JPS63264525A - Medicine composition containing piperazine derivative and having active oxygen production inhibiting and active oxygen removing action - Google Patents
Medicine composition containing piperazine derivative and having active oxygen production inhibiting and active oxygen removing actionInfo
- Publication number
- JPS63264525A JPS63264525A JP9696587A JP9696587A JPS63264525A JP S63264525 A JPS63264525 A JP S63264525A JP 9696587 A JP9696587 A JP 9696587A JP 9696587 A JP9696587 A JP 9696587A JP S63264525 A JPS63264525 A JP S63264525A
- Authority
- JP
- Japan
- Prior art keywords
- active oxygen
- oxirane
- ylcarbonyl
- piperazine
- composition containing
- 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.)
- Granted
Links
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- 229910052760 oxygen Inorganic materials 0.000 title claims abstract description 30
- 239000001301 oxygen Substances 0.000 title claims abstract description 30
- 238000004519 manufacturing process Methods 0.000 title claims abstract description 18
- 230000002401 inhibitory effect Effects 0.000 title claims abstract description 10
- 239000003814 drug Substances 0.000 title abstract description 27
- 239000000203 mixture Substances 0.000 title abstract description 12
- 150000004885 piperazines Chemical class 0.000 title abstract description 4
- 229940079593 drug Drugs 0.000 title description 25
- 150000003839 salts Chemical class 0.000 claims abstract description 13
- 231100000252 nontoxic Toxicity 0.000 claims abstract description 10
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- GLUUGHFHXGJENI-UHFFFAOYSA-N Piperazine Chemical compound C1CNCCN1 GLUUGHFHXGJENI-UHFFFAOYSA-N 0.000 abstract description 4
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- 230000001629 suppression Effects 0.000 description 1
- 208000024891 symptom Diseases 0.000 description 1
- 239000011975 tartaric acid Substances 0.000 description 1
- 235000002906 tartaric acid Nutrition 0.000 description 1
- 229940124597 therapeutic agent Drugs 0.000 description 1
- 125000005270 trialkylamine group Chemical group 0.000 description 1
- 210000003462 vein Anatomy 0.000 description 1
- 238000005303 weighing Methods 0.000 description 1
Abstract
Description
【発明の詳細な説明】
本発明は、ピペラジン誘導体を含有する活性酸素産生抑
制ならびに活性酸素除去作用を有する医薬組成物に関す
る。DETAILED DESCRIPTION OF THE INVENTION The present invention relates to a pharmaceutical composition containing a piperazine derivative, which has the effect of inhibiting active oxygen production and removing active oxygen.
安定状態の酸素(三重項酸素)がキサンチンオキシダー
ゼやNADP11オキシダーゼの関与により1電子を得
ることでスーパーオキサイドアニオンが生成し、さらに
ヒドロキシラジカル、過酸化水素、次亜塩素酸のアニオ
ン、1重項酸素などの活性酸素が生じる。Stable oxygen (triplet oxygen) acquires one electron through the involvement of xanthine oxidase and NADP11 oxidase, producing superoxide anion, which further generates hydroxyl radical, hydrogen peroxide, hypochlorous acid anion, and singlet oxygen. Active oxygen such as is generated.
これらの活性酸素のフリーラジカルは、顆粒球に関与し
ている。These active oxygen free radicals are involved in granulocytes.
従って、活性酸素の異常な産生を抑制する物質る。Therefore, it is a substance that suppresses the abnormal production of active oxygen.
そこで、本発明者らは、活性酸素産生を抑制する化合物
を見い出すべく鋭意研究を行ってきた。Therefore, the present inventors have conducted intensive research to find a compound that suppresses active oxygen production.
用を有することを見い出し、本発明を完成した。The present invention was completed based on this discovery.
従って、本発明の目的は、有用な活性酸素産生抑制なら
びに活性酸素除去作用を有する医薬組成物を提供するに
ある。Therefore, an object of the present invention is to provide a pharmaceutical composition that has useful effects of inhibiting active oxygen production and removing active oxygen.
詳細には、次の一般式(1)
nは0〜3の整数を示す)で表わされるピペラジンmA
体又はその無毒性塩を有効成分として含有する活性酸素
産生抑制ならびに活性酸素除去作用を有する医薬組成物
に関する。In detail, piperazine mA represented by the following general formula (1) where n is an integer of 0 to 3)
The present invention relates to a pharmaceutical composition containing active oxygen or a non-toxic salt thereof as an active ingredient and having an active oxygen production inhibiting and active oxygen removing action.
上記一般式(1)で表わされる化合物は、本発明者らに
より既に冠状動脈結紮による実験的心筋梗塞モデルで効
果を示し、心筋梗塞の予防および治療剤として有用であ
ることが知られている。The compound represented by the above general formula (1) has already been shown to be effective in an experimental myocardial infarction model using coronary artery ligation by the present inventors, and is known to be useful as a preventive and therapeutic agent for myocardial infarction.
(特開昭57−169478 、特開昭58−1268
79)前記一般式(I)中のRが低級アルキル基の場合
の例としては、メチル基、エチル基、プロピル基、イソ
ブチル基、n−ブチル基、5ec−ブチル基などが挙げ
られる。(Japanese Patent Publication No. 57-169478, Japanese Patent Application Publication No. 58-1268
79) Examples of the case where R in the general formula (I) is a lower alkyl group include a methyl group, an ethyl group, a propyl group, an isobutyl group, an n-butyl group, a 5ec-butyl group, and the like.
また、無毒性塩としては、ナトリウム、カリウム、カル
シウム、マグネシウム、さらには、トリアルキルアミン
、ジベンジルアミン、N−低級アルキルピペリジン、α
−フェネチルアミン、1−(1−ナフチル)エチルアミ
ン、N−ベンジル−β−フェネチルアミンなどの無毒性
塩、あるいは塩酸、臭化水素酸、ギ酸、硫酸、フマール
酸、マレイン酸、酒石酸などとの無毒性塩が挙げられる
。In addition, non-toxic salts include sodium, potassium, calcium, magnesium, trialkylamine, dibenzylamine, N-lower alkylpiperidine, α
- Non-toxic salts of phenethylamine, 1-(1-naphthyl)ethylamine, N-benzyl-β-phenethylamine, or non-toxic salts with hydrochloric acid, hydrobromic acid, formic acid, sulfuric acid, fumaric acid, maleic acid, tartaric acid, etc. can be mentioned.
前記一般式(I)で表わされる化合物は、たとえば次の
方法により得ることができる。The compound represented by the general formula (I) can be obtained, for example, by the following method.
C113Cl5−−→ (1)
(ロ)
(式中、Rおよびnは前記と同じ意味を来年=シー−−
す)
−i式(1)で表わされる化合物の具体例としては、下
記のものを挙げることができる。C113Cl5--→ (1) (b) (In the formula, R and n have the same meanings as above, next year = C--
-i Specific examples of the compound represented by formula (1) include the following.
(2R,3R) −3−((S) −1−(4−(4−
メトキシフェニルメチル)ピペラジン−1−イルカルボ
ニル)−3−メチルブチルカルバモイル〕オキシラン−
2−カルボン酸、
(2R,3R) −3−(TS)−1−(4−(3,4
−ジメトキシフェニルメチル)ピペラジン−1−イルカ
ルボニル)−3−メチルブチルカルバモイル〕オキシラ
ン−2−カルボン酸、
(2R,3R) −3−((S)−3−メチル−1−(
4−(2,3,4−)ジメトキシフェニルメチル)ピペ
ラジン−1−イルカルボニル)ブチルカルバモイル〕オ
キシラン−2−カルボン酸、
(2R,3R) −3−((5)−3−メチル−1−
(4−(3,4,5−トリメトキシフェニルメチル)ピ
ペラジン−1−イルカルボニル)ブチルカルバモイル〕
オキシラン−2−カルボン酸、
(21?、31?) −3−(TS)−1−(4−ベン
ジルピペラジン−1−イルカルボニル)−3−メチルブ
チルカルバモイル〕オキシラン−2−カルボン酸、(2
S、3S) −’3−((S) −1−(4−(4−メ
トキシフェニルメチル)ピペラジン−ニーイルカルボニ
ル)−3−メチルブチルカルバモイル〕オキシラン−2
−カルボン酸、
(2S、3S) −3−((S)−1−(4−(3,4
−ジメトキシフェニルメチル)ピペラジン−1−イルカ
ルボニル)−3−メチルブチルカルバモイル〕オキシラ
ン−2−カルボン酸、
(2S、3S) −3−((Sl−3−メチル−1−
(4−(2,3,4−トリメトキシフェニルメチル)ピ
ペラジン−1−イルカルボニル)ブチルカルバモイル〕
オキシラン−2−カルボン酸、
(2S、3S) −3−((S)−3−メチル−1−(
4−(3,4,5−トリメトキシフェニルメチル)ピペ
ラジン−1−イルカルボニル)ブチルカルバモイル〕オ
キシラン−2−カルボン酸、
(28,35) −3−((S)−1−(4−ベンジル
ピペラジン−1−イルカルボニル)−3−メチルブチル
カルバモイル〕オキシラン−2−カルボン酸。(2R,3R) -3-((S) -1-(4-(4-
methoxyphenylmethyl)piperazin-1-ylcarbonyl)-3-methylbutylcarbamoyl]oxirane
2-carboxylic acid, (2R,3R) -3-(TS)-1-(4-(3,4
-dimethoxyphenylmethyl)piperazin-1-ylcarbonyl)-3-methylbutylcarbamoyl]oxirane-2-carboxylic acid, (2R,3R) -3-((S)-3-methyl-1-(
4-(2,3,4-)dimethoxyphenylmethyl)piperazin-1-ylcarbonyl)butylcarbamoyl]oxirane-2-carboxylic acid, (2R,3R) -3-((5)-3-methyl-1-
(4-(3,4,5-trimethoxyphenylmethyl)piperazin-1-ylcarbonyl)butylcarbamoyl]
oxirane-2-carboxylic acid, (21?, 31?) -3-(TS)-1-(4-benzylpiperazin-1-ylcarbonyl)-3-methylbutylcarbamoyl]oxirane-2-carboxylic acid, (2
S, 3S) -'3-((S) -1-(4-(4-methoxyphenylmethyl)piperazine-neeylcarbonyl)-3-methylbutylcarbamoyl]oxirane-2
-carboxylic acid, (2S,3S) -3-((S)-1-(4-(3,4
-dimethoxyphenylmethyl)piperazin-1-ylcarbonyl)-3-methylbutylcarbamoyl]oxirane-2-carboxylic acid, (2S,3S) -3-((Sl-3-methyl-1-
(4-(2,3,4-trimethoxyphenylmethyl)piperazin-1-ylcarbonyl)butylcarbamoyl]
Oxirane-2-carboxylic acid, (2S,3S)-3-((S)-3-methyl-1-(
4-(3,4,5-trimethoxyphenylmethyl)piperazin-1-ylcarbonyl)butylcarbamoyl]oxirane-2-carboxylic acid, (28,35) -3-((S)-1-(4-benzyl) Piperazin-1-ylcarbonyl-3-methylbutylcarbamoyl]oxirane-2-carboxylic acid.
これらの化合物のエステル体または無毒性塩も本発明の
有効成分である。Ester forms or non-toxic salts of these compounds are also active ingredients of the present invention.
本発明における一般式(I)で表わされる化合物および
その無毒性塩が活性酸素産生抑制作用を有する医薬組成
物として有用であることは、1nvjtro及びin
vivoにおけるウサギ顆粒球からの活性酸素産生に及
ぼす薬物の影ツを観察することにより明らかになった。The fact that the compound represented by general formula (I) and its non-toxic salt in the present invention is useful as a pharmaceutical composition having an active oxygen production inhibiting effect has been demonstrated in 1nvjtro and in vitro studies.
This was revealed by observing the effects of drugs on active oxygen production from rabbit granulocytes in vivo.
すなわち、被験薬物として、(2R,3R) −3−(
(Sl −3−メチル−1−(4−(2,3,4−1−
リメトキシフェニルメチル)ピペラジン−1−イルカル
ボニル)ブチルカルバモイル〕オキシラン−2−カルボ
ン酸エチル%硫酸塩を用い、兎の顆粒球のformyl
−methiony+−1eucyl−phenyla
lanine (FMLP)刺激により発生ずるルミノ
ール依存性の化学発光に及ぼす影響を観察した実験にお
いて表1で示す様に被験薬物はコントロールに比較して
、活性酸素の産生を30μ門で90%抑制した。That is, as a test drug, (2R,3R) -3-(
(Sl -3-methyl-1-(4-(2,3,4-1-
rimethoxyphenylmethyl)piperazin-1-ylcarbonyl)butylcarbamoyl]oxirane-2-carboxylic acid ethyl% sulfate was used to formyl granulocytes from rabbits.
-methiony+-1eucyl-phenyla
In an experiment to observe the effect on luminol-dependent chemiluminescence generated by lanine (FMLP) stimulation, as shown in Table 1, the test drug inhibited the production of active oxygen by 90% at 30 μm compared to the control.
又in vivoにおける実験、すなわち被験薬物を兎
に20mg/kg静注した後得られた顆粒球を用いた実
験でも、コントロールに比べ有意の抑制を示した(表2
)。In addition, an in vivo experiment using granulocytes obtained after intravenously injecting the test drug into rabbits at 20 mg/kg also showed significant inhibition compared to the control (Table 2
).
さらに、本発明における一般式(1)で表わされる化合
物が除去(Scavenging)効果、すなわち発生
した活性酸素を除去する効果も有することが、ハイポキ
サンチン−キサンチンオキシダーゼ系で発生する活性酸
素に対する薬物の影舌を調べる実験(実験3)、ならび
にHtOz−NaOC/!系における薬物の効果(実験
4)を調べる実験により明らかになった。表4で示す様
にH20□−NaOCjl!系において、薬物は、30
μHで化学発光を60%抑制した。Furthermore, the fact that the compound represented by the general formula (1) in the present invention also has a scavenging effect, that is, an effect of removing generated active oxygen, indicates that the drug has no effect on active oxygen generated in the hypoxanthine-xanthine oxidase system. Experiment examining the tongue (Experiment 3) and HtOz-NaOC/! This was revealed through an experiment to investigate the effect of drugs on the system (Experiment 4). As shown in Table 4, H20□-NaOCjl! In the system, the drug is
Chemiluminescence was suppressed by 60% at μH.
また、本発明の有効成分である一般式(1)で表わされ
る化合物はマウスにおけ゛る急性毒性試験により、生体
に対して安全性の高い物質であることがわかる。Further, the compound represented by the general formula (1), which is the active ingredient of the present invention, has been found to be a highly safe substance for living organisms through an acute toxicity test in mice.
本発明における一般式(1)の化合物およびその無毒性
塩の投与量は、化合物の種類および患者の症状の程度に
よって異なるが、通常は1日約10rrg〜1gを患者
に投与すればよい。The dosage of the compound of general formula (1) and its nontoxic salt in the present invention varies depending on the type of compound and the severity of the patient's symptoms, but it is usually sufficient to administer about 10 rrg to 1 g per day to the patient.
一般式(1)で表わされる化合物およびその塩は、これ
を活性酸素産生抑制ならびに活性酸素除去作用を有する
医薬組成物として用いる場合、通六
常は製剤的担体と途に製剤組成物の形態とされる。When the compound represented by general formula (1) and its salts are used as a pharmaceutical composition having active oxygen production inhibiting and active oxygen removing effects, they are usually combined with a pharmaceutical carrier and in the form of a pharmaceutical composition. be done.
担体としては、使用形態に応じた薬剤を調製するのに通
常使用される増量剤、結合剤、崩壊剤、滑沢剤等の希釈
剤あるいは賦形剤が用いられる。As the carrier, diluents or excipients such as fillers, binders, disintegrants, lubricants, etc., which are commonly used to prepare drugs depending on the usage form, are used.
投与形態としては、注射剤、散剤、カプセル剤、顆粒剤
、錠剤などいずれの形態でも可能である。The dosage form may be any form such as injection, powder, capsule, granule, or tablet.
錠剤の形態として用いるに際しては担体として、例えば
乳糖、白糖、塩化ナトリウム、ブドウ糖婆、デンプン、
炭酸カルシウム、結晶セルロース、ケイ酸等の賦形剤、
水、エタノール、プロパツール、ブドウ直デンプン液、
ゼラチン溶液、カルボキシメチルセルロース、メチルセ
ルロース、リン酸カリウム等の結合剤、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、ステアリン酸モノグリセリド、デ
ンプン、乳糖等の崩壊剤、ステアリン酸塩、ホウ酸末、
固体ポリエチレングリコール等の滑沢剤等この分野で広
く用いられているものを使用することができる。更に必
要に応じて糖衣錠、ゼラチン被包錠、フィルムコーティ
ング錠等にすることもできる。When used in tablet form, carriers include, for example, lactose, sucrose, sodium chloride, glucose, starch,
Excipients such as calcium carbonate, crystalline cellulose, and silicic acid;
Water, ethanol, propatool, grape starch solution,
Gelatin solution, carboxymethylcellulose, methylcellulose, binders such as potassium phosphate, dried starch,
Disintegrants such as sodium alginate, agar powder, sodium bicarbonate, calcium carbonate, stearic acid monoglyceride, starch, lactose, stearate, boric acid powder,
Lubricants such as solid polyethylene glycol and other lubricants widely used in this field can be used. Furthermore, it can be made into sugar-coated tablets, gelatin-encapsulated tablets, film-coated tablets, etc., if necessary.
注射剤として調製される場合には、希釈剤として例えば
水、エチルアルコール、プロピレングリコール、ポリオ
キシエチレンソルビソト、ソルビタンエステル等をあげ
ることができる。この際、等張性の溶液を調製するのに
充分な世の食塩、ブドウ糖あるいはグリセリンを含有さ
せてもよく、また、通常の溶解補助剤、緩衝剤、無痛化
剤、保存剤等を必要に応じて含有させてもよい。When prepared as an injection, examples of diluents include water, ethyl alcohol, propylene glycol, polyoxyethylene sorbisoto, and sorbitan ester. At this time, sufficient common salt, glucose, or glycerin may be included to prepare an isotonic solution, and conventional solubilizing agents, buffering agents, soothing agents, preservatives, etc. may be necessary. It may be included depending on the situation.
以上に述べたように、前記一般式(I)で表わされるピ
ペラジン誘導体またはその無毒性塩は、優れた活性酸素
産生抑制ならびに活性酸素除去作有用である。As described above, the piperazine derivative represented by the general formula (I) or its nontoxic salt has excellent effects of inhibiting active oxygen production and removing active oxygen.
次に本発明において、有効成分として用いられ薬組成物
として有用であり、安全性が高いことを示す試験例と一
般式(1)の化合物の製剤例を示す実施例を挙げて本発
明を具体的に説明する。Next, the present invention will be specifically described with reference to test examples showing that it is used as an active ingredient, useful as a pharmaceutical composition, and highly safe, and examples showing formulation examples of the compound of general formula (1). Explain in detail.
実施例1
方−広
成果
ホルミル−メチオニル−ロイシル−フェニルアラニン(
FMLPと略す)、ルミノール、キサンチンオキシダー
ゼ(XODと略す)(0,61/mg蛋白)、カタラー
ゼ(26,0OOU/■蛋白)はシグマ社製を用いた。Example 1 - Hirokou formyl-methionyl-leucyl-phenylalanine (
Luminol, xanthine oxidase (abbreviated as XOD) (0.61/mg protein), and catalase (26.0 OOU/■ protein) manufactured by Sigma were used.
ハイポキサンチン、過酸化水素(30%)、珈。Hypoxanthine, hydrogen peroxide (30%), coffee.
次亜〃素酸(5%溶液)は、和光補薬(株製を用いた。Hypochlorous acid (5% solution) manufactured by Wako Hyakuyaku Co., Ltd. was used.
FMLPとルミノールは、IIEPBs−5aline
(5mFIのN−2−ヒドロキシエチルピペラジン−
N’−2−エタンスルホン酸pH7,4で緩衝化された
生理金食塩水)で希釈する前にジメチルスルホキサイド
(DMSO)に溶解した。反応混合物中のDMSOの最
終濃度は10μHで、この濃度は反応に影響を与えなか
ヘパリンを添加した血液(70〜80mj2)を雄性白
兎(2,2〜3.0kg)から得、生理食塩水中2%デ
キストラン(半井化学■製)に混和した。FMLP and Luminol are IIEPBs-5aline
(5mFI N-2-hydroxyethylpiperazine-
N'-2-ethanesulfonic acid was dissolved in dimethyl sulfoxide (DMSO) before dilution with normal gold saline buffered pH 7.4. The final concentration of DMSO in the reaction mixture was 10 μH; this concentration did not affect the reaction. Heparinized blood (70-80 mj2) was obtained from a male white rabbit (2,2-3.0 kg) and diluted in saline for 2 h. % dextran (manufactured by Hanui Kagaku ■).
赤血球を室温で30分間沈澱させた。白血球に富んだ血
しょうをナトリウムメトリゾエートフィコール溶液に−
ガアードNyegaard社製)に重層した後、4℃、
40分間8004で遠心分離した。Red blood cells were allowed to settle for 30 minutes at room temperature. Plasma rich in white blood cells is added to sodium metrizoate ficoll solution.
(manufactured by Nyegaard), and then heated at 4°C.
Centrifuged at 8004 for 40 minutes.
ベレットに155mMの塩化アンモニウム溶液を加え赤
血球を溶かした。残存する顆粒球を冷HEPES−Sa
lineで2度洗浄し、同じ溶媒に再懸濁した。A 155 mM ammonium chloride solution was added to the pellet to lyse the red blood cells. The remaining granulocytes were placed in cold HEPES-Sa.
The cells were washed twice with 100% chlorine and resuspended in the same solvent.
ヒ学 光(CLと す)の測
CLはルミフォトメーター(n+odel TD400
0; ラボサイエンス社製)で測定し、ミリボルトを記
録した。他で言及しない限り反応混合物は2.5m+の
CaC12および5mMのKClを含有するHEPHS
−3alineに浮遊させた細胞浮遊液(I X 10
)細胞/m1l)0.2111ルミノール(最終濃度3
0μM)および薬物より成り、0.5mj2のポリスチ
レン製のキュヘット中で反応を行った。薬物は、H20
□+Na0Cl系及びハイポキサンチン−XOD系で生
成したルミノール依存性のCLを抑制する能力について
もテストした。Higaku Hikari (CL) measurement CL is measured using a Lumiphotometer (n+odel TD400
0; manufactured by Labo Science) and recorded in millivolts. Unless otherwise stated, reaction mixtures were HEPHS containing 2.5 m+ CaC12 and 5mM KCl.
Cell suspension suspended in -3aline (I x 10
) cells/ml) 0.2111 luminol (final concentration 3
(0 μM) and drug, and the reaction was carried out in a 0.5 mj2 polystyrene cuchette. The drug is H20
The ability to suppress luminol-dependent CL produced by the □+Na0Cl and hypoxanthine-XOD systems was also tested.
同ff1(0,1njりの10 #M 8202と30
.crMのルミノールそして薬物又は緩衝液を予め混和
し、37℃に温度制御したルミフォトメーターの計数室
においたのち10μHのNa0C1(0,1ml>を注
入することで活性化した。Same ff1 (0,1nj ri no 10 #M 8202 and 30
.. crM luminol and drug or buffer were premixed and placed in the counting chamber of a lumiphotometer controlled at 37° C., and activated by injecting 10 μH of Na0C1 (0.1 ml).
XODで触媒されるスーパーオキサイドアニオンの生成
は、同様な方法により連続的にモニターした。20μl
の=;1・Φ・$61416(4tJ/mj?)をハイ
ポキサンチン(1mM)、ルミノール(30μM)そし
て種々の濃度の薬物又は緩衝液を含むキュベツトに添加
した。発光量はCL曲曲線面面積より評価し、コントロ
ールのCLと比較して抑制率を求めた。The production of superoxide anion catalyzed by XOD was continuously monitored by a similar method. 20μl
=;1.Φ.$61416 (4tJ/mj?) was added to cuvettes containing hypoxanthine (1mM), luminol (30μM) and various concentrations of drug or buffer. The luminescence amount was evaluated from the CL curved surface area, and the suppression rate was determined by comparing it with the control CL.
被験薬物としては、(2R,3R) −3−((31−
3−メチル−1−(4−(2,3,4−トリメトキシフ
ェニルメチル)ピペラジン−1−イルカル采ニル)ブチ
ルカルバモイル〕オキシラン−2−カルボン酸エチル2
硫i塩を用いた。The test drug was (2R,3R)-3-((31-
Ethyl 3-methyl-1-(4-(2,3,4-trimethoxyphenylmethyl)piperazin-1-ylcarbutyl)butylcarbamoyl]oxirane-2-carboxylate 2
A sulfur salt was used.
実験1 ルミノール依存性の化学発光生成に対する薬物
の効果(in vitro)
顆粒球(IXIO”細胞7m1)を種々の濃度の薬物と
37℃で30分間インキュベートしたのち遠心分離し薬
物を除くため2度HEPES−saline (4°C
)で洗浄した。その後、10分間インキュベート(37
℃)した後FMLP刺激により生成したCLを測定した
。その結果を表1に示す。Experiment 1 Effect of drugs on luminol-dependent chemiluminescence production (in vitro) Granulocytes (7 ml of IXIO" cells) were incubated with various concentrations of drugs for 30 minutes at 37°C, then centrifuged and incubated twice with HEPES to remove the drugs. -saline (4°C
). Then, incubate for 10 minutes (37
℃), and then the CL generated by FMLP stimulation was measured. The results are shown in Table 1.
表 1
実験2 ルミノール依存性の化学発光生成に対する薬物
の効果(in vivo)
12匹の雄性白兎(2,0〜2.3kg)を無作為に薬
物処置又はコントロール群に振り分けた。薬物(20r
rw/’ kg)は5 mllの生理食塩水に溶かし、
q沖
5分間を要し静注した。コントロールも同様に生理食塩
水を投与した。Table 1 Experiment 2 Effect of drugs on luminol-dependent chemiluminescence production (in vivo) Twelve male white rabbits (2.0-2.3 kg) were randomly assigned to drug treatment or control groups. Drugs (20r
rw/' kg) was dissolved in 5 ml of physiological saline,
It took 5 minutes for intravenous injection. Physiological saline was also administered to controls in the same manner.
注入5分後にヘパリン添加血液を得た。Heparinized blood was obtained 5 minutes after injection.
顆粒球は顆粒球の調製で記載した方法により得た。その
結果を表2に示す。Granulocytes were obtained by the method described for the preparation of granulocytes. The results are shown in Table 2.
表 2
* p < 0.05 (Mann−Whitney
U test)実験3 ハイポキサンチン−キサンチ
ンオキシダーゼ系のルミノール依存性化学発光に対する
薬物の効果(除去効果)
20μlのXOD (4U/ ml )をハイポキサン
チン(1mM)、ルミノール(50μM)、種々ノ薬物
を含むキュベツトに添加した。CL生成はCLカーブ下
の面積で評価し、CL反応を100%に設定したコント
ロールと比較した。その結果を表3に示す。Table 2 * p < 0.05 (Mann-Whitney
U test) Experiment 3 Effect of drugs on luminol-dependent chemiluminescence of hypoxanthine-xanthine oxidase system (removal effect) 20 μl of XOD (4 U/ml) containing hypoxanthine (1 mM), luminol (50 μM), and various drugs Added to cuvette. CL production was evaluated by the area under the CL curve and compared with a control in which the CL response was set at 100%. The results are shown in Table 3.
表3
実験4 1(zo□+Na0C12系のルミノール依存
性化学発光に対する薬物の効果(叶丈hpつ
表 4
本発明の活性成分である一般式(1)で表わされる化合
物は、実験1及び2から活性酸素産生抑制作用を有する
ことが明らかとなり、また実験3及び4から発生した活
性酸素の除去効果をも有することが明らかとなった。Table 3 Experiment 4 1 (Effect of drugs on luminol-dependent chemiluminescence of zo□+Na0C12 system) It has become clear that it has the effect of inhibiting the production of active oxygen, and from Experiments 3 and 4, it has also become clear that it has the effect of removing the active oxygen generated.
実施例2 2法責檀広慧 体重20〜28gのddN系雄性マウスを用いた。Example 2 2 Hōsendan Hirokei ddN male mice weighing 20 to 28 g were used.
ダ −
薬物は尾静脈より投与した。その結果、表φに不すよう
に本発明の薬剤は安全性が高いことが確認表り
但し、化合物1 (2[?、3R) −3−((S
) −3−メチル−1−(4−(2,3,4−トリメト
キシフェニルメチル)ピペラジン−1−イルカルボニル
)ブチルカルバモイル〕オキシラン−2−カルボン酸エ
チル2硫酸塩
化合物2 (2R,31?) −3−((51−3
−メチル−1−(4−(2,3,4−1−リメトキシフ
ェニルメチル)ピペラジン−1−イルカルボニル)ブチ
ルカルバモイル〕オキシラン−2−カルボン酸ナトリウ
ム
化合物3 (25,3S) −3−((31−3−
メチル−1−(4−(2,3,4−トリメトキシフェニ
ルメチル)ピペラジン−1−イルカルボニル)ブチルカ
ルバモイル〕オキシラン−2−カルボン酸エチル%硫酸
塩
化合物4 (2S、3S) −3−((Sl −3
−メチル−1−(4−(2,3,4−トリメトキシフェ
ニルメチル)ピペラジン−1−イルカルボニル)ブチル
カルバモイル〕オキシラン−2−カルボン酸ナトリウム
実施例3 製剤例(錠剤)
1錠(220mg)中下記成分を含有するフィルムコー
ティング錠とする。- The drug was administered through the tail vein. As a result, as shown in Table φ, it was confirmed that the drug of the present invention is highly safe. However, compound 1 (2[?, 3R) -3-((S
) -3-Methyl-1-(4-(2,3,4-trimethoxyphenylmethyl)piperazin-1-ylcarbonyl)butylcarbamoyl]oxirane-2-carboxylic acid ethyl disulfate Compound 2 (2R, 31?) ) -3-((51-3
-Methyl-1-(4-(2,3,4-1-rimethoxyphenylmethyl)piperazin-1-ylcarbonyl)butylcarbamoyl]oxirane-2-carboxylic acid sodium compound 3 (25,3S) -3-( (31-3-
Ethyl methyl-1-(4-(2,3,4-trimethoxyphenylmethyl)piperazin-1-ylcarbonyl)butylcarbamoyl]oxirane-2-carboxylate% sulfate Compound 4 (2S, 3S) -3-( (Sl-3
-Sodium methyl-1-(4-(2,3,4-trimethoxyphenylmethyl)piperazin-1-ylcarbonyl)butylcarbamoyl]oxirane-2-carboxylate Example 3 Formulation example (tablet) 1 tablet (220 mg) Film-coated tablets containing the following ingredients.
(2R,3R) −3−((31−3−メチル−I−(
4−(2,3,4−トリメトキシフェニルメチル)ピペ
ラジン−1−イルカル
ボニル)ブチルカルバモイル〕オキシ
ラン−2−カルボン酸ナトリウム 50■乳$J!
100 mg
結晶セルロース 50mgステアリ
ン酸マグネシウム 1mgヒドロキシプロ
ピルメチルセルロース15mgヒドロキシプロピルセル
ロース 4mg本発明において有効成分として用
いられる他の化合物も同様な処方によりフィルムコーテ
ィング錠とすることが可能である。(2R,3R) -3-((31-3-methyl-I-(
Sodium 4-(2,3,4-trimethoxyphenylmethyl)piperazin-1-ylcarbonyl)butylcarbamoyl]oxirane-2-carboxylate 50■ Milk $J!
100 mg Crystalline cellulose 50 mg Magnesium stearate 1 mg Hydroxypropyl methylcellulose 15 mg Hydroxypropyl cellulose 4 mg Other compounds used as active ingredients in the present invention can also be made into film-coated tablets using the same formulation.
実施例4 製剤例(顆粒) 顆粒1g中下記成分を含有する。Example 4 Formulation example (granules) 1 g of granules contains the following ingredients.
(2S、3S) −3−((31−3−メチル−1−(
4−(2,3,4−トリメトキシフェニルメチル)ピペ
ラジン−1−イルカル
ボニル)ブチルカルバモイル〕オキシ
ラン−2−カルボン酸エチル’A g酸塩00mg
乳 糖 500
mgトウモロコシデンプン 300rrg本
発明において有効成分として用いられる他の化合物も同
様な処方により顆粒とすることが可能である。(2S,3S) -3-((31-3-methyl-1-(
Ethyl 4-(2,3,4-trimethoxyphenylmethyl)piperazin-1-ylcarbonyl)butylcarbamoyl]oxirane-2-carboxylate 'A g acid salt 00mg Lactose 500
mg Corn starch 300rrg Other compounds used as active ingredients in the present invention can also be made into granules using a similar formulation.
実施例5 製剤例(注射剤) 1アンプル中下記成分を含有する。Example 5 Formulation example (injection) One ampoule contains the following ingredients.
(2R,3R) −3−((S) −3−メチル−1−
(4−(2,3,4−トリメトキシフェニルメチル)ピ
ペラジン−1−イルカル
ボニル)ブチルカルバモイル〕オキシ
ラン−2−カルボン酸エチル2硫酸塩20mg上記成分
に無菌蒸留水を10m1となるように加える。(2R,3R) -3-((S) -3-methyl-1-
(4-(2,3,4-trimethoxyphenylmethyl)piperazin-1-ylcarbonyl)butylcarbamoyl]oxirane-2-carboxylic acid ethyl disulfate 20 mg Add sterile distilled water to the above ingredients to a volume of 10 ml.
本発明において有効成分として用いられる他の化合物も
同様な処方により注射剤とすることが可能である。Other compounds used as active ingredients in the present invention can also be made into injections using the same formulation.
特許出願人 日本ケミファ株式会社 代表者丑山圭三Patent applicant: Nippon Chemifa Co., Ltd. Representative Keizo Ushiyama
Claims (1)
は0〜3の整数を示す)で表わされるピペラジン誘導体
又はその無毒性塩を有効成分として含有する活性酸素産
生抑制ならびに活性酸素除去作用を有する医薬組成物。[Claims] General formula ▲ Numerical formula, chemical formula, table, etc. ▼ (In the formula, R represents a hydrogen atom or a lower alkyl group, and n
is an integer of 0 to 3) or a non-toxic salt thereof as an active ingredient, the pharmaceutical composition has active oxygen production inhibiting and active oxygen removing effects.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP62096965A JP2515119B2 (en) | 1987-04-20 | 1987-04-20 | Pharmaceutical composition containing a piperazine derivative, which has an active oxygen production suppressing effect and an active oxygen removing effect |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP62096965A JP2515119B2 (en) | 1987-04-20 | 1987-04-20 | Pharmaceutical composition containing a piperazine derivative, which has an active oxygen production suppressing effect and an active oxygen removing effect |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| JPS63264525A true JPS63264525A (en) | 1988-11-01 |
| JP2515119B2 JP2515119B2 (en) | 1996-07-10 |
Family
ID=14178950
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP62096965A Expired - Lifetime JP2515119B2 (en) | 1987-04-20 | 1987-04-20 | Pharmaceutical composition containing a piperazine derivative, which has an active oxygen production suppressing effect and an active oxygen removing effect |
Country Status (1)
| Country | Link |
|---|---|
| JP (1) | JP2515119B2 (en) |
Cited By (9)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| JPH0656669A (en) * | 1992-06-11 | 1994-03-01 | Asahi Breweries Ltd | Pterine derivative preparation having active oxygen-scavenging action |
| EP0641563A1 (en) * | 1992-05-20 | 1995-03-08 | Taisho Pharmaceutical Co. Ltd | Remedy for cataract and production thereof |
| FR2767826A1 (en) * | 1997-08-18 | 1999-02-26 | Hoffmann La Roche | CYCLIC AMINE DERIVATIVES, PHARMACEUTICAL COMPOSITIONS CONTAINING SAME, PROCESSES FOR THEIR PREPARATION, AND THEIR USE AS A PHARMACEUTICAL PRINCIPLE AGAINST RESPIRATORY DISEASES |
| WO1999011640A1 (en) * | 1997-09-04 | 1999-03-11 | Nippon Chemiphar Co., Ltd. | Epoxysuccinamide derivatives |
| WO2001014333A1 (en) * | 1999-08-24 | 2001-03-01 | Astrazeneca Uk Limited | Substituted piperidine compounds useful as modulators of chemokine receptor activity |
| US6958350B2 (en) | 2001-02-19 | 2005-10-25 | Astrazeneca Ab | Chemical compounds |
| US6960602B2 (en) | 2001-03-22 | 2005-11-01 | Astrazeneca Ab | Piperidine derivatives as modulators of chemokine receptors |
| US7192973B2 (en) | 2001-11-15 | 2007-03-20 | Astrazeneca Ab | Piperidine derivatives and their use as modulators of chemokine receptor activity (especially CCR5) |
| US7294636B2 (en) | 2003-05-09 | 2007-11-13 | Astrazeneca Ab | Chemical compounds |
-
1987
- 1987-04-20 JP JP62096965A patent/JP2515119B2/en not_active Expired - Lifetime
Cited By (13)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| EP0641563A1 (en) * | 1992-05-20 | 1995-03-08 | Taisho Pharmaceutical Co. Ltd | Remedy for cataract and production thereof |
| EP0641563A4 (en) * | 1992-05-20 | 1995-04-19 | Taisho Pharmaceutical Co Ltd | Remedy for cataract and production thereof. |
| JPH0656669A (en) * | 1992-06-11 | 1994-03-01 | Asahi Breweries Ltd | Pterine derivative preparation having active oxygen-scavenging action |
| ES2154167A1 (en) * | 1997-08-18 | 2001-03-16 | Hoffmann La Roche | CCR-3 receptor antagonists |
| FR2767826A1 (en) * | 1997-08-18 | 1999-02-26 | Hoffmann La Roche | CYCLIC AMINE DERIVATIVES, PHARMACEUTICAL COMPOSITIONS CONTAINING SAME, PROCESSES FOR THEIR PREPARATION, AND THEIR USE AS A PHARMACEUTICAL PRINCIPLE AGAINST RESPIRATORY DISEASES |
| EP0903349A3 (en) * | 1997-08-18 | 2000-05-24 | F. Hoffmann-La Roche Ag | CCR-3 receptor antagonists |
| WO1999011640A1 (en) * | 1997-09-04 | 1999-03-11 | Nippon Chemiphar Co., Ltd. | Epoxysuccinamide derivatives |
| WO2001014333A1 (en) * | 1999-08-24 | 2001-03-01 | Astrazeneca Uk Limited | Substituted piperidine compounds useful as modulators of chemokine receptor activity |
| US6903085B1 (en) | 1999-08-24 | 2005-06-07 | Astrazeneca, Ab | Substituted piperidine compounds useful as modulators of chemokine receptor activity |
| US6958350B2 (en) | 2001-02-19 | 2005-10-25 | Astrazeneca Ab | Chemical compounds |
| US6960602B2 (en) | 2001-03-22 | 2005-11-01 | Astrazeneca Ab | Piperidine derivatives as modulators of chemokine receptors |
| US7192973B2 (en) | 2001-11-15 | 2007-03-20 | Astrazeneca Ab | Piperidine derivatives and their use as modulators of chemokine receptor activity (especially CCR5) |
| US7294636B2 (en) | 2003-05-09 | 2007-11-13 | Astrazeneca Ab | Chemical compounds |
Also Published As
| Publication number | Publication date |
|---|---|
| JP2515119B2 (en) | 1996-07-10 |
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