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JPH09255570A - Medicine and edible composition for lowering concentration of lipid in blood - Google Patents

Medicine and edible composition for lowering concentration of lipid in blood

Info

Publication number
JPH09255570A
JPH09255570A JP8064368A JP6436896A JPH09255570A JP H09255570 A JPH09255570 A JP H09255570A JP 8064368 A JP8064368 A JP 8064368A JP 6436896 A JP6436896 A JP 6436896A JP H09255570 A JPH09255570 A JP H09255570A
Authority
JP
Japan
Prior art keywords
soybean
glucoside
formula
lipid
isoflavone
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
JP8064368A
Other languages
Japanese (ja)
Inventor
Takehiko Uesugi
岳彦 植杉
Kunimasa Hirai
邦昌 平井
Toshiya Toda
登志也 戸田
Takenori Okudaira
武則 奥平
Kinji Ishida
均司 石田
Kunio Tsuji
邦郎 辻
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Fujicco Co Ltd
Original Assignee
Fujicco Co Ltd
Priority date (The priority date 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 date listed.)
Filing date
Publication date
Application filed by Fujicco Co Ltd filed Critical Fujicco Co Ltd
Priority to JP8064368A priority Critical patent/JPH09255570A/en
Publication of JPH09255570A publication Critical patent/JPH09255570A/en
Pending legal-status Critical Current

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  • Jellies, Jams, And Syrups (AREA)
  • Non-Alcoholic Beverages (AREA)
  • Saccharide Compounds (AREA)
  • Pyrane Compounds (AREA)
  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
  • Coloring Foods And Improving Nutritive Qualities (AREA)

Abstract

PROBLEM TO BE SOLVED: To obtain a highly safe medicine capable of improving the metabolism of lipid in vivo to lower the concentration of the lipid in blood and useful for treating and preventing hyperlipemia, arteriosclerosis, etc. SOLUTION: This medicine contains an isoflavone derivative of the formula [R<1> is H, OH; R<2> is OH, O-glucoside, O-(6"-O-succinyl)glucoside, O-(6"-O-malonyl) glucoside, O-(6"-O-acetyl)glucoside] in an amount of >=0.5wt.%, prefrably 2-25wt.%, as an active iugredient. This edible composition contains the compound of the formula in an amount of >=0.001wt.%, preferably 0.01-10wt.%. The compound of the formula is e.g. 7-O-glucopyranosy1-4'-hydroxy-isoflavone. The compound of the formula is administered at a daily dose of 0.1-4mg/kg, and is useful for preventing and treating ischemic cardiac diseases, cerebrovascular disorders, mammary cancer, colon cancer, etc.

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、高脂血症、動脈硬
化等の治療や予防に有用な薬剤及び可食性組成物に関す
る。さらに詳細には、イソフラボン誘導体を有効成分と
して含有することを特徴とし、高い安全性をもって、生
体内における脂質代謝を改善し、血中の脂質濃度を低減
せしめうる薬剤及び可食性組成物に関する。TECHNICAL FIELD The present invention relates to a drug and an edible composition useful for treating and preventing hyperlipidemia, arteriosclerosis and the like. More specifically, the present invention relates to a drug and an edible composition which are characterized by containing an isoflavone derivative as an active ingredient and which can improve lipid metabolism in vivo and reduce the lipid concentration in blood with high safety.

【0002】[0002]

【従来の技術及び発明が解決しようとする課題】近年、
ライフスタイルの変化や高齢化に伴い、運動不足、栄養
過多、ホルモンバランスの崩れ(閉経時等)などに起因
すると考えられる高脂血症が、大きな問題となってい
る。2. Description of the Related Art In recent years,
BACKGROUND ART Hyperlipidemia, which is considered to be caused by lack of exercise, overnutrition, hormonal imbalance (menopause, etc.), has become a major problem with changes in lifestyle and aging.

【0003】現在、高コレステロール血症を含む高脂血
症と、粥状動脈硬化との因果関係は半ば常識として知ら
れるところであり、かかる粥状動脈硬化は、現代の主要
な成人病である虚血性心疾患や脳血管障害の基礎をなす
という意味において、重大な意義を有している(荒井秀
典、「総コレステロールと動脈硬化」、臨床成人病、25
巻、10号、1200〜1204頁(1995))。At present, the causal relationship between hyperlipidemia including hypercholesterolemia and atherosclerosis is known as a common sense, and such atherosclerosis is a major adult disease of the present day. It has a significant significance in that it forms the basis of bloody heart disease and cerebrovascular accident (Hidenori Arai, "Total cholesterol and arteriosclerosis", Clinical adult disease, 25
Vol. 10, p. 1200-1204 (1995)).

【0004】また、最近の研究により、乳癌や大腸癌等
の発症とコレステロールとの因果関係も指摘され、種々
の実験に基づく立証がなされてきている。Further, recent studies have pointed out a causal relationship between the onset of breast cancer, colon cancer, etc. and cholesterol, and have been proved based on various experiments.

【0005】ところで、高脂血症に対する治療法または
予防法としては、運動療法、食事療法及び薬物療法が提
案されている。このうち現在採用されている高脂血症の
治療の基本は食事療法であるが、家庭で行う場合には栄
養学的に正しい知識が必要であり、ときに低栄養、特に
蛋白質、ビタミンまたはミネラル分等の不足を招きやす
く、患者にとって最も適切な態様にて実施することは困
難であるという実状にある。また、運動療法によれば、
血中の中性脂肪を有効に低下させることは可能であるも
のの、血中コレステロール値にはほとんど影響がないと
の報告がなされている(佐々木淳、「運動による血清脂
質コントロール、動脈硬化の予防」、臨床成人病、25巻
10号、1260〜1263頁(1995))。薬物療法に関しては、各
種の薬物が開発され、治療に供されているが、その有効
成分によっては、副作用を有したり、急激に強い効果を
発揮するものもあり、医師のもとで、充分なモニタリン
グを行いながら投与する必要がある。By the way, as therapeutic or preventive methods for hyperlipidemia, exercise therapy, diet therapy and drug therapy have been proposed. The basic treatment of hyperlipidemia that is currently adopted is diet therapy, but when it is performed at home, nutritionally correct knowledge is required, and sometimes undernutrition, especially protein, vitamins or minerals. In practice, it is difficult to carry out the administration in the most suitable manner for the patient, because it is likely to cause a shortage of time. Also, according to exercise therapy,
Although it is possible to effectively reduce blood triglyceride, it has been reported that it has almost no effect on blood cholesterol levels (Atsushi Sasaki, "Serum lipid control by exercise, prevention of arteriosclerosis") ], Clinical Adult Diseases, Volume 25
10, pp. 1260 to 1263 (1995)). Regarding drug therapy, various drugs have been developed and are being used for treatment. However, some active ingredients may have side effects or exert a strong effect rapidly, so it may It is necessary to administer the drug while performing detailed monitoring.

【0006】従って、副作用を伴わず、穏やかに血中の
脂質を低下せしめる作用を有する薬剤及び、食事などで
摂取することにより効果が発揮される可食性組成物は、
動脈硬化等の成人病予防の観点から極めて重要であり、
これらの開発が希求されているところである。[0006] Therefore, a drug having an action of gently lowering lipids in the blood without causing side effects and an edible composition exhibiting an effect by ingestion in meals are
It is extremely important from the perspective of preventing adult diseases such as arteriosclerosis,
These developments are being sought after.

【0007】かかる薬剤や組成物を提供すべく、EPA
及びDHA等のn-3系多価不飽和脂肪酸の研究が行われ
てきた。しかし、これら不飽和脂肪酸は、中性脂肪を効
果的に低下せしめることが示されたものの、総コレステ
ロール値の低下については、4年という長期間の投与を
必要とし、4年以下の短期間投与の場合には、むしろ総
コレステロール値を有意に上昇させうることが報告され
ている(浜崎智仁、「DHA・EPAの機能と治療効
果」、臨床成人病、25巻、10号、1265〜1269頁(199
5))。[0007] To provide such drugs and compositions, EPA
And n-3 polyunsaturated fatty acids such as DHA have been studied. However, although these unsaturated fatty acids have been shown to effectively reduce triglyceride, long-term administration of 4 years is required to reduce total cholesterol levels, and short-term administration of 4 years or less is required. In the case of, it has been reported that the total cholesterol level can be significantly increased (Tomohito Hamasaki, "Functions and therapeutic effects of DHA / EPA", Clinical Adult Disease, 25, No. 10, pp. 1265-1269. (199
Five)).

【0008】[0008]

【課題を解決するための手段】本発明は、上述した当該
技術分野における課題に鑑みて、本発明者らが様々な食
品成分について幅広く鋭意研究を重ねた結果、大豆など
に多く含まれるイソフラボン誘導体のうち一般式(I)
で示される化合物が、血清コレステロール値を有意に低
下させる作用を有しており、且つ、生体に対する安全性
も高いことを知見するに至って発明されたものであり、
以下の薬剤及び可食性組成物を提供する。In view of the above-mentioned problems in the technical field of the present invention, the present inventors have conducted extensive and extensive research on various food ingredients, and as a result, the isoflavone derivative contained in soybean and the like in a large amount. Of the general formula (I)
The compound represented by has the effect of significantly lowering the serum cholesterol level, and was invented to discover that it is also highly safe for living organisms,
The following agents and edible compositions are provided.

【0009】すなわち本発明は、以下の(1)から
(4)に記載する特徴を有するものである。That is, the present invention has the features described in (1) to (4) below.

【0010】(1)一般式(I)(1) General formula (I)

【0011】[0011]

【化3】 Embedded image

【0012】[式中、R1は、HまたはOHを表し、R2
は、OH、O-グルコシド基、O-(6"-O-サクシニル)グル
コシド基、O-(6"-O-マロニル)グルコシド基または、O-
(6"-O-アセチル)グルコシド基を表す]で示されるイソ
フラボン誘導体を有効成分として含有することを特徴と
する、血中脂質濃度を低減させる薬剤。[In the formula, R 1 represents H or OH, and R 2
Is OH, O-glucoside group, O- (6 "-O-succinyl) glucoside group, O- (6" -O-malonyl) glucoside group or O-
(Representing a 6 "-O-acetyl) glucoside group] is contained in the isoflavone derivative as an active ingredient, and a drug for reducing blood lipid concentration.

【0013】(2)前記イソフラボン誘導体が、ダイゼ
イン、ダイズイン、6"-O-サクシニルダイズイン、6"-O-
マロニルダイズインまたは6"-O-アセチルダイズインで
ある、前記(1)の薬剤。(2) The isoflavone derivative is daidzein, soybean in, 6 "-O-succinyl soybean in, 6" -O-
The agent according to (1) above, which is malonyl soybean in or 6 "-O-acetyl soybean.

【0014】(3)一般式(I)(3) General formula (I)

【0015】[0015]

【化4】 Embedded image

【0016】[式中、R1は、HまたはOHを表し、R2
は、OH、O-グルコシド基、O-(6"-O-サクシニル)グル
コシド基、O-(6"-O-マロニル)グルコシド基または、O-
(6"-O-アセチル)グルコシド基を表す]で示されるイソ
フラボン誘導体を有効成分として含有することを特徴と
する、血中脂質濃度を低減させるために用いられる可食
性組成物。[In the formula, R 1 represents H or OH, and R 2
Is OH, O-glucoside group, O- (6 "-O-succinyl) glucoside group, O- (6" -O-malonyl) glucoside group or O-
(Representing (6 "-O-acetyl) glucoside group] is contained as an active ingredient, the edible composition used for reducing the blood lipid concentration.

【0017】(4)前記イソフラボン誘導体が、ダイゼ
イン、ダイズイン、6"-O-サクシニルダイズイン、6"-O-
マロニルダイズインまたは6"-O-アセチルダイズインで
ある、前記(3)の可食性組成物。(4) The isoflavone derivative is daidzein, soybean in, 6 "-O-succinyl soybean in, 6" -O-
The edible composition according to (3) above, which is malonyl soybean in or 6 "-O-acetyl soybean in.

【0018】[0018]

【発明の実施の形態】本発明の血中脂質を低減させる薬
剤及び可食性組成物に有効成分として含有されるイソフ
ラボン誘導体は、一般式(I)BEST MODE FOR CARRYING OUT THE INVENTION The isoflavone derivative contained as an active ingredient in the drug and edible composition for reducing blood lipid of the present invention has the general formula (I).

【0019】[0019]

【化5】 Embedded image

【0020】[式中、R1は、HまたはOHを表し、R2
は、OH、O-グルコシド基、O-(6"-O-サクシニル)グル
コシド基、O-(6"-O-マロニル)グルコシド基または、O-
(6"-O-アセチル)グルコシド基を表す]で示される化合
物である。[In the formula, R 1 represents H or OH, and R 2
Is OH, O-glucoside group, O- (6 "-O-succinyl) glucoside group, O- (6" -O-malonyl) glucoside group or O-
Represents a (6 "-O-acetyl) glucoside group].

【0021】上記一般式(I)で示されるイソフラボン
誘導体のうち、ダイゼイン、ダイズイン、6"-O-サクシ
ニルダイズイン、6"-O-マロニルダイズインまたは6"-O-
アセチルダイズインが、有効成分として特に好ましい。Among the isoflavone derivatives represented by the above general formula (I), daidzein, soybean in, 6 "-O-succinyl soybean, 6" -O-malonyl soybean or 6 "-O-
Acetyl soybean in is particularly preferred as the active ingredient.

【0022】上記イソフラボン誘導体は、例えば大豆種
子もしくはその一部、または大豆発酵物、特に好ましく
は大豆胚軸または納豆などから抽出及び精製を行うこと
により得ることができる。具体的には、原料大豆胚軸ま
たは納豆のアルコール抽出物を、吸着カラムクロマトグ
ラフィー、ゲルカラムクロマトグラフィー、さらに逆相
系のカラムクロマトグラフィーに適用することで精製し
て、得られる。The above isoflavone derivative can be obtained, for example, by extracting and purifying soybean seed or a part thereof, or a soybean fermented product, particularly preferably soybean hypocotyl or natto. Specifically, it is obtained by applying a raw material soybean hypocotyl or an alcoholic extract of natto to an adsorption column chromatography, a gel column chromatography, and a reversed phase column chromatography for purification.

【0023】また、イソフラボン誘導体のうちダイズイ
ン及びダイゼインは、フジッコ株式会社製のものを入手
することも可能である。Of the isoflavone derivatives, soybean in and daidzein can be obtained from Fujicco Co., Ltd.

【0024】本発明の薬剤及び可食性組成物は、血中脂
質濃度、特に血清コレステロール値を低減させることが
できるので、高脂血症、動脈硬化症、ひいては、虚血性
心疾患、脳血管障害等、及び、例えば乳癌や大腸癌等の
一部の癌などの予防や治療において有用である。Since the drug and the edible composition of the present invention can reduce the blood lipid level, especially the serum cholesterol level, hyperlipidemia, arteriosclerosis, and eventually ischemic heart disease, cerebrovascular disorder. Etc. and, for example, in the prevention and treatment of some cancers such as breast cancer and colon cancer.

【0025】一般式(I)で示されるイソフラボン誘導
体は、後記した急性毒性試験の結果に示すように、いず
れも経口及び皮下に、5,000〜10,000mg/kgの技術的限
界量をマウスまたはラットに対して投与した場合に、こ
れらの化合物に起因すると考えられる死亡例及び中毒症
状は一切認められなかった。従ってこれらの化合物は低
毒性であり、極めて安全性が高く、所望の作用効果を得
るために用いられる物質として好適である。As shown in the results of the acute toxicity test described below, the isoflavone derivative represented by the general formula (I) is orally or subcutaneously administered to mice or rats at a technical limit of 5,000 to 10,000 mg / kg. When administered in parallel, no deaths or poisoning symptoms attributable to these compounds were observed. Therefore, these compounds have low toxicity, are extremely safe, and are suitable as substances used to obtain desired effects.

【0026】一般式(I)で示されるイソフラボン誘導
体の投与または摂取量は、投与または摂取対象者の状態
や年齢、投与経路等により異なるが、通常、 0.1〜4 m
g/kg体重/日、好ましくは0.2〜1 mg/kg体重/日が用
いられる。投与または摂取は、一日一回、または必要に
応じて複数回に分けて、所定量を用いればよい。The administration or intake amount of the isoflavone derivative represented by the general formula (I) varies depending on the condition or age of the subject of administration or intake, administration route, etc., but is usually 0.1 to 4 m.
g / kg body weight / day, preferably 0.2-1 mg / kg body weight / day is used. Administration or ingestion may be carried out once a day, or may be divided into a plurality of doses as needed and used in a predetermined amount.

【0027】本発明の薬剤は、前記した種々の疾患状態
の予防や治療を目的として、好ましくは経口的に投与さ
れる。The drug of the present invention is preferably orally administered for the purpose of preventing or treating the various disease states mentioned above.

【0028】本発明の薬剤の投与に際しては、製剤用と
して当該技術分野において常用され、且つ混合時に有効
成分であるイソフラボン誘導体に対して反応性を呈した
り、それを失活せしめることのない、薬理的に許容しう
る担体を混合し、適宜、投与に適した単位服用形態の組
成物を調製するとよい。When the pharmaceutical agent of the present invention is administered, it is a pharmacological agent which is commonly used in the art as a pharmaceutical agent and which does not show reactivity or deactivate the isoflavone derivative which is an active ingredient when mixed. It is advisable to prepare a unit dosage form composition suitable for administration, by admixing a pharmaceutically acceptable carrier.

【0029】例えば経口投与に好適な剤形として、錠
剤、丸剤、カプセル剤、散剤もしくは顆粒剤等の固形製
剤を調製するためには、カルボキシメチルセルロースカ
ルシウム、ラクトース、グルコース、シュクロース等の
賦形剤、澱粉、アルギン酸ソーダ等の崩壊剤、ステアリ
ン酸マグネシウム、タルク等の滑沢剤、ポリビニルアル
コール、ヒドロキシプロピルセルロース、ゼラチン等の
結合剤、脂肪酸エステル等の表面活性剤、グリセリン等
の可塑剤などが用いられ、常法に従って製剤化される。
これら錠剤、顆粒剤、カプセル剤等は、例えば腸溶性製
剤のように、体内での崩壊、吸収を調節するために適宜
コーティングを施すことも可能である。For example, in order to prepare solid preparations such as tablets, pills, capsules, powders or granules as a dosage form suitable for oral administration, carboxymethylcellulose calcium, lactose, glucose, sucrose, etc. Agents, starch, disintegrators such as sodium alginate, lubricants such as magnesium stearate and talc, binders such as polyvinyl alcohol, hydroxypropyl cellulose and gelatin, surfactants such as fatty acid esters, plasticizers such as glycerin, etc. It is used and formulated according to a conventional method.
These tablets, granules, capsules and the like can be appropriately coated to control disintegration and absorption in the body, such as enteric coated preparations.

【0030】また、経口投与のために、例えば乳濁剤、
溶液剤、懸濁剤、シロップ剤もしくはエリキシル剤とい
った液体製剤を常法に従って製造してもよい。液体製剤
は、用時、水または他の適切な媒体に溶解または懸濁す
る形態としても提供されうる。For oral administration, for example, an emulsion,
Liquid preparations such as solutions, suspensions, syrups or elixirs may be manufactured according to a conventional method. Liquid formulations may also be presented in a form that dissolves or suspends in water or other suitable vehicle before use.

【0031】これらの製剤は、本発明のイソフラボン誘
導体を0.5重量%以上、好ましくは2〜25重量%の割合で
配合したものであるとよい。These preparations may contain the isoflavone derivative of the present invention in an amount of 0.5% by weight or more, preferably 2 to 25% by weight.

【0032】さらに、本発明の薬剤には、治療や予防に
有効であると考えられる他の有効成分が含有されてもよ
い。Further, the drug of the present invention may contain other active ingredients which are considered to be effective for treatment or prevention.

【0033】本発明の、一般式(I)で示されるイソフ
ラボン誘導体を有効成分として含有する、血中脂質濃度
を低減させるために用いられる可食性組成物は、前記有
効成分を、0.001重量%以上、好ましくは0.01〜10重量
%含有するものである。The edible composition containing the isoflavone derivative represented by the general formula (I) as an active ingredient of the present invention, which is used for reducing the lipid level in blood, contains 0.001% by weight or more of the active ingredient. , Preferably 0.01 to 10% by weight.

【0034】可食性組成物の形態としては、例えば、飲
料、菓子、加工食品、調味料等に適した、種々の形態と
することが可能であり、特に限定されるものではない。
可食性組成物とするために、通常使用される賦形剤、増
量剤、安定化剤、乳化剤、甘味剤、香味剤、着色剤及び
発色剤等を、適宜、有効成分に対して好ましくない影響
を及ぼさない限りにおいて配合し、製造すればよい。本
発明を以下の実施例にて更に詳細に説明するが、本発明
がこれら実施例の開示によって限定されるものではない
事はもちろんである。The form of the edible composition can be, for example, various forms suitable for beverages, confectionery, processed foods, seasonings and the like, and is not particularly limited.
Excipients, fillers, stabilizers, stabilizers, emulsifiers, sweeteners, flavors, colorants, colorants, etc., which are commonly used to form an edible composition, are used, as appropriate, against the active ingredients. As long as it does not exceed the range, it may be compounded and manufactured. The present invention will be described in more detail in the following examples, but it goes without saying that the present invention is not limited by the disclosure of these examples.

【0035】[0035]

【実施例】以下の実施例において、一般式(I)で示さ
れるイソフラボン誘導体のうち代表的な化合物である、
7-O-グルコピラノシル-4'-ヒドロキシ-イソフラボン
(すなわちダイズイン(純度99%以上、フジッコ株式会
社製))と、7,4'-ジヒドロキシ-イソフラボン(すなわ
ちダイゼイン(純度97%以上、フジッコ株式会社製))
を用いて、その作用効果を調べた。EXAMPLES In the following examples, typical isoflavone derivatives represented by the general formula (I),
7-O-glucopyranosyl-4'-hydroxy-isoflavone (that is, soybean (purity 99% or more, manufactured by Fujicco Co., Ltd.)) and 7,4'-dihydroxy-isoflavone (that is, daidzein (purity 97% or more, manufactured by Fujicco Co., Ltd.) ))
Was used to examine its action and effect.

【0036】(実施例1)卵巣摘除ラットにおける7-O-
グルコピラノシル-4'-ヒドロキシ-イソフラボンの血清
コレステロール値低下作用 卵巣摘除後7日目の11週齢雌性Sprague-Dawley系ラッ
ト5匹を一群とし、1%ヒドロキシプロピルセルロース
水溶液に懸濁したダイズインを、表1に示す種々の投与
量にて、通常の給水を行いながら4週間にわたり、ゾン
デを用いて連日経口投与した。1晩絶食させた後、各ラ
ットの下大静脈より採血し、血清中の中性脂肪、総コレ
ステロール、HDL−コレステロール及びLDL−コレ
ステロールの各濃度を定量した。対照群は、1%ヒドロ
キシプロピルセルロース水溶液のみを強制経口投与し
た。各脂質濃度の測定結果を表1に示す。(Example 1) 7-O- in ovariectomized rats
Glucopyranosyl-4'-hydroxy-isoflavone serum
Cholesterol level lowering action Five 11-week-old female Sprague-Dawley rats 7 days after ovariectomy were treated as one group, and soybean in suspended in a 1% hydroxypropylcellulose aqueous solution was added at various doses shown in Table 1, Oral administration was carried out daily using a sonde for 4 weeks with normal water supply. After fasting overnight, blood was collected from the inferior vena cava of each rat, and each concentration of serum neutral fat, total cholesterol, HDL-cholesterol and LDL-cholesterol was quantified. In the control group, only 1% hydroxypropylcellulose aqueous solution was forcibly orally administered. The measurement results of each lipid concentration are shown in Table 1.

【0037】[0037]

【表1】 [Table 1]

【0038】表1から明らかように、ダイズインを25mg
/kg/日から75mg/kg/日の範囲で投与することによ
り、用量依存的に血清中の総コレステロール、HDLお
よびLDLコレステロール濃度が低下し、ダイズインが
血清中のコレステロールを低減せしめる効果を有するこ
とが示された。As is clear from Table 1, 25 mg of soybean in
/ Kg / day to 75 mg / kg / day dose-dependently decreases serum total cholesterol, HDL and LDL cholesterol levels, and soyin has the effect of reducing serum cholesterol It has been shown.

【0039】(実施例2)卵巣摘除ラットにおける種々
のイソフラボン誘導体による血清コレステロール値低下
作用 卵巣摘除後7日目の11週齢雌性SpragueーDawley系ラッ
ト5匹を一群として、表2に示す各イソフラボン誘導体
を、各々の投与量にて、実施例1と同様に4週間にわた
り経口投与した後、絶食、採血して、各脂質濃度を定量
した。得られた結果を表2に示す。Example 2 Various in Ovariectomized Rats
Of serum cholesterol levels by isoflavone derivatives
Action On the 7th day after oophorectomy, 5 islets of 11-week-old female Sprague-Dawley rats were treated as a group, and each isoflavone derivative shown in Table 2 was orally administered at each dose for 4 weeks as in Example 1. After that, fasting and blood sampling were performed to quantify each lipid concentration. Table 2 shows the obtained results.

【0040】[0040]

【表2】 [Table 2]

【0041】表2に明らかに示されるように、用いたイ
ソフラボン誘導体はすべて、前記ダイズインと同様に血
清中の総コレステロール、HDLおよびLDLコレステ
ロール濃度の低下作用を有していた。As is clearly shown in Table 2, all of the isoflavone derivatives used had a lowering effect on serum total cholesterol, HDL and LDL cholesterol levels, similar to the above-mentioned soyin.

【0042】上記実施例1及び2から、一般式(I)で
示される化合物のうち代表的な化合物である、7-O-グル
コピラノシル-4'-ヒドロキシイソフラボン(ダイズイ
ン)、7,4'-ジヒドロキシイソフラボン(ダイゼイ
ン)、6"-O-サクシニルダイズイン、6"-O-マロニルダイ
ズイン及び6"-O-アセチルダイズインは、血清コレステ
ロール値の低下作用を有することが認められ、高脂血症
や動脈硬化症等の治療や予防に有効であることが確かめ
られた。From Examples 1 and 2 above, 7-O-glucopyranosyl-4'-hydroxyisoflavone (soybean in) and 7,4'-dihydroxy, which are typical compounds among the compounds represented by the general formula (I), are shown. Isoflavone (Daidzein), 6 "-O-succinyl soybean in, 6" -O-malonyl soybean in and 6 "-O-acetyl soybean in were observed to have a serum cholesterol lowering effect, and hyperlipidemia It was confirmed to be effective for the treatment and prevention of arteries and arteriosclerosis.

【0043】以下に、本発明の薬剤に含有されるイソフ
ラボン誘導体の急性毒性試験及び製剤例を示す。The acute toxicity test and formulation examples of the isoflavone derivative contained in the drug of the present invention are shown below.

【0044】急性毒性試験 5週齢のICR系マウスおよび5週齢のSprague-Dawley
系ラットの雌雄それぞれ10匹づつを一群とし、オリー
ブ油に懸濁したダイズインまたはダイゼインを、各々2,
500、5,000および10,000mg/kgの量で経口投与または、
1,250、2,000および5,000mg/kgの量で皮下投与し、投与
後14日間、観察を継続した。いずれの群においてもダ
イズインまたはダイゼインに起因すると考えられる死亡
例はなく、また中毒症状も認められなかった。従って、
LD50の算出は不可能であった。 Acute toxicity test 5-week-old ICR mice and 5-week-old Sprague-Dawley
Each group consisting of 10 male and 10 female rats was treated with 2, 2, and soybean or daidzein suspended in olive oil.
Orally in doses of 500, 5,000 and 10,000 mg / kg or
The doses of 1,250, 2,000 and 5,000 mg / kg were subcutaneously administered, and the observation was continued for 14 days after the administration. There were no deaths attributed to soybean or daidzein in any group, and no toxic symptoms were observed. Therefore,
The LD 50 could not be calculated.

【0045】製剤例1:本発明のイソフラボン誘導体を
含有する錠剤 以下の表3に記載した各成分を、所定量目ずつ準備し
た。Formulation Example 1: Isoflavone derivative of the present invention
Tablets Contained Each of the components listed in Table 3 below was prepared in predetermined amounts.

【0046】[0046]

【表3】 [Table 3]

【0047】各成分を、それぞれ60〜120メッシュ
の篩で分級し、次いで、V型混合機で一括して混合し
た。これを、直接打錠機(TG2S:エルエーカ社製)
で錠剤に成形し、直径8.5mmの普通面の素錠100
0個を製造した。Each component was classified with a sieve of 60 to 120 mesh and then mixed together by a V-type mixer. This is a direct compression machine (TG2S: manufactured by El Aka Co.)
To form a tablet with a plain surface plain tablet with a diameter of 8.5 mm 100
0 were produced.

【0048】製剤例2:本発明のイソフラボン誘導体を
含有するカプセル剤 下記表4に記載した各成分を、所定量目ずつ準備した。Formulation Example 2: The isoflavone derivative of the present invention
Capsules contained Each of the components shown in Table 4 below was prepared in predetermined amounts.

【0049】[0049]

【表4】 [Table 4]

【0050】各成分を、それぞれ60メッシュの篩で分
級し、次いで、V型混合機で一括して混合した。これを
1号カプセル1000錠に充填してカプセル剤とした。Each component was classified with a 60-mesh sieve, and then mixed together by a V-type mixer. This was filled in 1000 capsules of No. 1 capsule to prepare a capsule.

【0051】次に、本発明のイソフラボン誘導体を含有
する可食性組成物の調製例を示す。Next, a preparation example of an edible composition containing the isoflavone derivative of the present invention is shown.

【0052】調製例1:本発明のイソフラボン誘導体を
含有する飲料の調製 下記表5に記載した各材料を、所定量ずつ準備した。Preparation Example 1: The isoflavone derivative of the present invention
Preparation of Beverage Containing Each of the ingredients shown in Table 5 below was prepared in predetermined amounts.

【0053】[0053]

【表5】 [Table 5]

【0054】次に、水にダイズインを加えて懸濁させ、
その後、得られた液体に残りの材料を混合した後、12
2〜138℃で1秒間、瞬間殺菌して、180 ml容のガラ
ス瓶に充填した。Next, soybean in was added to water and suspended,
Then, after mixing the remaining ingredients with the obtained liquid,
It was instantly sterilized at 2 to 138 ° C. for 1 second and filled in a 180 ml glass bottle.

【0055】このようにして調製した飲料は、渋味や収
斂味が無く、また、果汁本来の風味が損なわれておらず
非常に美味であって、果汁入り清涼飲料として嗜好性及
び食品衛生上満足できるものであった。The beverage prepared in this manner has no astringency or astringent taste and is very delicious without impairing the original flavor of the fruit juice. It was satisfying.

【0056】調製例2:本発明のイソフラボン誘導体を
含有するゼリーの調製 まず、下記表6に示した材料を、所定量目ずつ準備し
た。Preparation Example 2: Isoflavone derivative of the present invention
Preparation of Containing Jelly First, the materials shown in Table 6 below were prepared in predetermined amounts.

【0057】[0057]

【表6】 [Table 6]

【0058】次に、水にダイゼインを加えて分散させ、
得られた液体に、果汁、水飴及び香料を添加混合し、別
途寒天とグラニュー糖を混合して混合液に添加した。Next, daidzein was added to water and dispersed,
To the obtained liquid, fruit juice, starch syrup and fragrance were added and mixed, and agar and granulated sugar were separately mixed and added to the mixed liquid.

【0059】これらをよくかき混ぜながら、約90℃ま
で加熱し、寒天を溶かした。この溶融物を50ml用の
プラスティックのカップに分注した後、カップの上面を
プラスティックフィルムでシールし、5〜10℃で冷却
して凝固させ、ゼリーを得た。While stirring well, these were heated to about 90 ° C. to melt the agar. After this melt was dispensed into a plastic cup for 50 ml, the upper surface of the cup was sealed with a plastic film and cooled at 5 to 10 ° C. to solidify to obtain a jelly.

【0060】このようにして調製したゼリーは、非常に
美味であり、「デザート」として優れた品質を有するも
のであった。The jelly thus prepared was very delicious and had an excellent quality as a "dessert".

【0061】[0061]

【発明の効果】本発明によれば、血中脂質濃度を低減さ
せることによって、高脂血症、特に高コレステロール血
症や、動脈硬化症等の予防及び治療に有効な薬剤及び可
食性組成物が提供される。INDUSTRIAL APPLICABILITY According to the present invention, a drug and an edible composition effective for the prevention and treatment of hyperlipidemia, particularly hypercholesterolemia, arteriosclerosis, etc. by reducing blood lipid concentration Will be provided.

【0062】また、本発明の薬剤及び可食性組成物の有
効成分である、一般式(I)で示されるイソフラボン誘
導体は、安全性という面においても、味や臭い等の食品
成分に要求される嗜好的な面においても優れているの
で、任意に様々な態様によって摂取・投与されうるとい
う利点を有するものである。Further, the isoflavone derivative represented by the general formula (I), which is an active ingredient of the medicine and the edible composition of the present invention, is required for food ingredients such as taste and odor also in terms of safety. Since it is also excellent in palatability, it has an advantage that it can be ingested / administered in various modes.

───────────────────────────────────────────────────── フロントページの続き (51)Int.Cl.6 識別記号 庁内整理番号 FI 技術表示箇所 // C07D 311/36 C07H 17/07 C07H 17/07 A23L 2/26 2/00 F (72)発明者 石田 均司 静岡県静岡市瀬名3107−2 (72)発明者 辻 邦郎 静岡県静岡市池田1375−11─────────────────────────────────────────────────── ─── Continuation of the front page (51) Int.Cl. 6 Identification code Internal reference number FI Technical display location // C07D 311/36 C07H 17/07 C07H 17/07 A23L 2/26 2/00 F (72) Inventor Hitoshi Ishida 3107-2 Sena, Shizuoka City, Shizuoka Prefecture (72) Inventor Kunio Tsuji 1375-11 Ikeda, Shizuoka City, Shizuoka Prefecture

Claims (4)

【特許請求の範囲】[Claims] 【請求項1】 一般式(I) 【化1】 [式中、R1は、HまたはOHを表し、R2は、OH、O-
グルコシド基、O-(6"-O-サクシニル)グルコシド基、O-
(6"-O-マロニル)グルコシド基または、O-(6"-O-アセチ
ル)グルコシド基を表す]で示されるイソフラボン誘導
体を有効成分として含有することを特徴とする、血中脂
質濃度を低減させる薬剤。1. A compound of the general formula (I) [In the formula, R 1 represents H or OH, and R 2 represents OH, O-
Glucoside group, O- (6 "-O-succinyl) glucoside group, O-
(6 "-O-malonyl) glucoside group or O- (6" -O-acetyl) glucoside group] is included as an active ingredient to reduce blood lipid concentration. Drugs that make you. 【請求項2】 前記イソフラボン誘導体が、ダイゼイ
ン、ダイズイン、6"-O-サクシニルダイズイン、6"-O-マ
ロニルダイズインまたは6"-O-アセチルダイズインであ
る、請求項1記載の薬剤。2. The drug according to claim 1, wherein the isoflavone derivative is daidzein, soybean in, 6 "-O-succinyl soybean, 6" -O-malonyl soybean or 6 "-O-acetyl soybean. 【請求項3】 一般式(I) 【化2】 [式中、R1は、HまたはOHを表し、R2は、OH、O-
グルコシド基、O-(6"-O-サクシニル)グルコシド基、O-
(6"-O-マロニル)グルコシド基または、O-(6"-O-アセチ
ル)グルコシド基を表す]で示されるイソフラボン誘導
体を有効成分として含有することを特徴とする、血中脂
質濃度を低減させるために用いられる可食性組成物。3. A compound of the general formula (I) [In the formula, R 1 represents H or OH, and R 2 represents OH, O-
Glucoside group, O- (6 "-O-succinyl) glucoside group, O-
(6 "-O-malonyl) glucoside group or O- (6" -O-acetyl) glucoside group] is included as an active ingredient to reduce blood lipid concentration. An edible composition used for producing. 【請求項4】 前記イソフラボン誘導体が、ダイゼイ
ン、ダイズイン、6"-O-サクシニルダイズイン、6"-O-マ
ロニルダイズインまたは6"-O-アセチルダイズインであ
る、請求項3記載の可食性組成物。4. The edible food according to claim 3, wherein the isoflavone derivative is daidzein, soybean in, 6 "-O-succinyl soybean, 6" -O-malonyl soybean or 6 "-O-acetyl soybean. Composition.
JP8064368A 1996-03-21 1996-03-21 Medicine and edible composition for lowering concentration of lipid in blood Pending JPH09255570A (en)

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