
【0040】製造例8 (R)−1−(4−クロロフェ
ニル)−3−(4−(2−メトキシエチル)ピペラジン
−1−イル)メチル−2−ピロリジノン硫酸塩一水和物
の製造(表3の化合物番号32の(R)−体) (R)−1−(4−クロロフェニル)−3−(4−(2
−メトキシエチル)ピペラジン−1−イル)メチル−2
−ピロリジノン352mgのエタノール(10ml)溶
液中に、濃硫酸101mgのエタノール(5ml)溶液
を加えた。室温で攪拌後3mlまで濃縮し、酢酸エチル
(5ml)を加え、析出した固体を濾取、乾燥して目的
物389mgを得た。 融点:166.4〜166.7℃1 H NMR(DMSO,δppm):1.84−1.
99(1H,m),2.15−4.35(21H,
m),7.44(2H,d),7.71(2H,d)Production Example 8 Production of (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone sulfate monohydrate (Table) (R) -form of compound No. 32 of No. 3) (R) -1- (4-chlorophenyl) -3- (4- (2
-Methoxyethyl) piperazin-1-yl) methyl-2
-To a solution of 352 mg of pyrrolidinone in 10 ml of ethanol was added a solution of 101 mg of concentrated sulfuric acid in 5 ml of ethanol. After stirring at room temperature, the mixture was concentrated to 3 ml, ethyl acetate (5 ml) was added, and the precipitated solid was collected by filtration and dried to obtain 389 mg of the desired product. Melting point: 166.4-166.7 ° C 1 H NMR (DMSO, δ ppm): 1.84-1.
99 (1H, m), 2.15-4.35 (21H,
m), 7.44 (2H, d), 7.71 (2H, d)
【0041】製造例9 (R)−1−(4−クロロフェ
ニル)−3−(4−(2−メトキシエチル)ピペラジン
−1−イル)メチル−2−ピロリジノンベンゼンスルホ
ン酸塩一水和物 ベンゼンスルホン酸一水和物176mgのエタノール
(10ml)溶液に、(R)−1−(4−クロロフェニ
ル)−3−(4−(2−メトキシエチル)ピペラジン−
1−イル)メチル−2−ピロリジノン352mgのエタ
ノール(10ml)溶液を加えた。濃縮残渣をエタノー
ルでスラッジ後、固体を濾取、乾燥して目的物407m
gを得た。 融点:82.2〜85.9℃1 H NMR(DMSO,δppm):1.88−1.
99(1H,m),2.31−3.81(21H,
m),7.31−7.36(3H,m),7.43(2
H,d),7.59−7.68(2H,m),7.69
−7.72(2H,m)Production Example 9 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone benzenesulfonate monohydrate benzenesulfone To a solution of 176 mg of acid monohydrate in ethanol (10 ml) was added (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazine-
A solution of 352 mg of 1-yl) methyl-2-pyrrolidinone in ethanol (10 ml) was added. After sludge the concentrated residue with ethanol, the solid was collected by filtration and dried to obtain 407 m of the desired product.
g was obtained. Melting point: 82.2-85.9 ° C. 1 H NMR (DMSO, δ ppm): 1.88-1.
99 (1H, m), 2.31-3.81 (21H,
m), 7.31-7.36 (3H, m), 7.43 (2
H, d), 7.59-7.68 (2H, m), 7.69.
-7.72 (2H, m)
【0042】製造例10 (R)−1−(4−クロロフ
ェニル)−3−(4−(2−メトキシエチル)ピペラジ
ン−1−イル)メチル−2−ピロリジノン二ベンゼンス
ルホン酸塩三.五水和物 ベンゼンスルホン酸一水和物352mgの酢酸エチル
(10ml)溶液に、(R)−1−(4−クロロフェニ
ル)−3−(4−(2−メトキシエチル)ピペラジン−
1−イル)メチル−2−ピロリジノン352mgの酢酸
エチル(10ml)溶液を加えた。室温で攪拌後冷却
し、析出した固体を濾取、乾燥して目的物585mgを
得た。 融点:162.5〜163.4℃1 H NMR(DMSO,δppm):1.78−1.
97(1H,m),2.18−3.84(22H,
m),7.23−7.36(6H,m),7.45−
7.49(2H,m),7.58−7.64(4H,
m),7.70−7.75(2H,m)Production Example 10 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone dibenzenesulfonate Pentahydrate To a solution of 352 mg of benzenesulfonic acid monohydrate in ethyl acetate (10 ml) was added (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazine-
A solution of 352 mg of 1-yl) methyl-2-pyrrolidinone in ethyl acetate (10 ml) was added. After stirring at room temperature and cooling, the precipitated solid was collected by filtration and dried to obtain 585 mg of the desired product. Melting point: 162.5-163.4 ° C. 1 H NMR (DMSO, δ ppm): 1.78-1.
97 (1H, m), 2.18-3.84 (22H,
m), 7.23-7.36 (6H, m), 7.45-
7.49 (2H, m), 7.58-7.64 (4H,
m), 7.70-7.75 (2H, m)
【0043】製造例11 (R)−1−(4−クロロフ
ェニル)−3−(4−(2−メトキシエチル)ピペラジ
ン−1−イル)メチル−2−ピロリジノン二p−トルエ
ンスルホン酸塩二水和物 p−トルエンスルホン酸一水和物380mgの酢酸エチ
ル(10ml)溶液に、(R)−1−(4−クロロフェ
ニル)−3−(4−(2−メトキシエチル)ピペラジン
−1−イル)メチル−2−ピロリジノン352mgの酢
酸エチル(10ml)溶液を加えた。室温で攪拌後冷却
し、析出した固体を濾取、乾燥して目的物712mgを
得た。 融点:209.8〜210.3℃1 H NMR(DMSO,δppm):1.85−2.
10(1H,m),2.25−2.50(1H,m),
2.29(6H,s),2.70−3.95(20H,
m),7.12(4H,d),7.30(2H,d),
7.45−7.49(6H,m)Production Example 11 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone dip-toluenesulfonate dihydrate Compound (R) -1- (4-Chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl was added to a solution of 380 mg of p-toluenesulfonic acid monohydrate in ethyl acetate (10 ml). A solution of 352 mg of 2-pyrrolidinone in ethyl acetate (10 ml) was added. After stirring at room temperature and cooling, the precipitated solid was collected by filtration and dried to obtain 712 mg of the desired product. Melting point: 209.8-210.3 ° C. 1 H NMR (DMSO, δ ppm): 1.85-2.
10 (1H, m), 2.25-2.50 (1H, m),
2.29 (6H, s), 2.70-3.95 (20H,
m), 7.12 (4H, d), 7.30 (2H, d),
7.45-7.49 (6H, m)
【0044】製造例12 (R)−1−(4−クロロフ
ェニル)−3−(4−(2−メトキシエチル)ピペラジ
ン−1−イル)メチル−2−ピロリジノンメタンスルホ
ン酸塩 (R)−1−(4−クロロフェニル)−3−(4−(2
−メトキシエチル)ピペラジン−1−イル)メチル−2
−ピロリジノン880mgの酢酸エチル(15ml)溶
液に、メタンスルホン酸240mgの酢酸エチル(5m
l)溶液を加えた。室温で攪拌後冷却し、析出した固体
を濾取、乾燥して目的物892mgを得た。1 H NMR(D2O,δppm):1.95−2.10
(1H,s),2.41−2.55(1H,s),2.
74−3.45(13H,m),2.80(3H,
s),3.39(3H,s),3.73−3.77(2
H,m),3.81−3.97(2H,m),7.46
(4H,s)Production Example 12 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone methanesulfonate (R) -1- (4-chlorophenyl) -3- (4- (2
-Methoxyethyl) piperazin-1-yl) methyl-2
-To a solution of 880 mg of pyrrolidinone in 15 ml of ethyl acetate was added 240 mg of methanesulfonic acid in ethyl acetate (5 m
l) The solution was added. After stirring at room temperature and cooling, the precipitated solid was collected by filtration and dried to obtain 892 mg of the desired product. 1 H NMR (D 2 O, δ ppm): 1.95-2.10.
(1H, s), 2.41-2.55 (1H, s), 2.
74-3.45 (13H, m), 2.80 (3H,
s), 3.39 (3H, s), 3.73-3.77 (2
H, m), 3.81-3.97 (2H, m), 7.46.
(4H, s)
【0045】製造例13 (R)−1−(4−クロロフ
ェニル)−3−(4−(2−メトキシエチル)ピペラジ
ン−1−イル)メチル−2−ピロリジノン二メタンスル
ホン酸塩 (R)−1−(4−クロロフェニル)−3−(4−(2
−メトキシエチル)ピペラジン−1−イル)メチル−2
−ピロリジノン880mgの酢酸エチル(15ml)溶
液に、メタンスルホン酸480mgの酢酸エチル(5m
l)溶液を加えた。室温で攪拌後冷却し、析出した固体
を濾取、乾燥して目的物1127mgを得た。1 H NMR(D2O,δppm):1.98−2.13
(1H,m),2.49−2.62(1H,m),2.
80(6H,s),3.31−4.19(17H,
m),3.41(3H,s),7.48(4H,s)Production Example 13 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone dimethanesulfonate (R) -1 -(4-chlorophenyl) -3- (4- (2
-Methoxyethyl) piperazin-1-yl) methyl-2
To a solution of 880 mg of pyrrolidinone in 15 ml of ethyl acetate was added 480 mg of methanesulfonic acid in ethyl acetate (5 m
l) The solution was added. After stirring at room temperature and cooling, the precipitated solid was collected by filtration and dried to give 1127 mg of the desired product. 1 H NMR (D 2 O, δ ppm): 1.98-2.13
(1H, m), 2.49-2.62 (1H, m), 2.
80 (6H, s), 3.31-4.19 (17H,
m), 3.41 (3H, s), 7.48 (4H, s)
【0046】製造例14 (R)−1−(4−クロロフ
ェニル)−3−(4−(2−メトキシエチル)ピペラジ
ン−1−イル)メチル−2−ピロリジノンL−乳酸塩 (R)−1−(4−クロロフェニル)−3−(4−(2
−メトキシエチル)ピペラジン−1−イル)メチル−2
−ピロリジノン352mgの酢酸エチル(10ml)溶
液中に、85%L−乳酸水溶液106mgと酢酸エチル
(10ml)の混合物を加えた。室温で攪拌後、濃縮残
渣をジエチルエーテルでスラッジし、乾燥して目的物1
80mgを得た。 融点:64.9〜86.0℃1 H NMR(DMSO,δppm):1.23(3
H,d),1.80−2.00(1H,m),2.15
−4.10(23H,m),7.43(2H,d),
7.70(2H,d)Production Example 14 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone L-lactate (R) -1- (4-chlorophenyl) -3- (4- (2
-Methoxyethyl) piperazin-1-yl) methyl-2
-To a solution of 352 mg of pyrrolidinone in 10 ml of ethyl acetate was added a mixture of 106 mg of an aqueous 85% L-lactic acid solution and 10 ml of ethyl acetate. After stirring at room temperature, the concentrated residue was sludged with diethyl ether and dried to obtain the desired product 1
80 mg were obtained. Melting point: 64.9-86.0 ° C. 1 H NMR (DMSO, δ ppm): 1.23 (3
H, d), 1.80-2.00 (1H, m), 2.15
-4.10 (23H, m), 7.43 (2H, d),
7.70 (2H, d)
【0047】製造例15 (R)−1−(4−クロロフ
ェニル)−3−(4−(2−メトキシエチル)ピペラジ
ン−1−イル)メチル−2−ピロリジノンL−酒石酸塩 L−酒石酸150mgのエタノール(10ml)溶液
に、(R)−1−(4−クロロフェニル)−3−(4−
(2−メトキシエチル)ピペラジン−1−イル)メチル
−2−ピロリジノン352mgの酢酸エチル(10m
l)溶液を加えた。室温で攪拌後冷却し、析出した固体
を濾取、乾燥して目的物488mgを得た。 融点:183.2〜184.9℃1 H NMR(DMSO,δppm):1.82−1.
94(1H,m),2.21−3.79(22H,
m),4.17(2H,s),7.40−7.46(2
H,m),7.67−7.73(2H,m)本化合物
は、以下の方法でも合成できる。 (R)−1−(4−クロロフェニル)−3−(4−(2
−メトキシエチル)ピペラジン−1−イル)メチル−2
−ピロリジノン5.00gとL−酒石酸2.13gを1
8%水−エタノール(62ml)に懸濁した。加熱還流
して均一溶液とした後、冷却し、析出した固体を濾取、
乾燥して目的物6.39gを得た。Production Example 15 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone L-tartrate L-tartaric acid 150 mg of ethanol (R) -1- (4-chlorophenyl) -3- (4-
352 mg of (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone in ethyl acetate (10 m
l) The solution was added. After stirring at room temperature and cooling, the precipitated solid was collected by filtration and dried to obtain 488 mg of the desired product. Melting point: 183.2-184.9 ° C. 1 H NMR (DMSO, δ ppm): 1.82-1.
94 (1H, m), 2.21-3.79 (22H,
m), 4.17 (2H, s), 7.40-7.46 (2
H, m), 7.67-7.73 (2H, m) The present compound can also be synthesized by the following method. (R) -1- (4-chlorophenyl) -3- (4- (2
-Methoxyethyl) piperazin-1-yl) methyl-2
-5.00 g of pyrrolidinone and 2.13 g of L-tartaric acid in 1
The suspension was suspended in 8% water-ethanol (62 ml). After heating to reflux to form a homogeneous solution, the mixture was cooled, and the precipitated solid was collected by filtration.
Drying yielded 6.39 g of the desired product.
【0048】製造例16 (R)−1−(4−クロロフ
ェニル)−3−(4−(2−メトキシエチル)ピペラジ
ン−1−イル)メチル−2−ピロリジノン二L−酒石酸
塩二水和物 L−酒石酸300mgのエタノール(20ml)溶液
に、(R)−1−(4−クロロフェニル)−3−(4−
(2−メトキシエチル)ピペラジン−1−イル)メチル
−2−ピロリジノン352mgのエタノール(10m
l)溶液を加えた。室温で攪拌後冷却し、析出した固体
を濾取、乾燥して目的物205mgを得た。 1 H NMR(DMSO,δppm):1.87−1.
98(1H,m),2.25−2.89(14H,
m),3.25(3H,s),3.41−3.51(2
H,m),3.74−3.80(2H,m),4.21
(4H,s),7.42(2H,dd),7.70(2
H,dd)Production Example 16 (R) -1- (4-chlorofu)
Enyl) -3- (4- (2-methoxyethyl) piperazine
N-1-yl) methyl-2-pyrrolidinone di-L-tartaric acid
Salt dihydrate L-tartaric acid 300mg ethanol (20ml) solution
In addition, (R) -1- (4-chlorophenyl) -3- (4-
(2-methoxyethyl) piperazin-1-yl) methyl
-2-pyrrolidinone 352 mg of ethanol (10 m
l) The solution was added. After stirring at room temperature, the solid precipitated
Was collected by filtration and dried to obtain 205 mg of the desired product. 1 1 H NMR (DMSO, δ ppm): 1.87-1.
98 (1H, m), 2.25-2.89 (14H,
m), 3.25 (3H, s), 3.41-3.51 (2
H, m), 3.74-3.80 (2H, m), 4.21
(4H, s), 7.42 (2H, dd), 7.70 (2
H, dd)
【0049】製造例17 (R)−1−(4−クロロフ
ェニル)−3−(4−(2−メトキシエチル)ピペラジ
ン−1−イル)メチル−2−ピロリジノン二D−酒石酸
塩 (R)−1−(4−クロロフェニル)−3−(4−(2
−メトキシエチル)ピペラジン−1−イル)メチル−2
−ピロリジノン176mgのエタノール(3ml)溶液
に、D−酒石酸75mgのエタノール(3ml)溶液を
加えた。室温で攪拌後冷却し、析出した固体を濾取、乾
燥して目的物110mgを得た。1 H NMR(DMSO,δppm):1.86−1.
94(1H,m),2.25−3.00(14H,
m),3.25(3H,s),3.47−3.51(2
H,m),3.74−3.80(2H,m),4.22
(2H,s),7.43(2H,d),7.70(2
H,d)Production Example 17 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone di-D-tartrate (R) -1 -(4-chlorophenyl) -3- (4- (2
-Methoxyethyl) piperazin-1-yl) methyl-2
-To a solution of 176 mg of pyrrolidinone in ethanol (3 ml) was added a solution of 75 mg of D-tartaric acid in ethanol (3 ml). After stirring at room temperature and cooling, the precipitated solid was collected by filtration and dried to obtain 110 mg of the desired product. 1 H NMR (DMSO, δ ppm): 1.86-1.
94 (1H, m), 2.25-3.00 (14H,
m), 3.25 (3H, s), 3.47-3.51 (2
H, m), 3.74-3.80 (2H, m), 4.22
(2H, s), 7.43 (2H, d), 7.70 (2
H, d)
【0050】製造例18 (R)−1−(4−クロロフ
ェニル)−3−(4−(2−メトキシエチル)ピペラジ
ン−1−イル)メチル−2−ピロリジノン二コハク酸塩 (R)−1−(4−クロロフェニル)−3−(4−(2
−メトキシエチル)ピペラジン−1−イル)メチル−2
−ピロリジノン880mgのエタノール(20ml)溶
液に、コハク酸591mgのエタノール(20ml)溶
液を加えた。室温で攪拌後冷却し、析出した固体を濾
取、乾燥して目的物356mgを得た。 融点:98.1〜99.1℃1 H NMR(DMSO,δppm):1.82−1.
96(1H,m),2.18−2.97(14H,
m),2.41(4H,s),3.23(3H,s),
3.41−3.45(2H,m),3.70−3.81
(2H,m),7.43(2H,d),7.70(2
H,d)Production Example 18 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone disuccinate (R) -1- (4-chlorophenyl) -3- (4- (2
-Methoxyethyl) piperazin-1-yl) methyl-2
-To a solution of 880 mg of pyrrolidinone in ethanol (20 ml) was added a solution of 591 mg of succinic acid in ethanol (20 ml). After stirring at room temperature and cooling, the precipitated solid was collected by filtration and dried to obtain 356 mg of the desired product. Melting point: 98.1-99.1 ° C. 1 H NMR (DMSO, δ ppm): 1.82-1.
96 (1H, m), 2.18-2.97 (14H,
m), 2.41 (4H, s), 3.23 (3H, s),
3.41-3.45 (2H, m), 3.70-3.81
(2H, m), 7.43 (2H, d), 7.70 (2
H, d)
【0051】製造例19 (R)−1−(4−クロロフ
ェニル)−3−(4−(2−メトキシエチル)ピペラジ
ン−1−イル)メチル−2−ピロリジノン二フマル酸塩 (R)−1−(4−クロロフェニル)−3−(4−(2
−メトキシエチル)ピペラジン−1−イル)メチル−2
−ピロリジノン5.00gとフマル酸3.30gを13
%水−エタノール(62ml)に懸濁した。加熱還流し
て均一溶液とした後、冷却し、析出した固体を濾取、乾
燥して目的物7.45gを得た。 融点:192−193℃1 H NMR(DMSO,δppm):1.82−1.
97(1H,m),2.19−2.31(1H,m),
2.35−2.97(13H,m),3.24(3H,
s),3.44−3.48(2H,m),3.73−
3.79(2H,m),6.60(4H,s),7.4
3(2H,d),7.70(2H,d)Production Example 19 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone difumarate (R) -1- (4-chlorophenyl) -3- (4- (2
-Methoxyethyl) piperazin-1-yl) methyl-2
5.00 g of pyrrolidinone and 3.30 g of fumaric acid in 13
% Water-ethanol (62 ml). After heating to reflux to form a homogeneous solution, the solution was cooled, and the precipitated solid was collected by filtration and dried to obtain 7.45 g of the desired product. Melting point: 192-193 ° C 1 H NMR (DMSO, δ ppm): 1.82-1.
97 (1H, m), 2.19-2.31 (1H, m),
2.35-2.97 (13H, m), 3.24 (3H,
s), 3.44-3.48 (2H, m), 3.73-
3.79 (2H, m), 6.60 (4H, s), 7.4
3 (2H, d), 7.70 (2H, d)
【0052】製造例20 (R)−1−(4−クロロフ
ェニル)−3−(4−(2−メトキシエチル)ピペラジ
ン−1−イル)メチル−2−ピロリジノン二マレイン酸
塩 (R)−1−(4−クロロフェニル)−3−(4−(2
−メトキシエチル)ピペラジン−1−イル)メチル−2
−ピロリジノン5.00gとマレイン酸3.30gを9
%水−エタノール(62ml)に懸濁した。加熱還流し
て均一溶液とした後、冷却し、析出した固体を濾取、乾
燥して目的物7.10gを得た。 融点:178.5−179.1℃1 H NMR(DMSO,δppm):1.76−1.
98(1H,m),2.23−2.35(1H,m),
2.66−3.30(13H,m),3.30(3H,
s),3.60−3.72(2H,m),3.76−
3.81(2H,m),6.14(4H,s),7.4
4(2H,d),7.71(2H,d)Production Example 20 (R) -1- (4-chlorophenyl) -3- (4- (2-methoxyethyl) piperazin-1-yl) methyl-2-pyrrolidinone dimaleate (R) -1- (4-chlorophenyl) -3- (4- (2
-Methoxyethyl) piperazin-1-yl) methyl-2
-5.00 g of pyrrolidinone and 3.30 g of maleic acid in 9
% Water-ethanol (62 ml). After heating to reflux to form a homogeneous solution, the mixture was cooled, and the precipitated solid was collected by filtration and dried to obtain 7.10 g of the desired product. Melting point: 178.5-179.1 ° C 1 H NMR (DMSO, δ ppm): 1.76-1.
98 (1H, m), 2.23-2.35 (1H, m),
2.66-3.30 (13H, m), 3.30 (3H,
s), 3.60-3.72 (2H, m), 3.76-
3.81 (2H, m), 6.14 (4H, s), 7.4
4 (2H, d), 7.71 (2H, d)
【0053】製剤例1(錠剤) 本発明化合物である活性成分と結晶セルロースの全量お
よびトウモロコシデンプンの一部を混合造粒し、トウモ
ロコシデンプンパスタにした。得られた粗粒子をふるい
にかけ、乾燥させて残りのトウモロコシデンプンおよび
ステアリン酸マグネシウムと混合した。次いでこの粗粒
子を1錠当たり、1mg、2mg、25mg、および5
0mgの活性成分を含有する錠剤に圧縮した。Formulation Example 1 (Tablets) The total amount of the active ingredient which is the compound of the present invention, crystalline cellulose and a part of corn starch were mixed and granulated to obtain corn starch pasta. The resulting grit was sieved, dried and mixed with the remaining corn starch and magnesium stearate. The coarse particles were then added at 1 mg, 2 mg, 25 mg, and 5 mg / tablet.
Compressed into tablets containing 0 mg of active ingredient.
【0054】 活性成分 1.0mg 2.0mg 25.0mg 50.0mg 結晶セルロース 49.25mg 48.75mg 37.25mg 100.0mg トウモロコシデンプン 49.25mg 48.75mg 37.25mg 4.25mg ステアリン酸マグネシウム 0.50mg 0.50mg 0.50mg 0.75mgActive ingredient 1.0 mg 2.0 mg 25.0 mg 50.0 mg Microcrystalline cellulose 49.25 mg 48.75 mg 37.25 mg 100.0 mg Maize starch 49.25 mg 48.75 mg 37.25 mg 4.25 mg Magnesium stearate 0.50 mg 0.50 mg 0.50 mg 0.75 mg
【0055】製剤例2(注射剤) 本発明化合物である活性成分600mgをとり、0.9
%生理食塩水10mlに溶かし、ろ過除菌し、10ml
アンプルに封入して注射剤とした。Formulation Example 2 (Injection) 600 mg of the active ingredient which is the compound of the present invention was taken, and 0.9 mg
Dissolved in 10 ml of 10% physiological saline and filtered to remove bacteria.
It was sealed in an ampoule to give an injection.
【0056】評価例1 効果増強作用 D2受容体遮断薬であるハロペリドールのアポモルヒネ誘
発クライミング行動抑制作用に対する試験化合物の効果
増強作用を評価した。5週令のddy系雄性マウスを使用
し、試験化合物経口投与10分後にハロペリドールを0.
23mg/kg(ED50)を経口投与した。その後60分後にアポ
モルヒネ3mg/kgを皮下投与し、20分後にクライミング
行動時間を2分間測定した。結果を表−1(表1)に示
す。試験の結果、本発明化合物は、ハロペリドールの効
果を有意に増強した。Evaluation Example 1 Effect Enhancing Effect The effect enhancing effect of the test compound on the apomorphine-induced climbing behavior inhibitory effect of haloperidol, a D2 receptor blocker, was evaluated. Using a 5-week-old ddy male mouse, haloperidol was added to 0. 10 minutes after oral administration of the test compound.
23 mg / kg (ED50) was orally administered. After 60 minutes, 3 mg / kg of apomorphine was subcutaneously administered, and after 20 minutes, the climbing action time was measured for 2 minutes. The results are shown in Table 1 (Table 1). As a result of the test, the compound of the present invention significantly enhanced the effect of haloperidol.
【0057】[0057]
【表1】 表−1 アポモルヒネクライミング抑制作用 ─────────────────────────────────── 被験薬 用量(mg/kg) クライミング行動時間(秒 ) 平均±SE、N=10 ─────────────────────────────────── 生理食塩水 − 98.9±4.5 試験化合物 3 83.0±6.1 ハロヘ゜リト゛ール 0.23 60.6±10.8** ハロヘ゜リト゛ール 0.23+試験化合物 0.3 52.0±8.3 ハロヘ゜リト゛ール 0.23+試験化合物 1 44.1±8.9 ハロヘ゜リト゛ール 0.23+試験化合物 3 20.3±4.6# ─────────────────────────────────── **:p<0.01 vs 生理食塩水、 #:p<0.05 vs ハロヘ゜リト゛ール単独Table 1 Table 1 Apomorphine climbing inhibitory effect 作用 Test drug dose ( mg / kg) Climbing time (seconds) Average ± SE, N = 10 ─────────────────────────────────生理 Saline − 98.9 ± 4.5 Test compound 3 83.0 ± 6.1 Halohelitol 0.23 60.6 ± 10.8 ** Halohelitol 0.23 + Test compound 0.3 52.0 ± 8.3 Halohelitol 0.23 + Test compound 1 44.1 ± 8.9 Halohelitol 0.23 + Test compound 3 20.3 ± 4.6 # ─────────────────────────────────── **: p <0.01 vs saline, #: p < 0.05 vs halo perimeter alone
【0058】評価例2 副作用軽減作用 D2受容体遮断薬であるハロペリドール誘発カタレプシー
に対する本発明化合物の抑制作用を評価した。7週令の
Wistar系雄性ラットを使用し、試験化合物の経口投与6
0分後にハロペリドールを経口投与し、その1、2、3
および6時間御にカタレプシー時間を最大210秒まで
測定した。カタレプシー時間は表−2(表2)に従いス
コアー化した。評価結果を表−3(表3)に示した。本
発明化合物は、ハロペリドール誘発の副作用であるカタ
レプシーを軽減した。Evaluation Example 2 Effect of Reducing Side Effects The inhibitory effect of the compound of the present invention on haloperidol-induced catalepsy, which is a D2 receptor blocker, was evaluated. 7 weeks old
Oral administration of test compound using Wistar male rats 6
0 minutes later, haloperidol was orally administered, and 1, 2, 3
At 6 hours, the catalepsy time was measured up to 210 seconds. Catalepsy time was scored according to Table-2 (Table 2). The evaluation results are shown in Table 3 (Table 3). The compounds of the present invention alleviated catalepsy, a side effect induced by haloperidol.
【0059】[0059]
【表2】 表−2 カタレプシーのスコアー ─────────────────────── カタレプシー時間(秒) スコアー ─────────────────────── 0 0 1〜30 1 31〜60 2 61〜90 3 91〜120 4 121〜150 5 151〜180 6 181〜210 7 211以上 8 ─────────────────────── [Table 2] Table 2 Catalepsy score ─────────────────────── Catalepsy time (seconds) Score ─────────── ──────────── 0 0 1 to 30 1 31 to 60 2 61 to 90 3 91 to 120 4 121 to 150 5 151 to 180 6 181 to 210 7 211 or more 8 ───── ──────────────────
【0060】[0060]
【表3】 [表−3] ハロペリドール誘発カタレプシー抑制作用 ─────────────────────────────────── 被験薬 用量 カタレプシースコアー (mg/kg p.o.) 平均±SE、N=6 ─────────────────────────────────── ハロヘ゜リト゛ール 0.9 4.3±0.4 ハロヘ゜リト゛ール 0.9+試験化合物 1 4.3±0.4 ハロヘ゜リト゛ール 0.9+試験化合物 3 2.1±0.3 ハロヘ゜リト゛ール 0.9+試験化合物 10 1.8±0.6 ───────────────────────────────────[Table 3] Haloperidol-induced catalepsy inhibitory activity-Test Drug dose Catalepsy score (mg / kg po) Mean ± SE, N = 6 ─────────────────────────────────ハ ロ Haloperitol 0.9 4.3 ± 0.4 Haloperitol 0.9 + Test compound 1 4.3 ± 0.4 Haloperitol 0.9 + Test compound 3 2.1 ± 0.3 Haloperitol 0.9 + Test compound 10 1.8 ± 0.6 ── ───────────────────
【0061】評価例3 副作用軽減作用 D2受容体遮断薬であるハロペリドールの認知障害に対す
る試験化合物の改善効果を評価した。5週令のWistar系
雄性ラットを使用し、シャトル箱を用いて条件回避行動
を調べた。条件回避訓練を1日20試行を10日間行
い、つづいて1日10試行を5日間行い、80%以上の
回避率を3日間連続して示したラットを実験に使用し
た。試験化合物の経口投与60分後にハロペリドールを
経口投与し、その0.5、1、3、6および24時間後に条件回
避行動を測定した。結果を表−4(表4)に示す。本発
明化合物は、ハロペリドールの認知障害を有意に改善し
た。Evaluation Example 3 Effect of Reducing Side Effects The effect of the test compound on the cognitive impairment of haloperidol, a D2 receptor blocker, was evaluated. Using five-week-old male Wistar rats, condition avoidance behavior was examined using a shuttle box. Rats that performed 20 avoidance trainings a day for 10 days, followed by 10 trials a day for 5 days, and showed an avoidance rate of 80% or more for 3 consecutive days were used in the experiments. Haloperidol was orally administered 60 minutes after the oral administration of the test compound, and conditioned avoidance behavior was measured at 0.5, 1, 3, 6, and 24 hours after the administration. The results are shown in Table 4 (Table 4). The compound of the present invention significantly improved haloperidol cognitive impairment.
【0062】[0062]
【表4】 表−4 ハロペリドールの認知障害に対する改善効果 ─────────────────────────────────── 被験薬 用量 条件行動回避率(%) (mg/kg p.o.) 平均±SE、N=6 ─────────────────────────────────── 生理食塩水 − 85.0±5.0 試験化合物 1 88.3±1.7 試験化合物 10 88.3±7.6 ハロヘ゜リト゛ール 0.5 23.3±12.8** ハロヘ゜リト゛ール 0.5+試験化合物 1 41.7±9.5 ハロヘ゜リト゛ール 0.5+試験化合物 3 80.0±5.2# ─────────────────────────────────── **:p<0.01 vs 生理食塩水、 #:p<0.05 vs ハロヘ゜リト゛ール単独Table 4 Table 4 Improvement effect of haloperidol on cognitive impairment 被 験 Test Medication Dose Conditional avoidance rate (%) (mg / kg po) Mean ± SE, N = 6 ──────────────────────────── ─────── Physiological saline − 85.0 ± 5.0 Test compound 1 88.3 ± 1.7 Test compound 10 88.3 ± 7.6 Halohelitol 0.5 23.3 ± 12.8 ** Halohelitol 0.5 + Test compound 1 41.7 ± 9.5 Halohelitol 0.5 + Test compound 3 80.0 ± 5.2 # ─────────────────────────────────── **: p <0.01 vs saline, #: p <0.05 vs haloperitol alone
【0063】[0063]
【発明の効果】上記の評価例から本発明の化合物は、ド
ーパミン拮抗薬の効果を増強させ、ドーパミン拮抗薬の
副作用を軽減、改善することから、ドーパミン拮抗薬を
治療に用いる疾患において、有用な薬剤であることが明
らかである。From the above evaluation examples, the compounds of the present invention enhance the effects of dopamine antagonists, reduce and improve the side effects of dopamine antagonists, and are therefore useful in diseases in which dopamine antagonists are used for treatment. It is clear that it is a drug.
───────────────────────────────────────────────────── フロントページの続き (72)発明者 長瀬 洋 千葉県茂原市東郷1144番地 三井化学株式 会社内 (72)発明者 掘込 和利 千葉県茂原市東郷1900番地の1 三井製薬 工業株式会社内 (72)発明者 高橋 真司 千葉県茂原市東郷1900番地の1 三井製薬 工業株式会社内 (72)発明者 高木 香 千葉県茂原市東郷1900番地の1 三井製薬 工業株式会社内 ──────────────────────────────────────────────────続 き Continuing on the front page (72) Inventor Hiroshi Nagase 1144 Togo, Mobara-shi, Chiba Mitsui Chemicals Co., Ltd. (72) Inventor Kazutoshi 1900-1, Togo, Togo, Mobara-shi, Chiba Mitsui Pharmaceutical Co., Ltd. (72) Inventor Shinji Takahashi 1900, Togo, Togo, Mobara-shi, Chiba Pref. (72) Inventor Kaoru 1,900-1, Togo, Togo, Mobara-shi, Chiba Pref.
Claims (8)
−(2−メトキシエチル)ピペラジン−1−イル]メチ
ル−2−ピロリジノン、またはその薬理学的に許容され
る塩およびその薬理学的に許容される塩の水和物を有効
成分として含有してなるドーパミン拮抗薬の効果増強
剤。1- (4-chlorophenyl) -3- [4
-(2-methoxyethyl) piperazin-1-yl] methyl-2-pyrrolidinone or a pharmacologically acceptable salt thereof and a hydrate of the pharmacologically acceptable salt thereof as an active ingredient. Dopamine antagonist effect enhancer.
−(2−メトキシエチル)ピペラジン−1−イル]メチ
ル−2−ピロリジノンの絶対配置がRである請求項1記
載のドーパミン拮抗薬の効果増強剤。2. 1- (4-chlorophenyl) -3- [4
The effect enhancer of a dopamine antagonist according to claim 1, wherein the absolute configuration of-(2-methoxyethyl) piperazin-1-yl] methyl-2-pyrrolidinone is R.
ある請求項2記載のドーパミン拮抗薬の効果増強剤。3. The dopamine antagonist effect enhancer according to claim 2, wherein the dopamine antagonist is a D2 receptor blocker.
剤、顆粒剤、散剤、懸濁剤、乳化剤、カプセル剤、また
はシロップ剤の経口投与剤、注射剤、座剤または輸液用
等張液である請求項1から3記載のドーパミン拮抗薬の
効果増強剤。4. The effect enhancer of a dopamine antagonist is a tablet, granule, powder, suspension, emulsifier, capsule, or syrup for oral administration, injection, suppository or isotonic solution for infusion. The agent for enhancing the effect of a dopamine antagonist according to any one of claims 1 to 3.
−(2−メトキシエチル)ピペラジン−1−イル]メチ
ル−2−ピロリジノン、またはその薬理学的に許容され
る塩およびその薬理学的に許容される塩の水和物を有効
成分として含有してなるドーパミン拮抗薬の副作用軽減
剤。5. 1- (4-chlorophenyl) -3- [4
-(2-methoxyethyl) piperazin-1-yl] methyl-2-pyrrolidinone or a pharmacologically acceptable salt thereof and a hydrate of the pharmacologically acceptable salt thereof as an active ingredient. A drug that reduces the side effects of a dopamine antagonist.
−(2−メトキシエチル)ピペラジン−1−イル]メチ
ル−2−ピロリジノンの絶対配置がRである請求項5記
載のドーパミン拮抗薬の副作用軽減剤。6. 1- (4-chlorophenyl) -3- [4
The agent for reducing a side effect of a dopamine antagonist according to claim 5, wherein the absolute configuration of-(2-methoxyethyl) piperazin-1-yl] methyl-2-pyrrolidinone is R.
ある請求項6記載のドーパミン拮抗薬の副作用軽減剤。7. The agent for reducing a side effect of a dopamine antagonist according to claim 6, wherein the dopamine antagonist is a D2 receptor blocker.
剤、顆粒剤、散剤、懸濁剤、乳化剤、カプセル剤、また
はシロップ剤の経口投与剤、注射剤、座剤または輸液用
等張液である請求項5から7記載のドーパミン拮抗薬の
副作用軽減剤。8. The agent for reducing side effects of a dopamine antagonist is a tablet, granule, powder, suspension, emulsifier, capsule, or syrup for oral administration, injection, suppository or isotonic solution for infusion. 8. The agent for reducing side effects of a dopamine antagonist according to claim 5.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP14304998A JPH11335286A (en) | 1998-05-25 | 1998-05-25 | Effect-reinforcing medicament for dopamine antagonist |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP14304998A JPH11335286A (en) | 1998-05-25 | 1998-05-25 | Effect-reinforcing medicament for dopamine antagonist |
Publications (1)
| Publication Number | Publication Date |
|---|---|
| JPH11335286A true JPH11335286A (en) | 1999-12-07 |
Family
ID=15329730
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP14304998A Pending JPH11335286A (en) | 1998-05-25 | 1998-05-25 | Effect-reinforcing medicament for dopamine antagonist |
Country Status (1)
| Country | Link |
|---|---|
| JP (1) | JPH11335286A (en) |
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| JP2004517937A (en) * | 2001-01-29 | 2004-06-17 | 大塚製薬株式会社 | 5-HT1A receptor subtype agonist |
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-
1998
- 1998-05-25 JP JP14304998A patent/JPH11335286A/en active Pending
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