JP2000026300A - Pharmaceutical composition for protecting vascular endothelial cell - Google Patents

Pharmaceutical composition for protecting vascular endothelial cell

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Publication number
JP2000026300A
JP2000026300A JP10202818A JP20281898A JP2000026300A JP 2000026300 A JP2000026300 A JP 2000026300A JP 10202818 A JP10202818 A JP 10202818A JP 20281898 A JP20281898 A JP 20281898A JP 2000026300 A JP2000026300 A JP 2000026300A
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JP
Japan
Prior art keywords
vascular endothelial
endothelial cell
acid
acceptable salt
pharmacologically acceptable
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
Application number
JP10202818A
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Japanese (ja)
Other versions
JP2000026300A5 (en
Inventor
Kunio Tsuji
邦郎 辻
Kinji Ishida
均司 石田
Makoto Fukushima
信 福島
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Pola Chemical Industries Inc
Original Assignee
Pola Chemical Industries Inc
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Priority to JP10202818A priority Critical patent/JP2000026300A/en
Publication of JP2000026300A publication Critical patent/JP2000026300A/en
Publication of JP2000026300A5 publication Critical patent/JP2000026300A5/ja
Pending legal-status Critical Current

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Abstract

PROBLEM TO BE SOLVED: To search for and obtain a compound having effects equal to those of an antithrombotic agent by protecting actions on a vascular endothelial cell. SOLUTION: This pharmaceutical composition such as a medicine or a food for the prophylaxis and/or therapy of diseases caused by injury to a vascular endothelial cell is obtained by including one or more kinds selected from a bile acid represented by the general formula (R denotes hydrogen or hydroxyl group), its taurine conjugate and a pharmacologically acceptable salt thereof. The bile acid such as ursodeoxycholic acid, cholic acid or taurodeoxycholic acid has protecting actions on the vascular endothelial cell and suppressing actions on the thrombogenesis. Thereby, the utilization of the composition containing the one or more kinds selected from the bile acid, the taurine conjugate and the pharmacologically acceptable salt thereof is considered as an agent for the prophylaxis of thrombi or even the prophylaxis of diseases such as thrombosis, hypoxia, infectious diseases, immune complex diseases diabetes or arteriosclerosis causing the injury to the vascular endothelial cell.

Description

【発明の詳細な説明】DETAILED DESCRIPTION OF THE INVENTION

【0001】[0001]

【発明の属する技術分野】本発明は、血管内皮細胞保護
作用を有する医薬や食品等の組成物に関する。より詳し
くは次に示す一般式で示される胆汁酸、そのタウリン抱
合体またはそれらの薬理学的に許容される塩を有効成分
とする血管内皮細胞保護作用を有する医薬組成物に関す
る。BACKGROUND OF THE INVENTION 1. Field of the Invention The present invention relates to a composition having a protective effect on vascular endothelial cells, such as a medicine or food. More specifically, the present invention relates to a pharmaceutical composition having a vascular endothelial cell protective effect, comprising a bile acid represented by the following general formula, a taurine conjugate thereof or a pharmaceutically acceptable salt thereof as an active ingredient.

【0002】[0002]

【化2】 (式中、Rは水素または水酸基を表す。)Embedded image (In the formula, R represents hydrogen or a hydroxyl group.)

【0003】[0003]

【従来の技術】末梢循環器障害や肺機能障害などによっ
て生じる血液系の低酸素症は、血管内皮への酸素供給の
低下により直接的に誘導される乳酸アシドーシスによる
血管内皮細胞障害を引き起こすが、その際、発生したラ
ジカルや生じた過酸化物の毒性のために更にその障害は
増加し、大きな内皮細胞障害が誘導される。内皮細胞に
障害が起こると、その部位に血小板が粘着・凝集し、更
に障害部分より放出された組織因子や異物(コラーゲ
ン)との接触により血液凝固系が活性化され、トロンピ
ンが生成される。トロンビンは血小板の活性化を促すほ
か、フィブリノーゲンをフィブリンへと転換し、血栓を
形成する。この過程が繰り返されることで、最終的に、
病的な血行障害に至ることが知られている。また、糖尿
病、高脂血症、高血圧、エンドトキシンなど様々な要因
によっても血行障害が起きる。2. Description of the Related Art Blood system hypoxia caused by peripheral circulatory disorders and pulmonary dysfunction causes vascular endothelial cell damage due to lactic acidosis, which is directly induced by a decrease in oxygen supply to the vascular endothelium. At that time, the damage is further increased due to the toxicity of the generated radical and the generated peroxide, and a large endothelial cell damage is induced. When an endothelial cell is damaged, platelets adhere and aggregate at the site, and the blood coagulation system is activated by contact with tissue factor or a foreign substance (collagen) released from the damaged portion, thereby producing thrombin. Thrombin stimulates platelet activation and also converts fibrinogen to fibrin, forming a thrombus. By repeating this process, eventually
It is known to lead to morbid blood circulation disorders. In addition, various factors such as diabetes, hyperlipidemia, hypertension, and endotoxin cause blood circulation disorders.

【0004】近年、動脈硬化の形成に、内皮細胞の傷害
あるいは活性化が関与することが注目されている。動脈
硬化は静かに進行し、突然、心筋梗塞や脳卒中という形
で表出する。その多くの原因は動脈血栓症であることか
ら、抗血栓剤が使われている。しかしながら、この様な
抗血栓剤には安全性上に問題があるばかりではなく、内
皮細胞に対する作用は知られておらず、従って根本的な
問題解決となっていない。[0004] In recent years, it has been noted that the formation or formation of arteriosclerosis involves injury or activation of endothelial cells. Atherosclerosis progresses quietly and suddenly manifests itself as a myocardial infarction or stroke. Antithrombotic agents are used because many of the causes are arterial thrombosis. However, such an antithrombotic agent not only has a problem in safety, but also has no known effect on endothelial cells, and thus has not solved a fundamental problem.

【0005】[0005]

【発明が解決しようとする課題】本発明の目的は、血管
内皮細胞の保護作用により、抗血栓剤と同等の効果を有
する化合物を探索し、提供することにある。SUMMARY OF THE INVENTION An object of the present invention is to search for and provide a compound having the same effect as an antithrombotic agent by protecting vascular endothelial cells.

【0006】[0006]

【課題を解決するための手段】本発明者は胆汁酸アルコ
ールおよび胆汁酸の薬理作用を研究していたところ、胆
汁酸が動物の血栓症モデルで効果を示すことを見いだ
し、本発明を完成させた。The present inventors have studied the pharmacological effects of bile acid alcohols and bile acids, and found that bile acids are effective in animal thrombosis models, and completed the present invention. Was.

【0007】なお、本発明に使用される胆汁酸のうちウ
ルソデオキシコール酸は、胆道系疾患および胆汁うっ滞
を伴う肝疾患における利胆、慢性肝疾患における肝機能
改善剤として、ケノデオキシコール酸はコレステロール
胆石溶解剤として使用されているが、それらの抗血栓や
血小板凝集抑制効果については知られていない。[0007] Among the bile acids used in the present invention, ursodeoxycholic acid is an agent for improving the bile function in biliary tract diseases and liver diseases accompanied by bile stasis and as a liver function improving agent in chronic liver diseases. Chenodeoxycholic acid is cholesterol. Although used as gallstone dissolving agents, their antithrombotic and platelet aggregation inhibitory effects are not known.

【0008】[0008]

【発明の実施の形態】本発明の胆汁酸およびそのタウリ
ン抱合体の薬理学的に許容される塩としては、例えぱナ
トリウム、カリウム、マグネシウム、カルシウム等の無
機塩が挙げられる。BEST MODE FOR CARRYING OUT THE INVENTION The pharmacologically acceptable salts of the bile acids and taurine conjugates thereof of the present invention include, for example, inorganic salts such as sodium, potassium, magnesium and calcium.

【0009】これらの胆汁酸およびそのタウリン抱合体
の薬理学的に許容される塩は通常の製剤担体を配合する
ことにより、錠剤、カプセル剤、散剤、細粒剤もしくは
顆粒剤等の固形製剤または注射剤、吸入剤、シロツプ
剤、懸濁剤もしくは乳剤等の液剤に調製することができ
る。The pharmacologically acceptable salts of these bile acids and their taurine conjugates can be mixed with solid pharmaceutical preparations such as tablets, capsules, powders, fine granules or granules by adding ordinary pharmaceutical carriers. Liquid preparations such as injections, inhalants, syrups, suspensions and emulsions can be prepared.

【0010】製剤担体としては、種々の賦形剤、結合
剤、滑沢剤、崩壊剤、被覆剤、溶解補助剤、乳化剤、懸
濁剤、安定化剤または溶剤等が拳げられる。As the pharmaceutical carrier, various excipients, binders, lubricants, disintegrants, coating agents, solubilizers, emulsifiers, suspending agents, stabilizers, solvents and the like can be used.

【0011】胆汁酸の種類、年齢症状等によリ、用法や
用量は異なるが、胆汁酸がウルソデオキシコール酸の場
合は、一般に成人に対し、1日あたり経口で10〜30
00mg、好ましくは50〜1500mg、静脈注射で
5〜100mg、好ましくは10〜60mgとし、これ
を1〜6回、好ましくは1〜3回に分けて用いるのが好
ましい。Although the usage and dosage vary depending on the type of bile acid, age symptoms, etc., when bile acid is ursodeoxycholic acid, it is generally 10 to 30 orally per day for adults.
The dose is 00 mg, preferably 50 to 1500 mg, and 5 to 100 mg, preferably 10 to 60 mg by intravenous injection, and it is preferable to use them in 1 to 6 times, preferably 1 to 3 times.

【0012】ケノデオキシコール酸の場合には、一般に
成人に対し、1日あたり経口で10〜3000mg、好
ましくは30〜1000mgとし、2〜3回に分けて用
いるのが好ましい。In the case of chenodeoxycholic acid, it is generally used orally in an adult at a dose of 10 to 3000 mg, preferably 30 to 1000 mg per day, and it is preferable to use it in two or three divided doses.

【0013】[0013]

【実施例】以下に、本発明の内容を実施例により詳細に
説明する。しかしながら、本発明がこれら実施例にのみ
限定されないことは言うまでもない。DESCRIPTION OF THE PREFERRED EMBODIMENTS The contents of the present invention will be described below in detail with reference to embodiments. However, it goes without saying that the present invention is not limited only to these examples.

【0014】1)乳酸誘導末梢動脈閉塞症モデル 岩本らの方法(薬理と治療14,41−49(1986))に準じて
モデル動物を作成した。即ち、予備飼育したラットを麻
酔下、仰位に固定し、右(あるいは左)の大腿部をバリ
カンで除毛後布製粘着テープで固定した。大腿部内側を
最小限に切開し、周囲組織より大腿動脈を約5mm剥離
した。次に、大腿動脈の血流を脳外科用のクリップで遮
断し、注射針を付けた1mlのシリンジを用いて、5%
乳酸一生理食塩水(pH 1.67)0.15mlを毎
秒0.05mlで大腿動脈内に注入した。その後、注入
部位よりの出血をアロンアルファによって止め、大腿動
脈の切開部位を縫合クリップで閉じた。疑似手術群には
5%乳酸一生理食塩水の代わりに生理食塩水を注入し
た。1) Lactate-induced peripheral arterial occlusion model A model animal was prepared according to the method of Iwamoto et al. (Pharmacology and Therapy 14, 41-49 (1986)). That is, the rats reared in advance were fixed in a supine position under anesthesia, the right (or left) thigh was removed with a clipper, and then fixed with a cloth adhesive tape. The inside of the thigh was incised to a minimum and the femoral artery was dissected about 5 mm from the surrounding tissue. Next, the blood flow in the femoral artery was cut off with a clip for neurosurgery, and 5% was injected using a 1 ml syringe with an injection needle.
0.15 ml of lactate-monosaline (pH 1.67) was injected into the femoral artery at 0.05 ml per second. Thereafter, bleeding from the injection site was stopped by Aron Alpha, and the incision site of the femoral artery was closed with a suture clip. The sham surgery group was injected with saline instead of 5% lactate-saline.

【0015】被検薬は生理食塩水に懸濁あるいは溶解さ
せた後、乳酸注入の2時間前に、経口投与した。The test drug was orally administered 2 hours before lactic acid injection after being suspended or dissolved in physiological saline.

【0016】評価は、足蹠の浮腫および壊疸の度合い、
血小板停滞率及び乳酸脱水素酵素(LDH)活性を指標
として行った。The evaluation was based on the degree of foot pad edema and gangrene,
Platelet retention and lactate dehydrogenase (LDH) activity were used as indices.

【0017】a)浮腫の程度はハリディー(Halliday
W.J)らの方法(J.Nat.Cancer Inst.,43,141−142(196
9))に準じて、乳酸注入の前と後に、乳酸を注入した
足蹠の厚さをノギスを用いて測定し求めた。A) The degree of edema is determined by Halliday
WJ) et al. (J. Nat. Cancer Inst., 43, 141-142 (196)
According to 9)), before and after the injection of lactic acid, the thickness of the footpad into which lactic acid was injected was measured using a caliper and determined.

【0018】b)各指の壊疽の度合いを、0から5まで
の数値(変化なし:0、黒変が爪先部に限られる:1、
黒変が指部に及ぶ:2、指の壊死(ミイラ化):3、指
の脱落:4、壊死が足蹠部まで及ぶ:5)で表し、5本
の指の数値の総和を求めて病変指数とした。B) The degree of gangrene of each finger is represented by a numerical value from 0 to 5 (no change: 0, black discoloration is limited to the toe portion: 1,
Black discoloration extends to the finger part: 2, finger necrosis (mummification): 3, finger fallout: 4, necrosis extends to the footpad part: 5), and sum the numerical values of five fingers The lesion index was used.

【0019】c)血小板粘着能(停滞率)の測定 ヘレム(Hellem)の方法(Scand.J.Haemat.,7,374-382
(1970))をもとにして測定した。C) Measurement of platelet adhesion (retention rate) Method of Helem (Scand. J. Haemat., 7, 374-382)
(1970)).

【0020】d)血清中LDH活性の測定;臨床検査キッ
トを使用した。D) Measurement of serum LDH activity; a clinical test kit was used.

【0021】<結果>表1に乳酸誘導末梢動脈閉塞症モ
デルラットにおける病態進行に及ぽす各種胆汁酸の効果
(単回投与)の結果を示す。<Results> Table 1 shows the results of the effects (single administration) of various bile acids on the progression of the disease state in a rat model of lactic acid-induced peripheral arterial occlusion.

【0022】[0022]

【表1】 UDCA;ウルソデオキシコール酸 (20.5μmole/Kg, p.o.) TUDCA;タウロウルソデオキシコール酸ナトリウム塩
(20.5μmole/Kg, p.o.) *, ** and *** show significant differences (p<0.0
5, 0.01 and 0.001) from the control, respectively.[Table 1] UDCA; ursodeoxycholic acid (20.5μmole / Kg, po) TUDCA; tauroursodeoxycholic acid sodium salt
(20.5μmole / Kg, po) *, ** and *** show significant differences (p <0.0
5, 0.01 and 0.001) from the control, respectively.

【0023】表2に乳酸誘導末梢動脈閉塞症モデルラッ
トにおける浮腫の進展及び血清乳酸脱炭酸酵素活性に及
ぽす胆汁酸の効果を示す。Table 2 shows the effects of bile acids on edema development and serum lactate decarboxylase activity in a rat model of lactic acid-induced peripheral arterial occlusion.

【0024】[0024]

【表2】 UDCA;ウルソデオキシコール酸 (20.5μmole/Kg, p.
o.) TUDCA;タウロウルソデオキシコール酸ナトリウム塩
(20.5μmole/Kg, p.o.) *, ** and *** show significant differences (p<0.0
5, 0.01 and 0.001) from the control, respectively.[Table 2] UDCA; ursodeoxycholic acid (20.5 μmole / Kg, p.
o.) TUDCA; Tauroursodeoxycholic acid sodium salt
(20.5μmole / Kg, po) *, ** and *** show significant differences (p <0.0
5, 0.01 and 0.001) from the control, respectively.

【0025】いずれの胆汁酸においても、病変指数の上
昇、足蹠の浮腫の進展及ぴ血清LDH活性の上昇を抑制
する効果を示した。All bile acids exhibited an effect of suppressing an increase in lesion index, development of foot pad edema and an increase in serum LDH activity.

【0026】表3に血清乳酸脱炭酸酵素活性に及ぽすU
DCAおよびアルガトロパンの効果を示す。Table 3 shows the effect of U on serum lactate decarboxylase activity.
4 shows the effects of DCA and argatropane.

【0027】[0027]

【表3】 UDCA;ウルソデオキシコール酸 *, ** and *** show significant differences (p<0.0
5, 0.01 and 0.001) from the control, respectively.[Table 3] UDCA; ursodeoxycholic acid *, ** and *** show significant differences (p <0.0
5, 0.01 and 0.001) from the control, respectively.

【0028】上昇するLDH活性に関し、LDHのアイ
ソザイムパターンを検討したところ、薬剤投与群と対照
群との活性値間に明らかな差の認められたのは、LDH
4とLDH5でその比は約1:4.5で、血管内皮細胞中
のLDHアイソザイム分析で得られたLDH4とLDH5
の比1:3.3と良く一致していた。When the isozyme pattern of LDH was examined with respect to the increased LDH activity, a clear difference was observed between the activity values of the drug-administered group and the control group.
The ratio between LDH 4 and LDH 5 was about 1: 4.5, and LDH 4 and LDH 5 obtained by analysis of LDH isozyme in vascular endothelial cells.
Ratio of 1: 3.3.

【0029】2)ストレプトゾトシン誘発糖尿病に対す
る影響 ウイスター系雄性ラット(10週齢)にストレプトゾト
シンを35mg/kgまたは45mg/kgの割合で尾
静脈内投与することにより糖尿病ラツトを作成した。コ
ントロール群には生理食塩水を投与した。評価は血糖
値、血小板停滞率、血清LDH活性を測定して行った。2) Influence on Streptozotocin-Induced Diabetes Diabetic rats were prepared by administering 35 mg / kg or 45 mg / kg of streptozotocin to male Wistar rats (10 weeks old) in the tail vein. A saline was administered to the control group. The evaluation was performed by measuring the blood glucose level, platelet retention rate, and serum LDH activity.

【0030】<結果>表4にストレプトゾトシン誘発糖
尿病ラットの血糖値に及ぽすウルソデオキシコール酸の
影響を示す。<Results> Table 4 shows the effect of ursodeoxycholic acid on the blood glucose level of streptozotocin-induced diabetic rats.

【0031】[0031]

【表4】 UDCA;ウルソデオキシコール酸 *, ** and *** show significant differences (p<0.0
5, 0.01 and 0.001) from the control, respectively.[Table 4] UDCA; ursodeoxycholic acid *, ** and *** show significant differences (p <0.0
5, 0.01 and 0.001) from the control, respectively.

【0032】表5にストレプトゾトシン誘発糖尿病ラッ
トの血小板停滞率および血清LDH活性に及ぼすウルソデ
オキシコール酸の影響を示す。Table 5 shows the effect of ursodeoxycholic acid on the platelet retention rate and serum LDH activity of streptozotocin-induced diabetic rats.

【0033】[0033]

【表5】 UDCA;ウルソデオキシコール酸 * shows significant differences (p<0.05) from the
control.[Table 5] UDCA; ursodeoxycholic acid * shows significant differences (p <0.05) from the
control.

【0034】被検薬を2週間連続経口投与することによ
り、血糖値に及ぼす影響を検討したところ、UDCAは
有意に血糖値、血小板停滞率を低下させた。また、血清
LDH活性の上昇を抑制する傾向を示した。When the effect on the blood glucose level was examined by orally administering the test drug for two weeks, UDCA significantly reduced the blood glucose level and the platelet retention rate. In addition, it showed a tendency to suppress an increase in serum LDH activity.

【0035】3)食事性高脂血症に対する影響 ウイスター系雄性ラットに1%コレステロール食自由摂
取させて高脂血症ラットを作成した。コントロール群に
は生理食塩水を投与した。評価は血糖値、全血凝固時
間、血清LDH活性を測定して行った。3) Effect on Dietary Hyperlipidemia Male Wistar rats were allowed to freely ingest 1% cholesterol diet to prepare hyperlipidemic rats. A saline was administered to the control group. The evaluation was performed by measuring the blood sugar level, the whole blood coagulation time, and the serum LDH activity.

【0036】<結果>被検薬を4週間連続経口投与する
ことにより、血清脂質に及ぼす影響を検討したところ、
ウルソデオキシコール酸ナトリウムは有意に上昇した血
清脂質値と血小板停滞率を低下させた。また、ウルソデ
オキシコール酸ナトリウムは血清LDH活性の上昇を有
意に抑制した。<Results> The effect on serum lipids by orally administering the test drug for 4 weeks was examined.
Sodium ursodeoxycholate significantly reduced serum lipid levels and platelet retention. In addition, sodium ursodeoxycholate significantly suppressed the increase in serum LDH activity.

【0037】[0037]

【発明の効果】以上のように、ウルソデオキシコール
酸、コール酸、タウロデオキシコール酸等の胆汁酸は、
血管内皮細胞を保護し血栓形成を抑制する作用を示し
た。従って、血栓予防の薬剤、あるいは、血管内皮細胞
の傷害を生じる血栓症や低酸素症、感染症、免疫複合体
症、糖尿病、動脈硬化症等の疾患の予防にも利用が考え
られる。As described above, bile acids such as ursodeoxycholic acid, cholic acid and taurodeoxycholic acid are
It has the effect of protecting vascular endothelial cells and suppressing thrombus formation. Therefore, it can be used as an agent for preventing thrombosis, or for preventing diseases such as thrombosis, hypoxia, infection, immune complex disease, diabetes, and arteriosclerosis that cause damage to vascular endothelial cells.

───────────────────────────────────────────────────── フロントページの続き (72)発明者 福島 信 神奈川県横浜市戸塚区柏尾町560 ポーラ 化成工業株式会社戸塚研究所内 Fターム(参考) 4B018 LB10 MS03 4C086 AA01 AA02 DA11 MA01 MA02 MA04 NA14 ZA36 ZA45 ZA54 ZC02 ZC35 4C091 AA02 BB01 CC01 DD01 EE04 FF01 GG02 GG13 HH01 JJ03 KK01 LL02 MM03 NN01 PA02 PA05 PB03 QQ01  ────────────────────────────────────────────────── ─── Continuing on the front page (72) Inventor Shin Fukushima 560 Kashio-cho, Totsuka-ku, Yokohama-shi, Kanagawa Prefecture F-term in the Totsuka Research Laboratories, Totsuka Laboratory Co., Ltd. 4B018 LB10 MS03 4C086 AA01 AA02 DA11 MA01 MA02 MA04 NA14 ZA36 ZA45 ZA54 ZC02 ZC35 4C091 AA02 BB01 CC01 DD01 EE04 FF01 GG02 GG13 HH01 JJ03 KK01 LL02 MM03 NN01 PA02 PA05 PB03 QQ01

Claims (5)

【特許請求の範囲】[Claims] 【請求項1】 次に示す一般式で示される胆汁酸、その
タウリン抱合体および薬理学的に許容されるそれらの塩
から選ばれる1種乃至は2種以上を含有する血管内皮細
胞の傷害に起因する疾患の予防及び/又は治療用の組成
物。 【化1】 (式中、Rは水素または水酸基を表す。)1. The method according to claim 1, wherein the vascular endothelial cell contains one or more bile acids represented by the following general formula, a taurine conjugate thereof and a pharmacologically acceptable salt thereof. A composition for preventing and / or treating a resulting disease. Embedded image (In the formula, R represents hydrogen or a hydroxyl group.) 【請求項2】 上記一般式に表される胆汁酸、そのタウ
リン抱合体および薬理学的に許容されるそれらの塩から
選ばれる1種乃至は2種以上がウルソデオキシコール酸
及び/またはその薬理学的に許容される塩である、請求
項1に記載の組成物。2. One or two or more kinds selected from bile acids represented by the above general formula, taurine conjugates thereof and pharmacologically acceptable salts thereof, are ursodeoxycholic acids and / or drugs thereof. The composition according to claim 1, which is a physically acceptable salt. 【請求項3】 血管内皮細胞の傷害に起因する疾患が血
栓症である請求項1又は2に記載の組成物。3. The composition according to claim 1, wherein the disease caused by damage to vascular endothelial cells is thrombosis. 【請求項4】 血管内皮細胞の傷害が低酸素症、感染
症、免疫複合体症、糖尿病、動脈硬化症、血管炎、ショ
ック及び汎発性血管内凝固症候群から選ばれる1種乃至
は2種以上であることを特徴とする、請求項1〜3の何
れか一項に記載の組成物。4. The vascular endothelial cell injury is one or two selected from hypoxia, infectious disease, immune complex disease, diabetes, arteriosclerosis, vasculitis, shock and generalized intravascular coagulation syndrome. The composition according to claim 1, wherein: 【請求項5】 医薬又は食品であることを特徴とする、
請求項1〜3の何れか一項に記載の組成物。5. A medicine or a food,
The composition according to claim 1.
JP10202818A 1998-07-02 1998-07-02 Pharmaceutical composition for protecting vascular endothelial cell Pending JP2000026300A (en)

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